Your search keyword '"Bhavani S. Sahu"' showing total 6 results

1. A haplotype variant of the human chromogranin A gene (CHGA) promoter increases CHGA expression and the risk for cardiometabolic disorders

Author

Malapaka Kiranmayi, Lakshmi Subramanian, Prasanna K.R. Allu, Abrar A. Khan, Ajit S. Mullasari, Saurabh Sharma, Nitish R. Mahapatra, Bhavani S. Sahu, and Madhu Khullar

Subjects

0301 basic medicine, Regulation of gene expression, Genetics, Linkage disequilibrium, Haplotype, Chromogranin A, Single-nucleotide polymorphism, Cell Biology, Biology, Biochemistry, 03 medical and health sciences, 030104 developmental biology, biology.protein, Allele, Molecular Biology, Allele frequency, Transcription factor

Abstract

The acidic glycoprotein chromogranin A (CHGA) is co-stored/co-secreted with catecholamines and crucial for secretory vesicle biogenesis in neuronal/neuroendocrine cells. CHGA is dysregulated in several cardiovascular diseases, but the underlying mechanisms are not well established. Here, we sought to identify common polymorphisms in the CHGA promoter and to explore the mechanistic basis of their plausible contribution to regulating CHGA protein levels in circulation. Resequencing of the CHGA promoter in an Indian population (n = 769) yielded nine single-nucleotide polymorphisms (SNPs): G-1106A, A-1018T, T-1014C, T-988G, G-513A, G-462A, T-415C, C-89A, and C-57T. Linkage disequilibrium (LD) analysis indicated strong LD among SNPs at the -1014, -988, -462, and -89 bp positions and between the -1018 and -57 bp positions. Haplotype analysis predicted five major promoter haplotypes that displayed differential promoter activities in neuronal cells; specifically, haplotype 2 (containing variant T alleles at -1018 and -57 bp) exhibited the highest promoter activity. Systematic computational and experimental analyses revealed that transcription factor c-Rel has a role in activating the CHGA promoter haplotype 2 under basal and pathophysiological conditions (viz. inflammation and hypoxia). Consistent with the higher in vitro CHGA promoter activity of haplotype 2, individuals carrying this haplotype had higher plasma CHGA levels, plasma glucose levels, diastolic blood pressure, and body mass index. In conclusion, these results suggest a functional role of the CHGA promoter haplotype 2 (occurring in a large proportion of the world population) in enhancing CHGA expression in haplotype 2 carriers who may be at higher risk for cardiovascular/metabolic disorders.

Published

2017

2. Coordinated Transcriptional Regulation of Hspa1a Gene by Multiple Transcription Factors: Crucial Roles for HSF-1, NF-Y, NF-κB, and CREB

Author

Nitish R. Mahapatra, Parshuram J. Sonawane, Bhavani S. Sahu, Vinayak Gupta, and Binu K. Sasi

Subjects

Chromatin Immunoprecipitation, Transcription, Genetic, Response element, Activating transcription factor, Electrophoretic Mobility Shift Assay, CREB, ATF/CREB, Heat Shock Transcription Factors, Sp3 transcription factor, Genes, Reporter, Structural Biology, HSP70 Heat-Shock Proteins, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Transcription factor, General transcription factor, biology, NF-kappa B, Computational Biology, Promoter, Molecular biology, cyclic AMP responsive element binding protein, forskolin, heat shock transcription factor 1, I kappa B, nuclear factor Y, cis acting element, immunoglobulin enhancer binding protein, small interfering RNA, tumor necrosis factor alpha, article, controlled study, down regulation, electrophoretic mobility, gene, gene activation, gene control, gene expression, genetic transcription, heart muscle ischemia, Hspa1a gene, human, human cell, myoblast, priority journal, protein motif, transactivation, transcription initiation, transcription regulation, animal cell, Article, base pairing, chromatin immunoprecipitation, embryo, gel mobility shift assay, gene expression regulation, gene interaction, hspa1a gene, in vitro study, in vivo study, mathematical analysis, mouse, nonhuman, promoter region, protein function, protein interaction, reporter gene, Artificial Gene Fusion, DNA-Binding Proteins, CCAAT-Binding Factor, Gene Expression Regulation, biology.protein, Transcription Factors

