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le 01/09/00  |
Biliary Tract
Carcinoembryonic antigen-related cell adhesion molecule 1 is
the 85-kilodalton pronase-resistant biliary glycoprotein in the
cholesterol crystallization promoting low density protein-lipid
complex (*Human Study*)
Milan Jirsa, Lucie Muchová, Lubica Dráberová,
Petr Dráber, Frantisek Smíd, Masahide Kuroki, Zdenk
Mareek, Albert K. Groen
A pronase resistant 85-kd glycoprotein in the Concanavalin Abinding
fraction (CABF) of biliary glycoproteins has been reported to
act as a promotor of cholesterol crystallization. De Bruijn et
al. (Gastroenterology 1996;110:1936-1944) found this protein in
a low-density protein-lipid complex (LDP) with potent cholesterol
crystallization promoting activity. This study identifies and
characterizes this protein. An LDP was prepared from CABF by discontinuous
gradient ultracentrifugation. Proteins were analyzed by sodium
dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE),
blotting and immunochemical staining with anti-carcinoembryonic
antigen, CEA-related adhesion molecule 1 (CEACAM1) cross-reacting
antibodies. Biliary concentrations of CEA cross-reacting proteins
were determined in patients with and without gallstones. Two isoforms
of CEACAM1 (85- and 115-kd bands), CEA and 2 CEA cross-reacting
protein bands of 40 and 50 kd were found in human bile. All bands
were also present in CABF, but only a subfraction of the 85-kd
band found in the LDP was resistant to digestion with pronase.
CEACAM1-85 exhibited potent cholesterol crystallization promoting
activity in vitro and accounted for most of the activity
in CABF. Total CEA cross-reacting protein concentrations were
the same in gallbladder biles from patients with cholesterol and
pigment gallstones but only half of those in biles from nongallstone
subjects. In conclusion, we have identified the protein component
of the cholesterol crystallization promoting LDP to be CEACAM1-85.
(HEPATOLOGY 2001;34:1075-1082.)
Chronic Liver Disease
The geographical distribution of primary biliary cirrhosis
in a well-defined cohort (*Human Study*)
Martin I. Prince, Amanda Chetwynd, Peter Diggle, Mikala Jarner,
Jane V. Metcalf, Oliver F. W. James
The incidence of primary biliary cirrhosis (PBC) varies widely
between regions. However, little is known about variation within
regions and the degree to which this may reflect environmental
risk factors. The aim of this study was to describe the spatial
distribution of cases of PBC in a defined region of Northeast
England over a defined period, and to assess the magnitude of
any departure from random spatial distribution. Seven hundred
seventy patients with established PBC were identified in a previous
comprehensive case finding study. A total of 3,044 control locations
were randomly selected from postcode (zip code) data weighted
for number of drop off points per postcode. Geographical analysis
was performed by testing both for spatial variation in risk and
local clustering by using previously described point process methods.
Both tests used the same null hypothesis that risk of disease
does not vary spatially and cases occur independently of each
other. Statistically significant spatial variations in risk were
found in the whole study region (P < .001) and in the
major urban area within the region (P < .004). Risk
was higher in the urban area of Tyneside than in the surrounding
rural area. Within the rural area, spatial variation in risk was
equivocal (P = .012), but there was significant (P
= .001) clustering of cases (estimated average cluster effect
approximately 10 excess cases within a 7-km radius). PBC occurred
to a density of 10.7 cases/km2 in the highest risk areas. In conclusion,
PBC is unevenly distributed in Northeast England. This may reflect
one or more environmental risk factors in its etiology. (HEPATOLOGY
2001;34:1083-1088.)
Impact of gastroenterology consultation on the outcomes of
patients admitted to the hospital with decompensated cirrhosis
(*Human Study*)
Edmund J. Bini, Elizabeth H. Weinshel, Ramon Generoso, Loay Salman,
Georges Dahr, Ivan Pena-Sing, Thomas Komorowski
Managed care has strongly discouraged generalists from referring
patients to specialists in an effort to reduce the costs of health
care. The aim of this study was to compare patient outcomes when
generalists work together with gastroenterologists or alone in
the management of patients admitted to the hospital with decompensated
cirrhosis. Consecutive patients admitted to the hospital with
decompensated cirrhosis over a 1-year period were identified.
We compared the length of stay, cost of hospitalization, incidence
of hospital readmission, and mortality for patients who did and
those who did not have a gastroenterology (GI) consultation. A
GI consultation was requested for 107 of the 197 patients (54.3%).
Patients who had a GI consultation had a significantly shorter
length of stay (5.6 ± 3.5 vs. 10.1 ± 5.8 days, P
< .001) and a lower cost of hospitalization ($6,004 ±
$4,994 vs. $10,006 ± $6,183, P < .001) than those
patients who were managed by generalists alone. The 30-day incidence
of readmission (13.3% vs. 27.8%, P = .01) and mortality
(7.5% vs. 16.7%, P = .045) were significantly lower in
the GI consultation group. During a median follow-up of 618 days
(range, 2-970), patients who had a GI consultation during hospitalization
had a significantly longer time to hospital readmission (P
< .001) and improved survival (P = .02) compared with
those who were managed by generalists alone. In conclusion, for
patients admitted to the hospital with decompensated cirrhosis,
individuals who were managed by generalists in conjunction with
gastroenterologists had better outcomes than those who were managed
by generalists alone. (HEPATOLOGY 2001;34:1089-1095.)
Propranolol for the prevention of first esophageal variceal
hemorrhage: A lifetime commitment? (*Human Study*)
Diane R. Abraczinskas, Rie Ookubo, Norman D. Grace, Roberto J.
Groszmann, Jaime Bosch, Guadalupe Garcia-Tsao, Caroline R. Richardson,
Daniel S. Matloff, Juan Rodés, Harold O. Conn
Although blockers have had significant impact in the treatment
of portal hypertension, the question of how long they should be
continued for prevention of variceal hemorrhage remains unknown.
Prospective studies on blockers to prevent variceal hemorrhage
lack long-term follow-up, and indefinite administration of blockers
for primary prevention of variceal bleeding has become standard
practice. The aim of this study was to determine the outcomes
of patients in whom blocker therapy was discontinued. Patients
completing a prospective, randomized, double-blind, placebo-controlled
trial of propranolol for the primary prevention of variceal hemorrhage
were tapered off of propranolol and placebo and followed prospectively
for subsequent events. Of the 49 patients in the follow-up study
(25 former propranolol, 24 former placebo), 9 experienced variceal
hemorrhage (6 former propranolol, 3 former placebo). Following
withdrawal of propranolol, the freedom from variceal bleeding
was not significantly different between these 2 groups of patients,
suggesting that the protective effect of propranolol against variceal
hemorrhage, noted previously, was no longer present. Seventeen
patients died (12 former propranolol, 5 former placebo) during
the follow-up study. Cumulative survival was longer in the placebo
group. These trends for EVH and survival were opposite to those
observed in the original study population while patients were
taking medication. When propranolol is withdrawn, the risk of
variceal hemorrhage returns to what would be expected in an untreated
population. Patients who discontinue blockers experience increased
mortality compared with an untreated population. These observations
support the current practice of indefinite prophylactic therapy.
(HEPATOLOGY 2001;34:1096-1102.)
Hepatic and intestinal cytochrome P450 3A activity in cirrhosis:
Effects of transjugular intrahepatic portosystemic shunts (*Human
Study*)
Naga Chalasani, J. Christopher Gorski, Nilesh H. Patel, Stephen
D. Hall, Raymond E. Galinsky
Transjugular intrahepatic portosystemic shunt (TIPS) is performed
to treat some complications of cirrhosis. This study investigated
the effects of cirrhosis and TIPS on intestinal and hepatic cytochrome
P450 3A (CYP3A) activity. Nine volunteers were cirrhotic patients
with TIPS, 9 were cirrhotic controls (matched for sex, age, etiology,
and Child-Pugh class), and 9 were sex- and age-matched healthy
volunteers. Simultaneous doses of midazolam were given intravenously
(0.05 mg/kg) and orally (3 mg of [15N3]midazolam). Peripheral
and portal venous blood samples were assayed for midazolam and
[15N3]midazolam. The systemic clearance of midazolam was significantly
greater (P < .05) in healthy volunteers (0.42 ±
0.10 L · h1 · kg1) compared with cirrhotic
controls (0.20 ± 0.05) and with cirrhotic patients with
TIPS (0.21 ± 0.09). Hepatic availability followed the same
trend. The bioavailability of midazolam was significantly higher
(P < .05) in cirrhotic patients with TIPS (0.76 ±
0.20) compared with cirrhotic controls (0.27 ± 0.14) and
with healthy volunteers (0.30 ± 0.10). The intestinal availability
was significantly greater (P < .05) in cirrhotic patients
with TIPS (0.83 ± 0.17) compared with cirrhotic controls
(0.32 ± 0.16) and with healthy volunteers (0.42±0.15).
As expected, hepatic CYP3A activity was reduced in cirrhosis.
However, in cirrhotic patients with TIPS, there was a marked loss
in first-pass metabolism of midazolam as a result of diminished
intestinal CYP3A activity. (HEPATOLOGY 2001;34:1103-1108.)
Contrast-enhanced doppler ultrasonography in the diagnosis
of hepatocellular carcinoma and premalignant lesions in patients
with cirrhosis (*Human Study*)
Anna Ludovica Fracanzani, Larry Burdick, Mauro Borzio, Massimo
Roncalli, Nicola Bonelli, Franco Borzio, Alessandra Maraschi,
Gemino Fiorelli, Silvia Fargion
Hepatocellular carcinogenesis in cirrhosis is a multistage process
that includes large regenerative nodules, dysplastic nodules,
and hepatocarcinoma. The aim of this study was to establish whether
contrast-enhanced Doppler ultrasonography (US) is able to distinguish
between early hepatocellular carcinoma (HCC) and small nonmalignant
nodules in cirrhosis. Between January 1998 and December 1999,
500 cirrhotic patients with no previous history of HCC or evidence
of hepatic focal lesions were enrolled and prospectively followed-up
with US every 6 months until December 2000. Sixty-one patients
developed focal lesions, 12 multifocal, and 49 monofocal. Biopsy
of focal lesions, contrast-enhanced Doppler US, and spiral computed
tomography (CT) were performed in 41 consecutive patients with
small (<3 cm) monofocal lesions. Twenty nodules were diagnosed
as HCC and 21 as nonmalignant (14 large regenerative nodules,
3 low-grade, and 4 high-grade dysplastic nodules) by liver biopsy.
Intratumoral arterial blood flow was detected in 19 of 20 (95%)
HCC and 6 of 21 (28%) nonmalignant nodules by contrast-enhanced
Doppler US (P<.0001). The mean peak resistance and pulsatility
indices were 0.82 ± 0.09 and 1.56 ± 0.2 in HCC and
0.62 ± 0.08 and 0.82 ± 0.08 in dysplastic lesions
(P = .002 and .0001), respectively. Spiral CT revealed
arterial perfusion in 19 of 20 HCC and in 4 of 21 nonmalignant
nodules (high-grade dysplastic nodules). Four of the apparently
false-positive nodules at enhanced Doppler US were high-grade
dysplastic nodules and 2 evolved to HCC during follow-up. In conclusion,
contrast-enhanced Doppler US is a noninvasive, very sensitive
technique in differentiating malignant and premalignant lesions
from nonmalignant focal lesions in the liver. (HEPATOLOGY 2001;34:1109-1112.)
Patterns of regional sympathetic nerve traffic in preascitic
and ascitic cirrhosis (*Human Study*)
Massimo Pozzi, Guido Grassi, Elena Redaelli, Raffaella Dell'Oro,
Laura Ratti, Alessandro Redaelli, Gerardo Foglia, Alessandro Di
Lelio, Giuseppe Mancia
Overactivity of the sympathetic nervous system and portal hypertension
are key factors in the development of ascites in cirrhosis. The
sympathoexcitation that characterizes the more advanced stages
of liver diseases is less clearly defined in preascitic cirrhosis.
