Hyd/UBR5定义了一种肿瘤抑制通路，它将多聚酶抑制复合体与组织生长控制和肿瘤发生过程中的调控蛋白降解联系起来。

IF 7.5 1区生物学 Q1 CELL BIOLOGY

Genes & development Pub Date : 2024-08-20 DOI:10.1101/gad.351856.124

Pei Wen, Huiyan Lei, Hua Deng, Su Deng, Carla Rodriguez Tirado, Meiling Wang, Ping Mu, Yonggang Zheng, Duojia Pan

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引用次数: 0

摘要

肿瘤抑制基因在正常组织稳态中发挥着关键作用，它们的失调是包括癌症在内的人类疾病的根源。除了人类遗传学之外，果蝇等模式生物在发现肿瘤抑制通路方面也发挥了重要作用，这些通路随后被证明与人类癌症高度相关。在这里，我们展示了增生盘（Hyd）和Lines（Lin），增生盘（Hyd）是最早从果蝇基因中分离出来的肿瘤抑制因子之一，编码一种迄今未知底物的E3泛素连接酶，而Lines（Lin）则因其在胚胎分割中的作用而闻名、确定了一种强制性肿瘤抑制蛋白复合物（Hyd-Lin），该复合物以含锌指的肿瘤蛋白 Bowl 为靶标进行泛素介导的降解，Lin 起着底物适配器的作用，将 Bowl 募集到 Hyd 上进行泛素化。有趣的是，Hyd-Lin 复合物的活性直接受到另一个锌指基因鼓槌（drumstick，drm）编码的一种微肽的抑制，这种微肽通过将 Bowl 从 Hyd-Lin 复合物中置换出来而发挥伪底物的功能，从而稳定 Bowl。我们进一步确定了表观遗传调节因子多聚核糖抑制复合体 1（PRC1）通过直接抑制微肽 drm 的转录而成为 Hyd-Lin-Bowl 通路的关键上游调节因子。与这些分子研究相一致，我们证明了遗传性失活 Hyd、Lin 或 PRC1 会导致体内 Bowl 依赖性增生组织过度生长。我们还提供了证据，证明哺乳动物的同源物 Hyd（UBR5，已知在多种人类癌症中反复失调）、Lin（LINS1）和 Bowl（OSR1/2）在人类细胞中构成了类似的蛋白质降解途径，而且 OSR2 促进了前列腺癌的发生。总之，这些发现定义了一种以前未被发现的肿瘤抑制途径，它将组织生长控制和肿瘤发生过程中的表观遗传程序与调控蛋白降解联系起来。

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Hyd/UBR5 defines a tumor suppressor pathway that links Polycomb repressive complex to regulated protein degradation in tissue growth control and tumorigenesis.

Tumor suppressor genes play critical roles in normal tissue homeostasis, and their dysregulation underlies human diseases including cancer. Besides human genetics, model organisms such as Drosophila have been instrumental in discovering tumor suppressor pathways that were subsequently shown to be highly relevant in human cancer. Here we show that hyperplastic disc (Hyd), one of the first tumor suppressors isolated genetically in Drosophila and encoding an E3 ubiquitin ligase with hitherto unknown substrates, and Lines (Lin), best known for its role in embryonic segmentation, define an obligatory tumor suppressor protein complex (Hyd-Lin) that targets the zinc finger-containing oncoprotein Bowl for ubiquitin-mediated degradation, with Lin functioning as a substrate adaptor to recruit Bowl to Hyd for ubiquitination. Interestingly, the activity of the Hyd-Lin complex is directly inhibited by a micropeptide encoded by another zinc finger gene, drumstick (drm), which functions as a pseudosubstrate by displacing Bowl from the Hyd-Lin complex, thus stabilizing Bowl. We further identify the epigenetic regulator Polycomb repressive complex1 (PRC1) as a critical upstream regulator of the Hyd-Lin-Bowl pathway by directly repressing the transcription of the micropeptide drm Consistent with these molecular studies, we show that genetic inactivation of Hyd, Lin, or PRC1 resulted in Bowl-dependent hyperplastic tissue overgrowth in vivo. We also provide evidence that the mammalian homologs of Hyd (UBR5, known to be recurrently dysregulated in various human cancers), Lin (LINS1), and Bowl (OSR1/2) constitute an analogous protein degradation pathway in human cells, and that OSR2 promotes prostate cancer tumorigenesis. Altogether, these findings define a previously unrecognized tumor suppressor pathway that links epigenetic program to regulated protein degradation in tissue growth control and tumorigenesis.

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来源期刊

Genes & development 生物-发育生物学

CiteScore

17.50

自引率

1.90%

发文量

审稿时长

3-6 weeks

期刊介绍： Genes & Development is a research journal published in association with The Genetics Society. It publishes high-quality research papers in the areas of molecular biology, molecular genetics, and related fields. The journal features various research formats including Research papers, short Research Communications, and Resource/Methodology papers. Genes & Development has gained recognition and is considered as one of the Top Five Research Journals in the field of Molecular Biology and Genetics. It has an impressive Impact Factor of 12.89. The journal is ranked #2 among Developmental Biology research journals, #5 in Genetics and Heredity, and is among the Top 20 in Cell Biology (according to ISI Journal Citation Reports®, 2021).