亲爱的研友该休息了!由于当前在线用户较少,发布求助请尽量完整地填写文献信息,科研通机器人24小时在线,伴您度过漫漫科研夜!身体可是革命的本钱,早点休息,好梦!

Abstract C87: EZH2 inhibition leads to decreased proliferation in SMARCA4-deleted ovarian cancer cell lines

PRC2 EZH2型 SMARCA4型 SMARCB1型 癌症研究 瑞士/瑞士法郎 染色质重塑 癌症 体重指数1 生物 染色质 组蛋白甲基转移酶 癌变 遗传学 基因
作者
Sarah K. Knutson,Allison E. Drew,Christopher Plescia,Robert A. Copeland,J. Joshua Smith,Heike Keilhack,Scott Ribich
出处
期刊:Molecular Cancer Therapeutics [American Association for Cancer Research]
卷期号:14 (12_Supplement_2): C87-C87 被引量:3
标识
DOI:10.1158/1535-7163.targ-15-c87
摘要

Abstract Introduction: The H3K27 histone methyltransferase EZH2 is the catalytic component of the polycomb repressive complex 2 (PRC2), and is amplified, overexpressed, or mutated in multiple cancer types, supporting its function as an oncogene. In addition to genetic alterations in EZH2 itself, distal genetic changes in other proteins can lead to oncogenic dependency on EZH2 activity. For example, we have previously established that cell lines and xenografts deficient in INI1 (SNF5/SMARCB1), a core component of the SWItch/Sucrose Non-Fermentable (SWI/SNF) chromatin remodeling complex, display profound sensitivity and durable regressions in the presence of the selective EZH2 inhibitor tazemetostat (EPZ-6438). Intriguingly, a complete response was observed in a patient with an INI1-negative rhabdoid tumor who participated in the tazemetostat Ph1 dose escalation study. This suggests that these tumors are addicted to dysregulated PRC2 activity, and confirms the previously proposed antagonistic relationship of SWI/SNF with PRC2, which is perturbed in INI1-deficient tumors. The loss of INI1 induces inappropriate SWI/SNF function, abrogating the repression of PRC2 activity, resulting in Polycomb target genes, such as those involved in differentiation and tumor suppression, to become aberrantly repressed. In addition to deletion of INI1, there are numerous reports describing genetic alterations in other SWI/SNF complex members. Given the oncogenic dependency of INI1-deficient tumors on PRC2 activity, we sought to investigate the sensitivity of other SWI/SNF mutated cancer types to EZH2 inhibition. Specifically, we investigated the effects of EZH2 inhibition in ovarian cancers carrying somatic mutations in the SWI/SNF complex members ARID1A and SMARCA4. Methods and results: A panel of ovarian cancer cell lines of different histologies was subjected to proliferation assays in 2-D tissue culture for 14 days in the presence of increasing concentrations of an EZH2 inhibitor. Selected cell lines were also tested in 3-D cultures, as it has been suggested in the literature that this context is necessary to observe anti-proliferative effects with EZH2 inhibitors. We found that ovarian cancer cell lines deficient in the SWI/SNF component SMARCA4 (also known as BRG1) are among the most sensitive in response to EZH2 inhibition, as demonstrated by decreased proliferation and/or morphology changes, at concentrations that are clinically achievable. In contrast, mutations in ARID1A, another SWI/SNF component, do not broadly confer sensitivity to EZH2 inhibition in ovarian cancer cell lines in either 2-D or 3-D in vitro assays. Furthermore, the effects of EZH2 inhibition on SMARCA4-negative ovarian cancer cells are context specific, since other cell types with SMARCA4 deletion, such as lung carcinoma cell lines, do not exhibit anti-proliferative affects with EZH2 inhibitor treatment. Conclusions: These data suggest that tazemetostat may have therapeutic benefit in SMARCA4-deleted ovarian cancer, such as small cell cancer of the ovary of the hypercalcemic type (SCCOHT), which shows a high degree of loss of SMARCA4 expression. Further in vitro and in vivo studies are underway to interrogate these initial results further. Citation Format: Sarah K. Knutson, Allison E. Drew, Christopher Plescia, Robert A. Copeland, Jesse J. Smith, Heike Keilhack, Scott Ribich. EZH2 inhibition leads to decreased proliferation in SMARCA4-deleted ovarian cancer cell lines. [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2015 Nov 5-9; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2015;14(12 Suppl 2):Abstract nr C87.

科研通智能强力驱动
Strongly Powered by AbleSci AI
科研通是完全免费的文献互助平台,具备全网最快的应助速度,最高的求助完成率。 对每一个文献求助,科研通都将尽心尽力,给求助人一个满意的交代。
实时播报
隐形曼青应助Jennie369采纳,获得10
2秒前
awa606发布了新的文献求助10
3秒前
卡卡发布了新的文献求助10
3秒前
cling完成签到 ,获得积分10
6秒前
研友_nq2AjZ完成签到,获得积分10
6秒前
molihuakai应助卡卡采纳,获得10
7秒前
大模型应助fnx采纳,获得10
11秒前
英俊的未来完成签到 ,获得积分10
11秒前
877633629完成签到 ,获得积分10
12秒前
OK应助轻松的寒松采纳,获得200
15秒前
16秒前
16秒前
小二郎应助科研通管家采纳,获得10
16秒前
16秒前
所所应助科研通管家采纳,获得10
16秒前
慕青应助科研通管家采纳,获得10
16秒前
ding应助科研通管家采纳,获得10
16秒前
16秒前
16秒前
loii举报sunny求助涉嫌违规
17秒前
17秒前
Jennie369发布了新的文献求助10
21秒前
yyy完成签到,获得积分10
23秒前
yimax完成签到 ,获得积分10
24秒前
tt完成签到 ,获得积分10
26秒前
CipherSage应助kk采纳,获得10
27秒前
温暖马里奥完成签到,获得积分20
28秒前
沐儿发布了新的文献求助10
34秒前
loii给sunny的求助进行了留言
36秒前
39秒前
39秒前
青木发布了新的文献求助10
44秒前
osteoclast发布了新的文献求助10
45秒前
newplayer完成签到,获得积分10
45秒前
47秒前
烟花应助Rita采纳,获得10
48秒前
Jennie369完成签到,获得积分10
49秒前
所所应助Dana采纳,获得10
50秒前
NexusExplorer应助awa606采纳,获得10
55秒前
56秒前
高分求助中
Principles of Economics, 11th Edition 10000
University Physics with Modern Physics, 16th edition 10000
(应助此贴封号)【重要!!请各用户(尤其是新用户)详细阅读】【科研通的精品贴汇总】 10000
Arthritis and Related Conditions, An Issue of Orthopedic Clinics 1000
Development of a Bridge Weigh-In-Motion System: A technology to convert the bridge response to the passage of traffic into data on vehicle configurations, speeds, times of travel and weights 1000
ズームレンズの光学設計に関する研究 800
Fundamentals of Pharmaceutical and Biologics Regulations: A Global Perspective, Second Edition 700
热门求助领域 (近24小时)
化学 材料科学 医学 生物 纳米技术 工程类 有机化学 化学工程 生物化学 计算机科学 内科学 物理 复合材料 催化作用 细胞生物学 无机化学 光电子学 物理化学 电极 基因
热门帖子
关注 科研通微信公众号,转发送积分 7289423
求助须知:如何正确求助?哪些是违规求助? 8908914
关于积分的说明 18856106
捐赠科研通 6957661
什么是DOI,文献DOI怎么找? 3209040
关于科研通互助平台的介绍 2378780
邀请新用户注册赠送积分活动 2184798