Neuropediatrics 2008; 39(6): 359-362
DOI: 10.1055/s-0029-1202835
Short Communication

© Georg Thieme Verlag KG Stuttgart · New York

Reversal of Hindbrain Herniation after Maternal-fetal Surgery for Myelomeningocele Subsequently Impacts on Brain Stem Function

E. Danzer 1 , R. S. Finkel 1 , N. E. Rintoul 1 , M. W. Bebbington 1 , E. S. Schwartz 1 , D. M. Zarnow 1 , N. S. Adzick 1 , M. P. Johnson 1
  • 1The Center for Fetal Diagnosis and Treatment, The Children's Hospital of Philadelphia and The University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania, USA
Further Information

Publication History

received 06.11.2008

accepted 25.01.2009

Publication Date:
30 June 2009 (online)

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Abstract

The aim of our study was to delineate whether the reversal of hindbrain herniation (HH) following fetal myelomeningocele (fMMC) closure subsequently reduces the incidence and severity of HH-associated brainstem dysfunction (BSD). Prior to the NIH-sponsored Management of Myelomeningocele Study (MOMS) trial, 54 children underwent fMMC closure at our institution. Forty-eight (89%) families participated in a structured survey focusing on HH-associated BSD (e.g., apnea, neurogenic dysphagia [ND], gastro-esophageal reflux disease [GERD], neuro-ophthalmologic disturbances [NOD]). Median age at follow-up was 72 months (range: 46–98). Fifty-percent required shunting. HH-related symptoms were completely absent in 15 (63%) non-shunted and 10 (42%) shunted children (P=0.15). No HH-related death occurred and none developed severe persistent cyanotic apnea. ND was reported in 2 (8%) non-shunted and 9 (38%) shunted infants (P=0.03). Mild GERD (medically managed) developed in 2 (8%) without and 6 (25%) with shunt placement (P=0.24). NOD was found in 6 (25%) and 13 (54%) of non-shunted and shunted children, respectively (P=0.07). The majority of fMMC children developed no or only mild BSD at follow-up. Our data support the hypothesis that neurodevelopmental deficits associated with MMC are at least partially acquired and that reversal of HH following fMMC surgery may help to reduce the incidence and severity of BSD.

References

Correspondence

M. P. JohnsonMD 

The Center for Fetal Diagnosis and Treatment

The Children's Hospital of Philadelphia

5th Wood Center

34th Street and Civic Center Boulevard

19104 Philadelphia

USA

Phone: +1/215/590 27 47

Fax: +1/215/590 24 47

Email: johnsonma@email.chop.edu