MDMX: from bench to bedside | Zendy

JeanChristophe Marine | Zendy; Michael A. Dyer | Zendy; Aart G. Jochemsen | Zendy

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MDMX: from bench to bedside

Author(s) -

JeanChristophe Marine,

Michael A. Dyer,

Aart G. Jochemsen

Publication year - 2007

Publication title -

journal of cell science

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.384

H-Index - 278

eISSN - 1477-9137

pISSN - 0021-9533

DOI - 10.1242/jcs.03362

Subject(s) - biology , bench to bedside , mdmx , genetics , medical physics , mdm2 , physics , cell culture

The tumor suppressor protein p53 is negatively regulated by Mdm2, a ubiquitin ligase protein that targets p53 for degradation. Mdmx (also known as Mdm4) is a relative of Mdm2 that was identified on the basis of its ability to physically interact with p53. An increasing body of evidence, including recent genetic studies, suggests that Mdmx also acts as a key negative regulator of p53. Aberrant expression of MDMX could thus contribute to tumor formation. Indeed, MDMX amplification and/or overexpression occurs in several diverse tumors. Strikingly, recent work identifies MDMX as a specific chemotherapeutic target for treatment of retinoblastoma. Specific MDMX antagonists should therefore be developed as a tool to ensure activation of 'dormant' p53 activity in tumors that retain wild-type p53.

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