Insulin-receptor substrates

Insulin Receptor. Figure 1 Structure and function of the insulin receptor. Binding of insulin to the a-subunits (yellow) leads to activation of the intracellular tyrosine kinase ((3-subunit) by autophosphorylation. The insulin receptor substrates (IRS) bind via a phospho-tyrosine binding domain to phosphorylated tyrosine residues in the juxtamembrane domain of the (3-subunit. The receptor tyrosine kinase then phosphorylates specific tyrosine motifs (YMxM) within the IRS. These tyrosine phosphorylated motifs serve as docking sites for some adaptor proteins with SRC homology 2 (SH2) domains like the regulatory subunit of PI 3-kinase. 

The catalytic pi 10 subunit has four isoforms, all of which contain a kinase domain and a Ras interaction site. In addition, the a, (3, and y isoforms possess an interaction site for the p85 subunit. The class I enzymes can be further subdivided class IA enzymes interact through their SH2 domains with phosphotyrosines present on either protein tyrosine kinases or to docking proteins such as insulin-receptor substrates (IRSs GAB-1) or linkers for activation of T cells (LATs in the case of T cells). 

Yenush L, Fernandez R, Myers MG Jr et al 1996 The Drosophila insulin receptor activates multiple signaling pathways but requires insulin receptor substrate proteins for DNA... 

IRS insulin receptor substrate MRI magnetic resonance imaging... 

Fig. 12. 3D Structure of a pTyr-containing oligopeptide bound to the IRS-1 (insulin receptor substrate) PTB domain (lIRS.pdb). The Asn-Pro-Ala-pTyr tetrapeptide sequence adopts a regular pi turn conformation [181]...

Once autophosphorylation begins, a complex of other events ensues. An insulin receptor substrate (IRS-1) binds the receptor and is phosphorylated on tyrosine residues, allowing proteins with SH2 (src homology) domains to bind to the. phosphotyrosine residues on IRS-1 and become active. In this way, the receptor activates several enzyme cascades, which involve ... 

Answen Q Proteins with SH2 domains might bind to the insulin receptor substrate-1 (IRS-1) to transmit signals from the insulin receptor, a tyrosine kinase type of receptor. PI-3 kinase is an example of an SH2 domain protein. SH2 domains are not involved in DNA binding (choices A and D). Examples of protein domains that bind DNA include zinc fingers (steroid receptors), leudne zippers (CREB protein), and helix-turn-helbc proteins (homeodomain proteins),... 

CHD coronary heart disease IRS insulin receptor substrate... 

The effects of insulin on transcription are shown on the left of the illustration. Adaptor proteins Crb-2 and SOS ( son of sevenless ) bind to the phosphorylated IRS (insulin-receptor substrate) and activate the G protein Ras (named after its gene, the oncogene ras see p.398). Ras activates the protein kinase Raf (another oncogene product). Raf sets in motion a phosphorylation cascade that leads via the kinases MEK and ERK (also known as MARK, mitogen-activated protein kinase ) to the phosphorylation of transcription factors in the nucleus. 

Activation of the enzyme PIS kinase (PI3K) constitutes a third pathway of Trk receptor signaling. The precise mechanism by which PI3K activation occurs has not yet been completely elucidated, but appears to involve Trk activation of intermediate proteins, such as insulin receptor substrate (IRS)-1,2 and the IRS-like protein Gabl. Downstream of PI3K activation is stimulation of the kinase Akt, which is largely responsible for the survival effects mediated by this pathway. 

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