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伤口修复过程中的炎症细胞:有益的、有害的和丑陋的。

Inflammatory cells during wound repair: the good, the bad and the ugly.

作者信息

Martin Paul, Leibovich S Joseph

机构信息

Department of Physiology, School of Medical Sciences, University of Bristol, University Walk, Bristol, UK BS8 1TD.

出版信息

Trends Cell Biol. 2005 Nov;15(11):599-607. doi: 10.1016/j.tcb.2005.09.002. Epub 2005 Oct 3.

Abstract

Damage to any tissue triggers a cascade of events that leads to rapid repair of the wound - if the tissue is skin, then repair involves re-epithelialization, formation of granulation tissue and contraction of underlying wound connective tissues. This concerted effort by the wounded cell layers is accompanied by, and might also be partially regulated by, a robust inflammatory response, in which first neutrophils and then macrophages and mast cells emigrate from nearby tissues and from the circulation. Clearly, this inflammatory response is crucial for fighting infection and must have been selected for during the course of evolution so that tissue damage did not inevitably lead to death through septicemia. But, aside from this role, exactly what are the functions of the various leukocyte lineages that are recruited with overlapping time courses to the wound site, and might they do more harm than good? Recent knockout and knockdown studies suggest that depletion of one or more of the inflammatory cell lineages can even enhance healing, and we discuss new views on how regulation of the migration of inflammatory cells to sites of tissue damage might guide therapeutic strategies for modulating the inflammatory response.

摘要

任何组织受损都会引发一系列事件,从而实现伤口的快速修复——如果受损组织是皮肤,那么修复过程包括上皮再形成、肉芽组织形成以及伤口下方结缔组织的收缩。受伤细胞层的这种协同努力伴随着强烈的炎症反应,并且可能也受到其部分调节,在炎症反应中,首先是中性粒细胞,然后是巨噬细胞和肥大细胞从附近组织和循环系统中迁移过来。显然,这种炎症反应对于抵抗感染至关重要,并且在进化过程中肯定是经过选择的,这样组织损伤就不会不可避免地因败血症而导致死亡。但是,除了这个作用之外,在重叠的时间进程中被招募到伤口部位的各种白细胞谱系究竟有哪些功能,它们会不会弊大于利呢?最近的基因敲除和敲低研究表明,耗尽一种或多种炎症细胞谱系甚至可能会促进愈合,我们将讨论关于如何调节炎症细胞向组织损伤部位迁移可能会指导调节炎症反应的治疗策略的新观点。

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