GGrantIndex
← Search

PROTEASE

$0P30FY2001CANIH

Wayne State University, Detroit MI

Investigators

Linked publications, trials & patents

Trial NCT06501040Trial NCT04479267Trial NCT04397679Trial NCT04266522Trial NCT04159896Trial NCT03875053Trial NCT03683420Trial NCT03456804Trial NCT03454529Trial NCT03453489Trial NCT03406858Trial NCT03252600Trial NCT03147885Trial NCT02824029Trial NCT02819024Trial NCT02723604Trial NCT02620865Trial NCT02568449Trial NCT02521090Trial NCT02520115Trial NCT02472275Trial NCT02470559Trial NCT02359019Trial NCT02178436Trial NCT02178163Trial NCT02173093Trial NCT02145078Trial NCT02094872Trial NCT02058706Trial NCT02037256Trial NCT01987596Trial NCT01958372Trial NCT01698658Trial NCT01504711Trial NCT01281163Trial NCT01175980Trial NCT01147016Trial NCT01116232Trial NCT01071564Trial NCT01051570Trial NCT01022138Trial NCT00984919Trial NCT00972023Trial NCT00942422Trial NCT00938626Trial NCT00935090Trial NCT00918762Trial NCT00914147Trial NCT00906503Trial NCT00903214Trial NCT00899665Trial NCT00897910Trial NCT00897741Trial NCT00897494Trial NCT00897247Trial NCT00890617Trial NCT00888654Trial NCT00769288Trial NCT00768118Trial NCT00717535Trial NCT00691015Trial NCT00559897Trial NCT00541099Trial NCT00527124Trial NCT00521261Trial NCT00520767Trial NCT00514215Trial NCT00503841Trial NCT00499694Trial NCT00482846Trial NCT00459121Trial NCT00438204Trial NCT00423826Trial NCT00410904Trial NCT00376948Trial NCT00369109Trial NCT00305747Trial NCT00303901Trial NCT00301808Trial NCT00293384Trial NCT00288028Trial NCT00258466Trial NCT00258310Trial NCT00258284Trial NCT00258245Trial NCT00258232Trial NCT00248560Trial NCT00248482Trial NCT00244946Trial NCT00244933Trial NCT00243048Trial NCT00238329Trial NCT00227721Trial NCT00217581Trial NCT00121264Trial NCT00118157Trial NCT00078923Trial NCT00068653Trial NCT00066326Trial NCT00056004

Abstract

Description: (Applicant's Description) The Protease Program is primarily a basic science program with an expanding emphasis in translational research. The members of this program come from three institutions: Wayne State University and Henry Ford Health Systems in Detroit and the University of Windsor in Windsor, Ontario. The basic research of this program focuses primarily on determining the roles of proteases and their endogenous inhibitors in malignant progression. Proteases of the matrix metalloproteinase, cysteine (calpain, caspase and cathepsin), serine and aspartic classes are currently under study. In terms of protease inhibitors, program members are investigating both endogenous protease inhibitors (e.g., tissue inhibitors of matrix metalloproteinases and cystatins) and designing and testing novel synthetic inhibitors for matrix metalloproteinases and cysteine (calpain and cathepsin) proteases. Translational research efforts are directed toward: 1) determining whether the proteases and their endogenous inhibitors might serve as prognostic indicators, 2) development of protease inhibitors as potential therapeutic agents, 3) determining whether cell surface binding proteins for proteases and inhibitors might serve as prognostic indicators and novel targets for therapeutic intervention, and 4) developing novel methods for in vitro and in vivo imaging of proteases. This work includes interprogrammatic collaborations with investigators in the Prostate, Breast Cancer and Developmental Therapeutics programs. Other basic research of the Protease Program addresses more fundamental issues such as the mechanisms for intracellular trafficking and secretion of proteases, the molecular and cellular mechanisms for regulation of protease expression and activity, and the roles of proteases and their inhibitors in diseases other than cancer, in normal development and in apoptotic responses to cell injury. The latter studies represent an alternative approach to designing effective anti-tumor agents. As the basic and translational research efforts of the Protease Program are successful, we anticipate that novel agents will be generated for testing in preclinical and ultimately in clinical

View original record on NIH RePORTER →