HIF Stabilizer Desidustat Protects against Complement-Mediated Diseases.

IF 1.7 Q3 PHARMACOLOGY & PHARMACY
Drug Research Pub Date : 2024-09-01 Epub Date: 2024-07-11 DOI:10.1055/a-2347-9919
Vishal J Patel, Amit A Joharapurkar, Samadhan G Kshirsagar, Maulik S Patel, Hardikkumar H Savsani, Harshad S Dodiya, Milan H Rakhasiya, Ashvin K Patel, Rajesh Sundar, Mukul R Jain
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引用次数: 0

Abstract

Complement cascade is a defence mechanism useful for eliminating pathogenic microorganisms and damaged cells. However, activation of alternative complement system can also cause inflammation and promote kidney and retinal disease progression. Inflammation causes tissue hypoxia, which induces hypoxia-inducible factor (HIF) and HIF helps the body to adapt to inflammation. In this study, we investigated the effect of HIF stabilizer desidustat in complement-mediated diseases. Oral administration of desidustat (15 mg/kg) was effective to reduce the kidney injury in mice that was induced by either lipopolysaccharide (LPS), doxorubicin or bovine serum albumin (BSA)-overload. Complement activation-induced membrane attack complex (MAC) formation and factor B activity were also reduced by desidustat treatment. In addition, desidustat was effective against membranous nephropathy caused by cationic BSA and retinal degeneration induced by sodium iodate in mice. C3-deposition, proteinuria, malondialdehyde, and interleukin-1ß were decreased and superoxide dismutase was increased by desidustat treatment in cBSA-induced membranous nephropathy. Desidustat specifically inhibited alternative complement system, without affecting the lectin-, or classical complement pathway. This effect appears to be mediated by inhibition of factor B. These data demonstrate the potential therapeutic value of HIF stabilization by desidustat in treatment of complement-mediated diseases.

HIF 稳定剂 Desidustat 可预防补体介导的疾病
补体级联是一种防御机制,有助于消除病原微生物和受损细胞。然而,替代性补体系统的激活也会引起炎症,促进肾脏和视网膜疾病的发展。炎症会导致组织缺氧,从而诱导缺氧诱导因子(HIF),HIF 帮助机体适应炎症。本研究探讨了 HIF 稳定剂 desidustat 对补体介导疾病的影响。口服去度斯塔(15 毫克/千克)能有效减轻脂多糖(LPS)、多柔比星或牛血清白蛋白(BSA)超负荷诱导的小鼠肾损伤。地舒司他还能减少补体激活诱导的膜攻击复合物(MAC)的形成和因子 B 的活性。此外,地舒司他对阳离子白蛋白(BSA)引起的膜性肾病和碘酸钠引起的小鼠视网膜变性也有效。地舒司他能减少 cBSA 引起的膜性肾病中的 C3 沉淀、蛋白尿、丙二醛和白细胞介素-1ß,增加超氧化物歧化酶。地舒司他能特异性抑制替代性补体系统,而不影响凝集素或经典补体途径。这些数据证明了地司他稳定 HIF 对治疗补体介导疾病的潜在治疗价值。
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来源期刊
Drug Research
Drug Research PHARMACOLOGY & PHARMACY-
CiteScore
3.50
自引率
0.00%
发文量
67
期刊介绍: Drug Research (formerly Arzneimittelforschung) is an international peer-reviewed journal with expedited processing times presenting the very latest research results related to novel and established drug molecules and the evaluation of new drug development. A key focus of the publication is translational medicine and the application of biological discoveries in the development of drugs for use in the clinical environment. Articles and experimental data from across the field of drug research address not only the issue of drug discovery, but also the mathematical and statistical methods for evaluating results from industrial investigations and clinical trials. Publishing twelve times a year, Drug Research includes original research articles as well as reviews, commentaries and short communications in the following areas: analytics applied to clinical trials chemistry and biochemistry clinical and experimental pharmacology drug interactions efficacy testing pharmacodynamics pharmacokinetics teratology toxicology.
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