更新于：2024-05-01

SMARCA4

更新于：2024-05-01

基本信息

别名

ATP-dependent helicase SMARCA4、BAF190、BAF190A

+ [26]

简介

Involved in transcriptional activation and repression of select genes by chromatin remodeling (alteration of DNA-nucleosome topology). Component of SWI/SNF chromatin remodeling complexes that carry out key enzymatic activities, changing chromatin structure by altering DNA-histone contacts within a nucleosome in an ATP-dependent manner. Component of the CREST-BRG1 complex, a multiprotein complex that regulates promoter activation by orchestrating the calcium-dependent release of a repressor complex and the recruitment of an activator complex. In resting neurons, transcription of the c-FOS promoter is inhibited by SMARCA4-dependent recruitment of a phospho-RB1-HDAC repressor complex. Upon calcium influx, RB1 is dephosphorylated by calcineurin, which leads to release of the repressor complex. At the same time, there is increased recruitment of CREBBP to the promoter by a CREST-dependent mechanism, which leads to transcriptional activation. The CREST-BRG1 complex also binds to the NR2B promoter, and activity-dependent induction of NR2B expression involves the release of HDAC1 and recruitment of CREBBP. Belongs to the neural progenitors-specific chromatin remodeling complex (npBAF complex) and the neuron-specific chromatin remodeling complex (nBAF complex). During neural development, a switch from a stem/progenitor to a postmitotic chromatin remodeling mechanism occurs as neurons exit the cell cycle and become committed to their adult state. The transition from proliferating neural stem/progenitor cells to postmitotic neurons requires a switch in subunit composition of the npBAF and nBAF complexes. As neural progenitors exit mitosis and differentiate into neurons, npBAF complexes which contain ACTL6A/BAF53A and PHF10/BAF45A, are exchanged for homologous alternative ACTL6B/BAF53B and DPF1/BAF45B or DPF3/BAF45C subunits in neuron-specific complexes (nBAF). The npBAF complex is essential for the self-renewal/proliferative capacity of the multipotent neural stem cells. The nBAF complex along with CREST plays a role regulating the activity of genes essential for dendrite growth. SMARCA4/BAF190A may promote neural stem cell self-renewal/proliferation by enhancing Notch-dependent proliferative signals, while concurrently making the neural stem cell insensitive to SHH-dependent differentiating cues (By similarity). Acts as a corepressor of ZEB1 to regulate E-cadherin transcription and is required for induction of epithelial-mesenchymal transition (EMT) by ZEB1. Binds via DLX1 to enhancers located in the intergenic region between DLX5 and DLX6 and this binding is stabilized by the long non-coding RNA (lncRNA) Evf2 (By similarity). Binds to RNA in a promiscuous manner (By similarity). Binding to RNAs including lncRNA Evf2 leads to inhibition of SMARCA4 ATPase and chromatin remodeling activities (By similarity). In brown adipose tissue, involved in the regulation of thermogenic genes expression (By similarity).

关联

项与 SMARCA4 相关的药物

FHD-286

靶点

SMARCA2 x SMARCA4

作用机制

SMARCA2 抑制剂 [+1]

在研机构

Foghorn Therapeutics, Inc.

原研机构

Foghorn Therapeutics, Inc.

在研适应症

难治性急性髓细胞白血病 [+5]

非在研适应症

葡萄膜黑色素瘤

最高研发阶段临床1期

首次获批国家/地区-

首次获批日期1800-01-20

FHD-909

靶点-

作用机制

SMARCA2 抑制剂 [+1]

在研机构

Foghorn Therapeutics, Inc.

原研机构

Foghorn Therapeutics, Inc.

在研适应症

非小细胞肺癌 [+1]

非在研适应症-

最高研发阶段临床前

首次获批国家/地区-

首次获批日期1800-01-20

SMARCA2/4 Program(Proteovant Therapeutics)

靶点

SMARCA2 x SMARCA4

作用机制

SMARCA2 抑制剂 [+1]

在研机构

Proteovant Therapeutics, Inc.

原研机构

Proteovant Therapeutics, Inc.

