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体内注射后单克隆抗体与肾小球内皮、裂孔膜及上皮的结合。通过免疫电子显微镜对抗原和结合的免疫球蛋白进行定位。

Binding of monoclonal antibodies to glomerular endothelium, slit membranes, and epithelium after in vivo injection. Localization of antigens and bound IgGs by immunoelectron microscopy.

作者信息

Dekan G, Miettinen A, Schnabel E, Farquhar M G

机构信息

Department of Cell Biology, Yale University School of Medicine, New Haven, Connecticut.

出版信息

Am J Pathol. 1990 Oct;137(4):913-27.

Abstract

The antigens recognized by seven monoclonal antibodies (MAbs) raised against rat glomerular proteins were localized, and the sites of binding of the MAbs after in vivo injection were determined by immunoelectron microscopy. The antigens were localized in situ by immunoperoxidase and immunogold labeling to different domains and microdomains of the glomerular endothelium and epithelium. 23A recognized an antigen expressed exclusively on the luminal (apical) domain of the endothelium. 5A (anti-podocalyxin) and 26C (anti-DPPIV) recognized antigens expressed on the apical domains of both the endothelium and podocytes. 13A, 14A, 20B (anti-gp330), and 27A recognized antigens restricted to podocytes in the glomerulus. The 13A antigen was present on their basal surface and the 27A and 14A antigens were expressed on both their apical and basal domains. The 14A antigen also was associated with the filtration slit membranes. All these MAbS bound to their antigens after injection in vivo. Those that recognize endothelial antigens were rapidly cleared from the circulation and rapidly disappeared from glomeruli, whereas those that recognize epithelial antigens persisted in the circulation and were detectable in glomeruli for hours or days. The sites of binding of the MAbs differed: 23A and 5A IgG (antipodocalyxin) bound exclusively to the luminal domain of the endothelium, whereas 26C IgG (anti-DPPIV) bound to both the luminal endothelial membrane and the apical and basal domains of podocytes. The MAbs that recognize podocyte antigens bound to different domains of the podocyte plasmalemma: 13A and 27A IgGs to the basal domain, 14A to the slit membranes, and 20B to coated pits on the entire plasma membrane. 27A IgG led to the formation of small subepithelial immune deposits that remained up to 10 days. It is concluded that 1) glomerular membrane proteins vary considerably in their distribution among plasmalemmal domains and microdomains of endothelial and epithelial cells; 2) virtually all structures in the glomerulus and all domains and micro-domains of the endothelium and podocyte are accessible to circulating antibodies; and 3) the fate of immune complexes formed by binding to glomerular components varies with the location of the antigen within the glomerulus, with those that bind to the basal domain and slit membranes of the podocyte persisting longer than the others.

摘要

对7种针对大鼠肾小球蛋白产生的单克隆抗体(MAb)所识别的抗原进行了定位,并通过免疫电子显微镜确定了体内注射后这些MAb的结合位点。通过免疫过氧化物酶和免疫金标记将抗原原位定位到肾小球内皮细胞和上皮细胞的不同结构域和微结构域。23A识别一种仅在内皮细胞腔(顶端)结构域表达的抗原。5A(抗足细胞裂孔素)和26C(抗二肽基肽酶IV)识别在内皮细胞和足细胞顶端结构域均表达的抗原。13A、14A、20B(抗gp330)和27A识别局限于肾小球足细胞的抗原。13A抗原存在于足细胞基底表面,27A和14A抗原在足细胞顶端和基底结构域均有表达。14A抗原也与滤过裂隙膜相关。所有这些MAb在体内注射后均与它们的抗原结合。那些识别内皮细胞抗原的MAb迅速从循环中清除,并很快从肾小球消失,而那些识别上皮细胞抗原的MAb则在循环中持续存在,并在肾小球中可检测数小时或数天。MAb的结合位点各不相同:23A和5A IgG(抗足细胞裂孔素)仅结合到内皮细胞的腔结构域,而26C IgG(抗二肽基肽酶IV)则结合到内皮细胞膜腔面以及足细胞的顶端和基底结构域。识别足细胞抗原的MAb结合到足细胞质膜的不同结构域:13A和27A IgG结合到基底结构域,14A结合到裂隙膜,20B结合到整个质膜上的被膜小窝。27A IgG导致小的上皮下免疫沉积物形成,这些沉积物可持续长达10天。结论是:1)肾小球膜蛋白在其在内皮细胞和上皮细胞质膜结构域和微结构域中的分布差异很大;2)肾小球内几乎所有结构以及内皮细胞和足细胞的所有结构域和微结构域都可被循环抗体识别;3)与肾小球成分结合形成的免疫复合物的命运因抗原在肾小球内的位置而异,与足细胞基底结构域和裂隙膜结合的复合物比其他复合物持续时间更长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/21a0/1877537/bccd02ec2e8c/amjpathol00106-0172-a.jpg

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