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B cells, antibody-secreting cells, and virus-specific antibodies respond to herpes simplex virus 2 reactivation in skin

机译:B细胞,抗体分泌细胞和病毒特异性抗体对皮肤中的重新激活患有疱疹病毒2重新激活

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Tissue-based T cells are important effectors in the prevention and control of mucosal viral infections; less is known about tissue-based B cells. We demonstrate that B cells and antibody-secreting cells (ASCs) are present in inflammatory infiltrates in skin biopsy specimens from study participants during symptomatic herpes simplex virus 2 (HSV-2) reactivation and early healing. Both CD20~(+) B cells, most of which are antigen inexperienced based on their coexpression of IgD, and ASCs — characterized by dense IgG RNA expression in combination with CD138, IRF4, and Blimp-1 RNA — were found to colocalize with T cells. ASCs clustered with CD4~(+) T cells, suggesting the potential for crosstalk. HSV-2–specific antibodies to virus surface antigens were also present in tissue and increased in concentration during HSV-2 reactivation and healing, unlike in serum, where concentrations remained static over time. B cells, ASCs, and HSV-specific antibody were rarely detected in biopsies of unaffected skin. Evaluation of samples from serial biopsies demonstrated that B cells and ASCs followed a more migratory than resident pattern of infiltration in HSV-affected genital skin, in contrast to T cells. Together, these observations suggest the presence of distinct phenotypes of B cells in HSV-affected tissue; dissecting their role in reactivation may reveal new therapeutic avenues to control these infections.
机译:基于组织的T细胞在预防和控制粘膜病毒感染方面是重要的效果;较少是关于基于组织的B细胞。我们证明B细胞和抗体分泌细胞(ASCS)存在于症状病毒2(HSV-2)重新激活和早期愈合期间的研究参与者的皮肤活检标本中的炎性浸润中。 CD20〜(+)B细胞,其中大部分是基于它们的IGD的共表达而缺乏经验的抗原,并且ASCS的特征在于致密IgG RNA表达与CD138,IRF4和Blimp-1 RNA组合 - 与T结合细胞。 ascs与cd4〜(+)t细胞聚集,表明串扰的可能性。对于病毒表面抗原的HSV-2特异性抗体也存在于组织中并在HSV-2重新激活和愈合期间浓度增加,与血清不同,其中浓度随时间仍然保持静止。在未受影响的皮肤的活组织检查中很少检测到B细胞,ASC和HSV特异性抗体。与T细胞相比,来自连续活组织检查的样品的评估表明B细胞和ASC在HSV对生殖器皮肤中的血液浸润模式比常驻模式。这些观察结果表明HSV受影响的组织中B细胞的不同表型;将其在重新激活中解剖的作用可能揭示用于控制这些感染的新治疗途径。

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