HLA tapasin independence: broader peptide repertoire and HIV control

Arman A. Bashirova; Mathias Viard; Vivek Naranbhai; Alba Grifoni; Wilfredo Garcia-Beltran; Marjan Akdag; Yuko Yuki; Xiaojiang Gao; Colm O’hUigin; Malini Raghavan; Steven Wolinsky; Jay H. Bream; Priya Duggal; Jeremy Martinson; Nelson L. Michael; Gregory D. Kirk; Susan P. Buchbinder; David Haas; James J. Goedert; Steven G. Deeks; Jacques Fellay; Bruce Walker; Philip Goulder; Peter Cresswell; Tim Elliott; Alessandro Sette; Jonathan Carlson; Mary Carrington

doi:10.1073/pnas.2013554117

HLA tapasin independence: broader peptide repertoire and HIV control

Arman A. Bashirova, Mathias Viard, Vivek Naranbhai, Alba Grifoni, Wilfredo Garcia-Beltran, Marjan Akdag, Yuko Yuki, Xiaojiang Gao, Colm O’hUigin, Malini Raghavan, Steven Wolinsky, Jay H. Bream, Priya Duggal, Jeremy Martinson, Nelson L. Michael, Gregory D. Kirk, Susan P. Buchbinder, David Haas, James J. Goedert, Steven G. DeeksJacques Fellay, Bruce Walker, Philip Goulder, Peter Cresswell, Tim Elliott, Alessandro Sette, Jonathan Carlson, Mary Carrington

Bloomberg School of Public Health

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

6 Scopus citations

Abstract

Human leukocyte antigen (HLA) class I allotypes vary in thei ability to present peptides in the absence of tapasin, an essentia component of the peptide loading complex. We quantified tapasi dependence of all allotypes that are common in European an African Americans (n = 97), which revealed a broad continuum o values. Ex vivo examination of cytotoxic T cell responses to th entire HIV-1 proteome from infected subjects indicates tha tapasin-dependent allotypes present a more limited set of distinc peptides than do tapasin-independent allotypes, data supporte by computational predictions. This suggests that variation in tapa sin dependence may impact the strength of the immune response by altering peptide repertoire size. In support of this model, w observed that individuals carrying HLA class I genotypes charac terized by greater tapasin independence progress more slowly t AIDS and maintain lower viral loads, presumably due to increase breadth of peptide presentation. Thus, tapasin dependence level like HLA zygosity, may serve as a means to restrict or expan breadth of the HLA-I peptide repertoire across humans, ultimatel influencing immune responses to pathogens and vaccines.

Original language	English (US)
Pages (from-to)	28232-28238
Number of pages	7
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	117
Issue number	45
DOIs	https://doi.org/10.1073/pnas.2013554117
State	Published - Nov 10 2020

Keywords

HLA | tapasin | peptide repertoire

ASJC Scopus subject areas

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10.1073/pnas.2013554117

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Bashirova, A. A., Viard, M., Naranbhai, V., Grifoni, A., Garcia-Beltran, W., Akdag, M., Yuki, Y., Gao, X., O’hUigin, C., Raghavan, M., Wolinsky, S., Bream, J. H., Duggal, P., Martinson, J., Michael, N. L., Kirk, G. D., Buchbinder, S. P., Haas, D., Goedert, J. J., ... Carrington, M. (2020). HLA tapasin independence: broader peptide repertoire and HIV control. Proceedings of the National Academy of Sciences of the United States of America, 117(45), 28232-28238. https://doi.org/10.1073/pnas.2013554117

Bashirova, AA, Viard, M, Naranbhai, V, Grifoni, A, Garcia-Beltran, W, Akdag, M, Yuki, Y, Gao, X, O’hUigin, C, Raghavan, M, Wolinsky, S, Bream, JH , Duggal, P, Martinson, J, Michael, NL, Kirk, GD, Buchbinder, SP, Haas, D, Goedert, JJ, Deeks, SG, Fellay, J, Walker, B, Goulder, P, Cresswell, P, Elliott, T, Sette, A, Carlson, J & Carrington, M 2020, 'HLA tapasin independence: broader peptide repertoire and HIV control', Proceedings of the National Academy of Sciences of the United States of America, vol. 117, no. 45, pp. 28232-28238. https://doi.org/10.1073/pnas.2013554117