We measured sympathetic nerve traffic to skeletal muscle (peroneal
nerve) and to skin districts by microneurography in (1) 12 Child
class A cirrhotic patients with clinically significant portal
hypertension (portal pressure gradient > 10 mm Hg, 14.8 ±
1.2 mm Hg, mean ± SEM) but without actual or previous ascites,
(2) 16 Child class C cirrhotic patients with tense ascites, and
(3) 10 patients with mild congestive heart failure, a condition
paradigmatic of a marked sympathetic activation. Muscle sympathetic
nerve traffic was markedly increased in Child class C subjects
as compared with controls (23.9 ± 1.6 bursts/min, P
< .01) and superimposable to that recorded in heart failure
patients (52.9 ± 4.7 vs. 60.3 ± 2 bursts/min, P
= not significant). Muscle sympathetic nerve traffic was also
increased in Child class A subjects (41.6 ± 2 bursts/min,
P < .01 vs. controls) although to a lesser extent (P
< .05 vs. Child class C patients). Skin sympathetic nerve traffic
was within the normal range in all patients. Neurohormones were
all markedly increased in Child class C subjects. Only norepinephrine
was increased in Child class A patients. Our data show that sympathetic
nerve traffic activation (1) is already detectable in Child class
A cirrhosis when clinically significant portal hypertension is
present but ascites never developed and (2) is not generalized
because although muscle traffic is increased, skin traffic is
within normal range. The role of drugs modulating sympathoactivation
should be investigated in preascitic cirrhosis. (HEPATOLOGY 2001;34:1113-1118.)
Growth Regulation and Cancer
Activation of caspase-8 during N-(4-hydroxyphenyl)retinamideinduced
apoptosis in FAS-defective hepatoma cells
Kyung-Ran You, Myung-Nym Shin, Rae-Kil Park, Seung-Ok Lee, Dae-Ghon
Kim
We observed that N-(4-hydroxyphenyl)retinamide (4HPR),
a chemopreventive and chemotherapeutic agent, effectively induced
apoptosis in hepatoma cells. Interestingly, Fas-negative (Hep
3B and PLC/PRF/5) hepatoma cells were shown to be more susceptible
to apoptosis induced by 4HPR than were Fas-positive (Hep G2 and
SK-HEP-1) hepatoma cells. Thus, we explored the mechanisms underlying
4HPR-induced apoptosis in Fas-defective hepatoma cells. Hep 3B
cells stably expressing the dominant-negative Fas-associated death
domain (dnFADD) showed no alteration in 4HPR drug susceptibility,
but when stably expressing E1B19K, Crm A, or dominant-negative
FLICE (dnFLICE), Hep 3B cells were resistant, suggesting that
4HPR-induced apoptosis was mediated by caspase-8 activation. Furthermore,
apoptosis could be completely blocked by Z-VAD-FMK (a general
caspase inhibitor) or by IETD-CHO (a caspase-8 inhibitor), but
was only partially blocked by Ac-DEVD-CMK (a caspase-3 inhibitor),
by N-acetyl-L-cysteine (NAC) (an antioxidant), by N-acetyl-leucyl-leucyl-norleucinal
(ALLN) (a calpain inhibitor I), or by Z-LEHD-FMK (a caspase-9
inhibitor). Time-sequence analysis of the induction of apoptosis
by 4HPR revealed that an initial caspase-8 activation was followed
by late mitochondrial cytochrome c release and minor caspase-9
activation, which suggested that caspase-8 activation is the primary
upstream regulatory point. Activation of Bid or induction of proapoptotic
Bax was not observed during apoptosis. In contrast, Bcl-xL expression
was decreased during 4HPR-induced apoptosis. Taken together, these
results indicate that 4HPR may be a potential chemotherapeutic
drug, which is able to induce apoptosis in Fas-defective hepatoma
cells through caspase-8 activation. (HEPATOLOGY 2001;34:1119-1127.)
Immunohistologic study on the expressions of -fetoprotein and
protein induced by vitamin K absence or antagonist II in surgically
resected small hepatocellular carcinoma (*Human Study*)
Miwako Fujioka, Yutaka Nakashima, Osamu Nakashima, Masamichi Kojiro
Sixty-eight cases of single hepatocellular carcinoma (HCC) with
less than 3 cm of diameter were immunohistochemically examined
for the expressions of -fetoprotein (AFP) and protein induced
by vitamin K absence or antagonist II (PIVKA-II). In cancerous
tissues, the expression rate was significantly higher for PIVKA-II
(34 cases [50%]) than AFP (21 cases [31%]) (P < .05),
suggesting a higher specificity of PIVKA-II to small HCC. Sixteen
of the 68 cases (24%) were positive to both AFP and PIVKA-II,
and in 8 of the 16 cases, AFP and PIVKA-II expressing areas within
a nodule were clearly divided by a fibrous septum. According to
histologic grades, PIVKA-II expression was confirmed in 2 of the
15 well-differentiated HCCs, and in the well-differentiated component
of 6 of the 12 "nodule-in-nodule"type well-differentiated
HCCs. AFP expression was not found in well-differentiated HCCs,
but found in 16 of the 40 moderately differentiated HCCs (40%)
and in the moderately differentiated component of 3 of the 12
"nodule-in-nodule"type well-differentiated HCCs.
The positive rate in the tissues was correlated to the serum levels
for both AFP and PIVKA-II. In addition, frequency of tissuePIVKA-II
expression was higher than tissue-AFP expression in the cases
whose serum protein level was within the normal range. This indicates
that AFP and PIVKA-II have different patterns of tissue expression
and of secretion to the blood. In comparison with tissue-AFPnegative
cases, tissue-AFPpositive HCCs had a larger tumor size, higher
frequencies of portal vein invasion and intrahepatic metastasis,
a high Ki-67 labeling index, and a lower rate of recurrence-free
survival. Thus, tissue-AFPpositive HCCs are suggested to
be biologically more malignant than those HCCs that are AFP-negative
and PIVKA-IIpositive. (HEPATOLOGY 2001;34:1128-1134.)
Spatiotemporal expression of angiogenesis growth factor receptors
during the revascularization of regenerating rat liver
Mark A. Ross, Christina M. Sander, Talia B. Kleeb, Simon C. Watkins,
Donna Beer Stolz
Regenerating liver was evaluated for the spatiotemporal expression
of angiogenic growth factor receptors on endothelial cell (EC)
membranes during revascularization resulting from 70% partial
hepatectomy (PHx). Fractions enriched in EC membranes were examined
by Western blot for angiogenic growth factor receptor expression
from 1 to 14 days after PHx. Increases in vascular endothelial
growth factor (VEGF) receptors Flt-1 and Flk-1/KDR, angiopoietin
receptors Tie-1, Tie-2, and platelet-derived growth factor receptor
beta (PDGF-R), modest increases in epidermal growth factor receptor
(EGF-R), and no increase in hepatocyte growth factor receptor
(c-Met) or fibroblast growth factor receptors (FGF-R) were observed
in isolated membranes during EC proliferation. All receptors were
tyrosine phosphorylated, and therefore activated, during peak
expression. Immunofluorescence staining of regenerating liver
identified populations with increased receptor expression, indicating
cells receptive to ligand signaling. EGF-R was upregulated evenly
throughout the sinusoidal membrane, whereas c-Met was observed
on hepatocyte canaliculae, bile duct epithelium, and large vessel
EC. Tie-2 and PDGF-R were increased on sinusoidal and large vessel
EC, whereas Tie-1 was expressed in EC surrounding avascular hepatic
islands. Flk-1/KDR was increased on large vessels with slight
increases on sinusoidal EC, whereas Flt-1 was increased in arterioles,
sinusoidal EC as well as in hepatocytes. Although Flt-1 was phosphorylated
on isolated hepatocytes, vascular endothelial growth factor165
(VEGF165) did not induce a proliferative or motogenic response.
Proliferation assays on isolated EC indicated responsiveness to
VEGF165, but synergism among several growth factors including
PDGF-BB was also observed. The data identify novel autocrine and
paracrine interactions and indicate that each growth factor acts
on a specific set of EC at specific times during revascularization
of regenerating liver. (HEPATOLOGY 2001;34:1135-1148.)
Inflammation, Cytokines, and Fibrosis
Delivery of IB superrepressor gene with adenovirus reduces
early alcohol-induced liver injury in rats
Takehiko Uesugi, Matthias Froh, Gavin E. Arteel, Blair U. Bradford,
Erwin Gäbele, Michael D. Wheeler, Ronald G. Thurman
Chronic alcohol administration increases gut-derived endotoxin
in the portal blood, which activates Kupffer cells through nuclear
factor B (NF-B) to produce toxic mediators such as proinflammatory
cytokines, leading to liver injury. Therefore, a long-term intragastric
ethanol feeding protocol was used here to test the hypothesis
that NF-B inhibition would prevent early alcohol-induced liver
injury. Adenoviral vectors encoding either the transgene for IB
superrepressor (AdIB-SR) or the bacterial -galactosidase reporter
gene (AdlacZ) were administered intravenously to Wistar rats.
Animals were fed a high-fat liquid diet with either ethanol or
isocaloric maltose-dextrin (control) for 3 weeks. There was no
significant difference in mean urine alcohol concentrations between
the groups fed ethanol. IB-SR expression was increased for up
to 2 weeks after injection, but was undetectable at 3 weeks. NF-B
activation was increased by ethanol and associated with up-regulation
of tumor necrosis factor (TNF-). These increases were blunted
significantly up to 2 weeks by AdIB-SR. Dietary alcohol significantly
increased liver to body weight ratios and serum alanine transaminase
(ALT) levels in AdlacZ-treated animals, effects that were blunted
significantly in AdIB-SRtreated rats. Ethanol caused severe
steatosis, inflammation, and focal necrosis in AdlacZ-treated
animals. These pathologic changes were significantly decreased
by AdIB-SR. The protective effects of IB-SR were significant 2
weeks after injection, but were lost at 3 weeks when IB-SR was
no longer expressed. Ethanol increased 4-hydroxynonenal as a maker
of oxidative stress in both AdlacZ and AdIB groups. These data
support the hypothesis that NF-B inhibition prevents early alcohol-induced
liver injury even in the presence of oxidative stress. (HEPATOLOGY
2001;34:1149-1157.)
Gene expression of tumor necrosis factor and TNF-receptors,
p55 and p75, in nonalcoholic steatohepatitis patients (*Human
Study*)
Javier Crespo, Amalía Cayón, Pedro Fernández-Gil,
Manuel Hernández-Guerra, Marta Mayorga, Agustín
Domínguez-Díez, José Carlos Fernández-Escalante,
Fernando Pons-Romero
The main objective of this study was to analyze the pathogenic
role of the tumor necrosis factor (TNF-) system in the development
of nonalcoholic steatohepatitis (NASH). Fifty-two obese patients
were studied. We investigated: (1) the expression of mRNA of TNF-
and their p55 and p75-receptors by quantitative reverse-transcriptase
polymerase chain reaction (RT-PCR) in hepatic and adipose tissues;
and (2) the relationship between TNF-, p55, and p75 and the severity
of NASH. Obese patients without NASH were the control group. A
remarkable increase in the expression of mRNA of TNF- was found
in patients with NASH in hepatic tissue (0.65 ± 0.54) and
in peripheral fat (0.43 ± 0.45); in the control samples,
the mRNA expression was 0.28 ± 0.32, P < .007,
and 0.26 ± 0.22, P < .018, respectively. Furthermore,
we found a significant increase in the mRNA levels of p55 receptor
(2.42 ± 1.81 vs. 1.56 ± 1.17; P < .05);
however, the mRNA expression of the p75 receptor was similar in
both patients. Those patients with NASH with significant fibrosis
presented an increase in the expression of mRNA TNF- in comparison
with those with a slight or nonexistent fibrosis. An overexpression
of TNF- mRNA is found in the liver and in the adipose tissue of
NASH patients. The levels of mRNA-p55 are increased in the liver
tissue of NASH patients. This overexpression is more elevated
in patients with more advanced NASH. These findings suggest that
the TNF- system may be involved in the pathogenesis of NASH. (HEPATOLOGY
2001;34:1158-1163.)
