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1 hol-related liver disease (previously termed alcoholic liver disease).
2 nce as an early protective mechanism against alcoholic liver disease.
3 guing for an early protective effect against alcoholic liver disease.
4 to the pathogenesis of early stages of human alcoholic liver disease.
5 olymorphisms were evaluated in patients with alcoholic liver disease.
6 well as in liver biopsies from patients with alcoholic liver disease.
7 potential implication in the pathogenesis of alcoholic liver disease.
8 ent compared to counterparts with HCV and/or alcoholic liver disease.
9 dition developed in patients with underlying alcoholic liver disease.
10 162 (53.5%) patients had NASH and HCV and/or alcoholic liver disease.
11 serve as a potential therapeutic option for alcoholic liver disease.
12 effective therapeutics for the treatment of alcoholic liver disease.
13 terial overgrowth is common in patients with alcoholic liver disease.
14 products into the circulation contributes to alcoholic liver disease.
15 etween inflammation and hepatic steatosis in alcoholic liver disease.
16 to be an important factor in the etiology of alcoholic liver disease.
17 ulation by mucosal antimicrobial proteins in alcoholic liver disease.
18 and attenuate the steatosis associated with alcoholic liver disease.
19 HO-1 may be a useful therapeutic strategy in alcoholic liver disease.
20 developed as therapeutics for patients with alcoholic liver disease.
21 on has a central role in the pathogenesis of alcoholic liver disease.
22 tal metabolic disorder in the progression of alcoholic liver disease.
23 for the development of therapeutics to treat alcoholic liver disease.
24 m has been implicated in the pathogenesis of alcoholic liver disease.
25 ed biochemical/nutritional manifestations of alcoholic liver disease.
26 pplementation may have beneficial effects in alcoholic liver disease.
27 c cellular proliferation in a mouse model of alcoholic liver disease.
28 onships will guide hepatologists in managing alcoholic liver disease.
29 cs, detection, pathogenesis and treatment of alcoholic liver disease.
30 implicated in several pathologies, including alcoholic liver disease.
31 diseases including chronic HCV infection and alcoholic liver disease.
32 gy, pathogenesis, prognosis and treatment of alcoholic liver disease.
33 ons may be implicated in the pathogenesis of alcoholic liver disease.
34 ular SAH as potential therapeutic options in alcoholic liver disease.
35 tabolism and abnormal TNFalpha metabolism in alcoholic liver disease.
36 characteristic damage to hepatocytes seen in alcoholic liver disease.
37 or other approaches may be useful to prevent alcoholic liver disease.
38 alpha) is associated with the development of alcoholic liver disease.
39 for many of the dysfunctions associated with alcoholic liver disease.
40 ndotoxin plays a role in the pathogenesis of alcoholic liver disease.
41 nsaturated fat and iron, plays a key role in alcoholic liver disease.
42 l has been implicated in the pathogenesis of alcoholic liver disease.
43 in patients with type I hyperlipidemias and alcoholic liver disease.
44 ho were more likely to have the diagnosis of alcoholic liver disease.
45 r proteins may contribute to liver injury in alcoholic liver disease.
46 on, and pathological changes in experimental alcoholic liver disease.
47 tors on pathological changes in experimental alcoholic liver disease.
48 otein modification in rats with experimental alcoholic liver disease.
49 dothelial cell proliferation in experimental alcoholic liver disease.
50 provements in chronic outcomes, particularly alcoholic liver disease.
51 of hepatic steatosis markers in experimental alcoholic liver disease.
52 tic steatosis is an initial manifestation of alcoholic liver disease.
53 ) of deaths from suicide, drug overdose, and alcoholic liver disease.
54 cial in the prevention or treatment of human alcoholic liver disease.
55 lyceride accumulation, a hallmark feature of alcoholic liver disease.
56 ic hepatitis (AH) is the most severe form of alcoholic liver disease.
57 ts common genetic variant is associated with alcoholic liver disease.
58 s are available for noninvasive diagnosis of alcoholic liver disease.
59 P2B10 that may contribute to the etiology of alcoholic liver disease.
60 r each model, not shared with advanced human alcoholic liver disease.
61 e mucosal barrier facilitates progression of alcoholic liver disease.
62 olic hepatitis (AH), the most severe form of alcoholic liver disease.
63 rrhotic and precirrhotic stages of NAFLD and alcoholic liver disease.
64 novel therapeutic options for patients with alcoholic liver disease.
65 l on monocytes and macrophages contribute to alcoholic liver disease.
66 driving immune impairments in patients with alcoholic liver disease.
