Abstract
The islets of Langerhans are well embedded within the exocrine pancreas (the latter comprised of ducts and acini), but the nature of interactions between these pancreatic compartments and their role in determining normal islet function and survival are poorly understood. However, these interactions appear to be critical, as when pancreatic exocrine disease occurs, islet function and insulin secretion frequently decline to the point that diabetes ensues, termed pancreatogenic diabetes. The most common forms of pancreatogenic diabetes involve sustained exocrine disease leading to ductal obstruction, acinar inflammation, and fibro-fatty replacement of the exocrine pancreas that predates the development of dysfunction of the endocrine pancreas, as seen in chronic pancreatitis-associated diabetes and cystic fibrosis-related diabetes and, more rarely, MODY type 8. Intriguingly, a form of tumour-induced diabetes has been described that is associated with pancreatic ductal adenocarcinoma. Here, we review the similarities and differences among these forms of pancreatogenic diabetes, with the goal of highlighting the importance of exocrine/ductal homeostasis for the maintenance of pancreatic islet function and survival and to highlight the need for a better understanding of the mechanisms underlying these diverse conditions.
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Overview
Under normal conditions, the exocrine (acinar and ductal) and endocrine pancreas co-exist in harmony (Fig. 1a,c). The organisation of these pancreatic compartments is the topic of some excellent reviews [1, 2] and is not covered here. The nature of the interactions between exocrine and endocrine pancreas and the role thereof in homeostatic pancreatic function remain incompletely understood. Surgical resection of up to 50% of the pancreas does not necessarily lead to diabetes [3], suggesting there is considerable functional reserve.
Insufficient insulin secretion is the unifying defect in all forms of diabetes, such as autoimmune destruction of islet beta cells in type 1 diabetes or intrinsic and acquired beta cell dysfunction in type 2 diabetes. Beta cell dysfunction/deficiency can also occur secondary to exocrine pancreatic disease, leading to pancreatogenic diabetes, also known as type 3c diabetes [4,5,6]. Of note, average pancreatic volume is decreased in people with type 1 or type 2 diabetes compared with that in non-diabetic control individuals [7, 8], supporting a bi-directional interaction between the endocrine and exocrine pancreas; however, discussion of this is beyond the scope of this article. Here we review several forms of pancreatogenic diabetes, highlighting the importance of the exocrine pancreas for the maintenance of pancreatic islet beta cell function and mass. Furthermore, we explore the similarities and differences in the aetiology of these diseases, with the goal of improving our understanding of interactions between pancreatic acini/ducts and islets in health and disease.
Chronic pancreatitis-associated diabetes
Diabetes develops in 26–80% of patients with chronic pancreatitis, with a higher prevalence seen with alcohol-related disease, early development of pancreatic calcifications, and longer disease duration; the majority develop diabetes by the fifth decade of life [9,10,11]. Compared with chronic pancreatitis, a single episode of acute pancreatitis confers a lower risk of diabetes [12]; this occurs predominantly in patients exhibiting marked tissue destruction.
Chronic pancreatitis generally follows a period of recurrent episodes of acute pancreatitis that may not always be appreciated clinically. These episodes of acute acinar injury and ductal plugging by concretions eventually result in ongoing pancreatic inflammation resulting in acinar destruction and fibrosis (Fig. 1b,d). While chronic alcohol use is the most common underlying aetiology, pancreatic injury also occurs in disorders that affect pancreatic duct flow (duct scars, pancreas divisum and groove pancreatitis), tropical calcific pancreatitis endemic to regions of Asia and Africa, hereditary pancreatitis (i.e. PRSS1, SPINK1, CFTR and CTRC mutations [OMIM no. 167800; www.omim.org]) and idiopathic causes (reviewed in [13]). Most often, more than one genetic and/or environmental factor contribute to the development of pancreatitis [13]. Despite the varied underlying causes, as recurrent acute becomes chronic pancreatitis, dysfunction of the pancreatic duct leads to ongoing destruction and dysfunction of the exocrine pancreas.
Patients with chronic pancreatitis-associated diabetes may have a known history of pancreatitis and exocrine insufficiency resulting in steatorrhoea. In addition, patients without a prior diagnosis of pancreatitis may present with abdominal pain and/or symptoms of maldigestion or may only present with glucose intolerance/diabetes. While weight gain typically accompanies the onset of type 2 diabetes, weight loss can occur in those with severe hyperglycaemia. Despite this, reduced weight occurring at the time of diabetes diagnosis should prompt careful clinical evaluation for the presence of underlying pancreatic disease. Diagnostic criteria for chronic pancreatitis-associated diabetes include the presence of pancreatic exocrine insufficiency, pathological pancreatic imaging and absence of type 1 diabetes-associated autoantibodies [14]. Pancreatic enzyme replacement in pancreatogenic diabetes is important to address maldigestion and malabsorption (particularly of fat and fat-soluble vitamins such as vitamin D) and control symptoms of steatorrhoea, and to improve incretin hormone secretion and, consequently, insulin release, which ultimately improves glucose tolerance [15].
