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Post-Translational Dosage Compensation Buffers Genetic Perturbations to Stoichiometry of Protein Complexes

机译:翻译后剂量补偿缓冲液对蛋白质复合物化学计量的遗传扰动

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摘要

Understanding buffering mechanisms for various perturbations is essential for understanding robustness in cellular systems. Protein-level dosage compensation, which arises when changes in gene copy number do not translate linearly into protein level, is one mechanism for buffering against genetic perturbations. Here, we present an approach to identify genes with dosage compensation by increasing the copy number of individual genes using the genetic tug-of-war technique. Our screen of chromosome I suggests that dosage-compensated genes constitute approximately 10% of the genome and consist predominantly of subunits of multi-protein complexes. Importantly, because subunit levels are regulated in a stoichiometry-dependent manner, dosage compensation plays a crucial role in maintaining subunit stoichiometries. Indeed, we observed changes in the levels of a complex when its subunit stoichiometries were perturbed. We further analyzed compensation mechanisms using a proteasome-defective mutant as well as ribosome profiling, which provided strong evidence for compensation by ubiquitin-dependent degradation but not reduced translational efficiency. Thus, our study provides a systematic understanding of dosage compensation and highlights that this post-translational regulation is a critical aspect of robustness in cellular systems.
机译:了解各种扰动的缓冲机制对于理解蜂窝系统的鲁棒性至关重要。当基因拷贝数的变化不线性地转化为蛋白质水平时出现的蛋白质水平剂量补偿是一种缓冲遗传干扰的机制。在这里,我们提出一种使用遗传拉锯战技术通过增加单个基因的拷贝数来鉴定具有剂量补偿的基因的方法。我们对I号染色体的筛选表明,剂量补偿的基因约占基因组的10%,并且主要由多蛋白复合物的亚基组成。重要的是,因为亚单位水平以化学计量依赖的方式调节,所以剂量补偿在维持亚单位化学计量中起着至关重要的作用。确实,我们观察到当其亚基化学计量受到干扰时复合物水平的变化。我们进一步分析了使用蛋白酶体缺陷型突变体以及核糖体图谱的补偿机制,这为泛素依赖性降解而不是降低翻译效率提供了有力的证据。因此,我们的研究对剂量补偿提供了系统的理解,并强调了这种翻译后调节是细胞系统坚固性的关键方面。

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