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心脏毒素对心脏干细胞和祖细胞群体的影响。

Effects of Cardiotoxins on Cardiac Stem and Progenitor Cell Populations.

作者信息

Smith Andrew J

机构信息

Faculty of Biological Sciences, School of Biomedical Sciences, University of Leeds, Leeds, United Kingdom.

Faculty of Life Sciences and Medicine, Centre for Human and Applied Physiological Sciences, Centre for Stem Cell and Regenerative Medicine, School of Basic and Medical Biosciences, Guy's Campus, King's College London, London, United Kingdom.

出版信息

Front Cardiovasc Med. 2021 Apr 27;8:624028. doi: 10.3389/fcvm.2021.624028. eCollection 2021.

Abstract

As research and understanding of the cardiotoxic side-effects of anticancer therapy expands further and the affected patient population grows, notably the long-term survivors of childhood cancers, it is important to consider the full range of myocardial cell types affected. While the direct impacts of these toxins on cardiac myocytes constitute the most immediate damage, over the longer term, the myocardial ability to repair, or adapt to this damage becomes an ever greater component of the disease phenotype. One aspect is the potential for endogenous myocardial repair and renewal and how this may be limited by cardiotoxins depleting the cells that contribute to these processes. Clear evidence exists of new cardiomyocyte formation in adult human myocardium, along with the identification in the myocardium of endogenous stem/progenitor cell populations with pro-regenerative properties. Any effects of cardiotoxins on either of these processes will worsen long-term prognosis. While the role of cardiac stem/progenitor cells in cardiomyocyte renewal appears at best limited (although with stronger evidence of this process in response to diffuse cardiomyocyte loss), there are strong indications of a pro-regenerative function through the support of injured cell survival. A number of recent studies have identified detrimental impacts of anticancer therapies on cardiac stem/progenitor cells, with negative effects seen from both long-established chemotherapy agents such as, doxorubicin and from newer, less overtly cardiotoxic agents such as tyrosine kinase inhibitors. Damaging impacts are seen both directly, on cell numbers and viability, but also on these cells' ability to maintain the myocardium through generation of pro-survival secretome and differentiated cells. We here present a review of the identified impacts of cardiotoxins on cardiac stem and progenitor cells, considered in the context of the likely role played by these cells in the maintenance of myocardial tissue homeostasis.

摘要

随着对抗癌治疗心脏毒性副作用的研究和理解进一步深入,以及受影响患者群体的增加,尤其是儿童癌症的长期幸存者,考虑受影响的心肌细胞类型的全貌变得很重要。虽然这些毒素对心肌细胞的直接影响构成了最直接的损害,但从长期来看,心肌修复或适应这种损害的能力成为疾病表型中越来越重要的组成部分。一个方面是内源性心肌修复和更新的潜力,以及这种潜力如何可能因心脏毒素耗尽参与这些过程的细胞而受到限制。在成人心肌中存在新的心肌细胞形成的明确证据,同时在心肌中也鉴定出具有促再生特性的内源性干/祖细胞群体。心脏毒素对这些过程中任何一个的影响都会使长期预后恶化。虽然心脏干/祖细胞在心肌细胞更新中的作用似乎充其量有限(尽管在弥漫性心肌细胞丢失的情况下有更强的证据证明这一过程),但有强烈迹象表明它们通过支持受损细胞存活而具有促再生功能。最近的一些研究已经确定了抗癌治疗对心脏干/祖细胞的有害影响,无论是从长期使用的化疗药物如多柔比星,还是从较新的、心脏毒性不太明显的药物如酪氨酸激酶抑制剂中都能看到负面影响。不仅在细胞数量和活力方面直接观察到损害性影响,而且在这些细胞通过产生促存活分泌组和分化细胞来维持心肌的能力方面也观察到了损害性影响。我们在此综述已确定的心脏毒素对心脏干/祖细胞的影响,并结合这些细胞在维持心肌组织稳态中可能发挥的作用进行考虑。

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