AI Article Synopsis

  • Recent studies indicate that bone marrow-derived cells help with wound healing in skin by producing collagen type I, but their exact role in the process is still unclear.
  • Researchers used transgenic mice with specific genes linked to fluorescent and luciferase markers to track these collagen-producing cells during skin wound healing.
  • Findings showed that while most collagen production during healing comes from resident skin cells, some CD45-positive cells from bone marrow do contribute to collagen production in response to bleomycin, indicating a partial role of bone marrow cells in skin repair.

Article Abstract

Recent studies show that bone marrow (BM)-derived cells migrating into a dermal wound promote healing by producing collagen type I. However, their contribution to the repair process has not been fully verified yet. It is also unclear whether BM-derived cells participate in dermal fibrogenesis. We have addressed these issues using transgenic mice that harbor tissue-specific enhancer/promoter sequences of α2(I) collagen gene linked to either enhanced green fluorescent protein (COL/EGFP) or the luciferase (COL/LUC) reporter gene. Following dermal excision or subcutaneous bleomycin administration, a large number of EGFP-positive collagen-producing cells appeared in the dermis of COL/EGFP reporter mice. When wild-type mice were transplanted with BM cells from transgenic COL/EGFP animals and subjected to dermal excision, no EGFP-positive BM-derived collagen-producing cells were detected throughout the repair process. Luciferase assays of dermal tissues from COL/LUC recipient mice also excluded collagen production by BM-derived cells during dermal excision healing. In contrast, a limited but significant number of CD45-positive collagen-producing cells migrated from BM following bleomycin injection. These results indicate that resident cells in the skin are the major source of de novo collagen deposition in both physiological and pathological conditions, whereas BM-derived cells participate, in part, in collagen production during dermal fibrogenesis.

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Source
http://dx.doi.org/10.1038/jid.2010.314DOI Listing

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