What signs of respiratory distress in the neonate should be reported immediately?

Newborn respiratory distress syndrome (NRDS) happens when a baby's lungs are not fully developed and cannot provide enough oxygen, causing breathing difficulties. It usually affects premature babies.

Índice Show

Treatment before birth
Treatment after the birth
Internal bleeding
Lung scarring
Developmental disabilities
Differential diagnosis
Transient Tachypnea of the Newborn
Respiratory Distress Syndrome
Meconium Aspiration Syndrome
TRANSIENT TACHYPNEA OF THE NEWBORN
RESPIRATORY DISTRESS SYNDROME
MECONIUM ASPIRATION SYNDROME

It's also known as infant respiratory distress syndrome, hyaline membrane disease or surfactant deficiency lung disease.

Despite having a similar name, NRDS is not related to acute respiratory distress syndrome (ARDS).

NRDS usually occurs when the baby's lungs have not produced enough surfactant.

This substance, made up of proteins and fats, helps keep the lungs inflated and prevents them collapsing.

A baby normally begins producing surfactant sometime between weeks 24 and 28 of pregnancy.

Most babies produce enough to breathe normally by week 34.

If your baby is born prematurely, they may not have enough surfactant in their lungs.

Occasionally, NRDS affects babies that are not born prematurely.

For example, when:

the mother has diabetes
the baby is underweight
the baby's lungs have not developed properly

Around half of all babies born between 28 and 32 weeks of pregnancy develop NRDS.

In recent years the number of premature babies born with NRDS has been reduced with the use of steroid injections, which can be given to mothers during premature labour.

The symptoms of NRDS are often noticeable immediately after birth and get worse over the following few days.

They can include:

blue-coloured lips, fingers and toes
rapid, shallow breathing
flaring nostrils
a grunting sound when breathing

If you're not in hospital when you give birth and notice the symptoms of NRDS in your baby, call 999 immediately and ask for an ambulance.

A number of tests can be used to diagnose NRDS and rule out other possible causes.

These include:

a physical examination
blood tests to measure the amount of oxygen in the baby's blood and check for an infection
a pulse oximetry test to measure how much oxygen is in the baby's blood using a sensor attached to their fingertip, ear or toe
a chest X-ray to look for the distinctive cloudy appearance of the lungs in NRDS

The main aim of treatment for NRDS is to help the baby breathe.

Treatment before birth

If you're thought to be at risk of giving birth before week 34 of pregnancy, treatment for NRDS can begin before birth.

You may have a steroid injection before your baby is delivered. A second dose is usually given 24 hours after the first.

The steroids stimulate the development of the baby's lungs. It's estimated that the treatment helps prevent NRDS in a third of premature births.

You may also be offered magnesium sulphate to reduce the risk of developmental problems linked to being born early.

If you take magnesium sulphate for more than 5 to 7 days or several times during your pregnancy, your newborn baby may be offered extra checks. This is because prolonged use of magnesium sulphate in pregnancy has in rare cases been linked to bone problems in newborn babies.

Treatment after the birth

Your baby may be transferred to a ward that provides specialist care for premature babies (a neonatal unit).

If the symptoms are mild, they may only need extra oxygen. It's usually given through an incubator, a small mask over their nose or face or tubes into their nose.

If symptoms are more severe, your baby will be attached to a breathing machine (ventilator) to either support or take over their breathing.

These treatments are often started immediately in the delivery room before transfer to the neonatal unit.

Your baby may also be given a dose of artificial surfactant, usually through a breathing tube.

Evidence suggests early treatment within 2 hours of delivery is more beneficial than if treatment is delayed.

They'll also be given fluids and nutrition through a tube connected to a vein.

Some babies with NRDS only need help with breathing for a few days. But some, usually those born extremely prematurely, may need support for weeks or even months.

Premature babies often have multiple problems that keep them in hospital, but generally they're well enough to go home around their original expected delivery date.

The length of time your baby needs to stay in hospital will depend on how early they were born.

