Human beta cell mass and function in diabetes: Recent advances in knowledge and technologies to understand disease pathogenesis

Chen, Chunguang; Cohrs, Christian M.; Stertmann, Julia; Bozsak, Robert; Speier, Stephan

doi:10.1016/j.molmet.2017.06.019

Cited by 387 publications

(339 citation statements)

References 231 publications

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“…Islet size in db/db mice was consistently approximately 3.5 fold larger compared to lean mice (Supplemental Figure 1D-E), corroborating an earlier observation (24). These results are similar to the metabolic adaptations seen in pre-diabetic humans (1,25,26) making the db/db mouse an ideal model for studying mechanisms of islet compensation in early T2D.…”

Section: Higher Numbers Of Macrophages Within Islets Of Db/db Micesupporting

confidence: 85%

Islet macrophages drive islet vascular remodeling and compensatory hyperinsulinemia in the early stages of diabetes

Chittezhath

Gunaseelan

Zheng

et al. 2019

Preprint

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β-cells respond to peripheral insulin resistance by increasing circulating insulin in early type-2 diabetes (T2D). Islet remodeling supports this compensation but the drivers of this process remain poorly understood. Infiltrating macrophages have been implicated in late stage T2D but relatively little is known on islet resident macrophages, especially in early T2D. We hypothesize that islet resident macrophages contribute to islet vascular remodeling and hyperinsulinemia, the failure of which results in a rapid progression to T2D. Using genetic and dietinduced models of compensatory hyperinsulinemia we show that its depletion significantly compromises islet remodeling in terms of size, vascular density and insulin secretion capacity. Depletion of islet macrophages reduces VEGF-A secretion from both human and mouse islets ex vivo and the impact of reduced Highlights• The compensatory hyperinsulinemic phase of type-2 diabetes is accompanied with significant pancreatic islet remodeling.• Bona fide islet resident macrophages are increased during the diabetic compensation phase by largely in situ proliferation.• Ablating macrophages severely compromises the islet remodeling process and exacerbates glycemic control in vivo.• Mouse and human islet macrophages contribute VEGF-A to the islet environment.• Specific removal of islet macrophages delays islet vascularization in compensatory hyperinsulinemic mice.

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Section: Higher Numbers Of Macrophages Within Islets Of Db/db Micesupporting

confidence: 85%

Islet macrophages drive islet vascular remodeling and compensatory hyperinsulinemia in the early stages of diabetes

Chittezhath

Gunaseelan

Zheng

et al. 2019

Preprint

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“…; Chen et al. ). As the three‐dimensional structure of pancreatic islets supports viability and function of beta cells through cell‐cell and cell‐matrix communications (Rutter and Hodson ; Arous and Wehrle‐Haller ; Reissaus and Piston ; Briant et al.…”

Section: Introductionmentioning

confidence: 99%

“…The loss of functional beta cell mass is the central pathology for both type 1 and type 2 diabetes (Kahn 2001;Atkinson et al 2014;Chen et al 2017). As the threedimensional structure of pancreatic islets supports viability and function of beta cells through cell-cell and cell-matrix communications (Rutter and Hodson 2015;Arous and Wehrle-Haller 2017;Reissaus and Piston 2017;Briant et al 2018), it is critical to address beta cell pathophysiology in pancreatic islets.…”

Section: Introductionmentioning

confidence: 99%

Delivery of shRNA via lentivirus in human pseudoislets provides a model to test dynamic regulation of insulin secretion and gene function in human islets

et al. 2018

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AbstractsRodent islets are widely used to study the pathophysiology of beta cells and islet function, however, structural and functional differences exist between human and rodent islets, highlighting the need for human islet studies. Human islets are highly variable, deteriorate during culture, and are difficult to genetically modify, making mechanistic studies difficult to conduct and reproduce. To overcome these limitations, we tested whether pseudoislets, created by dissociation and reaggregation of islet cell suspensions, allow for assessment of dynamic islet function after genetic modulation. Characterization of pseudoislets cultured for 1 week revealed better preservation of first‐phase glucose‐stimulated insulin secretion (GSIS) compared with cultured‐intact islets and insulin secretion profiles similar to fresh islets when challenged by glibenclamide and KCl. qPCR indicated that pseudoislets are similar to the original islets for the expression of markers for cell types, beta cell function, and cellular stress with the exception of reduced proinflammatory cytokine genes (IL1B, CCL2, CXCL8). The expression of extracellular matrix markers (ASPN, COL1A1, COL4A1) was also altered in pseudoislets compared with intact islets. Compared with intact islets transduced by adenovirus, pseudoislets transduced by lentivirus showed uniform transduction and better first‐phase GSIS. Lastly, the lentiviral‐mediated delivery of short hairpin RNA targeting glucokinase (GCK) achieved significant reduction of GCK expression in pseudoislets as well as marked reduction of both first and second phase GSIS without affecting the insulin secretion in response to KCl. Thus, pseudoislets are a tool that enables efficient genetic modulation of human islet cells while preserving insulin secretion.

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“…We demonstrate that the 3D distribution of pancreatic beta cells as single cell or groups of cells within the islet of Langerhans can be readily imaged and quantified by our new approach demonstrating the islet size heterogeneity. Regional differences of islet size and distribution (head vs. tail) in human pancreas are well known, and alterations in beta cell mass occur in diverse metabolic disorders [47]. For instance in disease conditions like type 2 diabetes, regional changes of islet distribution leading to preferentially large islets in the head region occur [48].…”

Section: Discussionmentioning

confidence: 99%

Cellular and Molecular Probing of Intact Transparent Human Organs

Zhao

Todorov

Cai

et al. 2019

Preprint

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Optical tissue transparency permits cellular and molecular investigation of complex tissues in 3D, a fundamental need in biomedical sciences. Adult human organs are particularly challenging for this approach, owing to the accumulation of dense and sturdy molecules in decadesaged human tissues. Here, we introduce SHANEL method utilizing a new tissue permeabilization approach to clear and label stiff human organs. We used SHANEL to generate the first intact transparent adult human brain and kidney, and perform 3D histology using antibodies and dyes in centimeters depth. Thereby, we revealed structural details of sclera, iris and suspensory ligament in the human eye, and the vessels and glomeruli in the human kidney. We also applied SHANEL on transgenic pig organs to map complex structures of EGFP expressing beta cells in >10 cm size pancreas. Overall, SHANEL is a robust and unbiased technology to chart the cellular and molecular architecture of intact large mammalian organs.

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Human beta cell mass and function in diabetes: Recent advances in knowledge and technologies to understand disease pathogenesis

Cited by 387 publications

References 231 publications

Islet macrophages drive islet vascular remodeling and compensatory hyperinsulinemia in the early stages of diabetes

Islet macrophages drive islet vascular remodeling and compensatory hyperinsulinemia in the early stages of diabetes

Delivery of shRNA via lentivirus in human pseudoislets provides a model to test dynamic regulation of insulin secretion and gene function in human islets

Cellular and Molecular Probing of Intact Transparent Human Organs

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