Implications of advanced oxidation protein products (AOPPs), advanced glycation end products (AGEs) and other biomarkers in the development of cardiovascular diseases |
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| Authors: | Mahmood Rasool Arif Malik Tariq Tahir Butt Muhammad Abdul Basit Ashraf Rabia Rasool Ayesha Zahid Sulayman Waquar Muhammad Asif Ahmad Zaheer Abdul Jabbar Maryam Zain Asim Mehmood Tahira Batool Qaisrani Imran Riaz Malik Sami Ullah Khan Zeenat Mirza Absarul Haque Mohammed Hussein Al-Qahtani Sajjad Karim |
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| Affiliation: | 1. Center of Excellence in Genomic Medicine Research, King Abdulaziz University, Jeddah, Saudi Arabia;2. Institute of Molecular Biology and Biotechnology, The University of Lahore, Lahore, Pakistan;3. Department of Biotechnology, BUITEMS, Quetta, Pakistan;4. National Institute for Biotechnology and Genetic Engineering, Faisalabad, Pakistan;5. Department of Biotechnology, Mirpur University of Science and Technology (MUST), Mirpur-10250 (AJK), Pakistan;6. Department of Biochemistry and Biotechnology, The Women University, Multan, Pakistan;7. Department of Biosciences, COMSATS University Islamabad, Sahiwal Campus, Sahiwal, Pakistan;8. Faculty of Agricultural Sciences, Ghazi University, Dera Ghazi Khan, Pakistan;9. Department of Biotechnology, University of Sargodha, Sargodha, Pakistan;10. Department of Botany, Women University of Azad Jammu & Kashmir, Bagh, Pakistan;11. King Fahd Medical Research Center, King Abdulaziz University, Jeddah, Saudi Arabia |
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| Abstract: | ObjectiveTo study the putative effects of Advanced Oxidation Protein Products (AOPPs) and Advanced Glycation End Products (AGEs) in the development and progression of cardiovascular disease (CVD).MethodologyAGEs, AOPPs, e-NOS, lipid profile, circulating stress and inflammatory biomarkers were evaluated among fifty cardiovascular patients and fifty controls. Independent student’s t-test was done for statistical analysis.ResultsThe malondialdehyde mean level in CVD patients (5.45?nmol/ml) was significantly higher than control (1.36?nmol/ml) (p value?=?0.018). Nitric oxide in CVD patients (55.72?ng/ml) was remarkably increased as compared to normal subjects (19.19?ng/ml). A significant change in the mean serum level of AGEs in CVD patients (2.74?ng/ml) and normal individuals (0.85?ng/ml) was recorded (p value?=?0.000). The AOPPs also showed significant increased levels in CVD group (132.07?ng/ml) in comparison with normal subjects (83.05?ng/ml) (p value?=?0.011). The mean eNOS serum level in CVD group (15.50?U/L) was higher than control group (11.28?U/L) (p value?=?0.004). Cardiovascular disease patients, in comparison with healthy controls, showed increased level of total cholesterol (5.48?mmol/L vs 4.45?mmol/L), triglycerides (2.59?mmol/L vs 1.24?mmol/L), and low density lipoprotein (2.47?mmol/L vs 2.31?mmol/L) along with decrease in high density lipoprotein (1.39?mmol/L vs 1.74?mmol/L). The mean MMP-11 serum levels in CVD group (98.69?ng/ml) was almost double of control group (45.60?ng/ml) (p value?=?0.017). The mean serum level of TNF-α and IL1-α were 32.16?pg/ml and 6.64?pg/ml in CVD patient. The significant decreasing trend of SOD (p value?=?0.041), CAT (p value?=?0.018), GSH (p value?=?0.036) and GRx (p value?=?0.029) but increasing drift of GPx (0.023) level was observed in CVD patients.ConclusionThis study provides strong evidence that CVD patients presented with elevated oxidative stress, enhanced inflammation and lipid profile in their serum. Therefore, the study strongly approves that AGEs, AOPPs, inflammatory and lipoxidative biomarkers hold predictive potential in causing and aggravating the disease, thus by controlling these factors CVD progression can be inhibited. |
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| Keywords: | Cardiovascular diseases Advanced glycation end products Advanced oxidation protein products Endothelial nitric oxide synthase Matrix metalloproteinase-11 |
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