Ex vivo human pancreatic slice preparations offer a valuable model for studying pancreatic exocrine biology

Liang, Tao; Dolai, Subhankar; Xie, Lin; Winter, Erin; Orabi, Abrahim I.; Karimian, Negar; Cosen-Binker, Laura Iris; Huang, Ya-Chi; Thorn, Peter; Cattral, Mark S.; Gaisano, Herbert Y.

doi:10.1074/jbc.m117.777433

Cited by 48 publications

(54 citation statements)

References 39 publications

(73 reference statements)

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“…; Liang et al . ). A limited amount of work on acinar cell Ca 2+ signalling in pancreatic segments has confirmed that the basic character of such signals, as established in isolated cell studies, is also valid in the intact pancreas (Ashby et al .…”

Section: Introductionmentioning

confidence: 97%

“…Physiological, short-lasting and repetitive local Ca 2+ signals control acinar fluid and enzyme secretion (Petersen, 1992;, whereas sustained global elevations of the cytosolic Ca 2+ concentration ([Ca 2+ ] i ), elicited by pathological agents, play a key role in the development of the acinar cell damage and death leading to acute pancreatitis (AP) (Gerasimenko et al 2014). Most of the work on PAC Ca 2+ signalling has been carried out on isolated mouse cells, but the key results have been confirmed in studies on isolated human PACs (Murphy et al 2008;Liang et al 2017). A limited amount of work on acinar cell Ca 2+ signalling in pancreatic segments has confirmed that the basic character of such signals, as established in isolated cell studies, is also valid in the intact pancreas (Ashby et al 2003).…”

Section: Introductionmentioning

confidence: 99%

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Calcium signalling in the acinar environment of the exocrine pancreas: physiology and pathophysiology

Gryshchenko

Gerasimenko

Peng

et al. 2018

The Journal of Physiology

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Key points Ca2+ signalling in different cell types in exocrine pancreatic lobules was monitored simultaneously and signalling responses to various stimuli were directly compared.Ca2+ signals evoked by K+‐induced depolarization were recorded from pancreatic nerve cells. Nerve cell stimulation evoked Ca2+ signals in acinar but not in stellate cells.Stellate cells are not electrically excitable as they, like acinar cells, did not generate Ca2+ signals in response to membrane depolarization.The responsiveness of the stellate cells to bradykinin was markedly reduced in experimental alcohol‐related acute pancreatitis, but they became sensitive to stimulation with trypsin.Our results provide fresh evidence for an important role of stellate cells in acute pancreatitis. They seem to be a critical element in a vicious circle promoting necrotic acinar cell death. Initial trypsin release from a few dying acinar cells generates Ca2+ signals in the stellate cells, which then in turn damage more acinar cells causing further trypsin liberation. AbstractPhysiological Ca2+ signals in pancreatic acinar cells control fluid and enzyme secretion, whereas excessive Ca2+ signals induced by pathological agents induce destructive processes leading to acute pancreatitis. Ca2+ signals in the peri‐acinar stellate cells may also play a role in the development of acute pancreatitis. In this study, we explored Ca2+ signalling in the different cell types in the acinar environment of the pancreatic tissue. We have, for the first time, recorded depolarization‐evoked Ca2+ signals in pancreatic nerves and shown that whereas acinar cells receive a functional cholinergic innervation, there is no evidence for functional innervation of the stellate cells. The stellate, like the acinar, cells are not electrically excitable as they do not generate Ca2+ signals in response to membrane depolarization. The principal agent evoking Ca2+ signals in the stellate cells is bradykinin, but in experimental alcohol‐related acute pancreatitis, these cells become much less responsive to bradykinin and then acquire sensitivity to trypsin. Our new findings have implications for our understanding of the development of acute pancreatitis and we propose a scheme in which Ca2+ signals in stellate cells provide an amplification loop promoting acinar cell death. Initial release of the proteases kallikrein and trypsin from dying acinar cells can, via bradykinin generation and protease‐activated receptors, induce Ca2+ signals in stellate cells which can then, possibly via nitric oxide generation, damage more acinar cells and thereby cause additional release of proteases, generating a vicious circle.