67 th much smaller contributions from NAFLD and alcoholic liver disease.
68 model for end-stage liver disease score, and alcoholic liver disease.
69 thanol-induced liver injury in patients with alcoholic liver disease.
70 of patients had been transplanted because of alcoholic liver disease.
71 the microbiome contribute to pathogenesis of alcoholic liver disease.
72 of methylation-associated miRNA, miR-34a, in alcoholic liver diseases.
73 in HCV patients but not in alcoholic and non-alcoholic liver diseases.
74 with potential therapeutic benefits in human alcoholic liver diseases.
75 sociated with the development/progression of alcoholic liver diseases.
76 s of patients is recognized as a hallmark of alcoholic liver diseases.
77 s (HCV), hepatitis B virus (HBV), NAFLD, and alcoholic liver diseases; (2) performance of specific VC
79 of 60 years or older (17% [$32795]; P=.01); alcoholic liver disease (26% [$49596]; P=.002); Child-Pu
80 (PSC), 6 with non-A, non-B hepatitis, 6 with alcoholic liver disease, 4 with cryptogenic cirrhosis, 4
81 Etiologies for liver disease included non-alcoholic liver disease (58.0%), hepatitis C (26.0%), he
82 minant causes of alcohol-related deaths were alcoholic liver disease (65.1%), fibrosis and cirrhosis
83 angitis (SMR 11.0-4.2), and deterioration in alcoholic liver disease (8.3-24.0) and acute liver failu
84 hosis (adjusted odds ratio, 27.2; P <.0001), alcoholic liver disease (adjusted odds ratio, 7.4; P <.0
85 Recidivism after liver transplantation for alcoholic liver disease adversely impacts long-term surv
86 , i.e. non-alcoholic steatohepatitis (NASH), alcoholic liver disease (ALC), and hepatitis C virus (HC
89 g components and its inhibitory factors in 9 alcoholic liver disease (ALD) and 8 healthy control live
91 ethanol consumption, which also occurred in alcoholic liver disease (ALD) and in cirrhosis patients,
92 d hepcidin expression is a common feature in alcoholic liver disease (ALD) and in mouse models of eth
93 her CES1 played a role in the development of alcoholic liver disease (ALD) and methionine and choline
94 s significant overlap in the pathogenesis of alcoholic liver disease (ALD) and NAFLD, although studie
97 e model will be very useful for the study of alcoholic liver disease (ALD) and of other organs damage
98 vidence suggests that innate immunity drives alcoholic liver disease (ALD) and that the interferon re
99 Nonalcoholic fatty liver disease (NAFLD) and alcoholic liver disease (ALD) are common causes of chron
101 onic, excessive alcohol consumption leads to alcoholic liver disease (ALD) characterized by steatosis
106 s have had limited utility in distinguishing alcoholic liver disease (ALD) from nonalcoholic fatty li
109 It has been suggested that patients with alcoholic liver disease (ALD) have more impaired cogniti
110 ecords, the underlying CLD was attributed to alcoholic liver disease (ALD) in 44% of deaths, HCV infe
111 erally thought to promote the development of alcoholic liver disease (ALD) in alcoholics by releasing
120 nonalcoholic fatty liver disease (NAFLD) and alcoholic liver disease (ALD) is still unsettled, but es
121 eintegration was administered by phone to 84 alcoholic liver disease (ALD) OLTX recipients (ALDs) and
123 tion of ACSS2-mediated epigenetic control in alcoholic liver disease (ALD) remains incompletely under
126 absence of transplantation for patients with alcoholic liver disease (ALD) to assess survival benefit
127 s-species comparison was performed using the alcoholic liver disease (ALD) transcriptomic public data
128 observation in 1911 on the histopathology of alcoholic liver disease (ALD) was the first identificati
129 lic hepatitis (AH) is a distinct spectrum of alcoholic liver disease (ALD) with intense neutrophilic
130 izes endotoxin, a trigger of inflammation in alcoholic liver disease (ALD), activates two signaling p
131 trahepatic complications of viral hepatitis, alcoholic liver disease (ALD), and nonalcoholic fatty li
132 itis C virus (HCV), hepatitis B virus (HBV), alcoholic liver disease (ALD), and other liver disease u
133 an attractive vertebrate model for studying alcoholic liver disease (ALD), because they possess the
134 in-6 (IL-6) levels is always associated with alcoholic liver disease (ALD), but the significance of s
135 lammation in immune cells in mouse models of alcoholic liver disease (ALD), drug (acetaminophen, APAP
136 ith hepatitis C virus (HCV) infection, NASH, alcoholic liver disease (ALD), or a combination of HCV i
137 ological consequences for the development of alcoholic liver disease (ALD), the underlying mechanisms
138 AM), betaine, and folate in the treatment of alcoholic liver disease (ALD), which was organized by th
157 hibitor use increases the risk of developing alcoholic liver disease among alcohol-dependent patients
159 hemokines in liver tissue from patients with alcoholic liver disease and a range of disease control s
160 ies often utilize samples from patients with alcoholic liver disease and are confounded by variabilit
161 738409 in PNPLA3 is strongly associated with alcoholic liver disease and clinically evident alcoholic
163 stically significant association between non-alcoholic liver disease and FLI-based ultrasound (p < 0.
