A Novel Pathway of Insulin Sensitivity in Chromogranin A Null Mice

Gayen, Jiaur R.; Saberi, Maziyar; Schenk, Simon; Biswas, Nilima; Vaingankar, Sucheta M.; Cheung, Wai W.; Najjar, Sonia M.; O’Connor, Daniel T.; Bandyopadhyay, Gautam; Mahata, Sushil K.

doi:10.1074/jbc.m109.020636

Cited by 89 publications

(74 citation statements)

References 59 publications

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“…Consistent with an enhanced metabolic burden of ATP-dependent vesicular transport in Chga -KO mice, we found evidence for profound alteration in subcellular morphology of organelles involved in energy metabolism, including mitochondria, ER and GC. The ultrastructural findings correlate well with the pathophysiological findings reported earlier in Chga -KO mice (Bandyopadhyay et al 2015; Gayen et al 2009a, b; Mahapatra et al 2005). We also observed greatly enhanced glucose uptake and utilization in Chga -KO mice, consistent with increased metabolic burden on the chromaffin cell in the absence of CgA expression in the adrenal medulla.…”

Section: Discussionsupporting

confidence: 90%

“…One of the main functions of insulin is to stimulate glycogenesis and inhibit glycogenolysis. We have previously reported Chga -KO mice as being hypertensive, hyperadrenergic and sensitive to insulin (Bandyopadhyay et al 2015; Gayen et al 2009a, b; Mahapatra et al 2005). Therefore, increased glycogen granules in the adrenal medulla of Chga -KO mice may be a reflection of heightened insulin sensitivity in Chga -KO mice (Bandyopadhyay et al 2015; Gayen et al 2009b).…”

Section: Discussionmentioning

confidence: 99%

“…The extracellular function of CgA includes the generation of bioactive peptides, such as the insulin-regulatory hormone pancreastatin (Bandyopadhyay et al 2015; Gayen et al 2009b; Sanchez-Margalet et al 2010; Tatemoto et al 1986), the vasodilating and cardioprotective vasostatin (Aardal et al 1993; Tota et al 2008), the anti-adrenergic (Mahata et al 2003; Mahata, et al 2010; Mahata et al 1997), anti-hypertensive (Mahapatra et al 2005), anti-obesity (Bandyopadhyay et al 2012), proangiogenic (Theurl et al 2010) and cardioprotective catestatin (Angelone et al 2008; Mahata et al 2010) and the pro-adrenergic serpinin (Tota et al 2012). The intracellular function of CgA includes the initiation and regulation of DCV biogenesis and sequestration of hormones in neuroendocrine cells (Elias et al 2012; Iacangelo and Eiden 1995; Kim et al 2001; Taupenot et al 2002).…”

Section: Introductionmentioning

confidence: 99%

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Impact of Chromogranin A deficiency on catecholamine storage, catecholamine granule morphology and chromaffin cell energy metabolism in vivo

et al. 2015

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Chromogranin A (CgA) is a prohormone and granulogenic factor in neuroendocrine tissues with a regulated secretory pathway. The impact of CgA depletion on secretory granule formation has been previously demonstrated in cell culture. However, studies linking the structural effects of CgA deficiency with secretory performance and cell metabolism in the adrenomedullary chromaffin cells in vivo have not previously been reported. Adrenomedullary content of the secreted adrenal catecholamines norepinephrine (NE) and epinephrine (EPI) was decreased 30–40 % in Chga-KO mice. Quantification of NE and EPI-storing dense core (DC) vesicles (DCV) revealed decreased DCV numbers in chromaffin cells in Chga-KO mice. For both cell types, the DCV diameter in Chga-KO mice was less (100–200 nm) than in WT mice (200–350 nm). The volume density of the vesicle and vesicle number was also lower in Chga-KO mice. Chga-KO mice showed an ~47 % increase in DCV/DC ratio, implying vesicle swelling due to increased osmotically active free catecholamines. Upon challenge with 2 U/kg insulin, there was a diminution in adrenomedullary EPI, no change in NE and a very large increase in the EPI and NE precursor dopamine (DA), consistent with increased catecholamine biosynthesis during prolonged secretion. We found dilated mitochondrial cristae, endoplasmic reticulum and Golgi complex, as well as increased synaptic mitochondria, synaptic vesicles and glycogen granules in Chga-KO mice compared to WT mice, suggesting that decreased granulogenesis and catecholamine storage in CgA-deficient mouse adrenal medulla is compensated by increased VMAT-dependent catecholamine update into storage vesicles, at the expense of enhanced energy expenditure by the chromaffin cell.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Impact of Chromogranin A deficiency on catecholamine storage, catecholamine granule morphology and chromaffin cell energy metabolism in vivo

et al. 2015

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“…Gayen et al [52] observed an inverse relationship between pancreastatin and insulin. This CgA-derived peptide might antagonize the effect of insulin via the Akt/FOXO-1 and, administration of insulin could result in low plasma levels of pancreastatin in mice (the basal pancreastatin level dropped significantly following insulin injection).…”

