Optimal time for repeating the IgM anti-hepatitis A virus antibody test in acute hepatitis A patients with a negative initial testOptimal time for repeating the IgM anti-hepatitis A virus antibody test in acute hepatitis A patients with a negative initial test
- Other Titles
- Optimal time for repeating the IgM anti-hepatitis A virus antibody test in acute hepatitis A patients with a negative initial test
- Authors
- 현종진; 서연석; 안형진; 임선영; 서민호; 김혜숙; 김창하; 김지훈; 금보라; 김용식; 임형준; 이홍식; 엄순호; 김창덕; 유호상
- Issue Date
- 2012
- Publisher
- 대한간학회
- Keywords
- Acute hepatitis A; IgM anti-HAV; Alanine aminotransferase
- Citation
- Clinical and Molecular Hepatology, v.18, no.1, pp.56 - 82
- Indexed
- SCOPUS
KCI
- Journal Title
- Clinical and Molecular Hepatology
- Volume
- 18
- Number
- 1
- Start Page
- 56
- End Page
- 82
- URI
- https://scholar.korea.ac.kr/handle/2021.sw.korea/109979
- ISSN
- 2287-2728
- Abstract
- Background/Aims: The nonspecific clinical presentation of acute hepatitis A (AHA) mandates the detection of anti-hepatitis A virus IgM antibodies (IgM anti-HAV) in the serum for obtaining a definitive diagnosis. However, IgM anti-HAV might not be present during the early phase of the disease. The aim of this study was to determine the optimal time for repeating the IgM anti-HAV test (HAV test) in AHA patients with a negative initial test. Methods: In total, 261patients hospitalized with AHA were enrolled for this retrospective study. AHA was diagnosed when the test for IgM anti-HAV was positive and the serum alanine aminotransferase (ALT) level was ≥400 IU/L. Repeat HAV test was conducted after 1-2 weeks if the initial HAV test was negative but AHA was still clinically suspected. Results: The results of the initial HAV test were negative in 28 (10.7%) patients. The intervals from symptom onset to the initial-HAV-test day and from the peak-ALT day to the initial-HAV-test day were significantly shorter in the negative-initial-HAV-test group, but on multivariate analysis only the latter was significantly associated with negative results for the initial HAV test (β=-0.978;odds ratio [95% confidence interval]=0.376 [0.189-0.747]; P=0.005). The HAV test was positive in all patients when it was performed at least 2 days after the peak-ALT day. Conclusions: The results of HAV tests were significantly associated with the interval from the peak-ALT day to the HAV-test day. The optimal time for repeating the HAV test in clinically suspicious AHA patients with a negative initial HAV test appears to be at least 2 days after the peak-ALT day. (Korean J Hepatol 2012;18:56-62)
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