在研适应症

肿瘤

非在研适应症-

最高研发阶段药物发现

首次获批国家/地区-

首次获批日期1800-01-20

项与 SMARCA4 相关的临床试验

NCT04891757 / Recruiting临床1期

A Phase 1, Multicenter, Open-Label, Dose Escalation Study to Assess the Safety, Tolerability, Pharmacokinetics, Pharmacodynamics, and Clinical Activity of Orally Administered FHD-286, as Monotherapy or Combination Therapy, in Subjects With Advanced Hematologic Malignancies

This Phase 1, multicenter, open-label, dose escalation study is designed to assess the safety, tolerability, pharmacokinetics (PK), pharmacodynamics (PD), and preliminary clinical activity of FHD-286 administered orally as monotherapy or combination therapy, in subjects with advanced hematologic malignancies.

开始日期2021-06-14

申办/合作机构

Foghorn Therapeutics, Inc.

NCT04879017 / Terminated临床1期

A Phase 1, Multicenter, Open-Label, Dose Escalation and Expansion Study to Assess the Safety, Tolerability, Pharmacokinetics, Pharmacodynamics, and Clinical Activity of Orally Administered FHD-286 in Subjects With Metastatic Uveal Melanoma

This Phase 1, multicenter, open-label, dose escalation and expansion study is designed to assess the safety, tolerability, pharmacokinetics (PK), pharmacodynamics (PD), and preliminary clinical activity of FHD-286 oral monotherapy in subjects with metastatic Uveal Melanoma (UM).

开始日期2021-05-11

申办/合作机构

Foghorn Therapeutics, Inc.

100 项与 SMARCA4 相关的临床结果

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100 项与 SMARCA4 相关的转化医学

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0 项与 SMARCA4 相关的专利（医药）

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2,118

项与 SMARCA4 相关的文献（医药）

2024-12-31·Human vaccines & immunotherapeutics

Exploration of genetic characterization in hyperprogressive disease after immunotherapy retreatment in a patient with LCNEC: A case report.

Article

作者: Yao Zhang ; Jiayao Yang ; Tianyu Shao ; Jialu Chen ; Qijin Shu ; Liumei Shou

Immune checkpoint inhibitors (ICIs) have emerged as a promising therapeutic option for large cell neuroendocrine carcinoma (LCNEC). However, various studies have suggested a potential risk of hyperprogressive disease (HPD) in patients receiving ICI, which might be associated with gene alterations. Here, this is the first report on an unknown primary LCNEC patient who had achieved a long-term response from ICI treatment (atezolizumab), but developed HPD after tumor progression due to receiving another ICI agent (serplulimab). The mutation region of FAT4, SMARCA4, CYLD, CTNNB1, and KIT was altered prior to serplulimab treatment compared to before atezolizumab treatment. This case suggested a potential association between these mutated genes and HPD. Patients with the aforementioned genes should caution when selecting ICI treatment. These findings required further confirmation in a larger study cohort.

2024-02-23·Medicine

Efficacy of immune checkpoint inhibitors in SMARCA4-deficient and TP53 mutant undifferentiated lung cancer.

Article

作者: Jianxin Chen ; Qinhong Zheng ; Junhui Wang ; Xueli Zhang ; Yingguo Lv

The present study was conducted to characterize the clinicopathologic characteristics, immunohistochemical staining results, and immune checkpoint inhibitors (ICIs) efficacy in patients with SMARCA4-deficient/TP53 mutant lung cancer. Patients diagnosed with advanced or metastatic undifferentiated lung cancer harboring SMARCA4-deficient and TP53 mutations, however, without targetable sensitive mutations were retrieved from the electronic medical record system. Descriptive statistics were used to describe the baseline characteristics and clinical features including age, gender, eastern cooperative oncology group performance status, disease stage, smoking status, chief complaint, site of the primary mass, tumor size, gross type, symptoms, local invasion, and metastatic sizes. Immunological markers and potential drive genes were detected by immunohistochemical staining and next generation sequencing. Efficacy and safety profile of ICIs in included patients was evaluated with progression-free survival and overall survival. Between January 2019 and September 2022, there were 4 patients included within the inclusion criteria in the present study. Biomarkers including CK, CK7, and integrase interactor 1 were detected positive, however, other immunological markers including CK20, CD56, P63, P40, NapsinA, TTF-1, CgA, Syn, BRG1, or PD-L1 were detected negative among them. Results of next generation sequencing panel were failed to discover any targetable sensitive mutations. A total of 4 mutation types of TP53, including p.C141Y, p.S240G, p.E339X (terminator acquired), and p.L130F detected for the patients, respectively. Microsatellite stability status, as well as low tumor mutation burden was identified among all the patients. Median progression-free survival for ICIs as first line treatment and median overall survival were 3.25 months (range from 1.3 to 6.8 months), and 6.0 months (range from 2.7 to 9.6 months), respectively. Our results indicated that advanced lung cancer patients harboring co-occurring SMARCA4-deficient/TP53 mutations might respond to ICIs treatment, though within negative programmed cell death-ligand 1 expression or low tumor mutation burden. However, hyperprogressive disease by ICIs may also happen for such patients. The mutation types of TP53 might play a role during the exposure of ICIs, however, need further identification in basic experiments.