Section: Discussionmentioning

confidence: 99%

Chromogranin A is a reliable serum diagnostic biomarker for pancreatic neuroendocrine tumors but not for insulinomas

et al. 2014

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BackgroundPancreatic neuroendocrine tumors (PNETs) are a group of rare tumors. Chromogranin A (CgA) was considered as the most practical and useful serum tumor marker in PNET patients. But peripheral blood levels of CgA are not routinely tested in Chinese patients with PNETs. This study was to assess the diagnostic value of CgA in Chinese patients with PNETs especially in patients with insulinomas.MethodsEighty-nine patients with PNETs including 57 insulinomas and 32 non-insulinoma PNETs as well as 86 healthy participants were enrolled in this study between September 2003 and June 2013. Serum levels of CgA were measured by ELISA method. Expression of CgA protein was detected in 26 PNET tissues including 14 insulinomas by immunohistochemical staining.ResultsSerum levels of CgA in 89 PNET patients were significantly higher than that in healthy controls (P = 7.2 × 10−9). Serum levels of CgA in 57 patients with insulinomas (median 64.8 ng/ml, range 25–164) were slightly higher than the levels in healthy controls (median 53.4 ng/ml, range 39–94) but much lower than the levels in 32 patients with non-insulinoma PNETs (median 193 ng/ml, range 27–9021), P = 0.001. The serum CgA levels were reduced in 16 of 17 patients with insulinomas after tumor resection. ROC curve showed that CgA values at 60 ng/ml distinguished patients with insulinomas from healthy controls but its sensitivity and specificity were 66.7% and 73.3%, respectively. In contrast, CgA values at 74 ng/ml distinguished patients with non-insulinoma PNETs from healthy controls, and the sensitivity and specificity were 65.6% and 91.9%, respectively. Except for two insulinomas with negative staining of CgA, 12 insulinoma tissues showed positive staining of CgA.ConclusionCgA is a reliable serum diagnostic biomarker for PNETs but not for insulinomas.

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“…It should be pointed out that Chga -KO mice are unique showing increased insulin sensitivity in the face of persistent hypertension (Mahapatra et al . 2005, Gayen et al . 2009, Biswas et al .…”

Section: Discussionmentioning

confidence: 99%

Muscle injury, impaired muscle function and insulin resistance in Chromogranin A-knockout mice

Tang

Pasqua

Biswas

et al. 2017

Journal of Endocrinology

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Chromogranin A (CgA) is widely expressed in endocrine and neuroendocrine tissues as well as in the central nervous system. We observed CgA expression (mRNA and protein) in the gastrocnemius (GAS) muscle and found that performance of CgA-deficient Chga-KO mice in treadmill exercise was impaired. Supplementation with CgA in Chga-KO mice restored exercise ability suggesting a novel role for endogenous CgA in skeletal muscle function. Chga-KO mice display (i) lack of exercise-induced stimulation of pAKT, pTBC1D1 and phospho-p38 kinase signaling, (ii) loss of GAS muscle mass, (iii) extensive formation of tubular aggregates (TA), (iv) disorganized cristae architecture in mitochondria, (v) increased expression of the inflammatory cytokines Tnfα, Il6 and Ifnγ, and fibrosis. The impaired maximum running speed and endurance in the treadmill exercise in Chga-KO mice correlated with decreased glucose uptake and glycolysis, defects in glucose oxidation and decreased mitochondrial cytochrome C oxidase activity. The lack of adaptation to endurance training correlated with the lack of stimulation of p38MAPK that is known to mediate the response to tissue damage. As CgA sorts proteins to the regulated secretory pathway, we speculate that lack of CgA could cause misfolding of membrane proteins inducing aggregation of sarcoplasmic reticulum (SR) membranes and formation of tubular aggregates that is observed in Chga-KO mice. In conclusion, CgA deficiency renders the muscle energy deficient, impairs performance in treadmill exercise and prevents regeneration after exercise-induced tissue damage.

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A Novel Pathway of Insulin Sensitivity in Chromogranin A Null Mice

Cited by 89 publications

References 59 publications

Impact of Chromogranin A deficiency on catecholamine storage, catecholamine granule morphology and chromaffin cell energy metabolism in vivo

Impact of Chromogranin A deficiency on catecholamine storage, catecholamine granule morphology and chromaffin cell energy metabolism in vivo

Chromogranin A is a reliable serum diagnostic biomarker for pancreatic neuroendocrine tumors but not for insulinomas

Muscle injury, impaired muscle function and insulin resistance in Chromogranin A-knockout mice

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