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一种具有独特信号特性的大型生物活性 BMP 配体是通过选择性前转化酶加工产生的。

A large bioactive BMP ligand with distinct signaling properties is produced by alternative proconvertase processing.

机构信息

Department of Molecular Biology, Cell Biology, and Biochemistry, Brown University, Providence, RI 02912, USA.

出版信息

Sci Signal. 2012 Apr 3;5(218):ra28. doi: 10.1126/scisignal.2002549.

Abstract

Dimers of conventional transforming growth factor-β (TGF-β) and bone morphogenetic protein (BMP) ligands are composed of two 100- to 140-amino acid peptides that are produced through the proteolytic processing of a proprotein precursor by proconvertases, such as furin. We report the identification of an evolutionarily conserved furin processing site in the amino terminus (NS) of the Glass bottom boat (Gbb; the Drosophila ortholog of vertebrate BMP5, 6, and 7) proprotein that generates a 328-amino acid, active BMP ligand distinct from the conventional 130-amino acid ligand. Gbb38, the large ligand form of Gbb, exhibited greater signaling activity and a longer range than the shorter form Gbb15. The abundance of Gbb15 and Gbb38 varied among different tissues, raising the possibility that differential processing could account for tissue-specific behaviors of BMPs. In human populations, mutations that abolished the NS cleavage site in BMP4, BMP15, or anti-Müllerian hormone were associated with cleft lip with or without cleft palate (BMP4), premature ovarian failure (BMP15), and persistent Müllerian duct syndrome (anti-Müllerian hormone), suggesting the importance of NS processing during development. The identification of this large BMP ligand form and the functional differences between large and small ligands exemplifies the potential for differential proprotein processing to substantially affect BMP and TGF-β signaling output in different tissue and cellular contexts.

摘要

传统转化生长因子-β (TGF-β) 和骨形态发生蛋白 (BMP) 配体的二聚体由两个 100-140 个氨基酸肽组成,这些肽是通过前蛋白原的蛋白水解加工产生的,如弗林蛋白酶。我们报告了在 Glass bottom boat (Gbb; 脊椎动物 BMP5、6 和 7 的果蝇同源物) 前蛋白的氨基末端 (NS) 中鉴定出一个进化上保守的弗林蛋白酶加工位点,该位点产生了一种 328 个氨基酸的活性 BMP 配体,与传统的 130 个氨基酸配体不同。Gbb38 是 Gbb 的大配体形式,其信号活性和作用范围大于较短的 Gbb15 形式。不同组织中 Gbb15 和 Gbb38 的丰度不同,这表明差异加工可能解释了 BMP 在组织中的特异性行为。在人类群体中,破坏 BMP4、BMP15 或抗苗勒管激素 NS 切割位点的突变与唇裂伴或不伴腭裂 (BMP4)、卵巢早衰 (BMP15) 和持续苗勒管综合征 (抗苗勒管激素) 有关,这表明 NS 加工在发育过程中的重要性。这种大 BMP 配体形式的鉴定以及大配体和小配体之间的功能差异,说明了差异前蛋白原加工在不同组织和细胞环境中对 BMP 和 TGF-β 信号输出产生重大影响的潜力。

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