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Abstract

Grant Number: 1P41GM081282-01

Project Title: Pilot-Scale Library Production Based on Phosphine Catalysis of Allenes

PI Information: Name Email Title

KWON, OHYUN ohyun@chem.ucla.edu

Abstract: DESCRIPTION (provided by applicant): Small organic molecules are often used to modulate the function of disease-related proteins and thereby promote and restore human health. In the chemical genetics approach, libraries of small molecules are used systematically to perturb and thereby elucidate protein function. When the protein of interest is a cause for human disease, the hit from the screening in biological assays may also find its use in therapeutic remedies. If chemical genetic screens are to result in the discovery of new small molecules with powerful physiological effects, libraries of unique and diverse small molecules are desired. Ideally, a library of small molecules should be able to perturb most of the proteins in humans, but this ideal chemical library does not yet exist. As a step toward this goal, diversity-oriented synthesis (DOS) has emerged as a new paradigm. The goal in DOS is to generate an array of small molecules that differ in their three-dimensional scaffolds; however, gaining access to scaffold diversity has proven to be more challenging than creating a library of compounds derived from one scaffold, as in combinatorial chemistry. In this proposal we analyze the current state of DOS and propose a powerful mechanism for it: combinatorial scaffolding. In the combinatorial scaffolding strategy a multiplicative increase in the number of scaffolds is achieved with an additive increase in the number of reaction conditions. To achieve combinatorial scaffolding, the development of phosphine-catalyzed allenoate annulations is proposed. When the proposed annulations are performed on the resin-bound allenoates, a library of compounds with 53 different scaffolds will be generated. Since the products from the proposed library contain at least one variable substituent, the project will produce a library of libraries. These libraries will be submitted to the NIH Molecular Libraries Small-Molecule Repository (MLSMR) for high-throughput biological screening. The process of developing the proposed chemical synthesis has already produced 171 model compounds. Preliminary assays using these compounds have resulted in the discovery of small molecule enzyme inhibitors for GGTase I, FTase, palmitoyltransferase, and phosphatases, as well as several more chemicals with interesting biological activities. The four enzymes are implicated in diverse human disorders, such as cancer, heart diseases, diabetes, and Alzheimer's; therefore, the small molecule ligands we discovered in our initial library have significant medical implications.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
chemical registry /resource, combinatorial chemistry, small molecule
NIH Roadmap Initiative tag

Institution: UNIVERSITY OF CALIFORNIA LOS ANGELES

Office of Research Administration

LOS ANGELES, CA 90095

Fiscal Year: 2007

Department: CHEMISTRY AND BIOCHEMISTRY

Project Start: 04-SEP-2007

Project End: 31-AUG-2010

ICD: NATIONAL INSTITUTE OF GENERAL MEDICAL SCIENCES

IRG: ZGM1

Grant Number:	1P41GM081282-01
Project Title:	Pilot-Scale Library Production Based on Phosphine Catalysis of Allenes

PI Information:	Name	Email	Title
	KWON, OHYUN	ohyun@chem.ucla.edu

Institution:	UNIVERSITY OF CALIFORNIA LOS ANGELES
	Office of Research Administration
	LOS ANGELES, CA 90095
Fiscal Year:	2007
Department:	CHEMISTRY AND BIOCHEMISTRY
Project Start:	04-SEP-2007
Project End:	31-AUG-2010
ICD:	NATIONAL INSTITUTE OF GENERAL MEDICAL SCIENCES
IRG:	ZGM1