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1. II: The Effects of Recombinant Human Insulin-Like Growth Factor-1 on Immunological Recovery in the Malnourished Alcoholic Rat

Author

C L, Mendenhall, G A, Roselle, C J, Grossman, and P, Gartside

Subjects
Alcohol Drinking, T-Lymphocytes, Body Weight, Immunity, Nutritional Status, Medicine (miscellaneous), Feeding Behavior, Thymus Gland, Toxicology, Protein-Energy Malnutrition, Recombinant Proteins, Nutrition Disorders, Rats, Alcoholism, Disease Models, Animal, Psychiatry and Mental health, Rats, Inbred Lew, Animals, Insulin-Like Growth Factor I, Energy Intake, Spleen
Abstract

Immunological abnormalities are frequently observed in alcoholics with severe liver disease and are typically in association with immune abnormalities. Concomitantly, serum levels of insulin-like growth factor-1 (IGF-1) are frequently very low in these patients. Because IGF-1 is known to modulate both nutrition and immune status, the present study was undertaken to evaluate an in vivo rat model of alcoholism and malnutrition, the possibility of a therapeutic application for IGF-1.Controlled injury was induced by 14 days of calorie restriction and alcohol feeding that resulted in a 9% loss of body mass. Changes were compared with normal unrestricted control rats that gained 28% above their pretreatment body mass during the same period. Immunological impairment was assessed using thymus and spleen mass, cellularity and spleen T-lymphocyte function. Recovery was evaluated after 28 days of treatment using various combinations of: (1) high calorie intake, (2) cessation from alcohol feeding, and (3) IGF-1.The thymus was most severely affected, losing 52.3% of its mass and 55.7% of its cellularity. The spleen was diminished, losing 31.2% of its mass and 41.9% of its cellularity. All of the spleen T-lymphocyte subsets were diminished, with CD5 affected the least (37.1 %) and CD8 affected the most severely (51.7%). During recovery, only the group treated with high calorie intake, no alcohol intake, and IGF-1 (group 8) had complete restoration of all immunological parameters, including a recovery of T-lymphocyte function. Continuous consumption of alcohol, even in the presence of high calories and IGF-1, produced an incomplete recovery.Cessation of alcohol coupled with high calorie nutrition and IGF-1 treatment produced an accelerated improvement in host immunity. These animal studies suggest that IGF-1 is efficacious for this condition and supports the need for additional clinical studies.

Published
1997
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2. A simple, rapid method for measurement of acetate in tissue and serum.

Author

R G Richards, C L Mendenhall, and J MacGee

Subjects
Biochemistry, QD415-436
Abstract

A simple and rapid method is described for determining the free acetate concentration in liver and serum. After extraction, the acetate is converted to its benzyl ester by thermal degradation of its benzyldimethylphenylammonium salt in the vaporizer of a gas chromatography. Good quantitation is achieved in the range of 0.033-2.5 mumoles of acetate per gram of liver or per milliliter of serum.

Published
1975
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3. Diagnostic status and treatment recommendations for Persian Gulf War Veterans with multiple nonspecific symptoms

Author

D G, Baker, I G, McQuarrie, M G, Murray, L M, Lund, B A, Dashevsky, and C L, Mendenhall

Subjects
Adult, Male, Middle East, Warfare, Statistics as Topic, Humans, Female, Persian Gulf Syndrome, Health Surveys, United States, Veterans
Abstract

Unexplained symptoms have frequently been observed in deployed Persian Gulf War veterans (GWVs). Using factor analysis, the Centers for Disease Control and Prevention (CDC) has established criteria for Gulf War illness (GWI). We report here on the prevalence of GWI, identify comorbidities, and compare these with those of veterans without GWI.GWVs who consented to complete questionnaires and laboratory measures were given complete physical and mental health examinations. Outcome measures included CDC criteria for GWI, the Medical Outcomes Study Short Form 36 (SF-36), clinical and laboratory evaluations, and structured psychiatric interviews.One hundred twenty GWVs were enrolled, and 89 received complete physical and mental health examinations; 83% met CDC criteria for GWI. Veterans with GWI (1) were older, (2) reported more combat exposure, (3) scored higher on measures of depression, post-traumatic stress disorder, and fibromyalgia, and (4) had poorer health-related quality of life. More than half had anxiety or depressive disorders, and 93% had at least one medical and/or psychiatric diagnosis. The SF-36 predicted mental health status with a positive predictive value of 81.58. By adding the Hamilton D rating for depression, the positive predictive value increased to 88.57.The CDC criteria accurately identified GWVs negative for GWI. Most GWVs were positive for GWI. Neither CDC criteria nor CDC severity rankings distinguish between veterans with psychiatric syndromes and those without: both groups endorsed the same symptoms. More than half of those with GWI had a treatable anxiety or depressive disorder. The SF-36 was a valid predictor of mental health status, particularly when paired with the Hamilton depression interview.

Published
2001

4. The antigenic heterogeneity of the bile duct epithelium in alcoholic liver disease. VA Cooperative Study Group 275

Author

A, Chedid, C L, Mendenhall, and T E, Moritz

Subjects
Male, Antibodies, Monoclonal, Humans, Bile Ducts, Antigenic Variation, Liver Diseases, Alcoholic, Epithelium
Abstract

The chronic alcoholic patient is usually immunosuppressed, but the significance of this phenomenon in terms of bile duct injury is unclear. The immunoreactivity of the bile duct cells was examined in a series of 69 frozen liver biopsy specimens obtained from patients with alcoholic liver disease, comprising 29 cases of cirrhosis, 26 of alcoholic hepatitis, 10 cases of alcoholic fatty liver, and 4 specimens from normal livers. Liver diseases such as primary biliary cirrhosis and human hepatic allograft rejection, known to have an autoimmune basis, share the characteristic feature of damage to the bile duct epithelial cells. In both instances the damage seems to be immune mediated, but the nature of the antigens involved is not established. We used the avidin-biotin-peroxidase complex method to test in alcoholic liver disease for the expression of a battery of surface antigen markers that have been incriminated in tissue injury and are usually present in lymphoid cells but also expressed by epithelium. In this study we investigated the expression of the following molecules: HLA class I (ABC) and class II (HLA-DR, HLA-DP, HLA-DQ), CD29, CD45RA, CD45RO, CD56, interleukin 1 (IL-I), IL-2, IL-4, interferon (IFN-gamma), tumor necrosis factor beta, and transforming growth factor beta1 (TGF-beta1). The bile duct epithelial cells strongly expressed HLA-ABC in all cases, CD56 in 47 of 55, IL-4 in 15 of 41, TGF-beta1 in 14 of 25, and CD29 in 4 of 25 cases. The other markers including IFN-gamma, HLA-DR, HLA-DP, and HLA-DQ were not expressed by bile duct cells. The expression of HLA class I agrees with previous observations while the absence of class II expression does not. The expression by the bile duct epithelium of CD56 confirms our own previous report. A new observation is the finding of molecules such as IL-4, TGF-beta1, and CD29 strongly expressed in the bile ducts cells. The presence of these molecules, taken together with the lack of IFN-gamma expression, contradicts previous speculations that attributed to IFN-gamma a role in the induction of major histocompatibility antigens and adhesion molecules in immune-mediated alcoholic liver disease.

Published
1999

5. Host response to mycobacterial infection in the alcoholic rat: male and female dimorphism

Author

X, Li, C J, Grossman, C L, Mendenhall, P, Hurtubise, S D, Rouster, G A, Roselle, and P, Gartside

Subjects
CD4-Positive T-Lymphocytes, Male, Mycobacterium Infections, Ethanol, Body Weight, CD4-CD8 Ratio, CD8-Positive T-Lymphocytes, Mycobacterium bovis, Rats, Rats, Sprague-Dawley, Alcoholism, T-Lymphocyte Subsets, Immune System, Animals, Female, Lymphocyte Count, Spleen
Abstract

Increased susceptibility to tuberculosis occurs in the alcoholic. One explanation for the altered susceptibility is a change in T-lymphocyte modulation. To evaluate this, 24 male and 24 female Sprague-Dawley rats were treated with either a Lieber-type liquid ethanol diet (LED) or an isocaloric control (LCD). After 2 weeks, half the subjects were infected with BCG (10(8) colony-forming units) and sacrificed after 42 days. Splenic helper (CD4) and suppressor/cytoxic (CD8) cells were quantitated by flow cytometry. By three-way analysis of variance, splenic cellularity was significantly increased by infection (p0.0001) but suppressed by LED (p = 0.0002). There was a marginal sexual difference (p = 0.065) with females exhibiting a 35% lower response while on alcohol. Examining lymphocyte subsets, the most significant changes were observed after infection (BCG) and alcohol treatment (LED). CD4 levels were diminished by LED (p = 0.0002) but markedly increased by infection (p0.0001), producing a highly significant interaction that affected both absolute number (p0.0001) and relative percent present (p = 0.0078). CD8 was influenced only by infection (p0.0001). This resulted in a infection-related increase in the CD4/CD8 ratio which was lower with LED (p = 0.0032). Splenic T-lymphocytes, predominately CD4, are involved in the host response to BCG hepatitis and are adversely influenced by LED, which may contribute to increased susceptibility.

