Reduced Mitogenic Action of Insulin Evaluated as ³H-Thymidine Uptake in Diabetic Cultured Fibroblasts

 

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Summary

As cultured diabetic fibroblasts have a shorter lifespan than normal subjects, the mitogenic activity of foetal calf serum (FCS) and insulin have been studied by taking skin biopsies from 5 patients with juvenile onset diabetes (JODM), 8 with adult onset diabetes (AODM) and 5 with chemical (latent) diabetes (CDM). In controls a high dose of insulin (20 μg/ml) produced a tritiated thymidine uptake lower than 10 % FCS. At lower doses (0.1 to 1.0 μg/ml) a dose-dependent uptake was observed. In diabetic fibroblasts 10 % FCS produced a lower ³H-thymidine uptake than in controls, with p < 0.005 in JODM, p < 0.01 in AODM and p < 0.01 in CDM. A high dose of insulin produced a lower uptake in patients with JODM (p < 0.01), AODM (p < 0.01) and CDM (p < 0.05) when compared with controls. However, when lower doses of insulin were used, 2 out of 5 cases of JODM and 4 out of 8 cases of AODM showed a similar response to controls, while ³H-thymidine uptake was low or absent in the remaining cases, including all those with CDM.

This study indicates that a reduced mitogenic action of FCS and insulin exists in many patients affected by clinical or chemical diabetes. Our results suggest, however, that the sensitivity to the two mitogenic factors seems to be dissociated: in fact, while a reduced response to FCS is present in all patients, the response to insulin seems to be correlated to the patient's equilibrium at the time of skin biopsy.