164 mplications for the liver injury observed in alcoholic liver disease and genetic hemochromatosis in c
170 Inroads are being made into the genetics of alcoholic liver disease and new phenomena are being unco
171 eases that include hepatitis B, hepatitis C, alcoholic liver disease and non-alcoholic steatohepatiti
172 d bacterial translocation in liver fibrosis, alcoholic liver disease and non-alcoholic steatohepatiti
174 variation in the progression and outcomes of alcoholic liver disease and nonalcoholic fatty liver dis
175 ctors that contribute to the pathogenesis of alcoholic liver disease and nonalcoholic fatty liver dis
176 tary and alternative medicine agents in both alcoholic liver disease and nonalcoholic steatohepatitis
177 in liver tissues from patients with advanced alcoholic liver disease and nonalcoholic steatohepatitis
178 IL-8 levels and were higher in patients with alcoholic liver disease and parenchymal neutrophil infil
179 r dietary fatty acids in the pathogenesis of alcoholic liver disease and provide a promising therapeu
180 ed 55 to 64 years, primarily attributable to alcoholic liver disease and psychiatric disorders due to
181 apidly through drug overdoses, suicides, and alcoholic liver disease and when the decline in mortalit
182 e the candidate to liver transplantation for alcoholic liver diseases and severe acute alcoholic hepa
183 aine have shown efficacy in animal models of alcoholic liver disease, and "knockout" mice that develo
184 ients with cured HCV, 1.32% in patients with alcoholic liver disease, and 1.24% in patients with NAFL
187 y cirrhosis, primary sclerosing cholangitis, alcoholic liver disease, and chronic hepatitis C), and h
190 ng human liver after submassive necrosis, in alcoholic liver disease, and in focal nodular hyperplasi
191 sative stress are key to the pathogenesis of alcoholic liver disease, and there is now greater emphas
194 ne system and the mechanisms of apoptosis in alcoholic liver disease are better appreciated, especial
195 nalcoholic fatty liver diseases (NAFLD); and alcoholic liver disease, are a leading cause of morbidit
196 ontaining liquid diet for 6 months developed alcoholic liver disease as measured by serum alanine tra
198 ve therapeutic potential in the treatment of alcoholic liver diseases associated with inflammation, o
200 evious malignancy (HR, 1.34; P < 0.001), and alcoholic liver disease, autoimmune, nonalcoholic steato
201 ghts are being made into the pathogenesis of alcoholic liver disease but safe and effective therapies
202 There have been no treatment advances for alcoholic liver disease but, on balance, steroids are st
203 sidered independent risk factors involved in alcoholic liver disease, but mutual relationships or int
204 n to occur in both experimental and clinical alcoholic liver disease, but the signaling pathway remai
205 thionine cycle, its deficiency could promote alcoholic liver disease by enhancing ethanol-induced per
206 n diseases, such as AIDS, Alzheimer disease, alcoholic liver disease, cardiovascular disease, diabete
207 hs and diseases including alcohol addiction, alcoholic liver disease, cardiovascular disease, diabete
208 important role in non-HHC diseases, such as alcoholic liver disease, chronic viral hepatitis, and po
209 mellitus, atherosclerosis, alcoholic and non-alcoholic liver disease, cirrhosis, hepatocellular carci
210 cysts, hepatitis B virus, hepatitis C virus, alcoholic liver disease, cirrhosis, inflammatory bowel d
214 bowel disease, hepatitis B, alcoholism, and alcoholic liver disease did not reduce the risk for ICC
215 a potential therapeutic option to ameliorate alcoholic liver disease, due to its antioxidant, antiapo
216 ic hepatitis (AH) is the most severe form of alcoholic liver disease for which there are no effective
219 rated fatty acids against the development of alcoholic liver disease has long been known, but the und
222 group (uninsured Hispanic men with viral or alcoholic liver disease) has not been reached through ed
223 from fully alcohol-attributable causes (eg, alcoholic liver disease) have increased in the past deca
224 nt indications for liver transplantation are alcoholic liver disease, hepatocellular carcinoma, and v
