A RA-dependent, tumour-growth suppressive transcription complex is the target of the PML-RARalpha and T18 oncoproteins

S Zhong; L Delva; C Rachez; C Cenciarelli; D Gandini; H Zhang; S Kalantry; L P Freedman; P P Pandolfi

doi:10.1038/15463

A RA-dependent, tumour-growth suppressive transcription complex is the target of the PML-RARalpha and T18 oncoproteins

Nat Genet. 1999 Nov;23(3):287-95. doi: 10.1038/15463.

Authors

S Zhong¹, L Delva, C Rachez, C Cenciarelli, D Gandini, H Zhang, S Kalantry, L P Freedman, P P Pandolfi

Affiliation

¹ Department of Human Genetics, Molecular Biology Program, Memorial Sloan-Kettering Cancer Center, Sloan-Kettering Division, Graduate School of Medical Sciences, Cornell University, New York, New York, USA.

PMID: 10610177
DOI: 10.1038/15463

Abstract

PML and Tif1a are fused to RARA and Braf, respectively, resulting in the production of PML-RARalpha and Tif1alpha-B-Raf (T18) oncoproteins. Here we show that PML, Tif1alpha and RXRalpha/RARalpha function together in a transcription complex that is dependent on retinoic acid (RA). We found that PML acts as a ligand-dependent coactivator of RXRalpha/RARalpha. PML interacts with Tif1alpha and CBP. In Pml-/- cells, the RA-dependent induction of genes such as RARB2 and the ability of Tif1alpha and CBP to act as transcriptional coactivators on RA are impaired. We show that both PML and Tif1alpha are growth suppressors required for the growth-inhibitory activity of RA. T18, similar to PML-RARalpha, disrupts the RA-dependent activity of this complex in a dominant-negative manner resulting in a growth advantage. Our data define a new pathway for the control of cell growth and tumorigenesis, and provide a new model for the pathogenesis of acute promyelocytic leukaemia (APL).

Publication types

Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, P.H.S.

MeSH terms

Animals
CREB-Binding Protein
Cell Differentiation / drug effects
Cell Division / drug effects
Cell Line
Cell Nucleus / metabolism
Cell Transformation, Neoplastic / drug effects
Cell Transformation, Neoplastic / genetics
Cell Transformation, Neoplastic / metabolism
Cell Transformation, Neoplastic / pathology
DNA / genetics
DNA / metabolism
Gene Expression Regulation, Neoplastic* / drug effects
Genes, Tumor Suppressor / genetics
Genes, Tumor Suppressor / physiology
Humans
Leukemia, Promyelocytic, Acute / genetics*
Leukemia, Promyelocytic, Acute / metabolism
Leukemia, Promyelocytic, Acute / pathology
Mutation
Neoplasm Proteins / chemistry
Neoplasm Proteins / genetics
Neoplasm Proteins / metabolism*
Nuclear Proteins / antagonists & inhibitors
Nuclear Proteins / chemistry
Nuclear Proteins / metabolism*
Oncogene Proteins, Fusion / chemistry
Oncogene Proteins, Fusion / genetics
Oncogene Proteins, Fusion / metabolism*
Promoter Regions, Genetic / genetics
Protein Binding
Protein Isoforms / genetics
Protein Isoforms / metabolism
Receptors, Retinoic Acid / genetics
Receptors, Retinoic Acid / metabolism*
Retinoid X Receptors
Trans-Activators / metabolism
Transcription Factors / antagonists & inhibitors
Transcription Factors / chemistry
Transcription Factors / genetics
Transcription Factors / metabolism*
Transfection
Tretinoin / metabolism
Tretinoin / pharmacology*

Substances

Neoplasm Proteins
Nuclear Proteins
Oncogene Proteins, Fusion
Protein Isoforms
Receptors, Retinoic Acid
Retinoid X Receptors
Trans-Activators
Transcription Factors
promyelocytic leukemia-retinoic acid receptor alpha fusion oncoprotein
transcriptional intermediary factor 1
Tretinoin
DNA
CREB-Binding Protein
CREBBP protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding