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吡啶甲酸铬对肥胖 Zucker 大鼠血糖控制和肾脏的影响。

Effects of chromium picolinate on glycemic control and kidney of the obese Zucker rat.

机构信息

Department of Oral Biology, School of Dentistry, Medical College of Georgia Augusta, Georgia 30912, USA.

出版信息

Nutr Metab (Lond). 2009 Dec 10;6:51. doi: 10.1186/1743-7075-6-51.

Abstract

BACKGROUND

Chromium picolinate (Cr(pic)3) is advocated as adjuvant therapy for impaired glycemic control, despite concerns for DNA damage. Potential toxicity of Cr(pic)3 should be greater for the kidney that accumulates chromium. Therefore, we tested the hypothesis that Cr(pic)3 treatment of obese Zucker rats (OZR) exacerbates renal abnormalities associated with dysglycemia.

METHODS

Male OZR were treated with diets lacking or containing 5 and 10 mg/kg of chromium, as Cr(pic)3, for 20 weeks; lean Zucker rats (LZR) served as controls. Glycemic and renal effects of Cr(pic)3 were determined in the context of indices of oxidative stress and inflammation.

RESULTS

The OZR displayed increased fasting plasma glucose and insulin in association with enlarged pancreatic islets exhibiting collagen and periodic acid Schiff-positive deposits compared to LZR; Cr(pic)3 treatment did not affect these parameters. The OZR, irrespective of Cr(pic)3, excreted more albumin than LZR. Also, other indices of renal function or histopathology were not affected by Cr(pic)3 treatment. Urinary excretion of 8-hydroxydeoxyguanosine (8-OHdG), an index of oxidative DNA damage, was greater in the OZR than LZR; dietary Cr(pic)3 treatment attenuated 8-OHdG excretion. However, immunostaining of kidney for 8-OHdG revealed similar staining pattern and intensity, despite significant renal accumulation of chromium in Cr(pic)3-treated groups. Finally, increased renal nitrotyrosine and cyclooxygenase-2 levels and urinary excretion of monocyte chemoattractant protein-1 of OZR were partially reversed by Cr(pic)3 treatment.

CONCLUSION

Dietary Cr(pic)3 treatment of OZR does not beneficially influence glycemic status or increase the risk for oxidative DNA damage; rather, the treatment attenuates indices of oxidative stress and inflammation.

摘要

背景

尽管存在对 DNA 损伤的担忧,但吡啶甲酸铬 (Cr(pic)3) 仍被提倡作为改善血糖控制的辅助治疗方法。肾脏会积累铬,因此对 Cr(pic)3 的潜在毒性应该更大。因此,我们测试了 Cr(pic)3 治疗肥胖 Zucker 大鼠 (OZR) 是否会加剧与糖代谢异常相关的肾脏异常的假设。

方法

雄性 OZR 用缺乏或含有 5 和 10mg/kg 铬的 Cr(pic)3 的饮食处理 20 周;瘦 Zucker 大鼠 (LZR) 作为对照。在氧化应激和炎症指标的背景下确定 Cr(pic)3 治疗对血糖和肾脏的影响。

结果

OZR 空腹血糖和胰岛素升高,与胰岛胶原和过碘酸希夫阳性沉积物增大有关,与 LZR 相比;Cr(pic)3 治疗并未影响这些参数。无论 Cr(pic)3 如何,OZR 的白蛋白排泄量都高于 LZR。此外,Cr(pic)3 治疗并未影响肾功能或组织病理学的其他指标。8-羟基脱氧鸟苷 (8-OHdG) 的尿排泄量,氧化 DNA 损伤的指标,在 OZR 中高于 LZR;膳食 Cr(pic)3 治疗减轻了 8-OHdG 的排泄。然而,肾脏 8-OHdG 的免疫染色显示出相似的染色模式和强度,尽管 Cr(pic)3 治疗组的肾脏中积累了大量的铬。最后,Cr(pic)3 治疗部分逆转了 OZR 肾脏中硝基酪氨酸和环氧化酶-2 水平以及单核细胞趋化蛋白-1 的尿排泄增加。

结论

膳食 Cr(pic)3 治疗 OZR 不会有益地影响血糖状态或增加氧化 DNA 损伤的风险;相反,该治疗减轻了氧化应激和炎症的指标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7314/2799425/d46fd791e322/1743-7075-6-51-2.jpg

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