Effects of EOS789, a novel pan-phosphate transporter inhibitor, on phosphate metabolism : Comparison with a conventional phosphate binder.

IF 0.7 Q4 MEDICINE, RESEARCH & EXPERIMENTAL JOURNAL OF MEDICAL INVESTIGATION Pub Date : 2023-01-01 DOI:10.2152/jmi.70.260
Kazuya Tanifuji, Yuji Shiozaki, Megumi Koike, Minori Uga, Aoi Komiya, Mizuki Miura, Ayami Higashi, Takaaki Shimohata, Akira Takahashi, Noriko Ishizuka, Hisayoshi Hayashi, Yasuhiro Ichida, Shuichi Ohtomo, Naoshi Horiba, Ken-Ichi Miyamoto, Hiroko Segawa
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Abstract

Background: Inorganic phosphate (Pi) binders are the only pharmacologic treatment approved for hyperphosphatemia. However, Pi binders induce the expression of intestinal Pi transporters and have limited effects on the inhibition of Pi transport. EOS789, a novel pan-Pi transporter inhibitor, reportedly has potent efficacy in treating hyperphosphatemia. We investigated the properties of EOS789 with comparison to a conventional Pi binder.

Methods: Protein and mRNA expression levels of Pi transporters were measured in intestinal and kidney tissues from male Wistar rats fed diets supplemented with EOS789 or lanthanum carbonate (LC). 32Pi permeability was measured in intestinal tissues from normal rats using a chamber.

Results: Increased protein levels of NaPi-2b, an intestinal Pi transporter, and luminal Pi removal were observed in rats treated with LC but not in rats treated with EOS789. EOS789 but not LC suppressed intestinal protein levels of the Pi transporter Pit-1 and sodium/hydrogen exchanger isoform 3. 32Pi flux experiments using small intestine tissues from rats demonstrated that EOS789 may affect transcellular Pi transport in addition to paracellular Pi transport.

Conclusion: EOS789 has differing regulatory effects on Pi metabolism compared to LC. The properties of EOS789 may compensate for the limitations of LC therapy. The combined or selective use of EOS789 and conventional Pi binders may allow tighter control of hyperphosphatemia. J. Med. Invest. 70 : 260-270, February, 2023.

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新型泛磷酸盐转运蛋白抑制剂EOS789对磷酸盐代谢的影响:与传统磷酸盐结合剂的比较。
背景:无机磷酸盐(Pi)结合剂是唯一被批准用于高磷血症的药物治疗。然而,Pi结合物诱导肠道Pi转运蛋白的表达,对Pi转运的抑制作用有限。EOS789是一种新型pan-Pi转运蛋白抑制剂,据报道在治疗高磷血症方面有强有力的疗效。我们研究了EOS789的性能,并与传统的Pi粘合剂进行了比较。方法:分别饲喂添加EOS789和碳酸镧(LC)的雄性Wistar大鼠,测定其肠道和肾脏组织中Pi转运蛋白和mRNA的表达水平。采用腔室法测定正常大鼠肠组织的32Pi通透性。结果:LC处理的大鼠肠道Pi转运蛋白NaPi-2b和管腔Pi清除蛋白水平升高,而EOS789处理的大鼠则没有。EOS789而非LC抑制Pi转运蛋白Pit-1和钠/氢交换物异构体3的肠道蛋白水平。利用大鼠小肠组织进行的Pi通量实验表明,EOS789除了影响细胞旁Pi转运外,还可能影响Pi的跨细胞转运。结论:与LC相比,EOS789对Pi代谢具有不同的调节作用。EOS789的特性可以弥补LC治疗的局限性。联合或选择性使用EOS789和传统的Pi粘合剂可以更严格地控制高磷血症。中国医学杂志,30(2),2023。
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来源期刊
JOURNAL OF MEDICAL INVESTIGATION
JOURNAL OF MEDICAL INVESTIGATION MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
1.20
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0.00%
发文量
55
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