Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes

Tara Bancroft; Blair L. DeBuysscher; Connor Weidle; Allison Schwartz; Abigail Wall; Matthew D. Gray; Junli Feng; Holly R. Steach; Kristin S. Fitzpatrick; Mesfin M. Gewe; Patrick D. Skog; Colleen Doyle-Cooper; Takayuki Ota; Roland K. Strong; David Nemazee; Marie Pancera; Leonidas Stamatatos; Andrew T. McGuire; Justin J. Taylor

doi:10.1084/jem.20190164

Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes

Tara Bancroft
, Blair L. DeBuysscher
, Connor Weidle
, Allison Schwartz
, Abigail Wall
, Matthew D. Gray
, Junli Feng
, Holly R. Steach
, Kristin S. Fitzpatrick
, Mesfin M. Gewe
, Patrick D. Skog
, Colleen Doyle-Cooper
, Takayuki Ota
, Roland K. Strong
, David Nemazee
, Marie Pancera
, Leonidas Stamatatos
, Andrew T. McGuire
, Justin J. Taylor

Biomedical and Pharmaceutical Sciences

Fred Hutchinson Cancer Research Center
Scripps Research Institute
University of Washington

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

21 Scopus citations

Abstract

Many tested vaccines fail to provide protection against disease despite the induction of antibodies that bind the pathogen of interest. In light of this, there is much interest in rationally designed subunit vaccines that direct the antibody response to protective epitopes. Here, we produced a panel of anti-idiotype antibodies able to specifically recognize the inferred germline version of the human immunodeficiency virus 1 (HIV-1) broadly neutralizing antibody b12 (iglb12). We determined the crystal structure of two anti-idiotypes in complex with iglb12 and used these anti-idiotypes to identify rare naive human B cells expressing B cell receptors with similarity to iglb12. Immunization with a multimerized version of this anti-idiotype induced the proliferation of transgenic murine B cells expressing the iglb12 heavy chain in vivo, despite the presence of deletion and anergy within this population. Together, our data indicate that anti-idiotypes are a valuable tool for the study and induction of potentially protective antibodies.

Original language	English
Pages (from-to)	2331-2347
Number of pages	17
Journal	Journal of Experimental Medicine
Volume	216
Issue number	10
DOIs	https://doi.org/10.1084/jem.20190164
State	Published - 2019

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10.1084/jem.20190164

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Bancroft, T., DeBuysscher, B. L., Weidle, C., Schwartz, A., Wall, A., Gray, M. D., Feng, J., Steach, H. R., Fitzpatrick, K. S., Gewe, M. M., Skog, P. D., Doyle-Cooper, C., Ota, T., Strong, R. K., Nemazee, D., Pancera, M., Stamatatos, L., McGuire, A. T., & Taylor, J. J. (2019). Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes. Journal of Experimental Medicine, 216(10), 2331-2347. https://doi.org/10.1084/jem.20190164

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title = "Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes",

abstract = "Many tested vaccines fail to provide protection against disease despite the induction of antibodies that bind the pathogen of interest. In light of this, there is much interest in rationally designed subunit vaccines that direct the antibody response to protective epitopes. Here, we produced a panel of anti-idiotype antibodies able to specifically recognize the inferred germline version of the human immunodeficiency virus 1 (HIV-1) broadly neutralizing antibody b12 (iglb12). We determined the crystal structure of two anti-idiotypes in complex with iglb12 and used these anti-idiotypes to identify rare naive human B cells expressing B cell receptors with similarity to iglb12. Immunization with a multimerized version of this anti-idiotype induced the proliferation of transgenic murine B cells expressing the iglb12 heavy chain in vivo, despite the presence of deletion and anergy within this population. Together, our data indicate that anti-idiotypes are a valuable tool for the study and induction of potentially protective antibodies.",

