Abstract
It has been generally assumed that insulin circulates freely in blood. However it can also interact with plasma proteins. Insulin receptors are located in the membrane of target cells and consist of an alpha and beta subunits with a tyrosine kinase cytoplasmic domain. The ectodomain, called soluble insulin receptor (SIR) has been found elevated in patients with diabetes mellitus. We explored if insulin binds to SIRs in circulation under physiological conditions and hypothesize that this SIR may be released by hepatocytes in response to high insulin concentrations. The presence of SIR in rat and human plasmas and the culture medium of hepatocytes was explored using Western blot analysis. A purification protocol was performed to isolated SIR using affinity, gel filtration, and ion exchange chromatographies. A modified reverse hemolytic plaque assay was used to measure SIR release from cultured hepatocytes. Incubation with 1 nmol l−1 insulin induces the release of the insulin receptor ectodomains from normal rat hepatocytes. This effect can be partially prevented by blocking protease activity. Furthermore, plasma levels of SIR were higher in a model of metabolic syndrome, where rats are hyperinsulinemic. We also found increased SIR levels in hyperinsulinemic humans. SIR may be an important regulator of the amount of free insulin in circulation. In hyperinsulinemia, the amount of this soluble receptor increases and this could lead to higher amounts of insulin bound to this receptor, rather than free insulin, which is the biologically active form of the hormone. This observation could enlighten the mechanisms of insulin resistance.
Highlights
Insulin is the most important hypoglycemic hormone in mammals
We explored if insulin binds to soluble insulin receptor (SIR) in circulation under physiological conditions and hypothesize that this SIR may be released by hepatocytes in response to high insulin concentrations
In this study we tested the hypothesis that a certain amount of plasma insulin does not travel freely in circulation, but rather it is bound to proteins, predominantly produced by the liver
Summary
Insulin is the most important hypoglycemic hormone in mammals. It is secreted by pancreatic beta cells in response to glucose stimulation and enters the portal circulation before inflowing the general circulation. The IR has been extensively studied for more than 40 years. It is an acidic protein with an isoelectric point of 4.0 that constitutes a heavily glycosylated disulfide-linked homodimer [1, 2]. Each monomer is formed by an alpha subunit (130 kDa) and a beta subunit (95 kDa) [3]. The entire alpha chain and a short sequence of the beta chain comprise the ectodomain; beta-subunits have membrane spanning regions and cytoplasmic tyrosine kinase (TK) domains [4]. The IR belongs to a family of receptors with TK activity, and it is closely related to the type-1 insulin-like growth factor receptor (IGF-1R) [5]
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