Neonatal and Newborn

Published on 08/04/2017 by admin

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 http://evolve.elsevier.com/McCuistion/pharmacology

This chapter focuses on drugs commonly administered to the neonate, which includes late preterm newborns immediately after delivery.
As discussed in Chapter 49, A thorough medical history, such as acquired immunodeficiency syndrome (AIDS), Group B streptococcal infection, and viral hepatitis B or hepatitis C should be conducted. Labor is determined to be preterm if it commences before 37 weeks of pregnancy. If there are no contraindications to halting preterm labor, tocolytic therapy is administered to delay birth (see Chapter 49 for more information on pregnancy and preterm labor drugs). However, when preterm labor is not arrested, premature delivery of the neonate occurs, which puts the newborn at risk for health problems. Premature neonates are at risk for respiratory distress, hypothermia, hypoglycemia, and hyperbilirubinemia, and they may have feeding difficulties.

Drug Administered to Preterm Neonates

Synthetic Surfactant

Respiratory distress syndrome (RDS) can occur because of immature lung development and breathing control and decreased airway muscle tone and surfactant level. Surfactant, a lipoprotein, is necessary to decrease the surface tension of the alveoli (air sacs) to allow the lungs to fill with air and prevent the alveoli from deflating. Immature lungs have lower than normal levels of surfactant; the more premature the neonate is, the higher the chance of RDS. One approach used to minimize respiratory difficulties in the preterm neonate is surfactant replacement. Supplementing the amount of endogenous surfactant available to maintain distension of the alveolar sacs is the focus of this therapy.
The U.S. Food and Drug Administration (FDA) has approved the use of beractant, calfactant, and poractant alfa. Beractant intratracheal suspension, a natural bovine lung extract, contains phospholipids, neutral lipids, fatty acids, and surfactant-associated proteins to which colfosceril palmitate (dipalmitoylphosphatidylcholine, or DPPC), palmitic acid, and tripalmitin are added. Beractant does not require reconstitution. Calfactant also does not require reconstitution, nor does it need to be warmed at room temperature prior to use, unlike beractant and poractant. Poractant alfa is porcine lung surfactant and is indicated for rescue treatment, whereas beractant and calfactant are approved for prophylaxis and rescue treatment. Poractant should be slowly warmed to room temperature and also does not need reconstitution. Each of these products defines prophylactic and rescue use differently and has different dosing and administration requirements. Table 51.1 lists the surfactant drugs used for prevention and treatment of RDS along with their dosages, uses, and considerations.

TABLE 51.1

Exogenous Surfactant Therapy for Prevention and Treatment of Respiratory Distress Syndrome

Generic Route and Dosage Uses and Considerations
Beractant PN: IT: 4 mL/kg per dose divided into four equal amounts; administer each quarter amount followed by repositioning and extra ventilation; repeat q6h.
Bovine-derived surfactant to be administered IT for prophylaxis and treatment of RDS in premature infants <1250 g birthweight or with evidence of surfactant deficiency within 15 min of birth or neonate with confirmed RDS requiring ET intubation by 8 h.
Drug must be given by health care personnel experienced with using ventilators for prevention or rescue in treatment of RDS.
Administer through a 5-French end-hole catheter as a dosing catheter inserted into an ET tube; do not shake; warm 20 min at room temperature or in the hand for at least 8 min.
Reposition infant to distribute drug followed by ventilation for 20 s after each quarter dose.
Does not affect the CYP450 isoenzymes.
Calfactant PN: IT: 3 mL/kg per dose divided in two equal amounts; administer each half amount over a total of 20-30 breaths during the inspiratory phase followed by repositioning and monitoring respiratory status; repeat q12h.
Calf-derived surfactant to be administered IT for prophylaxis and treatment of RDS in premature infants <29 wk of gestational age at risk for RDS or ≤72 h of age with RDS requiring ET intubation.
Drug must be given by health care personnel experienced with ventilators and RDS.
Gently swirl the vial to ensure a uniform suspension; avoid foaming.
Draw dose with a 20-gauge needle; do not filter or dilute; administer via a 5-French end-hole catheter inserted into the proximal end of the ET tube.
Poractant alfa PN: IT: 2.5 mL/kg per dose divided in two equal amounts; administer each half amount to each main bronchus followed by repositioning and monitoring respiratory status; repeat q12h.
Porcine-derived surfactant to be administered IT for the treatment of RDS in premature infants within 15 h of birth.
Drug must be given by health care personnel experienced with ventilators and RDS.
Warm to room temperature; gently invert to obtain uniform suspension.
Draw dose with a 20-gauge or larger needle; do not filter or dilute; administer via a 5-French end-hole catheter inserted into the proximal end of the ET tube.

CYP450, Cytochrome P450; ET, endotracheal; h, hour; IT, intratracheally; min, minute; PN, premature neonate; q, every; RDS, respiratory distress syndrome; s, second; wk, weeks; <, less than; ≤, less than or equal to.

All exogenous surfactants require a patent endotracheal (ET) tube for administration and specified alterations in positioning the infant throughout the procedure to ensure even drug dispersion. These precise position changes allow gravity to assist in the distribution of the product in the lungs, particularly at the alveolar surface.
Crackles and moist breath sounds may be a transient finding after administration of these products, particularly with beractant. Exogenous surfactant can cause postadministration complications such as hyperoxia (excessive oxygenation) and hypocarbia (decreased carbon dioxide [CO2]). Additionally, transient endotracheal reflux can obstruct the ET tube and lead to oxygen desaturation, cyanosis, bradycardia, and apnea. These issues do not usually lead to serious long-term complications when properly managed. Unless obvious signs of airway obstruction are noted, suctioning should not be performed immediately after administration of supplemental surfactant. Dosing is slowed or halted if the infant (1) becomes dusky colored, (2) becomes agitated, (3) experiences transient bradycardia, (4) has oxygen saturation increases of more than 95%, (5) experiences improved chest expansion, or (6) has arterial or transcutaneous CO2 levels below 30 mm Hg. Suctioning before dosing decreases the chance for ET tube blockage during dosing. No long-term complications or sequelae of synthetic surfactant therapy have been reported. Surfactant replacement therapy has been found effective in reducing the severity of RDS; rapid improvements in lung compliance and oxygenation may require immediate decreases in ventilator settings to prevent lung overdistension and pulmonary air leak.
 
icon Nursing Process: Patient-Centered Collaborative Care
Drug Administered to Preterm Neonate: Synthetic Surfactant

Assessment

• Obtain informed consent. Separate consents are needed for multifetal births.
• Assess the infant’s vital signs, perform a physical examination, and monitor arterial blood gases (ABGs).

Nursing Diagnoses

• Gas Exchange, Impaired related to inadequate lung surfactant secondary to fetal immaturity
• Knowledge, Deficient (parents) related to treatment needs of the infant

Planning

• The infant’s oxygen requirement and respiratory effort will decrease.
• The infant’s need for mechanical ventilation will be quickly reduced.
• The infant will experience no respiratory distress after surfactant administration.

Nursing Interventions

• Maintain a patent airway.
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