Dapoigny M, Abitbol J L, Fraitag B
Department of Hepato-Gastroenterology, Hôtel Dieu, Clermont-Ferrand, France.
Dig Dis Sci. 1995 Oct;40(10):2244-9. doi: 10.1007/BF02209014.
The efficacy and safety of the peripheral kappa agonist fedotozine was evaluated in a double-blind, multicenter study involving 238 patients with the irritable bowel syndrome. After a two-week washout, patients were assigned to one of four groups to receive either placebo or fedotozine three times a day at doses of 3.5, 15, or 30 mg for six weeks. Patient assessment of mean symptom intensity indicated that the 30-mg dose of fedotozine was superior to placebo in relieving maximal daily abdominal pain (P = 0.01), mean daily pain (P = 0.007), and abdominal bloating (P = 0.02). Changes in bowel function and defecation disorders could not be evaluated reliably. According to the investigators, the highest dose of fedotozine markedly reduced overall disease severity (P = 0.003) and the pain component of the symptomatic profile (P = 0.009). Clinical and laboratory safety was very good. Fedotozine 30 mg three times a day therefore appears to be effective and safe in the treatment of the abdominal pain and bloating associated with IBS.
在一项涉及238例肠易激综合征患者的双盲、多中心研究中,对外周κ激动剂非多托嗪的疗效和安全性进行了评估。经过两周的洗脱期后,患者被分配到四组中的一组,接受安慰剂或非多托嗪治疗,剂量为3.5、15或30毫克,每日三次,持续六周。患者对平均症状强度的评估表明,30毫克剂量的非多托嗪在缓解每日最大腹痛(P = 0.01)、每日平均疼痛(P = 0.007)和腹胀(P = 0.02)方面优于安慰剂。肠道功能和排便障碍的变化无法可靠评估。据研究人员称,非多托嗪的最高剂量显著降低了总体疾病严重程度(P = 0.003)和症状特征中的疼痛成分(P = 0.009)。临床和实验室安全性非常好。因此,每日三次服用30毫克非多托嗪在治疗与肠易激综合征相关的腹痛和腹胀方面似乎是有效且安全的。
