All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity

<p>Abstract</p> <p>Background</p> <p>The recent 2009 (H1N1) influenza A pandemic saw a rapid spread of the virus to essentially all parts of the world. In the course of its evolution, the virus acquired many mutations, some of which have been investigated in the context...

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Main Authors: Eisenhaber Frank, Sirota Fernanda L, Cui Lin, Maria de Paiva Terezinha, Santos Cecília LS, Lee Raphael TC, Maurer-Stroh Sebastian
Format: Article
Language:English
Published: BMC 2010-11-01
Series:Virology Journal
Online Access:http://www.virologyj.com/content/7/1/297
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spelling doaj-e9aaacc87e834a3f82fbfb148ba7e2bd2020-11-25T01:01:01ZengBMCVirology Journal1743-422X2010-11-017129710.1186/1743-422X-7-297All that glitters is not gold - founder effects complicate associations of flu mutations to disease severityEisenhaber FrankSirota Fernanda LCui LinMaria de Paiva TerezinhaSantos Cecília LSLee Raphael TCMaurer-Stroh Sebastian<p>Abstract</p> <p>Background</p> <p>The recent 2009 (H1N1) influenza A pandemic saw a rapid spread of the virus to essentially all parts of the world. In the course of its evolution, the virus acquired many mutations, some of which have been investigated in the context of increased severity due to high occurrences in fatal cases. For example, statements such as: "42.9% of individuals who died from laboratory-confirmed cases of the pandemic (H1N1) were infected with the hemagglutinin (HA) Q310 H mutant virus." give the impression that HA-Q310 H would be highly dangerous or important, while careful consideration of all available data suggests that this is unlikely to be the case.</p> <p>Results</p> <p>We compare the mutations HA-Q310 H, PB2-K340N, HA-D239N and HA-D239G using whole genome phylogenetic trees, structural modeling in their 3 D context and complete epidemiological data from sequences to clinical outcomes. HA-Q310 H and PB2-K340N appear as isolated subtrees in the phylogenetic analysis pointing to founder effects which is consistent with their clustered temporal appearance as well as the lack of an immediate structural basis that could explain a change of phenotypes. Considering the prevailing viral genomic background, shared origin of samples (all from the city of Sao Paulo) and narrow temporal window (all death case samples within 1 month), it becomes clear that HA-Q310 H was actually a generally common mutation in the region at that time which could readily explain its increased occurrence among the few analyzed fatal cases without requiring necessarily an association with severity. In further support of this, we highlight 3 mild cases with the HA-Q310 H mutation.</p> <p>Conclusions</p> <p>We argue that claims of severity of any current and future flu mutation need to be critically considered in the light of phylogenetic, structural and detailed epidemiological data to distinguish increased occurrence due to possible founder effects rather than real phenotypic changes.</p> http://www.virologyj.com/content/7/1/297
collection DOAJ
language English
format Article
sources DOAJ
author Eisenhaber Frank
Sirota Fernanda L
Cui Lin
Maria de Paiva Terezinha
Santos Cecília LS
Lee Raphael TC
Maurer-Stroh Sebastian
spellingShingle Eisenhaber Frank
Sirota Fernanda L
Cui Lin
Maria de Paiva Terezinha
Santos Cecília LS
Lee Raphael TC
Maurer-Stroh Sebastian
All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
Virology Journal
author_facet Eisenhaber Frank
Sirota Fernanda L
Cui Lin
Maria de Paiva Terezinha
Santos Cecília LS
Lee Raphael TC
Maurer-Stroh Sebastian
author_sort Eisenhaber Frank
title All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
title_short All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
title_full All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
title_fullStr All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
title_full_unstemmed All that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
title_sort all that glitters is not gold - founder effects complicate associations of flu mutations to disease severity
publisher BMC
series Virology Journal
issn 1743-422X
publishDate 2010-11-01
description <p>Abstract</p> <p>Background</p> <p>The recent 2009 (H1N1) influenza A pandemic saw a rapid spread of the virus to essentially all parts of the world. In the course of its evolution, the virus acquired many mutations, some of which have been investigated in the context of increased severity due to high occurrences in fatal cases. For example, statements such as: "42.9% of individuals who died from laboratory-confirmed cases of the pandemic (H1N1) were infected with the hemagglutinin (HA) Q310 H mutant virus." give the impression that HA-Q310 H would be highly dangerous or important, while careful consideration of all available data suggests that this is unlikely to be the case.</p> <p>Results</p> <p>We compare the mutations HA-Q310 H, PB2-K340N, HA-D239N and HA-D239G using whole genome phylogenetic trees, structural modeling in their 3 D context and complete epidemiological data from sequences to clinical outcomes. HA-Q310 H and PB2-K340N appear as isolated subtrees in the phylogenetic analysis pointing to founder effects which is consistent with their clustered temporal appearance as well as the lack of an immediate structural basis that could explain a change of phenotypes. Considering the prevailing viral genomic background, shared origin of samples (all from the city of Sao Paulo) and narrow temporal window (all death case samples within 1 month), it becomes clear that HA-Q310 H was actually a generally common mutation in the region at that time which could readily explain its increased occurrence among the few analyzed fatal cases without requiring necessarily an association with severity. In further support of this, we highlight 3 mild cases with the HA-Q310 H mutation.</p> <p>Conclusions</p> <p>We argue that claims of severity of any current and future flu mutation need to be critically considered in the light of phylogenetic, structural and detailed epidemiological data to distinguish increased occurrence due to possible founder effects rather than real phenotypic changes.</p>
url http://www.virologyj.com/content/7/1/297
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