预约演示

更新于：2025-05-07

ACTA1

更新于：2025-05-07

基本信息

别名

ACTA、ACTA1、actin alpha 1, skeletal muscle

+ [4]

简介

Actins are highly conserved proteins that are involved in various types of cell motility and are ubiquitously expressed in all eukaryotic cells.

关联

项与 ACTA1 相关的药物

WO2023186189

专利挖掘

靶点

ACTA1

作用机制-

在研机构

扬州大学

原研机构

扬州大学

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

100 项与 ACTA1 相关的临床结果

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100 项与 ACTA1 相关的转化医学

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0 项与 ACTA1 相关的专利（医药）

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1,741

项与 ACTA1 相关的文献（医药）

2025-06-01·Stem Cell Research

Generation of an induced pluripotent stem cell line (NCHi023-A) from a 41-year-old male with nemaline myopathy carrying autosomal dominant ACTA1 c.809-10C>A mutation

Article

作者: Ye, Shiqiao ; Yu, Yang ; Zhao, Ming-Tao ; Zhu, Jingting ; Rashnonejad, Afrooz ; Hanley, Meghan ; Flanigan, Kevin ; Lin, Hui

Nemaline myopathy is a rare genetic condition characterized by weakened muscles due to thread-like rods, called nemaline bodies, in muscle fibers. This condition varies in time of onset and severity. Although there is no cure, therapies and treatments are available to reduce symptoms. This iPSC line, NCHi023-A, was reprogrammed using Sendai virus from skin fibroblasts from a male patient with nemaline myopathy carrying a pathogenic heterozygous ACTA1 mutation. Characterization of this line was successful, with validation of cell identity, normal morphology and karyotype, positive expression of germ layer and pluripotency markers, and negative expression for mycoplasma and transgenes.

2025-05-01·American Journal of Physiology-Lung Cellular and Molecular Physiology

Succinate aggravates pulmonary fibrosis through the succinate/SUCNR1 axis

Article

作者: Mooslechner, Agnes Anna ; Heinemann, Akos ; Angiari, Stefano ; Platzer, Wolfgang ; Kwapiszewska, Grazyna ; Schweighofer, Hannah ; Rajesh, Rishi ; Pahernik, Svetlana ; Benazzo, Alberto ; Bärnthaler, Thomas ; Marsh, Leigh ; Atallah, Reham ; Aigner, Clemens ; Lanz, Ilse

This paper highlights the role of the succinate/SUCNR1 axis in pulmonary fibrosis. Receptor activation leads to profibrotic changes in IPF patient-derived fibroblasts. This finding could also be replicated in a mouse model of pulmonary fibrosis.

2025-04-01·The American Journal of Pathology

Piezo2 Is a Key Mechanoreceptor in Lung Fibrosis that Drives Myofibroblast Differentiation

Article

作者: Sime, Patricia J ; Thatcher, Thomas H ; Robila, Valentina ; Perelas, Apostolos ; Camus, Sarah V ; Freeberg, Margaret A T

Idiopathic pulmonary fibrosis (IPF) and other progressive fibrotic interstitial lung diseases have limited treatment options. Fibroblasts are key effector cells that sense matrix stiffness through conformation changes in mechanically sensitive receptors, leading to activation of downstream profibrotic pathways. Here, the role of Piezo2, a mechanosensitive ion channel, in human and mouse lung fibrosis, and its function in myofibroblast differentiation in primary human lung fibroblasts (HLFs) was investigated. Human samples from patients with IPF and mouse tissue from bleomycin-induced pulmonary fibrosis were assessed. Primary HLFs from nonfibrotic donors were grown on substrates of different stiffness to induce myofibroblast differentiation and treated with a Piezo2 inhibitor. Piezo2 expression was up-regulated in tissue from patients with IPF and in fibrotic mouse lung tissue. Additionally, analysis of published single-cell RNA-sequencing data showed that Piezo2 was expressed in the profibrotic collagen triple helix repeat containing 1 (Cthrc1)⁺ fibroblast subpopulation. Myofibroblast differentiation was increased in HLFs grown on substrates with fibrotic levels of stiffness compared with that seen in softer substrates. Piezo2 inhibition reduced stiffness-induced expression α-smooth muscle actin and fibronectin in HLFs. Piezo2 expression was elevated in fibrotic lung disease in both patients and rodents, and its presence was key in the differentiation of fibroblasts to the profibrotic myofibroblasts. Blocking Piezo2 may play a key role in fibrosis and, thus, be a novel therapeutic approach to treat pulmonary fibrosis.

