Intraislet SLIT–ROBO signaling is required for beta-cell survival and potentiates insulin secretion

Yang, Yu Hsuan Carol; Fox, Jocelyn E. Manning; Zhang, Kevin L.; MacDonald, Patrick E.; Johnson, James D.

doi:10.1073/pnas.1214312110

Cited by 57 publications

(62 citation statements)

References 56 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Besides functioning as axon guidance molecules, the Slit/Robo pathway proteins also regulate functions such as morphogenesis of tissue as well as performing many non-neuronal roles such as cell growth, migration and cell survival [92]. Slit/Robo is often downregulated in the advanced stage of most tumors [31,85,86].…”

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

“…Slit/Robo is often downregulated in the advanced stage of most tumors [31,85,86]. In vitro studies suggested that expression of Slit can be regulated by stress and optimum function can be achieved by modulating the endoplasmic reticulum (ER), Ca 2+ homeostasis and actin in β cells [92]. For example, cytokines, thapsigargin and palmitate suppress Slit2 expression and serum deprivation downregulates Slit3 [92].…”

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

“…In vitro studies suggested that expression of Slit can be regulated by stress and optimum function can be achieved by modulating the endoplasmic reticulum (ER), Ca 2+ homeostasis and actin in β cells [92]. For example, cytokines, thapsigargin and palmitate suppress Slit2 expression and serum deprivation downregulates Slit3 [92]. Cancer cells have the tendency to become aggressive and metastatic under extreme stress (low glucose, hypoxic condition) as compared with normoxic conditions [93].…”

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

See 2 more Smart Citations

Slit/Robo pathway: a promising therapeutic target for cancer

Gara

Kumari

Ganju

et al. 2015

Drug Discovery Today

View full text Add to dashboard Cite

Axon guidance molecules, slit glycoprotein (Slit) and Roundabout receptor (Robo), have implications in the regulation of physiological processes. Recent studies indicate that Slit and Robo also have important roles in tumorigenesis, cancer progression and metastasis. The Slit/Robo pathway can be considered a master regulator for multiple oncogenic signaling pathways. Herein, we provide a comprehensive review on the role of these molecules and their associated signaling pathways in cancer progression and metastasis. Overall, the current available data suggest that the Slit/Robo pathway could be a promising target for development of anticancer drugs.

show abstract

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

Section: Future Prospects For Slit/robo Pathway As a Drug Targetmentioning

confidence: 99%

See 1 more Smart Citation

Slit/Robo pathway: a promising therapeutic target for cancer

Gara

Kumari

Ganju

et al. 2015

Drug Discovery Today

View full text Add to dashboard Cite

show abstract

“…While depth and coverage remain technical hurdles, these approaches will soon shed much-needed light on the functional heterogeneity of human islet cell subtypes and states, as well as the variability observed in in vitro derived cultures. Although insulin is by far the major secreted product of primary beta cells, this cell type likely expresses hundreds of other secreted proteins [52], several of which have known physiological roles [52][53][54]. Future studies should also address the completeness of insulin processing, as it is possible that improperly processed and/or secreted insulin can provoke or accelerate beta cell directed autoimmunity [55].…”

Section: Remaining Obstacles-deep Phenotypingmentioning

confidence: 99%

The quest to make fully functional human pancreatic beta cells from embryonic stem cells: climbing a mountain in the clouds

