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Diabetes mellitus (DM) in pregnancy consists of gestational diabetes mellitus (GDM) and pregestational diabetes mellitus. GDM is an abnormal glucose tolerance that develops during pregnancy, while pregestational diabetes mellitus is DM that is present before conception. Both conditions are associated with an increased risk for maternal and fetal complications. Individuals with pregestational DM may have clinical features of DM, whereas individuals with GDM are usually asymptomatic. Early detection and management of diabetes in pregnancy is essential to reduce complications. Screening for GDM is recommended for all individuals at 24–28 weeks' gestation; high-risk individuals should be additionally screened at the initial prenatal visit for undiagnosed pregestational diabetes. Management of diabetes in pregnancy usually involves a multidisciplinary team including endocrinology, maternal-fetal medicine, and dietitians. If medication is required, insulin is recommended. Patients require careful monitoring; antepartum fetal surveillance is usually recommended from 32 weeks' gestation because of the high rate of fetal complications. GDM usually resolves after delivery, and patients with GDM should be assessed for resolution at 4–12 weeks postpartum. Patients with GDM are at elevated lifetime risk of diabetes mellitus and require ongoing screening for diabetes every 1–3 years.

Overview of diabetes in pregnancy
Features	Gestational diabetes mellitus [1][2]	Pregestational diabetes mellitus [3]
Definition	Abnormal glucose tolerance diagnosed during pregnancy May be able to be controlled by diet alone (class A1GDM) or may need medication (class A2GDM) Associated with an increased risk of maternal and fetal morbidity	T1DM or T2DM diagnosed prior to pregnancy Associated with a significantly increased risk for maternal complications during pregnancy and delivery, and congenital abnormalities
Epidemiology	5–9% of pregnancies [1] Usually in the second and third trimesters	1% of pregnancies
Pathophysiology	Insulin requirements vary during pregnancy. First trimester: insulin sensitivity increases; risk of hypoglycemia Second and third trimesters: Hormonal changes trigger progressive insulin resistance that results in hyperglycemia, particularly after mealtimes.
Risk factors	Risk factors for T2DM Obstetric Gestational diabetes in a previous pregnancy Recurrent pregnancy loss At least one birth of a child diagnosed with fetal macrosomia	See “Etiology of DM.”
Clinical features	Usually asymptomatic May present with edema; warning signs include polyhydramnios or large-for-gestational age infants (> 90th percentile)	See “Clinical features of diabetes mellitus.”
Screening and diagnosis [3]	Screening for GDM at 24–28 weeks' gestation for all individuals without pregestational diabetes	Screen high risk individuals for undiagnosed pregestational diabetes in the first trimester. Screen for complications of DM. See also “Management of high-risk pregnancies.”
Treatment	Prenatal patient education (e.g., on nutrition, physical activity) Strict glycemic control during pregnancy with: Diet [3][4] Medication (usually insulin) [3][4] Regular monitoring of fetal growth and wellbeing (e.g., ultrasound, antepartum fetal surveillance) Delivery planning, e.g.: [3][4] Early delivery if glycemic control is poor or complications occur Cesarean delivery if estimated fetus weight > 4500 g Tight control of blood glucose during delivery (e.g., insulin infusion) [3]
Complications	Maternal complications of diabetes in pregnancy include hypertensive pregnancy disorders, UTI, and birth complications. Fetal and neonatal complications of DM in pregnancy include diabetic embryopathy and diabetic fetopathy.
Prognosis [4]	In most cases, GDM resolves after pregnancy. Increased risk of developing T2DM (∼50% over 10 years) Screen for DM4–12 weeks postpartum (one-step OGTT) Repeat every 1–3 years Increased risk of gestational diabetes recurring in subsequent pregnancies (∼ 50%)	As for other forms of diabetes mellitus

Screening for undiagnosed pregestational diabetes [5][6]

Indications: any preexisting indication for diabetes screening
Modality: Perform either of the following at the initial prenatal visit (see “Interpretation of hyperglycemia studies” for results).
- HbA1c testing (before 15 weeks' gestation only)
- Fasting blood glucose
Follow-up
- Screen positive: Manage as pregestational diabetes.
- Screen negative: Perform routine screening for GDM.

