更新于：2024-11-01

CEBPB

更新于：2024-11-01

基本信息

别名

C/EBP beta、C/EBP-beta、CCAAT enhancer binding protein beta

+ [13]

简介

Important transcription factor regulating the expression of genes involved in immune and inflammatory responses (PubMed:1741402, PubMed:9374525, PubMed:12048245, PubMed:18647749). Also plays a significant role in adipogenesis, as well as in the gluconeogenic pathway, liver regeneration, and hematopoiesis. The consensus recognition site is 5'-T[TG]NNGNAA[TG]-3'. Its functional capacity is governed by protein interactions and post-translational protein modifications. During early embryogenesis, plays essential and redundant roles with CEBPA. Has a promitotic effect on many cell types such as hepatocytes and adipocytes but has an antiproliferative effect on T-cells by repressing MYC expression, facilitating differentiation along the T-helper 2 lineage. Binds to regulatory regions of several acute-phase and cytokines genes and plays a role in the regulation of acute-phase reaction and inflammation. Also plays a role in intracellular bacteria killing (By similarity). During adipogenesis, is rapidly expressed and, after activation by phosphorylation, induces CEBPA and PPARG, which turn on the series of adipocyte genes that give rise to the adipocyte phenotype. The delayed transactivation of the CEBPA and PPARG genes by CEBPB appears necessary to allow mitotic clonal expansion and thereby progression of terminal differentiation (PubMed:20829347). Essential for female reproduction because of a critical role in ovarian follicle development (By similarity). Restricts osteoclastogenesis: together with NFE2L1; represses expression of DSPP during odontoblast differentiation (By similarity). Acts as a dominant negative through heterodimerization with isoform 2 (PubMed:11741938). Promotes osteoblast differentiation and osteoclastogenesis (By similarity). Essential for gene expression induction in activated macrophages. Plays a major role in immune responses such as CD4(+) T-cell response, granuloma formation and endotoxin shock. Not essential for intracellular bacteria killing.

关联

项与 CEBPB 相关的药物

Lucicebtide

靶点

CEBPB

作用机制

CEBPB抑制剂

在研机构

Sapience Therapeutics, Inc.初创企业

原研机构

Sapience Therapeutics, Inc.初创企业

在研适应症

晚期恶性实体瘤 [+6]

非在研适应症-

最高研发阶段临床1/2期

首次获批国家/地区-

首次获批日期1800-01-20

KMU-3

靶点

CEBPB x FASN x PPARα/γ x STMN3

作用机制

CEBPB抑制剂 [+3]

在研机构

Keimyung University

原研机构

Keimyung University

在研适应症

肥胖

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

exoASO-C/EBPβ

靶点

CEBPB

作用机制

CEBPB modulators

在研机构-

原研机构

Codiak BioSciences, Inc.

在研适应症-

非在研适应症

膀胱癌 [+3]

最高研发阶段终止

首次获批国家/地区-

首次获批日期1800-01-20

项与 CEBPB 相关的临床试验

NCT04478279 / Active, not recruiting临床1/2期

A Phase 1-2 Dose-escalation and Expansion Study of ST101 in Patients With Advanced Unresectable and Metastatic Solid Tumors

This is an open-label, two-part, phase 1-2 dose-finding study designed to determine the safety, tolerability, PK, PD, and proof-of-concept efficacy of ST101 administered IV in patients with advanced solid tumors. The study consists of two phases: a phase 1 dose escalation/regimen exploration phase and a phase 2 expansion phase.

开始日期2020-07-01

申办/合作机构

Sapience Therapeutics, Inc.初创企业

100 项与 CEBPB 相关的临床结果

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100 项与 CEBPB 相关的转化医学

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0 项与 CEBPB 相关的专利（医药）

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2,604

项与 CEBPB 相关的文献（医药）

2025-01-01·Biochimica et Biophysica Acta (BBA) - Molecular Basis of Disease

S100A4 mediates the accumulation and functions of myeloid-derived suppressor cells via GP130/JAK2/STAT3 signaling in acute myeloid leukemia

