High-resolution antibody dynamics of vaccine-induced immune responses

Uri Laserson; Francois Vigneault; Daniel Gadala-Maria; Gur Yaari; Mohamed Uduman; Jason A. Vander Heiden; William Kelton; Sang Taek Jung; Yi Liu; Jonathan Laserson; Raj Chari; Je Hyuk Lee; Ido Bachelet; Brendan Hickey; Erez Lieberman-Aiden; Bozena Hanczaruk; Birgitte B. Simen; Michael Egholm; Daphne Koller; George Georgiou; Steven H. Kleinstein; George M. Church

doi:10.1073/pnas.1323862111

High-resolution antibody dynamics of vaccine-induced immune responses

Uri Laserson
, Francois Vigneault
, Daniel Gadala-Maria
, Gur Yaari
, Mohamed Uduman
, Jason A. Vander Heiden
, William Kelton
, Sang Taek Jung
, Yi Liu
, Jonathan Laserson
, Raj Chari
, Je Hyuk Lee
, Ido Bachelet
, Brendan Hickey
, Erez Lieberman-Aiden
, Bozena Hanczaruk
, Birgitte B. Simen
, Michael Egholm
, Daphne Koller
, George Georgiou

Steven H. Kleinstein, George M. Church

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

143 Scopus citations

Abstract

The adaptive immune system confers protection by generating a diverse repertoire of antibody receptors that are rapidly expanded and contracted in response to specific targets. Next-generation DNA sequencing now provides the opportunity to survey this complex and vast repertoire. In the present work, we describe a set of tools for the analysis of antibody repertoires and their application to elucidating the dynamics of the response to viral vaccination in human volunteers. By analyzing data from38 separate blood samples across 2 y, we found that the use of the germ-line library of V and J segments is conserved between individuals over time. Surprisingly, there appeared to be no correlation between the use level of a particular VJ combination and degree of expansion. We found the antibody RNA repertoire in each volunteer to be highly dynamic, with each individual displaying qualitatively different response dynamics. By using combinatorial phage display, we screened selected VH genes paired with their corresponding VL library for affinity against the vaccine antigens. Altogether, this work presents an additional set of tools for profiling the human antibody repertoire and demonstrates characterization of the fast repertoire dynamics through time in multiple individuals responding to an immune challenge.

Original language	English
Pages (from-to)	4928-4933
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	111
Issue number	13
DOIs	https://doi.org/10.1073/pnas.1323862111
State	Published - 1 Apr 2014
Externally published	Yes

Funding

Funders	Funder number
National Human Genome Research Institute	T32HG002295
NIH Office of the Director	DP2OD008540
U.S. National Library of Medicine	T15LM007056

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

Immunology
Influenza
Next-generation sequencing

Access to Document

10.1073/pnas.1323862111

Cite this

Laserson, U., Vigneault, F., Gadala-Maria, D., Yaari, G., Uduman, M., Vander Heiden, J. A., Kelton, W., Jung, S. T., Liu, Y., Laserson, J., Chari, R., Lee, J. H., Bachelet, I., Hickey, B., Lieberman-Aiden, E., Hanczaruk, B., Simen, B. B., Egholm, M., Koller, D., ... Church, G. M. (2014). High-resolution antibody dynamics of vaccine-induced immune responses. Proceedings of the National Academy of Sciences of the United States of America, 111(13), 4928-4933. https://doi.org/10.1073/pnas.1323862111

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title = "High-resolution antibody dynamics of vaccine-induced immune responses",

abstract = "The adaptive immune system confers protection by generating a diverse repertoire of antibody receptors that are rapidly expanded and contracted in response to specific targets. Next-generation DNA sequencing now provides the opportunity to survey this complex and vast repertoire. In the present work, we describe a set of tools for the analysis of antibody repertoires and their application to elucidating the dynamics of the response to viral vaccination in human volunteers. By analyzing data from38 separate blood samples across 2 y, we found that the use of the germ-line library of V and J segments is conserved between individuals over time. Surprisingly, there appeared to be no correlation between the use level of a particular VJ combination and degree of expansion. We found the antibody RNA repertoire in each volunteer to be highly dynamic, with each individual displaying qualitatively different response dynamics. By using combinatorial phage display, we screened selected VH genes paired with their corresponding VL library for affinity against the vaccine antigens. Altogether, this work presents an additional set of tools for profiling the human antibody repertoire and demonstrates characterization of the fast repertoire dynamics through time in multiple individuals responding to an immune challenge.",

