Sodium thiosulfate treatment rescues hyperglycaemia-induced pronephros damage in zebrafish by upregulating nitric oxide signalling.

The Journal of Physiology Pub Date : 2024-09-12 DOI:10.1113/jp286398

Hannes Ott,Katrin Bennewitz,Xin Zhang,Mariia Prianichnikova,Carsten Sticht,Gernot Poschet,Jens Kroll

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Abstract

Sodium thiosulfate (STS) is gaining increasing attention in research for its potential therapeutic applications across a spectrum of disease processes beyond its current uses. However, the precise mechanisms of action remain incompletely understood. We investigated the efficacy of STS in treating hyperglycaemia-induced pronephros damage in zebrafish to gain further insight into the underlying mechanisms. Hyperglycaemia was induced in zebrafish by suppressing the pdx1 transcription factor, which plays a crucial role in maintaining physiological pancreatic function. STS was administered by introducing it into the medium of zebrafish larvae. The pronephros structure was analysed at 48 h post-fertilization. Metabolomic profiling and RNA sequencing were conducted on groups exposed to various experimental conditions. Our findings reveal a downregulation of nitric oxide (NO) signalling in zebrafish with a knocked-down pdx1 gene, both metabolomically and transcriptionally. Notably, treatment with STS led to a compensatory upregulation of the NO signalling, ultimately resulting in the rescue of the pronephros structure. Our study provides compelling evidence that targeting NO metabolism by the administration of STS offers a promising strategy for addressing hyperglycaemia-induced organ damage. These findings underscore the potential of STS as a promising therapeutic agent for diabetic complications and warrant further investigation of its clinical applications. KEY POINTS: Sodium thiosulfate (STS) is increasingly drawing attention in research for its potential therapeutic applications across a spectrum of disease processes. Here, we demonstrate that STS treatment rescues hyperglycaemia-induced pronephros damage in zebrafish. We identified upregulation of nitric oxide signalling as the major driver behind STS-mediated rescue. Our data suggest that STS offers a promising strategy for addressing hyperglycaemia-induced organ damage, including diabetic nephropathy.

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硫代硫酸钠处理通过上调一氧化氮信号来挽救斑马鱼因高血糖引起的前肾损伤。

硫代硫酸钠（STS）因其在多种疾病过程中的潜在治疗应用而越来越受到研究人员的关注。然而，人们对其确切的作用机制仍不甚了解。我们研究了 STS 在治疗高血糖诱导的斑马鱼前肾损伤方面的疗效，以进一步了解其潜在机制。我们通过抑制 pdx1 转录因子诱导斑马鱼发生高血糖，该转录因子在维持胰腺生理功能方面发挥着关键作用。在斑马鱼幼体的培养基中加入 STS。受精后 48 小时对前肾结构进行分析。对暴露于各种实验条件下的斑马鱼组进行了代谢组学分析和 RNA 测序。我们的研究结果表明，在pdx1基因被敲除的斑马鱼体内，一氧化氮（NO）信号在代谢和转录两方面都出现了下调。值得注意的是，用 STS 治疗会导致一氧化氮信号的代偿性上调，最终导致代肾脏结构的恢复。我们的研究提供了令人信服的证据，即通过施用 STS 来靶向 NO 代谢，为解决高血糖诱发的器官损伤提供了一种前景广阔的策略。这些发现凸显了 STS 作为糖尿病并发症治疗药物的潜力，值得进一步研究其临床应用。关键点：硫代硫酸钠（STS）因其在多种疾病过程中的潜在治疗应用而日益受到研究人员的关注。在这里，我们证明了硫代硫酸钠治疗可挽救高血糖诱导的斑马鱼前肾损伤。我们发现一氧化氮信号的上调是 STS 介导的救治背后的主要驱动因素。我们的数据表明，STS 为解决高血糖诱导的器官损伤（包括糖尿病肾病）提供了一种前景广阔的策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Journal of Physiology

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