Strengthening the skin with topical delivery of keratinocyte growth factor-1 using a novel DNA plasmid.

利用新型DNA质粒局部递送角质细胞生长因子-1,从而增强皮肤

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作者:Dou Chunqing, Lay Frank, Ansari Amir Mehdi, Rees Donald J, Ahmed Ali Karim, Kovbasnjuk Olga, Matsangos Aerielle E, Du Junkai, Hosseini Sayed Mohammad, Steenbergen Charles, Fox-Talbot Karen, Tabor Aaron T, Williams James A, Liu Lixin, Marti Guy P, Harmon John W
Fragile skin, susceptible to decubitus ulcers and incidental trauma, is a problem particularly for the elderly and for those with spinal cord injury. Here, we present a simple approach to strengthen the skin by the topical delivery of keratinocyte growth factor-1 (KGF-1) DNA. In initial feasibility studies with the novel minimalized, antibiotic-free DNA expression vector, NTC8385-VA1, the reporter genes luciferase and enhanced green fluorescent protein were delivered. Transfection was documented when luciferase expression significantly increased after transfection. Microscopic imaging of enhanced green fluorescent protein-transfected skin showed green fluorescence in hair follicles, hair shafts, and dermal and superficial epithelial cells. With KGF-1 transfection, KGF-1 mRNA level and protein production were documented with quantitative reverse transcriptase-polymerase chain reaction and immunohistochemistry, respectively. Epithelial thickness of the transfected skin in the KGF group was significantly increased compared with the control vector group (26 ± 2 versus 16 ± 4 µm) at 48 hours (P = 0.045). Dermal thickness tended to be increased in the KGF group (255 ± 36 versus 162 ± 16 µm) at 120 hours (P = 0.057). Biomechanical assessment showed that the KGF-1-treated skin was significantly stronger than control vector-transfected skin. These findings indicate that topically delivered KGF-1 DNA plasmid can increase epithelial thickness and strength, demonstrating the potential of this approach to restore compromised skin.

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