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N-乙酰-L-半胱氨酸或牛磺酸预处理或后处理对六价铬染毒小鼠心、脾、肺和睾丸的有益作用。

Beneficial Effects of N-Acetyl-L-cysteine or Taurine Pre- or Post-treatments in the Heart, Spleen, Lung, and Testis of Hexavalent Chromium-Exposed Mice.

机构信息

Department of Toxicology, Faculty of Pharmacy, Erciyes University, 38280, Kayseri, Turkey.

Department of Toxicology, Faculty of Pharmacy, Ankara University, 06100, Ankara, Turkey.

出版信息

Biol Trace Elem Res. 2019 Aug;190(2):437-445. doi: 10.1007/s12011-018-1571-z. Epub 2018 Nov 12.

Abstract

Hexavalent chromium[Cr(VI)] compounds may induce toxic effects, possibly via reactive intermediates and radicals formed during Cr(VI) reduction. In this study, we probed the possible effects of N-acetyl-L-cysteine (NAC) and taurine pre- or post-treatments on Cr(VI)-induced changes in lipid peroxidation and nonprotein thiols (NPSH) in mice heart, lung, spleen, and testis tissues. The mice were randomly assigned to six groups, consisting of control, Cr(VI)-exposed (20 mg Cr/kg, intraperitoneal ,ip), NAC (200 mg/kg, ip) as pre-treatment and post-treatment, and taurine (1 g/kg, ip) pre-treatment and post-treatment groups. Lipid peroxidation and NPSH levels were determined and the results were compared with regard to tissue- and antioxidant-specific basis. Exposure to Cr(VI) significantly increased lipid peroxidation in all tissues as compared to the control (p < 0.05); and consistent with this data, NPSH levels were significantly decreased (p < 0.05). Notably, administration of NAC and taurine, either before or after Cr(VI) exposure, was able to ameliorate the lipid peroxidation (p < 0.05) in all tissues. In the case of NPSH content, while the decline could be alleviated by both NAC and taurine pre- and post-treatments in the spleen, diverging results were obtained in other tissues. The effects of Cr(VI) on the lung thiols were abolished by pre-treatment with NAC and taurine; however, post-treatments could not exert significant effect. While thiol depletion in the heart was totally replenished by NAC and taurine administrations, NAC pre-treatment was partially more effective than post-treatment. In contrast with lipid peroxidation data, NAC treatment could not provide a statistically significant beneficial effect on NPSH content of the testis, whereas the effect in this tissue by taurine was profound. Thus, these data highlight the importance of tissue-specific factors and the critical role of administration time. Overall, our data suggest that NAC and taurine may have potential in prevention of Cr(VI)-induced toxicity in the heart, lung, spleen, and testis tissues.

摘要

六价铬[Cr(VI)]化合物可能通过 Cr(VI)还原过程中形成的活性中间体和自由基诱导毒性效应。在这项研究中,我们研究了 N-乙酰-L-半胱氨酸(NAC)和牛磺酸预先或事后处理对 Cr(VI)诱导的小鼠心、肺、脾和睾丸组织中脂质过氧化和非蛋白巯基(NPSH)变化的可能影响。将小鼠随机分为六组,包括对照组、Cr(VI)暴露组(20 mg Cr/kg,腹腔注射,ip)、NAC(200 mg/kg,ip)预处理和后处理组以及牛磺酸(1 g/kg,ip)预处理和后处理组。测定脂质过氧化和 NPSH 水平,并根据组织和抗氧化剂特异性基础进行比较。与对照组相比,Cr(VI)暴露显著增加了所有组织的脂质过氧化(p<0.05);与这一数据一致,NPSH 水平显著降低(p<0.05)。值得注意的是,NAC 和牛磺酸的给药,无论是在 Cr(VI)暴露之前还是之后,都能够改善所有组织的脂质过氧化(p<0.05)。就 NPSH 含量而言,虽然 NAC 和牛磺酸的预处理和后处理都可以减轻脾脏中 NPSH 含量的下降,但在其他组织中得到了不同的结果。Cr(VI)对肺巯基的影响被 NAC 和牛磺酸的预处理所消除;然而,后处理则不能发挥显著的作用。虽然 NAC 和牛磺酸的给药完全补充了心脏中的巯基耗竭,但 NAC 的预处理比后处理更有效。与脂质过氧化数据相比,NAC 处理不能对睾丸组织的 NPSH 含量提供统计学上显著的有益效果,而牛磺酸在该组织中的作用则非常显著。因此,这些数据强调了组织特异性因素的重要性和给药时间的关键作用。总的来说,我们的数据表明,NAC 和牛磺酸可能具有预防 Cr(VI)诱导的心脏、肺、脾和睾丸组织毒性的潜力。

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