MDM4 is a key therapeutic target in cutaneous melanoma

Agnieszka Gembarska; Flavie Luciani; Clare Grace Fedele; Elizabeth A Russell; Michael Dewaele; Stephanie Villar; Aleksandra Zwolinska; Sue Haupt; Job de Lange; Dana Yip; James Goydos; Jody Haigh; Yagl Haupt; Lionel Larue; Aart Jochemsen; Hubing Shi; Gatien Moriceau; Roger S Lo; Ghanem Ghanem; Mark Shackleton; Federico Bernal; Jean-Christophe Marine

doi:10.1038/nm.2863

MDM4 is a key therapeutic target in cutaneous melanoma

Agnieszka Gembarska, Flavie Luciani, Clare Grace Fedele, Elizabeth A Russell, Michael Dewaele, Stephanie Villar, Aleksandra Zwolinska, Sue Haupt, Job de Lange, Dana Yip, James Goydos, Jody Haigh, Yagl Haupt, Lionel Larue, Aart Jochemsen, Hubing Shi, Gatien Moriceau, Roger S Lo, Ghanem Ghanem, Mark ShackletonFederico Bernal, Jean-Christophe Marine

Biochemistry & Molecular Biology

Research output: Contribution to journal › Article › Research › peer-review

253 Citations (Scopus)

Abstract

The inactivation of the p53 tumor suppressor pathway, which often occurs through mutations in TP53 (encoding tumor protein 53) is a common step in human cancer. However, in melanoma-a highly chemotherapy-resistant disease-TP53 mutations are rare, raising the possibility that this cancer uses alternative ways to overcome p53-mediated tumor suppression. Here we show that Mdm4 p53 binding protein homolog (MDM4), a negative regulator of p53, is upregulated in a substantial proportion ( approximately 65 ) of stage I-IV human melanomas and that melanocyte-specific Mdm4 overexpression enhanced tumorigenesis in a mouse model of melanoma induced by the oncogene Nras. MDM4 promotes the survival of human metastatic melanoma by antagonizing p53 proapoptotic function. Notably, inhibition of the MDM4-p53 interaction restored p53 function in melanoma cells, resulting in increased sensitivity to cytotoxic chemotherapy and to inhibitors of the BRAF (V600E) oncogene. Our results identify MDM4 as a key determinant of impaired p53 function in human melanoma and designate MDM4 as a promising target for antimelanoma combination therapy.

Original language	English
Pages (from-to)	1239-1247
Number of pages	9
Journal	Nature Medicine
Volume	18
Issue number	8
DOIs	https://doi.org/10.1038/nm.2863
Publication status	Published - 2012

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Cite this

Gembarska, A., Luciani, F., Fedele, C. G., Russell, E. A., Dewaele, M., Villar, S., Zwolinska, A., Haupt, S., de Lange, J., Yip, D., Goydos, J., Haigh, J., Haupt, Y., Larue, L., Jochemsen, A., Shi, H., Moriceau, G., Lo, R. S., Ghanem, G., ... Marine, J.-C. (2012). MDM4 is a key therapeutic target in cutaneous melanoma. Nature Medicine, 18(8), 1239-1247. https://doi.org/10.1038/nm.2863

@article{cec9ed8d589347a3abc2ac5b2993e68d,

title = "MDM4 is a key therapeutic target in cutaneous melanoma",

abstract = "The inactivation of the p53 tumor suppressor pathway, which often occurs through mutations in TP53 (encoding tumor protein 53) is a common step in human cancer. However, in melanoma-a highly chemotherapy-resistant disease-TP53 mutations are rare, raising the possibility that this cancer uses alternative ways to overcome p53-mediated tumor suppression. Here we show that Mdm4 p53 binding protein homolog (MDM4), a negative regulator of p53, is upregulated in a substantial proportion ( approximately 65 ) of stage I-IV human melanomas and that melanocyte-specific Mdm4 overexpression enhanced tumorigenesis in a mouse model of melanoma induced by the oncogene Nras. MDM4 promotes the survival of human metastatic melanoma by antagonizing p53 proapoptotic function. Notably, inhibition of the MDM4-p53 interaction restored p53 function in melanoma cells, resulting in increased sensitivity to cytotoxic chemotherapy and to inhibitors of the BRAF (V600E) oncogene. Our results identify MDM4 as a key determinant of impaired p53 function in human melanoma and designate MDM4 as a promising target for antimelanoma combination therapy.",

