抑制 KDM1A/LSD1 可增强卵巢癌的化疗反应。

IF 3 2区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Molecular Carcinogenesis Pub Date : 2024-10-01 Epub Date: 2024-07-11 DOI:10.1002/mc.23792
Yihong Chen, Jessica D Johnson, Sridharan Jayamohan, Yi He, Prabhakar P Venkata, Diksha Jamwal, Salvador Alejo, Yi Zou, Zhao Lai, Suryavathi Viswanadhapalli, Ratna K Vadlamudi, Edward Kost, Gangadhara R Sareddy
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引用次数: 0

摘要

卵巢癌(OCa)是最致命的妇科癌症。卵巢癌的标准治疗方法是铂类化疗,如卡铂或顺铂联合紫杉醇。大多数患者最初对这些治疗方法有反应,但近 90% 的患者会出现复发,并不可避免地死于化疗耐药。最近的研究发现,表观遗传修饰因子赖氨酸特异性组蛋白去甲基化酶1A(KDM1A/LSD1)在OCa中高度过表达。然而,KDM1A在化疗耐药性中的作用以及抑制KDM1A是否会增强OCa的化疗反应仍不确定。对TCGA数据集的分析表明,KDM1A在化疗反应差的患者中高表达。Western印迹分析显示,化疗药物顺铂、卡铂和紫杉醇会增加KDM1A在OCa细胞中的表达。KDM1A敲除(KD)或KDM1A抑制剂NCD38和SP2509能使已建立的和患者来源的OCa细胞对化疗药物敏感,从而降低细胞活力和克隆存活率并诱导细胞凋亡。此外,KDM1A的敲除使卡铂耐药的A2780-CP70细胞对卡铂治疗敏感,使紫杉醇耐药的SKOV3-TR细胞对紫杉醇敏感。RNA-seq分析显示,KDM1A-KD和顺铂联合治疗会导致上皮-间质转化(EMT)相关基因下调。有趣的是,顺铂处理增加了NF-κB通路基因的子集,而KDM1A-KD或KDM1A抑制则逆转了这种效应。重要的是,与单一治疗相比,KDM1A-KD与顺铂联合治疗可显著降低正位滑囊内OCa异种移植模型中的肿瘤生长。总之,这些研究结果表明,KDM1A抑制剂与化疗的结合可能是治疗OCa的一种很有前景的治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
KDM1A/LSD1 inhibition enhances chemotherapy response in ovarian cancer.

Ovarian cancer (OCa) is the deadliest of all gynecological cancers. The standard treatment for OCa is platinum-based chemotherapy, such as carboplatin or cisplatin in combination with paclitaxel. Most patients are initially responsive to these treatments; however, nearly 90% will develop recurrence and inevitably succumb to chemotherapy-resistant disease. Recent studies have revealed that the epigenetic modifier lysine-specific histone demethylase 1A (KDM1A/LSD1) is highly overexpressed in OCa. However, the role of KDM1A in chemoresistance and whether its inhibition enhances chemotherapy response in OCa remains uncertain. Analysis of TCGA datasets revealed that KDM1A expression is high in patients who poorly respond to chemotherapy. Western blot analysis show that treatment with chemotherapy drugs cisplatin, carboplatin, and paclitaxel increased KDM1A expression in OCa cells. KDM1A knockdown (KD) or treatment with KDM1A inhibitors NCD38 and SP2509 sensitized established and patient-derived OCa cells to chemotherapy drugs in reducing cell viability and clonogenic survival and inducing apoptosis. Moreover, knockdown of KDM1A sensitized carboplatin-resistant A2780-CP70 cells to carboplatin treatment and paclitaxel-resistant SKOV3-TR cells to paclitaxel. RNA-seq analysis revealed that a combination of KDM1A-KD and cisplatin treatment resulted in the downregulation of genes related to epithelial-mesenchymal transition (EMT). Interestingly, cisplatin treatment increased a subset of NF-κB pathway genes, and KDM1A-KD or KDM1A inhibition reversed this effect. Importantly, KDM1A-KD, in combination with cisplatin, significantly reduced tumor growth compared to a single treatment in an orthotopic intrabursal OCa xenograft model. Collectively, these findings suggest that combination of KDM1A inhibitors with chemotherapy could be a promising therapeutic approach for the treatment of OCa.

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来源期刊
Molecular Carcinogenesis
Molecular Carcinogenesis 医学-生化与分子生物学
CiteScore
7.30
自引率
2.20%
发文量
112
审稿时长
2 months
期刊介绍: Molecular Carcinogenesis publishes articles describing discoveries in basic and clinical science of the mechanisms involved in chemical-, environmental-, physical (e.g., radiation, trauma)-, infection and inflammation-associated cancer development, basic mechanisms of cancer prevention and therapy, the function of oncogenes and tumors suppressors, and the role of biomarkers for cancer risk prediction, molecular diagnosis and prognosis.
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