Evolutionary seroepidemiology of viral hepatitis and the gap in hepatitis C care cascades among uraemic patients receiving haemodialysis in Taiwan-the Formosa-Like Group.
Yu-Ju WeiPo-Yao HsuJia-Jung LeeSheng-Wen NiuJiun-Chi HuangCheng-Ting HsuTyng-Yuan JangMing-Lun YehChing-I HuangPo-Cheng LiangYi-Hung LinMing-Yen HsiehMeng-Hsuan HsiehSzu-Chia ChenChia-Yen DaiZu-Yau LinShinn-Cherng ChenJee-Fu HuangJer-Ming ChangShang-Jyh HwangWan-Long ChuangChung-Feng HuangYi-Wen ChiuMing-Lung YuPublished in: Journal of viral hepatitis (2021)
Uraemic patients undergoing haemodialysis are at high risk of hepatitis B virus (HBV) and hepatitis C virus (HCV) infection. We aimed to evaluate the evolutionary seroprevalence of viral hepatitis and the gap in HCV care cascades in this special population by a large-scale surveillance study in Taiwan. Uraemic patients on maintenance haemodialysis from 22 sites (FORMOSA-LIKE group) in 2012 (n = 1,680) and 2019 (n = 2,326) were recruited for this study. The distributions and sequential changes of viral hepatitis markers were analysed. The prevalence of anti-HCV antibody and hepatitis B surface antigen (HBsAg) seropositivity was 13.6% (316/2326) and 11.5% (267/2326), respectively, in 2019 compared with 17.3% (290/1680, P = .002) and 13.6% (229/1680, P = .046), respectively, in 2012. The HCV-viremic rate among anti-HCV-seropositive patients was significantly lower in 2019 than in 2012 (56.3% [178/316] vs. 73.8% [214/290], P < .001). The HCV treatment rate increased from 2.3% (5/217) in 2012 to 21.7% (49/226) in 2019 (P < .001). In the sequential analysis of the 490 patients who participated in both screens, 17 of the 55 HCV-viremic patients became HCV RNA seronegative, including 13 by antivirals and four spontaneously. By contrast, one anti-HCV-seropositive but nonviremic patient became viremic, and six anti-HCV-seronegative patients became anti-HCV-seropositive in 2019. The annual incidence of new HCV was 0.2%/year. Seven HBsAg-seropositive patients experienced HBsAg loss (1.25%/year). Two patients had new anti-HBc seropositivity (new HBV exposure: 0.57%/year). The seroprevalence of viral hepatitis decreased in an 8-year follow-up but remained prevalent, and the treatment of HCV infection was underutilized in uraemic patients. Additional efforts are needed to enhance the HCV treatment uptake of uraemic patients. Clinical Trial IDs: NCT03803410, NCT01766895.
Keyphrases
- hepatitis c virus
- end stage renal disease
- hepatitis b virus
- clinical trial
- ejection fraction
- chronic kidney disease
- newly diagnosed
- peritoneal dialysis
- human immunodeficiency virus
- prognostic factors
- patients undergoing
- healthcare
- sars cov
- computed tomography
- randomized controlled trial
- palliative care
- case report
- dna methylation
- study protocol
- genome wide
- patient reported outcomes
- pain management
- combination therapy
- smoking cessation
- quality improvement