Angiotensin II type 1 receptor inhibition markedly improves the blood perfusion, oxygen tension and first phase of glucose-stimulated insulin secretion in revascularised syngeneic mouse islet grafts

Kampf, Caroline; Lau, Thomas K.H.; Olsson, Richard F.; Leung, Po Sing; Carlsson, Per‐Ola

doi:10.1007/s00125-005-1761-z

Cited by 53 publications

(46 citation statements)

References 42 publications

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“…The chosen model to evaluate graft function also enabled us to separately evaluate the effects of improved vascular engraftment on the insulin release kinetics from transplanted islets. It is noteworthy that the peak of the first phase of glucose-stimulated insulin secretion was substantially higher in the better revascularized islet grafts, which is similar to what we have previously observed when improving blood perfusion, but not revascularization, by angiotensin II receptor inhibition (47). However, in contrast to when only the blood perfusion was improved, we observed in the present study also an augmented second phase of glucose-stimulated insulin secretion.…”

Section: Discussionsupporting

confidence: 90%

Improved Vascular Engraftment and Graft Function After Inhibition of the Angiostatic Factor Thrombospondin-1 in Mouse Pancreatic Islets

et al. 2008

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OBJECTIVE-Insufficient development of a new intra-islet capillary network after transplantation may be one contributing factor to the failure of islet grafts in clinical transplantation. The present study tested the hypothesis that the angiostatic factor thrombospondin-1 (TSP-1), which is normally present in islets, restricts intra-islet vascular expansion posttransplantation. RESEARCH DESIGN AND METHODS-Pancreatic islets of TSP-1-deficient (TSP-1Ϫ/Ϫ ) mice or wild-type islets transfected with siRNA for TSP-1 were transplanted beneath the renal capsule of syngeneic or immunocompromised recipient mice. RESULTS-Both genetically TSP-1Ϫ/Ϫ islets and TSP-1 siRNAtransfected islet cells demonstrated an increased vascular density when compared with control islets 1 month after transplantation. This was also reflected in a markedly increased blood perfusion and oxygenation of the grafts. The functional importance of the improved vascular engraftment was analyzed by comparing glucose-stimulated insulin release from islet cells transfected with either TSP-1 siRNA or scramble siRNA before implantation. These experiments showed that the increased revascularization of grafts composed of TSP-1 siRNA-transfected islet cells correlated to increments in both their first and second phase of glucose-stimulated insulin secretion.CONCLUSIONS-Our findings demonstrate that inhibition of TSP-1 in islets intended for transplantation may be a feasible strategy to improve islet graft revascularization and function.

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Section: Discussionsupporting

confidence: 90%

Improved Vascular Engraftment and Graft Function After Inhibition of the Angiostatic Factor Thrombospondin-1 in Mouse Pancreatic Islets

et al. 2008

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“…Moreover, in humans, weight gain and obesity per se seem to activate the RAS (18). Note that the upregulation of AT1R expression in db/db islets from type 2 diabetes observed in the present study is similar to that observed following transplantation of normal islets (19). In that case, not only a disturbance in (pro)insulin biosynthesis regulation but also a defect in islet blood flow were attributed to impaired glucose-induced insulin release.…”

Section: Discussionsupporting

confidence: 84%

Angiotensin II Type 1 Receptor Blockade Improves β-Cell Function and Glucose Tolerance in a Mouse Model of Type 2 Diabetes

