Project Details
Projekt
Role of ABCB5+ MSCs in niche homeostasis and repair after trauma (C05)
Subject Area
Dermatology
Cell Biology
Cell Biology
Term
since 2015
Project identifier
Deutsche Forschungsgemeinschaft (DFG) - Project number 251293561
We found that MSCs sense and shape their neighborhood at different trauma sites with accelerated tissue repair. Unexpectedly, combined TXT and skin trauma led to accelerated wound healing of the skin. Thus, the overarching hypothesis is that in vivo priming of MSCs in their skin niches results in improved healing. This is due to a sustained epigenetic memory of the priming event which upon wounding unleashes regenerative signaling events faster. Therefore, we explore whether 1) combined trauma (TXT, skin) primes MSCs and distinct fibroblast lineages with improved skin wound healing, 2) trauma of other organs (brain, bone) enforces an adaptive skin response and enhances MSC functionality; and 3) priming of resident skin MSCs with S100A8/9 or laser treatment enforces a subsequent regenerative wound healing.
DFG Programme
Collaborative Research Centres
Subproject of
SFB 1149:
Danger Response, Disturbance Factors and Regenerative Potential after Acute Trauma
Applicant Institution
Universität Ulm
Project Head
Professorin Dr. Karin Scharffetter-Kochanek