Liver Cell Injury and Apoptosis
Adenosine monophosphateactivated protein kinase mediates
the protective effects of ischemic preconditioning on hepatic
ischemia-reperfusion injury in the rat
Carmen Peralta, Ramón Bartrons, Anna Serafin, Cristina
Blázguez, Manuel Guzmán, Neus Prats, Carme Xaus,
Blanca Cutillas, Emilio Gelpí, Joan Roselló-Catafau
Hepatic ischemia-reperfusion (I/R) injury associated with liver
transplantation and hepatic resections are an unresolved problem
in the clinical practice. Preconditioning is known to preserve
energy metabolism in liver during sustained ischemia, but the
molecular mechanisms underlying this effect are still unclear.
Different metabolic signals, including adenosine monophosphate
(AMP) and nitric oxide (NO), have been implicated in preconditioning.
AMP-activated protein kinase (AMPK) protects cells by acting as
a low-fuel warning system, becoming switched on by adenosine triphosphate
(ATP) depletion. NO synthesis is induced by AMPK in the heart
during ischemia. The aim of this study was to investigate: 1)
whether preconditioning induces AMPK activation; and 2) if AMPK
activation leads to ATP preservation and reduced lactate accumulation
during prolonged ischemia and its relationship with NO. Preconditioning
activated AMPK and concomitantly reduced ATP degradation, lactate
accumulation, and hepatic injury. The administration of an AMPK
activator, AICAR, before ischemia simulated the benefits of preconditioning
on energy metabolism and hepatic injury. The inhibition of AMPK
abolished the protective effects of preconditioning. The effect
of AMPK on energy metabolism was independent of NO because the
inhibition of NO synthesis in the preconditioned group and the
administration of the NO donor before ischemia, or to the preconditioned
group with previous inhibition of AMPK, had no effect on energy
metabolism. Both preconditioning and AICAR pretreatment, through
AMPK activation, may be useful surgical and pharmacologic strategies
aimed at reducing hepatic I/R injury. (HEPATOLOGY 2001;34:1164-1173.)
Disturbances in hepatic cell-cycle regulation in mice with
assembly-deficient keratins 8/18
Diana M. Toivola, Mikko I. Nieminen, Michael Hesse, Tao He, Hélène
Baribault, Thomas M. Magin, M. Bishr Omary, John E. Eriksson
Simple epithelial tissues such as liver and pancreas express keratins
8 (K8) and 18 (K18) as their major intermediate filament proteins.
K8 and K18 null mice and transgenic mice that express mutant K18
(K18C) manifest several hepatocyte abnormalities and demonstrate
that K8/18 are important in maintaining liver tissue and cell
integrity, although other potential functions remain uncharacterized.
Here, we report an additional abnormal liver phenotype, which
is similar in K8 null, K18 null, and K18C mouse models. Liver
histologic examination showed large polynuclear areas that lacked
cell membranes, desmosomal structures, and filamentous actin.
Similar, but less prominent, areas were observed in the pancreas.
The parenchyma outside the polynuclear areas displayed irregular
sinusoidal structures and markedly enlarged nuclei. Most K8 null
hepatocytes were positive for the proliferating cell nuclear antigen
(PCNA) with a doubled DNA content in comparison with the predominantly
PCNA-negative wild-type hepatocytes. The distribution of the 14-3-3
protein was also altered in K8 null mice. Taken together, our
results indicate that absence of keratin filaments causes disturbances
in cell-cycle regulation, driving cells into the S-G2 phase and
causing aberrant cytokinesis. These effects could stem from disturbed
functions of K8/18-dependent cell-cycle regulators, such as the
signaling integrator, 14-3-3. (HEPATOLOGY 2001;34:1174-1183.)
Molecular Cell Biology
Notch receptor expression in adult human liver: A possible
role in bile duct formation and hepatic neovascularization (*Human
Study*)
Sarbjit S. Nijjar, Heather A. Crosby, Lorraine Wallace, Stefan
G. Hubscher, Alastair J. Strain
Notch signaling is an evolutionarily conserved mechanism, used
to regulate cell fate decisions. Four Notch receptors have been
identified in man (Notch-1 to -4). In this study, semiquantitative
reverse transcription polymerase chain reaction (RT-PCR) and immunohistochemistry
were used to examine the expression pattern of Notch receptor
genes in whole adult human liver and isolated liver cell preparations.
All 4 receptors were expressed in the adult liver, with no significant
differences in the levels of Notch-1, -2, and -4 messenger RNA
(mRNA) between normal and diseased liver. However, Notch-3 expression
appeared to be increased in diseased tissue. The distribution
of Notch-1 and -4 in normal tissue was similar, with Notch-1 also
detectable at low levels in the sinusoidal endothelium. Notch-2
expression was more widely distributed, and detectable in hepatocytes,
medium-sized bile ducts, and the sinusoidal endothelium. Notch-3
expression was seen on hepatocytes, with weaker expression detectable
in portal veins, hepatic arteries, and the sinusoids. In normal
liver tissue Notch-1, -2, and -3 were found to be coexpressed
on bile duct epithelium; however, with the exception of Notch-3
in primary sclerosing cholangitis (PSC) livers, expression was
absent on proliferating ductules in all disease states examined.
Interestingly, the expression of Notch-2 and -3 was associated
with numerous small vessels within the portal tract septa of diseased
tissue. The absence of Notch receptor expression on proliferating
bile ductules and its presence on neovessels suggests that Notch
signaling may be important for normal bile duct formation and
the aberrant neovascularization seen in diseased liver tissue.
(HEPATOLOGY 2001;34:1184-1192.)
Viral Hepatitis
The influence of human immunodeficiency virus coinfection on
chronic hepatitis C in injection drug users: A long-term retrospective
cohort study (*Human Study*)
Vincent Di Martino, Pierre Rufat, Nathalie Boyer, Philippe Renard,
Françoise Degos, Michèle Martinot-Peignoux, Sophie
Matheron, Vincent Le Moing, François Vachon, Claude Degott,
Dominique Valla, Patrick Marcellin
In this study we analyzed the influence of human immunodeficiency
virus (HIV) infection on the course of chronic hepatitis C through
multivariate analysis including age, alcohol consumption, immune
status, and hepatitis C virus (HCV)-related virologic factors.
Eighty HIV-positive and 80 HIV-negative injection drug users included
between 1980 and 1995 were matched according to age, gender, and
duration of HCV infection and followed-up during 52 months. The
progression to cirrhosis was the primary outcome measure. The
impact of HIV on HCV-RNA load, histologic activity index, response
to interferon therapy, and liver-related death was also considered.
In HIV-positive patients, chronic hepatitis C was characterized
by higher serum HCV-RNA levels (P = .012), higher total
Knodell score (P = .011), and poorer sustained response
to interferon therapy (P = .009). High serum HCV-RNA level
was associated with low CD4-lymphocyte count (P = .001).
Necroinflamatory score was higher in HIV-positive patients (P
= .023) independently of the CD4-lymphocyte count, whereas increased
fibrosis was related to decreased CD4-lymphocyte count (P
= .011). The progression to cirrhosis was accelerated in HIV-positive
patients with low CD4 cell count (RR = 4.06, P = .024)
and in interferon-untreated patients (RR = 4.76, P = .001),
independently of age at HCV infection (P = .001). Cirrhosis
caused death in 5 HIV-positive patients. The risk of death related
to cirrhosis was increased in heavy drinkers (RR = 10.8, P
= .001) and in HIV-positive patients with CD4 cell count less
than 200/mm3 (RR = 11.9, P = .007). In this retrospective
cohort study, HIV coinfection worsened the outcome of chronic
hepatitis C, increasing both serum HCV-RNA level and liver damage
and decreasing sustained response to interferon therapy. Age and
alcohol were cofactors associated with cirrhosis and mortality.
Interferon therapy had a protective effect against HCV-related
cirrhosis no matter what the patient's HIV status was. (HEPATOLOGY
2001;34:1193-1199.)
Prevalence and risk factors for hepatitis C virus infection
at an Urban Veterans administration medical center (*Human
Study*)
Megan E. Briggs, Christiane Baker, Robert Hall, J. Michael Gaziano,
David Gagnon, Natalie Bzowej, Teresa L. Wright
This study was designed to determine the seroprevalence and risk
factors for hepatitis C virus (HCV) infection in veterans. Anti-HCV
testing was performed in 1,032 patients and a questionnaire regarding
sociodemographic characteristics and potential risk factors was
administered. Adjusted prevalence of unique HCV-positive patients
using outpatient services was 17.7% (95% confidence interval [CI]
17.2%, 18.2%). The following risk factors were associated with
HCV infection: a history of injection drug use (IDU), receipt
of blood transfusion prior to 1992, history of tattoo (odds ratio
[OR], 2.93; 95% CI, 1.70-5.08), combat job as a medical worker
(OR, 2.68; 95% CI, 1.25-5.60), history of incarceration over 48
hours (OR, 2.56; 95% CI, 1.52-4.32), greater than 15 lifetime
sexual partners (OR, 1.61; 95% CI, 0.94-2.76) and sexual relations
with a prostitute (OR, 0.46; 95% CI, 0.25-0.82). We concluded
that HCV is common in veterans. Risk factors independently associated
with infection are IDU, prior transfusion, prior tattoo, combat
medical work, incarceration, and multiple opposite sex partners.
Infection with HCV among veterans is strongly associated with
traditional risk factors for infection and less strongly associated
with combat-related risk. (HEPATOLOGY 2001;34:1200-1205.)
Different hepatitis C virus nonstructural protein 3 (Ns3)-DNAexpressing
vaccines induce in HLA-A2.1 transgenic mice stable cytotoxic T
lymphocytes that target one major epitope
Carine Brinster, Stéphanie Muguet, Yu-Chun Lone, Delphine
Boucreux, Nathalie Renard, Anne Fournillier, François Lemonnier,
Geneviève Inchauspé
The immunogenicity of the Hepatitis C virus (HCV) nonstructural
protein 3 (NS3) was investigated using different DNA-based strategies
and a preclinical mouse model transgenic for the HLA-A2.1 molecule.
Plasmids expressing NS3 either as a wild-type protein, as a fusion
with murine lysosome-associated-membrane protein-1 specific sequences,
or under the control of the Semliki Forest virus replicase were
evaluated in vitro and in vivo. All plasmids were
shown to express the expected size protein. These 3 NS3-expressing
vaccines induced overall comparable levels of CTLs when measured
at different times postvaccination although mice injected with
the NS3-LAMP expressing plasmid showed a particularly homogeneous
and overall vigorous response (specific lysis ranged from 60%
to 90 % for an E:T ratio of 33.3:1 with a mean CTL precursor frequency
of 1:2.105 cells). Out of the four HLA-A2.1-restricted NS3 epitopes
previously described in HCV infected patients (aa 1073-1081, aa
1406-1415; aa 1169-1177 and aa 1287-1296), the NS3-DNA generated
CTLs were predominantly targeted at the aa 1073-1081 epitope.
Peptide-based immunization showed that the mouse repertoire was
intact for all epitopes tested except one (aa 1287-1296). In conclusion,
the 3 NS3-DNA vaccines although based on different mode of action,
shared a comparable efficacy at inducing CTL. Surprisingly, the
breadth of such response was restricted to a single, major epitope.
(HEPATOLOGY 2001;34:1206-1217.)
Hepatitis B virus X protein transactivates inducible nitric
oxide synthase gene promoter through the proximal nuclear factor
B-binding site: Evidence that cytoplasmic location of X protein
is essential for gene transactivation (*Human Study*)
Pedro Majano, Enrique Lara-Pezzi, Manuel López-Cabrera,
Arantxa Apolinario, Ricardo Moreno-Otero, Carmelo García-Monzón
Nitric oxide appears to play a central role in the pathogenesis
of many inflammatory disorders. We have previously shown that
there is an enhanced intrahepatic expression of the inducible
nitric oxide synthase (iNOS) gene during chronic hepatitis B virus
infection, and that viral X protein (HBx) transcriptionally activates
this cellular gene, but the molecular basis for this activation
remains to be defined. We aimed to explore the involvement of
different cis-acting elements of the human iNOS promoter in the
HBx-mediated up-regulation as well as the effect of the intracellular
distribution of the HBx on its transacting function. Cotransfection
of human hepatocyte-derived cells with wild-type or mutated iNOS
promoter and with an HBx expression vector showed that functional
inactivation of the proximal nuclear factor B (NF-B)binding
site of the iNOS promoter markedly reduced the HBx-mediated transcriptional
activity. Mobility shift assays showed increased DNA-protein complexes
comprising mainly the p50 and p65 members of NF-B family in the
nuclear extracts from HBx-transfected cells. Transient transfection
experiments with HBx-expressing plasmids containing distinct cellular
localization sequences showed that cytoplasmic location of this
viral protein activated the iNOS promoter but when HBx was targeted
to the nucleus, the HBx-induced luciferase activity was almost
completely abrogated. In conclusion, cytoplasmic location of HBx
protein is essential for the transcriptional activation of the
iNOS gene through the nuclear translocation of p50-p65 heterodimers.
