卵巢切除术通过肠道 TNF+T 细胞和 Th17 细胞的微生物依赖性转运诱导骨丢失。
Ovariectomy induces bone loss via microbial-dependent trafficking of intestinal TNF+ T cells and Th17 cells.
机构信息
Division of Endocrinology, Metabolism and Lipids, Department of Medicine and.
Emory Microbiome Research Center, Emory University, Atlanta, Georgia, USA.
出版信息
J Clin Invest. 2021 Feb 15;131(4). doi: 10.1172/JCI143137.
Abstract
Estrogen deficiency causes a gut microbiome-dependent expansion of BM Th17 cells and TNF-α-producing T cells. The resulting increased BM levels of IL-17a (IL-17) and TNF stimulate RANKL expression and activity, causing bone loss. However, the origin of BM Th17 cells and TNF+ T cells is unknown. Here, we show that ovariectomy (ovx) expanded intestinal Th17 cells and TNF+ T cells, increased their S1P receptor 1-mediated (S1PR1-mediated) egress from the intestine, and enhanced their subsequent influx into the BM through CXCR3- and CCL20-mediated mechanisms. Demonstrating the functional relevance of T cell trafficking, blockade of Th17 cell and TNF+ T cell egress from the gut or their influx into the BM prevented ovx-induced bone loss. Therefore, intestinal T cells are a proximal target of sex steroid deficiency relevant for bone loss. Blockade of intestinal T cell migration may represent a therapeutic strategy for the treatment of postmenopausal bone loss.
摘要
雌激素缺乏导致肠道微生物组依赖性 BM Th17 细胞和 TNF-α产生 T 细胞的扩增。由此导致的 BM 中 IL-17a(IL-17)和 TNF 的增加刺激 RANKL 表达和活性,导致骨丢失。然而,BM Th17 细胞和 TNF+T 细胞的来源尚不清楚。在这里,我们表明卵巢切除术(ovx)扩增了肠道 Th17 细胞和 TNF+T 细胞,增加了它们通过 S1P 受体 1 介导(S1PR1 介导)从肠道排出的能力,并通过 CXCR3 和 CCL20 介导的机制增强了它们随后进入 BM 的流入。证明 T 细胞迁移的功能相关性,阻断 Th17 细胞和 TNF+T 细胞从肠道排出或进入 BM 可预防 ovx 诱导的骨丢失。因此,肠道 T 细胞是与骨丢失相关的性激素缺乏的近端靶标。阻断肠道 T 细胞迁移可能代表治疗绝经后骨丢失的一种治疗策略。
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