Lubiprostone in chronic kidney disease: Insights into mitochondrial function and polyamines from a randomized phase 2 clinical trial

鲁比前列酮治疗慢性肾脏病:一项随机 II 期临床试验揭示线粒体功能和多胺的机制

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作者:Shun Watanabe,Masaaki Nakayama,Takashi Yokoo,Satoru Sanada,Yoshifumi Ubara,Atsushi Komatsuda,Katsuhiko Asanuma,Yusuke Suzuki,Tsuneo Konta,Junichiro J Kazama,Takehiro Suzuki,Shinji Fukuda,Tomoyoshi Soga,Takuji Yamada,Sayaka Mizutani,Mitsuharu Matsumoto,Yuji Naito,Kensei Taguchi,Kei Fukami,Hitomi Kashiwagi,Koichi Kikuchi,Chitose Suzuki,Hidetaka Tokuno,Marina Urasato,Ryota Kujirai,Yotaro Matsumoto,Yasutoshi Akiyama,Yoshihisa Tomioka,Shun Itai,Yoshiyasu Tongu,Eikan Mishima,Chiharu Kawabe,Tomoko Kasahara,Yoshiaki Ogata,Takafumi Toyohara,Takeya Sato,Tetsuhiro Tanaka,Takaaki Abe

Abstract

Chronic kidney disease (CKD) is a life-threatening condition, and constipation is a progressive risk factor. We evaluated changes in uremic toxins, renal function, and the safety of lubiprostone, a selective chloride channel activator, in patients with CKD. In this phase 2, randomized, double-blind, placebo-controlled trial across nine centers in Japan, 150 patients with stage IIIb-IV CKD received lubiprostone (8 or 16 micrograms) or placebo for 24 weeks. The primary end point was change in indoxyl sulfate levels. Secondary end points included other uremic toxins and renal function markers. Lubiprostone did not alter uremic toxin levels but improved or preserved estimated glomerular filtration rate and its slope in the 16-microgram group. Mild-to-moderate gastrointestinal events occurred in the placebo and 16-microgram groups. Multiomics analysis revealed that lubiprostone modulated the gut microbial agmatine pathway and increased spermidine levels, thereby improving renal mitochondrial function. Lubiprostone is a previously unknown and safe therapeutic option to mitigate renal decline in CKD.

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