The Relationship of Acute Transfusion-Associated Hepatitis to the Development of Cirrhosis in the Presence of Alcohol Abuse

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	Harris, D. R.

BRIEF COMMUNICATION

The Relationship of Acute Transfusion-Associated Hepatitis to the Development of Cirrhosis in the Presence of Alcohol Abuse

D. Robert Harris, PhD; René Gonin, PhD; Harvey J. Alter, MD; Elizabeth C. Wright, PhD; Zelma J. Buskell, BS; F. Blaine Hollinger, MD; Leonard B. Seeff, MD, for the National Heart, Lung, and Blood Institute Study Group

16 January 2001 | Volume 134 Issue 2 | Pages 120-124

Background: Although concomitant alcoholism is widely believedto enhance liver disease progression in persons with hepatitisC virus (HCV) infection, this relationship has not been wellquantified.

Objective: To quantify the relationship of transfusion-associatedHCV infection and history of heavy alcohol abuse to developmentof cirrhosis.

Design: Retrospective cohort study.

Setting: Liver clinics in university and government hospitals.

Patients: Extended follow-up of 1030 patients in prospectiveinvestigations of transfusion-associated viral hepatitis conductedin the United States between 1968 and 1980.

Measurements: Development of cirrhosis and history of heavyalcohol abuse were determined from review of interviews withpatients or their proxies, medical records, death certificates,and autopsy and biopsy reports. Logistic regression was usedto estimate the risk for cirrhosis associated with transfusion-associatedHCV infection and history of heavy alcohol abuse.

Results: The absolute risk for cirrhosis was 17% among patientswith transfusion-associated HCV; 3.2% among patients with transfusion-associatednon-A, non-B, non-C hepatitis; and 2.8% among controls. Patientswith transfusion-associated HCV were more likely than controlsto develop cirrhosis (odds ratio, 7.8 [95% CI, 4.0 to 15.1]).A history of heavy alcohol abuse was associated with a fourfoldincreased risk for cirrhosis. Hepatitis C virus infection plusa history of heavy alcohol abuse led to a substantial increasein risk for cirrhosis (odds ratio, 31.1 [CI, 11.4 to 84.5])compared with controls without such a history.

Conclusions: Heavy alcohol abuse greatly exacerbates the riskfor cirrhosis among patients with HCV infection. This findingemphasizes the need to counsel such patients about their drinkinghabits.

Author and Article Information

From Westat, Rockville, Maryland; National Institute of Diabetes and Digestive and Kidney Diseases and National Institutes of Health, Bethesda, Maryland; New England Research Institutes, Watertown, Massachusetts; Veterans Affairs Medical Center and Georgetown University School of Medicine, Washington, D.C.; and Baylor College of Medicine, Houston, Texas.

Acknowledgments: The authors thank Song Li and David Chang,Westat, Rockville, Maryland, for data processing and statisticalprogramming support and Jim Korelitz and Stephen Durako forreview and comment on earlier drafts of the manuscript.

Grant Support: By contracts N01-HB-87047 and N01-HB-37093 fromthe National Heart, Lung, and Blood Institute.

Requests for Single Reprints: Leonard B. Seeff, MD, NationalInstitutes of Health, National Institute of Diabetes and Digestiveand Kidney Disorders, 31 Center Drive, Room 9A18, Mail DropMSC2560, Bethesda, MD 20892-2560; e-mail, seeffl{at}extra.niddk.nih.gov.

Current Author Addresses: Drs. Harris and Gonin: Westat, 1650Research Boulevard, Rockville, MD 20850.

Dr. Alter: Department of Transfusion Medicine, National Institutesof Health, Building 10, IN307, 9000 Rockville Pike, Rockville,MD 20892.

Dr. Wright: New England Research Institute, 9 Galen Street,Watertown, MA 02472.

Ms. Buskell: Hepatitis Research, Room 3A-128, Veterans AffairsMedical Center, 50 Irving Street NW, Washington, DC 20422.

Dr. Hollinger: Baylor College of Medicine, NS BCM 3B5, One BaylorPlaza, Houston, TX 77030.

Dr. Seeff: National Institutes of Health, National Instituteof Diabetes and Digestive and Kidney Disorders, 31 Center Drive,Room 9A18, Mail Drop MSC2560, Bethesda, MD 20892-2560.

Author Contributions: Conception and design: D.R. Harris, R.Gonin, E.C. Wright, Z.J. Buskell, F.B. Hollinger, L.B. Seeff.

Analysis and interpretation of the data: D.R. Harris, R. Gonin,Z.J. Buskell, F.B. Hollinger, L.B. Seeff.

Drafting of the article: D.R. Harris, R. Gonin, H.J. Alter,L.B. Seeff.

Critical revision of the article for important intellectualcontent: D.R. Harris, R. Gonin, H.J. Alter, E.C. Wright, Z.J.Buskell, F.B. Hollinger, L.B. Seeff.

Final approval of the article: D.R. Harris, R. Gonin, H.J. Alter,E.C. Wright, Z.J. Buskell, F.B. Hollinger, L.B. Seeff.

Provision of study materials or patients: H.J. Alter, F.B. Hollinger,L.B. Seeff.

Statistical expertise: D.R. Harris, R. Gonin, E.C. Wright.

Administrative, technical, or logistic support: D.R. Harris,Z.J. Buskell, L.B. Seeff.

Collection and assembly of data: D.R. Harris, R. Gonin, H.J.Alter, Z.J. Buskell, F.B. Hollinger, L.B. Seeff.

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