Mitchell Goldstein, MD
Division of Neonatology
Department of Pediatrics
Loma Linda University Children’s Hospital
11175 Campus Street, Suite #11121
Loma Linda, CA 92350
mgoldstein@llu.edu
Benjamin Harding, MD
Division of Neonatology
Department of Pediatrics
Loma Linda University Children’s Hospital
11175 Campus Street, Suite #11121
Loma Linda, CA 92350
bharding@llu.edu
Elba Fayard, MD
Division of Neonatology
Department of Pediatrics
Loma Linda University Children’s Hospital
11175 Campus Street, Suite #11121
Loma Linda, CA 92350
efayard@llu.edu
Disclosures: The authors have no relevant conflicts of interest.
Keywords: RSV, palivizumab, prophylaxis, NPA, AAP
Palivizumab is a synthetic monoclonal antibody targeting the F-protein
spike of the Respiratory Syncytial Virus. First approved by the United
States Food and Drug Administration (FDA) in 1998, its indicated usage
mirrored the American Academy of Pediatrics, Committee on Infectious
Disease (AAP- COID) guidance through the first few years following its
approval. At that time, primarily based on expert opinion and cost
considerations, the AAP-COID progressively decreased its guidance,
culminating in a policy statement released in 2014 that excluded 75% of
the patients initially covered by the FDA
indication.1,2 The National Perinatal Association
(NPA) first became concerned with the continued ratcheting down of
coverage in 2009 when it released its first of three guidances on
palivizumab prophylaxis. The intent was to provide an alternative to the
AAP guidance and subsequent policy statement that increasingly deviated
from the original FDA indication and failed to recognize myriad
peer-reviewed studies that confirmed disease severity, prevalence,
hospitalization, and response to prophylaxis.
The NPA guidance was first presented to Loma Linda University Children’s
Hospital (LLUCH) Neonatologists in 2009. At that time, usage of this
guidance or the AAP guidance (at that time, less restrictive) was
optional. The attending neonatologist would indicate which guidance the
baby was to be discharged home on and the rationale for the decision.
With the release of the AAP 2014 policy, the NPA guidance was
encouraged, as reflected by a change in the LLUCH NICU resident
manual.3,4 LLU neonatal physicians met with a local
pharmacy to streamline RSV prophylaxis administration to those at-risk
patients. In 2018, the most recent NPA guidance was officially adopted
by LLUCH Neonatologists.2 A dot-phrase was built into
the EHR to assure compliance. Year over year, RSV inpatient dose
administration increased from 115 in 2017-2018, to 117 in 2018, to 176
in 2019-2020. Outpatient dosing increased from 0 (reported) in
2017-2018, to 175 in 2018-2019, and 487 in 2019-2020. (p<0.01)
Although the current study provides information regarding the
demographics of the patients who received palivizumab before and after
changes in the AAP COID policy, compliance remains an issue to any
guidance or policy. The unintended effects of a restrictive policy often
extend beyond the boundaries of its intended advice. In many locations,
palivizumab cannot be obtained for even those patients who clearly
qualify by both metrics.5 Unrecognized morbidities are
substantial. Most studies do not adequately capture cough, wheeze,
secondary infection, and failure to thrive.6 Lost
productivity from parents and other caregivers having to remain at home
with a sick child is not considered. Hospital billing data versus actual
payment and palivizumab cost data versus actual payment can be
manipulated to denigrate a highly effective biologic with a demonstrated
safety profile.
In sum, the authors have presented compelling data regarding
palivizumab’s efficacy but have just begun to scratch the surface. Loma
Linda is the only level 4 NICU in San Bernardino County, the largest in
the state. As they pointed out, many inpatients from LLUCH NICU do wind
up seeking care at alternate centers and may receive doses of
palivizumab from other pharmacies. Extended to other centers,
differences in practice patterns and palivizumab administration may
reveal gaps in coverage. Changes in the practice pattern of the LLUCH
Neonatologists and administration of palivizumab in subsequent years may
provide an even more compelling argument for prophylaxis according to
FDA indication.
References:
1. Goldstein M, Krilov LR, Fergie J, et al. Respiratory Syncytial Virus
Hospitalizations among U.S. Preterm Infants Compared with Term Infants
Before and After the 2014 American Academy of Pediatrics Guidance on
Immunoprophylaxis: 2012-2016. Am J Perinatol.2018;35(14):1433-1442.
2. Goldstein M, Phillips R, DeVincenzo J, et al. National Perinatal
Association 2018 Respiratory Syncytial Virus (RSV) prevntion clinical
practice guideline: An evidence-based interdisciplinary collaboration.Neonatology Today. 2017;12(10):10.
3. American Academy of Pediatrics Committee on Infectious D, American
Academy of Pediatrics Bronchiolitis Guidelines C. Updated guidance for
palivizumab prophylaxis among infants and young children at increased
risk of hospitalization for respiratory syncytial virus infection.Pediatrics. 2014;134(2):415-420.
4. Goldstein M, Merritt T, Phillips R, Martin G, Hall S, Yogev R.
National Perinatal Association 2015 respiratory syncytial virus (RSV)
prevention guideline. Neonatology Today. 2014;9(11):1-11.
5. Goldstein M, Krilov LR, Fergie J, et al. Unintended Consequences
Following the 2014 American Academy of Pediatrics Policy Change for
Palivizumab Prophylaxis among Infants Born at Less than 29 Weeks’
Gestation. Am J Perinatol. 2020.
6. Blanken MO, Rovers MM, Molenaar JM, et al. Respiratory syncytial
virus and recurrent wheeze in healthy preterm infants. The New
England journal of medicine. 2013;368(19):1791-1799.