Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa

Angelique Hölzemer; Christina F. Thobakgale; Camilo A. Jimenez Cruz; Wilfredo F. Garcia-Beltran; Jonathan M. Carlson; Nienke H. van Teijlingen; Jaclyn K. Mann; Manjeetha Jaggernath; Seung-Gu Kang; Christian Körner; Amy W. Chung; Jamie L. Schafer; David T. Evans; Galit Alter; Bruce D. Walker; Philip J. Goulder; Mary Carrington; Pia Hartmann; Thomas Pertel; Ruhong Zhou; Thumbi Ndung'u; Marcus Altfeld

doi:https://doi.org/10.1371/journal.pmed.1001900

Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa

Angelique Hölzemer, Christina F. Thobakgale, Camilo A. Jimenez Cruz, Wilfredo F. Garcia-Beltran, Jonathan M. Carlson, Nienke H. van Teijlingen, Jaclyn K. Mann, Manjeetha Jaggernath, Seung-Gu Kang, Christian Körner, Amy W. Chung, Jamie L. Schafer, David T. Evans, Galit Alter, Bruce D. Walker, Philip J. Goulder, Mary Carrington, Pia Hartmann, Thomas Pertel, Ruhong ZhouThumbi Ndung'u, Marcus Altfeld

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

60 Citations (Scopus)

Abstract

Viruses can evade immune surveillance, but the underlying mechanisms are insufficiently understood. Here, we sought to understand the mechanisms by which natural killer (NK) cells recognize HIV-1-infected cells and how this virus can evade NK-cell-mediated immune pressure. Two sequence mutations in p24 Gag associated with the presence of specific KIR/HLA combined genotypes were identified in HIV-1 clade C viruses from a large cohort of infected, untreated individuals in South Africa (n = 392), suggesting viral escape from KIR+ NK cells through sequence variations within HLA class I-presented epitopes. One sequence polymorphism at position 303 of p24 Gag (TGag303V), selected for in infected individuals with both KIR2DL3 and HLA-C*03:04, enabled significantly better binding of the inhibitory KIR2DL3 receptor to HLA-C*03:04-expressing cells presenting this variant epitope compared to the wild-type epitope (wild-type mean 18.01 ± 10.45 standard deviation [SD] and variant mean 44.67 ± 14.42 SD, p = 0.002). Furthermore, activation of primary KIR2DL3+ NK cells from healthy donors in response to HLA-C*03:04+ target cells presenting the variant epitope was significantly reduced in comparison to cells presenting the wild-type sequence (wild-type mean 0.78 ± 0.07 standard error of the mean [SEM] and variant mean 0.63 ± 0.07 SEM, p = 0.012). Structural modeling and surface plasmon resonance of KIR/peptide/HLA interactions in the context of the different viral sequence variants studied supported these results. Future studies will be needed to assess processing and antigen presentation of the investigated HIV-1 epitope in natural infection, and the consequences for viral control. These data provide novel insights into how viruses can evade NK cell immunity through the selection of mutations in HLA-presented epitopes that enhance binding to inhibitory NK cell receptors. Better understanding of the mechanisms by which HIV-1 evades NK-cell-mediated immune pressure and the functional validation of a structural modeling approach will facilitate the development of novel targeted immune interventions to harness the antiviral activities of NK cells

Original language	English
Pages (from-to)	e1001900; discussion e1001900
Journal	PLoS medicine
Volume	12
Issue number	11
DOIs	https://doi.org/10.1371/journal.pmed.1001900
Publication status	Published - 2015

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https://doi.org/10.1371/journal.pmed.1001900

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Hölzemer, A., Thobakgale, C. F., Jimenez Cruz, C. A., Garcia-Beltran, W. F., Carlson, J. M., van Teijlingen, N. H., Mann, J. K., Jaggernath, M., Kang, S.-G., Körner, C., Chung, A. W., Schafer, J. L., Evans, D. T., Alter, G., Walker, B. D., Goulder, P. J., Carrington, M., Hartmann, P., Pertel, T., ... Altfeld, M. (2015). Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa. PLoS medicine, 12(11), e1001900; discussion e1001900. https://doi.org/10.1371/journal.pmed.1001900

