Clinical Review

Fetal macrosomia: 3 management dilemmas

OBG Manag. 2003 December;15(12):28-36

This condition—and its most-feared complication—is impossible to predict with accuracy. What’s more, there is no evidence supporting a specific intervention. So, what is the best approach? Dr. Resnik offers practical observations.

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References

1. Chauhan SP, Hendrix NW, Magann EF, et al. Limitations of clinical and sonographic estimates of birthweight: experience with 1034 parturients. Obstet Gynecol. 1998;91:72-77.

2. Gonen R, Spiegel D, Abend M. Is macrosomia predictable, and are shoulder dystocia and birth trauma preventable? Obstet Gynecol. 1996;88:526-529.

3. Benacerraf BR, Gelman R, Frigoletto FD, Jr. Sonographically estimated fetal weights: accuracy and limitation. Am J Obstet Gynecol. 1988;159:1118-1121.

4. Larsen CE, Serdula MK, Sullivan KM. Macrosomia: influence of maternal overweight among the low income population. Am J Obstet Gynecol. 1990;162:490-494.

5. Schwartz R, Gruppuso PA, Petzold K, et al. Hyperinsulinemia and macrosomia in the fetus of the diabetic mother. Diabetes Care. 1994;17:640-648.

6. Hoegsberg B, Gruppuso PA, Coustan DR. Hyperinsulinemia and macrosomic infants of non-diabetic mothers. Diabetes Care. 1993;16:32-36.

7. Jaksic J, Mikulandr AF, Perisa M, et al. Effective insulin and insulin-like growth factor I on fetal macrosomia in healthy women. Coll Anthropol. 2001;25:535-543.

8. Menticoglou SM, Manning FA, Morrison I, et al. Must macrosomic fetuses be delivered by a cesarean section? A review of outcome for 786 babies >4500 g. Aust N Z J Obstet Gynaecol. 1992;32:100-103.

9. Nesbitt TS, Gilbert WM, Herrchen B. Shoulder dystocia and associated risk factors with macrosomic infants born in California. Am J Obstet Gynecol. 1998;179:476-480.

10. Baskett TF, Allen AC. Perinatal implications of shoulder dystocia. Obstet Gynecol. 1995;86:14-17.

11. Keller JD, Lopez-Zeno JA, Dooly SL, et al. Shoulder dystocia and birth trauma in gestational diabetes: a five-year experience. Am J Obstet Gynecol. 1991;165:928-930.

12. Bryant DR, Leonardi MR, Landwehr JB, et al. Limited usefulness of fetal weight in predicting neonatal brachial plexus injury. Am J Obstet Gynecol. 1998;179(3 pt 1):686-689.

13. Weeks JW, Pitman T, Spinnato JA. 2nd Fetal macrosomia: does antenatal prediction affect delivery route and birth outcome? Am J Obstet Gynecol. 1995;173:1215-1219.

14. Kolderup LB, Laros Jr RK, Musci TJ. Incidence of persistent birth injury in macrosomic infants: association with mode of delivery. Am J Obstet Gynecol. 1997;177:37-41.

15. Gonen O, Rosen DJD, Dolfin Z. Induction of labor versus expectant management in macrosomia: a randomized study. Obstet Gynecol. 1997;89:913-917.

16. American College of Obstetricians and Gynecologists. ACOG Practice Bulletin #22: Fetal Macrosomia. Washington, DC: ACOG; 2000.

17. American College of Obstetricians and Gynecologists. ACOG Practice Bulletin #40: Shoulder Dystocia. Washington, DC: ACOG; 2002.

18. Alexander GR, Himes JH, Kaufman RB, et al. A United States national reference for fetal growth. Obstet Gynecol. 1996;87:163-168.

19. Boulet SL, Alexander GR, Salihu HM, et al. Macrosomic births in the United States—determinants, outcomes, and proposed grades of risk. Am J Obstet Gynecol. 2003;188:1372-1378.

KEY POINTS

Women with borderline glucose tolerance, as well as those with normal glucose tolerance but mildly hyperinsulinemic fetuses, are at risk of delivering macrosomic infants.
Maternal risk factors include obesity, excessive weight gain, and a history of delivering a macrosomic infant.
The precision of ultrasound measurements declines as fetal weight increases.
Estimating birth weight does not accurately predict the risk of brachial plexus injury.
Neither routine cesarean delivery nor induction of labor is appropriate routine management for suspected macrosomia.

