ARK5 is Transcriptionally Regulated by the Large-MAF Family and Mediates IGF-1-induced Cell Invasion in Multiple Myeloma: ARK5 As a New Molecular Determinant of Malignant Multiple Myeloma

Overview

Journal Oncogene

Specialties Molecular Biology
Oncology

Date 2005 Jul 27

PMID 16044163

Citations 36

Authors

Atsushi Suzuki

Shinsuke Iida

Miyuki Kato-Uranishi

Emi Tajima

Fenghuang Zhan

Ichiro Hanamura

Yongsheng Huang

Tsutomu Ogura

Satoru Takahashi

Ryuzo Ueda

Bart Barlogie

John Shaughnessy Jr

Hiroyasu Esumi

Affiliations

Soon will be listed here.

Abstract

ARK5, AMP-activated protein kinase (AMPK)-related protein kinase mediating Akt signals, is closely involved in tumor progression, and its stage-associated expression was observed in colorectal cancer. In this study, we found ARK5 expression in multiple myeloma cell lines expressing c-MAF and MAFB. In addition, gene expression profiling of 351 clinical specimens revealed ARK5 expression in primary myelomas expressing c-MAF and MAFB, suggesting that ARK5 may be a transcriptional target of the Large-MAF family. Sequence analysis of the ARK5 gene promoter revealed that it contains two putative MAF-recognition element (MARE) sequences. In support of this hypothesis, ARK5 was induced when an MAFB or c-MAF expression vector was introduced into non-ARK5-expressing colon cancer cells. Furthermore, ARK5 promoter activity was dramatically decreased by mutation or deletion of MARE sequences. Chromatin immunoprecipitation assays revealed an interaction between the Large-MAF family proteins and MARE sequences in the ARK5 promoter. Moreover, in ARK5 mRNA-expressing multiple myeloma lines, but not in ARK5-negative lines, insulin-like growth factor (IGF)-1 increased invasion activity. IGF-1-induced invasion was reproduced when ARK5 was overexpressed in Burkitt's lymphoma and plasmacytoma lines. Based on results, we conclude that ARK5 is a transcriptional target of the Large-MAF family through MARE sequence and that ARK5 may in part mediate the aggressive phenotype associated with c-MAF- and MAFB-expressing myelomas.

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