Meal Timing and Glycemic Control during Pregnancy—Is There a Link?

Gestational diabetes mellitus (GDM) and hyperglycemia during pregnancy are important public health problems due to their prevalence and long-term consequences both for maternal and child health. GDM affects approximately one in six births worldwide with the majority of the GDM cases reported in low- and middle-income countries [1]. The prevalence of GDM has almost doubled from 2006 (4.6%) to 2016 (8.2%) in the United States, while it appears to disproportionally affect low-income and minority populations [2].

Diagnosis of GDM can be confirmed using an one-step or two-step strategy at 24–28 weeks of gestation [3]. For the one-step strategy, a single elevated value of fasting plasma glucose (FPG) ≥ 92 mg/dL, 1 h post 75 g oral glucose tolerance test (OGTT) ≥ 180 mg/dL or 2 h post 75 g OGTT ≥ 153 mg/dL is consistent with the diagnosis of GDM. The two-step strategy includes a 1 h 50 g glucose load test (GLT) followed by a 100 g OGTT for those who screen positive (plasma glucose levels ≥ 130, 135, or 140 mg/dL 1 h post 50 g GLT). Using the two-step strategy, the diagnosis of GDM can be established when two or more of the following criteria are met during a 100 g OGTT: FPG ≥ 95 mg/dL, 1 h post 100 g OGTT ≥ 180 mg/dL, 2 h post 100 g OGTT ≥ 155 mg/dL, 3 h post 100 g OGTT ≥ 140 mg/dL.

Hyperglycemia during gestation and GDM have been tied to complications during pregnancy and the development of cardiometabolic disease for the mother and offspring. Specifically, hyperglycemia during pregnancy has been associated with increased odds for gestational hypertension, pre-eclampsia, and premature delivery [4,5,6,7]. Moreover, fetuses exposed to hyperglycemia in utero have a three-fold higher probability of fetal macrosomia [8], which is associated with increased odds of labor abnormalities, shoulder dystocia, and cesarean section [9]. After birth, infants born by mothers with GDM are more likely to experience hypoglycemia due to the existing hyperinsulinemia and hyperglycemia in utero [10,11]. Women with past medical history of GDM are at risk for the development of type 2 diabetes, hypertension, and cardiovascular disease during the first decade postpartum [12,13,14]. Similarly, offspring exposed to hyperglycemia during pregnancy are at high risk of development of the same chronic diseases later in life, which may be due to hyperglycemia-induced epigenetic changes [15].

The management of GDM and hyperglycemia during pregnancy involves lifestyle modifications with or without administration of glucose-lowering medications [16]. Adequate nutrition to promote fetal development and optimal weight gain, decreased simple carbohydrate intake, frequent self-blood glucose monitoring, and regular physical activity are the first-line treatment approach against hyperglycemia during pregnancy and GDM [17]. However, adopting behavioral modifications in a short period of time (even with adequate support) can be challenging [18]. Some patients may also require the administration of glucose-lowering agents to achieve glycemic control. Insulin administration is the primary pharmacological approach for the management of GDM [16]. Although insulin administration is very efficacious in the management of hyperglycemia, it requires carbohydrate counting with each meal to match insulin administration to the carbohydrate intake to achieve glycemic control. Glyburide and metformin have been also approved for the treatment of GDM by the US Food and Drug Administration [16]. However, their use is not recommended as a first-line pharmacological approach for the treatment of GDM, as their metabolites can cross the placenta, and their long-term safety remains to be determined [16]. Considering the limitations of the current modalities for the management of hyperglycemia during pregnancy, further research is needed to establish efficacious and safe approaches to improve glycemic control during pregnancy.

Over the last decade, there has been intense scientific interest to better understand the role of meal timing in metabolic health. Evidence from studies in rodents support that the synchronization of meal timing to the endogenous circadian rhythms regulating the efficiency of mechanisms involved in nutrient metabolism can improve metabolic health [19,20]. Recent findings support that restricting the daily eating window and/or shifting the timing of dietary intake earlier in the day may lead to improved glycemic control and insulin sensitivity in the non-pregnant state [21,22,23,24,25]. Further evidence supports that energy and/or carbohydrate distribution throughout the day and eating frequency may also affect glycemic control [26,27,28]. Therefore, synchronizing food intake to the endogenous timekeeping mechanisms affecting metabolic efficiency could conceivably improve maternal metabolic health and pregnancy outcomes. The purpose of this review is to summarize and critically evaluate the current literature on the interrelationship between meal timing, frequency, 24 h energy, and carbohydrate distribution on glucose homeostasis during pregnancy.

