Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes

The evolution of hepatitis B virus (HBV), particularly its origins and evolutionary timescale, has been the subject of debate. Three major scenarios have been proposed, variously placing the origin of HBV in humans and great apes from some million years to only a few thousand years ago (ka). To comp...

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Main Authors: Paraskevis, D., Angelis, K., Magiorkinis, G., Kostaki, E., Ho, S.Y.W., Hatzakis, A.
Format: Article in Journal/Newspaper
Language:English
Published: 2015
Subjects:
Online Access:https://pergamos.lib.uoa.gr/uoa/dl/object/uoadl:3009673
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spelling ftnkunivathens:oai:lib.uoa.gr:uoadl:3009673 2024-02-11T10:01:32+01:00 Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes Paraskevis, D. Angelis, K. Magiorkinis, G. Kostaki, E. Ho, S.Y.W. Hatzakis, A. 2015-01-01 https://pergamos.lib.uoa.gr/uoa/dl/object/uoadl:3009673 Αγγλικά English eng uoadl:3009673 https://pergamos.lib.uoa.gr/uoa/dl/object/uoadl:3009673 scientific_publication_article Επιστημονική δημοσίευση - Άρθρο Περιοδικού Scientific publication - Journal Article 2015 ftnkunivathens 2024-01-18T18:11:41Z The evolution of hepatitis B virus (HBV), particularly its origins and evolutionary timescale, has been the subject of debate. Three major scenarios have been proposed, variously placing the origin of HBV in humans and great apes from some million years to only a few thousand years ago (ka). To compare these scenarios, we analyzed 105 full-length HBV genome sequences from all major genotypes sampled globally. We found a high correlation between the demographic histories of HBV and humans, as well as coincidence in the times of origin of specific subgenotypes with human migrations giving rise to their host indigenous populations. Together with phylogenetic evidence, this suggests that HBV has co-expanded with modern humans. Based on the co-expansion, we conducted a Bayesian dating analysis to estimate a precise evolutionary timescale for HBV. Five calibrations were used at the origins of F/H genotypes, D4, C3 and B6 from respective indigenous populations in the Pacific and Arctic and A5 from Haiti. The estimated time for the origin of HBV was 34.1ka (95% highest posterior density interval 27.6-41.3ka), coinciding with the dispersal of modern non-African humans. Our study, the first to use full-length HBV sequences, places a precise timescale on the HBV epidemic and also shows that the "branching paradox" of the more divergent genotypes F/H from Amerindians is due to an accelerated substitution rate, probably driven by positive selection. This may explain previously observed differences in the natural history of HBV between genotypes F1 and A2, B1, and D. © 2015 Elsevier Inc. Article in Journal/Newspaper Arctic Pergamos - Library and Information Center of National and Kapodistrian University of Athens Arctic Pacific
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description The evolution of hepatitis B virus (HBV), particularly its origins and evolutionary timescale, has been the subject of debate. Three major scenarios have been proposed, variously placing the origin of HBV in humans and great apes from some million years to only a few thousand years ago (ka). To compare these scenarios, we analyzed 105 full-length HBV genome sequences from all major genotypes sampled globally. We found a high correlation between the demographic histories of HBV and humans, as well as coincidence in the times of origin of specific subgenotypes with human migrations giving rise to their host indigenous populations. Together with phylogenetic evidence, this suggests that HBV has co-expanded with modern humans. Based on the co-expansion, we conducted a Bayesian dating analysis to estimate a precise evolutionary timescale for HBV. Five calibrations were used at the origins of F/H genotypes, D4, C3 and B6 from respective indigenous populations in the Pacific and Arctic and A5 from Haiti. The estimated time for the origin of HBV was 34.1ka (95% highest posterior density interval 27.6-41.3ka), coinciding with the dispersal of modern non-African humans. Our study, the first to use full-length HBV sequences, places a precise timescale on the HBV epidemic and also shows that the "branching paradox" of the more divergent genotypes F/H from Amerindians is due to an accelerated substitution rate, probably driven by positive selection. This may explain previously observed differences in the natural history of HBV between genotypes F1 and A2, B1, and D. © 2015 Elsevier Inc.
format Article in Journal/Newspaper
author Paraskevis, D.
Angelis, K.
Magiorkinis, G.
Kostaki, E.
Ho, S.Y.W.
Hatzakis, A.
spellingShingle Paraskevis, D.
Angelis, K.
Magiorkinis, G.
Kostaki, E.
Ho, S.Y.W.
Hatzakis, A.
Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
author_facet Paraskevis, D.
Angelis, K.
Magiorkinis, G.
Kostaki, E.
Ho, S.Y.W.
Hatzakis, A.
author_sort Paraskevis, D.
title Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
title_short Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
title_full Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
title_fullStr Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
title_full_unstemmed Dating the origin of hepatitis B virus reveals higher substitution rate and adaptation on the branch leading to F/H genotypes
title_sort dating the origin of hepatitis b virus reveals higher substitution rate and adaptation on the branch leading to f/h genotypes
publishDate 2015
url https://pergamos.lib.uoa.gr/uoa/dl/object/uoadl:3009673
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