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二价铬-半胱氨酸补充可以降低血糖、CRP、MCP-1、ICAM-1、肌酐,这显然是通过提高血液中维生素 C 和脂联素水平以及抑制 NFkappaB、Akt 和肝脏中的 Glut-2 来实现的,在 Zucker 糖尿病肥胖大鼠中。

Chromium dinicocysteinate supplementation can lower blood glucose, CRP, MCP-1, ICAM-1, creatinine, apparently mediated by elevated blood vitamin C and adiponectin and inhibition of NFkappaB, Akt, and Glut-2 in livers of zucker diabetic fatty rats.

机构信息

Department of Pediatrics, Louisiana State University Health Sciences Center, Shreveport, LA 71130, USA.

出版信息

Mol Nutr Food Res. 2010 Sep;54(9):1371-80. doi: 10.1002/mnfr.200900177.

Abstract

Chromium and cysteine supplementation can improve glucose metabolism in animal studies. This study examined the hypothesis that a cysteinate complex of chromium is significantly beneficial than either of them in lowering blood glucose and vascular inflammation markers in Zucker diabetic fatty (ZDF) rats. Starting at the age of 6 wk, ZDF rats were supplemented orally (daily gavages for 8 more weeks) with saline-placebo (D) or chromium (400 microg Cr/Kg body weight) as chromium dinicocysteinate (CDNC), chromium dinicotinate (CDN) or chromium picolinate (CP) or equimolar L-cysteine (LC, img/Kg body weight), and fed Purina 5008 diet for 8 wk. ZDF rats of 6 wk age before any supplementations and onset of diabetes were considered as baseline. D rats showed elevated levels of fasting blood glucose, HbA(1), CRP, MCP-1, ICAM-1 and oxidative stress (lipid peroxidation) and lower adiponectin and vitamin C, when compared with baseline rats. In comparison to D group, CDNC group had significantly lower blood glucose, HbA(1), CRP, MCP-1, ICAM-1 and lipid peroxidation and increased vitamin C and adiponectin levels. CDN, CP or LC showed significantly less or no effect on these biomarkers. Only CDNC lowered blood creatinine levels in comparison to D. While CDN and CP had no effect, activation of NFkappaB, Akt and glucose transporter-2 levels were decreased, insulin receptor substrate 1 (IRS-1) activation increased in livers of CDNC-rats. CDNC effect on glycemia, NFkappaB, Akt and IRS-1 in liver was significantly greater compared with LC. Blood chromium levels did not differ between Cr-groups. Exogenous vitamin C supplementation significantly inhibited MCP-1 secretion in U937 monocytes cultured in high-glucose-medium. CDNC is a potent hypoglycemic compound with anti-inflammatory activity apparently mediated by elevated blood vitamin C and adiponectin and inhibition of NFkappaB, Akt, and Glut-2 and increased IRS-1 activation in livers of type 2 diabetic rats.

摘要

铬和半胱氨酸补充可以改善动物研究中的葡萄糖代谢。这项研究检验了一个假设,即铬半胱氨酸络合物在降低 Zucker 糖尿病肥胖(ZDF)大鼠的血糖和血管炎症标志物方面明显优于其中任何一种。从 6 周龄开始,ZDF 大鼠每天口服补充(再持续 8 周)盐水-安慰剂(D)或铬(400μg Cr/kg 体重)作为二价铬-半胱氨酸(CDNC)、二价铬-烟酸(CDN)或吡啶甲酸铬(CP)或等摩尔 L-半胱氨酸(LC,img/kg 体重),并喂食 Purina 5008 饮食 8 周。在开始任何补充和糖尿病发病之前,6 周龄的 ZDF 大鼠被视为基线。与基线大鼠相比,D 组大鼠的空腹血糖、HbA(1)、CRP、MCP-1、ICAM-1 和氧化应激(脂质过氧化)水平升高,而脂联素和维生素 C 水平降低。与 D 组相比,CDNC 组的血糖、HbA(1)、CRP、MCP-1、ICAM-1 和脂质过氧化水平显著降低,维生素 C 和脂联素水平升高。CDN、CP 或 LC 对这些生物标志物的影响明显较小或没有。只有 CDNC 与 D 相比降低了血肌酐水平。虽然 CDN 和 CP 没有效果,但 NFkappaB、Akt 和葡萄糖转运蛋白-2 水平的激活降低,CDNC 大鼠肝脏中的胰岛素受体底物 1(IRS-1)激活增加。与 LC 相比,CDNC 对肝脏中血糖、NFkappaB、Akt 和 IRS-1 的作用明显更大。各组血液中的铬水平没有差异。外源性维生素 C 补充显著抑制了高糖培养基中 U937 单核细胞中 MCP-1 的分泌。CDNC 是一种有效的降血糖化合物,具有抗炎活性,显然是通过提高血液中维生素 C 和脂联素水平、抑制 NFkappaB、Akt、Glut-2 和增加 2 型糖尿病大鼠肝脏中的 IRS-1 激活来介导的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/50b7/3138725/0711ec4a4bf3/nihms261415f1.jpg

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