Functional Gly297Ser Variant of the Physiological Dysglycemic Peptide Pancreastatin Is a Novel Risk Factor for Cardiometabolic Disorders

Allu, P K R and Kiranmayi, M and Mukherjee, S D and Chirasani, V R and Garg, R and Vishnuprabu, D and Ravi, S and Subramanian, L and Sahu, B S and Iyer, D R and Maghajothi, S and Sharma, S and Ravi, M S and Khullar, M and Munirajan, A K and Gayen, J R and Senapati, S and Mullasari, A S and Mohan, V and Radha, V and Naga Prasad, S V and Mahapatra, N R (2021) Functional Gly297Ser Variant of the Physiological Dysglycemic Peptide Pancreastatin Is a Novel Risk Factor for Cardiometabolic Disorders. Diabetes, 71 (3). p. 538. ISSN 0012-1797

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Abstract

Pancreastatin (PST), a chromogranin A-derived potent physiological dysglycemic peptide, regulates glucose/insulin homeostasis. We have identified a nonsynonymous functional PST variant (p.Gly297Ser; rs9658664) that occurs in a large section of human populations. Association analysis of this single nucleotide polymorphism with cardiovascular/metabolic disease states in Indian populations (n = 4,300 subjects) displays elevated plasma glucose, glycosylated hemoglobin, diastolic blood pressure, and catecholamines in Gly/Ser subjects as compared with wild-type individuals (Gly/Gly). Consistently, the 297Ser allele confers an increased risk (∼1.3-1.6-fold) for type 2 diabetes/hypertension/coronary artery disease/metabolic syndrome. In corroboration, the variant peptide (PST-297S) displays gain-of-potency in several cellular events relevant for cardiometabolic disorders (e.g., increased expression of gluconeogenic genes, increased catecholamine secretion, and greater inhibition of insulin-stimulated glucose uptake) than the wild-type peptide. Computational docking analysis and molecular dynamics simulations show higher affinity binding of PST-297S peptide with glucose-regulated protein 78 (GRP78) and insulin receptor than the wild-type peptide, providing a mechanistic basis for the enhanced activity of the variant peptide. In vitro binding assays validate these in silico predictions of PST peptides binding to GRP78 and insulin receptor. In conclusion, the PST 297Ser allele influences cardiovascular/metabolic phenotypes and emerges as a novel risk factor for type 2 diabetes/ hypertension/coronary artery disease in human populations.

Item Type:Article
Official URL/DOI:http://dx.doi.org/10.2337/db21-0289
Uncontrolled Keywords:Cardiometabolic , Risk Factor
Subjects:Biochemistry,Cell and Molecular Signalling
Divisions:Department of Epidemiology
Department of Advanced Research Biochemistry
ID Code:1299
Deposited By:surendar radha
Deposited On:10 Mar 2022 10:23
Last Modified:10 Mar 2022 10:24

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