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EX527,一种 SIRT1 抑制剂,通过下调细胞 FLICE 抑制蛋白使 T 细胞白血病对死亡受体介导的细胞凋亡敏感。

EX527, a sirtuins 1 inhibitor, sensitizes T-cell leukemia to death receptor-mediated apoptosis by downregulating cellular FLICE inhibitory protein.

机构信息

Department of Clinical Laboratory, The Third Affiliated Hospital of Xinxiang Medical University, Xinxiang, China.

Henan Key Laboratory of Immunology and Targeted Drugs, School of Laboratory Medicine, Xinxiang Medical University, Xinxiang, China.

出版信息

Cancer Biol Ther. 2024 Dec 31;25(1):2402588. doi: 10.1080/15384047.2024.2402588. Epub 2024 Sep 17.

DOI:10.1080/15384047.2024.2402588
PMID:39286953
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11409494/
Abstract

Death receptor-mediated extrinsic apoptosis system had been developed as a promising therapeutic strategy in clinical oncology, such as TRAIL therapy. However, multiple studies have demonstrated that TRAIL resistance is the biggest problem for disappointing clinical trials despite preclinical success. Targeting cellular FLICE inhibitory protein (cFLIP) is one strategy of combinatorial therapies to overcome resistance to DR-mediated apoptosis due to its negative regulator of extrinsic apoptosis. E × 527 (Selisistat) is a specific inhibitor of SIRT1 activity with safe and well tolerance in clinical trials. Here, we show that E × 527 could strengthen significantly activation of rhFasL-mediated apoptotic signaling pathway and increased apoptotic rate of T leukemia cells with high expression of cFLIP. Mechanically, Inhibition of SIRT1 by E × 527 increased polyubiquitination level of cFLIP via increasing acetylation of Ku70, which could promote proteosomal degradation of cFLIP protein. It implied that combinatorial therapies of E × 527 plus TRAIL may have a potential as a novel clinical application for TRAIL-resistant hematologic malignancies.

摘要

死亡受体介导的外在凋亡系统已被开发为临床肿瘤学中的一种有前途的治疗策略,例如 TRAIL 治疗。然而,多项研究表明,尽管在临床前取得了成功,但 TRAIL 耐药性是临床试验令人失望的最大问题。靶向细胞 FLICE 抑制蛋白(cFLIP)是克服 DR 介导的凋亡抵抗的联合治疗策略之一,因为它是外在凋亡的负调节剂。E × 527(Selisistat)是 SIRT1 活性的特异性抑制剂,在临床试验中具有安全和良好的耐受性。在这里,我们表明 E × 527 可以显著增强 rhFasL 介导的凋亡信号通路的激活,并增加高表达 cFLIP 的 T 白血病细胞的凋亡率。在机制上,E × 527 通过增加 Ku70 的乙酰化来抑制 SIRT1,从而增加 cFLIP 的多泛素化水平,这可以促进 cFLIP 蛋白的蛋白酶体降解。这表明 E × 527 联合 TRAIL 的联合治疗可能具有作为 TRAIL 耐药性血液恶性肿瘤的新型临床应用的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/f78ee26c68f0/KCBT_A_2402588_F0006_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/d1e056520776/KCBT_A_2402588_F0001_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/cd8432738c60/KCBT_A_2402588_F0002_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/c447f3e05694/KCBT_A_2402588_F0003_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/e8d87a13a3fc/KCBT_A_2402588_F0004_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/c96428cf5b15/KCBT_A_2402588_F0005_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/f78ee26c68f0/KCBT_A_2402588_F0006_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/d1e056520776/KCBT_A_2402588_F0001_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/cd8432738c60/KCBT_A_2402588_F0002_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/c447f3e05694/KCBT_A_2402588_F0003_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/e8d87a13a3fc/KCBT_A_2402588_F0004_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/c96428cf5b15/KCBT_A_2402588_F0005_OC.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c625/11409494/f78ee26c68f0/KCBT_A_2402588_F0006_OC.jpg

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本文引用的文献

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Harnessing TRAIL-induced cell death for cancer therapy: a long walk with thrilling discoveries.利用 TRAIL 诱导的细胞死亡进行癌症治疗:充满惊险发现的漫长之旅。
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c-FLIP is involved in tumor progression of peripheral T-cell lymphoma and targeted by histone deacetylase inhibitors.c-FLIP参与外周T细胞淋巴瘤的肿瘤进展,并被组蛋白去乙酰化酶抑制剂靶向作用。
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An exploratory double-blind, randomized clinical trial with selisistat, a SirT1 inhibitor, in patients with Huntington's disease.一项针对亨廷顿舞蹈症患者,使用SirT1抑制剂塞利西利进行的探索性双盲随机临床试验。
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