PAX4 preserves endoplasmic reticulum integrity preventing beta cell degeneration in a mouse model of type 1 diabetes mellitus

Mellado-Gil, José Manuel; Jiménez-Moreno, Carmen M.; Martín-Montalvo, Aléjandro; Álvarez‐Mercado, Ana I.; Fuente-Martín, Esther; Cobo-Vuilleumier, Nadia; Lorenzo, Petra I.; Bru-Tarí, Eva; Herrera-Gómez, Irene de Gracia; López-Noriega, Livia; Pérez-Florido, Javier; Santoyo-López, Javier; Spyrantis, Andreas; Meda, Paolo; Boehm, Bernhard O.; Quesada, Iván; Gauthier, Benoit R.

doi:10.1007/s00125-016-3864-0

Cited by 34 publications

(36 citation statements)

References 48 publications

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“…In contrast, their expression levels were decreased in the cells overexpressing PAX4 R192H but not PAX4 P321H variant protein (Figure 4). In consistence with the previous report, 24 we also observed that PAX4 R121W, a diabetes-linked variant reported in Japanese with T2D, 12 was less efficient to activate the expression of Lgals9 and Calr genes than the wild-type PAX4 protein ( Figure 4). These data illustrated that PAX4 R192H variant protein impaired transcription activation on target genes that required to maintain β-cell function, proliferation and survival.…”

Section: Ins-1 Cell Viability Under Hyperglycemic Stress Conditionsupporting

confidence: 91%

PAX4 R192H and P321H polymorphisms in type 2 diabetes and their functional defects

et al. 2016

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We have previously identified PAX4 mutations causing MODY9 and a recent genome-wide association study reported a susceptibility locus of type 2 diabetes (T2D) near PAX4. In this study, we aim to investigate the association between PAX4 polymorphisms and T2D in Thai patients and examine functions of PAX4 variant proteins. PAX4 rs2233580 (R192H) and rs712701 (P321H) were genotyped in 746 patients with T2D and 562 healthy normal control subjects by PCR and restriction-fragment length polymorphism method. PAX4 variant proteins were investigated for repressor function on human insulin and glucagon promoters and for cell viability and apoptosis upon high glucose exposure. Genotype and allele frequencies of PAX4 rs2233580 were more frequent in patients with T2D than in control subjects (P=0.001 and 0.0006, respectively) with odds ratio of 1.66 (P=0.001; 95% confidence interval, 1.22-2.27). PAX4 rs712701 was not associated with T2D but it was in linkage disequilibrium with rs2233580. The 192H/321H (A/A) haplotype was more frequent in T2D patients than in controls (9.5% vs 6.6%; P=0.009). PAX4 R192H, but not PAX4 P321H, impaired repression activities on insulin and glucagon promoters and decreased transcript levels of genes required to maintain β-cell function, proliferation and survival. Viability of β-cell was reduced under glucotoxic stress condition for the cells overexpressing either PAX4 R192H or PAX4 P321H or both. Thus these PAX4 polymorphisms may increase T2D risk by defective transcription regulation of target genes and/or decreased β-cell survival in high glucose condition.

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Section: Ins-1 Cell Viability Under Hyperglycemic Stress Conditionsupporting

confidence: 91%

PAX4 R192H and P321H polymorphisms in type 2 diabetes and their functional defects

et al. 2016

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“…The pro-proliferative and anti-apoptotic role of PAX4 has been validated in vivo in a mouse model that conditionally over-express PAX4 specifically in β-cells. Over-expression of PAX4 in vivo protects β-cells from apoptosis induced by streptozotocin (STZ) and in a mouse model of experimental autoimmune diabetes (RIPB7.1 mice) [37,39]. Remarkably, in the latter model, PAX4 overexpression decreases islet immune cell infiltration (insulitis), suggesting a novel immunomodulatory function of PAX4 [39].…”

Section: Pax4 In Islet Physiology: Key Player In β-Cell Generationmentioning

confidence: 99%

“…Moreover, long-term in vivo ectopic expression of PAX4 increases c-Myc and Cdk4 mRNA levels, correlating with the increase in proliferation of PDX1 + /insulin − β-cells [37]. Remarkably, transcriptome analysis of islet cells after PAX4 overexpression in vivo revealed the downregulation of cyclin-dependent kinase inhibitor 2A, which strongly inhibits Cdk4 , [39]. Further analysis or these microarray data revealed a functional enrichment in cell cycle pathway after PAX4 overexpression.…”

Section: Pax4 Mechanism Of Action: Downstream Regulated Genesmentioning

confidence: 99%

The Diabetes-Linked Transcription Factor PAX4: From Gene to Functional Consequences

