Targeting SUMOylation dependency in human cancer stem cells through a unique SAE2 motif revealed by chemical genomics

Benoit Yannick D.; Mitchell Ryan R.; Wang WenliangOrlando LucaBoyd Allison L.Tanasijevic BorkoAslostovar LiliShapovalova ZoyaDoyle MeaghanBergin Christopher J.Vojnits KingaCasado Fanny L.Di Lu JustinPorras Deanna P.Garcia-Rodriguez Juan LuisRussell JenniferZouggar AichaMasibag Angelique N.Caba CodyKoteva KalinkaKinthada Lakshmana K.Patel Jagdish SureshAndres Sara N.Magolan JakobCollins Tony J.Wright Gerard D.Bhatia Mickie

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Targeting SUMOylation dependency in human cancer stem cells through a unique SAE2 motif revealed by chemical genomics

机译：通过化学基因组学揭示的独特 SAE2 基序靶向人类癌症干细胞中的 SUMoylation 依赖性

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Natural products (NPs) encompass a rich source of bioactive chemical entities. Here, we used human cancer stem cells (CSCs) in a chemical genomics campaign with NP chemical space to interrogate extracts from diverse strains of actinomycete for anti-cancer properties. We identified a compound (McM25044) capable of selectively inhibiting human CSC function versus normal stem cell counterparts. Biochemical and molecular studies revealed that McM025044 exerts inhibition on human CSCs through the small ubiquitin-like modifier (SUMO) cascade, found to be hyperactive in a variety of human cancers. McM025044 impedes the SUMOylation pathway via direct targeting of the SAE1/2 complex. Treatment of patient-derived CSCs resulted in reduced levels of SUMOylated proteins and suppression of progenitor and stem cell capacity measured in vitro and in vivo. Our study overcomes a barrier in chemically inhibiting oncogenic SUMOylation activity and uncovers a unique role for SAE2 in the biology of human cancers.

机译：天然产物（NP）包含丰富的生物活性化学实体来源。在这里，我们在化学基因组学活动中使用了人类癌症干细胞（CSCs）和NP化学空间，以研究不同放线菌菌株的提取物的抗癌特性。我们发现了一种化合物（MCM25044），与正常干细胞相比，能够选择性抑制人CSC功能。生化和分子研究表明，MCM025044 通过小泛素样修饰剂（SUMO）级联反应对人 CSC 施加抑制作用，发现在多种人类癌症中具有超活跃性。MCM025044 通过直接靶向 SAE1/2 复合物阻碍 SUMO化途径。患者来源的 CSC 的治疗导致 SUMO 化蛋白水平降低，并在体外和体内测量祖细胞和干细胞容量受到抑制。我们的研究克服了化学抑制致癌SUMO化活性的障碍，并揭示了SAE2在人类癌症生物学中的独特作用。

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《Cell chemical biology》 |2021年第10期|1394-+|共24页
作者
Benoit Yannick D.; Mitchell Ryan R.; Wang WenliangOrlando LucaBoyd Allison L.Tanasijevic BorkoAslostovar LiliShapovalova ZoyaDoyle MeaghanBergin Christopher J.Vojnits KingaCasado Fanny L.Di Lu JustinPorras Deanna P.Garcia-Rodriguez Juan LuisRussell JenniferZouggar AichaMasibag Angelique N.Caba CodyKoteva KalinkaKinthada Lakshmana K.Patel Jagdish SureshAndres Sara N.Magolan JakobCollins Tony J.Wright Gerard D.Bhatia Mickie;
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McMaster Univ;

Univ Ottawa;

Univ Idaho;

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原文格式 PDF
正文语种英语
中图分类普通生物学;生物化学;
关键词
ACUTE MYELOID-LEUKEMIA; NATURAL-PRODUCTS; STATISTICAL-MODEL; IDENTIFICATION; DISCOVERY; DRUGS; AML; COMBINATION; PLURAMYCINS; INSIGHTS;

机译：急性髓系白血病;天然产品;统计模型;识别;发现;药物;反洗钱;组合;普鲁霉素;见解;

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1. Human induced pluripotent stem cells labeled with fluorescent magnetic nanoparticles for targeted imaging and hyperthermia therapy for gastric cancer [J] . Chao Li, Jing Ruan, Meng Yang, 癌症生物学与医学：英文版 . 2015,第003期
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3. Growth differentiation factor 6, a repressive target of EZH2, promotes the commitment of human embryonic stem cells to mesenchymal stem cells [J] . Pend Deng, Yongxin Yu, Christine Hong, 骨研究（英文版） . 2020,第4期
4. Functional Genomics In Vivo Reveal Metabolic Dependencies of Pancreatic Cancer Cells [J] . Zhu Xiphias Ge, Chudnovskiy Aleksey, Baudrier LouPrizer BenjaminLiu YuyangOstendorf Benjamin N.Yamaguchi NorihiroArab AbolfozlTavora BernardoTimson RebeccaHeissel Sorende Stanchina ElisaMolina HenrikVictora Gabriel D.Goodarzi HaniBirsoy Kivanc Cell metabolism . 2021,第1期

机译：Functional Genomics In Vivo Reveal Metabolic Dependencies of Pancreatic Cancer Cells
5. Target-enriched nanopore sequencing and de novo assembly reveals co-occurrences of complex on-target genomic rearrangements induced by CRISPR-Cas9 in human cells [J] . Geng Keyi, Merino Lara G., Wedemann LindaMartens AniekSobota MalgorzataSanchez Yerma P.Sondergaard Jonas NorskovWhite Robert J.Kutter Claudia Genome research . 2022,第10期

机译：Target-enriched nanopore sequencing and de novo assembly reveals co-occurrences of complex on-target genomic rearrangements induced by CRISPR-Cas9 in human cells
6. Human embryonic stem cell-derived neural crest model unveils CD55 as a cancer stem cell regulator for therapeutic targeting in MYCN -amplified neuroblastoma [J] . Zhihui Weng, Jiacheng Lin, Jiaozi HeLin GaoSien LinLai Ling TsangHang ZhangXiaoyan HeGuang WangXuesong YangHu ZhouHui ZhaoGang LiLin ZouXiaohua Jiang Neuro-oncology . 2022,第6期

机译：Human embryonic stem cell-derived neural crest model unveils CD55 as a cancer stem cell regulator for therapeutic targeting in MYCN -amplified neuroblastoma
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机译：https://researchopenworld.com/development-of-synthetic-cell-differentiation-agent-formulations-for-the-prevention-and-therapy-of-cancer-via-targeting-of-cancer-stem-cells/#

Targeting SUMOylation dependency in human cancer stem cells through a unique SAE2 motif revealed by chemical genomics

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