首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Early Antiretroviral Therapy Preserves Functional Follicular Helper T and HIV-Specific B Cells in the Gut Mucosa of HIV-1-Infected Individuals
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Early Antiretroviral Therapy Preserves Functional Follicular Helper T and HIV-Specific B Cells in the Gut Mucosa of HIV-1-Infected Individuals

机译:早期的抗逆转录病毒治疗在HIV-1感染的个体的肠粘膜中保留功能性滤泡辅助T和HIV特异性B细胞

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摘要

HIV-1 infection is associated with B cell dysregulation and dysfunction. In HIV-1-infected patients, we previously reported preservation of intestinal lymphoid structures and dendritic cell maturation pathways after early combination antiretroviral therapy (e-ART), started during the acute phase of the infection, compared with late combination antiretroviral therapy started during the chronic phase. In this study, we investigated whether the timing of combination antiretroviral therapy initiation was associated with the development of the HIV-1-specific humoral response in the gut. The results showed that e-ART was associated with higher frequencies of functional resting memory B cells in the gut. These frequencies correlated strongly with those of follicular Th cells in the gut. Importantly, frequencies of HIV-1 Env gp140-reactive B cells were higher in patients given e-ART, in whom gp140-reactive IgG production by mucosal B cells increased after stimulation. Moreover, IL-21 release by PBMCs stimulated with HIV-1 peptide pools was greater with e-ART than with late combination antiretroviral therapy. Thus, early treatment initiation helps to maintain HIV-1-reactive memory B cells in the gut as well as follicular Th cells, whose role is crucial in the development of potent affinity-matured and broadly neutralizing Abs.
机译:HIV-1感染与B细胞失调和功能障碍有关。在HIV-1感染的患者中,我们之前报道了在早期组合抗逆转录病毒治疗(E-ART)后的肠淋巴结结构和树突细胞成熟途径的保存,在感染的急性期开始,与后期组合抗逆转录病毒治疗开始慢性阶段。在这项研究中,我们研究了组合抗逆转录病毒治疗开始的时间是否与肠道中HIV-1特异性体液反应的发展有关。结果表明,电子技术有关肠道中功能静态存储器B细胞的较高频率。这些频率与肠道中的滤泡细胞强烈相关。重要的是,在给定患者的患者中,HIV-1 Env GP140-反应性B细胞的频率较高,在刺激后,通过粘膜B细胞产生GP140-反应性IgG产生。此外,通过与晚期组合抗逆转录病毒治疗的E-ART刺激的PBMC刺激的IL-21释放较大。因此,早期治疗开始有助于将肠道和滤泡细胞中的HIV-1-反应性记忆B细胞维持,其作用在发育有效的亲和成熟和广泛中和ABS的发展中至关重要。

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    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Ctr Hosp Reg Orleans La Source Serv Malad Infect &

    Trop F-45000 Orleans France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Univ Paris Est Creteil Vaccine Res Inst Fac Med F-94010 Creteil France;

    Grp Henri Mondor Albert Chenevier AP HP Dept Pathol F-94010 Creteil France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Pasteur Inst Dept Immunol Lab Humoral Response Pathogens F-75015 Paris France;

    Pasteur Inst Dept Immunol Lab Humoral Response Pathogens F-75015 Paris France;

    Grp Henri Mondor Albert Chenevier AP HP Serv Immunol Biol F-94010 Creteil France;

    Grp Henri Mondor Albert Chenevier AP HP Serv Immunol Biol F-94010 Creteil France;

    Ctr Hosp Reg Orleans La Source Serv Hepatogastroenterol F-45000 Orleans France;

    Ctr Hosp Reg Orleans La Source Serv Malad Infect &

    Trop F-45000 Orleans France;

    Grp Henri Mondor Albert Chenevier AP HP Serv Hepatogastroenterol F-94010 Creteil France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Univ Paris Est Creteil Vaccine Res Inst Fac Med F-94010 Creteil France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

    Univ Paris Est Creteil Fac Med INSERM Equipe 16 U955 F-94010 Creteil France;

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  • 正文语种 eng
  • 中图分类 免疫遗传学;
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