Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals

SPARTAC Trial Investigators; Trial Steering Committee (TSC); Data and Safety Monitoring Committee (DSMC); Clinical Endpoint Review Committee

doi:10.1098/rstb.2014.0241

Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals

SPARTAC Trial Investigators, Trial Steering Committee (TSC), Data and Safety Monitoring Committee (DSMC), Clinical Endpoint Review Committee

Research output: Contribution to journal › Article › peer-review

22 Citations (Scopus)

Abstract

Advances in immunoglobulin (Ig) sequencing technology are leading to new perspectives on immune system dynamics. Much research in this nascent field has focused on resolving immune responses to viral infection. However, the dynamics of B-cell diversity in early HIV infection, and in response to antiretroviral therapy, are still poorly understood. Here, we investigate these dynamics through bulk Ig sequencing of samples collected over 2 years from a group of eight HIV-1 infected patients, five of whom received antiretroviral therapy during the first half of the study period. We applied previously published methods for visualizing and quantifying B-cell sequence diversity, including the Gini index, and compared their efficacy to alternative measures. While we found significantly greater clonal structure in HIVinfected patients versus healthy controls, within HIV patients, we observed no significant relationships between statistics of B-cell clonal expansion and clinical variables such as viral load and CD4⁺ count. Although there are many potential explanations for this,we suggest that important factors include poor sampling resolution and complex B-cell dynamics that are difficult to summarize using simple summary statistics. Importantly,we find a significant association between observed Gini indices and sequencing read depth, andwe conclude that more robust analytical methods and a closer integration of experimental and theoretical work is needed to further our understanding of B-cell repertoire diversity during viral infection.

Original language	English
Journal	Philosophical transactions of the Royal Society of London. Series B, Biological sciences
Volume	370
Issue number	1676
DOIs	https://doi.org/10.1098/rstb.2014.0241
Publication status	Published - 20 Jul 2015
Externally published	Yes

Bibliographical note

Publisher Copyright:
© 2015 The Authors.

Keywords

B-cell receptor
Diversity
Gini index

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1098/rstb.2014.0241

Cite this

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title = "Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals",

abstract = "Advances in immunoglobulin (Ig) sequencing technology are leading to new perspectives on immune system dynamics. Much research in this nascent field has focused on resolving immune responses to viral infection. However, the dynamics of B-cell diversity in early HIV infection, and in response to antiretroviral therapy, are still poorly understood. Here, we investigate these dynamics through bulk Ig sequencing of samples collected over 2 years from a group of eight HIV-1 infected patients, five of whom received antiretroviral therapy during the first half of the study period. We applied previously published methods for visualizing and quantifying B-cell sequence diversity, including the Gini index, and compared their efficacy to alternative measures. While we found significantly greater clonal structure in HIVinfected patients versus healthy controls, within HIV patients, we observed no significant relationships between statistics of B-cell clonal expansion and clinical variables such as viral load and CD4+ count. Although there are many potential explanations for this,we suggest that important factors include poor sampling resolution and complex B-cell dynamics that are difficult to summarize using simple summary statistics. Importantly,we find a significant association between observed Gini indices and sequencing read depth, andwe conclude that more robust analytical methods and a closer integration of experimental and theoretical work is needed to further our understanding of B-cell repertoire diversity during viral infection.",

keywords = "B-cell receptor, Diversity, Gini index",

author = "{SPARTAC Trial Investigators} and {Trial Steering Committee (TSC)} and {Data and Safety Monitoring Committee (DSMC)} and {Clinical Endpoint Review Committee} and Hoehn, {Kenneth B.} and Astrid Gall and Rachael Bashford-Rogers and Fidler, {S. J.} and S. Kaye and Weber, {J. N.} and McClure, {M. O.} and Paul Kellam and Pybus, {Oliver G.} and A. Breckenridge and P. Clayden and C. Conlon and F. Conradie and J. Kaldor and F. Maggiolo and F. Ssali and Cooper, {D. A.} and P. Kaleebu and G. Ramjee and M. Schechter and G. Tambussi and J. Weber and S. Fidler and A. Babiker and T. Peto and A. McLaren and V. Beral and G. Chene and J. Hakim and K. Porter and M. Thomason and F. Ewings and M. Gabriel and D. Johnson and K. Thompson and A. Cursley and K. Donegan and E. Fossey and P. Kelleher and K. Lee and B. Murphy and D. Nock and R. Phillips and J. Frater and {Ohm Laursen}, L. and N. Robinson and P. Goulder and H. Brown and M. McClure and S. Taylor",

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doi = "10.1098/rstb.2014.0241",

language = "English",

volume = "370",

journal = "Philosophical transactions of the Royal Society of London. Series B, Biological sciences",

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SPARTAC Trial Investigators, Trial Steering Committee (TSC), Data and Safety Monitoring Committee (DSMC) & Clinical Endpoint Review Committee 2015, 'Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals', Philosophical transactions of the Royal Society of London. Series B, Biological sciences, vol. 370, no. 1676. https://doi.org/10.1098/rstb.2014.0241

Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals. / SPARTAC Trial Investigators; Trial Steering Committee (TSC); Data and Safety Monitoring Committee (DSMC) et al.
In: Philosophical transactions of the Royal Society of London. Series B, Biological sciences, Vol. 370, No. 1676, 20.07.2015.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals

AU - SPARTAC Trial Investigators

AU - Trial Steering Committee (TSC)

AU - Data and Safety Monitoring Committee (DSMC)

AU - Clinical Endpoint Review Committee

AU - Hoehn, Kenneth B.