Article

作者: Qi, Xiaolan ; Bai, Jingdi ; Guo, Pengxiang ; Dai, Yun ; Wu, ChangXue ; Hong, Wei ; Zeng, Zhu ; Zhang, Ting ; Xie, Xin ; Zhang, Jian ; Duan, Juanjuan ; Wang, Chanjuan ; Liang, Xinming ; Yu, Wenfeng ; Fu, Wenli ; Fan, Daogui ; Peng, Yuhui ; Zhou, Jing ; Li, Yi ; Zeng, Hongmei ; Chen, Pingping ; He, Yan ; Zhang, Qifang ; Bai, Hua

BACKGROUNDAcute myeloid leukemia (AML) is an immunosuppressive hematologic malignancy with a poor prognosis. An immunosuppressive microenvironment blunts AML therapy. However, the prognostic and therapeutic roles of the factors that mediate immunosuppression in AML remain elusive.METHODSS100 calcium-binding protein A4 (S100A4) was identified as an immunosuppression-mediating factor by analyzing The Cancer Genome Atlas AML project (TCGA-LAML) transcriptome data and data from AML-bearing mice and AML patients. The S100A4-mediated signaling pathway in myeloid-derived suppressor cells (MDSCs) was evaluated.RESULTSElevated S100A4 expression was positively associated with worse survival of AML patients, MDSCs, macrophages and immune checkpoints. S100A4 silencing downregulated the expression levels of MDSC-associated CD14, CCR2 and CCL2, reduced MDSC expansion and impaired MDSC-mediated inhibition of T cell activation and proliferation. S100A4-based prognostic signature (SPS) was an independent risk factor for AML patients. The high-risk group based on SPS was not only associated with adverse survival, MDSCs and macrophages and immune checkpoints but also insensitive to 25 chemotherapy drugs. It was also found that CCAAT enhancer binding protein beta (CEBPB) mediated S100A4 transcription. CEBPB silencing downregulated the expression levels of MDSC-associated CD14, CCR2 and CCL2. Mechanistically, S100A4 activated GP130/JAK2/STAT3 signaling in MDSCs by interacting with the cytokine-binding domain of GP130. Moreover, S100A4 mediated MDSC expansion through JAK2/STAT3 signaling.CONCLUSIONThis study uncovers the critical role of S100A4 in MDSC accumulation, and S100A4-based prognostic signature may guide chemotherapy sensitivity in patients with AML.

2024-12-01·JOR spine

Identifying critical modules and biomarkers of intervertebral disc degeneration by using weighted gene co-expression network.

Article

作者: Liu, Zongchao ; Xie, Xianping ; Mei, Yongliang ; Lv, Jiale ; Guo, Daru ; Cheng, Kang ; Liu, Tao ; Gao, Silong ; Zhou, Daqian ; Cai, Weiye

BackgroundIntervertebral disc degeneration (IVDD) is an age-related orthopedic degenerative disease characterized by recurrent episodes of lower back pain, the pathogenesis of which is not fully understood. This study aimed to identify key biomarkers of IVDD and its causes.MethodsWe acquired three gene expression profiles from the Gene Expression Omnibus (GEO) database, GSE56081, GSE124272, and GSE153761, and used limma fast differential analysis to identify differentially expressed genes (DEGs) between normal and IVDD samples after removing batch effects. We applied weighted gene co-expression network (WGCNA) to identify the key modular genes in GSE124272 and intersected these with DEGs. Next, A protein-protein interaction network (PPI) was constructed, and Cytoscape was used to identify the Top 10 hub genes. Functional enrichment analyses were performed using gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) databases. Three key genes were validated using Western Blot (WB) and qRT-PCR. Additionally, we predicted miRNAs involved in hub gene co-regulation and analyzed miRNA microarray data from GSE116726 to identify four differentially expressed miRNAs.ResultsWe identified 10 hub genes using bioinformatics analysis, gene function enrichment analysis revealed that they were primarily enriched in pathways, such as the TNF signaling pathway. We chose JUNB, SOCS3, and CEBPB as hub genes and used WB and qRT-PCR to confirm their expression. All three genes were overexpressed in the IVDD model group compared to the control group. Furthermore, we identified four miRNAs involved in the co-regulation of the hub genes using miRNet prediction: mir-191-5p, mir-20a-5p, mir-155-5p, and mir-124-3p. Using limma difference analysis, we discovered that mir-191-5p, mir-20a-5p, and mir-155-5p were all down-regulated and expressed in IVDD samples, but mir-124-3p showed no significant change.ConclusionJUNB, SOCS3, and CEBPB were identified as key genes in IVDD, regulated by specific miRNAs, providing potential biomarkers for early diagnosis and therapeutic targets.