Published
1998

6. A four-year review of patients with hepatitis C antibody in Department of Veterans Affairs facilities

Author

G A, Roselle, L H, Danko, and C L, Mendenhall

Subjects
United States Department of Veterans Affairs, Seroepidemiologic Studies, Incidence, Population Surveillance, Humans, Hepatitis C Antibodies, Hepatitis C, United States, Veterans
Abstract

Hepatitis C virus [HCV] has recently been recognized as an emerging pathogen of surprising proportions. The clinical liver illness associated with HCV infection can be minimal or none, but in a notable number of persons it can ultimately cause debilitating chronic liver disease, fibrosis, cirrhosis, and hepatic failure, and it is likely related to an increased incidence of hepatocellular carcinoma. From 1991 to 1994, an annual electronic census was sent to 168 Veterans Health Administration facilities requesting serologic data on HCV in patients seen in Department of Veterans Affairs facilities. Response rate to the mandatory survey was 100%. In 1991, 6,612 individual patients were reported as positive for HCV antibody in the Department of Veterans Affairs system. This increased yearly from 1992 to 1994 with 8,365, 14,097, and finally 18,854 persons, respectively. This represents an increase of more than 285% during the 4-year period. Increases in HCV antibody for the same period were seen in all major regions of the United States and in the specified large metropolitan areas. In the New York area and in coastal California, this trend of new case identification may have plateaued during 1993 and 1994. Overall, total patients seen nationally in the Veterans Health Administration increased by only 4.87% during the same period, 1991 to 1994. Thus, the increase in persons positive for HCV antibody is not based on work load alone. The impact of HCV disease on patient well-being and health care costs cannot be overestimated.

Published
1997

7. Relationship between posttraumatic stress disorder and self-reported physical symptoms in Persian Gulf War veterans

Author

D G, Baker, C L, Mendenhall, L A, Simbartl, L K, Magan, and J L, Steinberg

Subjects
Adult, Male, Stress Disorders, Post-Traumatic, Middle East, Warfare, Surveys and Questionnaires, Odds Ratio, Humans, Female, Psychophysiologic Disorders, Veterans
Abstract

While prior studies show that combat veterans with posttraumatic stress disorder (PTSD) report more physical symptoms than veterans without PTSD, the link between PTSD and somatic complaints in Persian Gulf War veterans (PGWVs) is yet to be evaluated.A questionnaire booklet was completed by 188 PGWVs, of whom half were patients in a veterans health screening clinic and half were non-treatment-seeking volunteers on active duty. The booklet included the Combat Exposure Scale, the Mississippi Post-Traumatic Stress Disorder Scale (MPTSD), and a subjective symptom-based health questionnaire.The 24 PGWVs (12.8%) with PTSD (MPTSD scoreor = 116) reported more combat exposure (P = .02) and a greater number of physical symptoms (P = .001) than other PGWVs. Fatigue, nausea, muscle aches, dizziness, back pain, stomach ache, and numbness were much more likely to be reported by those with PTSD (MPTSD scoreor = 116) than by those without PTSD (MPTSD scoreor = 95).Physicians examining PGWVs should be alert to the possibility of PTSD in this group and that those with PTSD are more likely to report physical symptoms that may overlap with those in Persian Gulf syndrome. Consequently, mental health screening is essential, since for those veterans with PTSD diagnosis of other coexisting conditions may be confounded and early effective treatment of their PTSD may be delayed. Also, given the increased reporting of certain symptoms by those with PTSD, those seeking the cause of Persian Gulf syndrome should control for PTSD when determining the symptom cluster that may constitute this condition.

Published
1997

8. Effects of recombinant human insulin-like growth factor-1 and recombinant human growth hormone on anabolism and immunity in calorie-restricted alcoholic rats

Author

C L, Mendenhall, G A, Roselle, P, Gartside, and C J, Grossman

Subjects
Male, Dose-Response Relationship, Drug, Human Growth Hormone, T-Lymphocytes, Lymphocyte Activation, Protein-Energy Malnutrition, Recombinant Proteins, Rats, Rats, Sprague-Dawley, Alcoholism, Growth Hormone, Animals, Humans, Insulin-Like Growth Factor I, Energy Intake, Energy Metabolism
Abstract

Patients with severe alcoholic liver injury exhibit very low serum insulin-like growth factor-1 (IGF-1) concentrations, along with many of the symptoms that might occur with an IGF-1 deficiency state (including severe protein calorie malnutrition and immunosuppression). This study was performed to assess the effects of recombinant human (rh) IGF-1 and/or rh growth hormone (rhGH) on anabolism and immunity in the calorie-restricted, immunosuppressed alcoholic rat.Undernutrition was induced by calorie restriction such that each animal consumed 40% of ad libitum-fed controls. Alcohol was administered orally in the diet such that the mean daily intake was 9.4 g/kg/day. rhIGF-1 was administered by continuous subcutaneous infusion (380 micrograms/day) using a 14-day miniosmotic pump; rhGH was given by subcutaneous injections (400 micrograms/day). Matching placebo groups were also studied.On this regimen, ad libitum-fed controls were well nourished and increased body weight 34%, whereas Restricted controls lost 7.7% and Restricted alcohol-fed rats lost 15.2%. Significant but incomplete reversal of undernutrition was achieved with hormone therapy. Best improvement was obtained with combined therapy: rhIGF-1 + rhGH (p0.005; placebo versus active treatments). Immunologic impairment was observed to be severe in both thymus and spleen. The most severe changes were seen in thymi of the calorie-restricted, alcohol-fed rats, wherein 98% of the T lymphocytes were lost. rhIGF-1 treatment, but not rhGH, produced significant improvements in thymus. This was most pronounced in control rats (p0.005). Splenic T lymphocytes were less impaired and were more responsive to rhIGF-1 treatment; there was a maximum loss of 71% of T cells in Restricted, alcohol-fed rats. rhIGF-1 treatment completely restored splenic cellularity, as well as each of the T lymphocytes studied: CD5, CD4, and CD8. Functional status of splenic T lymphocytes was assessed by blast transformation after concanavalin A stimulation. Calorie restriction did not impair significantly this function in controls [Lieber-DeCarli control diet (LCD)]. However, it was significantly impaired in the Restricted, alcohol-fed rats (p = 0.003). In the presence of continued calorie restriction and alcohol, this function was not restored with either hormone (rhIGF-1 and/or rhGH). Their role in facilitating functional recovery after calories is restored, and alcohol is discontinued is under investigation.

Published
1997

9. Human hepatocyte growth factor in alcoholic liver disease: a comparison with change in alpha-fetoprotein. Department of Veterans Affairs Cooperative Study Group 275

Author

C L, Mendenhall, F, Roos, T E, Moritz, G A, Roselle, A, Chedid, C J, Grossman, S D, Rouster, G L, Bennett, and J R, Lake

Subjects
Male, Liver, Hepatitis, Alcoholic, Hepatocyte Growth Factor, Liver Cirrhosis, Alcoholic, Humans, Nutritional Status, alpha-Fetoproteins, Middle Aged, Energy Intake, Liver Diseases, Alcoholic, Severity of Illness Index, Liver Regeneration
Abstract

To evaluate the hepatic regenerative response in patients with alcoholic liver disease, sera from 263 patients with severe alcoholic hepatitis and/or cirrhosis were analyzed for hepatocyte growth factor (HGF) and alpha-fetoprotein (AFP). HGF concentration was elevated above healthy controls in 95% of the patients (median level = 2.4 ng/ml), whereas AFP tended to be depressed below controls (median level = 4.1 ng/ml). Correlations with parameters of liver injury (i.e., ascites, encephalopathy, AST bilirubin, and protime) all showed a more significant correlation with HGF concentrations than those of AFP. Patients with HGF levels below the mean (4 ng/ml) exhibited significantly better survival (median survival = 35 months vs. 8.5 months for those with HGFor = 4 ng/ml; p = 0.007). Serum HGF levels were associated with various specific histologic features of alcoholic hepatitis that included, but were not exclusively related to, necrosis.