Abstract

Although the transcript level of inducible heat shock protein 70.3 (Hsp70.3, also known as Hspa1a) is altered in various disease states, its transcriptional regulation remains incompletely understood. Here, we systematically analyzed the Hspa1a promoter to identify major cis elements and transcription factors that may govern the constitutive/inducible gene expression. Computational analyses coupled with extensive in vitro (promoter-reporter activity and electrophoretic mobility shift assays) and in vivo (chromatin immunoprecipitation assays) revealed interaction of several transcription factors with Hspa1a promoter motifs: HSF-1 (heat shock factor 1) at - 114/- 97 bp and - 788/- 777 bp, NF-Y (nuclear transcription factor Y) at - 73/- 58 bp, NF-?B (nuclear factor kappa B) at - 133/- 124 bp, and CREB (cAMP response element binding protein) at - 483/- 476 bp. Consistently, siRNA (small interfering RNA)-mediated down-regulation of each of these transcription factors caused substantial reduction of endogenous Hspa1a expression. Heat-shock-induced activation of Hspa1a was coordinately regulated by HSF-1 and NF-Y/NF-?B. The Hspa1a expression was augmented by TNF-? (tumor necrosis factor-alpha) and forskolin in NF-?B and CREB-dependent manners, respectively. NF-?B and CREB also activated Hspa1a transcription in cardiac myoblasts upon exposure to ischemia-like conditions. Taken together, this study discovered previously unknown roles for NF-?B and CREB to regulate Hspa1a expression and a coordinated action by several transcription factors for Hspa1a transactivation under heat-shock/ischemia-like conditions and thereby provided new insights into the mechanism of Hspa1a regulation. � 2013 Elsevier Ltd.

Published

2014

3. Peptide/Receptor Co-evolution Explains the Lipolytic Function of the Neuropeptide TLQP-21

Author

Megin E. Nguyen, Mihaela Pavlicev, Leslie J. Baier, Scott M. O'Grady, Louis J. Muglia, Sushil K. Mahata, Alessandro Bartolomucci, John D. McCorvy, Ruijun Han, Yuk Y. Sham, Lauren J. Laskowski, Paolo Piaggi, Bhavani S. Sahu, Maria Razzoli, Cheryl Cero, and Pedro Rodriguez

Subjects

Male, 0301 basic medicine, Amino Acid Motifs, Peptide, Mice, Transient receptor potential channel, 0302 clinical medicine, Adipocytes, Receptor, innate immunity, Peptide sequence, lcsh:QH301-705.5, chemistry.chemical_classification, Chemistry, Drug discovery, VGF, lipolytic catecholamine resistance, Ligand (biochemistry), Receptors, Complement, Cell biology, granin peptides, Pharmacophore, Protein Binding, Agonist, Adult, transient receptor potential channel, medicine.drug_class, Adipose Tissue, White, Lipolysis, Neuropeptide, Models, Biological, Article, General Biochemistry, Genetics and Molecular Biology, drug discovery, Evolution, Molecular, 03 medical and health sciences, Adrenergic Agents, 3T3-L1 Cells, medicine, Animals, Humans, Computer Simulation, Obesity, Homology modeling, Binding site, G protein-coupled receptor, Neuropeptides, obesity, Peptide Fragments, Mice, Inbred C57BL, 030104 developmental biology, lcsh:Biology (General), Structural Homology, Protein, Calcium, Extracellular Space, 030217 neurology & neurosurgery

Abstract

SUMMARY Structural and functional diversity of peptides and GPCR result from long evolutionary processes. Even small changes in sequence can alter receptor activation, affecting therapeutic efficacy. We conducted a structure-function relationship study on the neuropeptide TLQP-21, a promising target for obesity, and its complement 3a receptor (C3aR1). After having characterized the TLQP-21/C3aR1 lipolytic mechanism, a homology modeling and molecular dynamics simulation identified the TLQP-21 binding motif and C3aR1 binding site for the human (h) and mouse (m) molecules. mTLQP-21 showed enhanced binding affinity and potency for hC3aR1 compared with hTLQP-21. Consistently, mTLQP-21, but not hTLQP-21, potentiates lipolysis in human adipocytes. These findings led us to uncover five mutations in the C3aR1 binding pocket of the rodent Murinae subfamily that are causal for enhanced calculated affinity and measured potency of TLQP-21. Identifying functionally relevant peptide/receptor co-evolution mechanisms can facilitate the development of innovative pharmacotherapies for obesity and other diseases implicating GPCRs., In Brief GPCRs and neuropeptide ligands are under intense evolutionary pressure and are major pharmacological targets. Sahu et al. identify a cluster of mutations within the C3aR1 receptor and the TLQP-21 peptide in the Murinae subfamily of rodents, resulting in enhanced binding affinity and potency, leading to potentiation of adrenergic-receptor-induced lipolysis., Graphical Abstract

