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Abstract

Grant Number: 5R44AR046167-03

PI Name: SZABO, CSABA

PI Email: szabocsaba@aol.com

PI Title: VICE PRESIDENT FOR RESEARCH

Project Title: Adenosine-3 agonists for the suppression of arthritis

Abstract: DESCRIPTION (provided by the applicant): Based on promising in vitro and in vivo data, the applicants are developing novel classes of compounds with anti-inflammatory effects, and with anti-arthritic potential. In this proposal, we present evidence that selected ligands of the adenosine-3 receptor are (1) inhibitors of the production of macrophage-derived pro-inflammatory mediators and enhancers of the production of anti-inflammatory mediators in vitro and in vivo (2) potent anti-inflammatory agents in a variety of inflammatory conditions including collagen-induced arthritis, and endotoxin-induced systemic inflammation. The applicants intend to develop a selected adenosine 3 receptor agonist as an anti-arthritic drug. The applicants have collaborated with a prominent group in the field of adenosine receptor ligands, and have identified candidates, with selectivity towards the adenosine 3 subtype in human systems, which are deemed suitable leads for further drug development, efficacy studies, and eventual formal pharmacokinetic and toxicology studies. The specific aims of the present proposal are (1) to identify a lead adenosine-3 ligand, with acceptable efficacy profile in human systems (2) to perform efficacy studies with the compound in terms of suppression of pro-inflammatory mediators in human cell systems (3) to synthesize larger, GLP and GMP-quality quantities of a lead adenosine-3 agonist compound, and (4) to perform in-house and subcontracted pharmacokinetic and toxicity studies in two species according to FDA requirements. The current scope of work will bring the applicants forward to the level of an IND application for Phase I clinical testing of a selected adenosine-3 ligand. PROPOSED COMMERCIAL APPLICATION: The domestic market for a novel, effective therapy for arthritis is estimated at >$1 billion per annum. Global markets are estimated at $4 billion. Current market entrants are incompletely effective: Arthritis-related morbidity is substantial, with chronic disability, loss of employment, and exercise intolerance. A novel A3 receptor agonist may represent a useful anti-inflammatory adjunct to current therapeutic regimens; funding of the current SBIR Phase II will allow for starting human safety trials in 2 years.
Thesaurus Terms:
adenosine, antiarthritic agent, arthritis, drug design /synthesis /production, drug screening /evaluation, purinergic receptor, stimulant /agonist
antiinflammatory agent, cytokine, drug adverse effect, interleukin 10, nitric oxide synthase, oral administration, pharmacokinetics, rheumatoid arthritis
Macaca fascicularis, clinical research, human tissue, laboratory mouse, laboratory rat

Institution: INOTEK PHARMACEUTICALS CORPORATION

100 CUMMINGS CTR, STE 419E

BEVERLY, MA 01915

Fiscal Year: 2003

Department:

Project Start: 15-SEP-1999

Project End: 31-AUG-2004

ICD: NATIONAL INSTITUTE OF ARTHRITIS AND MUSCULOSKELETAL AND SKIN DISEASES

IRG: ZRG1

Grant Number:	5R44AR046167-03
PI Name:	SZABO, CSABA
PI Email:	szabocsaba@aol.com
PI Title:	VICE PRESIDENT FOR RESEARCH
Project Title:	Adenosine-3 agonists for the suppression of arthritis

Institution:	INOTEK PHARMACEUTICALS CORPORATION
	100 CUMMINGS CTR, STE 419E
	BEVERLY, MA 01915
Fiscal Year:	2003
Department:
Project Start:	15-SEP-1999
Project End:	31-AUG-2004
ICD:	NATIONAL INSTITUTE OF ARTHRITIS AND MUSCULOSKELETAL AND SKIN DISEASES
IRG:	ZRG1