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Abstract

Grant Number: 1R03NS050849-01

Project Title: High H3-K9 Methyltransferase Inhibitor Screen (RMI)

PI Information: Name Email Title

WRIGHT, KENNETH L. ken.wright@moffitt.org ASSISTANT PROFESSOR

Abstract: DESCRIPTION (provided by applicant): Tumor development and progression has long been known to involve both genetic and epigenetic alterations in the gene expression profile of tumor cells. Of particular importance is the silencing of tumor suppressor genes. Epigenetic mechanisms of gene silencing include histone deacetylation, DMA methylation, and histone methylation. Each of these mechanisms are interrelated and influence each other. Inhibitors of both histone deacetylation and DMA methylation are available and are in use as promising anti-cancer agents. However, only recently has the role of histone methylation become apparent. H3-K9 methyltransferases have been linked to the function of tumor suppressor genes, cellular senescence and regulating telomere length. In both breast and prostate cancer the H3-K27 methyltransferase EZH2 is over-expressed and is a strong prognostic factor for aggressive or metastatic tumors. In addition specific transcription factors recruit individual histone methyltransferases necessary for their gene silencing function. These rapidly developing links between histone methylation and tumors and cell growth control suggest an exciting new therapeutic target. However, existing technologies limit our ability to rapidly pursue these developments. Strikingly, no specific inhibitors of histone methylation exist. This proposal seeks to eliminate this limitation by developing a simple, quantitative high throughput assay capable of individually measuring the activity of each of the histone H3 lysine methylating enzymes. To this goal the specific aims are: 1) Migrate existing histone methyltransferase assays into a high throughput format using competitive fluorescence polarization. This aim will combine existing technologies and reagents into a sensitive and rapid assay. The assay will be initially utilized and further tested on the NCI Structural Diversity set of compounds to identify lead compounds for drug discovery.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
drug screening /evaluation, enzyme activity, enzyme inhibitor, fluorescence polarization, high throughput technology, methyltransferase, technology /technique development
cell growth regulation, drug discovery /isolation, gene expression, histone, lysine, methylation, neoplasm /cancer pharmacology, neoplastic cell, neoplastic growth, tumor progression

Institution: H. LEE MOFFITT CANCER CTR & RES INST

TAMPA, FL 336129497

Fiscal Year: 2004

Department:

Project Start: 30-SEP-2004

Project End: 29-SEP-2005

ICD: NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS AND STROKE

IRG: ZNS1

Grant Number:	1R03NS050849-01
Project Title:	High H3-K9 Methyltransferase Inhibitor Screen (RMI)

PI Information:	Name	Email	Title
	WRIGHT, KENNETH L.	ken.wright@moffitt.org	ASSISTANT PROFESSOR

Institution:	H. LEE MOFFITT CANCER CTR & RES INST
	TAMPA, FL 336129497
Fiscal Year:	2004
Department:
Project Start:	30-SEP-2004
Project End:	29-SEP-2005
ICD:	NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS AND STROKE
IRG:	ZNS1