Cystic fibrosis-related diabetes
Diabetes affects 20% of adolescents and ~ 50% of adults with cystic fibrosis [16]. Cystic fibrosis occurs due to biallelic loss-of-function mutations in the cystic fibrosis transmembrane conductance regulator (CFTR). This disrupts anion transport across epithelial cells, predominantly in the pancreas, lung and gut, and results in severe, multiorgan disease that leads to premature death, usually due to lung disease [17]. One of the earliest manifestations of cystic fibrosis is the dilation of pancreatic ducts and ductal obstruction due to plugging with viscous secretions [18]. This ductal pathology leads to fibro-fatty replacement of acinar tissue (Fig. 1b,e) and pancreatic insufficiency in ~85% of individuals [19]. While CFTR mutations resulting in complete or near-complete loss of CFTR function lead to exocrine pancreas destruction very early in life, less severe CFTR mutations may be associated with pancreatitis later in life, or spare the pancreas even when sinopulmonary disease is present [20]. Clinically evident pancreatitis is uncommon in individuals with pancreatic-insufficient cystic fibrosis. As described above for chronic pancreatitis with pancreatic exocrine insufficiency, pancreatic enzyme replacement improves incretin secretion and thereby insulin release that is beneficial for glucose tolerance [21].
Of particular concern, cystic fibrosis-related diabetes is associated with decreased lung function, increased pulmonary exacerbations, increased catabolism, lower BMI and an approximately four-fold increase in mortality risk [22] relative to individuals with cystic fibrosis without diabetes. Moreover, the presence of abnormal glucose tolerance is also associated with a significant decline in lung function [23], worse survival and higher lung transplant rates [24], illustrating that even mild abnormalities in glucose metabolism have adverse effects on cystic fibrosis outcomes. Although the risk of diabetes in individuals with cystic fibrosis increases with CFTR mutation severity, the increase in mortality risk induced by diabetes is independent of CFTR mutation severity; even among those with severe mutations, the presence of diabetes significantly increases mortality risk [22].
Rarer forms of pancreatogenic diabetes
Several rare pancreatic diseases provide additional evidence that healthy exocrine tissue supports the maintenance of islet function and glucose homeostasis.
Autoimmune pancreatitis is often accompanied by diabetes [25]. Type 1 autoimmune pancreatitis is associated with antibodies against lactoferrin, carbonic anhydrase II or α-2A-amylase and a lymphoplasmacytic sclerosing pancreatitis histopathology (reviewed in [26]). Type 2 autoimmune pancreatitis has negative serology and shows idiopathic duct-centric pancreatitis with granulocytic epithelial lesions [27]. In autoimmune pancreatitis, although islet-directed antibodies are not present [26], pancreatic histopathology shows inflammatory cells in contact with islets and loss of beta cells. Importantly, glucocorticoids not only alleviate pancreatitis in autoimmune pancreatitis, but also improve insulin secretion and help resolve diabetes [28].
MODY type 8 (MODY8, OMIM no. 609812) is caused by mutations in carboxyl-ester lipase (CEL) [29]. CEL is released from acinar cells, and is the only pancreatic bile-activated lipase present in ductal secretions. Despite a lack of clinically detectable pancreatitis, individuals with MODY8 develop slowly progressive pancreatic insufficiency, pancreatic cysts, fibro-fatty replacement of acinar tissue and insulin deficiency [30]. Mechanistic understanding of this insulin deficiency has been hampered by the fact that pancreas-specific Cel−/− mice do not recapitulate the exocrine disease or diabetes seen in humans [31], a shortcoming also seen in mouse models of other pancreatic diseases (e.g. Cftr−/− mice).
Two additional forms of MODY highlight the shared developmental aspects of the endocrine and exocrine pancreas and are important to consider, especially in young people presenting with deficient exocrine and endocrine pancreas function. MODY4 (OMIM no. 606392) is caused by heterozygous mutations in pancreatic and duodenal homeobox 1 (PDX1). Homozygous mutations cause pancreatic agenesis, including absence of both exocrine and endocrine components [32]. Similarly, MODY5 (OMIM no. 137920), caused by heterozygous mutations in HNF1 homeobox B (HNF1B), is associated with mild pancreatic exocrine deficiency and frequent aplasia of the body and tail of the pancreas [33].