Most babies with NRDS can be successfully treated, although they have a high risk of developing further problems later in life.

Air leaks

Air can sometimes leak out of the baby's lungs and become trapped in their chest cavity. This is known as a pneumothorax.

The pocket of air places extra pressure on the lungs, causing them to collapse and leading to additional breathing problems.

Air leaks can be treated by inserting a tube into the chest to allow the trapped air to escape.

Internal bleeding

Babies with NRDS may have bleeding inside their lungs (pulmonary haemorrhage) and brain (cerebral haemorrhage).

Bleeding into the lungs is treated with air pressure from a ventilator to stop the bleeding and a blood transfusion.

Bleeding into the brain is quite common in premature babies, but most bleeds are mild and do not cause long-term problems.

Lung scarring

Sometimes ventilation (begun within 24 hours of birth) or the surfactant used to treat NRDS causes scarring to the baby's lungs, which affects their development.

This lung scarring is called bronchopulmonary dysplasia (BPD).

Symptoms of BPD include rapid, shallow breathing and shortness of breath.

Babies with severe BPD usually need additional oxygen from tubes into their nose to help with their breathing.

This is usually stopped after a few months, when the lungs have healed.

But children with BPD may need regular medicine, such as bronchodilators, to help widen their airways and make breathing easier.

Developmental disabilities

If the baby's brain is damaged during NRDS, either because of bleeding or a lack of oxygen, it can lead to long-term developmental disabilities, such as learning difficulties, movement problems, impaired hearing and impaired vision.

But these developmental problems are not usually severe. For example, 1 survey estimated that 3 out of 4 children with developmental problems only have a mild disability, which should not stop them leading a normal adult life.

Page last reviewed: 29 March 2021
Next review due: 29 March 2024

Please note that all guidance is currently under review and some may be out of date. We recommend that you also refer to more contemporaneous evidence in the interim.

Respiratory distress syndrome (RDS) is when the neonate has difficulty breathing due to surfactant deficiency at birth. RDS, also known as hyaline membrane disease (HMD), is the dominant clinical problem faced by preterm infants and is directly related to structurally immature and surfactant deficient lungs.

The greatest risk factor is low gestational age and the development of the disease begins with the impaired synthesis of pulmonary surfactant associated with prematurity.

The disease is exacerbated by treatable and preventable factors including:

The diagnosis is made on the basis of the combination of clinical features including:

tachypnoea (generally > 60 breaths per minute in term and > 80 breaths per minute in preterm infants)
nasal flaring
grunting respirations
intercostal retraction
cyanosis
increased oxygen requirement
radiological features.

Figure 1: Intercostal retraction
Photo courtesy of Janele Alby MD

The natural history is for the clinical signs to develop within six hours of life, with progressive worsening over the first 48-72 hours of life followed by recovery.

The condition can be prevented, or the severity reduced, by antenatal administration of betamethasone. The course of the disease is altered by exogenous surfactant therapy and assisted ventilation.

Attention to thermoregulation and oxygenation can decrease the severity of RDS.

The level of experience and expertise dictate what technical procedures (peripheral intravenous (IV) catheter insertion and ETT insertion) are used prior to arrival of the PIPER Neonatal transport team.

Infants requiring greater than 60 per cent oxygen should be managed in a Level 6 Neonatal Unit.

Differential diagnosis

Signs and radiolological appearance of RDS are not specific and other causes of respiratory distress should be considered.

In particular it is difficult to exclude sepsis as a possible diagnosis initially, and antibiotic therapy should be given until blood cultures prove negative.

‘Wet lung’ and lung malformations as well as non-pulmonary causes of respiratory distress are uncommon in the preterm infant but should be excluded using the appropriate tests.

The clinical presentation of respiratory distress in the newborn includes apnea, cyanosis, grunting, inspiratory stridor, nasal flaring, poor feeding, and tachypnea (more than 60 breaths per minute). There may also be retractions in the intercostal, subcostal, or supracostal spaces. Respiratory distress occurs in approximately 7 percent of infants,1 and preparation is crucial for physicians providing neonatal care. Most cases are caused by transient tachypnea of the newborn, respiratory distress syndrome, or meconium aspiration syndrome, but various other causes are possible (Table 1).

Transient Tachypnea of the Newborn

Transient tachypnea of the newborn is the most common cause of neonatal respiratory distress, constituting more than 40 percent of cases.1 A benign condition, it occurs when residual pulmonary fluid remains in fetal lung tissue after delivery. Prostaglandins released after delivery dilate lymphatic vessels to remove lung fluid as pulmonary circulation increases with the first breath. When fluid persists despite these mechanisms, transient tachypnea of the newborn can result. Risk factors include maternal asthma,2 male sex, macrosomia, maternal diabetes,3 and cesarean delivery.4

The clinical presentation includes tachypnea immediately after birth or within two hours, with other predictable signs of respiratory distress. Symptoms can last from a few hours to two days. Chest radiography shows diffuse parenchymal infiltrates, a “wet silhouette” around the heart, or intralobar fluid accumulation5 (Figure 1).

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Respiratory Distress Syndrome

Respiratory distress syndrome of the newborn, also called hyaline membrane disease, is the most common cause of respiratory distress in premature infants, correlating with structural and functional lung immaturity. It occurs in 24,000 infants born in the United States annually.6 It is most common in infants born at fewer than 28 weeks' gestation and affects one third of infants born at 28 to 34 weeks' gestation, but occurs in less than 5 percent of those born after 34 weeks' gestation.6 The condition is more common in boys,7 and the incidence is approximately six times higher in infants whose mothers have diabetes, because of delayed pulmonary maturity despite macrosomia.8

The pathophysiology is complex. Immature type II alveolar cells produce less surfactant, causing an increase in alveolar surface tension and a decrease in compliance. The resultant atelectasis causes pulmonary vascular constriction, hypoperfusion, and lung tissue ischemia. Hyaline membranes form through the combination of sloughed epithelium, protein, and edema. Persistent respiratory distress syndrome leads to bronchopulmonary dysplasia, characterized by typical chest radiography findings and chronic oxygen dependence. The syndrome is associated with recurrent wheezing in children and a higher risk of hospital admission for asthma.9

The diagnosis of respiratory distress syndrome should be suspected when grunting, retractions, or other typical distress symptoms occur in a premature infant immediately after birth. Hypoxia and cyanosis often occur. Chest radiography shows homogenous opaque infiltrates and air bronchograms, indicating contrast in airless lung tissue seen against air-filled bronchi5 (Figure 2); decreased lung volumes also can be detected.

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Meconium Aspiration Syndrome

Meconium-stained amniotic fluid occurs in approximately 15 percent of deliveries, causing meconium aspiration syndrome in the infant in 10 to 15 percent of those cases, typically in term and post-term infants.10 Meconium is composed of desquamated cells, secretions, lanugo, water, bile pigments, pancreatic enzymes, and amniotic fluid. Although sterile, meconium is locally irritative, obstructive, and a medium for bacterial culture. Meconium passage may represent hypoxia or fetal distress in utero. Similar symptoms can occur after aspiration of blood or nonstained amniotic fluid.

Meconium aspiration syndrome causes significant respiratory distress immediately after delivery. Hypoxia occurs because aspiration takes place in utero. Chest radiography shows patchy atelectasis or consolidation5 (Figure 3).

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Bacterial infection is another possible cause of neonatal respiratory distress. Common pathogens include group B streptococci (GBS), Staphylococcus aureus, Streptococcus pneumoniae, and gram-negative enteric rods. Pneumonia and sepsis have various manifestations, including the typical signs of distress as well as temperature instability. Unlike transient tachypnea, respiratory distress syndrome, and meconium aspiration syndrome, bacterial infection takes time to develop, with respiratory consequences occurring hours to days after birth.

