一项随机、双盲、安慰剂对照、单次和多次递增剂量的 1 期研究，旨在确定口服给予健康受试者伊贝佐单抗的安全性、药代动力学以及食物和粪便微生物组的影响。

A randomized, double-blind, placebo-controlled, single and multiple ascending dose Phase 1 study to determine the safety, pharmacokinetics and food and faecal microbiome effects of ibezapolstat administered orally to healthy subjects.

机构信息

University of Houston, Houston, TX, USA.

Altasciences Clinical Kansas, Overland Park, KS, USA.

出版信息

J Antimicrob Chemother. 2020 Dec 1;75(12):3635-3643. doi: 10.1093/jac/dkaa364.

BACKGROUND

Clostridioides difficile infection is the most common cause of healthcare-associated infections in the USA, with limited treatment options. Ibezapolstat is a novel DNA polymerase IIIC inhibitor with in vitro activity against C. difficile.

OBJECTIVES AND METHODS

Randomized, double-blind, placebo-controlled study to assess the safety, tolerability and pharmacokinetics of ibezapolstat in healthy volunteers. Microbiome changes associated with ibezapolstat were compared with vancomycin over a 10 day course using shotgun metagenomics.

RESULTS

A total of 62 subjects aged 31 ± 7 years (45% female; average BMI: 25 ± 3 kg/m2) were randomized. Ibezapolstat was well tolerated with a safety signal similar to placebo. Ibezapolstat had minimal systemic absorption with the majority of plasma concentrations less than 1 µg/mL. In the multiday, ascending dose study, ibezapolstat concentrations of 2000 µg/g of stool were observed by Day 2 and for the remainder of the dosing time period. In the multiday, multiple-dose arm, baseline microbiota was comparable between subjects that received ibezapolstat compared with vancomycin. At Day 10 of dosing, differential abundance analysis and β-diversity demonstrated a distinct difference between the microbiome in subjects given vancomycin compared with either dose of ibezapolstat (P = 0.006). α-Diversity changes were characterized as an increase in the Actinobacteria phylum in subjects that received ibezapolstat and an increase in Proteobacteria in subjects given vancomycin.

CONCLUSIONS

Ibezapolstat was shown to be safe and well tolerated, with minimal systemic exposure, high stool concentrations and a distinct microbiome profile compared with oral vancomycin. These results support further clinical development of ibezapolstat for patients with C. difficile infection.

背景

艰难梭菌感染是美国最常见的医疗相关感染，治疗选择有限。Ibezapolstat 是一种新型的 DNA 聚合酶 IIIC 抑制剂，具有体外抗艰难梭菌的活性。

目的和方法

这是一项随机、双盲、安慰剂对照的研究，旨在评估健康志愿者中 Ibezapolstat 的安全性、耐受性和药代动力学。使用 shotgun 宏基因组学比较 Ibezapolstat 与万古霉素在 10 天疗程中引起的微生物组变化。

结果

共有 62 名年龄在 31±7 岁（45%为女性；平均 BMI：25±3kg/m2）的受试者随机分组。Ibezapolstat 耐受性良好，安全性信号与安慰剂相似。Ibezapolstat 全身吸收极少，大多数血浆浓度低于 1μg/ml。在多日递增剂量研究中，第 2 天观察到粪便中 Ibezapolstat 浓度达到 2000μg/g，并且在整个给药期间保持在这一水平。在多日多剂量组中，与万古霉素相比，接受 Ibezapolstat 的受试者基线微生物组具有可比性。在第 10 天给药时，差异丰度分析和β多样性显示接受万古霉素的受试者的微生物组与接受任何剂量 Ibezapolstat 的受试者之间存在明显差异（P=0.006）。α多样性变化的特征是接受 Ibezapolstat 的受试者放线菌门数量增加，而接受万古霉素的受试者变形菌门数量增加。