2024-11-01·Drug Resistance Updates

CBX4 counteracts cellular senescence to desensitize gastric cancer cells to chemotherapy by inducing YAP1 SUMOylation

Article

作者: Fang, Yuan ; Shen, Haoyang ; Ma, Pei ; Shao, Jun ; Wu, Xi ; Song, Yu ; Zhang, Jingxin ; Hu, Tong ; Gu, Yunru ; Xia, Yang ; Shu, Yongqian ; Xu, Yangyue ; Xu, Tingting

AIMSAs our comprehension of the intricate relationship between cellular senescence and tumor biology continues to evolve, the therapeutic potential of cellular senescence is gaining increasing recognition. Here, we identify chromobox 4 (CBX4), a Small Ubiquitin-related Modifier (SUMO) E3 ligase, as an antagonist of cellular senescence and elucidate a novel mechanism by which CBX4 promotes drug resistance and malignant progression of gastric cancer (GC).METHODSIn vitro and in vivo models were conducted to investigate the manifestation and impact of CBX4 on cellular senescence and chemoresistance. High-throughput sequencing, chromatin immunoprecipitation, and co-immunoprecipitation techniques were utilized to identify the upstream regulators and downstream effectors associated with CBX4, revealing its intricate regulatory network.RESULTSCBX4 diminishes the sensitivity of GC cells to cellular senescence, facilitating chemoresistance and GC development by deactivating the senescence-related Hippo pathway. Mechanistically, low-dose cisplatin transcriptionally downregulates CBX4 through CEBPB. In addition, CBX4 preserves the stability and cytoplasm-nuclear transport of YAP1, the key player of Hippo pathway, by inducing SUMO1 modification at K97 and K280, which competitively inhibits YAP1-S127 phosphorylation.CONCLUSIONSOur study highlights the anti-senescence role of CBX4 and suggests that CBX4 inhibition in combination with low-dose cisplatin has the potential to overcome chemoresistance and effectively restrict GC progression.

