Your search keyword '"Hobbs, Ryan P."' showing total 3 results

1. A role for keratin 17 during DNA damage response and tumor initiation.

Author

Nair, Raji R., Hsu, Joshua, Jacob, Justin T., Pineda, Christopher M., Hobbs, Ryan P., and Coulombe, Pierre A.

Subjects

DNA damage, INTERMEDIATE filament proteins, KERATIN, CURCUMIN, DNA repair, TREATMENT effectiveness, COMMERCIAL products

Abstract

High levels of the intermediate filament protein keratin 17 (K17) are associated with poor prognoses for several human carcinomas. Studies in mouse models have shown that K17 expression is positively associated with growth, survival, and inflammation in skin and that lack of K17 delays onset of tumorigenesis. K17 occurs in the nucleus of human and mouse tumor keratinocytes where it impacts chromatin architecture, gene expression, and cell proliferation. We report here that K17 is induced following DNA damage and promotes keratinocyte survival. The presence of nuclear K17 is required at an early stage of the double-stranded break (DSB) arm of the DNA damage and repair (DDR) cascade, consistent with its ability to associate with key DDR effectors, including A-H2A.X, 53BP1, and DNA-PKcs. Mice lacking K17 or with attenuated K17 nuclear import showed curtailed initiation in a two-step skin carcinogenesis paradigm. The impact of nuclear-localized K17 on DDR and cell survival provides a basis for the link between K17 induction and poor clinical outcomes for several human carcinomas. [ABSTRACT FROM AUTHOR]

Published

2021

2. Sam68 is required for the growth and survival of nonmelanoma skin cancer.

Author

Fu, Kai, Sun, Xin, Xia, Xue, Hobbs, Ryan P., Guo, Yajuan, Coulombe, Pierre A., and Wan, Fengyi

Subjects

SKIN cancer, NF-kappa B, DELAYED onset of disease, BASAL cell carcinoma, DNA damage, DNA repair

Abstract

Although targeting DNA repair signaling pathways has emerged as a promising therapeutic for skin cancer, the relevance of DNA damage responses (DDR) in the development and survival of nonmelanoma skin cancer (NMSC), the most common type of skin cancer, remains obscure. Here, we report that Src‐associated substrate during mitosis of 68 kDa (Sam68), an early signaling molecule in DDR, is elevated in skin tumor tissues derived from NMSC patients and skin lesions from Gli2‐transgenic mice. Downregulation of Sam68 impacts the growth and survival of human tumor keratinocytes and genetic ablation of Sam68 delays the onset of basal cell carcinomas (BCC) in Gli2‐transgenic mice. Moreover, Sam68 plays a critical role in DNA damage‐induced DNA repair and nuclear factor kappa B (NF‐κB) signaling pathways in keratinocytes, hence conferring keratinocyte sensitivity to DNA damaging agents. Together, our data reveal a novel function of Sam68 in regulating DDR in keratinocytes that is crucial for the growth and survival of NMSC. [ABSTRACT FROM AUTHOR]

Published

2019

3. Sam68/KHDRBS1-dependent NF-κB activation confers radioprotection to the colon epithelium in γ-irradiated mice.

Author

Kai Fu, Xin Sun, Wier, Eric M., Hodgson, Andrea, Hobbs, Ryan P., and Fengyi Wan

Subjects

*DNA damage, *RADIATION-protective agents, *NF-kappa B, *GENETIC toxicology, *GENE expression in mammals, *PSYCHOLOGICAL stress, *DISEASES

Abstract

Previously we reported that Src-associated-substrate-during-mitosis-of-68kDa (Sam68/KHDRBS1) is pivotal for DNA damage-stimulated NF-κB transactivation of anti-apoptotic genes (Fu et al., 2016). Here we show that Sam68 is critical for genotoxic stress-induced NF-κB activation in the γ-irradiated colon and animal and that Sam68-dependent NF-κB activation provides radioprotection to colon epithelium in vivo. Sam68 deletion diminishes γ-irradiation-triggered PAR synthesis and NF-κB activation in colon epithelial cells (CECs), thus hampering the expression of anti-apoptotic molecules in situ and facilitating CECs to undergo apoptosis in mice post wholebody γ-irradiation (WBIR). Sam68 knockout mice suffer more severe damage in the colon and succumb more rapidly from acute radiotoxicity than the control mice following WBIR. Our results underscore the critical role of Sam68 in orchestrating genotoxic stress-initiated NF-κB activation signaling in the colon tissue and whole animal and reveal the pathophysiological relevance of Sam68-dependent NF-κB activation in colonic cell survival and recovery from extrinsic DNA damage. [ABSTRACT FROM AUTHOR]

Published

2016