Role of albumin in the metabolism and excretion of ochratoxin A.

IF 2.6 4区 医学 Q2 MYCOLOGY Mycotoxin Research Pub Date : 2024-08-01 Epub Date: 2024-05-14 DOI:10.1007/s12550-024-00538-1
Michael Kuhn, Reham Hassan, Daniela González, Maiju Myllys, Zaynab Hobloss, Gisela H Degen, Hans-Ulrich Humpf, Jan G Hengstler, Benedikt Cramer, Ahmed Ghallab
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Abstract

Ochratoxin A (OTA) is known to be strongly bound to serum albumin, but it remains unknown how albumin affects its metabolism and kinetics. To close this gap, we used a mouse model, where heterozygous albumin deletion reduces serum albumin to concentrations similar to hypoalbuminemic patients and completely eliminates albumin by a homozygous knockout. OTA and its potential metabolites (OTα, 4-OH-OTA, 7'-OH-OTA, OTHQ, OP-OTA, OTB-GSH, OTB-NAC, OTB) were time-dependently analyzed in plasma, bile, and urine by LC-MS/MS and were compared to previously published hepatotoxicity and nephrotoxicity data. Homozygous albumin deletion strongly accelerated plasma clearance as well as biliary and urinary excretion of the parent compound and its hydroxylation products. Decreasing albumin in mice by the heterozygous and even more by the homozygous knockout leads to an increase in the parent compound in urine which corresponded to increased nephrotoxicity. The role of albumin in OTA-induced hepatotoxicity is more complex, since heterozygous but not homozygous nor wild-type mice showed a strong biliary increase in the toxic open lactone OP-OTA. Correspondingly, OTA-induced hepatotoxicity was higher in heterozygous than in wild-type and homozygous animals. We present evidence that albumin-mediated retention of OTA in hepatocytes is required for formation of the toxic OP-OTA, while complete albumin elimination leads to rapid biliary clearance of OTA from hepatocytes with less formation of OP-OTA. In conclusion, albumin has a strong influence on metabolism and toxicity of OTA. In hypoalbuminemia, the parent OTA is associated with increased nephrotoxicity and the open lactone with increased hepatotoxicity.

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白蛋白在赭曲霉毒素 A 的代谢和排泄中的作用。
众所周知,赭曲霉毒素A(OTA)与血清白蛋白的结合力很强,但白蛋白如何影响其代谢和动力学仍是未知数。为了填补这一空白,我们使用了一种小鼠模型,在这种模型中,杂合性白蛋白缺失会使血清白蛋白降低到与低白蛋白血症患者相似的浓度,而同源性白蛋白缺失则会完全消除白蛋白。通过 LC-MS/MS,对血浆、胆汁和尿液中的 OTA 及其潜在代谢物(OTα、4-OH-OTA、7'-OH-OTA、OTHQ、OP-OTA、OTB-GSH、OTB-NAC、OTB)进行了时间依赖性分析,并与之前公布的肝毒性和肾毒性数据进行了比较。同基因白蛋白缺失强烈加速了母体化合物及其羟化产物的血浆清除、胆汁排泄和尿液排泄。通过杂合子和同源基因敲除减少小鼠体内的白蛋白会导致尿液中母体化合物的增加,从而增加肾毒性。白蛋白在 OTA 诱导的肝毒性中的作用更为复杂,因为杂合子小鼠而非同合子小鼠或野生型小鼠显示出毒性开放内酯 OP-OTA 的强烈胆汁增加。相应地,OTA 诱导的肝毒性在杂合子动物中高于野生型和同源动物。我们提出的证据表明,白蛋白介导的 OTA 在肝细胞中的滞留是毒性 OP-OTA 形成的必要条件,而白蛋白的完全清除会导致肝细胞中 OTA 的快速胆汁清除,并减少 OP-OTA 的形成。总之,白蛋白对 OTA 的代谢和毒性有很大影响。在低白蛋白血症的情况下,母体 OTA 的肾毒性增加,而开放内酯的肝毒性增加。
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来源期刊
Mycotoxin Research
Mycotoxin Research MYCOLOGYTOXICOLOGY-TOXICOLOGY
CiteScore
6.40
自引率
6.70%
发文量
29
期刊介绍: Mycotoxin Research, the official publication of the Society for Mycotoxin Research, is a peer-reviewed, scientific journal dealing with all aspects related to toxic fungal metabolites. The journal publishes original research articles and reviews in all areas dealing with mycotoxins. As an interdisciplinary platform, Mycotoxin Research welcomes submission of scientific contributions in the following research fields: - Ecology and genetics of mycotoxin formation - Mode of action of mycotoxins, metabolism and toxicology - Agricultural production and mycotoxins - Human and animal health aspects, including exposure studies and risk assessment - Food and feed safety, including occurrence, prevention, regulatory aspects, and control of mycotoxins - Environmental safety and technology-related aspects of mycotoxins - Chemistry, synthesis and analysis.
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