Literature DB >> 26434982

Age-associated inflammation connects RAS-induced senescence to stem cell dysfunction and epidermal malignancy.

L Golomb1, A Sagiv1, I S Pateras2, A Maly3, V Krizhanovsky1, V G Gorgoulis4,5,6,7, M Oren1, A Ben-Yehuda3.   

Abstract

Aging is the single biggest risk factor for malignant transformation. Among the most common age-associated malignancies are non-melanoma skin cancers, comprising the most common types of human cancer. Here we show that mutant H-Ras activation in mouse epidermis, a frequent event in cutaneous squamous cell carcinoma (SCC), elicits a differential outcome in aged versus young mice. Whereas H-Ras activation in the young skin results in hyperplasia that is mainly accompanied by rapid hair growth, H-Ras activation in the aged skin results in more dysplasia and gradual progression to in situ SCC. Progression is associated with increased inflammation, pronounced accumulation of immune cells including T cells, macrophages and mast cells as well as excessive cell senescence. We found not only an age-dependent increase in expression of several pro-inflammatory mediators, but also activation of a strong anti-inflammatory response involving enhanced IL4/IL10 expression and immune skewing toward a Th2 response. In addition, we observed an age-dependent increase in the expression of Pdl1, encoding an immune suppressive ligand that promotes cancer immune evasion. Moreover, upon switching off oncogenic H-Ras activity, young but not aged skin regenerates successfully, suggesting a failure of the aged epidermal stem cells to repair damaged tissue. Our findings support an age-dependent link between accumulation of senescent cells, immune infiltration and cancer progression, which may contribute to the increased cancer risk associated with old age.

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Year:  2015        PMID: 26434982      PMCID: PMC4648323          DOI: 10.1038/cdd.2015.21

Source DB:  PubMed          Journal:  Cell Death Differ        ISSN: 1350-9047            Impact factor:   15.828


  74 in total

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  18 in total

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Review 2.  When Wounds Are Good for You: The Regenerative Capacity of Fractional Resurfacing and Potential Utility in Chronic Wound Prevention.

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Review 4.  Two-Step Senescence-Focused Cancer Therapies.

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6.  Type XVII collagen coordinates proliferation in the interfollicular epidermis.

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Review 10.  Cancer and Aging - the Inflammatory Connection.

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