Published
1996

10. Protein energy malnutrition in severe alcoholic hepatitis: diagnosis and response to treatment. The VA Cooperative Study Group #275

Author

C L, Mendenhall, T E, Moritz, G A, Roselle, T R, Morgan, B A, Nemchausky, C H, Tamburro, E R, Schiff, C J, McClain, L S, Marsano, and J I, Allen

Subjects
Adult, Male, Hand Strength, Hepatitis, Alcoholic, CD8 Antigens, Middle Aged, Combined Modality Therapy, Protein-Energy Malnutrition, Lymphocyte Subsets, Blood Cell Count, Oxandrolone, Skinfold Thickness, Anabolic Agents, Double-Blind Method, CD4 Antigens, Humans, Regression Analysis, Energy Intake, Muscle, Skeletal
Abstract

Active nutrition therapy and the anabolic steroid oxandrolone (OX), in selected patients with severe alcoholic hepatitis, significantly improved liver status and survival. We report here on the changes in their nutritional parameters.Protein energy malnutrition (PEM) was evaluated and expressed as percent of low normal in 271 patients initially, at 1 month and at 3 months. Active therapy consisted of OX plus a high caloric food supplement vs a matching placebo and a low calorie supplement.PEM was present in every patient; mean PEM score 60% of low normal. Most of the parameters improved significantly from baseline on standard care; the largest improvement seen in visceral proteins, the smallest in fat stores (skinfold thickness). Total PEM score significantly correlated with 6 month mortality (p = .0012). Using logistic regression analysis, creatinine height index, hand grip strength and total peripheral blood lymphocytes were the best risk factors for survival. When CD lymphocyte subsets replaced total lymphocyte counts in the equation, CD8 levels became a significant risk factor (p = .004). Active treatment produced significant risk factor (p = .004). Active treatment produced significant improvements in those parameters related to total body and muscle mass (ie, mid arm muscle area, p = .02; creatinine height index, p = .03; percent ideal body weight, p = .04).Deterioration in nutritional parameters is a significant risk factor for survival in severe patients with alcoholic hepatitis. This deterioration is reversible with standard hospital care. Active therapy further improves creatinine height index, mid arm muscle area and total lymphocyte counts. Hence, these later parameters appear to be the best indicators for follow-up assessments.

Published
1995

11. Alcohol modulation of immune function: clinical and experimental data. Veterans Affairs Cooperative Study Groups 119 and 275

Author

G A, Roselle, C L, Mendenhall, A, Chedid, T E, Moritz, and P, Gartside

Subjects
Oxandrolone, Survival Rate, Liver, Hepatitis, Alcoholic, T-Lymphocyte Subsets, Prednisolone, Food, Fortified, Animals, Humans, Lymphocyte Count, Combined Modality Therapy, Follow-Up Studies
Abstract

In both animal and human studies, ethanol seems to modulate host immune function. In a variety of animal studies, ethanol has been shown to decrease lymphocyte function and number. In human studies of patients with alcoholic hepatitis, these abnormalities were also seen with specific correlation with protein malnutrition. Hepatic pathological lesions were also correlated with lymphocyte subset infiltration. However, peripheral blood lymphocytes did not correlate consistently with hepatic histopathology.

Published
1995

12. Helicobacter pylori is a risk factor for hepatic encephalopathy in acute alcoholic hepatitis: the ammonia hypothesis revisited. The Veterans Administration Cooperative Study Group No. 275

Author

G P, Gubbins, T E, Moritz, L S, Marsano, R, Talwalkar, C J, McClain, and C L, Mendenhall

Subjects
Cohort Studies, Male, Oxandrolone, Helicobacter pylori, Ammonia, Hepatitis, Alcoholic, Risk Factors, Hepatic Encephalopathy, Humans, Prospective Studies, Middle Aged, Helicobacter Infections
Abstract

To determine whether infection with Helicobacter pylori is a risk factor for portosystemic encephalopathy in patients with acute, moderate or severe alcoholic hepatitis.Prospective, multicenter cohort study.Eight Veterans Affairs Hospitals.A cohort of 273 male patients enrolled in a Department of Veterans Affairs Cooperative Study performed to evaluate the efficacy of oxandrolone in combination with nutritional supplementation in moderate or severe alcoholic hepatitis.Admission serum IgG antibody titers against H. pylori by a specific and sensitive ELISA, demographic characteristics of patients, degree of protein calorie malnutrition, presence of ascites, bilirubin level, and known risk factors for hepatic encephalopathy (gastrointestinal bleeding, azotemia, hepatorenal syndrome, infection, and severity of disease); outcome was the presence of portosystemic encephalopathy.Of 188 patients with decompensated alcoholic hepatitis available for analysis, 117 (62.2%) had encephalopathy. Ninety-two (78.6%) of these were infected with H. pylori, compared with 62% of patients without encephalopathy (p = 0.013). In a step-wise regression model, H. pylori was an independent risk factor (relative risk: 2.4, 95% CI: 1.2-4.8) adjusting for ascites and protein-calorie malnutrition.Patients with acute, moderate or severe alcoholic hepatitis have a high H. pylori infection rate (as determined by serology), and those infected are at higher risk for portosystemic encephalopathy.

Published
1993

13. Expression of the beta 1 chain (CD29) of integrins and CD45 in alcoholic liver disease. The VA Cooperative Study Group No. 275

Author

A, Chedid, C L, Mendenhall, T E, Moritz, S W, French, T S, Chen, and T R, Morgan

Subjects
Immunoenzyme Techniques, Male, Integrins, Liver, Antigens, CD, Biopsy, Integrin beta1, Humans, Leukocyte Common Antigens, Liver Diseases, Alcoholic
Abstract

In the active stages of alcoholic liver disease (ALD), we have shown previously an enhanced expression of either CD4 or CD8 molecules on CD3+T cells. Class I and II MHC molecules expression were enhanced on lymphocytes, and on the cell membrane of hepatocytes, thus suggesting that an intrahepatic antigen-dependent lymphocyte-hepatocyte interaction occurs. Here we report the pattern of expression of several additional molecules known to participate in nonspecific cell-cell adhesion preceding alloantigen recognition i.e., the beta 1 chain of integrins (CD29) and the isoforms of the leukocyte common antigen CD45RA and CD45RO.Frozen liver samples from 38 patients with advanced ALD were examined immunohistochemically by the avidin-biotin-peroxidase complex method using monoclonal antibodies. Nine patients with alcoholic fatty liver and six patients with only hepatitis C infection were included as controls and studied in a similar manner.CD29 was strongly expressed on the cell membrane of hepatocytes in 18/20 patients with cirrhosis, in 17/18 with alcoholic hepatitis without cirrhosis, in 5/9 of fatty liver and in all six with hepatitis C. CD45RA was present in 5/18 cases of alcoholic hepatitis and in 3/20 cases of cirrhosis on the hepatocytes plasma membrane, in none of the controls, and rarely on lymphocytes. CD45RO was expressed on the surface of lymphocytes in 14/18 cases of alcoholic hepatitis, 13/20 patients with cirrhosis, in 5/9 of fatty liver and in one with hepatitis C. The CD45RO lymphocytes were predominantly CD8 positive.Our results indicate that in ALD the hepatocytes exhibit on their plasma membrane an enhanced expression of the beta 1 chain of the integrins and less commonly CD45RA. Furthermore, the expression of only CD45RO on the surface of lymphocytes favors the postulate that the intrahepatic lymphocytes in ALD are most likely of the "memory" type. The results of this study lend further support to the contention that a cell-cell contact precedes a cell-mediated mechanism in the pathogenesis of ALD.

Published
1993

14. The impact of age on alcohol toxicity in the rat

Author

C L, Mendenhall, S D, Rouster, C J, Grossman, G A, Roselle, S, Ghosn, and P, Gartside

Subjects
Male, Ethanol, Age Factors, Bilirubin, gamma-Glutamyltransferase, Alkaline Phosphatase, Liver Regeneration, Rats, Rats, Sprague-Dawley, Liver, Animals, Aspartate Aminotransferases, Energy Intake, Triglycerides
Abstract

This study was performed to determine whether the severity of chronic alcohol toxicity is altered by age and duration of drinking. Alcohol as 35% of calorie intake (ED treatment) was administered to Sprague-Dawley rats at predetermined ages beginning at 1, 6, 12, 18, 24 and 27 months for a duration of treatment varying from 1 to 3 months. The degree of injury was compared to controls (CD treatment) of comparable age and duration of treatment. ED was associated with significantly higher serum levels of AST, total bilirubin and alkaline phosphatase (P0.0001 for each test) without detectable differences due to age and duration of treatment. Liver triglycerides (as a measure of alcoholic fatty steatosis) were significantly increased by ED (P0.0001) and influenced by both age and duration of treatment. The greatest toxicity was observed in young animals. ED treatment beginning at 1 month of age was associated with an AST level 69% above CD and liver triglycerides 463% above CD; beginning at 18 months of age, ED produced an increase of 24% in AST and 175% in liver triglycerides. The hepatic regenerative capacity, as measured by 3H-thymidine uptake into nuclear DNA, was similarly affected by both ED and age. Regeneration was significantly higher in youth. ED produced a 62% increase above CD at 1 month compared to an 11% increase beginning at 18 months of age. These observations suggest that juveniles develop more severe injury from alcohol but that a greater regenerative capacity exists in youth. This may explain the observed clinical relationship between age and prognosis seen in patients with severe alcoholic liver injury.

