4.6 Article

Proteasome activator Blm10 levels and autophagic degradation directly impact the proteasome landscape

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JOURNAL OF BIOLOGICAL CHEMISTRY
卷 296, 期 -, 页码 -

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ELSEVIER
DOI: 10.1016/j.jbc.2021.100468

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  1. National Institutes of Health (National Institute of General Medical Science: K-INBRE program) [P20GM103418, R01GM118660]

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The proteasome selectively degrades proteins and consists of different complexes, which are poorly understood in terms of regulation and response to changing physiological conditions. The study focused on Blm10 and RP, showing that controlling Blm10 levels affects the formation of RP-CP complexes through autophagy. Reducing Blm10 levels can increase CP-binding surfaces and impact proteasome function, providing important insights into maintaining the proteasome landscape.
The proteasome selectively degrades proteins. It consists of a core particle (CP), which contains proteolytic active sites that can associate with different regulators to form various complexes. How these different complexes are regulated and affected by changing physiological conditions, however, remains poorly understood. In this study, we focused on the activator Blm10 and the regulatory particle (RP). In yeast, increased expression of Blm10 outcompeted RP for CP binding, which suggests that controlling the cellular levels of Blm10 can affect the relative amounts of RP-bound CP. While strong overexpression of BLM10 almost eliminated the presence of RP-CP complexes, the phenotypes this should induce were not observed. Our results show this was due to the induction of Blm10-CP autophagy under prolonged growth in YPD. Similarly, under conditions of endogenous BLM10 expression, Blm10 was degraded through autophagy as well. This suggests that reducing the levels of Blm10 allows for more CP-binding surfaces and the formation of RP-CP complexes under nutrient stress. This work provides important insights into maintaining the proteasome landscape and how protein expression levels affect proteasome function.

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