CRBM, University of Montpellier, CNRS, Montpellier, France.
BioCampus Montpellier, University of Montpellier, CNRS, INSERM, Montpellier, France.
Cell Rep. 2021 Oct 19;37(3):109867. doi: 10.1016/j.celrep.2021.109867.
Phosphatidylinositol 3-kinase-related kinases (PIKKs) are a family of kinases that control fundamental processes, including cell growth, DNA damage repair, and gene expression. Although their regulation and activities are well characterized, little is known about how PIKKs fold and assemble into active complexes. Previous work has identified a heat shock protein 90 (Hsp90) cochaperone, the TTT complex, that specifically stabilizes PIKKs. Here, we describe a mechanism by which TTT promotes their de novo maturation in fission yeast. We show that TTT recognizes newly synthesized PIKKs during translation. Although PIKKs form multimeric complexes, we find that they do not engage in cotranslational assembly with their partners. Rather, our findings suggest a model by which TTT protects nascent PIKK polypeptides from misfolding and degradation because PIKKs acquire their native state after translation is terminated. Thus, PIKK maturation and assembly are temporally segregated, suggesting that the biogenesis of large complexes requires both dedicated chaperones and cotranslational interactions between subunits.
磷脂酰肌醇 3-激酶相关激酶(PIKKs)是一类激酶,它们控制着包括细胞生长、DNA 损伤修复和基因表达在内的基本过程。尽管它们的调节和活性已得到很好的描述,但对于 PIKKs 如何折叠并组装成活性复合物知之甚少。先前的工作已经确定了热休克蛋白 90(Hsp90)共伴侣 TTT 复合物,它可以特异性稳定 PIKKs。在这里,我们描述了 TTT 促进裂殖酵母中 PIKKs 从头成熟的机制。我们表明 TTT 在翻译过程中识别新合成的 PIKKs。尽管 PIKKs 形成多聚体复合物,但我们发现它们不会与伴侣进行共翻译组装。相反,我们的发现表明 TTT 通过保护新生 PIKK 多肽免于错误折叠和降解来发挥作用,因为 PIKKs 在翻译终止后获得其天然状态。因此,PIKK 的成熟和组装是时间上分开的,这表明大型复合物的生物发生既需要专用伴侣,也需要亚基之间的共翻译相互作用。
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