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一个稳定的生态位支持人表皮干细胞在器官型培养物中的长期维持。

A stable niche supports long-term maintenance of human epidermal stem cells in organotypic cultures.

作者信息

Muffler Sonja, Stark Hans-Jürgen, Amoros Mara, Falkowska-Hansen Berit, Boehnke Karsten, Bühring Hans-Jörg, Marmé Alexander, Bickenbach Jackie R, Boukamp Petra

机构信息

Division of Genetics of Skin Carcinogenesis, German Cancer Research Center, Heidelberg, Germany.

出版信息

Stem Cells. 2008 Oct;26(10):2506-15. doi: 10.1634/stemcells.2007-0991. Epub 2008 Jul 24.

Abstract

Stem cells in human interfollicular epidermis are still difficult to identify, mainly because of a lack of definitive markers and the inability to label human beings for label-retaining cells (LRCs). Here, we report that LRCs could be identified and localized in organotypic cultures (OTCs) made with human cells. Labeling cultures for 2 weeks with iododeoxyuridine (IdU) and then chasing for 6-10 weeks left <1% of basal cells retaining IdU label. Whole mounts demonstrated that LRCs were individually dispersed in the epidermal basal layer. Some LRCs, but not all, colocalized with cells expressing melanoma chondroitin sulfate proteoglycan, a putative stem cell marker. Although we found LRCs in both collagen- and scaffold-based OTCs, only the scaffold-OTCs supported long-term survival and regeneration. LRCs ' short survival in collagen-OTCs was not due to loss of appropriate growth factors from fibroblasts. Instead, it was due to expression of metalloproteinases, especially matrix metalloproteinase (MMP)-2 and MMP-14, which caused collagen fragmentation, matrix degradation, and dislocation of specific basement membrane components bound to epidermal integrins. Blocking MMP activation not only abrogated MMP-dependent matrix degradation but also increased longevity of the epidermis and the LRCs in these cultures. Such findings indicate that the stem cell niche, the microenvironment surrounding and influencing the stem cell, is essential for stem cell survival and function, including long-term tissue regeneration. Disclosure of potential conflicts of interest is found at the end of this article.

摘要

人类毛囊间表皮中的干细胞仍然难以识别,主要原因是缺乏明确的标志物,并且无法对人类进行标记以识别标记保留细胞(LRCs)。在此,我们报告称,可以在用人细胞构建的器官型培养物(OTCs)中识别并定位LRCs。用碘脱氧尿苷(IdU)对培养物标记2周,然后追踪6 - 10周,发现<1%的基底细胞保留了IdU标记。整装标本显示,LRCs单独分散在表皮基底层。一些(但并非全部)LRCs与表达黑素瘤硫酸软骨素蛋白聚糖(一种假定的干细胞标志物)的细胞共定位。尽管我们在基于胶原蛋白和支架的OTCs中都发现了LRCs,但只有支架OTCs支持长期存活和再生。LRCs在胶原蛋白OTCs中的短生存期并非由于成纤维细胞中适当生长因子的丧失。相反,这是由于金属蛋白酶的表达,尤其是基质金属蛋白酶(MMP)-2和MMP-14,它们导致胶原蛋白片段化、基质降解以及与表皮整合素结合的特定基底膜成分错位。阻断MMP激活不仅消除了MMP依赖性基质降解,还延长了这些培养物中表皮和LRCs的寿命。这些发现表明,干细胞龛,即围绕并影响干细胞的微环境,对于干细胞的存活和功能(包括长期组织再生)至关重要。潜在利益冲突的披露见本文末尾。

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