Published
1993

15. Epidemiology of hepatitis C among veterans with alcoholic liver disease. The VA Cooperative Study Group 275

Author

C L, Mendenhall, T, Moritz, S, Rouster, G, Roselle, A, Polito, S, Quan, and R K, DiNelle

Subjects
Humans, Middle Aged, Hepatitis C, Liver Diseases, Alcoholic, United States, Veterans
Abstract

Of 288 patients with alcoholism and various stages of alcoholic hepatitis, 18.4% (53 of 288) reacted serologically for hepatitis C (HCV). An evaluation of the risk factors associated with HCV indicated that parenteral drug use, even in the distant past, increased the risk for infection 10.1-fold (p = 0.0001). Ethnicity was also a significant, independent risk factor. Minorities (i.e., African-Americans or Hispanic-Americans) had a 2.4-fold increase (p = 0.038). Prior blood transfusions, even if multiple, showed only a tendency toward increased infections (p = 0.088) in this population. An interaction between age and contact with parenteral drug users was demonstrated such that the risk of HCV infection was increased by contact with drug users. This was further increased with increasing age (p = 0.006). There was no relationship between HCV reactivity and the severity of the liver disease; however, the liver injury appeared to be accelerated since it occurred at a younger age (p = 0.0001) and was associated with more frequent hospitalizations (p = 0.0005).

Published
1993

16. Cell-mediated hepatic injury in alcoholic liver disease. Veterans Affairs Cooperative Study Group 275

Author

A, Chedid, C L, Mendenhall, T E, Moritz, S W, French, T S, Chen, T R, Morgan, G A, Roselle, B A, Nemchausky, C H, Tamburro, and E R, Schiff

Subjects
Male, Immunity, Cellular, CD3 Complex, Liver, Tumor Necrosis Factor-alpha, T-Lymphocytes, Histocompatibility Antigens Class I, Histocompatibility Antigens Class II, Humans, Liver Diseases, Alcoholic, Interleukin-1
Abstract

The mechanism responsible for the initiation and perpetuation of alcoholic liver disease (ALD) remains poorly understood. This investigation attempted to elucidate the role of cell-mediated immune phenomena in the pathogenesis of ethanol-induced liver injury.Frozen liver biopsy specimens from 144 patients with moderate to severe ALD were examined by the avidin-biotin immunoperoxidase technique for the expression of antigenic markers of T and B lymphocytes, natural killer cells, and class I and II MHC molecules in the tissue.Expression of CD3 by lymphocytes correlated significantly with regenerating nodules, intralobular inflammation, central sclerosis, and abnormalities of Kupffer cells. B cells were rarely present, and natural killer cells were absent. CD3+ lymphocytes expressed either CD4 or CD8 surface molecules. Enhanced class I MHC expression correlated significantly with portal inflammation, limiting plate erosion, vascular abnormalities, and hemosiderosis. Expression of class II MHC molecules correlated significantly with necrosis, bile stasis, and Mallory bodies.The distribution and persistence of CD4+ and CD8+ cells in actively advancing ALD, the enhanced MHC expression on hepatocytes, and their relationship to alcoholic hyalin and necrosis lend support to the hypothesis that a cytotoxic T lymphocyte-hepatocyte interaction plays a role, perhaps via lymphokine production, in the genesis or perpetuation of ALD.

Published
1993

17. Relevance of anti-HCV reactivity in patients with alcoholic hepatitis. VA cooperative Study Group #275

Author

C L, Mendenhall, T, Moritz, A, Chedid, A J, Polito, S, Quan, S, Rouster, and G, Roselle

Subjects
Immunoenzyme Techniques, Male, Hepatitis, Alcoholic, Risk Factors, Immunoblotting, Multivariate Analysis, Humans, Hepacivirus, Hepatitis Antibodies, Hepatitis C Antibodies, Middle Aged, Hepatitis C
Abstract

From 8 Department of Veterans Affairs Medical Centers, 296 patients with varying degrees of alcoholic liver disease were tested for hepatitis C (HCV) infection using an EIA and RIBA 2. A high frequency of positive response was observed with 13.9% reactive to both and an additional 4.4% positive only to RIBA 2 (total 18.3%). An evaluation of known risk factors (injection drug use and prior blood transfusions) failed to account for the mode of transmission in 42.6% of the HCV+ patients. The clinical severity of the liver disease and degree of liver pathology were nearly identical in HCV+ vs. HCV- patients. However, the process was accelerated in the HCV+ patients occurring at a 12.8% younger age (p0.0001) with a 43% increase in ALT (p = 0.05). The most striking differences were observed in immune parameters. In peripheral blood, total lymphocyte counts were increased 20% (p = 0.01) accompanied by a 56% increase in B cells (p = 0.01) and a 35% elevation of IgG levels (p = 0.0001) in HCV+ patients. T cell changes consisted of a 50% increase in CD8 cells (p = 0.047). However, lymphocyte infiltration into liver was not significantly different (HCV+ vs. HCV-) for any of the subsets studied (CD4, CD8, B cells, NK cells). The combined presence of HCV and alcohol injury did not significantly increase mortality but did significantly increase the number of hospitalizations from 2.4 to 4.0 per year (p = 0.0005).

Published
1993

18. Biochemical and clinical effects of aspartame in patients with chronic, stable alcoholic liver disease

Author

Z I, Hertelendy, C L, Mendenhall, S D, Rouster, L, Marshall, and R, Weesner

Subjects
Male, Methanol, Phenylalanine, Middle Aged, Milk, Liver, Risk Factors, Hepatic Encephalopathy, Animals, Drug Evaluation, Humans, Amino Acids, Aspartame, Liver Diseases, Alcoholic
Abstract

Aspartame is an artificial sweetener completely metabolized in the gut and absorbed as aspartate, phenylalanine, and methanol. Phenylalanine is thought to mediate or exacerbate hepatic encephalopathy, and an impaired liver may not be able to cope with the ammoniagenic properties of the amino acid constituents, or adequately metabolize methanol. Thus, we compared the clinical and biochemical effects of a single ingestion of aspartame (15 mg/kg) to skim milk (phenylalanine content equimolar to aspartame) and placebo in patients with chronic, alcoholic liver disease in a randomized, crossover study. Aspartame produced an elevation of plasma phenylalanine significantly greater than milk and placebo (Cmax 14.55 +/- 7.38, 10.95 +/- 4.95, 8.84 +/- 4.55 mumol/dl, respectively; p0.01). However, quantified encephalopathic changes were observed only with milk (p0.05). Plasma aspartate, methanol, formate, and ammonia levels remained unchanged after all treatments. The lack of clinical derangements in encephalopathic indices, methanol accumulation, or biochemical changes in liver status suggests that a single large dose of aspartame (representing 5 times the average daily intake of adults) may be used safely by patients with chronic, stable liver disease.