2024-02-21·The Journal of neuroscience : the official journal of the Society for Neuroscience

SMARCA4 loss and mutated β-catenin induce proliferative lesions in the murine embryonic cerebellum.

Article

作者: Carolin Göbel ; Melanie Schoof ; Dörthe Holdhof ; Michael Spohn ; Ulrich Schüller

Almost all medulloblastomas (MB) of the Wingless/Int-1 (WNT) type are characterized by hotspot mutations in CTNNB1, and mouse models have convincingly demonstrated the tumor-initiating role of these mutations. Additional alterations in SMARCA4 are detected in around 20% of WNT MB, but their functional role is mostly unknown. We therefore amended previously described Blbp-cre::Ctnnb1(ex3)^fl/wt mice by the introduction of floxed Smarca4 alleles. Unexpectedly, mutated and thereby stabilized β-catenin on its own induced severe developmental phenotypes in male and female Blbp-cre::Ctnnb1(ex3)^fl/wt mice in our hands, including a thinned cerebral cortex, hydrocephalus, missing cerebellar layering, and cell accumulations in the brain stem and cerebellum. An additional loss of SMARCA4 even resulted in prenatal death for most mice. Respective Blbp-cre::Ctnnb1(ex3)^fl/wt::Smarca4^fl/rec mutants (male and female) developed large proliferative lesions in the cerebellum evolving from E13.5 to E16.5. Histological and molecular analysis of these lesions by DNA methylation profiling and single-cell RNA sequencing suggested an origin in early undifferentiated SOX2-positive cerebellar progenitors. Furthermore, upregulated WNT signaling, altered actin/cytoskeleton organization, and reduced neuronal differentiation were evident in mutant cells. In vitro, cells harboring alterations in both Ctnnb1 and Smarca4 were negatively selected and did not show tumorigenic potential after transplantation in adult female recipient mice. However, in cerebellar explant cultures, mutant cells displayed significantly increased proliferation, suggesting an important role of the embryonic microenvironment in the development of lesions. Altogether, these results represent an important first step towards the unravelling of tumorigenic mechanisms induced by aberrant WNT signaling and SMARCA4 deficiency.Significance Statement Our study shows cooperative effects between activated Wingless/Int-1 (WNT) signaling induced by a stabilizing β-catenin mutation and a loss of chromatin remodeler SMARCA4 in driving the development of highly proliferative cerebellar lesions. This observation could have important implications for WNT medulloblastoma patients, who are frequently affected by both alterations with the functional role of SMARCA4 mutations in tumorigenesis not deciphered so far. Additionally, this work highlights divergence of mouse phenotypes after brain-specific activation of WNT signaling from previously published studies and proposes potential reasons for varying recombination using the brain lipid binding protein (Blbp)-cre mouse strain.

