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哺乳动物骨骼肌和心肌的再生:非灵长类动物模型与人类病理学相似吗?

Regeneration of skeletal and cardiac muscle in mammals: do nonprimate models resemble human pathology?

作者信息

Borisov A B

机构信息

Department of Anatomy and Cell Biology, University of Michigan Medical School, Ann Arbor, Mich. 48109-0616, USA.

出版信息

Wound Repair Regen. 1999 Jan-Feb;7(1):26-35. doi: 10.1046/j.1524-475x.1999.00026.x.

Abstract

Most of the available information regarding the regenerative potential and compensatory remodeling of mammalian tissues has been obtained from nonprimate animals, mainly rodent experimental models. The increasing use of transgenic mice for studies of the mechanisms controlling organogenesis and regeneration also requires a clear understanding of their applicability as experimental models for studies of similar processes in humans and other mammals. Application of modern cell biology methods to studies of regenerative processes has provided new insights into similarity and differences in cellular responses to injury in the tissues of different mammalian species. During more than 200-million years of progressive divergent evolution of mammals, cellular mechanisms of tissue regeneration and compensatory remodeling evolved together with increasingly adaptive functional specialization and structural complexity of mammalian tissues and organs. Rodents represent a phylogenetically ancient order of mammals that has conservatively retained a number of morphofunctional characteristics of early representatives of this class, which include enhanced regenerative capacity of tissues. A comparative analysis of regenerative processes in skeletal and cardiac muscle, as well as in several other mammalian tissues, shows that time courses and intensities of regeneration in response to the same type of injury vary even within taxonomically related species (e.g., rat, mouse, and hamster). The warm bloodedness of mammals facilitated the development of more complex mechanisms of metabolic, immune, and neurohumoral regulation, which resulted in a stronger dependence of regenerative processes on vascularization and innervation. For this reason, interspecies modifications of regenerative responses are limited by the capacity of the animal to resorb rapidly the foci of necrosis and to revascularize and reinnervate the volume of the regenerating tissue. These differences, among other factors, result in significantly lower rates of reparative regeneration in mammals possessing larger body sizes than rodents. A review of these data strongly indicates that the phylogenetic age and biological differences between different species should be taken into account before extrapolation of regenerative properties of nonprimate tissues on the regenerative responses in the primates.

摘要

关于哺乳动物组织再生潜能和代偿性重塑的现有信息大多来自非灵长类动物,主要是啮齿类实验模型。越来越多地使用转基因小鼠来研究控制器官发生和再生的机制,这也需要清楚地了解它们作为人类和其他哺乳动物类似过程研究的实验模型的适用性。将现代细胞生物学方法应用于再生过程的研究,为不同哺乳动物物种组织中细胞对损伤反应的异同提供了新的见解。在哺乳动物超过2亿年的渐进性分歧进化过程中,组织再生和代偿性重塑的细胞机制与哺乳动物组织和器官日益适应的功能特化和结构复杂性共同进化。啮齿类代表了一个系统发育上古老的哺乳动物目,保守地保留了该类早期代表的一些形态功能特征,其中包括组织增强的再生能力。对骨骼肌、心肌以及其他几种哺乳动物组织再生过程的比较分析表明,即使在分类学相关的物种(如大鼠、小鼠和仓鼠)中,对同类型损伤的再生时间进程和强度也有所不同。哺乳动物的温血特性促进了更复杂的代谢、免疫和神经体液调节机制的发展,这导致再生过程对血管化和神经支配的依赖性更强。因此,再生反应的种间变化受到动物快速吸收坏死灶以及使再生组织区域重新血管化和重新神经支配能力的限制。这些差异以及其他因素导致体型比啮齿类大的哺乳动物的修复性再生率显著降低。对这些数据的综述强烈表明,在将非灵长类组织的再生特性外推至灵长类的再生反应之前,应考虑不同物种的系统发育年龄和生物学差异。

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