首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Antibodies to the 280-kd coated pit protein target of teratogenic antibodies produce alterations in the traffic of internalized proteins.
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Antibodies to the 280-kd coated pit protein target of teratogenic antibodies produce alterations in the traffic of internalized proteins.

机译:致畸抗体的靶标是280 kd包被的基坑蛋白的抗体会改变内在蛋白的运输量。

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摘要

Previous studies have identified two high-molecular weight (280 and 330 kd) glycoproteins expressed by coated pits of the proximal renal tubule and yolk sac and have further established that, in vivo, antibodies to gp280 but not to gp330 induce fetal malformations. In the present study, we report the effect of these antibodies on the endocytic process by yolk sac visceral epithelial cells of rat embryos explanted at day 10 of gestation. Antibodies to gp280 markedly altered development of the yolk sac and embryo, induced malformations, inhibited by 40% the uptake of [14C] sucrose and perturbed the intracellular traffic of internalized proteins. Under control conditions, rat immunoglobulin G present in the culture medium was immunolocalized in lysosomes of epithelial cells, whereas in the presence of antibody, it was detected in small vesicles scattered through the apical cytoplasm. Alterations of the endocytic pathway were confirmed by experiments analyzing the uptake of peroxidase added to the medium for 2 to 60 minutes. The initial compartments of endocytosis visualized by peroxidase were increased in size and abnormal in shape and the transfer of the internalized peroxidase to the lysosomal compartment was delayed. In contrast, antibodies to gp330 had a minimal effect on embryonic development and did not induce fetal malformations. Endocytosis was only modestly altered; uptake of [14C] sucrose was decreased by 25%, and only minor modifications of the intracellular transit of peroxidase could be detected. We suggest that the key role of anti-gp280 antibodies is via trapping of the target antigen in the early endocytic compartment thus preventing its normal function in lysosomal transfer.
机译:先前的研究已经确定了由近端肾小管和卵黄囊的包膜小凹表达的两种高分子量(280和330 kd)糖蛋白,并进一步确定了在体内,针对gp280的抗体而非针对gp330的抗体诱导胎儿畸形。在本研究中,我们报告了这些抗体对妊娠第10天移植的大鼠胚胎的卵黄囊内脏上皮细胞的内吞过程的影响。 gp280抗体显着改变卵黄囊和胚胎的发育,引起畸形,被[14C]蔗糖摄取抑制40%,并扰乱了内在化蛋白质的细胞内运输。在对照条件下,存在于培养基中的大鼠免疫球蛋白G被免疫定位在上皮细胞的溶酶体中,而在存在抗体的情况下,在散布于顶端细胞质的小囊泡中被检测到。通过分析添加到培养基中2至60分钟的过氧化物酶摄取的实验,证实了内吞途径的改变。通过过氧化物酶可见的内吞作用的初始区室的大小增加并且形状异常,并且内化的过氧化物酶向溶酶体区室的转移被延迟。相反,针对gp330的抗体对胚胎发育的影响很小,并且不会诱导胎儿畸形。内吞作用仅适度改变; [14C]蔗糖的摄取降低了25%,并且只能检测到过氧化物酶在细胞内转运的微小修饰。我们建议抗gp280抗体的关键作用是通过将靶抗原捕获在早期内吞区室中,从而阻止其在溶酶体转移中的正常功能。

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