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Emerging roles for the BAI1 protein family in the regulation of phagocytosis, synaptogenesis, neurovasculature, and tumor development

机译:BAI1蛋白家族在吞噬作用,突触形成,神经脉管系统和肿瘤发展中的调节作用

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摘要

While G-protein-coupled receptors (GPCRs) have received considerable attention for their biological activity in a diversity of physiological functions and have become targets for therapeutic intervention in many diseases, the function of the cell adhesion subfamily of GPCRs remains poorly understood. Within this group, the family of brain angiogenesis inhibitor molecules (BAI1-3) has become increasingly appreciated for their diverse roles in biology and disease. In particular, recent findings suggest emerging roles for BAI1 in the regulation of phenomena including phagocytosis, synaptogenesis, and the inhibition of tumor growth and angiogenesis via the processing of its extracellular domain into secreted vasculostatins. Here we summarize the known biological features of the BAI proteins, including their structure, proteolysis events, and interacting partners, and their recently identified ability to regulate certain signaling pathways. Finally, we discuss the potential of the BAIs as therapeutics or targets for diseases as varied as cancer, stroke, and schizophrenia.
机译:尽管G蛋白偶联受体(GPCR)因其在多种生理功能中的生物学活性而受到相当大的关注,并已成为许多疾病中治疗干预的目标,但对GPCR的细胞粘附亚家族的功能仍然知之甚少。在这一组中,脑血管生成抑制剂分子(BAI1-3)家族因其在生物学和疾病中的多种作用而受到越来越多的赞赏。特别是,最近的发现表明BAI1在调节现象中起着新的作用,包括吞噬作用,突触形成以及通过将其胞外域加工成分泌的血管抑制素来抑制肿瘤的生长和血管生成。在这里,我们总结了BAI蛋白质的已知生物学特征,包括它们的结构,蛋白水解事件和相互作用的伴侣,以及它们最近发现的调节某些信号通路的能力。最后,我们讨论了BAI作为癌症或中风和精神分裂症等疾病的治疗剂或靶标的潜力。

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