(HEPATOLOGY 2001;34:1218-1224.)
New challenge of hepatorenal syndrome: Prevention and treatment
Florence Wong, Laurence Blendis
Hepatorenal syndrome (HRS) remains one of the major therapeutic
challenges in hepatology today. The pathogenesis is complex, but
the final common pathway seems to be that sinusoidal portal hypertension,
in the presence of severe hepatic decompensation, leads to splanchnic
and systemic vasodilatation and decreased effective arterial blood
volume. Renal vasoconstriction increases concomitantly, renal
hemodynamics worsens, and renal failure occurs. Renal failure
was shown 15 years ago to be potentially reversible after liver
transplantation. This potential reversibility together with increased
understanding of the pathogenesis has led to successful preliminary
attempts to reverse HRS nonsurgically with combinations of splanchnic
vasoconstrictors and colloid volume expansion, insertion of transjugular
intrahepatic portovenous shunt radiologically, and improved forms
of dialysis. Recent classification of HRS into the acute onset
or severe type 1 with virtually 100% mortality and the more insiduous
less severe type II promises to shed more light on the pathogenesis
of HRS, especially on the currently unrecognized precipitating
factors. It is hoped that this classification will be included
in the necessary and carefully performed clinical trials, which
should lead to clearer indications for the available therapies.
The challenge now is to use all this information to improve our
management of cirrhotic patients to prevent occurrence of HRS
in the future. (HEPATOLOGY 2001;34:1242-1251.)
WNT1 Inducible Signaling Pathway Protein 3, WISP-3,
a Novel Target Gene in Colorectal Carcinomas With Microsatellite
Instability
LIN THORSTENSEN, CHIEU B. DIEP, GUNN I. MELING, TRUDE H. AAGESEN,
CHRISTIAN H. AHRENS, TORLEIV O. ROGNUM, and RAGNHILD A. LOTHE
Gastroenterology 2001 121: 1275-1280. Published online Nov 14
2001.Background & Aims: Microsatellite instability
(MSI) is the phenotype of colorectal carcinomas with defect mismatch
repair. Genes with repetitive sequences within their coding regions
are targets for mutations in these tumors. We have evaluated 2 novel
candidate genes for potential involvement in development of MSI
colorectal carcinomas and compared them with alterations in known
target genes. Methods: The MSI status was determined by
multiplex polymerase chain reactions (PCRs) of 5-17 markers in
a Norwegian series of 275 colorectal carcinomas. All MSI
tumors were analyzed for gene mutations using fluorescence PCR
followed by capillary electrophoresis. Two novel candidate genes,
WNT1-inducible signaling pathway protein 3 (WISP-3)
and caspase-1, and 9 known target genes were analyzed.
Results: Thirteen percent of the tumors were MSI-high (H)
and 12% were MSI-low (L). Thirty-three of 37 MSI-H vs. 1 of
34 MSI-L tumors showed mutations in the target genes (P < 0.001).
WISP-3 was mutated in 31% of the MSI-H tumors. The frequencies
of frameshift mutations in the known target genes were comparable
with other studies. Conclusions: The relative high frequency
of mutation, higher than those seen for other known target genes,
the predicted truncation of the protein product, and the homology
with WISP-1 and WISP-2, 2 proteins induced downstream of
WNT1 signaling, strongly suggest WISP-3 as a novel target in development
of MSI-H colorectal carcinomas.
CLINICAL SCIENCE:
Gastric Surgery Is Not a Risk for Barrett's Esophagus or
Esophageal Adenocarcinoma
BENJAMIN AVIDAN, AMNON SONNENBERG, THOMAS G. SCHNELL, and STEPHEN
J. SONTAG
Gastroenterology 2001 121: 1281-1285. Published online Nov 29
2001.Background & Aims: The contribution
of duodeno-gastroesophageal reflux to the development of Barrett's
esophagus has remained an interesting but controversial topic.
The present study assessed the risk for Barrett's esophagus after
partial gastrectomy. Methods: The data of outpatients from
a medicine and gastroenterology clinic who underwent upper gastrointestinal
endoscopy for any reason were analyzed in a case-control study.
A case population of 650 patients with short- segment and
366 patients with long-segment Barrett's esophagus was compared
in a multivariate logistic regression to a control population
of 3047 subjects without Barrett's esophagus or other types
of gastroesophageal reflux disease. Results: In the case
population, 25 (4%) patients with short-segment and 15 (4%)
patients with long-segment Barrett's esophagus presented with
a history of gastric surgery compared with 162 (5%) patients
in the control population, yielding an adjusted odds ratio of
0.89 with a 95% confidence interval of 0.54-1.46 for short-segment
and an adjusted odds ratio of 0.71 (0.30-1.72) for long-segment
Barrett's esophagus. Similar results were obtained in separate
analyses of 64 patients with Billroth-1 gastrectomy, 105 patients
with Billroth-2 gastrectomy, and 33 patients with vagotomy
and pyloroplasty for both short- and long-segment Barrett's esophagus.
Caucasian ethnicity, the presence of hiatus hernia, and alcohol
consumption were all associated with elevated risks for Barrett's
esophagus. Conclusions: Gastric surgery for benign peptic
ulcer disease is not a risk factor for either short- or long-segment
Barrett's esophagus. This lack of association between gastric
surgery and Barrett's esophagus suggests that reflux of bile without
acid is not sufficient to damage the esophageal mucosa.
Risk of Adenocarcinomas of the Esophagus and Gastric Cardia
in Patients With Gastroesophageal Reflux Diseases and After Antireflux
Surgery
WEIMIN YE, WONG-HO CHOW, JESPER LAGERGREN, LI YIN, and OLOF NYRÉN
Gastroenterology 2001 121: 1286-1293. Published online Nov 29
2001. Background & Aims: Gastroesophageal
reflux has been proposed as an important risk factor for esophageal
and gastric cardia adenocarcinoma, but prospective data are lacking.
Furthermore, the effect of antireflux surgery has not yet been
studied. We conducted a population-based retrospective cohort
study to fill these gaps. Methods: A cohort of 35,274 male
and 31,691 female patients with a discharge diagnosis of
gastroesophageal reflux diseases, and another cohort of 6406 male
and 4671 female patients who underwent antireflux surgery,
were identified in the Swedish Inpatient Register. Follow-up was
attained through record linkage with several nationwide registers.
Standardized incidence ratio (SIR) was used to estimate relative
risk of upper gastrointestinal cancers, using the general Swedish
population as reference. Results: After exclusion of the
first year follow-up, 37 esophageal and 36 gastric cardia
adenocarcinomas were observed among male patients who did not
have surgery (SIR, 6.3, 95% confidence interval [CI], 4.5-8.7;
SIR, 2.4, 95% CI, 1.7-3.3, respectively). SIR for esophageal
adenocarcinoma increased with follow-up time (P = 0.03 for
trend). Among male patients who had undergone antireflux surgeries,
risks were also elevated (16 esophageal adenocarcinoma, SIR,
14.1, 95% CI, 8.0-22.8; 15 gastric cardia adenocarcinomas,
SIR, 5.3, 95% CI, 3.0-8.7) and remained elevated with time
after surgery. The cancer risk pattern in women was similar to
that for men, but the number of cases were much smaller. Conclusions:
Gastroesophageal reflux is strongly associated with the risk of
esophageal adenocarcinoma, and to a lesser extent, with gastric
cardia adenocarcinoma. The risk of developing adenocarcinomas
of the esophagus and gastric cardia remains increased after antireflux
surgery.
Extraesophageal Associations of Gastroesophageal Reflux
Disease in Children Without Neurologic Defects
HASHEM B. EL-SERAG, MARK GILGER, MARK KUEBELER, and LINDA RABENECK
Gastroenterology 2001 121: 1294-1299. Published online Nov 29
2001. Background & Aims: The potential association
between gastroesophageal reflux disease (GERD) and extraesophageal
manifestations remains unknown in children without neurological
defects. We conducted a large case-control study to examine the
association between GERD and several upper and lower respiratory
disorders in these children. Methods: We identified all
patients between 2 and 18 years of age with GERD who
were seen at Texas Children's Hospital between 1996 and 2000. Patients
seen during the same time period without GERD were randomly selected
as controls (4:1 ratio). Patients with mental retardation, cerebral
palsy, or congenital esophageal anomalies were excluded. We compared
the presence of several predefined upper and lower respiratory
disorders in cases and controls. Results: We identified
1980 patients with GERD and 7920 controls without GERD.
Cases and controls were without neurological deficits or congenital
esophageal anomalies. Cases were older than controls (9.2 years ± 4.6 vs.
8.6 ± 4.9, P < 0.0001), and
were more likely to be female (51.2% vs. 47.2%, P = 0.0028)
and white (60.2% vs. 41.2%, P < 0.0001). Compared
with controls in univariate analyses, cases with GERD had more
sinusitis (4.2% vs. 1.4%, P < 0.0001), laryngitis
(0.7% vs. 0.2%), asthma (13.2% vs. 6.8%, P < 0.0001),
pneumonia (6.3% vs. 2.3%, P < 0.0001), and
bronchiectasis (1.0% vs. 0.1%, P < 0.0001). However,
otitis media was less common in cases than controls (2.1% vs.
4.6%, P < 0.0001). After adjusting for differences
in age, gender, and ethnicity in the regression analyses, GERD
remained a significant risk factor for sinusitis (adjusted odds
ratio [OR], 2.3; 95% confidence intervals [CI], 1.7-3.2; P < 0.0001),
laryngitis (OR, 2.6; CI, 1.2-5.6; P = 0.0228), asthma (OR,
1.9; CI, 1.6-2.3; P < 0.0001), pneumonia (OR,
2.3; CI, 1.8-2.9; P < 0.0001), and bronchiectasis
(OR, 2.3; CI, 1.1-4.6; P = 0.0193). Conclusions:
GERD in children without neurological defects is associated with
a several-fold increase in the risk of sinusitis, laryngitis,
asthma, pneumonia, and bronchiectasis. Further studies are needed
to examine whether a cause-effect relationship exists between
GERD and these disorders in children.
Extensive Methylation of hMLH1 Promoter Region
Predominates in Proximal Colon Cancer With Microsatellite Instability
YASUYUKI MIYAKURA, KOKICHI SUGANO, FUMIO KONISHI, AKIRA ICHIKAWA,
MASATO MAEKAWA, KAZUHISA SHITOH, SEIJI IGARASHI, KENJIRO KOTAKE,
YASUO KOYAMA, and HIDEO NAGAI
Gastroenterology 2001 121: 1300-1309. Published online Nov 29
2001. Background & Aims: Methylation of the
hMLH1 promoter region has been suggested to cause microsatellite
instability (MSI) in sporadic colorectal carcinoma (CRC). We studied
the methylation profile in a wide region of the hMLH1 promoter
and compared with the hMLH1 protein expression and MSI status
in 88 cases of sporadic CRC. Methods: Na-bisulfite
treatment and polymerase chain reaction single-strand conformation
polymorphism analysis was performed using 5 sets of polymerase
chain reaction primers spanning the promoter region of the hMLH1
to examine methylation status. Results were compared with immunostaining
using anti-hMLH1 monoclonal antibody and MSI status of the tumor
samples. Results: Methylation status was classified as
full or partial methylation. Full methylation indicates the methylation
of all CpG sites in the examined regions. Methylation of the hMLH1
promoter was observed in 88.9% (16 of 18) of CRCs showing
high frequency MSI (MSI-H), among which 89% (14 of 16) had
full methylation with reduced hMLH1 protein expression. All cases
showing full methylation were proximal colon tumors with MSI-H.
