RhoB Promotes Cancer Initiation by Protecting Keratinocytes from UVB-Induced Apoptosis but Limits Tumor Aggressiveness

Meyer, Nicolas; Peyret-Lacombe, Alexis; Canguilhem, Bruno; Medale-Giamarchi, Claire; Mamouni, Kenza; Cristini, Agnese; Monferran, Sylvie; Lamant, Laurence; Filleron, Thomas; Pradines, Anne; Sordet, Olivier; Favre, Gilles

doi:10.1038/jid.2013.278

Cited by 29 publications

(20 citation statements)

References 34 publications

(47 reference statements)

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“…6). We recently reported that RhoB-deficient human skin tumors also have elevated ␥H2AX levels compared to RhoB-proficient tumors (63). Hence, our findings suggest that loss of RhoB could promote oncogenesis by increasing DSB-mediated genomic instability.…”

Section: Discussionmentioning

confidence: 53%

RhoB Promotes γH2AX Dephosphorylation and DNA Double-Strand Break Repair

Mamouni

Cristini

Guirouilh‐Barbat

et al. 2014

Molecular and Cellular Biology

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c Unlike other Rho GTPases, RhoB is rapidly induced by DNA damage, and its expression level decreases during cancer progression. Because inefficient repair of DNA double-strand breaks (DSBs) can lead to cancer, we investigated whether camptothecin, an anticancer drug that produces DSBs, induces RhoB expression and examined its role in the camptothecin-induced DNA damage response. We show that in camptothecin-treated cells, DSBs induce RhoB expression by a mechanism that depends notably on Chk2 and its substrate HuR, which binds to RhoB mRNA and protects it against degradation. RhoB-deficient cells fail to dephosphorylate ␥H2AX following camptothecin removal and show reduced efficiency of DSB repair by homologous recombination. These cells also show decreased activity of protein phosphatase 2A (PP2A), a phosphatase for ␥H2AX and other DNA damage and repair proteins. Thus, we propose that DSBs activate a Chk2-HuR-RhoB pathway that promotes PP2A-mediated dephosphorylation of ␥H2AX and DSB repair. Finally, we show that RhoB-deficient cells accumulate endogenous ␥H2AX and chromosomal abnormalities, suggesting that RhoB loss increases DSB-mediated genomic instability and tumor progression.

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Section: Discussionmentioning

confidence: 53%

RhoB Promotes γH2AX Dephosphorylation and DNA Double-Strand Break Repair

Mamouni

Cristini

Guirouilh‐Barbat

et al. 2014

Molecular and Cellular Biology

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“…Therefore, correlation of experimental observations made in murine models and in human tissue is of prime importance for demonstrating relevance to human disease. Mouse models, most notably those employing the SKH-1 hairless immunocompetent mouse, proved to be useful and allowed the identification of critical molecular and biologic changes that trigger skin tumour development [[14], [15]]. They are also commonly used to assess the preclinical efficacy of novel treatments on SCC however, rather than on AK lesions [[10]; [9], [8], [16]].…”

Section: Discussionmentioning

confidence: 99%

Actinic keratosis modelling in mice: A translational study

et al. 2017

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BackgroundActinic keratoses (AK) are pre-malignant cutaneous lesions caused by prolonged exposure to ultraviolet radiation. As AKs lesions are generally accepted to be the initial lesions in a disease continuum that progresses to squamous cell carcinoma (SCC), AK lesions have to be treated. They are also the second most common reason for visits to the dermatologist. Several treatments are available but their efficacy still needs to be improved. The UV-B-induced KA lesion mouse model is used in preclinical studies to assess the efficacy of novel molecules, even though it is often more representative of advanced AK or SCC.ObjectivesHere we report on a translational study, comparing the various stages of AK development in humans and in the UV-B irradiated mouse model, as well as the optimization of photograph acquisition of AK lesions on mouse skin.MethodsHuman and mouse skin lesions were analysed by histology and immunohistochemistry. Mouse lesions were also assessed using a digital dermatoscope.ResultsAn histological and phenotypic analysis, including p53, Ki67 and CD3 expression detection, performed on human and mouse AK lesions, shows that overall AK modelling in mice is relevant in the clinical situation. Some differences are observed, such as disorganization of keratinocytes of the basal layer and a number of atypical nuclei which are more numerous in human AK, whereas much more pronounced acanthosis is observed in skin lesion in mice. Thanks to this translational study, we are able to select appropriate experimental conditions for establishing either early or advanced stage AK or an SCC model. Furthermore, we optimized photograph acquisition of AK lesions on mouse skin by using a digital dermatoscope which is also used in clinics and allows reproducible photograph acquisition for further reliable assessment of mouse lesions. Use of this camera is illustrated through a pharmacological study assessing the activity of CARAC®.ConclusionThese data demonstrate that this mouse model of UV-B-induced skin lesions is predictive for the identification of novel therapeutic treatments for both early and advanced stages of the disease.

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“…For example, early studies revealed that ablation of the RhoB gene in mice (a gene deleted in many human cancers) enhances carcinogen-induced skin cancer (15). Rhob −/− mice are less prone to form squamous cell carcinomas following chronic exposure to UVB, arguing that RhoB favors early stages of oncogenesis, however RhoB could also limit the progression to highly aggressive tumors (16). Deletion of the RhoC gene in the MMTV-PyVT mouse model of breast cancer significantly reduces lung metastasis of mammary tumors (17).…”

Section: Distinctive Roles For Rho Gtpases In Cancer Initiation and Pmentioning

confidence: 99%

The Rac GTPase in Cancer: From Old Concepts to New Paradigms

2017

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Rho family GTPases are critical regulators of cellular functions that play important roles in cancer progression. Aberrant activity of Rho small G-proteins, particularly Rac1 and their regulators, is a hallmark of cancer, and contributes to the tumorigenic and metastatic phenotypes of cancer cells. This review examines the multiple mechanisms leading to Rac1 hyperactivation, particularly focusing on emerging paradigms that involve gain-of-function mutations in Rac and guanine nucleotide exchange factors (GEFs), defects in Rac1 degradation, and mislocalization of Rac signaling components. The unexpected pro-oncogenic functions of Rac GTPase activating proteins (GAPs) also challenged the dogma that these negative Rac regulators solely act as tumor suppressors. The potential contribution of Rac hyperactivation to resistance to anti-cancer agents, including targeted therapies, as well as to the suppression of anti-tumor immune response, highlights the critical need to develop therapeutic strategies to target the Rac pathway in a clinical setting.

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RhoB Promotes Cancer Initiation by Protecting Keratinocytes from UVB-Induced Apoptosis but Limits Tumor Aggressiveness

Cited by 29 publications

References 34 publications

RhoB Promotes γH2AX Dephosphorylation and DNA Double-Strand Break Repair

RhoB Promotes γH2AX Dephosphorylation and DNA Double-Strand Break Repair

Actinic keratosis modelling in mice: A translational study

The Rac GTPase in Cancer: From Old Concepts to New Paradigms

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