María Isabel Cerezo-Guisado scite author profile

of the TGFβ pathway and for faster wound healing in the AhRnull neo-epithelium. Consistently, a TGFβ neutralizing antibody decreased keratinocyte migration in culture and halted reepithelialization in Ahr -/-mice. Moreover, in vivo treatment with an antisense oligonucleotide for AhR increased TGFβ signaling and improved re-epithelialization in wounds of wild-type mice. These data indicate that AhR is relevant for wound repair and suggest that AhR downmodulation might be a potential new tool for the treatment of chronic, surgical or accidental wounds. Supplementary material available online at

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Implication of Akt, ERK1/2 and alternative p38MAPK signalling pathways in human colon cancer cell apoptosis induced by green tea EGCG

Cerezo-Guisado

Zur

Lorenzo

et al. 2015

Food and Chemical Toxicology

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p38 MAPK Down-regulates Fibulin 3 Expression through Methylation of Gene Regulatory Sequences

Arechederra¹,

Priego²,

Vázquez-Carballo³

et al. 2015

Journal of Biological Chemistry

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Background: p38␣ MAPK regulates migration/invasion. Results: p38␣ induces hypermethylation of Fibulin 3 gene regulatory sequences leading to Fibulin 3 down-regulation. This contributes to regulate migration and invasion in MEFs and HCT116 cells. Conclusion: p38␣ down-regulates fibulin 3 expression through promoter methylation to control p38␣-mediated migration and invasion. Significance: To understand the function of new p38␣ targets in migration/invasion and tumorigenesis.

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Evidence of p38γ and p38δ involvement in cell transformation processes

Cerezo-Guisado

Reino

Rémy

et al. 2011

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The p38 mitogen-activated protein kinase (p38MAPK) signal transduction pathway is an important regulator of cell processes, whose deregulation leads to the development and progression of cancer. Defining the role of each p38MAPK family member in these processes has been difficult. To date, most studies of the p38MAPK pathways focused on function of the p38α isoform, which is widely considered to negatively regulate malignant transformation; nonetheless, few reports address the p38γ and p38δ isoforms. Here, we used embryonic fibroblasts derived from mice lacking p38γ or p38δ and show evidence that these isoforms participate in several processes involved in malignant transformation. We observed that lack of either p38γ or p38δ increased cell migration and metalloproteinase-2 secretion, whereas only p38δ deficiency impaired cell contact inhibition. In addition, lack of p38γ in K-Ras-transformed fibroblasts led to increased cell proliferation as well as tumorigenesis both in vitro and in vivo. Our results indicate that p38γ and p38δ have a role in the suppression of tumor development.

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