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The thioredoxin‐1 and glutathione/glutaredoxin‐1 systems redundantly fuel murine B‐cell development and responses

机译:硫氧还蛋白检测——1,谷胱甘肽/ glutaredoxin 1系统冗余燃料小鼠B细胞发展和响应

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Abstract Antioxidant systems maintain cellular redox homeostasis. The thioredoxin‐1 (Trx1) and the glutathione (GSH)/glutaredoxin‐1 (Grx1) systems are key players in preserving cytosolic redox balance. In fact, T lymphocytes critically rely on reducing equivalents from the Trx1 system for DNA biosynthesis during metabolic reprogramming upon activation. We here show that the Trx1 system is also indispensable for development and functionality of marginal zone (MZ) B?cells and B1 cells in mice. In contrast, development of conventional B?cells, follicular B‐cell homeostasis, germinal center reactions, and antibody responses are redundantly sustained by both antioxidant pathways. Proliferating B2 cells lacking Txnrd1 have increased glutathione (GSH) levels and upregulated cytosolic Grx1 , which is barely detectable in expanding thymocytes. These results suggest that the redox capacity driving proliferation is more robust and flexible in B?cells than in T?cells, which may have profound implications for the therapy of B and T‐cell neoplasms.
机译:摘要保持细胞抗氧化系统氧化还原内稳态。系统保存胞质中的关键球员氧化还原平衡。依靠从Trx1系统减少等价物在DNA生物合成代谢重新激活。Trx1系统也是必不可少的边缘地带的发展和功能(MZ) B ?发展传统B ?B细胞内稳态,应承担的生发中心反应,和抗体反应是多余地持续由抗氧化途径。细胞缺乏Txnrd1增加谷胱甘肽(谷胱甘肽)水平和调节胞质Grx1,难以觉察的是在扩大胸腺细胞。驾驶扩散更健壮和能力在B灵活吗?对B的治疗产生深远的影响和T细胞肿瘤。

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