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首页> 外文期刊>Developmental biology >Cell death and tissue remodeling in planarian regeneration.
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Cell death and tissue remodeling in planarian regeneration.

机译:涡虫再生中的细胞死亡和组织重塑。

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Many long-lived organisms, including humans, can regenerate some adult tissues lost to physical injury or disease. Much of the previous research on mechanisms of regeneration has focused on adult stem cells, which give rise to new tissue necessary for the replacement of missing body parts. Here we report that apoptosis of differentiated cells complements stem cell division during regeneration in the planarian Schmidtea mediterranea. Specifically, we developed a whole-mount TUNEL assay that allowed us to document two dramatic increases in the rate of apoptosis following amputation-an initial localized response near the wound site and a subsequent systemic response that varies in magnitude depending on the type of fragment examined. The latter cell death response can be induced in uninjured organs, occurs in the absence of planarian stem cells, and can also be triggered by prolonged starvation. Taken together, our results implicate apoptosis in the restoration of proper anatomical scale and proportion through remodeling of existing tissues. We also report results from initial mechanistic studies of apoptosis in planarians, which revealed that a S. mediterranea homolog of the antiapoptotic gene BCL2 is required for cell survival in adult animals. We propose that apoptosis is a central mechanism working in concert with stem cell division to restore anatomical form and function during metazoan regeneration.
机译:许多长寿命的生物体,包括人类,都可以再生一些因人身伤害或疾病而丧失的成年组织。先前有关再生机制的许多研究都集中在成体干细胞上,这产生了新的组织,这些新组织是替换缺失的身体部位所必需的。在这里,我们报告分化的细胞凋亡补充了在涡虫Schmidtea mediterranea再生过程中的干细胞分裂。具体而言,我们开发了一种完整的TUNEL检测方法,使我们能够记录截肢后凋亡率的两个显着增加-伤口部位附近的初始局部反应和随后的全身反应,其幅度取决于所检查片段的类型。后者的细胞死亡反应可以在未受伤的器官中诱导,在没有涡虫干细胞的情况下发生,也可以由长期饥饿触发。两者合计,我们的结果暗示凋亡通过重建现有组织来重建适当的解剖学规模和比例。我们还报告了从刨刀中细胞凋亡的初步机理研究的结果,该研究表明抗凋亡基因BCL2的S. mediterranea同系物对于成年动物的细胞存活是必需的。我们提出凋亡是与干细胞分裂协同工作以恢复后生动物再生期间的解剖形式和功能的中心机制。

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