| Literature DB >> 24633815 |
Abstract
The insulin receptor (IR) is an important hub in insulin signaling and its activation is tightly regulated. Upon insulin stimulation, IR is activated through autophosphorylation, and consequently phosphorylates several insulin receptor substrate (IRS) proteins, including IRS1-6, Shc and Gab1. Certain adipokines have also been found to activate IR. On the contrary, PTP, Grb and SOCS proteins, which are responsible for the negative regulation of IR, are characterized as IR inhibitors. Additionally, many other proteins have been identified as IR substrates and participate in the insulin signaling pathway. To provide a more comprehensive understanding of the signals mediated through IR, we reviewed the upstream and downstream signal molecules of IR, summarized the positive and negative modulators of IR, and discussed the IR substrates and interacting adaptor proteins. We propose that the molecular events associated with IR should be integrated to obtain a better understanding of the insulin signaling pathway and diabetes.Entities:
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Year: 2014 PMID: 24633815 PMCID: PMC3967058 DOI: 10.1007/s13238-014-0030-7
Source DB: PubMed Journal: Protein Cell ISSN: 1674-800X Impact factor: 14.870
Figure 1The diagram illustrating the inputs and outputs of insulin receptor. (A) Classical IR inputs and outputs. (B) Summary of proteins associating with IR which include positive modulator (purple), negative modulator (red), alternative substrates (green) and interactors (blue). Arrow: stimulation; Line: interaction; Arrow with flathead: inhibition
Proteins associated with the inputs and outputs of insulin receptor
| Protein | Function | References |
|---|---|---|
|
| ||
| Glypican-4 | Binds IR α subunits. Facilitates insulin-induced formational change of IR | Ussar et al. |
|
| ||
| PTP1B | Major PTP involved in insulin signaling. Dephosphorylates IR tyrosine | Salmeen et al. |
| TCPTP | Cooperates with PTP1B. Dephosphorylate IR tyrosine | Galic et al. |
| PTPRF | Dephosphorylates IR tyrosine | Hashimoto et al. |
| PKCδ | Predominant in muscle. Phosphorylates IR serine | Braiman et al. |
| PKCε | Predominant in liver. Phosphorylates IR serine | Samuel et al. |
| Grb7 | Binds IR | Kasus-Jacobi et al. |
| Grb10 | Binds IR. Blocks IRS1/2 | Wick et al. |
| Grb14 | Binds IR. Blocks PTP1B | Nouaille et al. |
| SOCS1 | Binds IR. Interrupts IRS2 | Ueki et al. |
| SOCS3 | Binds IR. Interrupts IRS1/2, STAT5B | Emanuelli et al. |
| SOCS6 | Binds IR. Interrupts IRS1 | Mooney et al. |
| ENPP1 | Binds IR α subunits. Inhibits insulin-induced conformational change of IR | Maddux and Goldfine, |
| AHSG | Binds IR β subunits extracellular region | Mathews et al. |
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| ||
| ADRB2 | Transmembrane protein. Phosphorylated by IR | Baltensperger et al. |
| Calmodulin | Calcium-dependent protein. Phosphorylated by IR | Sacks et al. |
| CEACAM1 | Transmembrane protein. Phosphorylated by IR | Poy et al. |
| Dok1 | GAP-associated protein. Phosphorylated by IR | Wick et al. |
| FABP4 | Fatty acid-binding protein. Phosphorylated by IR | Buelt et al. |
| FAK1 | Integrin signaling pathway. Phosphorylated by IR | Baron et al. |
| FRS2 | FGFR substrate. Phosphorylated by IR | Delahaye et al. |
| PTP1C | Protein tyrosine phosphatase. Phosphorylated by IR | Uchida et al. |
| SH2B1 | Interacts with IR and phosphorylated upon insulin stimulation | Kotani et al. |
| SH2B2 | Interacts with IR and phosphorylated upon insulin stimulation | Moodie et al. |
| STAT5B | Transcriptional factor. Phosphorylated by IR | Chen et al. |
| SYNCRIP | RNA-binding protein. Phosphorylated by IR | Hresko and Mueckler, |
| Sam68 | RNA-binding protein. Phosphorylated by IR | Sanchez-Margalet and Najib, |
| Vav3 | Interacts with and phosphorylated by IR activation | Zeng et al. |
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| ARF | Interacts with activated IR. PLD regulation | Shome et al. |
| hMAD2 | Interacts with inactivated IR | O’Neill et al. |
| JAK1 | Interacts with activated IR. Enhances IRS1 activation | Gual et al. |
| PLCγ1 | Interacts with activated IR. Enhances MAPK activation | Kwon et al. |
| PTP1D | Interacts with activated IR. Enhances IRS1 activation | Kharitonenkov et al. |
| RACK1 | Interacts with activated IR. Facilitates STAT3 activation | Zhang et al. |
| SORBS1 | Interacts with inactivated IR | Lin et al. |