项与 CEBPB 相关的新闻（医药）

2024-10-23

·兰卫医学

【学术前沿】单细胞结合空间转录组的研究思路和案例分享——肿瘤免疫研究领域（下）

学术前沿单细胞结合空间转录组的研究思路和案例分享 ——肿瘤免疫研究领域（下） 01 引言单细胞转录组测序是在单个细胞水平进行高通量转录组测序的一项技术，其能有效解决细胞异质性以及之前bulk RNA-seq被掩盖的种种问题。随着该技术在分辨率和通量方面的不断优化，研究者从异质性样本中分析细胞类型特异性基因调控网络的能力也相对提高，但是在细胞的空间位置水平尚有欠缺。空间转录组技术于2020年被《自然》杂志评为年度技术，可以解析时间和空间维度上单个细胞的基因表达模式，以及细胞类群的空间位置关系及生物学特征。其原理是将空间条形码寡核苷酸引物固定在载玻片上，然后将组织贴于载玻片实现组织内转录组序列的捕获与检测。随着10x Genomics的空间Visium技术的登场和不断更新加强，单细胞联合空间转录组的研究如火如荼的开展，遍布了遗传、发育、肿瘤、免疫等多个生物科研和医学热门领域。一、研究目的 1.某肿瘤中，整体的细胞图谱、空间图谱及细胞间机制探索。 2.某肿瘤中，不同进展期（病变期）、不同亚型、特殊基因表达或原发灶与转移灶样本之间差异机制探索。 3.某肿瘤中，肿瘤对治疗方案的疗效应答中的差异机制探索。二、样本选择 1. 某癌种中，根据其样本类型的特殊性，选择一定数量的样本，包括新鲜组织、冰冻组织或石蜡样本。 2. 某癌种中，根据原发灶和转移灶、免疫类型（浸润型、沙漠型、排斥型）、基因表达（阴/阳）或不同病理亚型的分组取样。 3. 某癌种中，根据PD1免疫药物治疗/靶向药物治疗/常规放化疗等治疗药物，新辅助、转化治疗等方案，选取应答/无应答、治疗前/治疗后的样本分组取样检测。三、研究方法 1.主要研究方法：主要应用在发现探索阶段的方法,一般包括流式细胞技术(Facs)、单细胞组学（scRNA-seq）、空间转录组(visium HD)、多重免疫荧光染色(mIF)、探针原位杂交（Xenium）等； 2.其他辅助方法：辅助研究方法应用在机制验证方面，会根据验证模型的不同水平，比如细胞水平、动物模型、人源组织、类器官、网络数据库等等，对应各种生物检测分析方法并没有固定的思路。四、分析思路 1.单细胞图谱：细胞类型的空间分布特征，亚群的图谱分类； 2.空间图谱绘制：细胞类型的空间分布特征，亚群的定位； 3.各个亚群细胞中的特征，寻找对比差异显著的细胞亚群，从剖析细胞/基因功能空间动态变化、空间细胞分化规律（拟时序）去分析细胞发生的机制和可能作用； 4.各类细胞亚群的相关性，通过细胞通讯、ST定位以及IHC或mIF等图像直观证明细胞亚群间特异的互动关系； 5.实验验证靶点和机制：细胞水平、类器官水平、动物模型水平做敲除干预治疗等验证。五、文献分享案例1 《单细胞和空间转录组分析揭示了肝转移性结直肠癌的细胞异质性》发表期刊：Cell，影响因子：11.5 研究背景：结直肠癌(CRC)是世界上第三大最常见的恶性肿瘤，而转移性 CRC 的生存率很低。CRC转移过程是一个多步骤的过程，包含了癌细胞和基质细胞之间的交流通过分泌细胞因子、生长因子和蛋白酶来促进转移性扩散，从而重塑肿瘤微环境。TME 的细胞组成非常复杂，包括多种成纤维细胞和免疫细胞，它们在癌症逃避、转移和治疗反应中发挥着重要作用。癌症相关成纤维细胞（CAF）是许多类型恶性肿瘤（包括 CRC、乳腺癌和胰腺癌）的主要基质细胞成分。为了全面绘制结直肠癌和匹配的肝转移的细胞景观，研究人员使用scRNA-seq结合空间转录组(ST)和免疫组织化学(IHC)染色以及流式细胞术生成了高分辨率的细胞图谱。检测技术组合：流式细胞术、单细胞转录组、空间转录组样本类型：1. 6例CRC患者的27份样本，包括原发性结直肠癌(CC)、邻近正常结直肠粘膜(CN)、肝转移(LM)、邻近正常肝组织(LN)和外周血(PB)五种组织类型用于单细胞转录组检测。 2. 6例CRC患者，包含4例CRC原发性肿瘤（C1至C4）和2例肝转移性肿瘤（L1和L2）采用空间转录组。主要结果： 1.根据免疫和非免疫细胞群，分别展示了CRC原发肿瘤和CRC肝转移性肿瘤的单细胞转录组图基本分类，以及原发和转移的差异。 Fig.1.CRC原发及肝转移中的全球细胞景观 2.CRC原发性肿瘤和CRC源性肝转移性肿瘤的空间分布在ST组织中鉴定出B细胞、 T细胞、 NK细胞、浆细胞、髓样细胞、肿瘤细胞、成纤维细胞和内皮细胞。这些细胞簇的比例和分数在每个地区都不同。与C1、C3和C4的肿瘤旁组织相比，肿瘤组织中浆细胞的比率降低。 Fig.2.空间转录组样本的细胞鉴定 3.原发性肿瘤和肝转移性肿瘤之间肿瘤细胞的转录组异质性亚聚类分析揭示了肿瘤细胞的不同分化谱系。在各群中鉴定出簇状细胞的分化标志基因。肿瘤细胞群的异质性表明肿瘤细胞的分化潜力。为了进一步研究不同肿瘤细胞簇的功能通路和转录程序，进行了基因集变异分析（GSVA）和转录因子（TF）分析。结果显示，表明CA2可能是TME中的干细胞亚群。 Fig.3.原发性和转移性肿瘤细胞的转录组特征和异质性 4.TME重塑髓系细胞的组成鉴定出三种髓系细胞：单核细胞/巨噬细胞、树突状细胞和肥大细胞。