HbA1c is not reliable after 15 weeks' gestation because of rapid red blood cell turnover in pregnancy. [6]

Screening for GDM [5][7][8]

Indications: all individuals without pregestational diabetes
Modality: OGTT at 24–28 weeks' gestation (see “Diagnosis of GDM” for details)
Follow-up
- Screen positive: Manage as GDM.
- Screen negative: No further testing is necessary unless clinical features of DM develop.

Perform diagnostics for any individual with clinical features of DM. Diagnostic studies are otherwise performed as part of routine screening for diabetes in pregnancy.

Diagnosis of pregestational diabetes

See “Diagnosis of diabetes mellitus.”

Diagnosis of GDM

Modality: either two-step OGTT (preferred) or one-step OGTT [5][6]
Interpretation of results [4][6]
- One-step OGTT: GDM is confirmed if any of the following values are obtained.
  - Fasting glucose ≥ 92 mg/dL
  - 1-hour glucose ≥ 180 mg/dL
  - 2-hour glucose ≥ 153 mg/dL
- Two-step OGTT: GDM is confirmed if ≥ 2 of the following values are obtained. [6]
  - Fasting glucose ≥ 95 mg/dL
  - 1-hour glucose ≥ 180 mg/dL
  - 2-hour glucose ≥ 155 mg/dL
  - 3-hour glucose ≥ 140 mg/dL

Most pregnant individuals with diabetes are referred to specialists (e.g., endocrinology, maternal-fetal medicine) for management.

Prenatal care

All patients [9][10]

Initiate routine prenatal care.
Offer supportive services (e.g., social work, diabetes education).
Address coexisting conditions related to diabetes (e.g., obesity, hypertensive pregnancy disorders, ASCVD).
Discuss glycemic control in pregnancy. [3]
Initiate antepartum fetal surveillance based on risk factors. [3][4]
- Pregestational DM or GDM that is poorly controlled or needs medication: Usually from 32 weeks' gestation
- Well-controlled diet-controlled GDM: Fetal surveillance may not be required, follow local guidance.

Patients with pregestational diabetes [3]

Obtain the following at the first prenatal visit:
- HbA1c
- Thyroid function tests
- ECG
- Diabetic retinopathy screen [4][9]
- 24 hour urine profile (if no baseline)
Adjust medications as necessary (see “Antihyperglycemic treatment in pregnancy” and “Pharmacotherapy during pregnancy”). [3][9]
Educate on the increased risk of diabetic ketoacidosis and hypoglycemia during pregnancy. [3]
- Advise patients to check urinary ketones if glucose levels exceed 200 mg/dL.
- Discuss hypoglycemia management; ensure patients carry glucose tablets and glucagon.
Screen for hypertensive pregnancy disorders; start aspirin prophylaxis against preeclampsia at 12–16 weeks. [3][9]

Patients with GDM [4]

Advise that most individuals can control GDM with diet and exercise. [4][9]
- Refer to a dietitian to plan meals and snacks.
- Recommend 30 minutes of moderate-intensity exercise at least 5 days a week.
Review glycemic control and start antihyperglycemic treatment in pregnancy if lifestyle changes alone are insufficient. [11]

Good glycemic control during pregnancy reduces the risk of maternal and fetal complications. [3]

Peripartum management [3][4]

Timing of delivery [3][4]
- Well-controlled DM: at 39 weeks' gestation [4]
- Poorly controlled DM, previous stillbirth, or existing complications of diabetes : 37–38 weeks' gestation
Mode of delivery [3]
- Usually vaginal
- Consider cesarean delivery if estimated fetal weight is ≥ 4500 g.
Medication management
- Insulin management during delivery [3]
  - Patients on insulin are usually maintained on long-acting insulin and started on an insulin infusion for delivery
  - Blood glucose is checked hourly; target serum glucose is < 110 mg/dL.
- After delivery
  - Patients with pregestational diabetes: Reduce insulin doses immediately after delivery to one-third to one-half of previous levels. [3]
  - Patients with GDM: Stop antihyperglycemic medication immediately after delivery. [9]

Delivery is recommended at a facility able to manage peripartum insulin delivery and common complications (e.g., shoulder dystocia, neonatal hypoglycemia). [3][4]

Postpartum care

All patients [3][4]

Initiate standard postpartum care including postpartum contraception for all patients.
Encourage breastfeeding. [10]
Offer lifestyle recommendations for patients with diabetes mellitus.

