GREB1 Isoform 4 is Specifically Transcribed by MITF and Required for Melanoma Proliferation

Overview

Journal Oncogene

Specialties Molecular Biology
Oncology

Date 2023 Sep 1

PMID 37658191

Authors

Koei Shinzawa

Shinji Matsumoto

Ryota Sada

Akikazu Harada

Kaori Saitoh

Keiko Kato

Satsuki Ikeda

Akiyoshi Hirayama

Kazunori Yokoi

Atsushi Tanemura

Keisuke Nimura

Masahito Ikawa

Tomoyoshi Soga

Akira Kikuchi

Affiliations

Soon will be listed here.

Abstract

Growth regulation by estrogen in breast cancer 1 (GREB1) is involved in hormone-dependent and -independent tumor development (e.g., hepatoblastoma). In this study, we found that a GREB1 splicing variant, isoform 4 (Is4), which encodes C-terminal half of full-length GREB1, is specifically expressed via microphthalmia-associated transcription factor (MITF) in melanocytic melanoma, and that two MITF-binding E-box CANNTG motifs at the 5'-upstream region of GREB1 exon 19 are necessary for GREB1 Is4 transcription. MITF and GREB1 Is4 were strongly co-expressed in approximately 20% of the melanoma specimens evaluated (17/89 cases) and their expression was associated with tumor thickness. GREB1 Is4 silencing reduced melanoma cell proliferation in association with altered expression of cell proliferation-related genes in vitro. In addition, GREB1 Is4 targeting by antisense oligonucleotide (ASO) decreased melanoma xenograft tumor formation and GREB1 Is4 expression in a BRAF; PTEN melanoma mouse model promoted melanoma formation, demonstrating the crucial role of GREB1 Is4 for melanoma proliferation in vivo. GREB1 Is4 bound to CAD, the rate-limiting enzyme of pyrimidine metabolism, and metabolic flux analysis revealed that GREBI Is4 is necessary for pyrimidine synthesis. These results suggest that MITF-dependent GREB1 Is4 expression leads to melanoma proliferation and GREB1 Is4 represents a new molecular target in melanoma.

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