Risk factors for pneumonia include prolonged rupture of membranes, prematurity, and maternal fever. Prevention of GBS infection through universal screening and antepartum treatment reduces rates of early-onset disease, including pneumonia and sepsis, by 80 percent.11 Current U.S. protocol mandates screening for GBS in all pregnant patients late in pregnancy and treating those who have positive results with intrapartum antibiotics at least four hours before delivery.12

Chest radiography helps in the diagnosis, with bilateral infiltrates suggesting in utero infection. Pleural effusions are present in two thirds of cases.13 Serial blood cultures may be obtained to later identify an infecting organism.

Pneumothorax, defined as air in the pleural space, can be a cause of neonatal respiratory distress when pressure within the pulmonary space exceeds extrapleural pressure. It can occur spontaneously or as a result of infection, meconium aspiration, lung deformity, or ventilation barotrauma. The incidence of spontaneous pneumothorax is 1 to 2 percent in term births,14 but it increases to about 6 percent in premature births.15

Persistent pulmonary hypertension of the newborn occurs when pulmonary vascular resistance fails to decrease soon after birth as with normal transition. The etiology may be idiopathic or secondary to meconium aspiration syndrome, pneumonia or sepsis, respiratory distress syndrome, or transient tachypnea of the newborn. Maternal use of selective serotonin reup-take inhibitors in the third trimester also has been implicated.16

Certain congenital malformations can lead to respiratory distress; these include pulmonary hypoplasia, congenital emphysema, esophageal atresia, and diaphragmatic hernia. Upper airway obstructions from choanal atresia or vascular rings may cause similar results. Obstructive lesions include choanal atresia, macroglossia, Pierre Robin syndrome, lymphangioma, teratoma, mediastinal masses, cysts, subglottic stenosis, and laryngotracheomalacia. Congenital heart disease also may be implicated. Cyanotic heart disease includes transposition of the great arteries and tetralogy of Fallot. Noncyanotic heart lesions may cause a pulmonary overflow state leading to congestive heart failure. These lesions include large septal defects, patent ductus arteriosus, and coarctation of the aorta. Malformations can sometimes be found on antepartum imaging.

Neurologic disorders such as hydrocephalus and intracranial hemorrhage can cause respiratory distress. Central respiratory depression can occur after maternal exposure to medications, including labor analgesia and illicit drugs.

Metabolic and hematologic derangements (e.g., hypoglycemia, hypocalcemia, polycythemia, anemia) can also cause respiratory symptoms. Inborn errors of metabolism should also be considered.

Finally, a small but significant number of infants do not fit previously described patterns. Delayed transition is diagnosed retrospectively when symptoms resolve within the first few hours of life instead of progressing as respiratory distress syndrome, transient tachypnea of the newborn, or meconium aspiration syndrome. The etiology is most likely a combination of retained fluid and incompletely expanded alveoli. Treatment is supportive until the distress resolves in a few hours as the transition completes.

Treatment for neonatal respiratory distress can be both generalized and disease-specific. Physicians should be aware of current neonatal resuscitation protocols. Oxygenation can be enhanced with blow-by oxygen, nasal cannula, or mechanical ventilation in severe cases. Surfactant administration may be required. Antibiotics are often administered if bacterial infection is suspected clinically or because of leukocytosis, neutropenia, or hypoxemia. Ampicillin and gentamicin are often used together based on their effectiveness and synergy.12 Extracorporeal membrane oxygenation, similar to an artificial external lung, is used as a last resort in critical circumstances. Oral feedings are often withheld if the respiratory rate exceeds 80 breaths per minute.

If pneumothorax occurs, needle decompression or chest tube drainage may be required. Small pneumothoraces can be treated in term infants without invasive management through nitrogen washout. Administration of 100% oxygen can accelerate the resolution of the pneumothorax as readily absorbed oxygen replaces nitrogen in the extrapulmonary space. This technique can reduce pneumothorax duration from two days to eight hours.17

Because evidence in the specific treatment of neonatal respiratory distress continues to evolve, family physicians should work conjointly with neonatal intensivists. If services required for the neonate are unavailable at the family physician's facility, care should be transferred to a higher acuity hospital.