Pancreatic ductal adenocarcinoma-associated diabetes
Pancreatic ductal adenocarcinoma is the most common and lethal form of pancreatic cancer and shares a bi-directional association with diabetes. Obesity and type 2 diabetes are risk factors for pancreatic ductal adenocarcinoma, with insulin resistance and the resultant hyperinsulinaemia promoting tumour survival/proliferation, via insulin and IGF-1 receptor signalling [34]. Intriguingly, there is also evidence that pancreatic ductal adenocarcinoma may lead to the development of diabetes via a paraneoplastic effect of the developing tumour on islet beta cell function. In support of this, recent evidence shows bi-directional blood flow in the pancreas [35]. This provides a mechanism for delivery of high levels of insulin (and other beta cell products, such as cholecystokinin [36]) from the beta cell to acinar/ductal/tumour cells, along with the supply of tumour-derived factors to the beta cell.
Diabetes is present more often at diagnosis of pancreatic ductal adenocarcinoma than other cancers [37]. Among individuals with pancreatic ductal adenocarcinoma and diabetes, the majority were diagnosed with diabetes within 24 months prior to cancer diagnosis and often presented with weight loss at the time of diabetes diagnosis [6]. Thus, as discussed above, when patients present at diabetes diagnosis with disproportionate weight loss (relative to diabetes severity), pancreatic imaging not only allows for assessment of pancreatogenic diabetes but may also allow for early detection of pancreatic cancer.
Islet failure in pancreatogenic forms of diabetes
The aetiology of islet beta cell failure in pancreatogenic diabetes remains poorly understood. Most studies relate to chronic pancreatitis and especially cystic fibrosis, with potential novel mechanisms emerging from several recent studies, as described in the next section.
In both chronic pancreatitis and cystic fibrosis, fibrotic and/or fatty replacement of acinar tissue disrupts normal pancreas microarchitecture, resulting in progressive exocrine dysfunction. This results in nutrient maldigestion/malabsorption and contributes to the development of impaired glucose intolerance and, eventually, diabetes. Measures of pancreatic exocrine and endocrine function (Table 1) are significantly correlated in chronic pancreatitis [38, 39] and insulin secretion is significantly worse in individuals with cystic fibrosis with pancreatic insufficiency [40], providing additional evidence for the interrelated pathology of the islet and exocrine pancreas.
Impaired insulin secretion is the key defect underlying the development of hyperglycaemia in both chronic pancreatitis and cystic fibrosis. In chronic pancreatitis, impaired insulin secretion is evident even without the presence of diabetes [41]. In cystic fibrosis, impaired insulin secretion is present in most individuals [40, 42,43,44], including young children [40, 43]. In cystic fibrosis, beta cell function is progressively impaired across the glucose tolerance spectrum, beginning with an elevated 1 h OGTT and ultimately resulting in cystic fibrosis-related diabetes [44]. Despite substantial destruction of exocrine pancreas in both chronic pancreatitis and cystic fibrosis, the loss of islet beta cells is generally modest, even in individuals with long-standing pancreatic disease (reviewed in [45, 46]). Thus, while a reduction in beta cell mass may contribute to the loss of insulin release in chronic pancreatitis and cystic fibrosis, it is unlikely to be the sole cause. In addition, there may be dynamic developmental changes in islet mass in cystic fibrosis pancreatic disease. Histopathological investigation of the pancreas of young children with cystic fibrosis resulted in the hypothesis that new islet formation was occurring [47]. Similarly, young ferrets with cystic fibrosis undergo loss of detectable pancreatic endocrine cells during active exocrine tissue destruction, followed by a transient expansion of beta cells [48]. The source of these new islets remains uncertain.