项与 ACTA1 相关的新闻（医药）

2022-06-14

·生物谷

新发现！科学家揭示了结直肠癌成纤维细胞异质性新机制

结直肠癌是世界上第三大常见恶性肿瘤，预计到2030年，全球发病率将超过200万，死亡率将达到100万。在结直肠癌等实体瘤患者中，超过90%的死亡是由于转移。结直肠癌是世界上第三大常见恶性肿瘤，预计到2030年，全球发病率将超过200万，死亡率将达到100万。在结直肠癌等实体瘤患者中，超过90%的死亡是由于转移。这突出了研究CRC进展生物学的重要性，以确定更好的预后标志物和设计有针对性的治疗。全球公认的分类系统将结直肠癌和分层患者的共识分子亚型(CM)定义为四个亚组(CMS1-4)。其中，CMS4预后最差，与肿瘤转移和化疗耐药有关。重要的是，这个亚型在突变负担、体细胞拷贝数改变或CpG岛甲基化方面与其他亚型没有区别，而是存在间质细胞和间充质(或转化生长因子-β激活)基因表达特征。因此，在转移细胞和转移细胞之间似乎存在着重要的联系。图片来源: https://doi-org.libproxy1.nus.edu.sg/10.1002/jev2.12226 近日，来自南安普敦大学的研究者们在J Extracell Vesicles杂志上发表了题为“Epithelial to mesenchymal transition influences fibroblast phenotype in colorectal cancer by altering miR-200 levels in extracellular vesicles”的文章，该研究为结直肠癌成纤维细胞异质性的发展提供了一种新的机制，通过EV介导的miRNAs转移，并解释了为什么转移潜能较大的结直肠癌富含CAF。具有间充质基因表达特征的结直肠癌(CRC)具有最大的远处转移倾向，其特征是与癌症相关的成纤维细胞在间质中聚集。研究者研究了结直肠癌细胞上皮向间充质转化的状态是否影响成纤维细胞的表型，重点是细胞外小泡(EV)的转移，作为细胞间通讯的受控手段。上皮性结直肠癌EVS抑制转化生长因子-β诱导的肌成纤维细胞分化，而间叶性结直肠癌EVS不抑制其分化。这是由miR-200(miR-200a/b/c，-141)驱动的，它富含上皮性CRC-EV，并转移到受体成纤维细胞。在成纤维细胞中异位表达miR-200或ZEB1基因敲除，同样抑制肌成纤维细胞的分化。研究者发现在TCGA数据集中的一组CRC患者中，miR-200和肌成纤维细胞标志物之间存在强烈的负相关。在体内实验中，研究者通过将上皮或间充质CRC细胞与成纤维细胞共同注射，并分析肌成纤维细胞表型的基质标记。与间叶性肿瘤相比，上皮性肿瘤的成纤维细胞表达更多的miR-200，表达更少的ACTA和FN。 CRC EMT在体内测定成纤维细胞表型中的作用图片来源: https://doi-org.libproxy1.nus.edu.sg/10.1002/jev2.12226 总体而言，本研究揭示了CMS4肿瘤中肌成纤维细胞间质积聚的机制，主要是成纤维细胞中的miR-200/ZEB1轴，以及肿瘤细胞来源的EVS对其调节。CRC的EMT状态决定成纤维细胞表型的证明是理解不同成纤维细胞表型如何在肿瘤中存在的关键环节。本研究为最近发表的实体癌间质异质性的观察提供了机制上的见解。更好地理解这一概念将使预后基质生物标志物的开发和调节CAF表型的能力获得治疗优势。（生物谷 Bioon.com）参考文献 Rahul Bhome et al. Epithelial to mesenchymal transition influences fibroblast phenotype in colorectal cancer by altering miR-200 levels in extracellular vesicles. J Extracell Vesicles. 2022 May;11(5):e12226. doi: 10.1002/jev2.12226.

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