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title = "Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa",

abstract = "Viruses can evade immune surveillance, but the underlying mechanisms are insufficiently understood. Here, we sought to understand the mechanisms by which natural killer (NK) cells recognize HIV-1-infected cells and how this virus can evade NK-cell-mediated immune pressure. Two sequence mutations in p24 Gag associated with the presence of specific KIR/HLA combined genotypes were identified in HIV-1 clade C viruses from a large cohort of infected, untreated individuals in South Africa (n = 392), suggesting viral escape from KIR+ NK cells through sequence variations within HLA class I-presented epitopes. One sequence polymorphism at position 303 of p24 Gag (TGag303V), selected for in infected individuals with both KIR2DL3 and HLA-C*03:04, enabled significantly better binding of the inhibitory KIR2DL3 receptor to HLA-C*03:04-expressing cells presenting this variant epitope compared to the wild-type epitope (wild-type mean 18.01 ± 10.45 standard deviation [SD] and variant mean 44.67 ± 14.42 SD, p = 0.002). Furthermore, activation of primary KIR2DL3+ NK cells from healthy donors in response to HLA-C*03:04+ target cells presenting the variant epitope was significantly reduced in comparison to cells presenting the wild-type sequence (wild-type mean 0.78 ± 0.07 standard error of the mean [SEM] and variant mean 0.63 ± 0.07 SEM, p = 0.012). Structural modeling and surface plasmon resonance of KIR/peptide/HLA interactions in the context of the different viral sequence variants studied supported these results. Future studies will be needed to assess processing and antigen presentation of the investigated HIV-1 epitope in natural infection, and the consequences for viral control. These data provide novel insights into how viruses can evade NK cell immunity through the selection of mutations in HLA-presented epitopes that enhance binding to inhibitory NK cell receptors. Better understanding of the mechanisms by which HIV-1 evades NK-cell-mediated immune pressure and the functional validation of a structural modeling approach will facilitate the development of novel targeted immune interventions to harness the antiviral activities of NK cells",

author = "Angelique H{\"o}lzemer and Thobakgale, {Christina F.} and {Jimenez Cruz}, {Camilo A.} and Garcia-Beltran, {Wilfredo F.} and Carlson, {Jonathan M.} and {van Teijlingen}, {Nienke H.} and Mann, {Jaclyn K.} and Manjeetha Jaggernath and Seung-Gu Kang and Christian K{\"o}rner and Chung, {Amy W.} and Schafer, {Jamie L.} and Evans, {David T.} and Galit Alter and Walker, {Bruce D.} and Goulder, {Philip J.} and Mary Carrington and Pia Hartmann and Thomas Pertel and Ruhong Zhou and Thumbi Ndung'u and Marcus Altfeld",

year = "2015",

doi = "https://doi.org/10.1371/journal.pmed.1001900",

language = "English",

volume = "12",

pages = "e1001900; discussion e1001900",

journal = "PLoS medicine",

issn = "1549-1277",

publisher = "Nature Publishing Group",

number = "11",

}

Hölzemer, A, Thobakgale, CF, Jimenez Cruz, CA, Garcia-Beltran, WF, Carlson, JM, van Teijlingen, NH, Mann, JK, Jaggernath, M, Kang, S-G, Körner, C, Chung, AW, Schafer, JL, Evans, DT, Alter, G, Walker, BD, Goulder, PJ, Carrington, M, Hartmann, P, Pertel, T, Zhou, R, Ndung'u, T & Altfeld, M 2015, 'Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa', PLoS medicine, vol. 12, no. 11, pp. e1001900; discussion e1001900. https://doi.org/10.1371/journal.pmed.1001900

Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa. / Hölzemer, Angelique; Thobakgale, Christina F.; Jimenez Cruz, Camilo A. et al.
In: PLoS medicine, Vol. 12, No. 11, 2015, p. e1001900; discussion e1001900.

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

TY - JOUR

T1 - Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa

AU - Hölzemer, Angelique

AU - Thobakgale, Christina F.

AU - Jimenez Cruz, Camilo A.

AU - Garcia-Beltran, Wilfredo F.

AU - Carlson, Jonathan M.

AU - van Teijlingen, Nienke H.

AU - Mann, Jaclyn K.

AU - Jaggernath, Manjeetha

AU - Kang, Seung-Gu

AU - Körner, Christian

AU - Chung, Amy W.

AU - Schafer, Jamie L.

AU - Evans, David T.

AU - Alter, Galit

AU - Walker, Bruce D.

AU - Goulder, Philip J.

