Molecular Epidemiology of HCV Infection among Multi-Transfused β-Thalassemia Patients in Eastern India: A Six-Year Observation

Author:

Dutta Supradip1ORCID,Biswas Aritra1ORCID,Bakshi Sagnik1ORCID,Choudhury Promisree1ORCID,Das Raina1ORCID,Nath Shreyasi1ORCID,Chowdhury Prosanto2ORCID,Bhattacharyya Maitreyee3,Chakraborty Sharmistha4,Dutta Shanta1,Sadhukhan Provash Chandra1

Affiliation:

1. Indian Council of Medical Research-National Institute of Cholera and Enteric Diseases P-33, Scheme XM, CIT Road, Beliaghata, Kolkata 700010, India

2. Peerless Hospital & B. K. Roy Research Centre 360 Panchasayar, Kolkata 700094, India

3. Department of Haematology, Kolkata Medical College & Hospital, 88 College Street, Kolkata 700012, India

4. Thalassaemia Unit with Pathology Department, Burdwan Medical College and Hospital Baburbag, Rajbati, Burdwan 713104, India

Abstract

Background: HCV infection is very common in multi-transfused β-thalassemia patients who need regular blood transfusions. Aim: The study was conducted to determine the epidemiology of HCV in multi-transfused β-thalassemia patients in West Bengal, India. Methods: Over a span of six years, blood samples were collected from HCV sero-reactive β-thalassemia patients and processed for viral RNA isolation followed by nested RT-PCR for qualitative viremia detection. The HCV genotype was determined by amplifying the partial HCV core gene by nested RT-PCR followed by DNA sequencing and NCBI genotyping tools. Phylogenetic and phylogeographic studies were performed with MEGA-X and BEAST software, respectively. Results: Out of 917 multi-transfused HCV sero-reactive β-thalassemia patients, 598 (65.21%) were HCV RNA positive while 250 (41.80%) had spontaneously cleared the virus. A significant percentage of male patients from rural areas (p = 0.042) and economically backward class (p = 0.002) were at higher risk of HCV infection. Female thalassemia patients and individuals belonging to ages 11–15 years had higher chances of spontaneous clearance. The most prevalent circulatory HCV genotype was 3a (78.26%) followed by 1b (12.04%). Phylogeographic analyses revealed that the 3a strains share genomic similarities with strains from Pakistan, Sri Lanka, and Thailand, whereas the 1b strains share similarities with strains from Thailand, Vietnam, Russia, and China. Uncommon HCV subtypes 3g and 3i were also detected. Conclusion: The high prevalence of HCV infection among β-thalassemia patients of West Bengal, India indicates NAT-based assays should be implemented for HCV screening in donor blood to eliminate HCV by 2030.

Publisher

MDPI AG

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