使用亚聚类分析确定了8个单核细胞/巨噬细胞簇和3个常规DC（cDC）簇，GSVA分析显示，Mac_SPP1亚群参与了与炎症反应相关的通路。拟时序显示Mac_CXCL9 和 Mac_SPP1 亚群均发生终末分化，表明它们是肿瘤激活的Mac亚群。cDC_LAMP3 亚群还表现出高水平的成本刺激分子CD40CD80和CD86 表达，它们是DC成熟的标志物。在LM中，cDC_LAMP3亚群的比例显著增加表明肿瘤细胞对TIME的重塑作用。 Fig.4.骨髓细胞的免疫景观 5.CXCL13T 细胞在肝转移性肿瘤中富集在 T 细胞中，7个CD8 T细胞簇、5个常规CD4 T（cCD4）细胞簇和2个调节T细胞簇被识别。从细胞比例显示，无论是CD8还是CD4的T细胞，LM的CXCL13T细胞子集比例都很高。GSVA分析显示，CD8_CXCL13亚群富含T细胞增殖通路，CD4_CXCL13 亚群富含G细胞+2-M检查点通路。用流式细胞术鉴定了CD69+CD103+CD8+T细胞。CC和LM的CD69+CD103+CD8+T细胞的Ki67表达水平均高于其他CD8+T细胞。然而，来自CN和LN的不同CD8+T细胞亚群的增殖特性几乎相同。 Fig.5.CXCL13+T细胞在肝转移瘤中富集 6.CXCL13 T细胞与CRC患者的良好预后相关在上图验证CD8_CXCL13细胞可能是肿瘤激活的亚群。进一步对CD8_CXCL13子集的特征做深入研究。与其他亚群相比，在CD8_CXCL13亚群中观察到高水平的耗竭标志物，且耗竭表型表明它们的肿瘤反应性。IHC难以检测组织中的CXCL13，因此选用CD69和CD103标记CXCL13细胞，结果显示该群T细胞比肿瘤组织中的其他CD8 T细胞更接近CK19肿瘤细胞。将基因表达综合（GEO）队列中的CRC患者分为CXCL13+高和CXCL13低组，发现CC中 CXCL13 的较高表达预示着更好的总生存期。 Fig.6. CXCL13+ T细胞的特性及预后影响 7.成纤维细胞的不同亚群存在于 CRC 的原发性和肝脏转移性肿瘤中在CRC的TME中鉴定出8个具有不同基因表达模式的成纤维细胞簇，然后研究人员对各类成纤维细胞分别做了转录组数据比较、IHC组化、拟时序分析、以及ST分析，在CRC原发性和肝转移性肿瘤之间观察到不同的表型谱和成纤维细胞的高度可变频率，这表明在不同癌症环境中TME内的细胞异质性。 Fig.7. 原发性和转移性肿瘤中成纤维细胞的转录组特征和异质性 8.在原发性肿瘤中富集的 F3 表达成纤维细胞亚群分泌促肿瘤因子，并与 CRC 患者的不良预后相关为了研究富含CC和LM的不同成纤维细胞对TME 的重塑，研究人员分析了F2_MCAM和F4_F3的特征。通过差异基因富集以及F4_F3细胞与肿瘤细胞之间揭示了通过NRG1和Erb-B2受体酪氨酸激酶3 （ERBB3）通路进行串扰。在ST中发现了两类细胞 F3与NRG1的共定位并通过transwell细胞实验迁移证明。最后在预后数据中发现F3和NRG1 高表达水平的CRC患者总生存期较差。 Fig.8. F3+成纤维细胞的特性及预后影响 9. LM的TME中表达MCAM的成纤维细胞通过Notch 信号通路调节CD8_CXCL13细胞的产生之前发现RBPJ在LM中的表达与CXCL13和ITGAE呈正相关。为了进一步了解两个亚群受到什么类型的细胞调节Notch信号，采用cellphoneDB分析，在内皮细胞中E2_DLL4亚群与CXCL13+ T细胞的相互作用最强，在成纤维细胞中F2_MCAM簇通JAG1-NOTCH1与CD8_CXCL13和CD4_CXCL13亚群相互作用。由于TME中成纤维细胞的分散分布模式，推测F2_MCAM亚群有助于CXCL13+ T细胞中Notch信号的激活。此外根据LM中F2_MCAM的比例高低，发现F2_MCAM高组患者LM中CD8_CXCL13亚群的浸润评分更高，并在ST中得到了验证，使用JASPAR预测表明RBPJ可能作TF影响CXCL13的表达。 Fig.9. TME中的NOTCH信号调节CD8_CXCL13细胞的生成 10.ST组织中的细胞间相互作用网络原发性肿瘤和肝转移性肿瘤ST中不同簇之间的细胞相互作用，表明ERBB3-NRG1相互作用在原发性肿瘤发生和转移中的潜在作用，发现在CRC原发肿瘤中富集的F3成纤维细胞可以通过产生各种促肿瘤因子（包括 NRG1）来调节发展和/或迁移，这些因子与肿瘤细胞上表达的ERBB3相互作用以发挥其促肿瘤功能。 Fig.10. ST组织中的细胞配体和受体相互作用案例2 《空间和单细胞转录组学揭示了HNSCC中与癌症相关的成纤维细胞亚群限制了CD8+ T细胞的浸润和抗肿瘤活性》发表期刊：Cancer Research，影响因子：12.5 样本类型：5例头颈部鳞状细胞癌HNSCC癌和癌旁组织；技术组合：单细胞RNA转录组、空间转录组、免疫组化、免疫荧光、其他等等；研究背景：免疫治疗可以延长一些HNSCC患者的生存期，但应答率仍然很低。阐明肿瘤微环境中cd8+t细胞浸润和功能障碍的关键机制有助于最大限度地发挥免疫治疗HNSCC的益处。