TRANSIENT TACHYPNEA OF THE NEWBORN

Treatment for transient tachypnea of the newborn is supportive because the condition is usually self-limited. Oral furosemide (Lasix) has not been shown to significantly improve status and should not be given.18 Data suggest that prenatal administration of corticosteroids 48 hours before elective cesarean delivery at 37 to 39 weeks' gestation reduces the incidence of transient tachypnea of the newborn; however, this has not become common practice.19

RESPIRATORY DISTRESS SYNDROME

Treatment for respiratory distress syndrome often requires some of the general interventions mentioned. In addition, prenatal administration of corticosteroids between 24 and 34 weeks' gestation reduces the risk of respiratory distress syndrome when the risk of preterm delivery is high, with an odds ratio of 0.53.20 Postnatal corticosteroid administration for respiratory distress syndrome may decrease mortality risk, but it may increase the risk of cerebral palsy.21 Inhaled nitric oxide may alleviate concomitant persistent pulmonary hypertension of the newborn, but its use in preterm infants is experimental.22

MECONIUM ASPIRATION SYNDROME

General treatment practices are often used for meconium aspiration syndrome. Standard prevention and treatment for meconium aspiration syndrome previously included suctioning the mouth and nares upon head delivery before body delivery. However, recent evidence suggests that aspiration occurs in utero, not at delivery; therefore, infant delivery should not be impeded for suctioning.23 After full delivery, the infant should be handed to a neonatal team for evaluation and treatment. Although infants previously have been given intubation and airway suctioning, current evidence favors expectant management unless certain criteria (i.e., spontaneous respiration, heart rate greater than 100 beats per minute, and reasonable tone) are absent (Figure 4).24

Meta-analyses have suggested that amnioinfusion reduces aspiration for thick meconium.25,26 A recent well-designed, randomized, multicenter trial with 1,998 women found that amnioinfusion for meconium (even thick meconium) does not decrease the incidence of meconium aspiration syndrome or perinatal death.27 There is insufficient evidence to recommend steroid administration.28

A detailed history is critical to proper evaluation. The differential diagnosis changes with gestational age: respiratory distress syndrome typically affects preterm infants, whereas meconium aspiration syndrome affects term or post-term neonates. Antepartum infection status is important, especially regarding GBS infection status and prophylaxis. Information about the duration of rupture, color of amniotic fluid, maternal temperature, maternal tachycardia, and fetal heart tracing status is vital to detect meconium aspiration and chorioamnionitis. Family history assists in identifying inheritable congenital defects. The onset and duration of respiratory symptoms also provide clues. Transient tachypnea of the newborn begins early and improves with time. Conversely, sepsis and pneumonia may have no early signs but may develop hours to days later. Respiratory distress syndrome begins early in premature infants without signs of spontaneous improvement.

Physical examination also is helpful. In the general assessment, physicians should look for apnea, tachypnea, or cyanosis. Cardiac auscultation detects murmurs suggestive of congenital heart anomalies. Lung auscultation may show asymmetrical chest movement in pneumothorax or crackles in pneumonia, or be completely clear in transient tachypnea or persistent pulmonary hypertension of the newborn.

The severity of distress should be estimated with an initial assessment. Mild distress may warrant observation and pulse oximetry. Severe distress, especially with a complicated birth history, requires immediate resuscitation, chest radiography, and laboratory tests. Newborns commonly demonstrate signs of respiratory compromise much earlier than cardiovascular collapse. The variation of neonatal distress makes application of a general algorithm difficult, although a “rule of two hours” for continuous reassessment has been suggested (Figure 5).29 During this time, chest radiography and blood tests can be performed (Table 2), and possible consultation or patient transfer can be implemented. This reassessment allows physicians to reevaluate symptom severity as well as to update and educate the parents.

The distinguishing features of transient tachypnea of the newborn, respiratory distress syndrome, and meconium aspiration syndrome are summarized in Table 3.2–8,19,20,23,27