项与 SMARCA4 相关的新闻（医药）

2024-04-02

·生物探索

Nature | 让癌细胞变回正常细胞！清除这个蛋白，有望逆转“无药可用”的癌症

引言虽然癌基因可以被小分子抑制，但肿瘤抑制蛋白的丢失更为常见，并且存在问题，因为肿瘤抑制蛋白不再存在靶向。值得注意的例子包括SMARCB1 突变癌症，这是由SWI/SNF（也称为 BAF）染色质重塑复合物亚基失活驱动的高度致命的恶性肿瘤。2024年3月27日，圣裘德儿童研究医院Charles W. M. Roberts及哈佛医学院Eric S. Fischer共同通讯在Nature 在线发表题为“Targeting DCAF5 suppresses SMARCB1-mutant cancer by stabilizing SWI/SNF”的研究论文，该研究表明靶向DCAF5通过稳定SWI/SNF抑制SMARCB1突变癌症。为了深入了解SMARCB1突变的后果并识别漏洞，研究人员将14个SMARCB1突变细胞系用于近全基因组CRISPR筛选，作为癌症依赖图谱项目的一部分。该研究报道了很少被研究的基因 DDB1-CUL4相关因子5 (DCAF5)是SMARCB1突变癌症存活所必需的。该研究发现DCAF5对SWI/SNF复合物具有质量控制功能，并在没有SMARCB1的情况下促进不完全组装的SWI/SNF复合物的降解。在DCAF5耗尽后，SMARCB1缺陷的SWI/SNF复合物重新积累，结合靶位点，并将SWI/SNF介导的基因表达恢复到足以逆转癌症状态的水平，包括在体内。因此，癌症的发生不是由于SMARCB1功能本身的丧失，而是由于DCAF5介导的SWI/SNF复合物的降解。这些数据表明，针对泛素介导的质量控制因子的治疗可能有效地逆转一些由肿瘤抑制复合物破坏驱动的恶性状态。SWI/SNF染色质重塑复合物水解ATP，动员核小体在增强子和启动子处调节DNA可及性和基因表达。核心亚基SMARCB1在分裂过程中对增强子功能和细胞记忆的控制至关重要，最近的结构研究表明，它作为一个锚点结合到核小体酸性补丁上，在那里它为SWI/SNF重塑活性提供了有利条件。编码SWI/SNF亚基的基因在近25%的癌症患者中发生突变。SWI/SNF亚基SMARCB1失活发生在几种侵袭性癌症类型中，包括横纹肌样肿瘤(RTs)和肉瘤。SMARCB1是一种真正的肿瘤抑制因子，因为种系突变易导致癌症，在小鼠中缺失SMARCB1会导致所有小鼠的快速发病癌症。RTs具有简单的二倍体基因组，SMARCB1的缺失通常是唯一确定的驱动突变。由于SMARCB1肿瘤抑制蛋白缺失，唯一的驱动突变不能直接靶向治疗。因此，识别SMARCB1突变细胞特有的遗传脆弱性有可能深入了解SMARCB1缺失促进癌症的机制，并为治疗方法提供信息。癌症依赖图谱项目(DepMap)是一个大规模的合作项目，利用数百种癌细胞系系统地识别遗传依赖性、小分子敏感性和识别预测它们的生物标志物。为了寻找SMARCB1突变癌症的遗传脆弱性，研究人员向DepMap提供了14个SMARCB1突变的RT系，用于近全基因组CRISPR-Cas9功能缺失筛查。RTs中DCAF5丢失的机制模型（Credit: Nature）该研究确定了一种作用不同的合成致死关系。而不是产生毒性，靶向灭活质量控制因子实质上恢复多亚基蛋白复合物的功能，否则在失去肿瘤抑制亚基后降解。之前已经证明，SMARCB1缺失通过损害高增殖祖细胞中增强子的激活来驱动癌症，从而阻断分化并使其持续增殖。从机制上讲，DCAF5的失活可恢复大量SWI/SNF功能，恢复分化并逆转癌症表型。研究发现，在SMARCB1缺失的情况下，DCAF5通过促进SWI/SNF亚基的降解，对SWI/SNF复合物具有质量控制功能。之前证明，SMARCB1的缺失比SMARCA4或ARID1A的缺失导致SWI/SNF复合物更大的不稳定，这可能解释了与其他SWI/SNF突变型癌症相比，SMARCB1突变型癌症对DCAF5的优先依赖性。总的来说，该研究揭示了一种机制，该机制是多蛋白复合物质量控制的基础，并构成了肿瘤抑制基因突变失活驱动的癌症中可靶向的合成致命易感性。原文链接https://www.nature.com/articles/s41586-024-07250-1责编|探索君排版|探索君文章来源|“iNature”End往期精选围观一文读透细胞死亡(Cell Death) | 24年Cell重磅综述（长文收藏版）热文Nature | 破除传统：为何我们需要重新思考肿瘤的命名方式热文Nature | 2024年值得关注的七项技术热文Nature | 自身免疫性疾病能被治愈吗？科学家们终于看到了希望热文CRISPR技术进化史 | 24年Cell综述

