Longitudinal Association of Maternal Pre-Pregnancy BMI and Third-Trimester Glycemia with Early Life Growth of Offspring: A Prospective Study among GDM-Negative Pregnant Women.

Jiaojiao Zou,Huijing Shi,Yunhui Zhang,Qian Wei,Yanting Yang

doi:10.3390/nu13113971

Abstract

Intrauterine modifiable maternal metabolic factors are essential to the early growth of offspring. The study sought to evaluate the associations of pre-pregnancy BMI and third-trimester fasting plasma glucose (FPG) with offspring growth outcomes within 24 months among GDM-negative pregnant women. Four hundred eighty-three mother –offspring dyads were included from the Shanghai Maternal-Child Pairs Cohort. The pregnant women were categorized into four mutually exclusive groups according to pre-pregnancy BMI as normal or overweight/obesity and third-trimester FPG as controlled or not controlled. Offspring growth in early life was indicated by the BAZ (BMI Z-score), catch-up growth, and overweight/obesity. Among those with controlled third-trimester FPG, pre-pregnancy overweight/obesity significantly increased offspring birth weight, BAZ, and risks of overweight/obesity (RR 1.83, 95% CI 1.23 to 2.73) within 24 months. Those who had uncontrolled third-trimester FPG had a reduced risk of offspring overweight/obesity within 24 months by 47%. The combination of pre-pregnancy overweight/obesity and maternal uncontrolled third-trimester FPG increased 5.24-fold risk of offspring catch-up growth within 24 months (p < 0.05). Maternal pre-pregnancy overweight/obesity and uncontrolled third-trimester glycemia among GDM-negative women both have adverse effects on offspring growth within 24 months. With the combination of increasing pre-pregnancy BMI and maternal third-trimester FPG, the possibility of offspring catch-up growth increases.

Highlights

Life is a sensitive period characterized by adipocyte proliferation; once the number of adipocytes is set, it does not decrease [1]
The theory of fetal programming emphasizes that pre-pregnancy obesity and poor glycemic control during pregnancy are the main burdens of intergenerational health [6,7]
Intrauterine hyperglycemia exposure and adipogenic intrauterine exposed have the potential for DNA methylation or epigenetic changes in the fetal phenotype; these intrauterine phenomena contributed to the elevated risk of development of glucose intolerance and overweight/obesity in progeny [6,8,9]

Summary

Introduction

Life is a sensitive period characterized by adipocyte proliferation; once the number of adipocytes is set, it does not decrease [1]. The number of overweight/obesity cases is increasing among children under the age of 5 years and even among toddlers, totaling more than 40 million [2], and this weight gain in early life predicts an increasing risk of lifetime chronic morbidity and premature mortality [3,4]. Fetal programming is considered as a key mechanism underlying the association between metabolic programing in utero and negative health outcomes in offspring [5]. The theory of fetal programming emphasizes that pre-pregnancy obesity and poor glycemic control during pregnancy are the main burdens of intergenerational health [6,7]. A high maternal prepregnancy BMI and abnormal glycemic control are interrelated factors and are associated with the growth of offspring in childhood [11]

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Results

Discussion

Conclusion