2006
DOI: 10.1124/mol.106.025999
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Rapid and Robust Protection against Cocaine-Induced Lethality in Rats by the Bacterial Cocaine Esterase

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Cited by 48 publications
(97 citation statements)
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References 29 publications
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“…The present results show that these properties combine with an ability to prevent cocaine access to critical biological targets, including heart and brain, and to block or reverse cardiovascular and neurological toxicity. The approximate 10-fold rightward shift in the doseresponse curve for seizure induction by cocaine after AlbuCocH is equivalent to the recently reported effect of bacterial cocaine esterase (Cooper et al, 2006). The bacterial enzyme lost its ability to protect in 30 min or less, but AlbuCocH treatment remained fully protective for 12 h. In both cases, protection required catalytic activity, and treatments were ineffective if the enzymes were inactivated in a manner expected to preserve cocaine binding.…”
Section: Albu-coch and Cocaine Toxicitysupporting
confidence: 63%
See 1 more Smart Citation
“…The present results show that these properties combine with an ability to prevent cocaine access to critical biological targets, including heart and brain, and to block or reverse cardiovascular and neurological toxicity. The approximate 10-fold rightward shift in the doseresponse curve for seizure induction by cocaine after AlbuCocH is equivalent to the recently reported effect of bacterial cocaine esterase (Cooper et al, 2006). The bacterial enzyme lost its ability to protect in 30 min or less, but AlbuCocH treatment remained fully protective for 12 h. In both cases, protection required catalytic activity, and treatments were ineffective if the enzymes were inactivated in a manner expected to preserve cocaine binding.…”
Section: Albu-coch and Cocaine Toxicitysupporting
confidence: 63%
“…MB1, a bacterium linked with coca plants (Bresler et al, 2000;Larsen et al, 2002;Turner et al, 2002). This enzyme can prevent lethal cocaine-induced seizures in rats and increase the dose for cocaine toxicity 10-fold (Cooper et al, 2006). Bacterial cocaine esterase deserves more study as a rescue agent.…”
Section: Discussion Previous Development Of Cocaine Hydrolases and Bimentioning
confidence: 99%
“…Although the wild-type (wt) form of CocE is capable of dose dependently protecting mice and rats against the cardiovascular, convulsant, and lethal effects of cocaine, it is rapidly inactivated at body temperature resulting in an in vivo half-life of B15 min (Cooper et al, 2006;Jutkiewicz et al, 2009;Ko et al, 2007Ko et al, , 2009Wood et al, 2010). Sitedirected mutagenesis studies aimed at improving the thermostability of CocE have identified an equally efficient mutant CocE (T172R/G173Q CocE, RQ CocE, DM CocE) with an in vivo half-life of B4.5 h in mice (Gao et al, 2009;Narasimhan et al, 2010), and a high degree of pharmacologic specificity (Brim et al, 2011).…”
Section: Introductionmentioning
confidence: 99%
“…found in the Rhizosphere soil surrounding the coca plant, CocE has a high V max toward cocaine (V max ϭ 2300 min Ϫ1 ) (Gao et al, 2009) and produces the same products as BchE (Bresler et al, 2000). CocE has previously been shown to block cocaine-induced cardiac disturbance, neurological changes, and lethality in rodents when administered before or after cocaine (Cooper et al, 2006;Jutkiewicz et al, 2009;Ko et al, 2007;Wood et al, 2010).…”
mentioning
confidence: 99%
“…The wild-type (wt) CocE cannot be used as a pharmacotherapy for cocaine abuse because of its 13.7-min half-life at 37°C (Cooper et al, 2006;Ko et al, 2007;Gao et al, 2009). We have previously identified a mutant of CocE (T172R and G173Q) that extends the half-life of CocE to ϳ4.5 h, as assessed by in vitro kinetic assays (at 37°C) or in vivo by protection against cocaine-induced lethality in mice (Gao et al, 2009).…”
mentioning
confidence: 99%