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首页> 外文期刊>Nature immunology >Transcriptional programs of lymphoid tissue capillary and high endothelium reveal control mechanisms for lymphocyte homing.
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Transcriptional programs of lymphoid tissue capillary and high endothelium reveal control mechanisms for lymphocyte homing.

机译:淋巴组织毛细血管和高内皮的转录程序揭示了淋巴细胞归巢的控制机制。

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摘要

Lymphocytes are recruited from blood by high-endothelial venules (HEVs). We performed transcriptomic analyses and identified molecular signatures that distinguish HEVs from capillary endothelium and that define tissue-specific HEV specialization. Capillaries expressed gene programs for vascular development. HEV-expressed genes showed enrichment for genes encoding molecules involved in immunological defense and lymphocyte migration. We identify capillary and HEV markers and candidate mechanisms for regulated recruitment of lymphocytes, including a lymph node HEV-selective transmembrane mucin; transcriptional control of functionally specialized carbohydrate ligands for lymphocyte L-selectin; HEV expression of molecules for transendothelial migration; and metabolic programs for lipid mediators of lymphocyte motility and chemotaxis. We also elucidate a carbohydrate-recognition pathway that targets B cells to intestinal lymphoid tissues, defining CD22 as a lectin-homing receptor for mucosal HEVs.
机译:淋巴细胞是通过高内皮小静脉(HEV)从血液中募集的。我们进行了转录组学分析,并确定了分子特征,这些特征将HEV与毛细管内皮细胞区分开来,并定义了组织特异性HEV专业化。毛细管表达了血管发育的基因程序。 HEV表达的基因对编码参与免疫防御和淋巴细胞迁移的分子的基因富集。我们确定毛细血管和混合动力车标志物和候选调节淋巴细胞募集的机制,包括淋巴结HEV选择性跨膜粘蛋白;淋巴细胞L-选择素功能上专门的碳水化合物配体的转录控制; HEV表达分子用于跨内皮迁移;淋巴细胞运动和趋化性脂质介体的代谢程序和代谢程序。我们还阐明了针对B细胞至肠淋巴组织的碳水化合物识别途径,将CD22定义为粘膜HEV的凝集素归巢受体。

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