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Pharmacokinetics of controlled release morphine (MST) in patients with liver carcinoma

Research Authors
HIM Kotb, SA El-Kady, SES Emara, EA Fouad, MY El-Kabsh
Research Date
Research Journal
British journal of anesthesia
Research Publisher
science direct
Research Vol
94
Research Website
doi: 10.1093/bja/aei007. Epub 2004 Oct 29.
Research Year
2005
Research Member
Research_Pages
95-99
Research Abstract

Background: There are no studies reported on the pharmacokinetics of controlled release morphine (MST) in patients with hepatocellular carcinoma, the fifth most common cancer in the world.

Methods: We have studied the pharmacokinetic profile of MST (30 mg) in 15 patients with liver carcinoma (eight with primary carcinoma on top of chronic hepatitis C, and seven with secondary metastatic liver malignancy as a result of other primary) compared with our previously published data for 10 healthy controls. Plasma morphine concentrations were measured in venous blood samples at intervals up to 12 h by high-pressure liquid chromatography. Total body clearance (Cl) and systemic bioavailability were estimated using a compartmental method.

Results: Morphine bioavailability showed a substantial increase in patients with primary liver and secondary metastatic carcinoma than that of controls (64.8, 62.1, and 16.8%, respectively). The area under the serum concentration-time curve increased 4-fold in primary carcinoma (416 [sem25] microg h(-1) litre(-1)) and 3-fold (303 [21] microg h(-1) litre(-1)) in metastatic liver patients compared with healthy control (92.5 [3] microg h(-1) litre(-1)). No significant difference was found in T(max) between the two malignant groups but C(max) was significantly greater in primary liver carcinoma patients. Impaired morphine elimination was noted in primary carcinoma only (t(1/2) 5.99 [0.39] h).

Conclusion: Careful administration of morphine is recommended in patients with liver cancer.