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Identification of a physiologic vasculogenic fibroblast state to achieve tissue repair

Author

Listed:
  • Durba Pal

    (Indiana University School of Medicine
    The Ohio State University
    Indian Institute of Technology Ropar)

  • Subhadip Ghatak

    (Indiana University School of Medicine
    The Ohio State University)

  • Kanhaiya Singh

    (Indiana University School of Medicine
    The Ohio State University)

  • Ahmed Safwat Abouhashem

    (Indiana University School of Medicine)

  • Manishekhar Kumar

    (Indiana University School of Medicine)

  • Mohamed S El Masry

    (Indiana University School of Medicine
    The Ohio State University)

  • Sujit K. Mohanty

    (Indiana University School of Medicine)

  • Ravichand Palakurti

    (Indiana University School of Medicine)

  • Yashika Rustagi

    (Indiana University School of Medicine)

  • Saba Tabasum

    (Indiana University School of Medicine)

  • Dolly K. Khona

    (Indiana University School of Medicine
    The Ohio State University)

  • Savita Khanna

    (Indiana University School of Medicine
    The Ohio State University)

  • Sedat Kacar

    (Indiana University School of Medicine)

  • Rajneesh Srivastava

    (Indiana University School of Medicine)

  • Pramod Bhasme

    (Indiana University School of Medicine)

  • Sumit S. Verma

    (Indiana University School of Medicine)

  • Edward Hernandez

    (Indiana University School of Medicine)

  • Anu Sharma

    (Indiana University School of Medicine)

  • Diamond Reese

    (Indiana University School of Medicine)

  • Priyanka Verma

    (Indiana University School of Medicine)

  • Nandini Ghosh

    (Indiana University School of Medicine
    The Ohio State University)

  • Mahadeo Gorain

    (Indiana University School of Medicine)

  • Jun Wan

    (Indiana University School of Medicine)

  • Sheng Liu

    (Indiana University School of Medicine)

  • Yunlong Liu

    (Indiana University School of Medicine)

  • Natalia Higuita Castro

    (The Ohio State University)

  • Surya C. Gnyawali

    (Indiana University School of Medicine
    The Ohio State University)

  • William Lawrence

    (The Ohio State University)

  • Jordan Moore

    (The Ohio State University
    The Ohio State University)

  • Daniel Gallego Perez

    (The Ohio State University
    The Ohio State University)

  • Sashwati Roy

    (Indiana University School of Medicine
    The Ohio State University)

  • Mervin C. Yoder

    (Indiana University School of Medicine)

  • Chandan K. Sen

    (Indiana University School of Medicine
    The Ohio State University
    The Ohio State University)

Abstract

Tissue injury to skin diminishes miR-200b in dermal fibroblasts. Fibroblasts are widely reported to directly reprogram into endothelial-like cells and we hypothesized that miR-200b inhibition may cause such changes. We transfected human dermal fibroblasts with anti-miR-200b oligonucleotide, then using single cell RNA sequencing, identified emergence of a vasculogenic subset with a distinct fibroblast transcriptome and demonstrated blood vessel forming function in vivo. Anti-miR-200b delivery to murine injury sites likewise enhanced tissue perfusion, wound closure, and vasculogenic fibroblast contribution to perfused vessels in a FLI1 dependent manner. Vasculogenic fibroblast subset emergence was blunted in delayed healing wounds of diabetic animals but, topical tissue nanotransfection of a single anti-miR-200b oligonucleotide was sufficient to restore FLI1 expression, vasculogenic fibroblast emergence, tissue perfusion, and wound healing. Augmenting a physiologic tissue injury adaptive response mechanism that produces a vasculogenic fibroblast state change opens new avenues for therapeutic tissue vascularization of ischemic wounds.

Suggested Citation

  • Durba Pal & Subhadip Ghatak & Kanhaiya Singh & Ahmed Safwat Abouhashem & Manishekhar Kumar & Mohamed S El Masry & Sujit K. Mohanty & Ravichand Palakurti & Yashika Rustagi & Saba Tabasum & Dolly K. Kho, 2023. "Identification of a physiologic vasculogenic fibroblast state to achieve tissue repair," Nature Communications, Nature, vol. 14(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-36665-z
    DOI: 10.1038/s41467-023-36665-z
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