Pregnancy constitutes a state during which numerous physiological adaptations take place to promote fetal development. Glucose availability in the circulation increases, especially in the late second and third trimester to (in principle) ensure adequate fuel supply for the developing fetus [29]. Changes in the secretion of several glucoregulatory hormones (e.g., growth hormone (GH), human chorionic somatomammotropin (hCS), cortisol, glucagon, estrogen, progesterone, melatonin, and prolactin) contribute to the altered glucose homeostasis during pregnancy. However, this physiological response can sometimes lead to chronic hyperglycemia. To accommodate the higher circulating glucose concentration, postprandial insulin secretion also increases (Figure 1) [30]. Insufficient insulin secretion due to β-cell dysfunction and increased insulin resistance leads to hyperglycemia during pregnancy and GDM [31]. The section below summarizes the changes in the circulating levels of the major glucoregulatory hormones during healthy pregnancy and their effect on glucose metabolism. Figure 2 provides an overview of the trends in the 24 h circulating concentrations of the major glucoregulatory hormones in healthy non-pregnant females and during the third trimester of healthy gestation [32,33,34,35,36].

Over the last decade, there has been intense scientific interest in the role of fasting in metabolic health. Short-term fasting without starvation has been associated with improved glucose metabolism in the non-pregnant state [20,25]. Although the mechanisms underlying the metabolic benefits of fasting are not yet fully understood, they are thought to include a switch in substrate utilization (from glucose to lipids) and cellular stress resistance (reviewed in detail in refs. [60,61]). Pregnancy constitutes a distinct physiologic state; thus, results from studies in non-pregnant adults may not directly translate to the pregnant state. The role of fasting duration in glucose homeostasis during pregnancy remains largely unknown, and only a few studies have attempted to address this question.

Ramadan is a religious fasting event that involves abstinence from caloric intake from sunrise to sunset. The authors of a recent prospective observational study reported that Ramadan fasting (≈14 h daytime fasting) during the second trimester of pregnancy was independently associated with lower odds of GDM [62]. Furthermore, participants with a high number of fasting days during Ramadan (21–29 days) experienced lower weight gain (≈0.5 kg) compared to those that did not fast or fasted for 20 days or less. Ramadan fasting was not associated with increased odds for adverse pregnancy and fetal outcomes.

Another recent cross-sectional study in Singapore investigated the role of fasting duration on glycemic control (assessed by an OGTT after an 8–10 h overnight fast) during the end of the second trimester of gestation [63]. Eleven to twelve hours of overnight fasting were independently associated with lower FPG concentrations (≈2 mg/dL) compared to 9.1–10.9 h of overnight fasting. There was no association between overnight fasting duration and the 2 h post 75 g OGTT plasma glucose concentration.

The results of these studies provide preliminary evidence supporting the notion that short-term fasting without starvation may have metabolic benefits on glycemic control during pregnancy. However, the methodological limitations of those investigations (including their observational nature, self-reported data, and lack of comprehensive metabolic testing) underscore the need for further research aiming to better comprehend the effect of fasting on glucose metabolism and overall metabolic health during pregnancy. Considering that fasting beyond 14 h may lead to a state of “accelerated starvation” [64] during pregnancy, prolonged fasting should be likely avoided. Further research is needed to determine what is a safe fasting duration during pregnancy.

Recent evidence in non-pregnant adults supports that meal timing manipulation is a promising lifestyle intervention against obesity and its related metabolic complications (23, 24). However, the role of meal timing in metabolic health during pregnancy remains poorly understood.

Sacks et al. [65] conducted a randomized crossover trial in patients with GDM. The participants were offered test meals either in the morning (07:00) or at night (21:00). The two test meals were closely matched for energy but not for macronutrient composition. Despite its lower carbohydrate content (44 vs. 51%), the night test meal led to a higher postprandial glycemic response at 3 to 9 h compared to the morning meal test. Consistent with these results, Peterson et al. [66] reported that the correlation between carbohydrate intake and the 1 h postprandial glucose concentration was the strongest for dinner followed by lunch and breakfast.

Another more recent study investigated the role of meal timing on metabolic health in pregnant women with or without night eating syndrome (NES) symptoms during the third trimester of gestation [67]. NES is an eating disorder that presents with nocturnal hyperphagia or awakening for food intake, insomnia, and morning anorexia [68]. NES symptoms were assessed using a validated questionnaire. NES was associated with higher fasting plasma insulin concentration and the HOMA-IR (Homeostatic Model Assessment for Insulin Resistance) index (calculated using the following formula: FPG (mmol/L) times fasting serum insulin (mU/L) divided by 22.5). Moreover, a higher NES score was correlated with higher fasting insulin, hemoglobin A1c, and high-density lipoprotein cholesterol.