In cases with partial methylation, only the upstream region of
the hMLH1 promoter was methylated. Partial methylation
was also shown in 33.3% (6 of 18) of the normal mucosa of
MSI-H cases. Frequencies of methylation were significantly correlated
with female gender (P = 0.0009) and aging (P = 0.007).
Conclusions: Full methylation of the hMLH1 promoter
region and subsequent gene inactivation may play a crucial role
in the carcinogenesis of MSI-H CRCs in the proximal colon. Methylation
upstream of the hMLH1 promoter appears to be an early event
in the carcinogenesis of MSI-H tumors.
Cystic Fibrosis Gene Mutations and Pancreatitis Risk: Relation
to Epithelial Ion Transport and Trypsin Inhibitor Gene Mutations
PEADAR G. NOONE, ZHAOQING ZHOU, LAWRENCE M. SILVERMAN, PAUL S.
JOWELL, MICHAEL R. KNOWLES, and JONATHAN A. COHN
Gastroenterology 2001 121: 1310-1319. Published online Nov 29
2001. Background & Aims: Nonalcoholic chronic
pancreatitis is usually idiopathic and often associated with cystic
fibrosis gene (CFTR) mutations. It is unknown whether pancreatitis
risk correlates with having 1 or 2 CFTR mutations,
abnormal epithelial ion transport, or mutations of other genes.
Methods: We tested 39 patients with idiopathic chronic
pancreatitis (mean age at diagnosis, 33 years) for common
mutations of CFTR and of genes encoding a trypsin inhibitor
(PSTI) and trypsinogen (PRSS1). To exclude hereditary
pancreatitis, we initially relied on family history and subsequently
tested for PRSS1 mutations. Twenty subjects were tested
for rare CFTR mutations (DNA sequencing) and 11 were
tested for extrapancreatic CFTR function (clinical and physiologic
evaluation). Results: Mutations were identified in 24 of
39 subjects. Nine patients had cystic fibrosis-causing mutations,
8 of whom also had mild-variable mutations. Eight others
had only mild-variable mutations. Nine subjects had the N34S PSTI
mutation and 1 had hereditary pancreatitis (R122H, PRSS1).
Pancreatitis risk was increased approximately 40-fold by having
2 CFTR mutations (P < 0.0001),
20-fold by having N34S (P < 0.0001), and 900-fold
by having both (P < 0.0001). Subjects with
2 CFTR mutations had abnormal nasal epithelial ion
transport and clinical findings suggesting residual CFTR function
between that in cystic fibrosis and in carriers. By contrast,
subjects with only PSTI mutations had normal CFTR function.
Conclusions: CFTR-related pancreatitis risk correlates
with having 2 CFTR mutations and reduced extrapancreatic
CFTR function. The N34S PSTI mutation increased risk separately.
Testing for pancreatitis-associated CFTR and PSTI genotypes
may be useful in nonalcoholic pancreatitis.
Epithelial Barrier Defects in Ulcerative Colitis: Characterization
and Quantification by Electrophysiological Imaging
ALFRED H. GITTER, FRIEDERIKE WULLSTEIN, MICHAEL FROMM, and JÖRG
DIETER SCHULZKE
Gastroenterology 2001 121: 1320-1328. Published online Nov 29
2001.Background & Aims: In ulcerative colitis
(UC), the epithelial barrier is impaired by erosion/ulcer-type
lesions and epithelial apoptosis causing local leaks, and generalized
tight junction alterations increasing the basal permeability.
We quantified the contribution of these mechanisms to the increased
colonic ion permeability. Methods: Sigmoid colon was stripped,
and the spatial distribution of current clamped across the viable
epithelium was recorded by a microelectrode probe, using the conductance
scanning method. Local leaks (circumscribed conductive peaks)
were marked, and structural changes were studied in H&E-stained
series sections. Results: Overall conductivity increased
from 8.4 ± 0.7 mS/cm2 (mean ± SEM)
in controls to 11.7 ± 0.6 in specimens with
mild inflammation (i.e., with intact epithelium) and 34.4 ± 6.2 mS/cm2
in moderate-to-severe inflammation (i.e., with visible epithelial
lesions). Only in part this was caused by a generalized increase
in basal conductivity (12.2 ± 1.5 mS/cm2
in moderate-to-severe UC vs. 8.3 ± 0.7 in
controls). More importantly, the spatial distribution of conductivity,
which was even in controls, showed dramatic leaks in UC. Leaks
found in mild inflammation without epithelial lesion turned out
to be foci of epithelial apoptosis. In moderate-to-severe inflammation,
leaks correlated with epithelial erosion/ulcer-type lesions or
crypt abscesses. Conclusions: In early UC, but not in controls,
seemingly intact epithelium comprises leaks at apoptotic foci.
With more intensive inflammation, erosion/ulcer-type lesions are
highly conductive, even if covered with fibrin. Local leaks contribute
19% to the overall epithelial conductivity in mild and 65% in
moderate-to-severe inflammation.
Celiac Disease-like Abnormalities in a Subgroup of Patients
With Irritable Bowel Syndrome
ULRICH WAHNSCHAFFE, R. ULLRICH, E. O. RIECKEN, and J. D. SCHULZKE
Gastroenterology 2001 121: 1329-1338. Published online Nov 29
2001. Background & Aims: Abdominal symptoms
in the absence of mucosal abnormalities are features of both the
irritable bowel syndrome (IBS) and latent/potential celiac disease
(cd). To identify a possible subgroup of IBS patients with latent/potential
cd, surrogate markers of cd were investigated in IBS patients.
Methods: IBS patients suffering from diarrhea (n = 102),
and patients with active cd (n = 10), treated cd (n = 26),
and latent cd (n = 5) were included in the study. We
measured serum immunoglobulin (Ig) A against gliadin and tissue-transglutaminase,
and IgA and IgM against gliadin, tissue-transglutaminase (intestinal
cd-associated antibodies), and the dietary proteins -lactoglobulin
and ovalbumin in duodenal aspirate by enzyme-linked immunosorbent
assay. Intraepithelial lymphocytes (IELs) were counted in histology
sections, and the expression of HLA-DQ2 (A1*0501/B1*0201) was
investigated by polymerase chain reaction. In 26 IBS patients,
the effect of 6 months of gluten withdrawal was examined.
Results: Most cd patients expressed HLA-DQ2 and had increased
intestinal cd-associated antibodies, whereas cd-associated serum
IgA and IEL counts were increased in active cd in contrast to
treated or latent cd. In IBS patients, 35% were HLA-DQ2-positive,
23% had increased IEL counts, and 0% and 30% had increased cd-associated
antibodies in serum and duodenal aspirate, respectively. Furthermore,
stool frequency and intestinal IgA decreased significantly under
a gluten-free diet in the subgroups of HLA-DQ2-positive and intestinal
antibody-positive IBS patients when compared with IBS patients
without these markers. Conclusions: HLA-DQ2 expression
and increased intestinal cd-associated antibodies are markers
that can identify latent/potential cd in a subgroup of IBS patients
who consequently appear to profit from a gluten-free diet.
-Up-regulation of Cyclooxygenase 2 Gene Expression Correlates
With Tumor Angiogenesis in Human Colorectal Cancer
FABIO CIANCHI, CAMILLO CORTESINI, PAOLO BECHI, ORNELLA FANTAPPIÈ,
LUCA MESSERINI, ALFREDO VANNACCI, IACOPO SARDI, GIANNA BARONI,
VIERI BODDI, ROBERTO MAZZANTI, and EMANUELA MASINI
Gastroenterology 2001 121: 1339-1347. Published online Nov 29
2001. Background & Aims: Recent studies have
shown that cyclooxygenase (COX)-2 and its products, prostaglandins
(PGs), may be involved in colorectal carcinogenesis. The aim of
this study was to determine whether COX-2 expression and PGE2
production correlate with microvessel density, vascular endothelial
growth factor (VEGF) expression, and tumor metastasis in human
colorectal cancer. Methods: Tumor samples and adjacent
normal mucosa were obtained from 31 surgical specimens. Immunohistochemical
expression of COX-2, VEGF, and CD31 was analyzed on paraffin-embedded
tissue sections. COX-2 and COX-1 proteins were determined by Western
blot analysis. COX-2 and VEGF messenger RNA expressions were evaluated
using Northern blot analysis. PGE2 production was determined by
specific radioimmunoassay. Results: The immunohistochemical
expressions of both COX-2 and VEGF were significantly correlated
with microvessel density (P = 0.02 and P = 0.002, respectively).
A significant correlation was found between COX-2 and VEGF expression
(P = 0.004). Western analysis confirmed the up-regulation
of COX-2 protein expression. COX-2 and VEGF genes were overexpressed
in tumor specimens as compared with normal mucosa. PGE2 levels
were significantly higher in metastatic tumors than in nonmetastatic
ones (P = 0.03). Conclusions: COX-2 is
related to tumor angiogenesis in colorectal cancer. It is likely
that VEGF is one of the most important mediators of the COX-2
angiogenic pathway.
Incidence of Gastric Cancer and Breast Cancer in CDH1 (E-Cadherin)
Mutation Carriers From Hereditary Diffuse Gastric Cancer Families
PAUL D. P. PHAROAH, PARRY GUILFORD, CARLOS CALDAS, and THE INTERNATIONAL
GASTRIC CANCER LINKAGE CONSORTIUM
Gastroenterology 2001 121: 1348-1353. Published online Nov 29
2001. Background & Aims: Germline mutations
in CDH1 are known to cause hereditary diffuse gastric cancer (HDGC).
Breast and colorectal cancer have also been reported in CDH1-associated
HDGC. The purpose of this study was to estimate the cumulative
risk of gastric and breast cancer in CDH1 mutation carriers. Methods:
Family data were collected by member groups of the International
Gastric Cancer Linkage Consortium. Eligible families had at least
3 cases of diffuse gastric cancer, and at least 1 affected
member had tested positive for a mutation in CDH1. Eleven families
met these criteria. We used the pedigree information to estimate
penetrance using the MENDEL program. The conditional likelihood
of the pedigree was maximized given the phenotype of the pedigree
and genotype of the index case at ascertainment. We parameterized
the model in terms of log relative risks for mutation carriers
compared with risks in the general population of the United Kingdom.
Noncarriers of the gene were assumed to develop the disease at
population incidence rates. Results: The estimated cumulative
risk of gastric cancer by age 80 years was 67% for men (95%
confidence interval [95% CI], 39-99) and 83% for women (95% CI,
58-99). For women, the cumulative risk of breast cancer was 39%
(95% CI, 12-84). The combined risk of gastric cancer and breast
cancer in women was 90% by age 80 years. Conclusions:
These penetrance estimates should be useful for genetic counseling
in multiple-case families. However, they may not apply to individuals
with a minimal family history, in whom the risks may be lower.
BASIC SCIENCE:
Prostanoid Production Via COX-2 as a Causative Mechanism
of Rodent Postoperative Ileus
NICOLAS T. SCHWARZ, JÖRG C. KALFF, ANDREAS TÜRLER, BRITTA
M. ENGEL, SIMON C. WATKINS, TIMOTHY R. BILLIAR, and ANTHONY J.
BAUER
Gastroenterology 2001 121: 1354-1371. Published online Nov 29
2001. Background & Aims: This study demonstrates
a significant role for cyclooxygenase (COX)-2 and prostanoid production
as mechanisms for surgically induced postoperative ileus. Methods:
Rats, COX-2+/+, and COX-2/ mice underwent simple intestinal manipulation.
Reverse-transcription polymerase chain reaction and immunohistochemistry
were used to detect and localize COX-2 expression. Prostaglandin
levels were measured from serum, peritoneal lavage fluid, and
muscularis culture media. Jejunal circular muscle contractions
were measured in an organ bath, and gastrointestinal transit was
measured in vivo. Results: The data show that intestinal
manipulation induces COX-2 messenger RNA and protein within resident
muscularis macrophages, a discrete subpopulation of myenteric
neurons and recruited monocytes. The manipulation-induced increase
in COX-2 expression resulted in significantly elevated prostaglandin
levels within the circulation and peritoneal cavity. The source
of these prostanoids could be directly attributed to their release
from the inflamed muscularis externa. As a consequence of the
molecular up-regulation of COX-2, we observed a decrease in in
vitro jejunal circular muscle contractility and gastrointestinal
transit, both of which could be alleviated pharmacologically with
selective COX-2 inhibition. These studies were corroborated with
the use of COX-2/ mice. Conclusions: Prostaglandins, through
the induction of COX-2, are major participants in rodent postoperative
ileus induced by intestinal manipulation.
