ورود
مقالات فارسیISIکنفرانسهاژورنالها

Vitamin D suppresses cellular pathways of diabetes complication in liver

Publish place: Iranian Journal of Basic Medical Sciences، Vol: 22، Issue: 6
Publish Year: 1398
نوع سند: مقاله ژورنالی
زبان: English
View: 361

This Paper With 5 Page And PDF Format Ready To Download

  • Certificate
  • من نویسنده این مقاله هستم

این Paper در بخشهای موضوعی زیر دسته بندی شده است:

استخراج به نرم افزارهای پژوهشی:

لینک ثابت به این Paper:
https://civilica.com/doc/942550

شناسه ملی سند علمی:

JR_IJBMS-22-6_015

تاریخ نمایه سازی: 20 مهر 1398

Abstract:

Objective(s): The aim of this study was to investigate the effect of vitamin D on glucose metabolism, as well as the expression of five key genes involved in the development of diabetes complications in liver tissue of diabetic rats. Materials and Methods: Twenty-four male Sprague–Dawley rats were randomly divided into three groups (8 rats in each group). The first group served as control and the other two groups received an intraperitoneal injection of 45 mg/kg streptozotocin to develop diabetes. Groups were treated for four weeks either with placebo or vitamin D (two injections of 20000 IU/kg). Thereafter, serum levels of glucose, insulin and HbA1c were assessed. Liver tissue was examined for the level of advanced glycation end products (AGEs) and the gene expression of AGE cellular receptor (AGER), glyoxalase-1 (GLO-1), aldose reductase (AR), O-linked N-acetylglucosamine transferase (OGT) and glutamine/ fructose-6-phosphate aminotransferase (GFAT). Results: Vitamin D injection resulted in a significant increase in plasma level of 25-hydroxycholecalciferol, which could improve hyperglycemia about 11% compared to placebo-receiving diabetic rats (P=0.005). Insulin level increased as a result of vitamin D treatment compared to control (3.31±0.65 vs. 2.15±0.79; P= 0.01). Serum HbA1c and liver AGE concentrations had a slight but insignificant reduction following vitamin D intake. Moreover, a significant decline was observed in gene expression of AGER and OGT in liver tissue (P=0.04 and PConclusion: Vitamin D might contribute in ameliorating diabetes complications not only by improving blood glucose and insulin levels, but also by suppressing AGER and OGT gene expression in the liver.

Keywords:

Advanced Glycation End Products , Cholecalciferol , Diabetes Complications , Hexosamine pathway , Vitamin D

Authors

Hoda Derakhshanian

Dietary Supplements and Probiotic Research Center, Alborz University of Medical Sciences, Karaj, Iran|Department of Biochemistry, Genetics and Nutrition, School of Medicine, Alborz University of Medical Sciences, Karaj, Iran

Mahmoud Djalali

Department of Cellular and Molecular Nutrition, School of Nutritional Sciences and Dietetics, Tehran University of Medical Sciences, Tehran, Iran

Mohammad Hassan Javanbakht

Department of Cellular and Molecular Nutrition, School of Nutritional Sciences and Dietetics, Tehran University of Medical Sciences, Tehran, Iran

Ehsan Alvandi

Department of Cellular and Molecular Nutrition, School of Nutritional Sciences and Dietetics, Tehran University of Medical Sciences, Tehran, Iran

مراجع و منابع این Paper:

لیست زیر مراجع و منابع استفاده شده در این Paper را نمایش می دهد. این مراجع به صورت کاملا ماشینی و بر اساس هوش مصنوعی استخراج شده اند و لذا ممکن است دارای اشکالاتی باشند که به مرور زمان دقت استخراج این محتوا افزایش می یابد. مراجعی که مقالات مربوط به آنها در سیویلیکا نمایه شده و پیدا شده اند، به خود Paper لینک شده اند :
  • Ogurtsova K, da Rocha Fernandes J, Huang Y, Linnenkamp U, ...
  • Herman WH. The Global burden of diabetes: An overview.  Diabetes ...
  • Madonna R, De Caterina R. Cellular and molecular mechanisms of ...
  • Forbes JM, Cooper ME. Mechanisms of diabetic complications. Physiol Rev. ...
  • Group DPPR. The 10-year cost-effectiveness of lifestyle intervention or metformin ...
  • Evert AB, Boucher JL, Cypress M, Dunbar SA, Franz MJ, ...
  • Ley SH, Hamdy O, Mohan V, Hu FB. Prevention and ...
  • Hyppönen E, Läärä E, Reunanen A, Järvelin M-R, Virtanen SM. ...
  • Pittas AG, Lau J, Hu FB, Dawson-Hughes B. The role ...
  • Kaur H, Donaghue KC, Chan AK, Benitez-Aguirre P, Hing S, ...
  • Shehab D, Al‐Jarallah K, Mojiminiyi O, Al Mohamedy H, Abdella ...
  • Diaz VA, Mainous AG, Carek PJ, Wessell AM, Everett CJ. ...
  • Olfert ED, Cross BM, McWilliam AA. Guide to the care ...
  • Husemoen LLN, Thuesen BH, Fenger M, Jørgensen T, Glümer C, ...
  • Zipitis CS, Akobeng AK. Vitamin D supplementation in early childhood ...
  • Park S, Kim DS, Kang S. Vitamin D deficiency impairs ...
  • Jayanarayanan S, Anju TR, Smijin S, Paulose CS. Vitamin D ...
  • Yang Z, Liu F, Qu H, Wang H, Xiao X, ...
  • Manna P, Jain SK. Vitamin D up-regulates glucose transporter 4 ...
  • Enciso PL, Wang L, Kawahara Y, Sakamoto S, Shimada S, ...
  • Beisswenger PJ, Howell SK, Russell GB, Miller ME, Rich SS, ...
  • Sveen KA, Karimé B, Jørum E, Mellgren SI, Fagerland MW, ...
  • Choudhuri S, Dutta D, Sen A, Chowdhury IH, Mitra B, ...
  • Ramasamy R, Vannucci SJ, Du Yan SS, Herold K, Yan ...
  • Brouwers O, Niessen PM, Ferreira I, Miyata T, Scheffer PG, ...
  • Kawai T, Takei I, Tokui M, Funae O, Miyamoto K, ...
  • Hashimoto Y, Yamagishi SI, Mizukami H, Yabe‐Nishimura C, Lim SW, ...
  • Akimoto Y, Miura Y, Toda T, Wolfert MA, Wells L, ...
  • Park SY, Ryu J, Lee W. O-GlcNAc modification on IRS-1 ...
  • Inbathamizh L, Padmini E. In silico studies on the inhibitory ...
    • نمایش کامل مراجع