CD8+T细胞与包括CAFs在内的其他类型细胞之间的相互作用决定了CD8+T细胞如何在这一动态TME中发挥作用，本研究对五对肿瘤和邻近组织的不同免疫浸润和单细胞RNA测序的HNSCC标本进行了空间转录组学分析，揭示了与cd8 + t细胞浸润限制和功能障碍相关的特定癌症相关成纤维细胞(CAF)亚群。技术路线：主要结果： 1. HNSCC肿瘤组织对CD8+T细胞具有招募趋化作用，CD8+T细胞存在于肿瘤基质中，且免疫排斥型的HNSCC中CD8a+被受限无法浸润到肿瘤巢中； Fig 1.CD8+T细胞在不同HNSCC肿瘤亚型中的分布 2.MHC-IhiCAFs（5亚群）是肿瘤组织中区别于癌旁组织的最主要的CAFs亚群，高表达CXCLs和MHC-I增强了CAFs与CD8+T的结合，且可通过限制CD8+T细胞的抗肿瘤能力造成预后不良； Fig 2.HNSCC肿瘤及邻近组织成纤维细胞的整体分析 3. MHC-IhiCAFs中存在LGALS9（编码galectin-9蛋白）的富集，大部分HNSCC肿瘤基质中均存在galectin-9蛋白的表达；MHC-IhiCAFs中galectin-9蛋白的表达依赖于干扰素信号； Fig3. TCF1 ~ GZMK ~ CD8 + T细胞与galectin-9的CAF细胞呈负相关 4.在CAFs中敲减LGALS9表达会降低CD8+T表达免疫检查点分子，同时促进干性和细胞毒性分子的表达，且动物实验证明Gal-9+CAFs促进干细胞样CD8+T细胞耗竭转化。图4. 动物实验验证MHC I类的高表达限制了cd8+T细胞的抗肿瘤功能案例3 《上皮细胞激活成纤维细胞促进食管癌的发展》发表期刊：Cancer cell，影响因子：48.8 样本类型：29例ESCC患者79个多期食管病变的正常上皮、癌前病变和癌组织；技术组合：单细胞RNA转录组、空间转录组、免疫组化、免疫荧光、其他等等；研究背景：食管鳞状细胞癌(ESCC)的发展经历了多阶段上皮癌的形成，即从正常上皮、低级别和高级别上皮内瘤变到浸润性癌。然而，癌前病变如何发展为癌机制尚未可知。主要结果： 1.ESCC多阶段肿瘤发生过程各种细胞类型图谱分析 Fig 1.单细胞转录组学分析揭示了ESCC多阶段肿瘤发生过程中的各种细胞类型 2.上皮细胞中ANXA1的功能失调可能是ESCC肿瘤发生中至关重要的事件； Fig 2.上皮细胞在ESCC肿瘤发生过程中逐渐抑制ANXA1表达 3.ESCC肿瘤发生过程中上皮细胞与成纤维细胞的相互作用，食管上皮细胞产生的ANXA1功能的丧失可能导致NF-CAF转化； Fig 3.上皮细胞抑制ANXA1可促进NF向CAFs转化 4.KLF4、KLF5、CEBPB和FOXA1与ANXA1的RNA水平呈正相关，细胞实验发现只有靶向KFL4的SiRNA可显著抑制ANXA1表达，KLF4调节ANXA1转录，促进NFs向myCAF的转化。图4.在体外和体内，抑制上皮细胞ANXA1可促进myCAF的激活参考文献： [1]Wang F, Long J, Li L, Wu ZX, Da TT, Wang XQ, Huang C, Jiang YH, Yao XQ, Ma HQ, Lian ZX, Zhao ZB, Cao J. Single-cell and spatial transcriptome analysis reveals the cellular heterogeneity of liver metastatic colorectal cancer. Sci Adv. 2023 Jun 16;9(24):eadf5464. doi: 10.1126/sciadv.adf5464. Epub 2023 Jun 16. PMID: 37327339; PMCID: PMC10275599. [2]Li C, Guo H, Zhai P, Yan M, Liu C, Wang X, Shi C, Li J, Tong T, Zhang Z, Ma H, Zhang J. Spatial and Single-Cell Transcriptomics Reveal a Cancer-Associated Fibroblast Subset in HNSCC That Restricts Infiltration and Antitumor Activity of CD8+ T Cells. Cancer Res. 2024 Jan 16;84(2):258-275. doi: 10.1158/0008-5472.CAN-23-1448. PMID: 37930937; PMCID: PMC10790129. [3]Chen Y, Zhu S, Liu T, Zhang S, Lu J, Fan W, Lin L, Xiang T, Yang J, Zhao X, Xi Y, Ma Y, Cheng G, Lin D, Wu C. Epithelial cells activate fibroblasts to promote esophageal cancer development. Cancer Cell. 2023 May 8;41(5):903-918.e8. doi: 10.1016/j.ccell.2023.03.001. Epub 2023 Mar 23. PMID: 36963399. 本文由科研学术部何鼎提供