author = "Tara Bancroft and DeBuysscher, \{Blair L.\} and Connor Weidle and Allison Schwartz and Abigail Wall and Gray, \{Matthew D.\} and Junli Feng and Steach, \{Holly R.\} and Fitzpatrick, \{Kristin S.\} and Gewe, \{Mesfin M.\} and Skog, \{Patrick D.\} and Colleen Doyle-Cooper and Takayuki Ota and Strong, \{Roland K.\} and David Nemazee and Marie Pancera and Leonidas Stamatatos and McGuire, \{Andrew T.\} and Taylor, \{Justin J.\}",

note = "Publisher Copyright: {\textcopyright} 2019 Bancroft et al.",

year = "2019",

doi = "10.1084/jem.20190164",

language = "English",

volume = "216",

pages = "2331--2347",

journal = "Journal of Experimental Medicine",

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Bancroft, T, DeBuysscher, BL, Weidle, C, Schwartz, A, Wall, A, Gray, MD, Feng, J, Steach, HR, Fitzpatrick, KS, Gewe, MM, Skog, PD, Doyle-Cooper, C, Ota, T, Strong, RK, Nemazee, D, Pancera, M, Stamatatos, L, McGuire, AT & Taylor, JJ 2019, 'Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes', Journal of Experimental Medicine, vol. 216, no. 10, pp. 2331-2347. https://doi.org/10.1084/jem.20190164

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T1 - Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes

AU - Bancroft, Tara

AU - DeBuysscher, Blair L.

AU - Weidle, Connor

AU - Schwartz, Allison

AU - Wall, Abigail

AU - Gray, Matthew D.

AU - Feng, Junli

AU - Steach, Holly R.

AU - Fitzpatrick, Kristin S.

AU - Gewe, Mesfin M.

AU - Skog, Patrick D.

AU - Doyle-Cooper, Colleen

AU - Ota, Takayuki

AU - Strong, Roland K.

AU - Nemazee, David

AU - Pancera, Marie

AU - Stamatatos, Leonidas

AU - McGuire, Andrew T.

AU - Taylor, Justin J.

PY - 2019

Y1 - 2019

N2 - Many tested vaccines fail to provide protection against disease despite the induction of antibodies that bind the pathogen of interest. In light of this, there is much interest in rationally designed subunit vaccines that direct the antibody response to protective epitopes. Here, we produced a panel of anti-idiotype antibodies able to specifically recognize the inferred germline version of the human immunodeficiency virus 1 (HIV-1) broadly neutralizing antibody b12 (iglb12). We determined the crystal structure of two anti-idiotypes in complex with iglb12 and used these anti-idiotypes to identify rare naive human B cells expressing B cell receptors with similarity to iglb12. Immunization with a multimerized version of this anti-idiotype induced the proliferation of transgenic murine B cells expressing the iglb12 heavy chain in vivo, despite the presence of deletion and anergy within this population. Together, our data indicate that anti-idiotypes are a valuable tool for the study and induction of potentially protective antibodies.

AB - Many tested vaccines fail to provide protection against disease despite the induction of antibodies that bind the pathogen of interest. In light of this, there is much interest in rationally designed subunit vaccines that direct the antibody response to protective epitopes. Here, we produced a panel of anti-idiotype antibodies able to specifically recognize the inferred germline version of the human immunodeficiency virus 1 (HIV-1) broadly neutralizing antibody b12 (iglb12). We determined the crystal structure of two anti-idiotypes in complex with iglb12 and used these anti-idiotypes to identify rare naive human B cells expressing B cell receptors with similarity to iglb12. Immunization with a multimerized version of this anti-idiotype induced the proliferation of transgenic murine B cells expressing the iglb12 heavy chain in vivo, despite the presence of deletion and anergy within this population. Together, our data indicate that anti-idiotypes are a valuable tool for the study and induction of potentially protective antibodies.

UR - https://www.scopus.com/pages/publications/85072994082

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DO - 10.1084/jem.20190164

M3 - Article

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AN - SCOPUS:85072994082

SN - 0022-1007

VL - 216

SP - 2331

EP - 2347

JO - Journal of Experimental Medicine

JF - Journal of Experimental Medicine

IS - 10

ER -

Detection and activation of HIV broadly neutralizing antibody precursor B cells using anti-idiotypes

Abstract

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