Published
1993

20. Bile duct changes in alcoholic liver disease. The Veterans Administration Cooperative Study Group

Author

M B, Ray, C L, Mendenhall, S W, French, and P S, Gartside

Subjects
Immunoenzyme Techniques, Metaplasia, Bile Ducts, Intrahepatic, Liver, Biopsy, Humans, Keratins, Bile Ducts, Liver Diseases, Alcoholic
Abstract

The histologic significance of various changes in the bile ductal structures as observed by cytokeratin immunoperoxidase assay was studied in 122 patients with alcoholic liver disease (ALD) as a part of a large Veterans Administration Cooperative Study on alcoholic hepatitis. Four types of morphologic changes in the biliary structures were observed: 1) proliferation of interlobular bile ducts in the portal tracts; 2) marginal bile ductular proliferation at the periphery of the portal tracts; 3) appearance of bile duct type cells ("oval cells") in the liver parenchyma; and 4) metaplasia of bile duct epithelium to cells resembling hepatocytes. These bile ductal changes correlated strongly with liver fibrosis (p = 0.0003; 0.0003; 0.05; 0.0035, for 1, 2, 3, and 4, respectively), cirrhosis (p0.0001 for all four parameters), portal inflammation (p0.0001 for 1, 2, and 4; p = 0.0024 for "oval cells"), and with overall histologic severity scores (p0.0001; p = 0.0001; p = 0.0017; p = 0.0005, respectively). However, these changes did not correlate significantly with fatty change, parenchymal degeneration and necrosis, cellular infiltrate or Kupffer cell hyperplasia, suggesting that they are probably not the direct consequences of liver cell necrosis. Periportal piecemeal necrosis correlated significantly with both portal bile duct (p = 0.0041) and marginal (p = 0.0078) bile ductular proliferation. Among all these changes, only marginal bile ductular proliferation correlated significantly with Mallory bodies present both in the hepatocytes (p = 0.05) and the bile ducts (p = 0.01).(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1993

21. Antibodies to hepatitis B virus and hepatitis C virus in alcoholic hepatitis and cirrhosis: their prevalence and clinical relevance. The VA Cooperative Study Group (No. 119)

Author

C L, Mendenhall, L, Seeff, A M, Diehl, S J, Ghosn, S W, French, P S, Gartside, S D, Rouster, Z, Buskell-Bales, C J, Grossman, and G A, Roselle

Subjects
Adult, Male, Hepatitis, Alcoholic, Immunoblotting, Enzyme-Linked Immunosorbent Assay, Hepacivirus, Middle Aged, Antibodies, Viral, Survival Analysis, Liver Cirrhosis, Alcoholic, Humans, Regression Analysis, Hepatitis B Antibodies, Follow-Up Studies
Abstract

Patients with overt alcoholic liver disease who had participated in a multicenter therapeutic trial and subgroups of controls (i.e., alcoholic patients without liver disease and patients with neither alcoholism nor liver disease) were tested for hepatitis B virus and hepatitis C virus antibodies to determine the prevalence of these antibodies to determine the prevalence of these antibodies and any clinical association in the progression and outcome of alcoholic liver disease. Antibodies to hepatitis B (anti-HBs and/or anti-HBc) were found in 29.2% of patients with alcoholic liver disease, in 26.1% of hospitalized alcoholic patients without liver disease and in 24.2% of hospitalized nonalcoholic patients without liver disease; frequencies were not significantly different from one another. HBsAg was not evaluated because HBsAg+ patients had been excluded from the original trial. The presence of these antibody markers correlated with ethnic origin of and immunoglobulin levels in the patients. In contrast, antibody to hepatitis C, as detected by enzyme immunoassay, was positive in 27.1%, 4.8% and 3.0% of the three groups, respectively, the first differing significantly from the other two. Antibody to hepatitis C virus positivity correlated significantly with clinical severity of the disease and with the presence of histological features that imply chronic viral infection (periportal inflammation, cirrhosis), despite the fact that the supplementary assay for antibody to hepatitis C virus, using recombinant immunoblot assay, reduced the positive rate by 79%.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1991

22. Prognostic factors in alcoholic liver disease. VA Cooperative Study Group

Author

A, Chedid, C L, Mendenhall, P, Gartside, S W, French, T, Chen, and L, Rabin

Subjects
Adult, Hepatitis, Alcoholic, Ascites, Alanine Transaminase, Middle Aged, Prognosis, Fatty Liver, Survival Rate, Liver Cirrhosis, Alcoholic, Risk Factors, Acute Disease, Prothrombin Time, Humans, Liver Diseases, Alcoholic, Veterans
Abstract

Two hundred eighty-one alcoholic patients were prospectively evaluated by clinical, biochemical, and histologic parameters during a 4-yr period to assess their prognosis. They were stratified into four categories of injury: 1) fatty liver (26 patients), 2) acute alcoholic hepatitis (106), 3) cirrhosis (39), and 4) cirrhosis with superimposed alcoholic hepatitis (111). The rate of survival and variables correlating with survival varied according to the group. At 48 months, 70% of the patients with fatty liver were alive, 58% in the alcoholic hepatitis group, 49% in cirrhosis, and 35% in alcoholic hepatitis superimposed upon cirrhosis. Within group one, deaths were due to causes unrelated to liver disease. In the alcoholic hepatitis group, factors significantly correlating with survival were ascites, alanine amino-transferase levels, grams of alcohol consumed, continuation of alcohol intake, and clinical severity of disease. Survival in patients of group three correlated significantly with prothrombin time and histologic severity score. Patients with combined cirrhosis and alcoholic hepatitis exhibited the worst prognosis, with the most significant predictors of survival being age, grams of alcohol consumed, the ratio of serum aminotransferases (AST:ALT) and the histologic and clinical severity of the disease. Although a different pattern of correlates was observed for each pathologic level of injury, knowledge of the various correlates aids in prognostic assessment.

Published
1991

23. Alpha-fetoprotein alterations in alcoholics with liver disease. V.A. Cooperative Study Groups

Author

C L, Mendenhall, A, Chedid, S W, French, M, Ray, G A, Roselle, C J, Grossman, R E, Weesner, and P S, Gartside

Subjects
Male, Alcoholism, Liver, Liver Function Tests, Biopsy, Hepatic Encephalopathy, Radioimmunoassay, Humans, alpha-Fetoproteins, Middle Aged, Liver Diseases, Alcoholic
Abstract

Sera on 409 male alcoholics with liver injury were assayed for alpha-fetoprotein (AFP) as part of a VA co-operative study on the natural history and therapy of alcoholic liver disease. In 78% of the patients values below normal were observed and 42% had undetectable levels. Clinically the lowest AFP concentrations were observed in the more severely ill patients with the poorest 1 year survival. Furthermore, improvement in AFP was associated with improved survival. Correlation analysis showed a relationship of AFP to (1) visceral protein concentrations (i.e. albumin, transferrin, retinal binding protein); (2) variables related to hepatic fibrogenesis (i.e. Ito cell activity, quantitative estimates of fibrosis and Kupffer cell abnormalities); and (3) changes in immunoglobulin levels particularly IgG. These findings suggest that AFP is a good index of disease prognosis.

Published
1991

24. Ito cell activation induced by chronic ethanol feeding in the presence of different dietary fats

Author

S W, French, H, Takahashi, K, Wong, and C L, Mendenhall

Subjects
Fatty Liver, Alcoholism, Liver, Hepatitis, Alcoholic, Liver Cirrhosis, Alcoholic, Animals, Dietary Fats, Liver Diseases, Alcoholic, Models, Biological, Rats
Abstract

Bronfenmajer et al. (1966) first studied Ito cells in alcoholic hepatitis (AH) by light microscopy (LM). The number of Ito cells and the number of fat droplets were increased. Okanoue et al. (1983) found that Ito cells were reduced by LM but increased by electron microscopy (EM) in scars in AH. Ito cells were activated in scars (increased RER and decreased fat in Ito cells with transition to fibroblasts). Minato et al. (1983) showed that increased RER in Ito cells correlated with increased collagen synthesis of liver biopsies in vitro. Mak et al. showed increased RER correlated with the degree of fibrosis in alcoholic baboons (1984) and alcoholic cirrhosis in man (1988). French et al. (1988b) showed morphometrically that Ito cell fat was decreased and RER was increased only in scars but not in normal sinusoids so that Ito cell activation was restricted to the scars. There was no correlation of sinusoidally located Ito cell fat or RER with the amount of perisinusoidal collagen. In rats fed ethanol and a nutritionally adequate diet including corn oil (25% of calories) by intragastric cannula for five months the fatty liver progressed to focal central fibrosis, and Ito cell activation (fat/RER) was increased. When tallow was substituted for corn oil the Ito cells were not activated and the liver histology was normal. Thus, the type of dietary fat and the local environment (scars) are important factors in the activation of Ito cells by alcohol in vivo.

