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J. Biol. Chem., Vol. 255, Issue 19, 9149-9155, 10, 1980
MK Raizada, G Tan and RE Fellows
Binding of 125I-insulin to cells cultured from the skin of nondiabetic and
diabetic (db/db) mice was 80 to 90% specific, time- and temperature-
dependent, and maximal at pH 8.0. Porcine insulin and desalanine insulin
competed equally for 125I-insulin binding, while proinsulin and
desoctapeptide insulin were 35% and 20% as potent, respectively. 125I-
Insulin dissociated from both types of fibroblasts with a T 1/2 of 7.5 min.
Analysis of the dissociation data resolved two rate constants of 3.0 and
1.0 X 10(-4) s-1 for nondiabetic, and 2.0 and 0.8 X 10(-4) s-1 for diabetic
fibroblasts. Binding of 125I-insulin to diabetic fibroblasts was 35 to 50%
of that to nondiabetic fibroblasts during at least 17 passages. Scatchard
analysis of the binding data resolved high (K1 = 2 X 10(10( M-1) and low
affinity K2 = 2 X 10(9) M-1) sites. Nondiabetic fibroblasts possessed 7.7 X
10(4) sites/cell, while diabetic fibroblasts possessed 2.9 X 10(4)/cell.
Incubation of nondiabetic fibroblasts with insulin resulted in a time- and
concentration-dependent decrease in the binding of 125I-insulin. Binding
activity returned to normal when insulin was removed and it was prevented
by cycloheximide. In contrast, diabetic fibroblasts did not exhibit
down-regulation of receptors. A half-maximal and maximum (85%) stimulation
of 2 deoxy-D-glucose uptake was observed with 0.75 nM and 16.7 nM insulin
in nondiabetic fibroblasts. In contrast, diabetic cultures required 3.5 nM
insulin for half-maximal stimulation of 2 deoxy-D-glucose uptake, and
maximum stimulation was 32% with 16.7 nM insulin. Similarly, diabetic
fibroblasts required higher concentrations of insulin (20 nM) to stimulate
ornithine decarboxylase activity to 42% of nondiabetic cells. These results
indicate that in comparison with fibroblastic cultures from nondiabetic
animals, those from diabetic animals expressed differences in insulin
receptor numbers which are maintained in culture over many generations and
are accompanied by diminished insulin responses.
Fibroblastic cultures from the diabetic db/db mouse. Demonstration of decreased insulin receptors and impaired responses to insulin
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