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内皮细胞质膜囊泡相关蛋白调节脾脏未成熟B细胞和B-1 B细胞的稳态。

Endothelial Plasmalemma Vesicle-Associated Protein Regulates the Homeostasis of Splenic Immature B Cells and B-1 B Cells.

作者信息

Elgueta Raul, Tse Dan, Deharvengt Sophie J, Luciano Marcus R, Carriere Catherine, Noelle Randolph J, Stan Radu V

机构信息

Department of Microbiology and Immunology, Geisel School of Medicine at Dartmouth, Lebanon, NH 03756.

Department of Immune Regulation and Intervention, Medical Research Council Centre for Transplantation, King's College London, Guy's Hospital, London, SE1 9RT, United Kingdom.

出版信息

J Immunol. 2016 Nov 15;197(10):3970-3981. doi: 10.4049/jimmunol.1501859. Epub 2016 Oct 14.

Abstract

Plasmalemma vesicle-associated protein (Plvap) is an endothelial protein with roles in endothelial diaphragm formation and maintenance of basal vascular permeability. At the same time, Plvap has roles in immunity by facilitating leukocyte diapedesis at inflammatory sites and controlling peripheral lymph node morphogenesis and the entry of soluble Ags into lymph node conduits. Based on its postulated role in diapedesis, we have investigated the role of Plvap in hematopoiesis and show that deletion of Plvap results in a dramatic decrease of IgMIgD B cells in both the spleen and the peritoneal cavity. Tissue-specific deletion of Plvap demonstrates that the defect is B cell extrinsic, because B cell and pan-hematopoietic Plvap deletion has no effect on IgMIgD B cell numbers. Endothelial-specific deletion of Plvap in the embryo or at adult stage recapitulates the full Plvap knockout phenotype, whereas endothelial-specific reconstitution of Plvap under the Chd5 promoter rescues the IgMIgD B cell phenotype. Taken together, these results show that Plvap expression in endothelial cells is important in the maintenance of IgM B cells in the spleen and peritoneal cavity.

摘要

质膜囊泡相关蛋白(Plvap)是一种内皮蛋白,在内皮隔膜形成和维持基础血管通透性方面发挥作用。同时,Plvap通过促进炎症部位的白细胞渗出以及控制外周淋巴结形态发生和可溶性抗原进入淋巴结管道,在免疫中发挥作用。基于其在渗出过程中的假定作用,我们研究了Plvap在造血中的作用,并表明Plvap的缺失导致脾脏和腹腔中IgM IgD B细胞显著减少。Plvap的组织特异性缺失表明该缺陷是B细胞外在的,因为B细胞和全造血Plvap缺失对IgM IgD B细胞数量没有影响。在胚胎期或成年期内皮细胞特异性缺失Plvap重现了完全Plvap基因敲除的表型,而在Chd5启动子下内皮细胞特异性重建Plvap可挽救IgM IgD B细胞表型。综上所述,这些结果表明内皮细胞中Plvap的表达对于维持脾脏和腹腔中的IgM B细胞很重要。

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