Ubiquitin receptors play redundant roles in the proteasomal degradation of the p53 repressor MDM2.

IF 3 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY FEBS Letters Pub Date : 2022-11-01 DOI:10.1002/1873-3468.14436
Alison Sparks, Christopher J Kelly, Mark K Saville
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Abstract

Much remains to be determined about the participation of ubiquitin receptors in proteasomal degradation and their potential as therapeutic targets. Suppression of the ubiquitin receptor S5A/PSMD4/hRpn10 alone stabilises p53/TP53 but not the key p53 repressor MDM2. Here, we observed S5A and the ubiquitin receptors ADRM1/PSMD16/hRpn13 and RAD23A and B functionally overlap in MDM2 degradation. We provide further evidence that degradation of only a subset of ubiquitinated proteins is sensitive to S5A knockdown because ubiquitin receptor redundancy is commonplace. p53 can be upregulated by S5A modulation while degradation of substrates with redundant receptors is maintained. Our observations and analysis of Cancer Dependency Map (DepMap) screens show S5A depletion/loss substantially reduces cancer cell line viability. This and selective S5A dependency of proteasomal substrates make S5A a target of interest for cancer therapy.

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泛素受体在p53抑制因子MDM2的蛋白酶体降解中发挥冗余作用。
关于泛素受体在蛋白酶体降解中的参与及其作为治疗靶点的潜力仍有待确定。单独抑制泛素受体S5A/PSMD4/hRpn10可以稳定p53/TP53,但不能稳定关键的p53抑制因子MDM2。在这里,我们观察到S5A和泛素受体ADRM1/PSMD16/hRpn13以及RAD23A和B在MDM2降解中的功能重叠。我们提供了进一步的证据表明,只有一部分泛素化蛋白的降解对S5A敲低敏感,因为泛素受体冗余是司空见惯的。p53可通过S5A调控上调,同时维持具有冗余受体的底物降解。我们对癌症依赖图谱(DepMap)的观察和分析显示,S5A的缺失大大降低了癌细胞系的生存能力。这一点以及蛋白酶体底物对S5A的选择性依赖使S5A成为癌症治疗的靶点。
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来源期刊
FEBS Letters
FEBS Letters 生物-生化与分子生物学
CiteScore
6.60
自引率
2.90%
发文量
303
审稿时长
1 months
期刊介绍: FEBS Letters is one of the world''s leading journals in molecular biology and is renowned both for its quality of content and speed of production. Bringing together the most important developments in the molecular biosciences, FEBS Letters provides an international forum for Minireviews, Research Letters and Hypotheses that merit urgent publication.
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