Immunoglobulin VH gene diversity and somatic hypermutation during SIV infection of rhesus macaques

被引:0
|
作者
Kejun Guo
Kalani Halemano
Kimberly Schmitt
Miki Katuwal
Yaqiong Wang
Michael S. Harper
Karl J. Heilman
Takeo Kuwata
Edward B. Stephens
Mario L. Santiago
机构
[1] University of Colorado Denver,Departments of Medicine, Immunology and Microbiology
[2] University of Kansas Medical Center,Department of Microbiology, Molecular Genetics and Immunology
[3] Kumamoto University,Center for AIDS Research
[4] Scripps Research Institute,undefined
来源
Immunogenetics | 2015年 / 67卷
关键词
Antibody repertoire; Deaminase; Somatic hypermutation; Rhesus macaque; Simian immunodeficiency virus; APOBEC3G;
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中图分类号
学科分类号
摘要
B cell functional defects are associated with delayed neutralizing antibody development in pathogenic lentivirus infections. However, the timeframe for alterations in the antibody repertoire and somatic hypermutation (SHM) remains unclear. Here, we utilized the SIV/rhesus macaque (RM) model to investigate the dynamics of immunoglobulin VH gene diversity and SHM following infection. Three RMs were infected with SIVmac239, and VH1, VH3, and VH4 genes were amplified from peripheral blood at 0, 2, 6, 24, and 36 weeks postinfection for next-generation sequencing. Analysis of over 3.8 million sequences against currently available RM germline VH genes revealed a highly biased VH gene repertoire in outbred RMs. SIV infection did not significantly perturb the predominant IgG1 response, but overall immunoglobulin SHM declined during the course of SIV infection. Moreover, SHM at the AID deamination hotspot, WRC, rapidly decreased and was suppressed throughout SIV infection. In contrast, a transient increase in mutations at the APOBEC3G deamination hotspot, CCC, coincided with a spike in APOBEC3G expression during acute SIV infection. The results outline a timetable for altered VH gene repertoire and IgG SHM in the SIV/RM model and suggest a burst of APOBEC3G-mediated antibody SHM during acute SIV infection.
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页码:355 / 370
页数:15
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