et al. 2006

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We identified an angiotensin-generating system in pancreatic islets and found that exogenously administered angiotensin II, after binding to its receptors (angiotensin II type 1 receptor [AT1R]), inhibits insulin release in a manner associated with decreased islet blood flow and (pro)insulin biosynthesis. The present study tested the hypothesis that there is a change in AT1R expression in the pancreatic islets of the obesity-induced type 2 diabetes model, the db/db mouse, which enables endogenous levels of angiotensin II to impair islet function. Islets from 10-week-old db/db and control mice were isolated and investigated. In addition, the AT1R antagonist losartan was administered orally to 4-week-old db/db mice for an 8-week period. We found that AT1R mRNA was upregulated markedly in db/db islets and double immunolabeling confirmed that the AT1R was localized to ␤-cells. Losartan selectively improved glucose-induced insulin release and (pro)insulin biosynthesis in db/db islets. Oral losartan treatment delayed the onset of diabetes, and reduced hyperglycemia and glucose intolerance in db/db mice, but did not affect the insulin sensitivity of peripheral tissues. The present findings indicate that AT1R antagonism improves ␤-cell function and glucose tolerance in young type 2 diabetic mice. Whether islet AT1R activation plays a role in the pathogenesis of human type 2 diabetes remains to be determined. Diabetes 55:367-374, 2006 T he prevalence of obesity is rising in North America, where 61% of adults are now overweight or obese, a trend mirrored worldwide (1). The accompanying epidemic of type 2 diabetes and its cardiovascular complications are evident in the Western world (2,3) and also in Asia (4). Therapies aimed at increasing insulin sensitivity offer only partial solutions, since ␤-cell dysfunction and ␤-cell loss may also contribute to disease progression. In this regard, the mechanisms that underlie islet failure have yet to be elucidated. A recently identified local renin-angiotensin system (RAS) may play an important role in pancreatic physiology and pathophysiology (5,6). While the acinar RAS regulates exocrine function (7) and pancreatitis (8), a local islet RAS also exists. The RAS constituents angiotensinogen, ACE, and angiotensin II types 1 and 2 receptors (AT1R and AT2R) have been demonstrated to be present in pancreatic islets, with the AT1R localized specifically to the ␤-cells (9). This local pancreatic islet RAS has the potential to regulate insulin release, in that AT1R activation may inhibit insulin release in response to glucose loading. This action is mediated, at least in part, through alterations in islet (pro)insulin synthesis and islet blood flow engendered by angiotensin II biosynthesis (9,10).The clinically observed benefits of RAS blockade in persons at risk for developing type 2 diabetes, namely a reduced incidence of developing diabetes (11,12), have been hard to explain. A better understanding of the protective effects of RAS inhibition on type 2 diabetes is of profound importance...

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“…This may reflect a less than optimal vascular organisation in transplanted islets relative to native islets. A vascular dysfunction with altered blood flow regulation has also been reported in transplanted islets [48].…”

Section: Discussionmentioning

confidence: 92%

“…It should be noted that islet endothelial cells can directly stimulate beta cell insulin secretion through paracrine effects [40]. Additionally, an acute increase in graft oxygen tension, through stimulation of blood perfusion, of islet renal subcapsular grafts has been shown to improve the first phase of glucose-stimulated insulin release [48].…”

Section: Discussionmentioning

confidence: 99%

Improved vascular engraftment and function of autotransplanted pancreatic islets as a result of partial pancreatectomy in the mouse and rat

2007

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Aims/hypothesis The few patients subjected to autotransplantation of pancreatic islets after pancreatectomy usually become normoglycaemic after using islets from the resected organ only, whereas allogeneic recipients usually require at least two grafts to retain normoglycaemia. Previous experimental studies have demonstrated that islets transplanted to non-pancreatectomised recipients acquire a markedly decreased blood vessel density, which leads to a hypoxic microenvironment. The aim of the present study was to test the hypothesis that autotransplanted islets have better vascular engraftment and function as a result of the pancreatic surgery involved. Materials and methods In the present study, athymic mice and inbred rats were subjected to a 60% pancreatectomy and transplanted with human or rat islets, respectively, 4 days later. Control animals underwent sham surgery. Blood flow, oxygen tension, vascular density and endocrine volume in the islet grafts were measured 1 month after transplantation. Separate grafts were used for perfusion experiments and for assessment of beta cell proliferation and endocrine cellular apoptosis at different time periods after transplantation.Results Islet grafts in partially pancreatectomised recipients had an increased blood flow, oxygen tension, blood vessel density and endocrine mass 1 month post-transplantation compared with control animals. They also exhibited increased insulin release in perfusion experiments performed 1 month post-transplantation, and decreased cellular apoptosis early after transplantation. Conclusions/interpretation The present study shows that the pancreatectomy procedure itself has beneficial effects on the engraftment of transplanted human and rat islets. Our results provide an additional explanation, besides diminished immunological responses, of the much better outcome of islet autotransplantations compared with allogeneic transplantations in the clinic.

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Angiotensin II type 1 receptor inhibition markedly improves the blood perfusion, oxygen tension and first phase of glucose-stimulated insulin secretion in revascularised syngeneic mouse islet grafts

Cited by 53 publications

References 42 publications

Improved Vascular Engraftment and Graft Function After Inhibition of the Angiostatic Factor Thrombospondin-1 in Mouse Pancreatic Islets

Improved Vascular Engraftment and Graft Function After Inhibition of the Angiostatic Factor Thrombospondin-1 in Mouse Pancreatic Islets

Angiotensin II Type 1 Receptor Blockade Improves β-Cell Function and Glucose Tolerance in a Mouse Model of Type 2 Diabetes

Improved vascular engraftment and function of autotransplanted pancreatic islets as a result of partial pancreatectomy in the mouse and rat

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