基因疗法

2024-03-26

·BioSpace

Foghorn to Host Conference Call and Webcast on Pipeline of Potential First-in-Class Medicines in Conjunction with the 2024 AACR Annual Meeting

Company management will review key pipeline programs, including an update on FHD-286 for AML, new preclinical data for the BRM selective inhibitor FHD-909 and for its selective CBP and EP300 degrader programs Conference call and webcast on April 9th at 5 p.m. ET / 2 p.m. PT CAMBRIDGE, Mass., March 26, 2024 (GLOBE NEWSWIRE) -- March 26, 2024 -- Foghorn® Therapeutics Inc. (Nasdaq: FHTX), a clinical-stage biotechnology company pioneering a new class of medicines that treat serious diseases by correcting abnormal gene expression, today announced plans to host a conference call and webcast on April 9th at 5 p.m. ET / 2 p.m. PT. Foghorn management will review key programs in its pipeline, including FHD-286 for acute myelogenous leukemia (AML), and new preclinical data being presented at the 2024 American Association for Cancer Research (AACR) Annual Meeting for potential first-in-class medicines including FHD-909, a BRM (SMARCA2) selective inhibitor, and for the selective CBP and selective EP300 degrader programs. Conference Call Details Tuesday, April 9, at 5 p.m. ET / 2 p.m. PT Toll Free: 1-877-704-4453 International: 1-201-389-0920 Conference ID: 13745314 Webcast: Foghorn Events and Presentations About Foghorn Therapeutics Foghorn® Therapeutics is discovering and developing a novel class of medicines targeting genetically determined dependencies within the chromatin regulatory system. Through its proprietary scalable Gene Traffic Control® platform, Foghorn is systematically studying, identifying and validating potential drug targets within the chromatin regulatory system. The Company is developing multiple product candidates in oncology. Visit our website at for more information on the Company, and follow us on X (formerly Twitter) and LinkedIn. About FHD-286 FHD-286 is a highly potent, selective, allosteric, and orally available small-molecule, enzymatic inhibitor of BRG1 (SMARCA4) and BRM (SMARCA2), two highly similar proteins that are the ATPases, or the catalytic engines, of the BAF complex, one of the key regulators within the chromatin regulatory system. In preclinical studies, FHD-286 has shown anti-tumor activity across a broad range of malignancies including both hematologic and solid tumors. About AML Adult acute myeloid leukemia (AML) is a cancer of the blood and bone marrow and the most common type of acute leukemia in adults. AML is a diverse disease associated with multiple genetic mutations. It is diagnosed in about 20,000 people every year in the United States. About FHD-909 FHD-909 (a.k.a. LY4050784) is a highly potent, allosteric and orally available small molecule that selectively inhibits the ATPase activity of BRM (SMARCA2) over its closely related paralog BRG1 (SMARCA4), two proteins that are the catalytic engines across all forms of the BAF complex, one of the key regulators of the chromatin regulatory system. In preclinical studies, tumors with mutations in BRG1 rely on BRM for BAF function. FHD-909 has shown significant anti-tumor activity across multiple BRG1-mutant lung tumor models. Forward-Looking Statements This press release contains “forward-looking statements.” Forward-looking statements include statements regarding the Company’s clinical trials, product candidates and research efforts, including statements relating to FHD-286, FHD-909 and its selective CBP and EP 300 degrader programs, and other statements identified by words such as “could,” “may,” “might,” “will,” “likely,” “anticipates,” “intends,” “plans,” “seeks,” “believes,” “estimates,” “expects,” “continues,” “projects” and similar references to future periods. Forward-looking statements are based on our current expectations and assumptions regarding capital market conditions, our business, the economy and other future conditions. Because forward-looking statements relate to the future, by their nature, they are subject to inherent uncertainties, risks and changes in circumstances that are difficult to predict. As a result, actual results may differ materially from those contemplated by the forward-looking statements. Important factors that could cause actual results to differ materially from those in the forward-looking statements include regional, national or global political, economic, business, competitive, market and regulatory conditions, including risks relating to our clinical trials and other factors set forth under the heading “Risk Factors” in the Company’s Annual Report on Form 10-K for the year ended December 31, 2023, as filed with the Securities and Exchange Commission. Any forward-looking statement made in this press release speaks only as of the date on which it is made. Contacts: Greg Dearborn, Foghorn Therapeutics Inc. (Investors) gdearborn@foghorntx.com Karin Hellsvik, Foghorn Therapeutics Inc. (Investors & Media) khellsvik@foghorntx.com Adam Silverstein, ScientPR (Media) adam@scientpr.com Peter Kelleher, LifeSci Advisors (Investors) pkelleher@lifesciadvisors.com

