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成年小鼠角膜上皮中的谱系追踪支持角膜缘上皮干细胞假说,即干细胞存在间歇性静止期。

Lineage tracing in the adult mouse corneal epithelium supports the limbal epithelial stem cell hypothesis with intermittent periods of stem cell quiescence.

作者信息

Dorà Natalie J, Hill Robert E, Collinson J Martin, West John D

机构信息

Centre for Integrative Physiology, University of Edinburgh Medical School, Hugh Robson Building, George Square, Edinburgh EH8 9XD, UK.

Medical and Developmental Genetics Section, MRC Human Genetics Unit, MRC IGMM, University of Edinburgh, Western General Hospital, Crewe Road, Edinburgh, EH4 2XU, UK.

出版信息

Stem Cell Res. 2015 Nov;15(3):665-677. doi: 10.1016/j.scr.2015.10.016. Epub 2015 Oct 28.

Abstract

The limbal epithelial stem cell (LESC) hypothesis proposes that LESCs in the corneal limbus maintain the corneal epithelium both during normal homeostasis and wound repair. The alternative corneal epithelial stem cell (CESC) hypothesis proposes that LESCs are only involved in wound repair and CESCs in the corneal epithelium itself maintain the corneal epithelium during normal homeostasis. We used tamoxifen-inducible, CreER-loxP lineage tracing to distinguish between these hypotheses. Clones of labelled cells were induced in adult CAGG-CreER;R26R-LacZ reporter mice and their distributions analysed after different chase periods. Short-lived clones, derived from labelled transient amplifying cells, were shed during the chase period and long-lived clones, derived from stem cells, expanded. At 6 weeks, labelled clones appeared at the periphery, extended centripetally as radial stripes and a few reached the centre by 14 weeks. Stripe numbers depended on the age of tamoxifen treatment. Stripes varied in length, some were discontinuous, few reached the centre and almost half had one end at the limbus. Similar stripes extended across the cornea in CAGG-CreER;R26R-mT/mG reporter mice. The distributions of labelled clones are inconsistent with the CESC hypothesis and support the LESC hypothesis if LESCs cycle between phases of activity and quiescence, each lasting several weeks.

摘要

角膜缘上皮干细胞(LESC)假说提出,角膜缘的LESC在正常稳态和伤口修复过程中均维持角膜上皮。另一种角膜上皮干细胞(CESC)假说则提出,LESC仅参与伤口修复,而角膜上皮自身的CESC在正常稳态期间维持角膜上皮。我们使用他莫昔芬诱导的CreER-loxP谱系追踪来区分这些假说。在成年CAGG-CreER;R26R-LacZ报告基因小鼠中诱导标记细胞的克隆,并在不同的追踪期后分析其分布。源自标记的短暂扩增细胞的短期克隆在追踪期内脱落,而源自干细胞的长期克隆则扩增。6周时,标记的克隆出现在周边,以放射状条纹向中心延伸,到14周时少数到达中心。条纹数量取决于他莫昔芬处理的年龄。条纹长度各异,有些不连续,少数到达中心,几乎一半的一端位于角膜缘。在CAGG-CreER;R26R-mT/mG报告基因小鼠中,类似的条纹横跨角膜延伸。如果LESC在活跃期和静止期之间循环,每个阶段持续数周,那么标记克隆的分布与CESC假说不一致,而支持LESC假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/305f/4686565/a7c4d80e3e2e/fx1.jpg

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