Degradome analysis to identify direct protein substrates of small-molecule degraders

IF 6.6 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Cell Chemical Biology Pub Date : 2024-11-12 DOI:10.1016/j.chembiol.2024.10.007
Marco Jochem, Anna Schrempf, Lina-Marie Wagner, Dmitri Segal, Jose Cisneros, Amanda Ng, Georg E. Winter, Jeroen Krijgsveld
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Abstract

Targeted protein degradation (TPD) has emerged as a powerful strategy to selectively eliminate cellular proteins using small-molecule degraders, offering therapeutic promise for targeting proteins that are otherwise undruggable. However, a remaining challenge is to unambiguously identify primary TPD targets that are distinct from secondary downstream effects in the proteome. Here we introduce an approach for selective analysis of protein degradation by mass spectrometry (DegMS) at proteomic scale, which derives its specificity from the exclusion of confounding effects of altered transcription and translation induced by target depletion. We show that the approach efficiently operates at the timescale of TPD (hours) and we demonstrate its utility by analyzing the cyclin K degraders dCeMM2 and dCeMM4, which induce widespread transcriptional downregulation, and the GSPT1 degrader CC-885, an inhibitor of protein translation. Additionally, we apply DegMS to characterize a previously uncharacterized degrader, and identify the zinc-finger protein FIZ1 as a degraded target.

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通过降解组分析确定小分子降解器的直接蛋白质底物
靶向蛋白质降解(TPD)已成为一种利用小分子降解剂选择性消除细胞蛋白质的强大策略,为靶向那些无法治疗的蛋白质提供了治疗前景。然而,如何明确识别蛋白质组中有别于次级下游效应的主要 TPD 靶点仍是一个挑战。在这里,我们介绍了一种在蛋白质组范围内通过质谱(DegMS)对蛋白质降解进行选择性分析的方法,其特异性来自于排除了靶标耗竭引起的转录和翻译改变的干扰效应。我们通过分析诱导广泛转录下调的细胞周期蛋白 K 降解剂 dCeMM2 和 dCeMM4 以及蛋白翻译抑制剂 GSPT1 降解剂 CC-885 证明了这种方法的实用性。此外,我们还应用 DegMS 鉴定了一种以前未鉴定过的降解器,并将锌指蛋白 FIZ1 鉴定为降解靶标。
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来源期刊
Cell Chemical Biology
Cell Chemical Biology Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
14.70
自引率
2.30%
发文量
143
期刊介绍: Cell Chemical Biology, a Cell Press journal established in 1994 as Chemistry & Biology, focuses on publishing crucial advances in chemical biology research with broad appeal to our diverse community, spanning basic scientists to clinicians. Pioneering investigations at the chemistry-biology interface, the journal fosters collaboration between these disciplines. We encourage submissions providing significant conceptual advancements of broad interest across chemical, biological, clinical, and related fields. Particularly sought are articles utilizing chemical tools to perturb, visualize, and measure biological systems, offering unique insights into molecular mechanisms, disease biology, and therapeutics.
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