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Hypertension from targeted ablation of chromogranin A can be rescued by the human ortholog

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TLDR
Loss of the physiological "brake" catestatin in Chga mice coupled with dysregulation of transmitter storage and release may act in concert to alter autonomic control of the circulation in vivo, eventuating in hypertension.
Abstract
The secretory prohormone chromogranin A (CHGA) is overexpressed in essential hypertension, a complex trait with genetic predisposition, while its catecholamine release–inhibitory fragment catestatin is diminished, and low catestatin predicts augmented adrenergic pressor responses. These findings from studies on humans suggest a mechanism whereby diminished catestatin might increase the risk for hypertension. We generated Chga–/– and humanized mice through transgenic insertion of a human CHGA haplotype in order to probe CHGA and catestatin in vivo. Chga–/– mice displayed extreme phenotypic changes, including: (a) decreased chromaffin granule size and number; (b) elevated BP; (c) loss of diurnal BP variation; (d) increased left ventricular mass and cavity dimensions; (e) decreased adrenal catecholamine, neuropeptide Y (Npy), and ATP contents; (f) increased catecholamine/ATP ratio in the chromaffin granule; and (g) increased plasma catecholamine and Npy levels. Rescue of elevated BP to normalcy was achieved by either exogenous catestatin replacement or humanization of Chga–/– mice. Loss of the physiological “brake” catestatin in Chga–/– mice coupled with dysregulation of transmitter storage and release may act in concert to alter autonomic control of the circulation in vivo, eventuating in hypertension.

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Chromogranin A is an autoantigen in type 1 diabetes

TL;DR: The peptide WE14 from chromogranin A (ChgA) is identified as the antigen for highly diabetogenic CD4+ T cell clones in the nonobese diabetic (NOD) mouse model of type 1 diabetes and supports the idea that autoreactive T cells respond to unusually presented self peptides.
Journal ArticleDOI

The Extended Granin Family: Structure, Function, and Biomedical Implications

TL;DR: The structure and function of granins and granin-derived peptides and expansive new genetic evidence are reviewed, including recent single-nucleotide polymorphism mapping, genomic sequence comparisons, and analysis of transgenic and knockout mice, which together support an important and evolutionarily conserved role for these proteins in large dense-core vesicle biogenesis and regulated secretion.
Journal Article

Continuous Relation Between Left Ventricular Mass and Cardiovascular Risk in Essential Hypertension

TL;DR: The detection of left ventricular (LV) hypertrophy on echocardiography is a powerful risk indicator in essential hypertension, but the prognostic impact of LV mass values within the “normal” range and the shape of the relation between LV mass and prognosis remain unclear.
Journal ArticleDOI

The endocrine role for chromogranin A: a prohormone for peptides with regulatory properties.

TL;DR: Endocrine regulations are indicated from in vivo studies, consistent with the postulated prohormone function of CgA for peptides with regulatory properties, implicating C gA peptides in regulation of calcium and glucose metabolism, cardiovascular functions, gastrointestinal motility and nociception, tissue repair, inflammatory responses and in the first phase of microbial invasions.
Journal ArticleDOI

CAPS-1 and CAPS-2 are essential synaptic vesicle priming proteins.

TL;DR: These findings demonstrate that CAPS proteins generate and maintain a highly fusion competent synaptic vesicle pool that supports phasic Ca(2+) triggered release of transmitters.
References
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Journal ArticleDOI

Pathways of protein secretion in eukaryotes.

TL;DR: Transfection of DNA encoding foreign secretory proteins into regulated secretory cells has provided insight into the specificity of sorting into secretory vesicles.
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The Chromogranin–Secretogranin Family

TL;DR: The members of the chromogranin–secretogran in family of peptide hormones, biogenic amines, and neurotransmitters are enclosed within vesicles in the neuroendocrine system and a variety of neurons.
Journal ArticleDOI

Pancreastatin, a novel pancreatic peptide that inhibits insulin secretion

TL;DR: The 49-residue peptide strongly inhibits glucose-induced insulin release from the isolated perfused pancreas and was therefore named pancreastatin and may be important in the regulation of insulin secretion and in the pathogenesis and treatment of diabetes mellitus.
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Regression of electrocardiographic left ventricular hypertrophy during antihypertensive treatment and the prediction of major cardiovascular events.

TL;DR: Less-severe electrocardiographic LVH by Cornell product and SokolowLyon voltage criteria during antihypertensive therapy is associated with lower likelihoods of CV morbidity and mortality, independent of blood pressure lowering and treatment modality in persons with essential hypertension.
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