Open Access Research

Effects of concurrent intravenous morphine sulfate and naltrexone hydrochloride on end-tidal carbon dioxide

Veeraindar Goli1,2,5*, Lynn R Webster3, Michael J Lamson1, Jody M Cleveland1, Kenneth W Sommerville1,2 and Eric Carter4

Author Affiliations

1 Pfizer Inc, Cary, NC, USA

2 Duke University Medical Center, Durham, NC, USA

3 Lifetree Clinical Research, Salt Lake City, UT, USA

4 Allergan, Inc. (formerly Pfizer Inc), Irvine, CA, USA

5 Pfizer Inc, 4000 CentreGreen Way, Suite 300, Cary, NC 27513, USA

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Harm Reduction Journal 2012, 9:13 doi:10.1186/1477-7517-9-13

Published: 15 March 2012

Abstract

Background

Respiratory depression, a potentially fatal side-effect of opioid-overdose, may be reversed by timely administration of an opioid antagonist, such as naloxone or naltrexone. Tampering with a formulation of morphine sulfate and sequestered naltrexone hydrochloride extended release capsules (MS-sNT) releases both the opioid morphine and the antagonist naltrexone. A study in recreational opioid-users indicated that morphine and naltrexone injected in the 25:1 ratio (duplicating the ratio of the formulation) found MS-sNT reduced morphine-induced euphoric effects vs intravenous (IV) morphine alone. In the same study, the effects of morphine + naltrexone on end-tidal carbon dioxide (EtCO2), a measure of respiratory-depression, were evaluated and these data are reported here.

Methods

Single-center, placebo-controlled, double-blind crossover study. Non-dependent male opioid users were randomized to receive single IV doses of placebo, 30 mg morphine alone, and 30 mg morphine + 1.2 mg naltrexone. EtCO2 was measured by noninvasive capnography.

Results

Significant differences in EtCO2 least-squares means across all treatments for maximal effect (Emax) and area under the effect curve (AUE0-2, AUE0-8, AUE0-24) were detected (all p ≤ 0.0011). EtCO2 Emax values for morphine + naltrexone were significantly reduced vs morphine alone (42.9 mm Hg vs 47.1 mm Hg, p < 0.0001) and were not significantly different vs placebo (41.9 mm Hg). Median time to reach maximal effect (TEmax) was delayed for morphine + naltrexone vs morphine alone (5.0 h vs 1.0 h).

Conclusions

Results provide preliminary evidence that the naltrexone:morphine ratio within MS-sNT is sufficient to significantly reduce EtCO2 when administered intravenously to non-dependent male recreational opioid-users. Further studies with multiple measures of respiratory-function are warranted to determine if risk of respiratory depression is also reduced by naltrexone in the tampered formulation.

Keywords:
Morphine; Naltrexone; Opioid; Opioid antagonist; Respiratory depression; Opioid overdose; Drug abuse