NR ANZC
AU Ryou,C.; Legname,G.; Peretz,D.; Craig,J.C.; Baldwin,M.A.; Prusiner,S.B.
TI Differential inhibition of prion propagation by enantiomers of quinacrine
QU Laboratory Investigation 2003 Jun; 83(6): 837-43
PT journal article
AB Prion diseases are fatal neurologic disorders caused by accumulation of a pathogenic isoform (PrPsc) of the prion protein (PrP). The recent discovery of the inhibitory action of quinacrine on PrPsc formation in scrapie-infected neuroblastoma (ScN2a) cells raised the possibility of a treatment for patients with prion disease. To investigate the efficacy of quinacrine enantiomers, we measured the inhibitory effect of these isomers on PrPsc formation in ScN2a cells. (S)-quinacrine exhibited superior antiprion activity compared with (R)-quinacrine and two generic quinacrines that appear to be racemates. Treatment with these various forms of quinacrine did not induce adverse changes affecting cell survival and the expression of marker proteins over a range of potentially therapeutic concentrations. Thus, quinacrine enantiomers demonstrated stereoselectivity on prion elimination but not cytotoxicity in ScN2a cells. Our results raise the possibility that in vivo treatment using one enantiomer of quinacrine may be superior to a racemic mixture, which is the form that is generally used when quinacrine is employed to treat parasitic diseases.
MH Cell Line; Cell Survival/drug effects; Dose-Response Relationship, Drug; Enzyme-Linked Immunosorbent Assay; Human; Kinetics; PrPsc Proteins/*antagonists & inhibitors; Prions/*antagonists & inhibitors; Quinacrine/*chemistry/*pharmacology; Stereoisomerism; Support, Non-U.S. Gov't; Support, U.S. Gov't, P.H.S.
AD Institute for Neurodegenerative Diseases (CR, GL, DP, MAB, SBP), Departments of Neurology (GL, DP, MAB, SBP), Pharmaceutical Chemistry (JCC, MAB), and Biochemistry and Biophysics (SBP), University of California, San Francisco, California.
SP englisch
PO USA