TY - JOUR
T1 - Epidemiological characteristics, risk factors, and clinical manifestations of acute non-A-E hepatitis
AU - Chu, Chia Ming
AU - Lin, Deng Yn
AU - Yeh, Chau Ting
AU - Sheen, I. Shyan
AU - Liaw, Yun Fan
PY - 2001
Y1 - 2001
N2 - A substantial proportion of acute non-A, non-B hepatitis was of unknown etiology and was termed non-A-E hepatitis. Analysis of the clinical features is needed while attempting to identify the causative agent(s). In this study, the clinical and biochemical features of 53 patients who were admitted to hospital with acute non-A-E hepatitis were compared with a cohort of patients with acute hepatitis C (n=70) and E (n=5). In acute non-A-E hepatitis, the sex ratio was 34:19, and ages ranged from 21 to 76 years (median 49). Biochemical tests [median (range)] revealed albumin 3.6 (2.2-4.4) g/dl, AST 714 (193-2311) U/I, ALT 896 (310-3,000) U/I, bilirubin 11.2 (0.9-36.3) mg/dl, and prothrombin time > 1.1 (0-11.5) seconds. No patients reported parenteral exp exposures or household contact. Forty-five percent had severe hepatitis (i.e., albumin < 3 g/dl, bilirubin > 15 mg/dl or prothrombin time > 3 sec), including 3% with fulminant hepatitis. Chronic evoluton was noted n 7%. These features were similar to those of hepatitis C or E, except for a significantly high frequency of parenteral exposures (20%), household contact (16%), and chronicity (70%) in hepatitis C. In conclusion, there is no obvious parenteral risk factor identified in acute non-A-E hepatitis. Clinical severity is similar to that of hepatitis C at least in hospitalized patients, but the rate of chronic evolution is much lower.
AB - A substantial proportion of acute non-A, non-B hepatitis was of unknown etiology and was termed non-A-E hepatitis. Analysis of the clinical features is needed while attempting to identify the causative agent(s). In this study, the clinical and biochemical features of 53 patients who were admitted to hospital with acute non-A-E hepatitis were compared with a cohort of patients with acute hepatitis C (n=70) and E (n=5). In acute non-A-E hepatitis, the sex ratio was 34:19, and ages ranged from 21 to 76 years (median 49). Biochemical tests [median (range)] revealed albumin 3.6 (2.2-4.4) g/dl, AST 714 (193-2311) U/I, ALT 896 (310-3,000) U/I, bilirubin 11.2 (0.9-36.3) mg/dl, and prothrombin time > 1.1 (0-11.5) seconds. No patients reported parenteral exp exposures or household contact. Forty-five percent had severe hepatitis (i.e., albumin < 3 g/dl, bilirubin > 15 mg/dl or prothrombin time > 3 sec), including 3% with fulminant hepatitis. Chronic evoluton was noted n 7%. These features were similar to those of hepatitis C or E, except for a significantly high frequency of parenteral exposures (20%), household contact (16%), and chronicity (70%) in hepatitis C. In conclusion, there is no obvious parenteral risk factor identified in acute non-A-E hepatitis. Clinical severity is similar to that of hepatitis C at least in hospitalized patients, but the rate of chronic evolution is much lower.
KW - Acute viral hepatitis
KW - Chronic hepatitis
KW - Fulminant hepatic failure
KW - Hepatitis C
KW - Hepatitis E
KW - Hepatitis non-A, non-B
KW - Hepatitis non-A-E
UR - http://www.scopus.com/inward/record.url?scp=0034860796&partnerID=8YFLogxK
U2 - 10.1002/jmv.2033
DO - 10.1002/jmv.2033
M3 - 文章
C2 - 11536236
AN - SCOPUS:0034860796
SN - 0146-6615
VL - 65
SP - 296
EP - 300
JO - Journal of Medical Virology
JF - Journal of Medical Virology
IS - 2
ER -