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abstract = "Human leukocyte antigen (HLA) class I allotypes vary in thei ability to present peptides in the absence of tapasin, an essentia component of the peptide loading complex. We quantified tapasi dependence of all allotypes that are common in European an African Americans (n = 97), which revealed a broad continuum o values. Ex vivo examination of cytotoxic T cell responses to th entire HIV-1 proteome from infected subjects indicates tha tapasin-dependent allotypes present a more limited set of distinc peptides than do tapasin-independent allotypes, data supporte by computational predictions. This suggests that variation in tapa sin dependence may impact the strength of the immune response by altering peptide repertoire size. In support of this model, w observed that individuals carrying HLA class I genotypes charac terized by greater tapasin independence progress more slowly t AIDS and maintain lower viral loads, presumably due to increase breadth of peptide presentation. Thus, tapasin dependence level like HLA zygosity, may serve as a means to restrict or expan breadth of the HLA-I peptide repertoire across humans, ultimatel influencing immune responses to pathogens and vaccines.",

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T2 - broader peptide repertoire and HIV control

AU - Bashirova, Arman A.

AU - Viard, Mathias

AU - Naranbhai, Vivek

AU - Grifoni, Alba

AU - Garcia-Beltran, Wilfredo

AU - Akdag, Marjan

AU - Yuki, Yuko

AU - Gao, Xiaojiang

AU - O’hUigin, Colm

AU - Raghavan, Malini

AU - Wolinsky, Steven

AU - Bream, Jay H.

AU - Duggal, Priya

AU - Martinson, Jeremy

AU - Michael, Nelson L.

AU - Kirk, Gregory D.

AU - Buchbinder, Susan P.

AU - Haas, David

AU - Goedert, James J.

AU - Deeks, Steven G.

AU - Fellay, Jacques

AU - Walker, Bruce

AU - Goulder, Philip

AU - Cresswell, Peter

AU - Elliott, Tim

AU - Sette, Alessandro

AU - Carlson, Jonathan

AU - Carrington, Mary

PY - 2020/11/10

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N2 - Human leukocyte antigen (HLA) class I allotypes vary in thei ability to present peptides in the absence of tapasin, an essentia component of the peptide loading complex. We quantified tapasi dependence of all allotypes that are common in European an African Americans (n = 97), which revealed a broad continuum o values. Ex vivo examination of cytotoxic T cell responses to th entire HIV-1 proteome from infected subjects indicates tha tapasin-dependent allotypes present a more limited set of distinc peptides than do tapasin-independent allotypes, data supporte by computational predictions. This suggests that variation in tapa sin dependence may impact the strength of the immune response by altering peptide repertoire size. In support of this model, w observed that individuals carrying HLA class I genotypes charac terized by greater tapasin independence progress more slowly t AIDS and maintain lower viral loads, presumably due to increase breadth of peptide presentation. Thus, tapasin dependence level like HLA zygosity, may serve as a means to restrict or expan breadth of the HLA-I peptide repertoire across humans, ultimatel influencing immune responses to pathogens and vaccines.

AB - Human leukocyte antigen (HLA) class I allotypes vary in thei ability to present peptides in the absence of tapasin, an essentia component of the peptide loading complex. We quantified tapasi dependence of all allotypes that are common in European an African Americans (n = 97), which revealed a broad continuum o values. Ex vivo examination of cytotoxic T cell responses to th entire HIV-1 proteome from infected subjects indicates tha tapasin-dependent allotypes present a more limited set of distinc peptides than do tapasin-independent allotypes, data supporte by computational predictions. This suggests that variation in tapa sin dependence may impact the strength of the immune response by altering peptide repertoire size. In support of this model, w observed that individuals carrying HLA class I genotypes charac terized by greater tapasin independence progress more slowly t AIDS and maintain lower viral loads, presumably due to increase breadth of peptide presentation. Thus, tapasin dependence level like HLA zygosity, may serve as a means to restrict or expan breadth of the HLA-I peptide repertoire across humans, ultimatel influencing immune responses to pathogens and vaccines.

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HLA tapasin independence: broader peptide repertoire and HIV control

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