免疫疗法寡核苷酸

2024-10-03

·PRNewswire

Sapience Therapeutics Announces Participation at the 4th Annual Needham Private Biotech Company Virtual 1x1 Forum

TARRYTOWN, N.Y., Oct. 3, 2024 /PRNewswire/ -- Sapience Therapeutics, Inc., a clinical-stage biotechnology company focused on the discovery and development of peptide therapeutics to address oncogenic and immune dysregulation that drive cancer, today announced its participation at the 4th Annual Needham Private Biotech Company Virtual 1x1 Forum, taking place October 8-9, 2024. Company management will participate in one-on-one meetings with investors during the conference. About Sapience Therapeutics Sapience Therapeutics, Inc. is a privately held, clinical-stage biotechnology company focused on discovering and developing peptide therapeutics to address oncogenic and immune dysregulation that drive cancer. With in-house discovery capabilities, Sapience has built a pipeline of therapeutic candidates called SPEARs™ (Stabilized Peptides Engineered Against Regulation) that disrupt intracellular protein-protein interactions, enabling targeting of transcription factors which have traditionally been considered undruggable, and can direct cargo to cell surface targets with their new class of molecule called SPARCs™ (Stabilized Peptides Against Receptors on Cancer), enabling delivery of payloads such as α-particles to cancer cells. Sapience is advancing two clinical programs through Phase 2 studies: ST316, a first-in-class antagonist of β-catenin, and ST101, a first-in-class antagonist of C/EBPβ. For more information on Sapience Therapeutics, please visit and engage with us on LinkedIn. Media and Investor Contact: Amy Conrad Juniper Point (858) 366-3243 [email protected] SOURCE Sapience Therapeutics, Inc. WANT YOUR COMPANY'S NEWS FEATURED ON PRNEWSWIRE.COM? 440k+ Newsrooms & Influencers 9k+ Digital Media Outlets 270k+ Journalists Opted In GET STARTED

临床2期

2024-10-02

·PipelineReview

Sapience Therapeutics Enrolls First Patient in Phase 2 Study of ST316, a First-in-Class β-catenin Antagonist, in Colorectal Cancer