AU - Carrington, Mary

AU - Hartmann, Pia

AU - Pertel, Thomas

AU - Zhou, Ruhong

AU - Ndung'u, Thumbi

AU - Altfeld, Marcus

PY - 2015

Y1 - 2015

N2 - Viruses can evade immune surveillance, but the underlying mechanisms are insufficiently understood. Here, we sought to understand the mechanisms by which natural killer (NK) cells recognize HIV-1-infected cells and how this virus can evade NK-cell-mediated immune pressure. Two sequence mutations in p24 Gag associated with the presence of specific KIR/HLA combined genotypes were identified in HIV-1 clade C viruses from a large cohort of infected, untreated individuals in South Africa (n = 392), suggesting viral escape from KIR+ NK cells through sequence variations within HLA class I-presented epitopes. One sequence polymorphism at position 303 of p24 Gag (TGag303V), selected for in infected individuals with both KIR2DL3 and HLA-C*03:04, enabled significantly better binding of the inhibitory KIR2DL3 receptor to HLA-C*03:04-expressing cells presenting this variant epitope compared to the wild-type epitope (wild-type mean 18.01 ± 10.45 standard deviation [SD] and variant mean 44.67 ± 14.42 SD, p = 0.002). Furthermore, activation of primary KIR2DL3+ NK cells from healthy donors in response to HLA-C*03:04+ target cells presenting the variant epitope was significantly reduced in comparison to cells presenting the wild-type sequence (wild-type mean 0.78 ± 0.07 standard error of the mean [SEM] and variant mean 0.63 ± 0.07 SEM, p = 0.012). Structural modeling and surface plasmon resonance of KIR/peptide/HLA interactions in the context of the different viral sequence variants studied supported these results. Future studies will be needed to assess processing and antigen presentation of the investigated HIV-1 epitope in natural infection, and the consequences for viral control. These data provide novel insights into how viruses can evade NK cell immunity through the selection of mutations in HLA-presented epitopes that enhance binding to inhibitory NK cell receptors. Better understanding of the mechanisms by which HIV-1 evades NK-cell-mediated immune pressure and the functional validation of a structural modeling approach will facilitate the development of novel targeted immune interventions to harness the antiviral activities of NK cells

AB - Viruses can evade immune surveillance, but the underlying mechanisms are insufficiently understood. Here, we sought to understand the mechanisms by which natural killer (NK) cells recognize HIV-1-infected cells and how this virus can evade NK-cell-mediated immune pressure. Two sequence mutations in p24 Gag associated with the presence of specific KIR/HLA combined genotypes were identified in HIV-1 clade C viruses from a large cohort of infected, untreated individuals in South Africa (n = 392), suggesting viral escape from KIR+ NK cells through sequence variations within HLA class I-presented epitopes. One sequence polymorphism at position 303 of p24 Gag (TGag303V), selected for in infected individuals with both KIR2DL3 and HLA-C*03:04, enabled significantly better binding of the inhibitory KIR2DL3 receptor to HLA-C*03:04-expressing cells presenting this variant epitope compared to the wild-type epitope (wild-type mean 18.01 ± 10.45 standard deviation [SD] and variant mean 44.67 ± 14.42 SD, p = 0.002). Furthermore, activation of primary KIR2DL3+ NK cells from healthy donors in response to HLA-C*03:04+ target cells presenting the variant epitope was significantly reduced in comparison to cells presenting the wild-type sequence (wild-type mean 0.78 ± 0.07 standard error of the mean [SEM] and variant mean 0.63 ± 0.07 SEM, p = 0.012). Structural modeling and surface plasmon resonance of KIR/peptide/HLA interactions in the context of the different viral sequence variants studied supported these results. Future studies will be needed to assess processing and antigen presentation of the investigated HIV-1 epitope in natural infection, and the consequences for viral control. These data provide novel insights into how viruses can evade NK cell immunity through the selection of mutations in HLA-presented epitopes that enhance binding to inhibitory NK cell receptors. Better understanding of the mechanisms by which HIV-1 evades NK-cell-mediated immune pressure and the functional validation of a structural modeling approach will facilitate the development of novel targeted immune interventions to harness the antiviral activities of NK cells

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JO - PLoS medicine

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Hölzemer A, Thobakgale CF, Jimenez Cruz CA, Garcia-Beltran WF, Carlson JM, van Teijlingen NH et al. Selection of an HLA-C*03:04-Restricted HIV-1 p24 Gag Sequence Variant Is Associated with Viral Escape from KIR2DL3+ Natural Killer Cells: Data from an Observational Cohort in South Africa. PLoS medicine. 2015;12(11):e1001900; discussion e1001900. doi: https://doi.org/10.1371/journal.pmed.1001900