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The biogenesis of active Protein Phosphatase 2A holoenzymes: a tightly regulated process creating phosphatase specificity

机译:活性蛋白磷酸酶2A全酶的生物发生:一个严格调节的过程,产生磷酸酶特异性

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摘要

Protein Phosphatase type 2A (PP2A) enzymes comprise a large family of Ser/Thr phosphatases with multiple functions in cellular signaling and physiology. The composition of heterotrimeric PP2A holoenzymes, resulting from the combinatorial assembly of a catalytic C, structural A and regulatory B-type subunit, provides the essential determinants for substrate specificity, subcellular targeting and fine-tuning of phosphatase activity, largely explaining why PP2A is functionally involved in so many diverse physiological processes, sometimes in seemingly opposing ways. In this review, we highlight how PP2A holoenzyme biogenesis and enzymatic activity are controlled by a sophisticatedly coordinated network of five PP2A modulators, consisting of α4, PTPA, LCMT1, PME-1 and potentially TIPRL1, which serve to prevent promiscuous phosphatase activity until the holoenzyme is completely assembled. Likewise, these modulators may come into play when PP2A holoenzymes are disassembled following particular cellular stresses. Malfunctioning of these cellular control mechanisms contributes to human disease. The potential therapeutic benefits or pitfalls of interfering with these regulatory mechanisms will be briefly discussed.
机译:2A型蛋白磷酸酶(PP2A)酶包含大量的Ser / Thr磷酸酶家族,在细胞信号传导和生理学中具有多种功能。异源三聚体PP2A全酶的组成是催化C型,结构A型和调节性B型亚基的组合装配,为底物特异性,亚细胞靶向和磷酸酶活性的微调提供了重要的决定因素,这在很大程度上解释了PP2A在功能上的原因涉及许多不同的生理过程,有时以相反的方式参与。在这篇综述中,我们着重介绍了如何由五个由PP4A调节剂(由α4,PTPA,LCMT1,PME-1和潜在的TIPRL1组成)的精密协调网络控制PP2A完整酶的生物发生和酶活性,这些酶可防止混杂的磷酸酶活性直至完整酶完全组装好了。同样,当特定的细胞应激后分解PP2A全酶时,这些调节剂可能会发挥作用。这些细胞控制机制的功能障碍导致人类疾病。将简要讨论干扰这些调节机制的潜在治疗益处或陷阱。

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