| Literature DB >> 27324226 |
Malapaka Kiranmayi1, Venkat R Chirasani1, Prasanna K R Allu1, Lakshmi Subramanian1, Elizabeth E Martelli1, Bhavani S Sahu1, Durairajpandian Vishnuprabu1, Rathnakumar Kumaragurubaran1, Saurabh Sharma1, Dhanasekaran Bodhini1, Madhulika Dixit1, Arasambattu K Munirajan1, Madhu Khullar1, Venkatesan Radha1, Viswanathan Mohan1, Ajit S Mullasari1, Sathyamangla V Naga Prasad1, Sanjib Senapati1, Nitish R Mahapatra2.
Abstract
Catestatin (CST), an endogenous antihypertensive/antiadrenergic peptide, is a novel regulator of cardiovascular physiology. Here, we report case-control studies in 2 geographically/ethnically distinct Indian populations (n≈4000) that showed association of the naturally-occurring human CST-Gly364Ser variant with increased risk for hypertension (age-adjusted odds ratios: 1.483; P=0.009 and 2.951; P=0.005). Consistently, 364Ser allele carriers displayed elevated systolic (up to ≈8 mm Hg; P=0.004) and diastolic (up to ≈6 mm Hg; P=0.001) blood pressure. The variant allele was also found to be in linkage disequilibrium with other functional single-nucleotide polymorphisms in the CHGA promoter and nearby coding region. Functional characterization of the Gly364Ser variant was performed using cellular/molecular biological experiments (viz peptide-receptor binding assays, nitric oxide [NO], phosphorylated extracellular regulated kinase, and phosphorylated endothelial NO synthase estimations) and computational approaches (molecular dynamics simulations for structural analysis of wild-type [CST-WT] and variant [CST-364Ser] peptides and docking of peptide/ligand with β-adrenergic receptors [ADRB1/2]). CST-WT and CST-364Ser peptides differed profoundly in their secondary structures and showed differential interactions with ADRB2; although CST-WT displaced the ligand bound to ADRB2, CST-364Ser failed to do the same. Furthermore, CST-WT significantly inhibited ADRB2-stimulated extracellular regulated kinase activation, suggesting an antagonistic role towards ADRB2 unlike CST-364Ser. Consequently, CST-WT was more potent in NO production in human umbilical vein endothelial cells as compared with CST-364Ser. This NO-producing ability of CST-WT was abrogated by ADRB2 antagonist ICI 118551. In conclusion, CST-364Ser allele enhanced the risk for hypertension in human populations, possibly via diminished endothelial NO production because of altered interactions of CST-364Ser peptide with ADRB2 as compared with CST-WT.Entities:
Keywords: chromogranin A; genetic association study; genetic variation; hypertension; nitric oxide
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Year: 2016 PMID: 27324226 PMCID: PMC4945419 DOI: 10.1161/HYPERTENSIONAHA.116.06568
Source DB: PubMed Journal: Hypertension ISSN: 0194-911X Impact factor: 10.190