Insulin and insulin propeptides at birth in offspring of diabetic mothers

Abstract

Maternal diabetes during pregnancy is associated with excess fetal growth and increased fetal insulin production. We hypothesized that insulin propeptides (proinsulin and 32-33 split proinsulin) might be more robust indicators of chronic fetal overproduction of insulin. We examined insulin-like molecules in cord blood (ILM) (insulin, proinsulin, and 32-33 split proinsulin) in relation to birth weight, maternal glycemia, and cord glucose in 140 offspring of mothers with type 1 diabetes (ODM) and 49 offspring of mothers who did not have diabetes (CONTROL) as well as degradation of ILM in response to sampling conditions at birth. Insulin propeptides were abundant in cord blood, comprising 50% of ILM in CONTROL and 36% in ODM (P < 0.0001) and more resistant to degradation than insulin (P < 0.05). Concentrations of all three ILM were highly intercorrelated with median values 2- to 5-fold higher in ODM than CONTROL [e.g. median (range): insulin ODM 110 (60-217) pmol/liter; CONTROL 22 (15-37) pmol/liter; P < 0.0001]. In ODM, 32-33 split proinsulin and proinsulin were more closely related to birth weight (Spearman r for ILM: r32-33 SPLIT= 0.54; rPROINSULIN: r = 0.54; rINSULIN = 0.40: r32-33 SPLIT and rPROINSULIN > rINSULINE P < 0.05) and fetal leptin (r32-33 SPLIT = 0.55; rPROINSULIN; r = 0.54; rINSULINE = 0.22: r32-33 SPLIT and rPROINSULIN > rINSULINE P < 0.05) than insulin). By contrast, insulin was more closely related to cord glucose (r32-33 SPLIT = 0.15; rPROINSULIN: r = 0.10; rINSULIN = 0.42: rINSULINE > r32-33 SPLIT and rPROINSULIN P < 0.05). In CONTROL, 32-33 split proinsulin was also more closely related to fetal leptin r32-33 SPLIT = 0.61; rPROINSULIN: r = 0.29; rINSULIN = 0.33: r32-33 SPLIT > rINSULIN P < 0.05). In ODM, 32-33 split proinsulin and proinsulin have closer relationships to fetal growth and leptin concentrations at birth than insulin. Measurement of insulin propeptides may be advantageous in assessment of the influence of maternal hyperglycemia on the newborn.