-Blockade of Endogenous IL-18 Ameliorates TNBS-Induced Colitis
by Decreasing Local TNF- Production in Mice
TESSA TEN HOVE, ANNE CORBAZ, HAGIT AMITAI, SHUKI ALONI, ILANA
BELZER, PIERRE GRABER, PAUL DRILLENBURG, SANDER J. H. VAN DEVENTER,
YOLANDE CHVATCHKO, and ANJE A. TE VELDE
Gastroenterology 2001 121: 1372-1379. Published online Nov 29
2001. Background & Aims: Interleukin (IL)
18 has proinflammatory effects. IL-18 plays a pivotal role
in Th1 responses, but its proinflammatory activities extend beyond
Th1 cells, including macrophages and production of tumor necrosis
factor (TNF) and IL-1. IL-18 is up-regulated in colonic
specimens of patients with Crohn's disease. The goal of this study
was to evaluate the role of IL-18. Methods: Activity of
IL-18 was neutralized using recombinant human IL-18 binding protein
isoform a (rhIL-18BPa) in trinitrobenzene sulfonic acid (TNBS)-induced
colitis. Results: Mice treated daily with rhIL-18BPa (8 mg/kg)
had significant reductions in clinical score, body weight loss,
and colon weight increase compared with saline-treated mice. Histologic
analysis showed that rhIL-18BPa-treated mice developed only mild
colitis without signs of ulceration, with a mean total score of9.8 ± 1.3 points
compared with 15.9 ± 1.1 points observed
in saline-treated mice with colitis. Analysis of cytokine levels
in colon homogenates showed a significant decrease in TNF-, IL-6,
and IL-1 after rhIL-18BPa treatment but no effect on interferon
. The therapeutic potential of rhIL-18BPa treatment was confirmed
in TNBS mice that were treated only on days 8 and 9 after
the start of the experiment. In these mice, significant reductions
in total colitis score and colon weight were also observed. Conclusions:
These findings show that inhibition of rhIL-18BPa bioactivity,
via rhIL-18BPa, may be beneficial for the treatment of IBD.
Human Pancreatic Acinar Cells Lack Functional Responses
to Cholecystokinin and Gastrin
BAOAN JI, YAN BI, DIANE SIMEONE, RICHARD M. MORTENSEN, and CRAIG
D. LOGSDON
Gastroenterology 2001 121: 1380-1390. Published online Nov 29
2001. Background & Aims: Pancreatic acinar
cells from various species express cholecystokinin (CCK) A, CCK-B,
or a combination of these CCK receptor subtypes. The presence
and functional roles of CCK receptors on human acinar cells remain
unclear. Methods: Acini isolated from human pancreas were
treated with CCK receptor agonists, CCK-8 and gastrin, and an
agonist for m3 muscarinic acetylcholine receptors (m3 AchR), carbachol.
Functional parameters measured included intracellular [Ca2+],
amylase secretion, and ERK phosphorylation. Binding studies were
performed using 125I-CCK-8. Expression of messenger RNAs (mRNAs)
was determined using real-time quantitative reverse-transcription
polymerase chain reaction (RT-PCR) and localized by in situ hybridization.
Results: Human acini did not respond to CCK agonists. In
contrast, they responded to carbachol with robust increases in
each of the functional parameters. Moreover, the cells responded
to CCK agonists after adenoviral-mediated gene transfer of CCK-A
or CCK-B receptors. A low level of specific and a high level of
nonspecific binding of 125I-CCK-8 were observed. Quantitative
RT-PCR indicated that the message levels for CCK-A receptors were
~30-fold lower than those of CCK-B receptors, which were ~10-fold
lower than those of m3 Ach receptors. In situ hybridization indicated
the presence of m3 Ach receptor and insulin mRNA but not CCK-A
or CCK-B receptor mRNAs in adult human pancreas. Conclusions:
These data indicate that human pancreatic acinar cells do not
respond to CCK receptor agonists in terms of expected functional
parameters and show that this is due to an insufficient level
of receptor expression.
Duodenal Reflux Induces Cyclooxygenase-2 in the Esophageal
Mucosa of Rats: Evidence for Involvement of Bile Acids
FAN ZHANG, NASSER K. ALTORKI, YU-CHUNG WU, ROBERT A. SOSLOW, KOTHA
SUBBARAMAIAH, and ANDREW J. DANNENBERG
Gastroenterology 2001 121: 1391-1399. Published online Nov 29
2001. Background & Aims: Reflux of duodenal
contents including bile acids is believed to contribute to esophageal
injury and Barrett's esophagus. Cyclooxygenase (COX)-2, an inducible
form of COX, has been implicated in both inflammation and carcinogenesis.
In this study, we investigated the effects of bile acids and duodenal
reflux on COX-2 expression in cultured esophageal cells and tissue,
respectively. Methods: Immunoblotting and Northern blotting
were used to assess the effects of bile acids on COX-2 expression
in esophageal cell lines. Immunoblotting and immunohistochemistry
were performed to evaluate the effects of duodenal reflux on COX-2
expression and cell proliferation in esophageal tissue. Results:
Unconjugated bile acids were about fivefold more potent inducers
of COX-2 messenger RNA, COX-2 protein, and prostaglandin synthesis
than conjugated bile acids. Acidifying the culture medium sensitized
esophageal cells to bile acid-mediated induction of COX-2. The
induction of COX-2 by bile acids was mediated by phosphatidylinositol-3
kinase and extracellular signal-regulated kinase 1/2 mitogen-activated
protein kinases. In experimental animals, duodenoesophageal reflux
led to esophagitis, marked thickening of the esophageal mucosa,
and enhanced expression of COX-2. Increased immunoreactivity for
Ki-67 and cyclin D1 indicated that enhanced cell proliferation
contributed to mucosal thickening. Conclusions: Reflux
of duodenal contents into the esophagus led to increased COX-2
expression and mucosal thickening. Bile acids are likely to contribute
to these effects.
D-Glucose Releases 5-Hydroxytryptamine from Human BON
Cells as a Model of Enterochromaffin Cells
MINSOO KIM, HELEN J. COOKE, NAJMA H. JAVED, HANNAH V. CAREY, FIEVOS
CHRISTOFI, and HELEN E. RAYBOULD
Gastroenterology 2001 121: 1400-1406. Published online Nov 29
2001. Background & Aims: 5-Hydroxytryptamine
(5-HT) is released from enterochromaffin cells and activates neural
reflex programs regulating motility and secretion. Although sugars
are reported to release 5-HT in vivo, it is unclear whether they
act directly on enterochromaffin cells or indirectly through an
intermediary messenger. The aim was to determine if D-glucose
is a stimulus for 5-HT release. Methods: Human BON cells,
derived from enterochromaffin cells, were treated with D-glucose,
galactose, and the nonmetabolizable methyl -D-glucopyranoside,
or with fructose. Results: Reverse-transcription polymerase
chain reaction together with Western blot analysis revealed an
SGLT-like protein. D-Glucose caused a concentration-dependent
increase in 5-HT release, which was mimicked by methyl -D-glucopyranoside
and galactose but not fructose. D-Glucose-stimulated 5-HT release
was significantly reduced by phloridzin. Concentrations of mannitol
below 75 mmol/L were ineffective in releasing 5-HT. Brefeldin
A abolished forskolin-stimulated 5-HT release without affecting
basal or constitutive release. Conclusions: The results
show that high concentrations of metabolizable and nonmetabolizable
hexoses activate signal transduction pathways, leading to release
of 5-HT. These findings imply a role for enterochromaffin cells
as "glucose sensors" during ingestion of a meal.
The Role of Mutant Apc in the Development of Dysplasia and
Cancer in the Mouse Model of Dextran Sulfate Sodium-Induced Colitis
HARRY S. COOPER, LYNETTE EVERLEY, WEN-CHI CHANG, GORDON PFEIFFER,
BRYAN LEE, SREEKANT MURTHY, and MARGIE L. CLAPPER
Gastroenterology 2001 121: 1407-1416. Published online Nov 29
2001. Background & Aims: Differences in genetic
background may play a role in the development of ulcerative colitis
(UC)-related neoplasia. Loss of heterozygosity (LOH) of APC has
been reported in human UC-associated neoplasia. To investigate
the role of genetic differences in UC-associated neoplasia, we
compared differences in dextran sodium sulfate (DSS) colitis-associated
neoplasia between wild-type C57BL/6J mice (WT-DSS) and C57BL/6J
mice with a germline mutation in Apc (Min-DSS). Methods:
DSS colitis was induced in female wild-type and Min mice. Age-
and sex-matched non-DSS-treated Mins were also studied. Animals
were sacrificed after 1 and 2 cycles of DSS. The cecums
and large intestines were studied for numbers of dysplasias/cancers.
Dysplasias were studied for LOH of Apc. Results: No WT-DSS,
100% of Min-DSS, and 50% of non-DSS-treated Mins had dysplasia.
The mean numbers of lesions per mouse were 0 (WT-DSS), 15.6 and
29.3 (1 and 2 cycles Min-DSS, respectively), 1.2 and
1.9 (age-matched control Min, 1 and 2 cycle equivalents,
respectively; P < 0.0002, Min-DSS vs.
WT-DSS and non-DSS-treated Min; P = 0.03, Min-DSS
2 cycle vs. Min-DSS 1 cycle). Cancers were seen in 0%,
22%, and 40% of non-DSS Min, Min-DSS-1 cycle, and Min-DSS-2 cycle
animals, respectively. LOH of Apc was observed in 90.6% of dysplasias
and 6% of nondysplastic mucosa. Conclusions: A germline
mutation in Apc contributes significantly to the development of
colitis-associated neoplasia. Colitis markedly accelerates the
development of dysplasia and cancer in the Min mouse. Dysplasia
in Min-DSS occurs through LOH of Apc.
Antral Mucosa Expresses Functional Leptin Receptors Coupled
to STAT-3 Signaling, Which Is Involved in the Control of Gastric
Secretions in the Rat
HÉLÈNE GOÏOT, SAMIR ATTOUB, STÉPHANIE
KERMORGANT, JEAN-PIERRE LAIGNEAU, BERNARD LARDEUX, THÉRÈSE
LEHY, MIGUEL J. M. LEWIN, and ANDRÉ BADO
Gastroenterology 2001 121: 1417-1427. Published online Nov 29
2001. Background & Aims: Leptin is a circulating
hormone that communicates the peripheral nutritional status to
the hypothalamus, which controls food intake, energy expenditure,
and body weight. This study characterizes leptin receptors and
leptin-sensitive STAT proteins in the antrum and investigates
the effects of leptin on gastric secretions. Methods: The
effects of leptin on gastrin messenger RNA (mRNA), plasma gastrin,
gastric acid in vivo in the rat, and on somatostatin and gastrin
secretions by isolated antral cells were determined in vitro.
Leptin receptors were investigated in isolated rat antral cells
by reverse transcription-polymerase chain reaction and binding
of [125I]-leptin studies. The effects of in vivo and in vitro
leptin on transduction signal STAT proteins were investigated
by immunoblotting antral extracts. Results: Peripheral
injection of leptin inhibited in a dose-dependent manner, basal
gastric secretion, gastrinemia, and mucosal gastrin mRNA in vivo.
mRNAs encoding the long (Ob-Rb) and short (Ob-Ra) receptor forms
were detected in rat antral mucosa, as were STAT-1, -3, and
-5b immunoreactive proteins. Isolated antral cells specifically
bound [125I]-leptin, and addition of leptin to these cells inhibited
the release of somatostatin and increased the release of gastrin.
These effects were associated with an increase in nuclear STAT-3
proteins in vitro and in vivo. Conclusions: This study
provides the first molecular evidence for the coexpression of
leptin receptors and STAT-3 in antral mucosa. It provides further
evidence for the involvement of leptin in the control of gastric
secretions.