Lorenzo

Juárez-Vicente

Cobo-Vuilleumier

et al. 2017

Genes

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Paired box 4 (PAX4) is a key factor in the generation of insulin producing β-cells during embryonic development. In adult islets, PAX4 expression is sequestered to a subset of β-cells that are prone to proliferation and more resistant to stress-induced apoptosis. The importance of this transcription factor for adequate pancreatic islets functionality has been manifested by the association of mutations in PAX4 with the development of diabetes, independently of its etiology. Overexpression of this factor in adult islets stimulates β-cell proliferation and increases their resistance to apoptosis. Additionally, in an experimental model of autoimmune diabetes, a novel immunomodulatory function for this factor has been suggested. Altogether these data pinpoint at PAX4 as an important target for novel regenerative therapies for diabetes treatment, aiming at the preservation of the remaining β-cells in parallel to the stimulation of their proliferation to replenish the β-cell mass lost during the progression of the disease. However, the adequate development of such therapies requires the knowledge of the molecular mechanisms controlling the expression of PAX4 as well as the downstream effectors that could account for PAX4 action.

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“…Given the effects of T4 supplementation in the promotion of beta cell proliferation and the increase of circulating insulin levels in healthy C57BL/6 mice, we next sought to determine whether T4 supplementation could blunt the onset of T1DM in the RIP-B7.1 model of EAD (Harlan et al, 1994;Mellado-Gil et al, 2016). To this end, RIP-B7.1 mice were treated with T4, (5 μg·mL À1 in drinking water) starting at 6 weeks of age.…”

Section: T4 Supplementation Improves Glycaemic Control In the Rip-b7mentioning

confidence: 99%

“…Female mice were treated or not with T4 starting at birth (s.c. injection of 18 ng·g À1 of body weight daily until weaning). After weaning, mice were supplemented with T4 in drinking water (50 μg·mL À1 ) (Spencer and West, 1961;Weinstein et al, 1991;Weinstein et al, 1994 Buras et al, 2014 For experiments related to EAD, transgenic RIP-B7.1 mice were used (Harlan et al, 1994;Mellado-Gil et al, 2016); these mice were supplied by Dr Bernhard. O. Boehm (Ulm University Medical Centre, Ulm, Germany).…”

Section: Animalsmentioning

confidence: 99%

Levothyroxine enhances glucose clearance and blunts the onset of experimental type 1 diabetes mellitus in mice

López-Noriega

Cobo-Vuilleumier

Narbona-Pérez

et al. 2017

British J Pharmacology

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Thyroid hormones induce several changes in whole body metabolism that are known to improve metabolic homeostasis. However, adverse side effects have prevented its use in the clinic. In view of the promising effects of thyroid hormones, we investigated the effects of levothyroxine supplementation on glucose homeostasis. EXPERIMENTAL APPROACHC57BL/6 mice were treated with levothyroxine from birth to 24 weeks of age, when mice were killed. The effects of levothyroxine supplementation on metabolic health were determined. C57BL/6 mice treated with levothyroxine for 2 weeks and then challenged with streptozotocin to monitor survival. Mechanistic experiments were conducted in the pancreas, liver and skeletal muscle. RIP-B7.1 mice were treated with levothyroxine for 2 weeks and were subsequently immunized to trigger experimental autoimmune diabetes (EAD). Metabolic tests were performed. Mice were killed and metabolic tissues were extracted for immunohistological analyses. KEY RESULTSLong-term levothyroxine supplementation enhanced glucose clearance and reduced circulating glucose in C57BL/6 mice. Levothyroxine increased simultaneously the proliferation and apoptosis of pancreatic beta cells, promoting the maintenance of a highly insulin-expressing beta cell population. Levothyroxine increased circulating insulin levels, inducing sustained activation of IRS1-AKT signalling in insulin-target tissues. Levothyroxine-treated C57BL/6 mice challenged with streptozotocin exhibited extended survival. Levothyroxine blunted the onset of EAD in RIP-B7.1 mice by inducing beta cell proliferation and preservation of insulin-expressing cells. CONCLUSIONS AND IMPLICATIONSInterventions based on the use of thyroid hormones or thyromimetics could be explored to provide therapeutic benefit in patients with type 1 diabetes mellitus.

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PAX4 preserves endoplasmic reticulum integrity preventing beta cell degeneration in a mouse model of type 1 diabetes mellitus

Cited by 34 publications

References 48 publications

PAX4 R192H and P321H polymorphisms in type 2 diabetes and their functional defects

PAX4 R192H and P321H polymorphisms in type 2 diabetes and their functional defects

The Diabetes-Linked Transcription Factor PAX4: From Gene to Functional Consequences

Levothyroxine enhances glucose clearance and blunts the onset of experimental type 1 diabetes mellitus in mice

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