Tyrosine kinase-defective insulin receptors undergo decreased endocytosis but do not affect internalization of normal endogenous insulin receptors

Grako, Kathryn A.

doi:10.1210/en.130.6.3441

Cited by 9 publications

(10 citation statements)

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“…Insulin binding to adipocytes was indeed found to be inhibited in obesity, reflecting a decrease in the number of adipocyte surface receptors [161, 162] following induction of receptor endocytosis in response to insulin binding [163, 164]. However, the remaining receptors were calculated to be sufficient to mediate a full response at high insulin concentrations, which is at odds with the greatly decreased maximum response of lipogenesis that was observed [165, 166].…”

Section: Mechanisms Of Insulin Resistance Of Adipocyte Lipogenesismentioning

confidence: 99%

Insulin signalling mechanisms for triacylglycerol storage

et al. 2013

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Insulin signalling is uniquely required for storing energy as fat in humans. While de novo synthesis of fatty acids and triacylglycerol occurs mostly in liver, adipose tissue is the primary site for triacylglycerol storage. Insulin signalling mechanisms in adipose tissue that stimulate hydrolysis of circulating triacylglycerol, uptake of the released fatty acids and their conversion to triacylglycerol are poorly understood. New findings include (1) activation of DNA-dependent protein kinase to stimulate upstream stimulatory factor (USF)1/USF2 heterodimers, enhancing the lipogenic transcription factor sterol regulatory element binding protein 1c (SREBP1c); (2) stimulation of fatty acid synthase through AMP kinase modulation; (3) mobilisation of lipid droplet proteins to promote retention of triacylglycerol; and (4) upregulation of a novel carbohydrate response element binding protein β isoform that potently stimulates transcription of lipogenic enzymes. Additionally, insulin signalling through mammalian target of rapamycin to activate transcription and processing of SREBP1c described in liver may apply to adipose tissue. Paradoxically, insulin resistance in obesity and type 2 diabetes is associated with increased triacylglycerol synthesis in liver, while it is decreased in adipose tissue. This and other mysteries about insulin signalling and insulin resistance in adipose tissue make this topic especially fertile for future research.

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Section: Mechanisms Of Insulin Resistance Of Adipocyte Lipogenesismentioning

confidence: 99%

Insulin signalling mechanisms for triacylglycerol storage

et al. 2013

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“…It has long been known that IR kinase activity is crucial for receptor endocytosis 42 , 43 , suggesting that IR endocytosis normally occurs after the receptor has been activated and has transduced signals downstream. However, how activated IR is selectively internalized remained largely unknown until our recent study.…”

Section: Introductionmentioning

confidence: 99%

Insulin receptor endocytosis in the pathophysiology of insulin resistance

Hall

Choi

2020

Exp Mol Med

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Insulin signaling controls cell growth and metabolic homeostasis. Dysregulation of this pathway causes metabolic diseases such as diabetes. Insulin signaling pathways have been extensively studied. Upon insulin binding, the insulin receptor (IR) triggers downstream signaling cascades. The active IR is then internalized by clathrin-mediated endocytosis. Despite decades of studies, the mechanism and regulation of clathrin-mediated endocytosis of IR remain incompletely understood. Recent studies have revealed feedback regulation of IR endocytosis through Src homology phosphatase 2 (SHP2) and the mitogen-activated protein kinase (MAPK) pathway. Here we review the molecular mechanism of IR endocytosis and its impact on the pathophysiology of insulin resistance, and discuss the potential of SHP2 as a therapeutic target for type 2 diabetes.

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“…Conversely, phosphorylation of a highly conserved serine residue on transcription factor ΔFosB protects it from proteasomal degradation [ 14 ]. Other proteins have been reported to have a faster turnover when activated, including the activation of receptor tyrosine kinases by growth factors and insulin receptors by insulin [ 15 , 16 ]. EGFR in wild-type cells was found to have a half-life of about 20 hours, but when EGF was added to the cells, the half-life dropped to about 9 hours [ 17 ].…”

Section: Introductionmentioning

confidence: 99%

Effects of Activating Mutations on EGFR Cellular Protein Turnover and Amino Acid Recycling Determined Using SILAC Mass Spectrometry

Greig

Niessen

Weinrich

et al. 2015

International Journal of Cell Biology

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Rapid mutations of proteins that are targeted in cancer therapy often lead to drug resistance. Often, the mutation directly affects a drug's binding site, effectively blocking binding of the drug, but these mutations can have other effects such as changing the protein turnover half-life. Utilizing SILAC MS, we measured the cellular turnover rates of an important non-small cell lung cancer target, epidermal growth factor receptor (EGFR). Wild-type (WT) EGFR, EGFR with a single activating mutant (Del 746–750 or L858R), and the drug-resistant double mutant (L858R/T790M) EGFR were analyzed. In non-small cell lung cancer cell lines, EGFR turnover rates ranged from 28 hours in A431 cells (WT) to 7.5 hours in the PC-9 cells (Del 746–750 mutant). The measurement of EGFR turnover rate in PC-9 cells dosed with irreversible inhibitors has additional complexity due to inhibitor effects on cell viability and results were reported as a range. Finally, essential amino acid recycling (K and R) was measured in different cell lines. The recycling was different in each cell line, but the overall inclusion of the effect of amino acid recycling on calculating EGFR turnover rates resulted in a 10–20% reduction in rates.

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Tyrosine kinase-defective insulin receptors undergo decreased endocytosis but do not affect internalization of normal endogenous insulin receptors

Cited by 9 publications

References 0 publications

Insulin signalling mechanisms for triacylglycerol storage

Insulin signalling mechanisms for triacylglycerol storage

Insulin receptor endocytosis in the pathophysiology of insulin resistance

Effects of Activating Mutations on EGFR Cellular Protein Turnover and Amino Acid Recycling Determined Using SILAC Mass Spectrometry

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