Molecular Markers in Patients with Chronic Wounds to Guide Surgical Debridement

清创术(牙科) 伤口愈合 医学 病理 纤维化 活检 基因表达谱 慢性伤口 基因表达 外科 生物 基因 生物化学
作者
Harold Brem,Olivera Stojadinović,Robert F. Diegelmann,Hyacinth Entero,Brian Lee,Irena Pastar,Michael Golinko,Harvey S. Rosenberg,Marjana Tomic‐Canic
出处
期刊:Molecular Medicine [BioMed Central]
卷期号:13 (1-2): 30-39 被引量:338
标识
DOI:10.2119/2006-00054.brem
摘要

Chronic wounds, such as venous ulcers, are characterized by physiological impairments manifested by delays in healing, resulting in severe morbidity. Surgical debridement is routinely performed on chronic wounds because it stimulates healing. However, procedures are repeated many times on the same patient because, in contrast to tumor excision, there are no objective biological/molecular markers to guide the extent of debridement. To develop bioassays that can potentially guide surgical debridement, we assessed the pathogenesis of the patients' wound tissue before and after wound debridement. We obtained biopsies from three patients at two locations, the nonhealing edge (prior to debridement) and the adjacent, nonulcerated skin of the venous ulcers (post debridement), and evaluated their histology, biological response to wounding (migration) and gene expression profile. We found that biopsies from the nonhealing edges exhibit distinct pathogenic morphology (hyperproliferative/hyperkeratotic epidermis; dermal fibrosis; increased procollagen synthesis). Fibroblasts deriving from this location exhibit impaired migration in comparison to the cells from adjacent nonulcerated biopsies, which exhibit normalization of morphology and normal migration capacity. The nonhealing edges have a specific, identifiable, and reproducible gene expression profile. The adjacent nonulcerated biopsies have their own distinctive reproducible gene expression profile, signifying that particular wound areas can be identified by gene expression profiling. We conclude that chronic ulcers contain distinct subpopulations of cells with different capacity to heal and that gene expression profiling can be utilized to identify them. In the future, molecular markers will be developed to identify the nonimpaired tissue, thereby making surgical debridement more accurate and more efficacious.
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