Widespread and Stable Pancreatic Gene Transfer by Adeno-Associated Virus Vectors via Different Routes

Wang, Zhong; Zhu, Tong; Rehman, Khaja K.; Bertera, Suzanne; Zhang, Jian; Chen, Chunlian; Papworth, Glenn D.; Watkins, Simon C.; Trucco, Massimo; Robbins, Paul D.; Li, Juan; Xiao, Xiao

doi:10.2337/diabetes.55.04.06.db05-0927

Cited by 117 publications

(168 citation statements)

References 43 publications

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“…28 Expression can be further restricted within the islet by coupling transgene expression to activation of the MIP, 28 thereby providing an opportunity to specifically target the expression of therapeutic genes within beta-cells. AAV vectors represent an innovative gene therapy tool, having reduced immunogenicity compared with that of adenoviruses, 36 while being capable of directing long-term expression of transgenes both in humans and in mice.…”

Section: Discussionmentioning

confidence: 99%

“…33 The observation that the majority of GLP-1-positive beta-cells are located in the periphery of the islet, is consistent with the intraperitoneal delivery route and has been observed previously for DsAAV8-mediated transgene expression in islets. 28 To investigate the mechanisms contributing to improved glucose tolerance in mice receiving DsAAV8-MIP-GLP-1, a pancreatic morphometric analysis was performed. Animals expressing beta-cell GLP-1 had similar total insulin-positive area (0.0033 ± 0.0004 in GLP-1-treated animals versus 0.0026 ± 0.0007 in control animals), but trended toward an increase in the total number of insulin-positive areas per mm 2 of pancreatic tissue (15.9 ± 1.5 versus 11.4 ± 1.9 in control animals; P ¼ 0.097) due to significant increase in the number of small insulin-positive clusters (Figures 5a and b).…”

Section: In Vivo Expression Of Glp-1 Increases Beta-cell Proliferatiomentioning

confidence: 99%

“…Several different AAV serotypes have now been identified, 26 with serotype-8 exhibiting an ability to efficiently transduce pancreatic tissue. 27,28 Wang et al 28 have recently shown that in vivo administration of AAV8 vectors containing enhanced greenfluorescent protein (eGFP) driven by the mouse insulin-II promoter (MIP) results in efficient transduction of pancreatic beta-cells. Furthermore, it has been shown that therapeutic genes can be delivered to beta-cells through intraperitoneal injection of AAV8.…”

Section: Introductionmentioning

confidence: 99%

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DsAAV8-mediated expression of glucagon-like peptide-1 in pancreatic beta-cells ameliorates streptozotocin-induced diabetes

et al. 2009

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Glucagon-like peptide-1 (GLP-1) is an incretin hormone that performs a wide array of well-characterized antidiabetic actions, including stimulation of glucose-dependent insulin secretion, upregulation of insulin gene expression and improvements in beta-cell survival. GLP-1-receptor agonists have been developed for treatment of diabetes; however, the short biological half-lives of these peptide-based therapeutics requires that frequent injections be administered to maintain sufficient circulating levels. Thus, novel methods of delivering GLP-1 remain an important avenue of active research. It has recently been demonstrated that self-complimentary, double-stranded, adeno-associated virus serotype-8 (DsAAV8) can efficiently transduce pancreatic beta-cells in vivo, resulting in long-term transgene expression. In this study, we engineered a DsAAV8 vector containing a GLP-1 transgene driven by the mouse insulin-II promoter (MIP). Biological activity of the GLP-1 produced from this transgene was assessed using a luciferase-based bioassay. DsAAV8-MIP-GLP-1 was delivered via intraperitoneal injection and beta-cell damage induced by multiple low dose streptozotocin (STZ) administration. Glucose tolerance was assessed following intraperitoneal glucose injections and beta-cell proliferation measured by PCNA expression. Expression of GLP-1 in Min6 beta-cells resulted in glucose-dependent secretion of biologically active GLP-1. Intraperitoneal delivery of DsAAV8-MIP-GLP-1 to mice led to localized GLP-1 expression in beta-cells and protection against development of diabetes induced by multiple low-dose STZ administration. This protection was associated with significant increase in beta-cell proliferation. Results from this study indicate that expression and secretion of GLP-1 from beta-cells in vivo via DsAAV8 represents a novel therapeutic strategy for treatment of diabetes.

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Section: Discussionmentioning

confidence: 99%

Section: In Vivo Expression Of Glp-1 Increases Beta-cell Proliferatiomentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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DsAAV8-mediated expression of glucagon-like peptide-1 in pancreatic beta-cells ameliorates streptozotocin-induced diabetes

et al. 2009

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“…Fibroblast growth factor receptor, αvβ5 integrin, and hepatocyte growth factor receptor have been reported to work as co-factors [36–38]. Among the many types of AAV, single-stranded AAV, such as serotypes 8 (AAV-8) and 9 (AAV-9), and double-stranded AAV have been reported to have effective transduction of transgenes into the pancreas [39–44]. …”

Section: Gene Therapy Delivery Systems For the Treatment Of Diabetes mentioning

confidence: 99%

“…In terms of administration routes of viral vectors for the delivery of transgenes to the pancreas in vivo , although intravenous administration has been used most often, intrapancreatic ductal injections might be more efficient because transgenes with viral vectors can more easily escape from phagocytes in the liver via this administration route [51]. The transduction efficiency of transgenes with viral vectors in the pancreas via intravenous administration was reported to improve under conditions of reduced blood flow to the liver, such as with a liver bypass or transient blockade of liver circulation [44,52]. However, other studies have reported that intravenous administration of AAV-8 or AAV-9 substantially delivered transgenes to the pancreas [40,53].…”

Section: Gene Therapy Delivery Systems For the Treatment Of Diabetes mentioning

confidence: 99%

Transgene and islet cell delivery systems using nano-sized carriers for the treatment of diabetes mellitus

Ookawara

Ishibashi

et al. 2017

Nano Reviews & Experiments

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Gene therapy that targets the pancreas and intestines with delivery systems using nano-sized carriers such as viral and non-viral vectors could improve the control of blood glucose levels, resulting in an improved prognosis for patients with diabetes mellitus. Allogenic pancreatic islet cell transplantations using such delivery systems have been developed as therapeutic options for diabetes mellitus. This review focuses on transgenes and islet cell delivery systems using nano-sized carriers for the treatment of diabetes mellitus.

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Gene Therapy for Diabetes

Haurigot

Jiménez

Bosch

2016

Textbook of Diabetes

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Widespread and Stable Pancreatic Gene Transfer by Adeno-Associated Virus Vectors via Different Routes

Abstract: Diabetes is a disease of epidemic proportions and is

Cited by 117 publications

References 43 publications

DsAAV8-mediated expression of glucagon-like peptide-1 in pancreatic beta-cells ameliorates streptozotocin-induced diabetes

DsAAV8-mediated expression of glucagon-like peptide-1 in pancreatic beta-cells ameliorates streptozotocin-induced diabetes

Transgene and islet cell delivery systems using nano-sized carriers for the treatment of diabetes mellitus

Gene Therapy for Diabetes

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