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所有哺乳动物的 Hedgehog 蛋白都以保守的方式与细胞粘附分子相互作用,而细胞粘附分子又受到癌基因下调蛋白(CDO)和 CDO 兄弟蛋白(BOC)的调节。

All mammalian Hedgehog proteins interact with cell adhesion molecule, down-regulated by oncogenes (CDO) and brother of CDO (BOC) in a conserved manner.

机构信息

Department of Biophysics and Biophysical Chemistry, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

J Biol Chem. 2010 Aug 6;285(32):24584-90. doi: 10.1074/jbc.M110.131680. Epub 2010 Jun 1.

Abstract

Hedgehog (Hh) signaling proteins stimulate cell proliferation, differentiation, and tissue patterning at multiple points in animal development. A single Hh homolog is present in Drosophila, but three Hh homologs, Sonic Hh, Indian Hh, and Desert Hh, are present in mammals. Distribution, movement, and reception of Hh signals are tightly regulated, and abnormal Hh signaling is associated with developmental defects and cancer. In addition to the integral membrane proteins Patched and Smoothened, members of the Drosophila Ihog family of adhesion-like molecules have recently been shown to bind Hh proteins with micromolar affinity and positively regulate Hh signaling. Cell adhesion molecule-related, down-regulated by oncogenes (CDO) and Brother of CDO (BOC) are the closest mammalian relatives of Drosophila Ihog, and CDO binds Sonic Hh with micromolar affinity and positively regulates Hh signaling. Despite these similarities, structural and biochemical studies have shown that Ihog and CDO utilize nonorthologous domains and completely different binding modes to interact with cognate Hh proteins. We report here biochemical and x-ray structural studies of Sonic, Indian, and Desert Hh proteins both alone and complexed with active domains of CDO and BOC. These results show that all mammalian Hh proteins bind CDO and BOC in the same manner. We also show that interactions between Hh proteins and CDO are weakened at low pH. Formation of Hh-mediated Hh oligomers is thought to be an important feature of normal Hh signaling, but no conserved self-interaction between Hh proteins is apparent from inspection of 14 independent Hh-containing crystal lattices.

摘要

刺猬 (Hh) 信号蛋白在动物发育的多个点刺激细胞增殖、分化和组织模式形成。果蝇中存在单个 Hh 同源物,但哺乳动物中存在三个 Hh 同源物,即 Sonic Hh、Indian Hh 和 Desert Hh。Hh 信号的分布、运动和接收受到严格调控,异常的 Hh 信号与发育缺陷和癌症有关。除了完整的膜蛋白 patched 和 smoothened 外,果蝇 Ihog 家族的粘附样分子的成员最近也被证明以微摩尔亲和力结合 Hh 蛋白,并正向调节 Hh 信号。细胞粘附分子相关,癌基因下调 (CDO) 和 CDO 的兄弟 (BOC) 是果蝇 Ihog 的最接近的哺乳动物亲属,CDO 以微摩尔亲和力结合 Sonic Hh 并正向调节 Hh 信号。尽管存在这些相似之处,但结构和生化研究表明,Ihog 和 CDO 利用非同源结构域和完全不同的结合模式与同源 Hh 蛋白相互作用。我们在这里报告了 Sonic、Indian 和 Desert Hh 蛋白的生化和 x 射线结构研究,这些蛋白单独存在或与 CDO 和 BOC 的活性结构域复合存在。这些结果表明,所有哺乳动物 Hh 蛋白以相同的方式与 CDO 和 BOC 结合。我们还表明,在低 pH 值下,Hh 蛋白与 CDO 的相互作用减弱。Hh 介导的 Hh 寡聚体的形成被认为是正常 Hh 信号的一个重要特征,但从 14 个独立的 Hh 包含的晶格检查中,没有明显的 Hh 蛋白之间的保守自我相互作用。

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