Primary Cilia in Pancreatic β- and α-Cells: Time to Revisit the Role of Insulin-Degrading Enzyme

Pablos, Marta I.; Casanueva-Álvarez, Elena; González-Casimiro, Carlos M.; Merino, Beatriz; Perdomo, Germán; Cózar‐Castellano, Irene

doi:10.3389/fendo.2022.922825

Cited by 3 publications

(3 citation statements)

References 223 publications

(315 reference statements)

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“…At a T2D signal on chromosome 11, risk variants increase the activity of a beta cell cRE linked to DEUP1 as well as DEUP1 expression in islets. DEUP1 is a component of cell division machinery 80 and, given in vitro evidence that DEUP1 can self-assemble 81 , increased DEUP1 activity and assembly may alter signal reception or microtubule dynamics 82 . Other genes linked to beta cell cREs affected by T2D risk variants include UBE2E2, which alters insulin secretion in mouse beta cells 83 , and CD101, which has no established role in beta cells.…”

Section: Discussionmentioning

confidence: 99%

Single cell multiome profiling of pancreatic islets reveals physiological changes in cell type-specific regulation associated with diabetes risk

Mummey,

Elison,

Korgaonkar

et al. 2024

Preprint

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Physiological variability in pancreatic cell type gene regulation and the impact on diabetes risk is poorly understood. In this study we mapped gene regulation in pancreatic cell types using single cell multiomic (joint RNA-seq and ATAC-seq) profiling in 28 non-diabetic donors in combination with single cell data from 35 non-diabetic donors in the Human Pancreas Analysis Program. We identified widespread associations with age, sex, BMI, and HbA1c, where gene regulatory responses were highly cell type- and phenotype-specific. In beta cells, donor age associated with hypoxia, apoptosis, unfolded protein response, and external signal-dependent transcriptional regulators, while HbA1c associated with inflammatory responses and gender with chromatin organization. We identified 10.8K loci where genetic variants were QTLs forcisregulatory element (cRE) accessibility, including 20% with lineage- or cell type-specific effects which disrupted distinct transcription factor motifs. Type 2 diabetes and glycemic trait associated variants were enriched in both phenotype- and QTL-associated beta cell cREs, whereas type 1 diabetes showed limited enrichment. Variants at 226 diabetes and glycemic trait loci were QTLs in beta and other cell types, including 40 that were statistically colocalized, and annotating target genes of colocalized QTLs revealed genes with putatively novel roles in disease. Our findings reveal diverse responses of pancreatic cell types to phenotype and genotype in physiology, and identify pathways, networks, and genes through which physiology impacts diabetes risk.

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Section: Discussionmentioning

confidence: 99%

Single cell multiome profiling of pancreatic islets reveals physiological changes in cell type-specific regulation associated with diabetes risk

Mummey,

Elison,

Korgaonkar

et al. 2024

Preprint

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“…This pathological state alters the functional capacity of the pancreas and liver, contributing to the pathogenicity of T2DM [7,9,10]. In this line of evidence our group has made a substantial contribution to explain the role of IDE in α-cells on hyperglucagonemia [15,16], however this topic is out of the scope of this thesis.…”

Section: I2 Liver Glucagon Signaling and Hyperglucagonemia In T2dmmentioning

confidence: 91%

“…Another putative explanation for GCGR lost may be cytoskeleton disarrangement. Recently, we reported that genetic depletion of Ide in α-cells (αTC1.9 cell line transfected with an Ide-targeting siRNA) resulted in cytoskeleton disarrangement and a significant reduction in the number of primary cilia [15,16].…”

Section: V31 Hepatic Glucagon Signaling In Hepatocytesmentioning

confidence: 99%

Hepatic insulin-degrading enzyme regulation and its role on glucagon signaling

Casimiro¹

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Fluorescence imaging of beta cell primary cilia

Cho

Woodhams

et al. 2022

Front. Endocrinol.

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Primary cilia are slender cell-surface organelles that project into the intercellular space. In pancreatic beta cells, primary cilia coordinate a variety of cell responses including GPCR signaling, calcium influx, and insulin secretion, along with likely many underappreciated roles in islet development and differentiation. To study cilia function in islet biology, direct visualization of primary cilia by microscopic methods is often a necessary first step. Ciliary abundance, distribution, and morphology are heterogeneous among islet cells and are best visualized by fluorescence microscopy, the tools for which are readily accessible to most researchers. Here we present a collection of fluorescence imaging methods that we have adopted and optimized for the observation of primary cilia in mouse and human islets. These include conventional confocal microscopy using fixed islets and pancreas sections, live-cell imaging with cilia-targeted biosensors and probes, cilia motion recordings, and quantitative analysis of primary cilia waveform in the ex vivo environment. We discuss practical considerations and limitations of our approaches as well as new tools on the horizon to facilitate the observation of primary cilia in pancreatic islets.

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Primary Cilia in Pancreatic β- and α-Cells: Time to Revisit the Role of Insulin-Degrading Enzyme

Cited by 3 publications

References 223 publications

Single cell multiome profiling of pancreatic islets reveals physiological changes in cell type-specific regulation associated with diabetes risk

Single cell multiome profiling of pancreatic islets reveals physiological changes in cell type-specific regulation associated with diabetes risk

Hepatic insulin-degrading enzyme regulation and its role on glucagon signaling

Fluorescence imaging of beta cell primary cilia

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