Johnson

2016

Diabetologia

Self Cite

View full text Add to dashboard Cite

The production of fully functional insulin-secreting cells to treat diabetes is a major goal of regenerative medicine. In this article, I review progress towards this goal over the last 15 years from the perspective of a beta cell biologist. I describe the current state-of-the-art, and speculate on the general approaches that will be required to identify and achieve our ultimate goal of producing functional beta cells. The need for deeper phenotyping of heterogeneous cultures of stem cell derived islet-like cells in parallel with a better understanding of the heterogeneity of the target cell type(s) is emphasised. This deep phenotyping should include high-throughput single-cell analysis, as well as comprehensive 'omics technologies to provide unbiased characterisation of cell products and human beta cells. There are justified calls for more detailed and well-powered studies of primary human pancreatic beta cell physiology, and I propose online databases of standardised human beta cell responses to physiological stimuli, including both functional and metabolomic/proteomic/ transcriptomic profiles. With a concerted, community-wide effort, including both basic and applied scientists, beta cell replacement will become a clinical reality for patients with diabetes.Keywords Embryonic stem cells . Glucose-stimulated insulin release . Human pancreatic islet beta cells . Review Abbreviation PDX1 Pancreatic and duodenal homeobox 1The case for beta cell replacement in diabetes Diabetes mellitus was recognised early in the era of regenerative medicine research as an obvious indication for a stem cell based therapy. Type 1 diabetes results from the loss of more than 80% of an individual's pancreatic beta cells, while type 2 diabetes occurs when there is insufficient functional beta cell mass to meet the body's needs. The replacement of lost or dysfunctional beta cells in all patients that require it is one of the most important, but elusive, goals of diabetes research. The rationale for beta cell replacement is clear, given the success with which islet cell transplants reduce dangerous hypoglycaemic events and slow the progression of complications [1][2][3]. Pancreatic beta cells have evolved as master regulators of metabolic homeostasis, sensing glucose and other nutrients and releasing appropriate insulin to induce their storage. We understand the basics of beta cell biology, especially the ionic mechanisms underlying insulin release in response to large and abrupt glucose stimuli, which include a rapid rise in cytosolic Ca 2+ subsequent to the metabolismdriven closure of K ATP channels, as well as a plethora of coupling factors [4]. However, we do not understand precisely how human beta cells respond to physiological stimuli and make fate decisions.There are a number of possible ways to replace beta cells in patients with diabetes. Beta cell proliferation could theoretically be induced from the few remaining beta cells in people Electronic supplementary material The online version of this article

show abstract

“…Measurements of intracellular calcium concentration for individual human islets from the different treatment groups were carried out by previously described methods (25,26) at glucose concentrations of 2.5 and 25 mmol/L. Glucose-stimulated increase in intracellular calcium concentration was expressed as area under the curve (AUC).…”

Section: Calcium Imagingmentioning

confidence: 99%

Antiaging Glycopeptide Protects Human Islets Against Tacrolimus-Related Injury and Facilitates Engraftment in Mice

et al. 2015

Self Cite

View full text Add to dashboard Cite

Clinical islet transplantation has become an established treatment modality for selected patients with type 1 diabetes. However, a large proportion of transplanted islets is lost through multiple factors, including immunosuppressant-related toxicity, often requiring more than one donor to achieve insulin independence. On the basis of the cytoprotective capabilities of antifreeze proteins (AFPs), we hypothesized that supplementation of islets with synthetic AFP analog antiaging glycopeptide (AAGP) would enhance posttransplant engraftment and function and protect against tacrolimus (Tac) toxicity. In vitro and in vivo islet Tac exposure elicited significant but reversible reduction in insulin secretion in both mouse and human islets. Supplementation with AAGP resulted in improvement of islet survival (Tac + vs. Tac+AAGP, 31.5% vs. 67.6%, P < 0.01) coupled with better insulin secretion (area under the curve: Tac + vs. Tac+AAGP, 7.3 vs. 129.2 mmol/L/60 min, P < 0.001). The addition of AAGP reduced oxidative stress, enhanced insulin exocytosis, improved apoptosis, and improved engraftment in mice by decreasing expression of interleukin (IL)-1b, IL-6, keratinocyte chemokine, and tumor necrosis factor-a. Finally, transplant efficacy was superior in the Tac+AAGP group and was similar to islets not exposed to Tac, despite receiving continuous treatment for a limited time. Thus, supplementation with AAGP during culture improves islet potency and attenuates long-term Tac-induced graft dysfunction.

show abstract

Intraislet SLIT–ROBO signaling is required for beta-cell survival and potentiates insulin secretion

Cited by 57 publications

References 56 publications

Slit/Robo pathway: a promising therapeutic target for cancer

Slit/Robo pathway: a promising therapeutic target for cancer

The quest to make fully functional human pancreatic beta cells from embryonic stem cells: climbing a mountain in the clouds

Antiaging Glycopeptide Protects Human Islets Against Tacrolimus-Related Injury and Facilitates Engraftment in Mice

Contact Info

Product

Resources

About