利福昔明靶向结肠治疗旅行者腹泻的随机、双盲、安慰剂对照 3 期研究。

Targeting of rifamycin SV to the colon for treatment of travelers' diarrhea: a randomized, double-blind, placebo-controlled phase 3 study.

机构信息

Center for Infectious Diseases, University of Texas School of Public Health, Houston, TX, USA.

出版信息

J Travel Med. 2014 Nov-Dec;21(6):369-76. doi: 10.1111/jtm.12168.

DOI:10.1111/jtm.12168

PMID:25345982

Abstract

BACKGROUND

Rifamycin SV is under development for treatment of travelers' diarrhea (TD) in a new oral formulation, Rifamycin SV MMX (RIF-MMX; Santarus Inc., San Diego, CA, USA), which targets its delivery to the colon, making it a unique rifamycin drug.

METHODS

This was a randomized, double-blind, phase 3 study of adult travelers to Mexico or Guatemala experiencing acute diarrhea. A total of 264 patients received RIF-MMX (2 × 200 mg twice daily for 3 days, n = 199) or placebo (n = 65) in a 3 : 1 ratio. The primary endpoint was the length of time between the administration of first dose of study drug and passage of the last unformed stool (TLUS; after which clinical cure was declared). Other endpoints included eradication of pathogens from the stools, pathogen minimum inhibitory concentration (MIC), and adverse events (AEs).

RESULTS

TLUS was significantly shorter in the RIF-MMX group (median: 46.0 hours) compared with placebo (median: 68.0 hours; p = 0.0008) and a larger percentage of RIF-MMX treated patients (81.4%) achieved clinical cure compared with placebo patients (56.9%). TLUS was significantly shorter in the subgroups of patients with enteroaggregative, enterotoxigenic, or diffusely adherent Escherichia coli infections (p = 0.0035) with nonsignificant activity against invasive bacteria (p = 0.3804). Overall pathogen eradication rates were numerically higher in the RIF-MMX group (67.0%) compared with placebo (54.8%) but the difference did not reach significance (p = 0.0836). In vitro resistance to rifamycin SV was observed in some bacteria remaining after treatment of patients with RIF-MMX but was not associated with lower efficacy in them. AEs appeared to be more frequent with placebo (38.5%) than with RIF-MMX (29.6%).

CONCLUSIONS

RIF-MMX shortened the duration of TD in patients with a broad range of pathogens and was well tolerated. The unique pharmacokinetic properties of the drug offer evidence that TD pathogens work at the level of the colon.

摘要

背景

利福霉素 SV 正在开发一种新的口服制剂 Rifamycin SV MMX（RIF-MMX；美国圣地亚哥 Santarus 公司），用于治疗旅行者腹泻（TD），该制剂旨在将药物靶向递送至结肠，使其成为一种独特的利福霉素药物。

方法

这是一项针对前往墨西哥或危地马拉的成年旅行者的随机、双盲、3 期研究，他们患有急性腹泻。共有 264 名患者以 3:1 的比例接受 RIF-MMX（2×200mg，每日两次，共 3 天，n=199）或安慰剂（n=65）治疗。主要终点是从服用首剂研究药物到最后一次未成形粪便排出（TLUS；此后宣布临床治愈）的时间。其他终点包括粪便中病原体的清除、病原体最小抑菌浓度（MIC）和不良事件（AE）。

结果

与安慰剂组（中位数：68.0 小时；p=0.0008）相比，RIF-MMX 组的 TLUS 显著缩短（中位数：46.0 小时），并且更多的 RIF-MMX 治疗患者（81.4%）达到临床治愈，而安慰剂患者（56.9%）。在肠聚集性、肠毒性或弥漫性粘附性大肠杆菌感染的患者亚组中，TLUS 显著缩短（p=0.0035），对侵袭性细菌的活性无显著差异（p=0.3804）。RIF-MMX 组的总体病原体清除率（67.0%）略高于安慰剂组（54.8%），但差异无统计学意义（p=0.0836）。在接受 RIF-MMX 治疗的患者中，仍有一些细菌对利福霉素 SV 产生耐药性，但与疗效降低无关。AE 似乎比 RIF-MMX（29.6%）更频繁地出现在安慰剂（38.5%）中。