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刺激内源性心脏修复。

Stimulating endogenous cardiac repair.

作者信息

Finan Amanda, Richard Sylvain

机构信息

Centre National de la Recherche Scientifique United Medical Resource 9214, Institut National de la Santé et de la Recherche Médicale U1046, Physiology and Experimental Medicine of the Heart and Muscles, University of Montpellier Montpellier, France.

出版信息

Front Cell Dev Biol. 2015 Sep 29;3:57. doi: 10.3389/fcell.2015.00057. eCollection 2015.

Abstract

The healthy adult heart has a low turnover of cardiac myocytes. The renewal capacity, however, is augmented after cardiac injury. Participants in cardiac regeneration include cardiac myocytes themselves, cardiac progenitor cells, and peripheral stem cells, particularly from the bone marrow compartment. Cardiac progenitor cells and bone marrow stem cells are augmented after cardiac injury, migrate to the myocardium, and support regeneration. Depletion studies of these populations have demonstrated their necessary role in cardiac repair. However, the potential of these cells to completely regenerate the heart is limited. Efforts are now being focused on ways to augment these natural pathways to improve cardiac healing, primarily after ischemic injury but in other cardiac pathologies as well. Cell and gene therapy or pharmacological interventions are proposed mechanisms. Cell therapy has demonstrated modest results and has passed into clinical trials. However, the beneficial effects of cell therapy have primarily been their ability to produce paracrine effects on the cardiac tissue and recruit endogenous stem cell populations as opposed to direct cardiac regeneration. Gene therapy efforts have focused on prolonging or reactivating natural signaling pathways. Positive results have been demonstrated to activate the endogenous stem cell populations and are currently being tested in clinical trials. A potential new avenue may be to refine pharmacological treatments that are currently in place in the clinic. Evidence is mounting that drugs such as statins or beta blockers may alter endogenous stem cell activity. Understanding the effects of these drugs on stem cell repair while keeping in mind their primary function may strike a balance in myocardial healing. To maximize endogenous cardiac regeneration, a combination of these approaches could ameliorate the overall repair process to incorporate the participation of multiple cellular players.

摘要

健康的成年心脏心肌细胞更新率较低。然而,心脏损伤后其更新能力会增强。参与心脏再生的细胞包括心肌细胞本身、心脏祖细胞和外周干细胞,尤其是骨髓来源的干细胞。心脏损伤后,心脏祖细胞和骨髓干细胞数量增加,迁移至心肌并支持再生。对这些细胞群体的耗竭研究已证明它们在心脏修复中发挥着必要作用。然而,这些细胞完全再生心脏的潜力有限。目前的研究重点是如何增强这些自然途径以改善心脏愈合,主要针对缺血性损伤,其他心脏疾病也适用。细胞和基因疗法或药物干预是提出的机制。细胞疗法已取得一定成效并进入临床试验阶段。然而,细胞疗法的有益效果主要在于其对心脏组织产生旁分泌作用以及募集内源性干细胞群体的能力,而非直接实现心脏再生。基因疗法致力于延长或重新激活自然信号通路。已证实其在激活内源性干细胞群体方面取得了积极成果,目前正在临床试验中进行测试。一个潜在的新途径可能是优化目前临床中使用的药物治疗。越来越多的证据表明他汀类药物或β受体阻滞剂等药物可能会改变内源性干细胞活性。在牢记这些药物主要功能的同时,了解它们对干细胞修复的影响,可能会在心肌愈合中找到平衡。为了最大限度地实现内源性心脏再生,综合运用这些方法可以改善整体修复过程,使多个细胞参与者共同参与。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a29e/4586501/a4da9f3dd7d1/fcell-03-00057-g0001.jpg

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