In chronic pancreatitis, the mechanism(s) underlying insulin secretory dysfunction is very poorly understood although, as mentioned above, decreased beta cell number and function both contribute (reviewed in [45]). In cystic fibrosis, more is known, although whether insulin secretory defects occur as a result of the effect of mutated CFTR within the beta cell itself is controversial. Several studies have reported beta cell CFTR activity and an effect on insulin release from human and rodent islets [49,50,51], and CFTR corrector therapy has been shown to rescue defective insulin release in a mouse model of cystic fibrosis [50]. Some of these data must be interpreted with caution due to reliance on pharmacological inhibitors (CFTR(inh)-172 or GlyH-101) and/or CFTR antibodies that lack specificity ([52, 53] and reviewed in [46]). In contrast, numerous recent studies show that beta cell CFTR expression is exceedingly low/difficult to detect. These studies utilised in situ hybridisation [53, 54], immunohistochemistry [52, 54, 55] and/or analysis of datasets comprising single cell or bulk islet RNA-seq data [46, 52]. In addition, a recent study did not find a CFTR current in human beta cells [52] and beta cell deletion of Cftr did not affect insulin release in a mouse model [52]. Taken together, these data suggest that effects of CFTR within beta cells is unlikely to be the sole cause of insulin secretory dysfunction. However, these findings could also be explained by beta cell subpopulation heterogeneity (i.e. CFTR being expressed in a small subset of beta cells, which could have large functional effects).
Non-beta cell intrinsic mechanisms are also likely to contribute to dysfunctional insulin secretion in pancreatogenic diabetes. Recent studies in cystic fibrosis models have suggested the presence of paracrine crosstalk between pancreatic ductal epithelial cells and beta cells [46, 53, 55], suggesting that alterations in secreted factors from diseased ducts could be a common mechanism underlying impaired insulin release in this and other pancreatogenic forms of diabetes, although the mechanisms underlying this crosstalk are entirely unknown. In addition, as pancreatic exocrine insufficiency predates the development of diabetes in both chronic pancreatitis and cystic fibrosis, the associated impairment in incretin secretion may chronically affect islet beta cell mass and function through disruption of the enteroinsular axis.
Another possibility involves the loss of exocrine-derived paracrine factors that support islet maintenance and function. One potential example is regenerating family member 3α (REG3A), also known as islet neogenesis associated protein (INGAP), an exocrine-derived paracrine factor whose expression is upregulated in perturbed acinar cells and which positively impacts islet mass [56]. However, it could be the case that in pancreatic disease associated with loss of exocrine tissue, REG3A is no longer synthesised, resulting in deficiency of this islet-protective factor.
Islet dysfunction in chronic pancreatitis and cystic fibrosis is not limited to the beta cell. While basal and stimulated glucagon release is increased with acute pancreatitis [57], glucagon release is reduced in chronic pancreatitis, especially in the presence of diabetes [57, 58]. In cystic fibrosis, glucagon release in response to arginine or following hypoglycaemia is reduced [40, 42, 59]. This defective glucagon release does not occur secondary to a loss of alpha cells. Rather, in chronic pancreatitis, alpha cell number is increased relative to islet area [60], while in cystic fibrosis an absolute increase in alpha cell number is evident (reviewed in [46]). In addition, impaired suppression of glucagon release may occur due to insulin deficiency in both chronic pancreatitis [61] and cystic fibrosis [62]. In line with this latter point, use of the CFTR modulator ivacaftor in individuals with cystic fibrosis improved insulin secretion, which was associated with more appropriate glucagon suppression [63].
CFTR corrector/potentiator therapies dramatically improve cystic fibrosis lung disease. Very limited data are available regarding the impact of these drugs on glucose tolerance/islet function, but positive effects are suggested [63, 64]. Additional studies are needed to uncover the mechanism of action and optimal age for treatment initiation for this new class of drugs.
In chronic pancreatitis, exocrine pancreas destruction and associated loss of nerve bundles is associated with the loss of islet vascularity and innervation [60]. Consequently, a profound loss of pancreatic polypeptide (PP) secretion, which depends on vagal afferents, is observed [65, 66]. This could also be related to destruction of the ventral pancreas, where the majority of PP-rich islets are located. In chronic pancreatitis, reduced PP secretion is seen early in the course of the disease [66], with PP responses being essentially absent when glucose tolerance is also impaired [65]. Similarly, in pancreatic-insufficient cystic fibrosis, a marked defect in PP cell function is also observed, regardless of glucose tolerance status [42, 67]. The underlying mechanism is less well understood in cystic fibrosis, but animal studies suggest loss of pancreatic/islet innervation [68]. Thus, decreased PP secretion appears to be a reliable early marker for endocrine dysfunction in these two pancreatic diseases [4, 42, 67].
