AI Article Synopsis

  • The limbus, the area connecting the cornea and conjunctiva, may protect against abnormal blood vessel growth in the cornea, but how it does this isn't fully understood.
  • Researchers studied ABCB5, a marker for limbal epithelial stem cells (LESCs), to explore its role in corneal blood vessel development and found it has different effects in young and adult mice.
  • The study revealed that ABCB5+ cells can inhibit blood vessel growth during development but promote it during inflammation in adults, suggesting a complex role that could be important for therapies aimed at preventing blindness.

Article Abstract

The limbus, the vascularized junction between the cornea and conjunctiva, is thought to function as a barrier against corneal neovascularization. However, the exact mechanisms regulating this remain unknown. In this study, the limbal epithelial stem cell (LESC) marker ABCB5 was used to investigate the role of LESCs in corneal neovascularization. In an ABCB5KO model, a mild but significant increase of limbal lymphatic and blood vascular network complexity was observed in developing mice (4 weeks) but not in adult mice. Conversely, when using a cornea suture model, the WT animals exhibited a mild but significant increase in the number of lymphatic vessel sprouts compared to the ABCB5KO, suggesting a contextual anti-lymphangiogenic effect of ABCB5 on the limbal vasculature during development, but a pro-lymphangiogenic effect under inflammatory challenge in adulthood. In addition, conditioned media from ABCB5-positive cultured human limbal epithelial cells (ABCB5+) stimulated human blood and lymphatic endothelial cell proliferation and migration. Finally, a proteomic analysis demonstrated ABCB5+ cells have a pro(lymph)angiogenic as well as an anti-inflammatory profile. These data suggest a novel dual, context-dependent role of ABCB5+ LESCs, inhibiting developmental but promoting inflammatory (lymph)angiogenesis in adulthood and exerting anti-inflammatory effects. These findings are of high clinical relevance in relation to LESC therapy against blindness.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10341195PMC
http://dx.doi.org/10.3390/cells12131731DOI Listing

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