Wound healing is a complex process involving multiple cellular events, including cell proliferation, migration, and tissue remodeling. ADAM12 (a disintegrin and metalloprotease 12) is a membrane-anchored metalloprotease, which has been implicated in activation/inactivation of growth factors that play an important role in wound healing, including heparin-binding EGF-like growth factor (HB-EGF) and insulin growth factor (IGF) binding proteins. Here we report that expression of ADAM12 is fivefold up-regulated in the non-healing edge of chronic ulcers compared to healthy skin, based on microarrays of biopsies taken from five patients and from healthy controls (p=0.013). The increase in ADAM12 expression in chronic ulcers was confirmed by quantitative real time-PCR. Moreover, immunohistochemical analysis demonstrated a pronounced increase in the membranous and intracellular signal for ADAM12 in the epidermis of chronic wounds compared to healthy skin. These findings, coupled with our previous observations that lack of keratinocyte migration contributes to the pathogenesis of chronic ulcers, prompted us to evaluate how the absence of ADAM12 affects the migration of mouse keratinocytes. Skin explants from newborn ADAM12−/− or WT mice were used to quantify keratinocyte migration out of the explants over a period of seven days. We found a statistically significant increase in the migration of ADAM12−/− keratinocytes compared to WT control (P=.0014) samples. Taken together, the upregulation of ADAM12 in chronic wounds, and the increased migration of keratinocytes in the absence of ADAM12 suggest that ADAM12 is an important mediator of wound healing. We hypothesize that increased expression of ADAM12 in chronic wounds impairs wound healing through the inhibition of keratinocyte migration, and that topical ADAM12 inhibitors may therefore prove useful for the treatment of chronic wounds.
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