The Renal and Liver Complications Development among Patients with Type 2 Diabetes Mellitus in Kirkuk City
DOI:
https://doi.org/10.51173/jt.v4i2.478Keywords:
Renal Disease, Type 2 Diabetes, Liver Disease, Complication, Glomerular Filtration RateAbstract
Diabetes is a chronic metabolic malady that has raised levels of blood glucose, which in last, it will cause severe harms to the heart, blood vessels, eyes, kidneys, and nerves. In this article trials to investigate the development of the renal and liver disorders among patients with T2DM in a population of Kirkuk city. The hospital-based cases- control study was conducted for patients with T2DM patients that attended the diabetic clinics in Kirkuk during the period from March 2021– to August 2021 and were screened for serum conc. of liver function tests (Alanine Aminotransferase (ALT), Aspartate Aminotransferase (AST) and Alkaline Phosphatase (ALP)), renal function tests (Creatinine and Urea) especially with (family history of diabetes, & hypertension. Patients recruited for this study, showed serum urea and creatinine significantly more than that in control, p < .001, while for renal glomerular filtration rates significantly lower than that in control group, p < 001. Their kidney disease stage frequencies were significantly different in diabetic patients than in control P< 0.001. Stage (II) was the most frequently stage within the T2DM group (n = 58, 58%), while stage (I) was the most frequently observed category within the control group (n = 28, 56%). The mean of AST for T2DM (30.63± 6.08) was significantly more than that in the control (25.13± 4.32). T2DM reveal significant differences in the mean value (32.51± 8.96) of ALT which was more than the control (20.59± 4.38). The estimation of GFR as soon as possible with testing of urea and creatinine confirms the diagnosis of renal disease and staging of the renal disease. The liver enzymes illustrate in T2DM a significant correlation in comparison to the control group.
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References
Artasensi A, Pedretti A, Vistoli G. Fumagalli L. Type 2 Diabetes Mellitus: A Review of Multi-Target Drugs. Molecules. 25, 1987; (2020).
Riddle M. C. Standards of Medical Care in diabetes. The Journal of Clinical and Applied Research and Education. (43), 1; s1–s212 (2020).
Zheng Y, Ley S. H, Hu F. B. Global aetiology and epidemiology of type 2 diabetes mellitus and its complications. Nature Reviews | Endocrinology, (14); 88- 98; (2018).
Selby N. M, Taal M. W. An updated overview of diabetic nephropathy: Diagnosis, prognosis, treatment goals, and latest guidelines. Diabetes Obes Metab. 22(Suppl. 1):3–15; (2020).
Ruiz-Ortega M, Rodrigues-Diez R. R, Lavoz C, Rayego-Mateos S. Special Issue “Diabetic Nephropathy: Diagnosis, Prevention, and Treatment”. J. Clin. Med., 9, 813; 1-4; (2020).
Jha S. K, Yadav N. K, Rizal Sh. Prevalence of elevated liver enzymes and its association with type 2 diabetes: A Descriptive Cross-Sectional Study among Nepalese Adults from Biratnagar, Nepal. Asian Journal of Medical Sciences, 12:6; 50-55; (2021).
Kim H, Lee D. S, An T. H, Park H, Kim W. K, Bae K, Oh K. Metabolic Spectrum of Liver Failure in Type 2 Diabetes and Obesity: From NAFLD to NASH to HCC. Int. J. Mol. Sci, 22, 4495; (2021).
Hsieh Y.-H, Wang W.-C, Hung T.-W, Lee C.-C, Tsai J.-P. C-C Motif Chemokine Ligand-17 as a Novel Biomarker and Regulator of Epithelial-Mesenchymal Transition in Renal Fibrogenesis. Cells, 10, 3345; 1- 14; (2021).
Kidney Health Australia. Fact sheet; Estimated Glomerular Filtration Rate (eGFR) (2020). www.kidney.org.au
Chiu H, Lee M‑Y, Wu P‑Y, Huang J‑Ch, Chen S‑Ch, Chang J‑M. Comparison of the effects of sibling and parental history of type 2 diabetes on metabolic syndrome. Scientific Reports |nature research. 10:22131; 1- 8; (2020).
Kyrou I, Tsigos C, Mavrogianni Ch, Cardon G, Stappen V. V, Latomme J, Kivelä J, Wikström K, Tsochev K, et al . Mateo-GallegoSociodemographic and lifestyle-related risk factors for identifying vulnerable groups for type 2 diabetes: a narrative review with emphasis on data from Europe. BMC Endocrine Disorders, 20(1):134; 1- 13; (2020).
Zeru M. A, Tesfa E, Mitiku A. A, Seyoum A, Bokoro T. A. Prevalence and risk factors of type‑2 diabetes mellitus in Ethiopia: systematic review and meta‑analysis. Scientific Reports | nature research, 11:21733; (2021).
Qiu Ch, Williams M. A, Leisenring W. M, Sorensen T. K, Frederick I. O, Dempsey J. C, Luthy D. A. Family History of Hypertension and Type 2 Diabetes in Relation to Preeclampsia Risk. Hypertension. 41:408- 413; (2003).
Radcliffe N. J, Seah J. M, Clarke M, MacIsaac R. J, Jerums G, Ekinci E. I. Clinical predictive factors in diabetic kidney disease progression. J Diabetes Investig. 8(1):6-18; (2017).
Luis-Lima S, Higueras L. T, Henríquez-Gómez L, Alonso-Pescoso R. Jimenez A, López-Hijazo A. M, Negrín-Mena N, Martín C, Sánchez-Gallego M, Galindo-Hernández S. J, et al. The error of estimated GFR in type 2 diabetes mellitus. J. Clin. Med, 8, 1543; (2019).
Shibabaw T, Dessie G, Molla M. D, Zerihun M. F, Ayelign B. Assessment of liver marker enzymes and its association with type 2 diabetes mellitus in Northwest Ethiopia. BMC Res Notes, 12:707; (2019).
Sunitha S, Gandham R, Wilma DS, Rao S. Evaluation of the significance of liver enzymes as screening tests for the early detection of clinically asymptomatic nonalcoholic fatty liver disease in type 2 diabetes mellitus patients. Int J Biomed Adv Res. 6(12):860–3; (2015).
Judi L, Toukan A, Khader Y, Ajlouni K, Khatib MA. Prevalence of elevated hepatic transaminases among Jordanian patients with type 2 diabetes mellitus. Ann Saudi Med. 30(1):25; (2010).
Acharya A, Wudneh E, Krishnan R, Ashraf A, Tohid H. Diabetes and Liver an Association: Hepatogenous Diabetes Mechanism and Some Evidence. J Cell Sci Ther, 7: 257; 1- 6; (2016).
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Copyright (c) 2022 Wasan Talib Abed, Walaa Esmael Jassim, Emad Mohamed Rasheed
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