Antibody Blockade of ICAM-1 and VCAM-1 Ameliorates Inflammation
in the SAMP-1/Yit Adoptive Transfer Model of Crohn's Disease in
Mice
R. CARTLAND BURNS, JESUS RIVERA-NIEVES, CHRISTOPHER A. MOSKALUK,
SATOSHI MATSUMOTO, FABIO COMINELLI, and KLAUS LEY
Gastroenterology 2001 121: 1428-1436. Published online Nov 29
2001. Background & Aims: Integrins (4 and
2) and their endothelial ligands vascular cell adhesion molecule-1
(VCAM-1) and intercellular adhesion molecule-1 (ICAM-1) play key
roles in leukocyte recruitment to areas of inflammation. ICAM-1
and VCAM-1 are expressed in inflamed intestinal tissues. This
study investigates a possible causative role of adhesion molecules
ICAM-1, VCAM-1, and 4 integrins in mediating the inflammatory
response in a murine model of Crohn's disease (CD). Methods:
CD4+ mesenteric lymph node cells from SAMP-1/Yit donor mice were
adoptively transferred into major histocompatibility complex-matched
severe combined immunodeficiency disease mice. Six weeks later,
these mice were left untreated or treated for 3 days with
monoclonal antibodies (mAbs) to ICAM-1, VCAM-1, or both, and 4,
or both ICAM-1 and 4, dexamethasone, or nonblocking isotype control
antibodies. On day 4 after treatment, tissues were investigated
for expression of ICAM-1, VCAM-1, and for severity of inflammation
using a semiquantitative inflammatory score. Dexamethasone treatment
resolved all measures of intestinal inflammation. Results:
Blocking either ICAM-1, VCAM-1, or 4 integrins had no significant
beneficial effect. However, blocking ICAM-1 and 4, or blocking
ICAM-1 and VCAM-1, showed a 70% resolution of the active inflammation,
but not chronic inflammation. Conclusions: These findings
suggest that blocking ICAM-1 and VCAM-1 may have therapeutic benefit
for the acute inflammatory component of Crohn's disease.
Phosphorylation of the Serine 60 Residue Within the Cdx2
Activation Domain Mediates Its Transactivation Capacity
EDMOND H. H. M. RINGS, FRANÇOIS BOUDREAU, JENNIFER K. TAYLOR,
JENNIFER MOFFETT, EUN RAN SUH, and PETER G. TRABER
Gastroenterology 2001 121: 1437-1450. Published online Nov 29
2001. Background & Aims: Cdx2 is critical
in intestinal proliferation and differentiation. Modulation of
Cdx2 function in response to cellular signaling is to be elucidated.
We hypothesize that phosphorylation of the Cdx2 activation domain
can modulate its function. Methods: The Cdx2 activation
domain was delineated in transient transfections using different
portions of Cdx2 fused to the Gal4-DNA binding domain. In vivo
phosphorylation was studied by metabolic labeling with 32P-orthophosphate.
To study a potential phosphorylation site, polyclonal antibodies
were generated: CNL was raised against amino acids 54-66 of Cdx2
and P-Cdx2-S60 against the same epitope in which serine 60 was
phosphorylated. Results: A critical region for transactivation
resides within amino acids 60-70. Substitution of serine 60 with
alanine reduces incorporation of 32P-orthophosphate substantially.
S60-phosphorylation decreases Cdx2 transactivation. Phosphorylation
of serine 60 can be inhibited with the mitogen-activated
protein kinase inhibitors PD98059 or UO126. P-Cdx2-S60 recognizes
phosphorylated serine 60 mainly in proliferative compartment
of the intestinal epithelial layer. In contrast, CNL recognizes
Cdx2 predominantly in the differentiated compartment. Conclusions:
The Cdx2 activation domain is phosphorylated at serine 60 via
the mitogen-activated protein kinase pathway. S60-phosphorylated
and S60-nonphosphorylated Cdx2 have different transcriptional
activity, as well as different spatial expression patterns in
the intestinal epithelium.
The Superoxide Dismutase Mimetic MnTBAP Prevents Fas-Induced
Acute Liver Failure in the Mouse
BENOÎT MALASSAGNE, PIERRE-JACQUES FERRET, RENAUD HAMMOUD,
MICHELINE TULLIEZ, SASSIA BEDDA, HÉLÈNE TRÉBÉDEN,
PATRICK JAFFRAY, YVON CALMUS, BERNARD WEILL, and FRÉDÉRIC
BATTEUX
Gastroenterology 2001 121: 1451-1459. Published online Nov 29
2001. Background & Aims: Acute liver failure
(ALF) of viral origin results from massive hepatocyte apoptosis
induced by the interaction between Fas expressed on hepatocytes
and Fas ligand on activated T lymphocytes. Because Fas-induced
apoptosis of hepatocytes involves mitochondrial damages and potential
reactive oxygen species (ROS) overproduction, we investigated
whether manganese III tetrakis (5,10,15,20 benzoic acid)
(MnTBAP), a nonpeptidyl mimic of superoxide dismutase (SOD), can
inhibit Fas-induced ALF. Methods: An agonist anti-Fas monoclonal
antibody was used to induce hepatocyte apoptosis in vitro and
ALF in vivo. Results: Preventive and curative treatments
by MnTBAP significantly increased survival rates and significantly
reduced aspartate aminotransferase levels and parenchymal lesions.
ROS generation was suggested by those beneficial effects and significant
increases in SOD and Gpx activities after anti-Fas injection.
Flow cytometry of isolated hepatocytes incubated with anti-Fas
monoclonal antibody showed that ROS production was associated
with the collapse of transmembrane potential and loss of cardiolipin
content. After injection of anti-Fas monoclonal antibody, mitochondrial
Bcl-2 was decreased, cytochrome c released, and caspase-3 activated.
Mitochondrial alterations and their consequences were abrogated
by MnTBAP. Conclusions: ROS are key executioners in Fas-induced
hepatocyte apoptosis. This finding explains why a nonpeptidyl
mimic of SOD can cure ALF in a model of viral hepatitis, pointing
out the potential interest of this molecule in humans.
Kupffer Cell-Mediated Recruitment of Rat Dendritic Cells
to the Liver: Roles of N-Acetylgalactosamine-Specific
Sugar Receptors
RYOSUKE UWATOKU, MAKOTO SUEMATSU, TAICHI EZAKI, TAKAHITO SAIKI,
MAKOTO TSUIJI, TATSURO IRIMURA, NORIFUMI KAWADA, TATSUO SUGANUMA,
MAKOTO NAITO, MASAYASU ANDO, and KENJIRO MATSUNO
Gastroenterology 2001 121: 1460-1472. Published online Nov 29
2001. Background & Aims: Tissue recruitment
of dendritic cells (DCs) is essential for antigen presentation.
This study aimed to examine cellular and molecular mechanisms
for DC recruitment to the liver. Methods: Purified rat
DCs were injected into circulation and their traffics were analyzed
in normal and Kupffer cell-depleted rats by intravital confocal
microscopy and immunohistology. Affinities of DCs to sinusoidal
cells were examined by a cell-binding assay. DC precursor recruitment
was induced by particulate injection. Results: Both DC
precursors and DCs at the antigen-transporting stage could be
recruited to the liver, and their majority initially showed a
selective binding to Kupffer cells. In the Kupffer cell-depleted
rats, DCs could neither be recruited to the liver nor adhere to
sinusoidal walls. Pretreatment with varied monosaccharides showed
that sugar residues consisting of N-acetylgalactosamine
were necessary for this binding. The binding was calcium-dependent,
implying the C-type lectin involvement. Furthermore, DCs could
endocytose N-acetylgalactosamine polymers in a receptor-specific
manner. Conclusions: The DC-Kupffer cell binding through
N-acetylgalactosamine-specific C-type lectin-like receptors
is crucial for DC recruitment to the liver. Rat DCs at least partly
possess receptors for endocytosis of galactosylated antigens.
These DC receptors as well as Kupffer cell lectins are presumably
responsible for this binding.
Adaptive Regulation of Bile Salt Transporters in Kidney
and Liver in Obstructive Cholestasis in the Rat
JOHN LEE, FRANCESCO AZZAROLI, LIN WANG, CAROL J. SOROKA, ALESSANDRO
GIGLIOZZI, KENNETH D. R. SETCHELL, WERNER KRAMER, and JAMES L.
BOYER
Gastroenterology 2001 121: 1473-1484. Published online Nov 29
2001. Background & Aims: Cholestasis results
in adaptive regulation of bile salt transport proteins in hepatocytes
that may limit liver injury. However, it is not known if changes
also occur in the expression of bile salt transporters that reside
in extrahepatic tissues, particularly the kidney, which might
facilitate bile salt excretion during obstructive cholestasis.
Methods: RNA and protein were isolated from liver and kidney
14 days after common bile duct ligation in rats and assessed
by RNA protection assays, Western analysis, and tissue immunofluorescence.
Sodium-dependent bile salt transport was also measured in brush
border membrane vesicles from the kidney. Results: After
common bile duct ligation, serum bile salts initially rose and
then declined to lower levels after 3 days. In contrast,
urinary bile salt excretion rose progressively over the 2-week
period. By that time, the ileal sodium-dependent bile salt transporter
messenger RNA and protein expression in total liver had increased
to 300% and 200% of controls, respectively, while falling to 46%
and 37% of controls, respectively, in the kidney. Sodium-dependent
uptake of 3H-taurocholate in renal brush border membrane vesicles
was decreased. In contrast, the multidrug resistance-associated
protein 2 expression in the kidney was increased 2-fold,
even 1 day after ligation. Immunofluorescent studies confirmed
the changes in the expression of these transporters in liver and
kidney. Conclusions: These studies show that the molecular
expression of bile salt transporters in the kidney and cholangiocytes
undergo adaptive regulation after common bile duct obstruction
in the rat. These responses may facilitate extrahepatic pathways
for bile salt excretion during cholestasis.
CASE REPORTS:
Treatment of Vitamin D Deficiency Due to Crohn's Disease
With Tanning Bed Ultraviolet B Radiation
POLYXENI KOUTKIA, ZHIREN LU, TAI C. CHEN, and MICHAEL F. HOLICK
Gastroenterology 2001 121: 1485-1488. Published online Nov 29
2001.POLYXENI KOUTKIA, ZHIREN LU, TAI C. CHEN, and MICHAEL
F. HOLICK
Vitamin D, Skin, and Bone Research Laboratory, Department of Medicine, Endocrinology, Nutrition, and Diabetes Section, Boston University School of Medicine, Boston, Massachusetts
In Crohn's disease, severe skeletal demineralization, secondary
hyperparathyroidism, and muscle weakness can occur. This may be
caused by impaired vitamin D absorption, resulting from extensive
intestinal disease and resection of duodenum and jejunum, where
vitamin D is absorbed. We report a 57-year-old woman with a long
history of Crohn's disease and short-bowel syndrome who had only
2 feet of small intestine remaining after 3 bowel resections.
She was taking a daily multivitamin containing 400 IU of
vitamin D3 and was dependent on total parenteral nutrition that
contained 200 IU of vitamin D and calcium (18 mEq in
a 1-L bag infused over 8 hours daily) for a period of 36 months.
Despite the above replacement, she complained of bone pain and
muscle weakness, and she continued to be vitamin D-deficient with
a 25(OH)D level <20 ng/mL. She was then exposed to ultraviolet
B (UVB) radiation in a tanning bed wearing a 1-piece bathing suit
for 10 minutes, 3 times a week for 6 months at
the General Clinical Research Center, Boston University Medical
Center. She tolerated the irradiation well without evidence of
erythema. After 4 weeks, her serum 25(OH)D level increased
by 357% from 7 to 32 ng/mL, parathyroid hormone level
decreased by 52% from 92 to 44 pg/mL, and the serum
calcium level increased from 7.8 to 8.5 mg/dL. After
6 months of UVB treatment, her serum 25(OH)D level was maintained
in the normal range and was free of muscle weakness, and bone
and muscle pain.