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Section: Introductionmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

Calcium signalling in the acinar environment of the exocrine pancreas: physiology and pathophysiology

Gryshchenko

Gerasimenko

Peng

et al. 2018

The Journal of Physiology

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“…Evidence supports a direct effect of CCK on CCK receptor signaling in rodent acinar cells. Although CCK receptor expression in human acinar cells is lower than observed in rodents, recent work supports a similar direct effect by physiologic and supraphysiologic concentrations of CCK on intracellular signaling and zymogen release in primary human acinar cells (Liang et al, 2017;Murphy et al, 2008). Alternatively, CCK has been shown to stimulate insulin secretion from beta cells (Lo et al, 2011), which in turn could modulate early tumorigenesis.…”

Section: Endocrine-exocrine Cck Signaling In Obesitymentioning

confidence: 92%

Endocrine-exocrine signaling drives obesity-associated pancreatic ductal adenocarcinoma

Chung¹,

Singh

Lawres

et al. 2019

Preprint

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SUMMARYObesity is a major modifiable risk factor for pancreatic ductal adenocarcinoma (PDAC), yet how and when obesity contributes to PDAC progression is not well understood. Leveraging an autochthonous mouse model, we demonstrate a causal and reversible role for obesity in early PDAC progression, showing that obesity markedly enhances tumorigenesis, while genetic or dietary induction of weight loss intercepts cancer development. Bulk and single cell molecular analyses of human and murine samples define microenvironmental consequences of obesity that promote tumor development rather than new driver gene mutations. We observe increased inflammation and fibrosis and also provide evidence for significant pancreatic islet cell adaptation in obesity-associated tumors. Specifically, we identify aberrant islet beta cell expression of the peptide hormone cholecystokinin (CCK) in tumors as an adaptive response to obesity. Furthermore, beta cell CCK expression promotes oncogenic Kras-driven pancreatic ductal tumorigenesis. Our studies argue that PDAC progression is driven by local obesity-associated changes in the tumor microenvironment – rather than systemic effects – and implicate endocrine-exocrine signaling beyond insulin in PDAC development. Furthermore, our demonstration that these obesity-associated adaptations are reversible supports the use of anti-obesity strategies to intercept PDAC early during progression.

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“…Responses to well characterized stimuli for the secretion of hormones [e.g. insulin (glucose, KCl) and glucagon (KCl, arginine)] and enzymes [amylase, lipase and trypsinogen (CCK-8, carbachol)] [117] can be assessed in real time under steady state conditions, and the experimental system can likely be modulated with the addition of inflammatory cytokines or other soluble factors to mimic or mollify the T1D microenvironment. The potential drawbacks of this platform include the confounding influence of pancreatic enzymes, as well as lack of innervation and blood flow limiting tissue thickness to limit hypoxia-induced stress.…”

Section: Ex Vivo Platforms For Studying Islet-immune Interactions In mentioning

confidence: 99%

Islet–immune interactions in type 1 diabetes: the nexus of beta cell destruction

Peters

Posgai

2019

Clinical and Experimental Immunology

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Recent studies in Type 1 Diabetes (T1D) support an emerging model of disease pathogenesis that involves intrinsic β-cell fragility combined with defects in both innate and adaptive immune cell regulation. This combination of defects induces systematic changes leading to organ-level atrophy and dysfunction of both the endocrine and exocrine portions of the pancreas, ultimately culminating in insulin deficiency and β-cell destruction. In this review, we discuss the animal model data and human tissue studies that have informed our current understanding of the cross-talk that occurs between β-cells, the resident stroma, and immune cells that potentiate T1D. Specifically, we will review the cellular and molecular signatures emerging from studies on tissues derived from organ procurement programs, focusing on in situ defects occurring within the T1D islet microenvironment, many of which are not yet detectable by standard peripheral blood biomarkers. In addition to improved access to organ donor tissues, various methodological advances, including immune receptor repertoire sequencing and single-cell molecular profiling, are poised to improve our understanding of antigen-specific autoimmunity during disease development. Collectively, the knowledge gains from these studies at the islet-immune interface are enhancing our understanding of T1D heterogeneity, likely to be an essential component for instructing future efforts to develop targeted interventions to restore immune tolerance and preserve β-cell mass and function.

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Ex vivo human pancreatic slice preparations offer a valuable model for studying pancreatic exocrine biology

Cited by 48 publications

References 39 publications

Calcium signalling in the acinar environment of the exocrine pancreas: physiology and pathophysiology

Calcium signalling in the acinar environment of the exocrine pancreas: physiology and pathophysiology

Endocrine-exocrine signaling drives obesity-associated pancreatic ductal adenocarcinoma

Islet–immune interactions in type 1 diabetes: the nexus of beta cell destruction

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