| Literature DB >> 18952249 |
Sibnarayan Datta1, Arup Banerjee, Partha Kumar Chandra, Avik Biswas, Rajesh Panigrahi, Pradip Kumar Mahapatra, Chinmoy Kumar Panda, Shekhar Chakrabarti, Sujit Kumar Bhattacharya, Runu Chakravarty.
Abstract
HBx genetic variability was explored in the Eastern Indian population with low HCC incidence. DNase I sensitive HBV DNA was detected in 53% samples, which differed significantly between clinical groups (P<0.001). HBV genotypes A (Aa/A1), C (Cs/C1) and D (D1, D2, D3, D5) were detected in 37.5%, 18.7% and 43.7% samples respectively. Population specific signature HBx residues A(36), V(88), S(101) in Aa/A1 and residues P(41), Q(110) in D5 were detected. Mutations T(127), M(130) and I(131) were detected in 66.7%, 91% and 75% of genotype A, C and D5 samples respectively. Very low occurrence of HCC associated mutations (V(5)M/L, P(38)S, and H(94)Y) and absence of C-terminal deletions were observed. Our study shows that HBV genotype associated clinically important HBx variations may evolve and act distinctly in different geo-ethnic populations. Further studies on HBx functions from the perspective of genetic variability are essential for the better understanding of the clinical significance of HBV.Entities:
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Year: 2008 PMID: 18952249 DOI: 10.1016/j.virol.2008.09.007
Source DB: PubMed Journal: Virology ISSN: 0042-6822 Impact factor: 3.616