Published
1991

25. Nuclear progestin receptors in rat thymic tissue

Author

H, Fujii-Hanamoto, C J, Grossman, G A, Roselle, C L, Mendenhall, and K, Seiki

Subjects
Cell Nucleus, Cytoplasm, Animals, Female, Rats, Inbred Strains, Thymus Gland, Receptors, Progesterone, Promegestone, Rats
Abstract

The thymus and its associated endothelial cells and lymphocytes act as an important immunological tissue. The endothelial cells of the thymus have been reported to synthesize cytoplasmic progestin receptor in response to estrogen priming. To measure nuclear progestin receptor, female rats were castrated and primed for 3 days with estradiol benzoate (30 micrograms/0.1 ml/d) and immediately before sacrifice injected subcutaneously with 0.2 mg of progesterone. By Scatchard plot analysis we found that specific progestin receptor (KA = 0.89 +/- 0.10 x 10(9) M-1) was present in the KCl-nuclear extract. The concentration of nuclear progestin receptor was found to be in the range of 312.6 +/- 49 fmole/g tissue (n = 9, 1 hour after progesterone injection) while the nuclear receptor was significantly reduced (approximately 44 fmol/g tissue) in the oil treated controls. This level verges on the limits of sensitivity for this assay. For cytoplasmic progestin receptor the concentration was 3.46 +/- 0.20 pmole/g tissue in oil treated controls (n = 14) and 3.36 +/- 0.20 pmole/g tissue in progesterone treated animals (n = 24). The KA of this thymic cytoplasmic progestin receptor was 1.35 +/- 0.06 x 10(9) M-1. By competition assay, the relative binding affinity of nuclear progestin receptor was: R5020 (a potent synthetic progestin) (100%), progesterone (9%), testosterone (0.56%), corticosterone (0.53%), estradiol-17 beta (0%). It is concluded that thymic reticuloepitheleal cells contain nuclear progestin receptor and this finding supports the hypothesis that progesterone, like other sex steroids may play a regulatory role in thymic cell function.

Published
1990

28. Inhibition of Hepatocarcinogenesis by Adrenocorticotropin in Aflatoxin B1-Treated Rats2

Author

A. Chedid, A. E. Bundeally, and C. L. Mendenhall

Subjects
Cancer Research, medicine.medical_specialty, Insulin, medicine.medical_treatment, Stimulation, Biology, Hyperplasia, medicine.disease, Lymphoma, Somatropin, Endocrinology, medicine.anatomical_structure, Oncology, Hepatocyte, Hepatocellular carcinoma, Internal medicine, medicine, Hormone
Abstract

We examined whether hormones would modify the carcinogenic action of aflatoxin B1 (AFB1). Four groups of inbred Fischer rats received AFB1, 125 mug per animal, weekly per os. In three of the groups, certain hormones were administered simultaneously: One group received 1 U growth hormone (GH) sc weekly, another was given 4 U adrenocorticotropin (ACTH) weekly, and a third received 0.5 U insulin weekly sc. AFB1, ACTH, and insulin were given for 20 weeks; GH was given for only 10 weeks. The control group did not receive hormone adjuvant. In each group, 4 animals were killed at 7, 14, 21, 28, and 35 weeks; the remaining rats were killed at 77 weeks. Their livers were carefully examined and samples prepared for light and electron microscopy. Animals receiving AFB1 and ACTH failed to exhibit hepatocellular carcinoma. On the other hand, malignant lymphoma appeared at 56 weeks in 3 of the 6 surviving males on this regime. AFB1, alone or when given with insulin or GH, caused hepatocellular carcinoma in all animals; in these, lymphoma was not observed. Lymphoma comprised two cell types, each with similar neclear characteristics but differing in their nucleocytoplasmic ratios and in the amount and distribution of cytoplasmic organelles. Alterations leading to hepatocellular carcinoma were examined at various stages of development. "Basophilic hyperplasia" reflected an increase in free ribosomes. "Hyperplastic nodules" were composed of hepatocyte aggregates with characteristics similar to those encountered in the earlier stage. Both the "neoplastic nodules" and hepatocellular carcinomas were formed by cells containing large, "smooth fingerprints" and free ribosomal aggregates. These features supported the concept that AFB1 impairs ribosomal binding to endoplasmic reticulum membranes. The failure of ACTH-treated animals to develop hepatocellular carcinoma was ascribed to the effect of adrenal cortical stimulation upon membrane-polysome binding.

Published
1977
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29. Peliosis hepatis

Author

A. Chedid and C. L. Mendenhall

Subjects
Male, Aflatoxin, medicine.medical_specialty, Ethanol, Physiology, business.industry, Gastroenterology, Drug Synergism, medicine.disease, medicine.disease_cause, Rats, Aflatoxins, Liver, Hepatic parenchyma, Chronic alcoholism, Internal medicine, Animals, Medicine, Peliosis hepatis, Chemical and Drug Induced Liver Injury, business, Carcinogenesis
Abstract

Peliosis hepatis, a condition characterized by blood-filled cystic spaces within the hepatic parenchyma, was observed in 5 of 26 male Holtzman rats after chronic treatment with ethanol (mean consumption 5 g/kg/day) and aflatoxin B1 (2 mg intraperitoneally in divided doses). Matched controls and aflatoxin-treated and ethanol-treated animals failed to exhibit these changes. Most of the peliotic lesions developed in the first two months of treatment. All were associated with death of the animal. No hepatocellular carinomas developed in any of the animals, even after one year of observation.

Published
1980
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30. Clinical pharmacokinetics of chlordiazepoxide in patients with alcoholic hepatitis

Author

C. L. Mendenhall, D. D. Morgan, and J. D. Robinson

Subjects
Adult, medicine.medical_specialty, Alcoholic liver disease, Metabolic Clearance Rate, Alcoholic hepatitis, Gastroenterology, Chlordiazepoxide, chemistry.chemical_compound, Pharmacokinetics, Lactate dehydrogenase, Internal medicine, medicine, Humans, Pharmacology (medical), Serum Albumin, Pharmacology, Liver injury, Hepatitis, Hepatitis, Alcoholic, business.industry, Albumin, General Medicine, Middle Aged, medicine.disease, Surgery, Kinetics, chemistry, Regression Analysis, business, Half-Life, medicine.drug
Abstract

The clearance of chlordiazepoxide from the systemic circulation was studied in 20 subjects which included 15 patients with alcoholic hepatitis and 5 normal volunteers. The half-life for the appearance of the drug in the systemic circulation was found to increase exponentially with age (r = 0.73, P less than 0.0005) and was independent of the presence of alcoholic hepatitis. The metabolic clearance of chlordiazepoxide was significantly lower in the patients than in the normal subjects (7.6 compared to 13.8 ml/kg-h, P less than 0.005). Linear regression analysis revealed a significant correlation between clearance and albumin (r = 0.77, P less than 0.00005). However, the predictive value of this relationship was shown to be minimal. Multiple regression analysis produced only a slight improvement in the correlation when both albumin and lactate dehydrogenase were used as variables (r = 0.83, P less than 0.00005). In six of the patients, a second clearance study was conducted three weeks following their initial one. All repeat subjects showed improvement both clinically and as reflected by their laboratory tests for liver injury, but there was not a significant change in their clearance of chlordiazepoxide. Multiple regression analysis of the clearance data on the initial and repeat subjects showed a significant correlation between clearance and the variables age, albumin and lactate dehydrogenase (r = 0.91, P less than 0.0025). This relationship suggests that over a short period of time (where age can be considered constant) changes in albumin and lactate dehydrogenase could be potentially useful in predicting clearance changes in a single individual.

Published
1981
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31. 'Nonalcoholic' chronic hepatitis in the alcoholic

Author

S J, Goldberg, C L, Mendenhall, A M, Connell, and A, Chedid

Subjects
Adult, Alcoholism, Ethanol, Liver, Biopsy, Needle, Chronic Disease, Animals, Humans, Alanine Transaminase, Aspartate Aminotransferases, Chemical and Drug Induced Liver Injury, Middle Aged, Hepatitis
Abstract

Ten alcoholic patients with biopsy proved chronic active or chronic persistent hepatitis were observed. In each patient, the responsible etiological agent appeared to be ethanol. Laboratory abnormalities could be distinguished statistically from those in a group of 121 patients with alcoholic hepatitis by their higher SGPT (262 +/- 139 versus 62 +/- 7 U per ml, P is less than 0.01), lower ratio of SGOT:SGPT (1.96 +/- 0.34 versus 4.71 +/- 0.40, P is less than 0.01), and lower white blood cell count 5,833 +/- 763 versus 10,370 +/- 742, P is less than 0.01). However, the overlap between the groups was sufficiently large that without histological confirmation the correct diagnosis was in doubt for any given patient.

Published
1977

32. Alteration of in vitro human lymphocyte function by ethanol, acetaldehyde and acetate

Author

G A, Roselle and C L, Mendenhall

Subjects
Antigens, Fungal, Ethanol, Trichophyton, Humans, Acetaldehyde, DNA, Lymphocytes, Acetates, Mitogens, Lymphocyte Activation, Cells, Cultured
Abstract

Infection is a major cause of morbidity and mortality in chronic alcoholics and may be attributable to altered lymphocyte function. To evaluate this possibility, the effects of physiologic concentrations of ethanol (ETH) and its metabolites, acetaldehyde (ACH) and acetate (ACT), were studied using in vitro mononuclear cell cultures prepared from normal human donors. ETH depressed DNA synthesis induced by both phytohemagglutinin-M(PHA) and Concanavalin A (Con A). ACH significantly impaired Con A and PHA stimulated lymphocyte DNA synthesis. Con A and PHA induced blastogenesis was also significantly reduced by the in vitro addition of ACT. Spontaneous lymphocyte transformation in these three-day cultures was not affected by ethanol but was decreased by the addition of high dose acetate and acetaldehyde. Lymphocyte response to candida and trichophyton antigens was significantly depressed by ETH and its metabolites. Monocyte depletion by adherence had no effect on these results. Treatment of lymphocytes with ETH, ACH or ACT did not change T cell binding of sheep erythrocytes or B cell expression of surface immunoglobulin or receptor sites for complement. It is concluded that both ethanol and its metabolites in physiologic concentrations significantly inhibited lymphocyte function without altering surface markers.