SPECIAL REPORTS AND REVIEWS:
Molecular Aspects of Iron Absorption and HFE Expression
SEPPO PARKKILA, ONNI NIEMELÄ, ROBERT S. BRITTON, ROBERT E.
FLEMING, ABDUL WAHEED, BRUCE R. BACON, and WILLIAM S. SLY
Gastroenterology 2001 121: 1489-1496. Published online Nov 29
2001. Hereditary hemochromatosis, a disease of iron overload,
occurs in about 1 in 200-400 Caucasians. The gene mutated
in this disorder is termed HFE. The product of this gene,
HFE protein, is homologous to major histocompatibility complex
class I proteins, but HFE does not present peptides to T cells.
Based on recent structural, biochemical, and cell biological studies,
transferrin receptor (TfR) is a ligand for HFE. This association
directly links HFE protein to the TfR-mediated regulation of iron
homeostasis. Although evidence is accumulating that binding of
HFE to TfR is critical for the effects of HFE, the final pieces
in the HFE puzzle have not been established. This review focuses
on recent advances in HFE research and presents a hypothetical
model of HFE function.
Prescriptions for antiulcer drugs in Australia: volume,
trends, and costs
Johanna I Westbrook, Anne E Duggan, and Jean H McIntosh
BMJ 2001; 323: 1338-1339. [Full
text]
H2 receptor antagonists and proton pump inhibitors have markedly changed the management of peptic ulcer and gastro-oesophageal reflux disease; they have also changed the profile of national drug budgets. Antiulcer drugs have retained the leading position in drug sales worldwide: sales of antiulcer drugs were valued at $US12.9 billion (£8.6bn) in 1998 and were increasing at 3% a year.1
Since 1992 the Australian government's pharmaceutical
benefits scheme has required prescribers of proton pump inhibitors
to certify the presence of peptic ulcer disease or ulcerating
oesophagitis (confirmed by endoscopy, radiography, or surgery)
and refractory to treatment with other drugs, scleroderma oesophagus,
or Zollinger-Ellison syndrome. The aim of this study was to assess
how these restrictions have affected prescribing of antiulcer
drugs....
ABC of the upper gastrointestinal tract: Indigestion: When
is it functional?
Nicholas J Talley, Nghi Phung, and Jamshid S Kalantar
BMJ 2001; 323: 1294-1297.
[Full text]
Patients often complain of indigestion, but what do they mean?
Indigestion is an old English word that means lack of adequate
digestion, but patients and doctors interpret this in different
ways. Many patients mean heartburn or acid regurgitation, the
classic symptoms of gastro-oesophageal reflux disease. Some describe
belching, abdominal rumblings, or even bad breath as indigestion.
Others mean pain localised to the epigastrium or a non-painful
discomfort in the upper abdomen which may be described as fullness,
bloating, or an inability to finish a normal meal (early satiety).
Dyspepsia is best restricted to mean pain or discomfort centred
in the upper abdomen......
Naltrexone in the Treatment of Alcohol Dependence
John H. Krystal, M.D., Joyce A. Cramer, B.S., William F.
Krol, Ph.D., Gail F. Kirk, M.S., Robert A. Rosenheck, M.D., for
the Veterans Affairs Naltrexone Cooperative Study 425 Group
Background Although naltrexone, an opiate-receptor
antagonist, has been approved by the Food and Drug Administration
for the treatment of alcohol dependence, its efficacy is uncertain.
Methods We conducted a multicenter, double-blind, placebo-controlled
evaluation of naltrexone as an adjunct to standardized psychosocial
treatment. We randomly assigned 627 veterans (almost all men)
with chronic, severe alcohol dependence to 12 months of naltrexone
(50 mg once daily), 3 months of naltrexone followed by 9 months
of placebo, or 12 months of placebo. All patients were offered
individual counseling and programs to improve their compliance
with study medication and were encouraged to attend Alcoholics
Anonymous meetings. Results There were 209 patients in
each group; all had been sober for at least five days before randomization.
At 13 weeks, we found no significant difference in the number
of days to relapse between patients in the two naltrexone groups
(mean, 72.3 days) and the placebo group (mean, 62.4 days; 95 percent
confidence interval for the difference between groups, 3.0
to 22.8). At 52 weeks, there were no significant differences among
the three groups in the percentage of days on which drinking occurred
and the number of drinks per drinking day. Conclusions Our
findings do not support the use of naltrexone for the treatment
of men with chronic, severe alcohol dependence.
EDITORIAL (texte)
Treatment for alcohol dependence has been limited almost entirely to various types of counseling. An exception has been the use of the medication disulfiram, which acts indirectly by making a person feel ill if he or she drinks alcohol. The efficacy of disulfiram is limited, however, because compliance is often poor, and it is not widely used.
Counseling patients with alcoholism leads to rates of remission similar to those achieved with treatment of other chronic medical conditions, such as asthma.1 Nonetheless, the large number of people dependent on alcohol in the United States (over 8.1 million2) and the substantial costs of alcoholism to society - an estimated $185 billion and 100,000 deaths each year - make it imperative that treatment be improved. Thus, it is not surprising that reports in 19923,4 that the opiate antagonist naltrexone reduced the relapse rate in people dependent on alcohol generated substantial interest. The reports suggested that treatment could be improved through the use of medication in conjunction with counseling.
Since the initial report by Volpicelli et al.3 and the confirmation by O'Malley et al.,4 there have been additional randomized, placebo-controlled clinical trials of the effectiveness of naltrexone in treating alcoholism.5,6,7,8,9,10,11 Six5,6,7,8,9,10 found that naltrexone was effective in preventing relapse in compliant patients. The clinical end points varied. Four studies3,6,7,8 defined relapse as having five or more drinks on one occasion, having five or more drinking occasions in one week, or arriving at a clinic visit intoxicated (blood alcohol concentration above 100 mg per deciliter). Two studies4,5 used the time to the first day of heavy drinking as a measure of the time to relapse; one of these4 also used the time to any drinking. One study9 found a greater reduction in the amount of alcohol consumed and in the levels of -glutamyltransferase in patients who were compliant with the naltrexone regimen, whereas another10 found significantly fewer heavy drinking days and fewer drinks on the days patients drank.
A double-blind, placebo-controlled trial of another opioid antagonist, nalmefene, found that it also prevented relapse of heavy drinking.12 A controlled study of naltrexone, nefazodone, and placebo in 183 patients found no benefit from naltrexone; naltrexone was associated with more adverse events than placebo and more attrition from the study than nefazodone and placebo.11 Finally, a recent meta-analysis found that naltrexone was moderately effective in reducing alcohol consumption in alcoholics.13
In this issue of the Journal, Krystal and his colleagues
from the Veterans Affairs Naltrexone Cooperative Study 425 Group
report the results of a multicenter, double-blind, placebo-controlled
evaluation of naltrexone as an adjunct to standardized counseling
for alcohol dependence.14 In 627 veterans (almost all men), they
found no benefit from naltrexone, as measured by the time to relapse,
the percentage of days on which drinking occurred, or the number
of drinks per drinking day. Although the study by Krystal et al.
is larger than the previous studies, additional factors may explain
the discordant findings.
The typical patient in the study by Krystal et al. was about 10 years older than the patients in the previous studies (except for one study, in which the objective was to study naltrexone in older patients7). The typical patient had also been drinking for a longer period of time. Alcoholics who have families and are employed have a better prognosis than those who live alone or are unemployed. Only one third of the veterans in the study by Krystal et al. were married or living with a partner; these are smaller percentages than in most of the previous studies. Employment data are not given, but one third of the veterans were receiving disability pensions, a fact that may have affected their motivation to stop drinking. As Krystal et al. acknowledge, their results may not be generalizable to people who are not veterans, to women, or to patients whose dependence on alcohol is of shorter duration.
One of the early studies of naltrexone also involved patients treated at a Veterans Affairs hospital.1 The study was conducted at a single site, and for three months patients returned to the hospital daily for six to eight hours of rehabilitation activities. In the study by Krystal et al.,14 which involved multiple sites, patients received outpatient counseling for one hour per week for 16 weeks and then at a decreasing frequency for the remainder of a year. It is possible that in order to benefit from naltrexone, patients with more severe alcohol dependence require more intensive counseling.
The studies involving naltrexone also vary in the types of
counseling used in conjunction with the medication. Four of the
studies that showed a benefit4,5,6,8 used coping-skills therapy
or relapse-prevention training. These types of counseling are
commonly used in the treatment of alcoholism. In both, patients
are taught to identify situations or mood states that place them
at high risk for a relapse and are helped to develop coping skills
to reduce the probability of a relapse. Although a negative study11
also used a relapse-prevention approach, the preponderance of
the evidence suggests that this approach should be used in combination
with naltrexone. Coping-skills therapy is different from the 12-step
facilitation counseling used in the study by Krystal et al., which
encourages involvement in Alcoholics Anonymous.
As the value of any medication is being established, randomized clinical trials are not always consistent in their findings. Our institute is currently supporting a multicenter, placebo-controlled clinical trial of naltrexone and acamprosate, another medication for the treatment of alcoholism, alone or in combination in a younger group of patients (30 percent of whom were women) than those in the study by Krystal et al. The efficacy of acamprosate appears to be similar to that of naltrexone. It is not an opiate antagonist, although the precise mechanism of its action is not known. Acamprosate affects the activity of N-methyl-d-aspartate receptors, which are components of the glutamate system; the effects of alcohol are mediated to some extent by this system. At least 12 of 14 controlled clinical trials conducted in Europe support its effectiveness.15 Diarrhea may be a side effect of acamprosate but is usually not severe enough to require cessation of treatment. Acamprosate is approved for use in most European countries, several Latin American countries, and Australia. In the United States, acamprosate is under review by the Food and Drug Administration.
If additional studies find that naltrexone works, it will be
important to identify which patients are likely to benefit and
which are not. If no benefit is found, such results, coupled with
the results of the study by Krystal et al., would weigh against
the use of naltrexone as an adjunctive treatment for alcoholism.
Until we have more information, we recommend that physicians continue
to prescribe naltrexone for patients they think might benefit.
Such patients appear to be those who have been drinking heavily
for 20 years or less and have stable social support and living
situations.
Advances in our understanding of the neurobiology of alcohol dependence provide the foundation for developing new medications to treat the disorder. In addition to the opioid system, preclinical studies have shown that alcohol affects neurotransmitters in the brain, including dopamine, serotonin, glutamate, -aminobutyric acid, and norepinephrine. Second-messenger systems, such as the isoform of protein kinase C and the hypothalamicpituitaryadrenal axis, are involved in problem drinking. The hypothalamicpituitaryadrenal axis also has a pivotal role in stress. A number of compounds affecting these systems have shown efficacy in reducing alcohol consumption in studies in animals. They include an N-methyl-d-aspartate agonist, a compound that is both a serotonin 1Areceptor agonist and a serotonin 2receptor antagonist, and a corticotropin-releasingfactor antagonist. At the clinical level, a recent trial indicated that ondansetron, a selective serotonin 3receptor antagonist,16 shows promise for the treatment of people who become dependent on alcohol before the age of 25 years. Because so many new approaches seem promising, we are optimistic that more effective medications will be found.
Richard K. Fuller, M.D.
Enoch Gordis, M.D.
National Institute on Alcohol Abuse and Alcoholism
Bethesda, MD 20892
Effect on treatment outcome of coinfection with SEN viruses
in patients with hepatitis C [Full
Text]
Basil Rigas, Izhar Hasan, Raja Rehman, Peter Donahue, Knut M Wittkowski,
Edward Lebovics
The newly discovered SEN D and SEN H viruses are transmitted parenterally
and can cause post-transfusion hepatitis. We assessed whether
coinfection of patients with chronic hepatitis C and SEN D or
SEN H correlates with the outcome of treatment with interferon
and ribavirin. Of 31 patients with hepatitis C studied, six were
positive for SEN D and seven for SEN H (one was positive for both).
All of those positive for SEN D and five of those positive for
SEN H failed to respond to therapy. Overall response (RNA titre
and alanine aminotransferase concentration after treatment) was
lower in SEN-infected patients than uninfected patients (p=0·025).
We conclude that coinfection with SEN viruses is frequent in chronic
hepatitis C patients and might adversely affect the outcome of
treatment with interferon and ribavirin.
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