Published

2019

4. Corrigendum to 'Coordinated Transcriptional Regulation of Hspa1a Gene by Multiple Transcription Factors: Crucial Roles for HSF-1, NF-Y, NF-κB, and CREB' [J. Mol. Biol. (2014) 426, 116–135]

Author

Nitish R. Mahapatra, Binu K. Sasi, Parshuram J. Sonawane, Vinayak Gupta, and Bhavani S. Sahu

Subjects

chemistry.chemical_compound, biology, Structural Biology, Chemistry, Mole, biology.protein, Transcriptional regulation, HSPA1A Gene, NF-κB, CREB, Molecular Biology, Transcription factor, Cell biology

Published

2019

5. Functional Genetic Variants of the Catecholamine-Release-Inhibitory Peptide Catestatin in an Indian Population

Author

Sanjib Senapati, Parshuram J. Sonawane, Samir K. Maji, Binu K. Sasi, Nitish R. Mahapatra, Bhavani S. Sahu, Giriraj Sahu, Pradeep K. Singh, Lakshmi Subramanian, Prasanna K.R. Allu, Ajit S. Mullasari, Jagan M. Obbineni, Amal Kanti Bera, and Balashankar Gomathi

Subjects

chemistry.chemical_classification, medicine.medical_specialty, Wild type, Chromogranin A, Peptide, Cell Biology, Biology, Biochemistry, Nicotinic acetylcholine receptor, Endocrinology, Nicotinic agonist, chemistry, Internal medicine, medicine, Catecholamine, biology.protein, Allele, Receptor, human activities, Molecular Biology, medicine.drug

Abstract

Catestatin (CST), a chromogranin A (CHGA)-derived peptide, is a potent inhibitor of catecholamine release from adrenal chromaffin cells and postganglionic sympathetic axons. We re-sequenced the CST region of CHGA in an Indian population (n = 1010) and detected two amino acid substitution variants: G364S and G367V. Synthesized CST variant peptides (viz. CST-Ser-364 and CST-Val-367) were significantly less potent than the wild type peptide (CST-WT) to inhibit nicotine-stimulated catecholamine secretion from PC12 cells. Consistently, the rank-order of blockade of nicotinic acetylcholine receptor (nAChR)-stimulated inward current and intracellular Ca2+ rise by these peptides in PC12 cells was: CST-WT > CST-Ser-364 > CST-Val-367. Structural analysis by CD spectroscopy coupled with molecular dynamics simulations revealed the following order of α-helical content: CST-WT > CST-Ser-364 > CST-Val-367; docking of CST peptides onto a major human nAChR subtype and molecular dynamics simulations also predicted the above rank order for their binding affinity with nAChR and the extent of occlusion of the receptor pore, providing a mechanistic basis for differential potencies. The G364S polymorphism was in strong linkage disequilibrium with several common CHGA genetic variations. Interestingly, the Ser-364 allele (detected in ∼15% subjects) was strongly associated with profound reduction (up to ∼2.1-fold) in plasma norepinephrine/epinephrine levels consistent with the diminished nAChR desensitization-blocking effect of CST-Ser-364 as compared with CST-WT. Additionally, the Ser-364 allele showed strong associations with elevated levels of plasma triglyceride and glucose levels. In conclusion, a common CHGA variant in an Indian population influences several biochemical parameters relevant to cardiovascular/metabolic disorders.

Published

2012

6. Molecular basis of altered expression of the HMG-CoA reductase gene in genetically hypertensive mice

Author

Bhavani S. Sahu, Nitish R. Mahapatra, Parshuram J. Sonawane, Govinda Lenka, and Binu K. Sasi

Subjects

7-Dehydrocholesterol reductase, biology, business.industry, HMG-CoA reductase, biology.protein, Medicine, Cardiology and Cardiovascular Medicine, business, Gene, Molecular biology

Published

2009