Taken together, these results suggest that meal timing and specifically eating in the night may affect metabolic health during pregnancy. Future prospective studies involving manipulation of meal timing are needed to determine its role in glucose homeostasis and insulin sensitivity during pregnancy.

Apart from the effect of meal timing and fasting duration on metabolic health, accumulating evidence supports that the distribution of energy and carbohydrate during the day may have important metabolic implications [26,27,69,70,71]. However, the role of energy and carbohydrate distribution throughout the day on metabolic health during pregnancy remains unclear, and only a small number of studies have investigated this relationship.

Chandler-Laney et al. conducted a cross sectional study to investigate the link between late-night energy and carbohydrate intake on glucose tolerance in healthy African American females in the third trimester of pregnancy [72]. Nighttime (20:00–05:59) energy intake was associated with lower dynamic β-cell response assessed by using a 2 h, 75 g OGTT in participants with obesity but not those with normal weight. In a larger cross-sectional study conducted in Singapore in predominantly Asian women during the second trimester of pregnancy, consumption of 50% or more daily energy intake at night (19:00–06:59) was independently associated with higher fasting glucose in lean participants [73] but not in participants with excessive adiposity (body mass index ≥23.0). Additionally, there was no association between postprandial glucose tolerance and daily energy distribution. The discrepancy in the reported results of those studies with regard to the modification effect of adiposity requires further investigation.

To further examine the link between 24 h energy/carbohydrate distribution, Rasmussen et al. performed a randomized crossover trial in normal weight patients with GDM. The participants followed a 4-day diet with high carbohydrate intake in the morning (50% daily energy/carbohydrate in breakfast and morning snack) and 4-day diet with high carbohydrate intake in the evening (50% daily energy energy/carbohydrate in dinner and night snack) [74]. High energy/carbohydrate intake in the morning led to lower FPG (83 vs. 92 mg/dL) compared to high energy and carbohydrate intake in the evening. Although having high energy and carbohydrate intake in the morning also improved the HOMA-IR index of insulin sensitivity, there were no significant differences between the two diets. The improvements in glycemic control with high energy and carbohydrate intake in the morning were also accompanied by an increase in mean glucose excursion and variability. These findings require further investigation as the small differences in the macronutrient intake between the two experimental conditions may confound the reported findings.

Current evidence supports that higher energy and/or carbohydrate intake later in the day may be linked to perturbed glucose homeostasis during pregnancy. Considering the limitations of the currently reported results (including cross-sectional study design or very short-term intervention with differences in total macronutrient composition and small number of participants), further research is needed to better understand the effect of the daily energy and macronutrient distribution in metabolic health during gestation.

The role of meal frequency in metabolic health has been an issue of scientific debate for several decades. Although a number of studies support that eating frequency may play a role in body weight regulation and metabolic health [75,76,77], others do not [78,79,80,81]. The relationship between meal frequency and metabolic health during pregnancy remains poorly understood. Results from a cross-sectional study indicate that the number of daily eating occasions is independently associated with higher 2 h postprandial glucose after 75 g OGTT in normal-weight females in the second trimester of gestation [63]. Eating frequency was not associated with fasting plasma glucose concentrations.

Current evidence (predominantly from observational studies and small short-term clinical investigations—summarized in Table 1) supports that meal timing may affect glycemic control during pregnancy. However, results from observational studies cannot be used to establish causation. Therefore, well-controlled intervention studies including detailed metabolic and other clinical outcomes are needed to comprehensively investigate the role of meal timing, frequency, and 24 h energy and macronutrient distribution in glucose homeostasis and metabolic health particularly in target populations at high risk for the development of metabolic disease. Once the answers to these questions have been clarified, it will be important to understand how this knowledge can be translated into clinical practice to safely and effectively improve maternal and neonatal health outcomes.

GDM and hyperglycemia during pregnancy affect a large percentage of women. In addition to the role of nutrition quantity and quality in metabolic health and pregnancy outcomes, it is also critical to understand the role of meal timing. Overall, the current literature supports that meal timing, frequency, and 24 h energy and macronutrient distribution may play a role in the regulation of metabolic health during gestation. However, important methodological limitations of the prior studies limit their ability to conclusively establish the role of meal timing in glycemic control during pregnancy. Further research is needed to determine the role of meal timing, frequency, daily energy, and macronutrient distribution on maternal and fetal metabolic regulation and outcomes. Future investigations will also help establish safe, efficacious, and equitable chrono-nutrition lifestyle interventions to improve the health of the population and generations to come.