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无瘢痕胎儿伤口与基质金属蛋白酶与组织源性金属蛋白酶抑制剂的比例增加有关。

Scarless fetal wounds are associated with an increased matrix metalloproteinase-to-tissue-derived inhibitor of metalloproteinase ratio.

作者信息

Dang Catherine M, Beanes Steven R, Lee Haofu, Zhang Xinli, Soo Chia, Ting Kang

机构信息

Department of Surgery, School of Medicine, University of California, Los Angeles, 90095, USA.

出版信息

Plast Reconstr Surg. 2003 Jun;111(7):2273-85. doi: 10.1097/01.PRS.0000060102.57809.DA.

Abstract

In contrast to adult cutaneous wounds, early fetal wounds heal scarlessly. Fetal rat skin transitions from scarless repair to healing, with scar formation between days 16.5 (E16) and 18.5 (E18) of gestation. Term gestation is 21.5 days. The composition of the extracellular matrix in fetal skin and wounds differs from that of the adult. Matrix metalloproteinases (MMPs) and their tissue-derived inhibitors (TIMPs) determine the architecture of the extracellular matrix. The authors hypothesized that differential expression of MMPs and TIMPs occurs during the ontogenetic transition to scar-forming repair in fetal skin and wounds. Full-thickness, excisional wounds (2 mm) were created on the dorsum of E16 (n = 42 fetuses) and E19 fetal rats (n = 42 fetuses). Wounds were harvested at 24, 48, and 72 hours. Nonwounded skin from littermates was also harvested as controls. Six E16 and E19 wounds were fixed 72 hours after injury, stained with hematoxylin and eosin, and examined by light microscopy. RNA was isolated from the remaining wounds and skin, and a reduced-cycle, primer-specific, reverse-transcriptase polymerase chain reaction was performed to semiquantitatively determine relative gene expression of MMP-1, MMP-2, MMP-7, MMP-9, and MMP-14 and of TIMP-1, TIMP-2, and TIMP-3. Significance was determined by unpaired two-tailed t test (p < 0.05) and analysis of variance. In both E16 and E19 wounds, reepithelialization was complete by 72 hours. E16 wounds healed scarlessly, whereas E19 wounds healed with scar. During late gestation, skin expression of MMP-1 and MMP-14 (membrane type-1 MMP) doubled, whereas MMP-2 expression increased nearly 50-fold. Levels of MMP-7 and MMP-9 were unchanged in developing skin. As for the TIMPs, skin expression of TIMP-2 increased more than four-fold, whereas TIMP-1 and TIMP-3 expression was unchanged. In both scarless and scarring wounds, up-regulation of MMP-1 and MMP-9 occurred. However, the maximal increase in MMP-1 and MMP-9 expression occurred much more rapidly and was much greater in the scarless E16 wounds (28-fold versus 23-fold for MMP-1 and 18-fold versus nine-fold for MMP-9). Unchanged in scarless wounds, MMP-2 levels decreased more than three-fold in scarring wounds. MMP-14 (membrane type-1 MMP) expression increased three-fold in scarless wounds but was unchanged in scarring wounds. In contrast, TIMP-1 and TIMP-3 expression in E19 scarring wounds increased six-fold and four-fold, respectively. MMP-7 and TIMP-2 expression did not change in response to injury. E16 scarless wounds have greater MMP relative to TIMP expression than E19 scarring wounds. This favors extracellular matrix turnover, facilitates migration of fetal cells, and promotes scarless repair.

摘要

与成年皮肤伤口不同,早期胎儿伤口能无瘢痕愈合。胎鼠皮肤在妊娠第16.5天(E16)至18.5天(E18)之间从无瘢痕修复转变为愈合,并形成瘢痕。足月妊娠为21.5天。胎儿皮肤和伤口中细胞外基质的组成与成年人不同。基质金属蛋白酶(MMPs)及其组织来源的抑制剂(TIMPs)决定了细胞外基质的结构。作者推测,在胎儿皮肤和伤口向形成瘢痕的修复的个体发育转变过程中,MMPs和TIMPs会出现差异表达。在E16(n = 42只胎儿)和E19胎鼠(n = 42只胎儿)的背部制作全层切除伤口(2毫米)。在24、48和72小时时采集伤口样本。同窝出生的未受伤皮肤也作为对照进行采集。6个E16和E19伤口在受伤72小时后固定,用苏木精和伊红染色,并通过光学显微镜检查。从剩余的伤口和皮肤中分离RNA,并进行减循环、引物特异性逆转录聚合酶链反应,以半定量测定MMP - 1、MMP - 2、MMP - 7、MMP - 9和MMP - 14以及TIMP - 1、TIMP - 2和TIMP - 3的相对基因表达。通过未配对双尾t检验(p < 0.05)和方差分析确定显著性。在E16和E19伤口中,72小时时上皮再形成均已完成。E16伤口无瘢痕愈合,而E19伤口有瘢痕愈合。在妊娠后期,MMP - 1和MMP - 14(膜型1 MMP)的皮肤表达增加了一倍,而MMP - 2的表达增加了近50倍。发育中的皮肤中MMP - 7和MMP - 9的水平没有变化。至于TIMPs,TIMP - 2的皮肤表达增加了四倍多,而TIMP - 1和TIMP - 3的表达没有变化。在无瘢痕和有瘢痕的伤口中,MMP - 1和MMP - 9均出现上调。然而,MMP - 1和MMP - 9表达的最大增加在无瘢痕的E16伤口中出现得更快且幅度更大(MMP - 1为28倍对23倍,MMP - 9为18倍对9倍)。在无瘢痕伤口中不变,MMP - 2水平在有瘢痕伤口中下降了三倍多。MMP - 14(膜型1 MMP)在无瘢痕伤口中的表达增加了三倍,但在有瘢痕伤口中没有变化。相比之下,E19有瘢痕伤口中TIMP - 1和TIMP - 3的表达分别增加了六倍和四倍。MMP - 7和TIMP - 2的表达对损伤没有变化。E16无瘢痕伤口相对于TIMP表达的MMP比E19有瘢痕伤口更多。这有利于细胞外基质更新,促进胎儿细胞迁移,并促进无瘢痕修复。

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