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CD138 mediates selection of mature plasma cells by regulating their survival

机译:CD138通过调节其存活来介导成熟血浆细胞的选择

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摘要

Antibody secreting cells (ASCs) are critical effector cells and long-lived sentinels for immune memory. ASCs are highly dependent on exogenous soluble factors such as interleukin-6 (IL-6) and APRIL, to prevent their cell death. We have found that the canonical surface marker of ASCs, CD138 (syndecan-1), which is upregulated during ASC maturation, is required in a cell-intrinsic manner to mount an effective long-term humoral immune response following immunization. Surface expression of CD138 increased heparan sulfate levels on ASCs, which are known to bind pro-survival cytokines, leading to increased survival in a cell-intrinsic manner in vivo. In IL-6 and APRIL-deficient hosts, ASCs underwent extensive apoptosis independently of CD138 expression. We propose a model in which CD138 expression on fully mature ASCs provides a selective survival advantage over less mature, newly minted ASCs, by enhancing pro-survival cytokine signaling.
机译:分泌细胞(ASCS)是关键效应细胞和用于免疫记忆的长期哨碱。 ASCS高度依赖于外介素-6(IL-6)和4月等的外源性可溶性因子,以防止其细胞死亡。 我们发现ASC的规范表面标记,CD138(Syndecan-1)在ASC成熟期间上调,以细胞内在的方式需要在免疫后载有有效的长期体液免疫应答。 CD138的表面表达增加了ASC的硫酸乙酰肝素水平,该硫酸盐水平已知已知用于结合促型细胞因子,导致在体内以细胞内在方式增加生存。 在IL-6和4月缺乏宿主中,ASCS接受了广泛的细胞凋亡,独立于CD138表达。 我们提出了一种模型,其中CD138在完全成熟的ASC上表达通过增强Pro-Survival细胞因子信号传导在更小的成熟,新的铸型ASC中提供了选择性存活优势。

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