AU - Gall, Astrid

AU - Bashford-Rogers, Rachael

AU - Fidler, S. J.

AU - Kaye, S.

AU - Weber, J. N.

AU - McClure, M. O.

AU - Kellam, Paul

AU - Pybus, Oliver G.

AU - Breckenridge, A.

AU - Clayden, P.

AU - Conlon, C.

AU - Conradie, F.

AU - Kaldor, J.

AU - Maggiolo, F.

AU - Ssali, F.

AU - Cooper, D. A.

AU - Kaleebu, P.

AU - Ramjee, G.

AU - Schechter, M.

AU - Tambussi, G.

AU - Weber, J.

AU - Fidler, S.

AU - Babiker, A.

AU - Peto, T.

AU - McLaren, A.

AU - Beral, V.

AU - Chene, G.

AU - Hakim, J.

AU - Porter, K.

AU - Thomason, M.

AU - Ewings, F.

AU - Gabriel, M.

AU - Johnson, D.

AU - Thompson, K.

AU - Cursley, A.

AU - Donegan, K.

AU - Fossey, E.

AU - Kelleher, P.

AU - Lee, K.

AU - Murphy, B.

AU - Nock, D.

AU - Phillips, R.

AU - Frater, J.

AU - Ohm Laursen, L.

AU - Robinson, N.

AU - Goulder, P.

AU - Brown, H.

AU - McClure, M.

AU - Taylor, S.

PY - 2015/7/20

Y1 - 2015/7/20

N2 - Advances in immunoglobulin (Ig) sequencing technology are leading to new perspectives on immune system dynamics. Much research in this nascent field has focused on resolving immune responses to viral infection. However, the dynamics of B-cell diversity in early HIV infection, and in response to antiretroviral therapy, are still poorly understood. Here, we investigate these dynamics through bulk Ig sequencing of samples collected over 2 years from a group of eight HIV-1 infected patients, five of whom received antiretroviral therapy during the first half of the study period. We applied previously published methods for visualizing and quantifying B-cell sequence diversity, including the Gini index, and compared their efficacy to alternative measures. While we found significantly greater clonal structure in HIVinfected patients versus healthy controls, within HIV patients, we observed no significant relationships between statistics of B-cell clonal expansion and clinical variables such as viral load and CD4+ count. Although there are many potential explanations for this,we suggest that important factors include poor sampling resolution and complex B-cell dynamics that are difficult to summarize using simple summary statistics. Importantly,we find a significant association between observed Gini indices and sequencing read depth, andwe conclude that more robust analytical methods and a closer integration of experimental and theoretical work is needed to further our understanding of B-cell repertoire diversity during viral infection.

AB - Advances in immunoglobulin (Ig) sequencing technology are leading to new perspectives on immune system dynamics. Much research in this nascent field has focused on resolving immune responses to viral infection. However, the dynamics of B-cell diversity in early HIV infection, and in response to antiretroviral therapy, are still poorly understood. Here, we investigate these dynamics through bulk Ig sequencing of samples collected over 2 years from a group of eight HIV-1 infected patients, five of whom received antiretroviral therapy during the first half of the study period. We applied previously published methods for visualizing and quantifying B-cell sequence diversity, including the Gini index, and compared their efficacy to alternative measures. While we found significantly greater clonal structure in HIVinfected patients versus healthy controls, within HIV patients, we observed no significant relationships between statistics of B-cell clonal expansion and clinical variables such as viral load and CD4+ count. Although there are many potential explanations for this,we suggest that important factors include poor sampling resolution and complex B-cell dynamics that are difficult to summarize using simple summary statistics. Importantly,we find a significant association between observed Gini indices and sequencing read depth, andwe conclude that more robust analytical methods and a closer integration of experimental and theoretical work is needed to further our understanding of B-cell repertoire diversity during viral infection.

KW - B-cell receptor

KW - Diversity

KW - Gini index

UR - http://www.scopus.com/inward/record.url?scp=85000814907&partnerID=8YFLogxK

U2 - 10.1098/rstb.2014.0241

DO - 10.1098/rstb.2014.0241

M3 - Article

C2 - 26194755

AN - SCOPUS:85000814907

SN - 0962-8436

VL - 370

JO - Philosophical transactions of the Royal Society of London. Series B, Biological sciences

JF - Philosophical transactions of the Royal Society of London. Series B, Biological sciences

IS - 1676

ER -

Dynamics of immunoglobulin sequence diversity in HIV-1 infected individuals

Abstract

Bibliographical note

Keywords

UN SDGs

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