Netzer P, Sendensky A, Wissmeyer M P, Baumeler S, Batista C, Scheurer U, Krause T, Reber P, Brenneisen R
Department of Gastroenterology, Inselspital, University Hospital Bern, Bern, Switzerland.
Aliment Pharmacol Ther. 2008 Dec 1;28(11-12):1334-41. doi: 10.1111/j.1365-2036.2008.03855.x.
Constipation is a significant side effect of opioid therapy. We have previously demonstrated that naloxone-3-glucuronide (NX3G) antagonizes the motility-lowering-effect of morphine in the rat colon.
To find out whether oral NX3G is able to reduce the morphine-induced delay in colonic transit time (CTT) without being absorbed and influencing the analgesic effect.
Fifteen male volunteers were included. Pharmacokinetics: after oral administration of 0.16 mg/kg NX3G, blood samples were collected over a 6-h period. Pharmacodynamics: NX3G or placebo was then given at the start time and every 4 h thereafter. Morphine (0.05 mg/kg) or placebo was injected s.c. 2 h after starting and thereafter every 6 h for 24 h. CTT was measured over a 48-h period by scintigraphy. Pressure pain threshold tests were performed.
Neither NX3G nor naloxone was detected in the venous blood. The slowest transit time was observed during the morphine phase, which was significantly different from morphine with NX3G and placebo. The pain perception was not significantly influenced by NX3G.
Orally administered NX3G is able to reverse the morphine-induced delay of CTT in humans without being detected in peripheral blood samples. Therefore, NX3G may improve symptoms of constipation in-patients using opioid medication without affecting opioid-analgesic effects.
便秘是阿片类药物治疗的一种显著副作用。我们之前已经证明,纳洛酮-3-葡萄糖醛酸苷(NX3G)可拮抗吗啡对大鼠结肠动力的降低作用。
探究口服NX3G是否能够减少吗啡引起的结肠转运时间(CTT)延迟,而不被吸收并影响镇痛效果。
纳入15名男性志愿者。药代动力学:口服0.16 mg/kg NX3G后,在6小时内采集血样。药效学:在开始时给予NX3G或安慰剂,此后每4小时给药一次。在开始后2小时皮下注射吗啡(0.05 mg/kg)或安慰剂,此后每6小时注射一次,共24小时。通过闪烁扫描法在48小时内测量CTT。进行压力痛阈测试。
静脉血中未检测到NX3G和纳洛酮。在吗啡阶段观察到最慢的转运时间,这与联合NX3G的吗啡组和安慰剂组有显著差异。NX3G对疼痛感知没有显著影响。
口服NX3G能够逆转吗啡引起的人体CTT延迟,且在外周血样本中未被检测到。因此,NX3G可能改善使用阿片类药物患者的便秘症状,而不影响阿片类药物的镇痛效果。
