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Langerhans Cells Facilitate Epithelial DNA Damage and Squamous Cell Carcinoma

  作者 Modi, BG; Neustadter, J; Binda, E; Lewis, J; Filler, RB; Roberts, SJ; Kwong, BY; Reddy, S; Overton, JD; Galan, A; Tigelaar, R; Cai, LN; Fu, P; Shlomchik, M; Kaplan, DH; Hayday, A; Girardi, M  
  选自 期刊  Science;  卷期  2012年335-6064;  页码  104-108  
  关联知识点  
 

[摘要]Polyaromatic hydrocarbons (PAHs) are prevalent, potent carcinogens, and 7,12-dimethylbenz[a]anthracene (DMBA) is a model PAH widely used to study tumorigenesis. Mice lacking Langerhans cells (LCs), a signatory epidermal dendritic cell (DC), are protected from cutaneous chemical carcinogenesis, independent of T cell immunity. Investigation of the underlying mechanism revealed that LC-deficient skin was relatively resistant to DMBA-induced DNA damage. LCs efficiently metabolized DMBA to DMBA-trans-3,4-diol, an intermediate proximal to oncogenic Hras mutation, and DMBA-treated LC-deficient skin contained significantly fewer Hras mutations. Moreover, DMBA-trans-3,4-diol application bypassed tumor resistance in LC-deficient mice. Additionally, the genotoxic impact of DMBA on human keratinocytes was significantly increased by prior incubation with human-derived LC. Thus, tissue-associated DC can enhance chemical carcinogenesis via PAH metabolism, highlighting the complex relation between immune cells and carcinogenesis.

 
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