Severity of coronary artery disease is associated with diminished circANRIL expression: A possible blood based transcriptional biomarker in East Africa

Author:

Akan Gokce12ORCID,Nyawawa Evarist3,Nyangasa Bashir3,Turkcan Mehmet Kerem4,Mbugi Erasto1,Janabi Mohammed3,Atalar Fatmahan15

Affiliation:

1. Biochemistry Department, MUHAS Genetics Laboratory, School of Medicine Muhimbili University of Health and Allied Sciences Dar es Salaam Tanzania

2. Near East University DESAM Research Institute Mersin North Cyprus Turkey

3. Jakaya Kikwete Cardiac Institute Dar es Salaam Tanzania

4. Department of Electrical Engineering Columbia University New York New York USA

5. Department of Rare Diseases Istanbul University, Child Health Institute Istanbul Turkey

Abstract

AbstractAntisense Noncoding RNA in the INK4 Locus (ANRIL) is the prime candidate gene at Chr9p21, the well‐defined genetic risk locus associated with coronary artery disease (CAD). ANRIL and its transcript variants were investigated for the susceptibility to CAD in adipose tissues (AT) and peripheral blood mononuclear cells (PBMCs) of the study group and the impact of 9p21.3 locus mutations was further analysed. Expressions of ANRIL, circANRIL (hsa_circ_0008574), NR003529, EU741058 and DQ485454 were detected in epicardial AT (EAT) mediastinal AT (MAT), subcutaneous AT (SAT) and PBMCs of CAD patients undergoing coronary artery bypass grafting and non‐CAD patients undergoing heart valve surgery. ANRIL expression was significantly upregulated, while the expression of circANRIL was significantly downregulated in CAD patients. Decreased circANRIL levels were significantly associated with the severity of CAD and correlated with aggressive clinical characteristics. rs10757278 and rs10811656 were significantly associated with ANRIL and circANRIL expressions in AT and PBMCs. The ROC‐curve analysis suggested that circANRIL has high diagnostic accuracy (AUC: 0.9808, cut‐off: 0.33, sensitivity: 1.0, specificity: 0.88). circANRIL has high diagnostic accuracy (AUC: 0.9808, cut‐off: 0.33, sensitivity: 1.0, specificity: 0.88). We report the first data demonstrating the presence of ANRIL and its transcript variants expressions in the AT and PBMCs of CAD patients. circANRIL having a synergetic effect with ANRIL plays a protective role in CAD pathogenesis. Therefore, altered circANRIL expression may become a potential diagnostic transcriptional biomarker for early CAD diagnosis.

Publisher

Wiley

Subject

Cell Biology,Molecular Medicine

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