Potential mechanisms underlying beta cell failure
Recent publications have begun to elucidate mechanisms that may underlie beta cell (and alpha cell failure) in chronic pancreatitis and cystic fibrosis. A small pancreatic histopathology study of chronic pancreatitis cases demonstrated increased inflammatory infiltration near islets (much greater than that seen in type 2 diabetes), along with a significant increase in ‘dedifferentiated’ cells, specifically chromogranin A-positive, hormone-negative cells [69]. For cystic fibrosis, recent studies demonstrated that islet inflammation, namely, increased IL-1β immunoreactivity (likely within beta cells) [70] and/or increased T cell presence (including cytotoxic CD8+ T cells) [52, 71], are early and common features of islet pathology in individuals with cystic fibrosis both with and without diabetes. The underlying aetiology of this islet cytokine expression/lymphocyte infiltration is currently unknown. Amyloid deposition within islets, a pathological hallmark of type 2 diabetes known to be associated with leucocyte activation, is present but does not correlate with islet IL-1β immunoreactivity in cystic fibrosis [70] and has not been widely studied in chronic pancreatitis. Islet macrophages are well known for production of proinflammatory cytokines [72], but are also required for islet regeneration [73, 74] and have been shown to stimulate islet angiogenesis and protect against islet cell loss during exocrine pancreas disease in mice [75]. Of note, macrophages are almost entirely absent from islets in adults with cystic fibrosis [70, 71]. Together, these new data suggest that strategies aimed at reducing islet cytokine expression, limiting T cell infiltration and/or replenishing islet macrophages could be effective in restoring beta cell function in pancreatogenic diabetes, although additional studies are needed to better define the underlying aetiology of islet inflammation in these disease states.
The mechanisms underlying pancreatic ductal adenocarcinoma-associated diabetes remain unknown. The observation that new-onset diabetes in pancreatic ductal adenocarcinoma can resolve following tumour resection when sufficient residual pancreatic tissue remains supports a paraneoplastic mechanism [6]. However, this effect is invariably reported following pancreaticoduodenectomy and so is confounded by independent effects of Roux-en-Y reconstruction with gastrojejunostomy on glucose homeostasis as seen with bariatric surgery [76]. In vitro evidence suggests that tumours may release peptide- and cytokine-containing exosomes that may result in impaired islet beta cell function [77], in an analogous fashion to the duct–islet paracrine interaction proposed for cystic fibrosis above, while histological examination of paraneoplastic pancreatic tissue resected from individuals with pancreatic ductal adenocarcinoma without diabetes demonstrates islet infiltration with an inflammatory cell infiltrate and reduced markers of differentiated beta cell identity [78], reminiscent of data from both chronic pancreatitis and cystic fibrosis. Increases in fasting glucose are detectable 3 years prior to diagnosis of pancreatic ductal adenocarcinoma [79], and whether this deterioration in glucose homeostasis may be combined with other potential cancer biomarkers to inform early diagnosis is under active clinical investigation [80].
Summary and implications
Diabetes occurs secondary to a collection of seemingly disparate diseases that affect pancreatic ducts and/or acini. Amazingly, islets generally survive within this diseased organ, albeit in a dysfunctional state. However, as pancreatic exocrine disease progresses, islet function becomes impaired, leading to pancreatogenic diabetes. This implies a functional connection between the two pancreatic compartments. Further study is needed to better understand the mechanistic links between these two entities, with the goal of developing better preventative/curative strategies for those affected by the diseases reviewed herein.
Abbreviations
- CEL:
-
Carboxyl-ester lipase
- CFTR:
-
Cystic fibrosis transmembrane conductance regulator
- PP:
-
Pancreatic polypeptide
- REG3A:
-
Regenerating family member 3α
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Acknowledgements
Due to the limit on the number of references allowed, many excellent papers in this field could not be included. However, these additional publications were important in shaping this review; we apologise to those whose work was not cited directly. We thank C. Liu of the Department of Surgery, University of Pennsylvania Perelman School of Medicine, for supplying images from H&E-stained control and chronic pancreatitis pancreas specimens.
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The authors declare that there are no relationships or activities that might bias, or be perceived to bias, their work.
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All authors developed the outline of the article, reviewed and discussed the relevant literature, and were responsible for drafting the article and revising it critically for important intellectual content. All authors approved the version to be published.
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Work in the authors’ laboratories is supported by National Institutes of Health grants R01 DK97830 (MRR), R01 DK115791 (AWN), and R01 DK088082 (RLH). AWN is also supported by the Fraternal Order of Eagles Diabetes Research Center. RLH is also supported by the Department of Veterans Affairs, VA Puget Sound Health Care System (Seattle, WA, USA) and Seattle Institute for Biomedical and Clinical Research (Seattle, WA, USA).
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Rickels, M.R., Norris, A.W. & Hull, R.L. A tale of two pancreases: exocrine pathology and endocrine dysfunction. Diabetologia 63, 2030–2039 (2020). https://doi.org/10.1007/s00125-020-05210-8
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DOI: https://doi.org/10.1007/s00125-020-05210-8