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Laserson, U, Vigneault, F, Gadala-Maria, D, Yaari, G, Uduman, M, Vander Heiden, JA, Kelton, W, Jung, ST, Liu, Y, Laserson, J, Chari, R, Lee, JH, Bachelet, I, Hickey, B, Lieberman-Aiden, E, Hanczaruk, B, Simen, BB, Egholm, M, Koller, D, Georgiou, G, Kleinstein, SH & Church, GM 2014, 'High-resolution antibody dynamics of vaccine-induced immune responses', Proceedings of the National Academy of Sciences of the United States of America, vol. 111, no. 13, pp. 4928-4933. https://doi.org/10.1073/pnas.1323862111

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T1 - High-resolution antibody dynamics of vaccine-induced immune responses

AU - Laserson, Uri

AU - Vigneault, Francois

AU - Gadala-Maria, Daniel

AU - Yaari, Gur

AU - Uduman, Mohamed

AU - Vander Heiden, Jason A.

AU - Kelton, William

AU - Jung, Sang Taek

AU - Liu, Yi

AU - Laserson, Jonathan

AU - Chari, Raj

AU - Lee, Je Hyuk

AU - Bachelet, Ido

AU - Hickey, Brendan

AU - Lieberman-Aiden, Erez

AU - Hanczaruk, Bozena

AU - Simen, Birgitte B.

AU - Egholm, Michael

AU - Koller, Daphne

AU - Georgiou, George

AU - Kleinstein, Steven H.

AU - Church, George M.

PY - 2014/4/1

Y1 - 2014/4/1

N2 - The adaptive immune system confers protection by generating a diverse repertoire of antibody receptors that are rapidly expanded and contracted in response to specific targets. Next-generation DNA sequencing now provides the opportunity to survey this complex and vast repertoire. In the present work, we describe a set of tools for the analysis of antibody repertoires and their application to elucidating the dynamics of the response to viral vaccination in human volunteers. By analyzing data from38 separate blood samples across 2 y, we found that the use of the germ-line library of V and J segments is conserved between individuals over time. Surprisingly, there appeared to be no correlation between the use level of a particular VJ combination and degree of expansion. We found the antibody RNA repertoire in each volunteer to be highly dynamic, with each individual displaying qualitatively different response dynamics. By using combinatorial phage display, we screened selected VH genes paired with their corresponding VL library for affinity against the vaccine antigens. Altogether, this work presents an additional set of tools for profiling the human antibody repertoire and demonstrates characterization of the fast repertoire dynamics through time in multiple individuals responding to an immune challenge.

AB - The adaptive immune system confers protection by generating a diverse repertoire of antibody receptors that are rapidly expanded and contracted in response to specific targets. Next-generation DNA sequencing now provides the opportunity to survey this complex and vast repertoire. In the present work, we describe a set of tools for the analysis of antibody repertoires and their application to elucidating the dynamics of the response to viral vaccination in human volunteers. By analyzing data from38 separate blood samples across 2 y, we found that the use of the germ-line library of V and J segments is conserved between individuals over time. Surprisingly, there appeared to be no correlation between the use level of a particular VJ combination and degree of expansion. We found the antibody RNA repertoire in each volunteer to be highly dynamic, with each individual displaying qualitatively different response dynamics. By using combinatorial phage display, we screened selected VH genes paired with their corresponding VL library for affinity against the vaccine antigens. Altogether, this work presents an additional set of tools for profiling the human antibody repertoire and demonstrates characterization of the fast repertoire dynamics through time in multiple individuals responding to an immune challenge.

KW - Immunology

KW - Influenza

KW - Next-generation sequencing

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C2 - 24639495

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JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 13

ER -

High-resolution antibody dynamics of vaccine-induced immune responses

Abstract

Funding

UN SDGs

Keywords

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