CRISP - Computer Retrieval of Information on Scientific Projects, Abstract Display

Version 2.5.2.0

Abstract

Grant Number: 1R21AI078708-01A1

Project Title: Identification of short functional motifs as potential drug targets for HIV

PI Information: Name Email Title

SCHILLER, MARTIN R. schiller@nso.uchc.edu

Abstract: DESCRIPTION (provided by applicant): Autoimmune Deficiency Syndrome (AIDS) is caused by the HIV retrovirus and is a deadly worldwide epidemic. One efficient strategy that viruses use is to hijack short functional motifs. These motifs are consensus sequences on different HIV proteins that are the binding sites or targets that host proteins act on to allow viral infection and replication. For example, the HIV envelope polyprotein (Env) contains a short consensus motif (Arg-x-Lys/Arg-Arg; "x" is any residue) for cleavage by the host protease, Furin. One of the major limitations in identifying short functional motifs is the lack of a systematic approach and simple accessibility for HIV researchers. Our cross-disciplinary team has built Minimotif Miner (MnM), a motif database and platform-independent web-tool that identifies short motif consensus sequences (less that 15 residues) in protein queries and thus new potential functions in these proteins (http://mmm.engr.unconn.edu/). Many of these consensus sequences are present in HIV proteins. To facilitate the study of short functional motifs in HIV proteins, we proposed to provide a free new web system infrastructure that integrates information for protein motifs with sequence conservation among HIV isolates and 3D structures of HIV proteins to allow HIV researchers to explore new functions in HIV proteins. Short functional motifs provide a plethora of potential targets for intervention in the viral life-cycle that have not been thoroughly explored (Aims 1 and 2). A second goal of this proposal is to test some of the more exciting motif predictions. Consensus motifs in HIV proteins will be validated by mutating the motif in recombinant viruses, testing for the effect of the mutation on viral infection and replication, and then assaying the direct function of the predicted motif (e.g. interaction with another protein; aim 3). PUBLIC HEALTH RELEVANCE: This project provides a key tool to help understand the process by which HIV infects and replicates within cells. The proposed experiments are likely to identify new lead compounds for treating HIV infection.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:

There are no thesaurus terms on file for this project.

Institution: UNIVERSITY OF CONNECTICUT SCH OF MED/DNT

Office of Research & Sponsored Programs

FARMINGTON, CT 06030

Fiscal Year: 2008

Department: MOLECULAR, MICROBIAL, & STRUC BIOL

Project Start: 15-JUN-2008

Project End: 31-MAY-2010

ICD: NATIONAL INSTITUTE OF ALLERGY AND INFECTIOUS DISEASES

IRG: AMCB

Grant Number:	1R21AI078708-01A1
Project Title:	Identification of short functional motifs as potential drug targets for HIV

PI Information:	Name	Email	Title
	SCHILLER, MARTIN R.	schiller@nso.uchc.edu

Institution:	UNIVERSITY OF CONNECTICUT SCH OF MED/DNT
	Office of Research & Sponsored Programs
	FARMINGTON, CT 06030
Fiscal Year:	2008
Department:	MOLECULAR, MICROBIAL, & STRUC BIOL
Project Start:	15-JUN-2008
Project End:	31-MAY-2010
ICD:	NATIONAL INSTITUTE OF ALLERGY AND INFECTIOUS DISEASES
IRG:	AMCB