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High risk of adrenal toxicity of N1-desoxy quinoxaline 1,4-dioxide derivatives and the protection of oligomeric proanthocyanidins (OPC) in the inhibition of the expression of aldosterone synthetase in H295R cells.

Toxicology.. 2016-02; 
Wang X, Yang C, Ihsan A, Luo X, Guo P, Cheng G, Dai M, Chen D, Liu Z, Yuan Z.
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Gene Synthesis ... ATF-1, Fwd: AGGACTCATCCGACAGCATA Rev: CAGCAGCAGAAACTCCAGAA, 150. SF-1, Fwd: TTGCTGATGACGCTCTTTG Rev: TTTATGTCCTCTTGGGTTAGTG, 281. Note: Primers were manufactured by GenScript (Nanjing) Co., Ltd. (Shanghai, PR China). ... Get A Quote

摘要

Quinoxaline 1,4-dioxide derivatives (QdNOs) with a wide range of biological activities are used in animal husbandry worldwide. It was found that QdNOs significantly inhibited the gene expression of CYP11B1 and CYP11B2, the key aldosterone synthases, and thus reduced aldosterone levels. However, whether the metabolites of QdNOs have potential adrenal toxicity and the role of oxidative stress in the adrenal toxicity of QdNOs remains unclear. The relatively new QdNOs, cyadox (CYA), mequindox (MEQ), quinocetone (QCT) and their metabolites, were selected for elucidation of their toxic mechanisms in H295R cells. Interestingly, the results showed that the main toxic metabolites of QCT, MEQ, and CYA were their N1-desox... More

关键词

Adrenal toxicity; Aldosterone; Cyadox; H295R cells; Mequindox; Quinocetone; Quinoxaline