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骨形态发生蛋白4(BMP4)前结构域中上游切割位点的突变导致组织特异性活性丧失。

Mutation of an upstream cleavage site in the BMP4 prodomain leads to tissue-specific loss of activity.

作者信息

Goldman Devorah C, Hackenmiller Renee, Nakayama Takuya, Sopory Shailaja, Wong Crispin, Kulessa Holger, Christian Jan L

机构信息

Department of Cell and Developmental Biology, Oregon Health and Sciences University, School of Medicine, 3181 SW Sam Jackson Park Road, Portland, OR 97239-3098, USA.

出版信息

Development. 2006 May;133(10):1933-42. doi: 10.1242/dev.02368. Epub 2006 Apr 19.

Abstract

ProBMP4 is initially cleaved at a site adjacent to the mature ligand (the S1 site) allowing for subsequent cleavage at an upstream (S2) site. Mature BMP4 synthesized from a precursor in which the S2 site cannot be cleaved remains in a complex with the prodomain that is targeted for lysosomal degradation, and is thus less active when overexpressed in Xenopus. Here we report that mice carrying a point mutation that prevents S2 processing show severe loss of BMP4 activity in some tissues, such as testes and germ cells, whereas other tissues that are sensitive to Bmp4 dosage, such as the limb, dorsal vertebrae and kidney, develop normally. In a haploinsufficient background, inability to cleave the S2 site leads to embryonic and postnatal lethality due to defects in multiple organ systems including the allantois, placental vasculature, ventral body wall, eye and heart. These data demonstrate that cleavage of the S2 site is essential for normal development and, more importantly, suggest that this site might be selectively cleaved in a tissue-specific fashion. In addition, these studies provide the first genetic evidence that BMP4 is required for dorsal vertebral fusion and closure of the ventral body wall.

摘要

前BMP4最初在与成熟配体相邻的位点(S1位点)被切割,随后可在上游(S2)位点进行切割。由无法切割S2位点的前体合成的成熟BMP4与靶向溶酶体降解的前结构域形成复合物,因此在非洲爪蟾中过表达时活性较低。我们在此报告,携带阻止S2加工的点突变的小鼠在某些组织,如睾丸和生殖细胞中显示出严重的BMP4活性丧失,而其他对Bmp4剂量敏感的组织,如肢体、背椎和肾脏,则发育正常。在单倍剂量不足的背景下,无法切割S2位点会导致胚胎和出生后死亡,原因是包括尿囊、胎盘血管、腹侧体壁、眼睛和心脏在内的多个器官系统存在缺陷。这些数据表明,S2位点的切割对于正常发育至关重要,更重要的是,表明该位点可能以组织特异性方式被选择性切割。此外,这些研究提供了首个遗传学证据,证明BMP4是背椎融合和腹侧体壁闭合所必需的。

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