Patients with pregestational diabetes [3]

Discuss glycemic control with breastfeeding. [3]
Advise individuals that erratic sleep and eating and reduced insulin requirements increase the risk of hypoglycemia. [9]
Continue standard diabetes management.

Patients with GDM [4]

Assess for resolution of GDM at 4–12 weeks' postpartum using the one-step OGTT. [4][9][10]
Further management depends on the results. [4][9]
- Normal level: Screen for diabetes every 1–3 years. [9]
- Impaired glucose tolerance
  - Advise weight loss and exercise.
  - Consider metformin.
  - Screen for diabetes yearly.
- Positive diabetes screen: Initiate diabetes management.

A history of GDM increases the risk of developing T2DM. Advise patients to plan for future pregnancies by optimizing weight, nutrition, and glucose control before conception. [9]

Advise patients that near physiologic glucose control decreases the risk of complications of diabetes in pregnancy. [3]

Monitoring

Monitor HbA1c monthly. [9][12]
Review home glucose monitoring records. [3][4][9]
- ≤ 24 weeks' gestation: every 1–2 weeks
- > 24 weeks' gestation: weekly

Glycemic targets during pregnancy [3][9]
	Thresholds
HbA1c	< 6%
Fasting glucose [4]	70–95 mg/dL
Postprandial glucose [4]	1 hour: 110–140 mg/dL 2 hour: 100–120 mg/dL

Hypoglycemia thresholds vary, but blood glucose levels < 70 mg/dL are generally considered too low. [9]

Antihyperglycemic treatment in pregnancy

Medication is usually started by a specialist.
Insulin is recommended for all patients requiring medication to control diabetes during pregnancy. [3][4][9]
- Use a multiple dose regimen of rapid or short-acting insulin and intermediate or long-acting insulin. [3][4]
  - Pregestational diabetes: Starting dose depends on the trimester. [3]
  - Gestational diabetes: starting dose 0.7–1.0 units/kg/day [3]
- Tailor insulin doses; requirements: [3]
  - May decrease in the first trimester
  - Increase in the second and third trimester
  - Typically increase if antenatal corticosteroids for fetal maturation are used [3]
For patients unwilling or unable to take insulin, oral antidiabetic medications can be used off-label.
- Options: metformin (preferred), glyburide [3][4][9]
- Use shared decision-making. [4]

Pregestational diabetes poses a greater risk of complications than gestational diabetes. Complications during the first trimester are more common in pregestational diabetes, while complications during the second and third trimesters are equally associated with pregestational and gestational diabetes. [13]

We list the most important complications. The selection is not exhaustive.

Hypertensive pregnancy disorders
Urinary tract infection in pregnancy [14]
Spontaneous abortion
Worsening of complications of DM (e.g., diabetic retinopathy)
Hypoglycemia
Hyperglycemic crises
Preterm labor
Polyhydramnios
Postpartum hemorrhage [15]
Need for cesarean delivery
Increased long-term risk of developing T2DM

Diabetic embryopathy

Definition: any anomaly in an embryo associated with maternal diabetes, typically developing during the main embryonic period
Onset: first trimester
Pathophysiology: hyperglycemia → inhibition of myo-inositol uptake → abnormalities in the arachidonic acid-prostaglandin pathway → congenital anomalies and early pregnancy loss [13]

Manifestations of diabetic embryopathy [13]

