| Literature DB >> 30439361 |
Tahir Ali1, Iram Mushtaq1, Sonia Maryam1, Anam Farhan1, Kiran Saba1, Muhammad Ishtiaq Jan1, Aneesa Sultan1, Mariam Anees1, Burcu Duygu2, Sadia Hamera3, Sobia Tabassum4, Qamar Javed5, Paula A da Costa Martins6, Iram Murtaza7.
Abstract
Early and specific diagnosis of oxidative stress linked diseases as cardiac heart diseases remains a major dilemma for researchers and clinicians. MicroRNAs may serve as a better tool for specific early diagnostics and propose their utilization in future molecular medicines. We aimed to measure the microRNAs expressions in oxidative stress linked cardiac hypertrophic condition induced through stimulants as Endothelin and Isoproterenol. Cardiac hypertrophic animal models were confirmed by BNP, GATA4 expression, histological assays, and increased cell surface area. High oxidative stress (ROS level) and decreased antioxidant activities were assessed in hypertrophied groups. Enhanced expression of miR-152, miR-212/132 while decreased miR-142-3p expression was observed in hypertrophic condition. Similar pattern of these microRNAs was detected in HL-1 cells treated with H2O2. Upon administration of antioxidants, the miRNAs expression pattern altered from that of the cardiac hypertrophied model. Present investigation suggests that oxidative stress generated during the cardiac pathology may directly or indirectly regulate anti-hypertrophy pathway elements through microRNAs including antioxidant enzymes, which need further investigation. The down-regulation of free radical scavengers make it easier for the oxidative stress to play a key role in disease progression.Entities:
Keywords: Cardiac hypertrophy; Endothelin; Isoproterenol; Oxidative stress; miRNAs
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Year: 2018 PMID: 30439361 DOI: 10.1016/j.abb.2018.11.007
Source DB: PubMed Journal: Arch Biochem Biophys ISSN: 0003-9861 Impact factor: 4.013