Evaluation of insulin binding and signaling activity of 
newly synthesized chromium(III) complexes in vitro

Mackowiak,Pawel; Krejpcio,Zbigniew; Sassek,Maciej; Kaczmarek,Przemyslaw; Hertig,Iwona; Chmielewska,Joanna; Wojciechowicz,Tatiana; Szczepankiewicz,Dawid; Wieczorek,Daria; Szymusiak,Henryk; Nowak,Krzysztof W.

doi:10.3892/mmr_00000264

Evaluation of insulin binding and signaling activity of newly synthesized chromium(III) complexes in vitro

Authors:
- Pawel Mackowiak
- Zbigniew Krejpcio
- Maciej Sassek
- Przemyslaw Kaczmarek
- Iwona Hertig
- Joanna Chmielewska
- Tatiana Wojciechowicz
- Dawid Szczepankiewicz
- Daria Wieczorek
- Henryk Szymusiak
- Krzysztof W. Nowak
View Affiliations

Affiliations: Department of Animal Physiology and Biochemistry, Poznan University of Life Sciences, Poznan, Poland
Published online on: March 1, 2010 https://doi.org/10.3892/mmr_00000264
Pages: 347-353

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Abstract

In the present study, the influence of chromium(III) complexes (acetate, chloride, glycinate, histidinate, lactate and propionate) on insulin binding and signal transduction [phosphorylation of tyrosine and serine in the insulin receptor substrate (IRS)-1] was investigated in vitro using three experimental models: isolated rat liver membranes and cultured mouse C2C12 myoblasts or 3T3-L1 preadipocytes. The examined complexes did not elevate the binding of insulin to the liver membranes. Moreover, chromium histidinate, lactate, acetate and propionate complexes diminished the specific binding of insulin. Simultaneously, chromium chloride, which did not significantly elevate insulin binding, increased the number of membrane accessible particles of the insulin receptors. However, it was accompanied by slightly diminished affinity of the receptor to the hormone. Chromium acetate and propionate significantly diminished the binding capacity of the low-affinity insulin receptor class. Investigations with the myoblast cell line C2C12 and preadipocyte cell line 3T3-L1 did not allow differentiation of the influence of the examined complexes on insulin binding. Immunodetection of phosphorylated forms of IRS-1 showed that the chromium compounds modulated the transduction of the insulin signal. Chromium glycinate, acetate and propionate decreased the amount of IRS-1 phosphorylated at serine. Since it is generally thought that phosphorylation of serine in IRS-1 may moderate insulin action, the above mentioned chromium complexes may, in this way, enhance insulin effects inside target cells. Phosphorylation of tyrosine in IRS-1, which acts as a stimulatory signal for further steps of insulin action, was elevated after the incubation of 3T3-L1 cells with insulin. Chromium supplementation did not additionally intensify this process. However, in the absence of insulin, chromium glycinate and acetate slightly elevated the level of IRS-1 phosphorylated at tyrosine. This fact may be important in vivo at low levels of insulin in blood. The results indicate that the action of chromium(III) complexes involves a direct effect on the number of receptors accessible to insulin, their affinity to the hormone and the modulation of the signal multiplying proteins by their phosphorylation.