AI Article Synopsis

  • Dysregulation in wound healing can lead to various skin issues like ulcers and different types of scars, linked to changes in the activity of healing components.
  • The collagen type V alpha 2 gene and TGF-β, a key factor in healing processes, are crucial in inflammation and collagen production, with disrupted TGF-β signaling contributing to abnormal scars.
  • A study of 71 female patients post-Caesarean section found no significant genetic differences in the occurrence of pathological scarring, suggesting further research with larger groups is needed to clarify the roles of specific gene variants.

Article Abstract

Dysregulation in the cutaneous wound-healing process is a consequence of alterations in the efficiency and activity of the various components involved in the healing process. This dysregulation may result in various clinical appearances of a lesion, such as skin ulcers, keloids, hypertrophic and atrophic scars. The collagen type V alpha 2 () gene provides a template for a component of type V collagen, found primarily within the skin basement membrane. Transforming growth factor (TGF)-β is involved in inflammation, angiogenesis, proliferation of fibroblasts, collagen synthesis and extracellular matrix remodeling. Hypertrophic scar fibroblasts possess a disrupted expression pattern of the TGF-β signaling compared to normal healing, while an increased TGF-β signaling reduces the epidermal proliferation rate, triggering atrophic scarring. In the present study, 71 female patients who had undergone planned Caesarean section, without postoperative complications, were examined. These patients were clinically and molecularly evaluated after developing scars in order to determine the role of TGF-β1 (rs201700967 and rs200230083) and COL5A2 (rs369072636) in pathological scarring. Clinical scar evaluation was carried out using SCAR and POSAS scales and genotyping was performed by RT-PCR. No statistical differences were found between the subgroups regarding the genotype and the pathological scarring, since all the patients included were wild-type allele carriers. Further investigations and a more representative study group may highlight the involvement of COL5A2 and TGF-β1 single nucleotide variants in pathological scarring.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8355659PMC
http://dx.doi.org/10.3892/etm.2021.10501DOI Listing

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