-ST316 will be evaluated in several combinations and lines of treatment- TARRYTOWN, NY, USA I October 1, 2024 I Sapience Therapeutics, Inc., a clinical-stage biotechnology company focused on the discovery and development of peptide therapeutics to address oncogenic and immune dysregulation that drive cancer, announced today that the first patient has been enrolled in its Phase 2 dose expansion study evaluating ST316, the Company’s first-in-class antagonist of β-catenin. Enrollment of the study’s Phase 1 monotherapy dose escalation portion was completed in July 2024. ST316 is designed to selectively shut down the Wnt/β-catenin signaling pathway in tumor cells but not in normal cells, allowing for anti-cancer activity without the toxicity related to broad inhibition of this pathway. The Wnt/β-catenin signaling pathway is one of the most active pathways in several cancers and drives more than 80% of colorectal cancers (CRCs), the first indication to be evaluated in the ST316 Phase 2 expansion. There are more than 1 million people living with CRC in the United States, with another 150,000 expected to be diagnosed this year alone. Dr. Abi Vainstein-Haras, Sapience’s Chief Medical Officer, stated, “The promising results seen in our Phase 1 study demonstrate ST316’s potential to be an effective therapy for Wnt pathway-driven cancers, including CRC among others. Given ST316’s favorable safety and tolerability profile, together with robust pre-clinical data, Sapience is committed to maximizing the potential of ST316 in various therapeutic combinations across lines of treatment.” “CRC patients who are refractory to current therapies desperately need new options like ST316,” said Dr. Barry Kappel, Sapience’s founder and Chief Executive Officer. “With CRC being the second-leading cause of cancer death in the United States, and with alarming increases in incidence among younger Americans, we are dedicated to widening the treatment options for this devastating disease.” ST316-101 ( NCT05848739 ) is a first-in-human, open-label, Phase 1-2 dose-escalation and expansion study designed to determine the safety, tolerability, PK, PD and early efficacy of ST316. The Phase 1 dose escalation portion of the study tested various dose levels of ST316 in patients with select advanced solid tumors that are known to harbor abnormalities of the Wnt/β-catenin signaling pathway, including CRC. The Phase 1 portion completed enrollment in July 2024. In the Phase 2 dose expansion portion of the study, ST316 is being tested in CRC patients in combination with relevant standards of care and in multiple lines of treatment. Sapience is conducting the Phase 2 study across several sites in the United States. About ST316 ST316 is a first-in-class peptide antagonist of the interaction between β-catenin and its co-activator, BCL9, a complex responsible for driving oncogene expression in multiple cancers where aberrant Wnt/β-catenin pathway signaling is observed. ST316 exposure in cancer cells prevents BCL9-driven nuclear localization of β-catenin and inhibits formation of the Wnt enhanceosome protein complex. Disruption of this interaction selectively suppresses the transcription of oncogenic Wnt target genes that regulate proliferation, migration, invasion and the metastatic potential of tumor cells, as well as genes that regulate the immunosuppression of the tumor microenvironment. ST316 creates a pro-immune tumor microenvironment and in preclinical models has shown to be synergistic with checkpoint inhibition. Due to its selectivity and downstream modulation of the Wnt/β-catenin pathway, ST316 presents an opportunity to safely and effectively target Wnt/β-catenin driven cancers without the toxicities previously seen with other Wnt pathway agents. About Sapience Therapeutics Sapience Therapeutics, Inc. is a privately held, clinical-stage biotechnology company focused on discovering and developing peptide therapeutics to address oncogenic and immune dysregulation that drive cancer. With in-house discovery capabilities, Sapience has built a pipeline of therapeutic candidates called SPEARs™ (Stabilized Peptides Engineered Against Regulation) that disrupt intracellular protein-protein interactions, enabling targeting of transcription factors which have traditionally been considered undruggable, and can direct cargo to cell surface targets with their new class of molecule called SPARCs™ (Stabilized Peptides Against Receptors on Cancer), enabling delivery of payloads such as α-particles to cancer cells. Sapience is advancing two clinical programs through Phase 2 studies: ST316, a first-in-class antagonist of β-catenin, and ST101, a first-in-class antagonist of C/EBPβ. For more information on Sapience Therapeutics, please visit www.sapiencetherapeutics.com and engage with us on LinkedIn . SOURCE: Sapience Therapeutics

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