AACR会议

2024-03-19

·Pharmaceutical Technology

Asieris showcases Phase III win in treating precancerous cervical lesions

According to GlobalData, there will be 123,846 cervical cancer cases in the eight major markets (UK, US, France, Germany, Spain, Italy, Japan, and urban China) by 2030. Credit: Ground Picture via Shutterstock. Asieris Pharmaceuticals has announced positive data indicating the Phase III trial of its cold light photodynamic drug-device combination Cevira (APL-1702) achieved its primary endpoint in participants with cervical high-grade squamous intraepithelial lesions (HSIL). HSIL are precancerous lesions linked to human papillomavirus (HPV) that can lead to cervical cancer. The results were presented at the 2024 Society of Gynecologic Oncology (SGO) Annual Meeting in San Diego, US, which was held 16-18 March. Cevira also demonstrated a tolerable safety profile. The therapy stimulates the body’s production of the photosensitiser protoporphyrin IX (PPIX), which selectively accumulates in tumour tissue, and upon exposure to specific wavelengths, triggers tumour cell apoptosis. The primary endpoint, which evaluated the response rate six months after administering Cevira, showed a statistically significant improvement of 89.4% compared to the placebo group. See Also: Dr. Reddy’s Laboratories files patent for 6-substituted pyridazine compounds for treating diseases dependent on SMARCA2/SMARCA4 The drug also showed an improved clearance rate of high-risk HPV16 and/or HPV18, with a 103.9% increase in the Cevira group compared to placebo. Cevira was developed through Phase I and II clinical trials by Norway-based Photocure ASA, with Asieris gaining commercialisation rights in July 2019. The Phase III trial (NCT04484415) enrolled 402 HSIL patients, defining the primary endpoint of response as the conversion of cervical epithelial tissue pathology to normal, or the conversion to low-grade squamous intraepithelial lesion (LSIL) while achieving baseline HPV clearance. Long-lasting infection with certain types of HPV, a common sexually transmitted infection, is the main cause of cervical cancer. If left untreated, HPV can be linked to 95% of cervical cancer cases, according to the World Health Organization. The China-based biotech now plans to submit a new drug application for Cevira in Q2 2024, according to Asieris’ chief development officer Linda Wu. According to a report on GlobalData’s Pharma Intelligence Center, the number of cervical cancer cases in the eight major markets (UK, US, France, Germany, Spain, Italy, Japan, and urban China) will reach 123,846 by 2030. GlobalData is the parent company of Clinical Trials Arena. In the announcement accompanying the data, Linda Wu said: “The study not only demonstrates remarkable efficacy but also exhibits a favourable safety profile, offering a new powerful artillery for the national cervical cancer prevention and control system. “Additionally, we are making significant progress in product development overseas, aiming to bring this innovative treatment to more patients as soon as possible.” The company also has other cancer candidates in the pipeline. Earlier this year, a Phase II trial of its repurposed antibiotic drug APL-1202 achieved its primary endpoint in participants with muscular invasive bladder cancer (MIBC). The drug is already approved to treat oesophagal squamous cell carcinoma in China and is also being reviewed by the US Food and Drug Administration to treat the same type of cancer.