Published
1982

33. The absorption of intramuscular chlordiazepoxide (Librium) in patients with severe alcoholic liver disease

Author

J D, Robinson, H A, Whitney, D L, Guisti, D D, Morgan, and C L, Mendenhall

Subjects
Adult, Male, Humans, Chlordiazepoxide, Female, Middle Aged, Injections, Intramuscular, Liver Diseases, Alcoholic, Absorption, Half-Life
Abstract

Intramuscular chlordiazepoxide (CDX) is commonly administered to alcoholic liver disease (ALD) patients requiring prompt management of alcohol agitation, anxiety, and delirium tremors. Sedative action is associated with plasma levels of approximately 2.0 mcg/ml, however, intramuscular CDX has been shown to produce peak concentrations consistently below 2.0 mcg/ml in normal subjects. The present study was designed to define the absorption characteristics of intramuscular 25 mg CDX in males with ALD. Five normal males had mean CDX absorption half-lives of 3.0 h and peaked at 0.8 mcg/ml in 7.2 h, while 11 males with ALD had mean absorption half-lives of 9.0 h, and peaked at 0.7 mcg/ml in 19.1 h when they received the drug dissolved in normal saline. Four other males with ALD who received CDX dissolved in the manufacturer's diluent had significantly slower mean absorption half-lives of 16.1 h which peaked at 0.3 mcg/ml in 35.2 h. Significant linear correlations were found with age (r = 0.60, p less than 0.01), body weight (r = 0.55, p less than 0.01), and serum albumin (r = 0.60, p less than 0.01). Because of the extremely slow intramuscular absorption of CDX dissolved in normal saline or the manufacturer's diluent in males with ALD, we do not recommend this route of administration in this population.

Published
1983

34. Effects of mixed bacterial toxins on immune response

Author

C J, Grossman, G A, Roselle, C L, Mendenhall, and P, Warth

Subjects
Male, Bacterial Toxins, Animals, Lymphocytes, Thymus Gland, Lymphocyte Activation, Orchiectomy, Spleen, Rats
Abstract

Mixed bacterial toxin (MBT) is an experimental substance for treatment of certain forms of cancer. To ascertain if the cancer regression affects reported for MBT might be mediated via immunoendocrine interactions, MBT was tested in vivo in male Wistar rats or in vitro on Thymic (Tc) or Splenic (S) lymphocytes prepared from these same animals. In order to evaluate gonadal steroid effects on this process, certain groups of these rats were also castrated before treatment. Tc or S lymphocytes were prepared from these groups and cell responsiveness was monitored by in vitro blastogenic assays. Certain assay wells also contained Concanavalin A as a mitogen. The addition of MBT in vitro significantly stimulated Tc-cell responses (p less than 0.05) for all experimental groups except for certain groups of castrate MBT injected rats. Furthermore, S cells did not respond in the presence of MBT added in vitro except after castration and pretreatment with MBT where in vitro addition of MBT to cultures significantly stimulated blastogenic responses (p less than 0.02). The results of these assays are consistent with the hypothesis that the anticancer effects attributed to MBT result from the ability of MBT to act as a nonspecific mitogen-like stimulator of immature Tc-cells and mature S-cells. These results also suggest that MBT may modulate a serum factor under the control of gonadal steroids and possibly of thymic origin which can effect T-cell responsiveness.

Published
1987

35. Intermittent idiopathic portal hypertension. A case report

Author

C L, Mendenhall, J, Sherman, and A, Chedid

Subjects
Guanethidine, Male, Periodicity, Time Factors, Biopsy, Hematemesis, Middle Aged, Esophageal and Gastric Varices, Liver, Melena, Recurrence, Chronic Disease, Hypertension, Portal, Humans, Spleen
Published
1974

36. Clinical and Therapeutic Aspects of Alcoholic Liver Disease

Author

C. L. Mendenhall

Subjects
Alcoholic liver disease, Cirrhosis, business.industry, Environmental health, Health impact, Medicine, Alcohol abuse, Alcoholic hepatitis, Alcoholic fatty liver, business, medicine.disease, Socioeconomic status, Medical expenses
Abstract

The socioeconomic health impact of alcoholism is enormous. In the United States in 1975, $ 12.74 billion was spent for health and medical expenses associated with alcoholism (Berry et al. 1977). The total number of deaths directly related to alcoholism in 1977 ranged between 18,066 and 34,724 (National Institute on Alcohol Abuse and Alcoholism 1978), 85% of these being associated with alcoholic liver disease. Indeed, death from cirrhosis ranks fourth among causes of death in the United States (US Bureau of Census 1975).

Published
1985
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37. Ethanol-induced alterations in lymphocyte function in the guinea pig

Author

G A, Roselle and C L, Mendenhall

Subjects
Leukocyte Count, Ethanol, Guinea Pigs, Animals, Lymphocytes, Lymphocyte Activation, Macrophage Migration-Inhibitory Factors, Skin Tests
Abstract

Infections and chronic liver injury are common causes of morbidity and mortality in alcoholics, and both of these may be related to an altered immune response. This study describes a guinea pig model of chronic ethanolism designed to selectively study the cellular immune system in a setting free from the malnutrition, socioeconomic deprivation, and severe underlying hepatic dysfunction seen in human disease. Animals were given 2.5 g/kg/day of ethanol as a 15% solution in 0.9% NaCl or isocaloric-dextrose-saline control solution intraperitoneally in 2 divided doses for 5 weeks. At 2 weeks, the mean serum ethanol level 1 hr after treatment was 20.4 mM (range 8.9-30.6) while the mean serum acetaldehyde level was 55.1 microM (range 17.0-111). At 5 weeks the serum levels for ethanol and acetaldehyde were 20.1 mM (13.3-32.9) and 41.5 microM (2.4-87.6), respectively. Weight gain was persistent throughout the study and did not differ significantly between ethanol and control groups. After 5 weeks of treatment, lymphocyte response to the mitogens, phytohemagglutinin, and concanavalin A was significantly decreased in the ethanol treated group (p less than 0.05). Response to the specific antigen, picrylated human serum albumin, TB cell per cent and number, skin test reactivity, peripheral white blood cell count, total lymphocyte count, and migration inhibitory factor production were not significantly altered by 5 weeks of ethanol treatment. Therefore, in a controlled animal model of chronic ethanolism, we observed a significant depression of lymphocyte blastogenic response which may, in part, explain the increased propensity to infection by intracellular pathogens seen in alcoholics.

Published
1984

38. Morphometric study of hepatic ultrastructure in alcoholic hepatitis. Veterans Administration Cooperative Study Group on Alcoholic Hepatitis

Author

T S, Chen, D P, Murphy, G, Marquet, A, Chedid, C L, Mendenhall, and L, Rabin

Subjects
Male, Liver, Liver Cirrhosis, Alcoholic, Biopsy, Liver Diseases, Humans
Abstract

We undertook a morphometric analysis of hepatocellular organelles in an attempt to correlate their changes with the clinical stages of patients with alcoholic hepatitis. Although hepatic ultrastructural alterations did not correlate with disease severity, we found significant differences between patient and control groups in the measured parameters of non-organelle cytoplasm, mitochondria, SER, RER, glycogen, and lipid.