Every clinician would like to avoid vaginal delivery of a macrosomic infant and the attendant potential for shoulder dystocia and permanent brachial plexus injury. Unfortunately, research findings offer little specific guidance, and we continue to wrestle with these dilemmas:

We cannot accurately identify which fetuses are macrosomic.
We cannot accurately predict serious morbidity in these fetuses.
Evidence does not support a policy of avoiding vaginal delivery for all macrosomic fetuses.

Patient care is thus based on estimating the likelihood of macrosomia and its complications, evaluating the risks and benefits of cesarean versus vaginal delivery in each woman, and being prepared for optimal labor management.

Dilemma 1How to identify a macrosomic fetus?

Ultrasound measurements are reasonably accurate for estimating the weights of smaller fetuses, but precision drops off as fetal weight increases. Studies using abdominal palpation and fundal height to estimate the risk of macrosomia report sensitivities of 10% to 43% and positive predictive values of 28% to 53%.^1,2

One investigation with results typical of other studies found that when birth weight exceeded 4,500 g, only 50% of fetuses weighed within 10% of the ultrasound estimate.³ Both clinical and ultrasound estimates either overestimate or underestimate birth weight to such a degree as to limit their clinical utility.

Maternal factors increase the risk of macrosomia (TABLE 1).

Obese women are more likely to have large infants than women with normal body mass.⁴
Excessive weight gain during pregnancy has been shown to increase risk of accelerated fetal growth.
History of macrosomia is another leading risk factor for a large birth-weight infant.
Maternal glucose intolerance is an established risk factor: Fetal growth is accelerated in women with poorly controlled type 1 or 2 diabetes mellitus. Less widely known is the fact that women with borderline glucose tolerance, as well as those with normal glucose tolerance but mildly hyperinsulinemic fetuses, have an increased risk of delivering macrosomic infants.

A study comparing pregnant women with and without insulin-dependent diabetes found that neonatal macrosomia was best correlated with umbilical total insulin, free insulin, and C-peptide levels.⁵

Fetal hyperinsulinemia. Many other studies corroborate the notion that fetal hyperinsulinemia is a major influence on excessive fetal growth. For example, Hoegsberg et al⁶ found that cord-blood plasma insulin levels in macrosomic newborns were twice those of normosomic infants (all neonates were of nondiabetic mothers). Another study comparing 207 macrosomic infants with 200 controls demonstrated that the macrosomic infants had higher levels of plasma insulin and insulin-like growth factor-1.⁷

TABLE 1

Risk factors for fetal macrosomia

MATERNAL
Excess weight
Excessive weight gain during pregnancy
History of macrosomia
Maternal glucose intolerance or borderline tolerance
Multiparity
Postterm gestation
FETAL
Hyperinsulinemia

Dilemma 2How likely is serious morbidity?

Fetal macrosomia poses a threat to mother and newborn alike. Once fetal birth weight exceeds the 90th percentile, maternal morbidity increases linearly. Not surprisingly, labor abnormalities are more common and, when birth weights exceed 4,500 g, cesarean delivery rates for laboring women double.⁸ Vaginal and perineal lacerations and postpartum hemorrhage are also more common following vaginal delivery of a large fetus compared with a newborn of normal size.

Predicting risk of shoulder dystocia. What worries the obstetrician most, however, is the potential for shoulder dystocia and permanent brachial plexus injury. Nesbitt et al⁹ examined nearly 176,000 vaginal births of infants weighing more than 3,500 g, all occurring in 1 year in California, and found risk factors for shoulder dystocia included maternal diabetes, increased birth weight, and assisted delivery (FIGURE). Some specifics:

In unassisted births not complicated by diabetes, the rate of shoulder dystocia was 5.2% for infants weighing 4,000 to 4,250 g; this rate rose to 9.1% for newborns weighing 4,250 to 4,500 g and jumped to 21.1% for those weighing 4,750 to 5,000 g.
In diabetic mothers, the risk of shoulder dystocia in unassisted births was 8.4% at birth weights from 4,000 to 4,250 g, rising to 23.5% at 4,750 to 5,000 g.
When delivery included use of forceps or vacuum, the incidence of shoulder dystocia rose by about 35% to 45% in nondiabetic mothers.

Of course, it must be noted that numerous cases of shoulder dystocia develop in fetuses weighing less than 4,000 g (TABLE 2).