DEFINITION AND INCIDENCE

Preterm birth is usually defined as one occurring after 20 weeks and before 37 completed weeks of gestation. Labor that occurs between these gestational ages is defined as preterm labor. Internationally, the lower boundary defining preterm birth varies between 20 and 24 weeks.

Preterm births in the United States have increased from 9.8% in 1981 to 12.7% in 2005. Between 1988 and 2004, the mortality rate for white infants declined by 55% to 5.7 infant deaths per 1000 live births, and the mortality rate for black infants declined by 45% to 13.6. In the past 10 years, the decline in infant mortality for both races has been less than anticipated. Because prematurity is the leading cause of infant mortality, the prevention of prematurity has become a high priority.

The estimated causes of preterm birth are listed in Table 12-1. Private patients have a much higher proportion of spontaneous preterm labor, whereas black patients in public institutions have a higher proportion of deliveries due to PPROM.

TABLE 12-1 ETIOLOGY OF PRETERM BIRTH

Cause	Estimated Percentage of Preterm Births
Spontaneous preterm labor	35-37
Multiple pregnancies^∗	12-15
Preterm premature rupture of membranes (PPROM)	12-15
Pregnancy-associated hypertension	12-14
Cervical incompetence or uterine anomalies	12-14
Antepartum hemorrhage	5-6
Intrauterine growth restriction (IUGR)	4-6

∗ Increasing proportion due to advancing maternal age and assisted reproductive technologies (ART).

Attempts have been made to define further the spontaneous preterm labor subgroup. Some experts now believe this may be caused by undiagnosed conditions of placental, infectious, immunologic, uterine, or cervical origin. Recently, genetic thrombophilias have been shown to account for a significant proportion of the uteroplacental problems leading to intrauterine growth restriction (IUGR) and preeclampsia, the two major reasons for the early induction of labor to avoid fetal death. In the past 10 years, closer surveillance of high-risk pregnancies has led to earlier delivery and an increase in late preterm deliveries (between 34 and 37 weeks), a major contribution to the increasing preterm birth rate.

Another reason for the increasing incidence of preterm birth is that more women are postponing childbirth as a lifestyle choice. This is associated with a greater risk for infertility and therefore greater use of assisted reproductive technologies (ART), which are associated with multiple gestations and increased risk for preterm birth. A variety of socioeconomic, psychosocial, and medical conditions have been found to carry an increased risk for preterm delivery in these women who postpone childbearing.

Socioeconomic Factors

In the United States, the incidence of preterm deliveries in the black population is twice as high as that in the white population. This factor cannot be viewed as a single entity but probably encompasses other characteristics of the population, such as poor access to and procurement of antenatal care, high stress levels, poor nutritional status, and the possibility of genetic differences.

Medical and Obstetric Factors

When one preterm birth has occurred, the relative risk for preterm delivery in the next pregnancy is 3.9, and the risk increases to 6.5 with two previous preterm deliveries.

Second-trimester abortions seem to carry an increased risk for subsequent preterm delivery, especially if a previous preterm birth has also occurred. The risk associated with induced first-trimester abortions is controversial. Repeated spontaneous first-trimester abortions, however, do increase the risk.

Other medical and obstetrical factors include bleeding in the first trimester, urinary tract infections, multiple gestation, uterine anomalies, polyhydramnios, and incompetent cervix.

Recently, attention has been directed toward maternal employment, physical activity, nutritional status, genital tract infections, stress, and anxiety as major risk factors for preterm birth.

PREVENTION

“Group education” has been shown to decrease preterm birth. All at-risk patients, together with a healthcare provider, should discuss how to adjust personal behaviors and lifestyles to decrease the risk.

Four potential pathways leading to preterm delivery have been identified:

1. Infection (cervical)

2. Placental-vascular

3. Psychosocial stress and work strain (fatigue)

4. Uterine stretch (multiple gestations)

DIAGNOSIS

The diagnosis of preterm labor occurring between 20 and 37 weeks is based on the following criteria in patients with ruptured or intact membranes: (1) documented uterine contractions (four per 20 minutes) and (2) documented cervical change (cervical effacement of 80% or cervical dilation of 2 cm or more). Uterine contractions are not a good predictor of preterm labor, but cervical changes are.