Published
1987

39. Lymphocyte subset alterations in patients with alcoholic hepatitis

Author

G A, Roselle, C L, Mendenhall, C J, Grossman, and R E, Weesner

Subjects
Patient Admission, Hepatitis, Alcoholic, Protein Deficiency, Temperance, Statistics as Topic, Humans, Lymphocytes, Lymphocyte Activation
Abstract

Twenty-three patients with alcoholic hepatitis (AH) were entered into a study to evaluate the relationship between alcoholic hepatitis, malnutrition, and immune status. In order to quantify these variables, objective parameters of nutritional status and lymphocyte phenotype and function were used. On admission to hospital, the mean number of CD4 helper/inducer cells, CD8 suppressor/cytotoxic cells, and CD3 lymphocytes were significantly reduced compared to age matched, non-hospitalized laboratory controls. In order to ascertain whether this abnormality was reversible, 12 patients, who were willing to remain in the hospital for 30 days, were treated for this entire period with oral nutritional supplementation using a commercially available preparation high in calories, protein, and branch chain amino acids. After 30 days of this therapy and abstinence, the number of CD4 cells increased from a mean (+/- SD) of 658 +/- 428 to 815 +/- 599/mm3. There was no difference in results of the lymphocyte transformation test comparing pre- and post-therapy values using either fetal calf or autologous serum. For all groups tested, cells cultured in autologous serum exhibited a significantly decreased response to mitogen compared to cells cultured in fetal calf serum. Both the total nutritional and the protein depletion (kwashiorkor) scores improved significantly during the 30 days of nutritional supplementation (p less than 0.0009 and p less than 0.0004, respectively). Therefore, we have observed an alteration in the numbers of helper lymphocytes in patients admitted with AH. This abnormality was modifiable by abstinence and nutritional supplementation over a brief period of hospitalization.

Published
1988

40. A new therapy for portal systemic encephalopathy

Author

C L, Mendenhall, S, Rouster, L, Marshall, and R, Weesner

Subjects
Male, Random Allocation, Double-Blind Method, Ammonia, Hepatic Encephalopathy, Drug Evaluation, Humans, Benzoic Acid, Middle Aged, Benzoates, Aged, Phenylacetates
Abstract

This report describes a new therapeutic approach to the treatment of adults with portal systemic encephalopathy using sodium benzoate and sodium phenylacetate, two compounds that increase conjugated nitrogen excretion in the urine and that have been shown to be an effective treatment for children with congenital hyperammonemia. The study was a double-blind cross-over study in which each patient was his own control. All patients either improved their mental status (six of eight) or maintained a mental status comparable to that achieved with conventional therapy [lactulose or neomycin (two of eight)]. All decreased their blood ammonias on these medications and seven of eight improved their portal systemic encephalopathy index. It is suggested that these medications may be useful in the treatment of portal systemic encephalopathy.

Published
1986

41. Protein-calorie malnutrition associated with alcoholic hepatitis. Veterans Administration Cooperative Study Group on Alcoholic Hepatitis

Author

C L, Mendenhall, S, Anderson, R E, Weesner, S J, Goldberg, and K A, Crolic

Subjects
Adult, Anthropometry, Hepatitis, Alcoholic, Liver Cirrhosis, Alcoholic, Humans, Middle Aged, Energy Intake, Protein-Energy Malnutrition, Aged, Diet
Abstract

Three hundred sixty-three alcoholic patients with alcoholic hepatitis were studied in six Veterans Administration medical centers. By history, alcohol consumption was 227.9 g per day, with a mean duration of 23.8 years. Cirrhosis accompanied the alcoholic hepatitis in 58.7 percent of the patients who underwent biopsy or autopsy. Complete nutritional assessment was performed in 284 patients, and observed nutritional changes were classified into those associated with marasmus or those characterizing kwashiorkor. A smaller comparison group of 21 alcoholic patients matched for age and alcohol consumption but without clinically evident liver disease was also studied in an identical manner. None of the patients with liver disease was completely free from malnutrition, whereas 62 percent of the alcoholic patients without liver disease showed abnormalities. In patients with alcoholic hepatitis, some findings associated with marasmus were seen in 86 percent, and some features of kwashiorkor were observed in 100 percent. When present together, the complete picture of kwashiorkor and marasmus correlated closely with the clinical severity of the liver disease (p less than 0.005). The nearly constant association of either complete or partial kwashiorkor or marasmus suggests that the separation of these two entities is artificial in alcoholic patients with liver disease. Although, experimentally, malnutrition may not be essential for the development of alcoholic hepatitis, clinically, it appears to precede the development of the liver injury, which suggests an interaction. Recognition is important so that appropriate nutritional therapy can be provided.

Published
1984

42. Age dependent alterations of host immune response in the ethanol-fed rat

Author

G A, Roselle, C L, Mendenhall, and C J, Grossman

Subjects
Male, Aging, Alcoholism, Immunity, Cellular, Animals, Rats, Inbred Strains, In Vitro Techniques, Lymphocyte Activation, Spleen, Rats, Skin Tests
Abstract

The interaction between ethanol and aging with respect to cellular immune response is unclear. For our studies, Sprague-Dawley rats were pair fed using a synthetic liquid control diet (LCD) or a diet in which ethanol was substituted for carbohydrate (LED). The special diets were started when the rats' age varied from 1-18 months and were continued for one, two, or three months. In a second set of experiments, rats were treated continuously with these diets for 24 months. At each study period blood was drawn for serum and the spleen cells removed. Immune response was assessed by the lymphocyte transformation test using combinations of cells and serum from each of the rat groups. When LCD or LED were started in aged rats (18 months), after three months, there was a significant decrease in the Concanavalin A induced lymphocyte transformation test using the serum from LCD rats compared to serum from LED rats with either cells from LCD (1,273 +/- 831 (DPM +/- SD) vs 302 +/- 139; p less than 0.04) or cells from LED animals (984 +/- 338 vs 420 +/- 196; p less than 0.02). When the diet started at younger age or for less than three months these effects were not seen. In the continuously LCD or LED fed rats, the blastogenic response peaked at three months of treatment (four months of age) and decreased at six months and remained constant over the remainder of the 24 month period. There was no difference in lymphocyte DNA synthesis comparing any of the serum or cell groups with respect to diet.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1989

43. Longevity among ethnic groups in alcoholic liver disease

Author

C L, Mendenhall, P S, Gartside, G A, Roselle, C J, Grossman, R E, Weesner, and A, Chedid

Subjects
Adult, Male, Longevity, Puerto Rico, Black People, Hispanic or Latino, Middle Aged, United States, White People, Alcoholism, United States Department of Veterans Affairs, Risk Factors, Ethnicity, Indians, North American, Humans, Multicenter Studies as Topic, Patient Compliance, Regression Analysis, Liver Diseases, Alcoholic, Aged, Follow-Up Studies
Abstract

As part of a multicenter V.A. Cooperative Study, 437 male veterans with varying stages of alcoholic liver injury were followed over a 4.5 year period. Their ethnic distribution consisted of 256 Caucasians, 109 black Afro-Americans, 63 Puerto Rican Hispanics, and 9 Native American Indians. Survival analyses revealed significant differences between groups (P = 0.0002): 66% of Afro-Americans were still living at 42 months; Caucasians were intermediate with 40% survival; and only 28% of Hispanics were alive. The number of Native American Indians enrolled was too small to draw conclusions but none of those enrolled survived beyond 24 months. Survival regression analysis of 30 clinical, laboratory, histologic and nutritional parameters, revealed the following significant risk factors: clinical severity (P less than 0.0001), histologic severity (P less than 0.0001), race (P = 0.001), age (P = 0.002), BUN (P = 0.01) and ALT (P = 0.02). These analyses indicated that ethnicity, independent of other variables, is significantly associated with outcome from the disease.

Published
1989

46. Origin of hepatic triglyceride fatty acids: quantitative estimation of the relative contributions of linoleic acid by diet and adipose tissue in normal and ethanol-fed rats

Author

C L, Mendenhall

Subjects
Glycerol, Male, Ethanol, Fatty Acids, Essential, Fatty Acids, Tritium, Dietary Fats, Diet, Rats, Fatty Liver, Adipose Tissue, Linoleic Acids, Liver, Chylomicrons, Animals, Chromatography, Thin Layer, Mathematics, Triglycerides
Abstract

The present study demonstrates that the rat liver obtains most of its triglyceride fatty acids from dietary sources. The dietary and adipose tissue contributions of linoleic acid for hepatic triglyceride esterification were shown to be 50.42 and 13.85 micro moles, respectively, during a 4-day period. When ethanol provided 40% of the caloric intake, fatty liver developed and hepatic triglyceride content increased threefold. Under these conditions, the dietary and adipose tissue contributions of linoleic acid were estimated at 192.85 and 10.73 micro moles, respectively. This increase in dietary fatty acid utilization was sufficient to account for the entire increase in esterified hepatic linoleic acid. Any explanation of these observations must include the high dietary fatty acid utilization in both control and ethanol-treated animals. One possibility is that most dietary lipids first enter a rapidly turning over pool in adipose tissue from which most hepatic triglyceride fatty acids are derived. Another is that dietary fatty acids, incorporated into chylomicrons, are stored separately and used preferentially by the liver as compared with lipids derived from adipose tissue and bound to albumin. The pros and cons of these possibilities are discussed.

Published
1972

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