There are many reasons to think that epigenetics is a key determinant of fetal growth variability across the normal population. Since and genes are major determinants of intrauterine growth, we examined the methylation of selected CpGs located in the regulatory region of these two genes. Cord blood was sampled in 159 newborns born to mothers prospectively followed during their pregnancy. A 142-item questionnaire was filled by mothers at inclusion, during the last trimester of the pregnancy and at the delivery. The methylation of selected CpGs located in the promoters of the and genes was measured in cord blood mononuclear cells collected at birth using bisulfite-PCR-pyrosequencing. Methylation at CpG-137 correlated negatively with birth length (  = 0.27,  = 3.5 × 10 ). The same effect size was found after adjustment for maternal age, parity, and smoking: a 10% increase in CpG-137 methylation was associated with a decrease of length by 0.23 SDS. The current results suggest that the methylation of CpG-137 contributes to the individual variation of fetal growth by regulating expression in fetal tissues.