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你需要一艘更大的(玻璃底)船。

You're going to need a bigger (glass bottom) boat.

机构信息

Department of Genetics, Cell Biology and Development, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Sci Signal. 2012 Apr 3;5(218):pe14. doi: 10.1126/scisignal.2002998.

DOI:10.1126/scisignal.2002998
PMID:22472647
Abstract

Signaling molecules of the transforming growth factor (TGF)-β family are generated from proprotein precursors containing prodomain sequences that are typically removed to allow signaling by the mature ligands. A form of a TGF-β family ligand that remains covalently attached to its prodomain but retains signaling activity has been identified. Glass bottom boat (Gbb), a Drosophila homolog of the bone morphogenetic protein 5/6/7/8 subfamily, is active as a carboxyl-terminal fragment of the proprotein (Gbb15) that is generated by a conventional processing event common to TGF-β ligands. Unexpectedly, a larger form (Gbb38) produced by processing at a newly identified furin site in the prodomain is also secreted and active. Contrary to the present paradigm in which TGF-β ligands require dissociation of the entire prodomain for activity, Gbb38 is active in cell culture and in vivo without additional processing at conventional sites. The large form can restore the viability of gbb mutant animals but has distinct signaling properties compared with the conventional form. Production of multiple functional ligands from one proprotein is a potential mechanism to fine-tune TGF-β signaling outputs. Mutations in TGF-β family members have been linked to human diseases, several of which affect potential furin cleavage sites in prodomains. However, given the diversity of potential furin processing sites and prodomain functions, direct experimentation will be required to determine whether production of active jumbo ligands is a general feature of TGF-β superfamily members.

摘要

转化生长因子 (TGF)-β 家族的信号分子由含有前导序列的前蛋白原产生,这些前导序列通常被去除,以使成熟配体能够进行信号传递。已经鉴定出一种 TGF-β 家族配体形式,其仍然共价连接到其前导序列,但保留信号活性。果蝇骨形态发生蛋白 5/6/7/8 亚家族的同源物玻璃底船 (Gbb) 作为前蛋白原 (Gbb15) 的羧基末端片段发挥活性,该片段通过 TGF-β 配体常见的常规加工事件产生。出乎意料的是,通过在前导区中新鉴定的弗林位点进行加工产生的更大形式 (Gbb38) 也被分泌并具有活性。与 TGF-β 配体需要整个前导区解离才能发挥活性的现有范例相反,Gbb38 在细胞培养和体内没有在常规位点进行额外加工的情况下具有活性。这种大形式可以恢复 gbb 突变体动物的活力,但与常规形式相比具有不同的信号特性。从一个前蛋白原产生多种功能配体是微调 TGF-β 信号输出的一种潜在机制。TGF-β 家族成员的突变与人类疾病有关,其中一些疾病影响前导区中的潜在弗林切割位点。然而,鉴于潜在弗林加工位点和前导区功能的多样性,需要进行直接实验来确定是否产生活性巨型配体是 TGF-β 超家族成员的一般特征。

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