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Identification of rat yolk sac target protein of teratogenic antibodies, gp280, as intrinsic factor-cobalamin receptor.

机译:鉴定致畸性抗体大鼠卵黄囊靶蛋白gp280作为内在因子钴胺素受体。

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摘要

Previous studies in the rat have shown that antibodies to gp280, a protein > 200 kD and closely associated with the early endocytic system can induce fetal malformations. Although gp280 is thought to act as a receptor, its ligand(s) is not known. In the current study, we report that purified gp280 from rat kidney, like the intrinsic factor-Cobalamin receptor (IFCR), binds to the intrinsic factor-cobalamin (IFCbl) complex with an association constant of 0.3 x 10(9) M-1 and mediates its internalization. Furthermore, antibodies raised to purified gp280 and IFCR inhibited the binding of IF-[57Co]Cbl complex to intestinal, renal, and yolk sac apical membranes and revealed a single identically sized protein on immunoblotting of the renal membranes. Both antibodies precipitated a single radiolabeled protein > 200 kD from cellular extract from [35S]methionine-labeled yolk sac epithelial cells, and antibody to gp280 inhibited the uptake and internalization of 125IF-Cbl. Immunoelectron microscopy using the two antibodies revealed that in the kidney, both proteins were colocalized. These observations suggest that IF-Cbl complex is a ligand for gp280 and that gp280 and IFCR are identical proteins.
机译:在大鼠中的先前研究表明,针对gp280的抗体(一种蛋白> 200 kD,与早期的内吞系统密切相关)可以诱导胎儿畸形。尽管认为gp280充当受体,但其配体是未知的。在当前的研究中,我们报告从大鼠肾脏中纯化的gp280,如内在因子-钴胺素受体(IFCR),以0.3 x 10(9)M-1的缔合常数与内在因子-钴胺素(IFCbl)复合物结合并调解其内部化此外,针对纯化的gp280和IFCR产生的抗体抑制IF- [57Co] Cbl复合物与肠,肾和卵黄囊膜的结合,并且在肾膜的免疫印迹中显示出一个大小相同的蛋白质。两种抗体均从[35S]蛋氨酸标记的卵黄囊上皮细胞的细胞提取物中沉淀出一个放射性标记的蛋白质,其> 200 kD,而gp280的抗体抑制了125IF-Cbl的摄取和内在化。使用这两种抗体的免疫电子显微镜检查显示,在肾脏中,这两种蛋白都共定位。这些观察结果表明IF-Cbl复合物是gp280的配体,并且gp280和IFCR是相同的蛋白质。

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