225 including nonalcoholic fatty liver disease, alcoholic liver disease, HIV/HCV co-infection and primar
226 4; 95% confidence interval [CI], 1.01-1.08), alcoholic liver disease (HR, 1.66; 95% CI, 1.02-2.71), a
229 Complement is involved in the development of alcoholic liver disease in mice; however, the mechanisms
230 e disrupts SIRT1 activity and contributes to alcoholic liver disease in rodents, but the exact pathog
231 untries, but the opposite is true elsewhere; alcoholic liver disease is a considerable burden worldwi
243 and clinical research into the mechanisms of alcoholic liver disease is making headway, but has yet t
247 is seen in the nonalcoholic steatohepatitis, alcoholic liver disease, ischemia/reperfusion injury, an
248 ften insufficient in chronic hepatitis C and alcoholic liver disease, leading to hyperabsorption of i
249 r HCC (hepatitis B virus, hepatitis C virus, alcoholic liver disease, liver cirrhosis, biliary cirrho
250 g M2 polarization during the early stages of alcoholic liver disease may represent an attractive stra
251 teatosis and steatohepatitis associated with alcoholic liver disease, metabolic dysfunction-associate
252 rrhotic patients with chronic hepatitis C or alcoholic liver disease (n = 1121), the T allele was ind
253 tis (n=81), hepatitis C virus (HCV) (n=945), alcoholic liver disease (n=495), alcohol and HCV (n=152)
256 roton pump inhibitors promote progression of alcoholic liver disease, non-alcoholic fatty liver disea
257 llowing chronic liver inflammation including alcoholic liver disease, non-alcoholic steatohepatitis,
258 cated in the pathogenesis of renal fibrosis, alcoholic liver disease, non-alcoholic steatohepatitis,
259 ed to influence histological liver damage in alcoholic liver disease, nonalcoholic fatty liver diseas
260 , occurring in 11 patients (31 percent), and alcoholic liver disease, occurring in 5 (13 percent).
261 Subjects were composed of 24 patients with alcoholic liver disease of whom 15 had histopathological
263 cidin expression, e.g., chronic hepatitis C, alcoholic liver disease, or hereditary hemochromatosis.
264 atients with primary sclerosing cholangitis, alcoholic liver disease, or nonalcoholic steatohepatitis
266 or C virus infection, autoimmune hepatitis, alcoholic liver disease, or without these diseases (cont
267 ular disease was significant only in PBC and alcoholic liver disease, owing to high mortality in the
269 relapse is common after liver transplant in alcoholic liver disease patients and can lead to worse o
274 nts with gram-negative bacterial infections, alcoholic liver disease (relative risk [RR] 4.87, 95% CI
275 by intestinal dysbiosis, and development of alcoholic liver disease requires gut-derived bacterial p
277 ethyltransferase activity is associated with alcoholic liver disease, resulting in phosphatidylcholin
279 used the intragastric feeding rat model for alcoholic liver disease to investigate the relationship
280 rite guidelines on Liver Transplantation for Alcoholic Liver Disease to summarize current knowledge a
281 patients with compensated and decompensated alcoholic liver disease, to test the hypothesis that alc
282 ucers of oxidative stress and key factors in alcoholic liver disease, to up-regulate alpha 2 collagen
285 oles of EVs in nonalcoholic steatohepatitis, alcoholic liver disease, viral hepatitis, cholangiopathi
286 This increase in risk is independent of alcoholic liver disease, viral hepatitis, or demographic
288 etabolism is involved in the pathogenesis of alcoholic liver disease was strengthened by our previous
292 titis B or C virus, autoimmune hepatitis, or alcoholic liver disease, we detected increased nuclear t
294 play an etiologic role in the initiation of alcoholic liver disease, we had earlier pioneered the de
295 te in promoting pathological liver injury in alcoholic liver disease, we investigated the role of LBP
296 l and polyunsaturated fatty acids (PUFAs) to alcoholic liver disease, we investigated whether chronic
297 es, use of 3.0 T, presence of cirrhosis, and alcoholic liver disease were all significantly associate
298 2E1 (CYP2E1) is suggested to play a role in alcoholic liver disease, which includes alcoholic fatty
300 a key role in the genesis and progression of alcoholic liver disease with ethanol exposure enhancing