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首页> 外文期刊>Cell stem cell >Drug Screening in Human PSC-Cardiac Organoids Identifies Pro-proliferative Compounds Acting via the Mevalonate Pathway
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Drug Screening in Human PSC-Cardiac Organoids Identifies Pro-proliferative Compounds Acting via the Mevalonate Pathway

机译:人PSC-Cardiac有机体中的药物筛选鉴定了通过甲羟戊酸途径作用的促型化合物

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摘要

We have previously developed a high-throughput bioengineered human cardiac organoid (hCO) platform, which provides functional contractile tissue with biological properties similar to native heart tissue, including mature, cell-cycle-arrested cardiomyocytes. In this study, we perform functional screening of 105 small molecules with pro-regenerative potential. Our findings reveal surprising discordance between our hCO system and traditional 2D assays. In addition, functional analyses uncovered detrimental effects of many hit compounds. Two pro-proliferative small molecules without detrimental impacts on cardiac function were identified. High-throughput proteomics in hCO revealed synergistic activation of the mevalonate pathway and a cell-cycle network by the pro-proliferative compounds. Cell-cycle reentry in hCO and in vivo required the mevalonate pathway as inhibition of the mevalonate pathway with a statin attenuated pro-proliferative effects. This study highlights the utility of human cardiac organoids for pro-regenerative drug development, including identification of underlying biological mechanisms and minimization of adverse side effects.
机译:我们以前开发出一种高通量生物工程人体心脏有机体(HCO)平台,其提供与天然心脏组织类似的生物学性质的功能性收缩组织,包括成熟,细胞周期被捕获的心肌细胞。在这项研究中,我们使用具有促果断潜力的105个小分子进行功能筛选。我们的调查结果揭示了我们的HCO系统和传统的2D测定之间的令人惊讶的不间断。此外,功能分析揭示了许多麦片化合物的不利影响。鉴定了两种没有对心脏功能产生不利影响的促增殖性小分子。 HCO中高通量蛋白质组学揭示了甲羟戊酯途径的协同活化和通过预增殖化合物的细胞周期网络。 HCO和体内中的细胞周期再入物需要甲羟戊酸途径作为抑制甲丙酮途径的抑制患者,其衰减的促进的促进促进作用。本研究突出了人体心脏有机体对促果解药物发育的效用,包括鉴定潜在的生物机制和最小化不良副作用。

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  • 来源
    《Cell stem cell》 |2019年第6期|共19页
  • 作者

    Mills Richard J.; Parker Benjamin L.; Quaife-Ryan Gregory A.; Voges Holly K.; Needham Elise J.; Bornot Aurelie; Ding Mei; Andersson Henrik; Polla Magnus; Elliott David A.; Drowley Lauren; Clausen Maryam; Plowright Alleyn T.; Barrett Ian P.; Wang Qing-Dong; James David E.; Porrello Enzo R.; Hudson James E.;

  • 作者单位

    Univ Queensland Sch Biomed Sci St Lucia Qld 4072 Australia;

    Univ Sydney Sch Life &

    Environm Sci Charles Perkins Ctr Sydney NSW 2006 Australia;

    Univ Queensland Sch Biomed Sci St Lucia Qld 4072 Australia;

    Univ Queensland Sch Biomed Sci St Lucia Qld 4072 Australia;

    Univ Sydney Sch Life &

    Environm Sci Charles Perkins Ctr Sydney NSW 2006 Australia;

    AstraZeneca Cambridge IMED Biotech Unit Discovery Sci Cambridge England;

    AstraZeneca Gothenburg IMED Biotech Unit Discovery Sci Gothenburg Sweden;

    AstraZeneca Gothenburg IMED Biotech Unit Discovery Sci Gothenburg Sweden;

    AstraZeneca Gothenburg IMED Biotech Unit Med Chem Cardiovasc Renal &

    Metab Gothenburg Sweden;

    Royal Childrens Hosp Murdoch Childrens Res Inst Parkville Vic 3052 Australia;

    AstraZeneca Gothenburg IMED Biotech Unit Biosci Heart Failure Cardiovasc Renal &

    Metab;

    AstraZeneca Gothenburg IMED Biotech Unit Discovery Sci Gothenburg Sweden;

    AstraZeneca Gothenburg IMED Biotech Unit Med Chem Cardiovasc Renal &

    Metab Gothenburg Sweden;

    AstraZeneca Cambridge IMED Biotech Unit Discovery Sci Cambridge England;

    AstraZeneca Gothenburg IMED Biotech Unit Biosci Heart Failure Cardiovasc Renal &

    Metab;

    Univ Sydney Sch Life &

    Environm Sci Charles Perkins Ctr Sydney NSW 2006 Australia;

    Univ Queensland Sch Biomed Sci St Lucia Qld 4072 Australia;

    Univ Queensland Sch Biomed Sci St Lucia Qld 4072 Australia;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
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