Department of Nutrition Science, Purdue University, West Lafayette, Indiana, USA; Division of Nephrology, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana, USA.
Department of Nutrition Science, Purdue University, West Lafayette, Indiana, USA.
Kidney Int. 2021 May;99(5):1225-1233. doi: 10.1016/j.kint.2020.09.035. Epub 2020 Oct 31.
The treatment of hyperphosphatemia remains challenging in patients receiving hemodialysis. This phase 1b study assessed safety and efficacy of EOS789, a novel pan-inhibitor of phosphate transport (NaPi-2b, PiT-1, PiT-2) on intestinal phosphate absorption in patients receiving intermittent hemodialysis therapy. Two cross-over, randomized order studies of identical design (ten patients each) compared daily EOS789 50 mg to placebo with meals and daily EOS789 100 mg vs EOS789 100 mg plus 1600 mg sevelamer with meals. Patients ate a controlled diet of 900 mg phosphate daily for two weeks and began EOS789 on day four. On day ten, a phosphate absorption testing protocol was performed during the intradialytic period. Intestinal fractional phosphate absorption was determined by kinetic modeling of serum data following oral and intravenous doses of Phosphate (P). The results demonstrated no study drug related serious adverse events. Fractional phosphate absorption was 0.53 (95% confidence interval: 0.39,0.67) for placebo vs. 0.49 (0.35,0.63) for 50 mg EOS789; and 0.40 (0.29,0.50) for 100 mg EOS789 vs. 0.36 (0.26,0.47) for 100 mg EOS789 plus 1600 mg sevelamer (all not significantly different). The fractional phosphate absorption trended lower in six patients who completed both studies with EOS789 100 mg compared with placebo. Thus, in this phase 1b study, EOS789 was safe and well tolerated. Importantly, the use of P as a sensitive and direct measure of intestinal phosphate absorption allows specific testing of drug efficacy. The effectiveness of EOS789 needs to be evaluated in future phase 2 and phase 3 studies.
在接受血液透析的患者中,治疗高磷血症仍然具有挑战性。这项 1b 期研究评估了新型肠道磷转运(NaPi-2b、PiT-1、PiT-2)全抑制剂 EOS789 对接受间歇性血液透析治疗的患者肠道磷吸收的安全性和疗效。两项完全相同设计的交叉、随机顺序研究(各 10 例患者)比较了每日 EOS789 50mg 与餐时安慰剂和每日 EOS789 100mg 与餐时 EOS789 100mg 加 1600mg 司维拉姆的疗效。患者接受为期两周的 900mg 磷酸盐控制饮食,第四天开始服用 EOS789。第十天,在透析期间进行了磷吸收测试方案。通过口服和静脉给予磷酸盐(P)后血清数据的动力学模型确定肠道磷吸收分数。结果显示,无与研究药物相关的严重不良事件。安慰剂组的磷吸收分数为 0.53(95%置信区间:0.39,0.67),50mg EOS789 组为 0.49(0.35,0.63),100mg EOS789 组为 0.40(0.29,0.50),100mg EOS789 加 1600mg 司维拉姆组为 0.36(0.26,0.47),均无显著差异。在完成两项 EOS789 100mg 研究的六名患者中,磷吸收分数呈下降趋势,与安慰剂相比。因此,在这项 1b 期研究中,EOS789 安全且耐受良好。重要的是,使用 P 作为肠道磷吸收的敏感和直接测量方法可以特异性测试药物疗效。EOS789 的有效性需要在未来的 2 期和 3 期研究中进行评估。