author = "Agnieszka Gembarska and Flavie Luciani and Fedele, {Clare Grace} and Russell, {Elizabeth A} and Michael Dewaele and Stephanie Villar and Aleksandra Zwolinska and Sue Haupt and {de Lange}, Job and Dana Yip and James Goydos and Jody Haigh and Yagl Haupt and Lionel Larue and Aart Jochemsen and Hubing Shi and Gatien Moriceau and Lo, {Roger S} and Ghanem Ghanem and Mark Shackleton and Federico Bernal and Jean-Christophe Marine",

year = "2012",

doi = "10.1038/nm.2863",

language = "English",

volume = "18",

pages = "1239--1247",

journal = "Nature Medicine",

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Gembarska, A, Luciani, F, Fedele, CG, Russell, EA, Dewaele, M, Villar, S, Zwolinska, A, Haupt, S, de Lange, J, Yip, D, Goydos, J, Haigh, J, Haupt, Y, Larue, L, Jochemsen, A, Shi, H, Moriceau, G, Lo, RS, Ghanem, G, Shackleton, M, Bernal, F & Marine, J-C 2012, 'MDM4 is a key therapeutic target in cutaneous melanoma', Nature Medicine, vol. 18, no. 8, pp. 1239-1247. https://doi.org/10.1038/nm.2863

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T1 - MDM4 is a key therapeutic target in cutaneous melanoma

AU - Gembarska, Agnieszka

AU - Luciani, Flavie

AU - Fedele, Clare Grace

AU - Russell, Elizabeth A

AU - Dewaele, Michael

AU - Villar, Stephanie

AU - Zwolinska, Aleksandra

AU - Haupt, Sue

AU - de Lange, Job

AU - Yip, Dana

AU - Goydos, James

AU - Haigh, Jody

AU - Haupt, Yagl

AU - Larue, Lionel

AU - Jochemsen, Aart

AU - Shi, Hubing

AU - Moriceau, Gatien

AU - Lo, Roger S

AU - Ghanem, Ghanem

AU - Shackleton, Mark

AU - Bernal, Federico

AU - Marine, Jean-Christophe

PY - 2012

Y1 - 2012

N2 - The inactivation of the p53 tumor suppressor pathway, which often occurs through mutations in TP53 (encoding tumor protein 53) is a common step in human cancer. However, in melanoma-a highly chemotherapy-resistant disease-TP53 mutations are rare, raising the possibility that this cancer uses alternative ways to overcome p53-mediated tumor suppression. Here we show that Mdm4 p53 binding protein homolog (MDM4), a negative regulator of p53, is upregulated in a substantial proportion ( approximately 65 ) of stage I-IV human melanomas and that melanocyte-specific Mdm4 overexpression enhanced tumorigenesis in a mouse model of melanoma induced by the oncogene Nras. MDM4 promotes the survival of human metastatic melanoma by antagonizing p53 proapoptotic function. Notably, inhibition of the MDM4-p53 interaction restored p53 function in melanoma cells, resulting in increased sensitivity to cytotoxic chemotherapy and to inhibitors of the BRAF (V600E) oncogene. Our results identify MDM4 as a key determinant of impaired p53 function in human melanoma and designate MDM4 as a promising target for antimelanoma combination therapy.

AB - The inactivation of the p53 tumor suppressor pathway, which often occurs through mutations in TP53 (encoding tumor protein 53) is a common step in human cancer. However, in melanoma-a highly chemotherapy-resistant disease-TP53 mutations are rare, raising the possibility that this cancer uses alternative ways to overcome p53-mediated tumor suppression. Here we show that Mdm4 p53 binding protein homolog (MDM4), a negative regulator of p53, is upregulated in a substantial proportion ( approximately 65 ) of stage I-IV human melanomas and that melanocyte-specific Mdm4 overexpression enhanced tumorigenesis in a mouse model of melanoma induced by the oncogene Nras. MDM4 promotes the survival of human metastatic melanoma by antagonizing p53 proapoptotic function. Notably, inhibition of the MDM4-p53 interaction restored p53 function in melanoma cells, resulting in increased sensitivity to cytotoxic chemotherapy and to inhibitors of the BRAF (V600E) oncogene. Our results identify MDM4 as a key determinant of impaired p53 function in human melanoma and designate MDM4 as a promising target for antimelanoma combination therapy.

U2 - 10.1038/nm.2863

DO - 10.1038/nm.2863

M3 - Article

SN - 1078-8956

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EP - 1247

JO - Nature Medicine

JF - Nature Medicine

IS - 8

ER -