Early pregnancy loss and perinatal death
Cardiovascular defects: congenital heart disease
- Transposition of the great vessels
- Ventricular septal defect
- Truncus arteriosus
- Coarctation of the aorta
- Patent ductus arteriosus
Central nervous system defects: neural tube defects
- Anencephaly
- Spina bifida
- Myelomeningocele
Genitourinary defects
- Renal agenesis
- Ureteral duplication
- Hydronephrosis
Skeletal defects
- Caudal regression syndrome: a congenital condition characterized by the partial or complete absence of the sacrum and often of the lower lumbar spine
  - Pathophysiology: The cause of caudal regression syndrome is unknown.
  - Maternal diabetes is a known risk factor.
  - Clinical features: based on the level of the spinal lesion and disease severity
    - Lower limb deformities or foot deformities (e.g., club foot)
    - Anorectal malformations
    - Aplasia or hypoplasia of the sacrum and/or lumbosacral spine
    - Mild to severe motor function impairment and paralysis
    - Flat buttocks and shallow gluteal clefts
    - Bowel and bladder dysfunction (e.g., neurogenic bladder, bladder incontinence)
  - May occur as part of other caudal syndromes (e.g., VACTERL, OEIS syndrome)
- Vertebral anomalies (e.g., hemivertebrae)
Gastrointestinal defects
- Small left colon syndrome: an abrupt decrease in intestinal diameter characterized by transient intestinal obstruction due to inability to pass meconium
- Duodenal atresia
- Anorectal malformation
Other: cleft palate

Diabetic fetopathy

Definition: any anomaly in a fetus associated with maternal diabetes, caused by fetal hyperinsulinemia during gestation
Onset: second and third trimesters
Pathophysiology: maternal hyperglycemia → fetal hyperglycemia → stimulation of fetal pancreas → fetal hyperinsulinemia → ↑ metabolic rate, oxygen consumption, and fetal hypoxemia → metabolic, respiratory, and cardiovascular complications

Manifestations of diabetic fetopathy [13]

Growth defect: : fetal macrosomia
Metabolic defects
- Neonatal hypoglycemia: maternal hyperglycemia → fetal hyperglycemia → beta cellhypertrophy and hyperfunctioning → fetal and neonatal hyperinsulinemia → transient hypoglycemia after birth (when maternal glucose supply stops)
- Neonatal polycythemia: maternal hyperglycemia → chronic fetal hyperglycemia → ↑ metabolic effects and oxygen demand → fetal hypoxemia → ↑ erythropoietin concentrations→ ↑ erythrocyte count
- Neonatal hypocalcemia and neonatal hypomagnesemia: maternal hyperglycemia → abnormal maternal calcium-phosphorus metabolism → ↑ maternal urinary Mg excretion → maternal hypomagnesemia → fetal hypomagnesemia → impaired PTH synthesis in the fetus → fetal hypocalcemia and hypomagnesemia
Respiratory defects
- Acute respiratory distress syndrome
- Transient tachypnea of the newborn
- Perinatal asphyxia
Cardiovascular defects: transient hypertrophic cardiomyopathy
- Definition: thickening of one or both of the ventricular walls and the interventricular septum
- Clinical features: often asymptomatic in infants but may manifest with symptoms of heart failure (e.g., tachypnea, poor feeding, irritability)
- Pathophysiology: maternal hyperglycemia → fetal hyperglycemia → fetal hyperinsulinemia → ↑ fat and glycogen in fetal myocardial cells → thickening of ventricular walls and the intraventricular septum in utero → ↓ ventricular size → left ventricular outflow obstruction and systolic and diastolic cardiac dysfunction
- Diagnostics: echocardiography showing thickened ventricular walls and interventricular septum
- Management: supportive care(e.g., intravenous fluids, beta blockers) for symptomatic infants
- Prognosis: Symptoms typically resolve as plasma insulin normalizes.

As part of routine preconception care: [10]
- Advise patients on weight management, diet, and exercise.
- Test individuals with indications for diabetes screening.
In the first trimester: Recommend a healthy diet and regular exercise (see “Prenatal patient education”) to reduce the risk of GDM. [9]