MANAGEMENT

Provided that membranes are not ruptured and there is no contraindication to a vaginal examination (e.g., placenta previa), an initial assessment must be done to ascertain cervical length and dilation and the station and nature of the presenting part. The patient should also be evaluated for the presence of any underlying correctable problem, such as a urinary tract or vaginal infection. She should be placed in the lateral decubitus position (taking the weight of the uterus off the great vessels and improving blood flow to the uterus), monitored for the presence and frequency of uterine activity, and reexamined for evidence of cervical change after an appropriate interval, unless she already meets the preceding criteria for preterm labor. During the period of observation, either oral or parenteral hydration should be initiated.

With adequate hydration and bed rest, uterine contractions cease in about 20% of patients. These patients, however, remain at high risk for recurrent preterm labor.

Because of the role of cervical colonization and vaginal infection in the etiology of preterm labor and premature rupture of membranes, cultures should be taken for group B streptococcus. Other organisms that may be important are Ureaplasma, Mycoplasma, and Gardnerella vaginalis. The latter is associated with bacterial vaginosis, a diagnosis that can be made by the presence of three of four clinical signs (vaginal pH > 4.5, amine odor after addition of 10% potassium hydroxide [KOH], and presence of clue cells or milky discharge).

Antibiotics should be administered to patients who are in preterm labor. For patients who are not allergic to penicillin, a 7-day course of ampicillin, erythromycin, or both can be given. Those allergic to penicillin can be given clindamycin.

Once the diagnosis of preterm labor has been made, the following laboratory tests should be obtained: complete blood cell count, random blood glucose level, serum electrolyte levels, urinalysis, and urine culture and sensitivity. An ultrasonic examination of the fetus should be performed to assess fetal weight, document presentation, assess cervical length, and rule out the presence of any accompanying congenital malformation. The test may also detect an underlying etiologic factor, such as twins or a uterine anomaly.

If the patient does not respond to bed rest and hydration, tocolytic therapy is instituted, provided there are no contraindications. Measures implemented at 28 weeks should be more aggressive than those initiated at 35 weeks. Similarly, a patient with advanced cervical dilation on admission requires more aggressive management than one whose cervix is closed and minimally effaced.

UTERINE TOCOLYTIC THERAPY

It is assumed that physiologic events leading to the initiation of labor also occur in preterm labor. The pharmacologic agents presently being used all seem to inhibit the availability of calcium ions, but they may also exert a number of other effects. The agents currently used and their dosages are presented in Box 12-1.

BOX 12-1 Uterine Tocolytic Agents

Prostaglandin Synthetase Inhibitors

Short-term use only

Magnesium Sulfate

In the United States, magnesium sulfate is frequently the drug of choice for initiating tocolytic therapy. Magnesium acts at the cellular level by competing with calcium for entry into the cell at the time of depolarization. Successful competition results in an effective decrease of intracellular calcium ions, resulting in myometrial relaxation.

Although magnesium levels required for tocolysis have not been critically evaluated, it appears that the levels needed may be higher than those required for prevention of eclampsia. Levels from 5.5 to 7.0 mg/dL appear to be appropriate. These can be achieved using the dosage regimen outlined in Box 12-1. After the loading dose is given, a continuous infusion is maintained, and plasma levels should be determined until therapeutic levels are reached. The drug should be continued at therapeutic levels until contractions cease unless the labor progresses. Because magnesium is excreted by the kidneys, adjustments must be made in patients with an abnormal creatinine clearance. Once successful tocolysis has been achieved, the infusion is continued for at least 12 hours, and then the infusion rate is weaned over 2 to 4 hours and then discontinued. In high-risk patients (advanced cervical dilation or continued labor in very-low-birth-weight cases), the infusion can be continued until the fetus has been exposed to glucocorticoids to enhance lung maturity.

A common minor side effect of magnesium therapy is a feeling of warmth and flushing on first administration. Respiratory depression is seen at magnesium levels of 12 to 15 mg/dL, and cardiac conduction defects and arrest are seen at higher levels.

In the fetus, plasma magnesium levels approach those of the mother, and a low plasma calcium level may also be demonstrated. The neonate may show some loss of muscle tone and drowsiness, resulting in a lower Apgar score. These effects are prolonged in the preterm neonate because of the decrease in renal clearance.

Long-term parenteral magnesium therapy has been used for control of preterm labor in selected patients. An important side effect seems to be loss of calcium, and it may be important in such patients to institute calcium therapy on a prophylactic basis.