Genetic Influence on Neurodevelopment in Nonsyndromic Craniosynostosis

Andrew T Timberlake; Alexandra Junn; Roberto Flores; David A Staffenberg; Richard P Lifton; John A Persing

doi:10.1097/PRS.0000000000008976

Genetic Influence on Neurodevelopment in Nonsyndromic Craniosynostosis

Plast Reconstr Surg. 2022 May 1;149(5):1157-1165. doi: 10.1097/PRS.0000000000008976. Epub 2022 Mar 14.

Authors

Andrew T Timberlake¹, Alexandra Junn¹, Roberto Flores¹, David A Staffenberg¹, Richard P Lifton¹, John A Persing¹

Affiliation

¹ From the Hansjörg Wyss Department of Plastic Surgery, New York University Langone Health; Department of Surgery, Division of Plastic Surgery, Yale School of Medicine; and Laboratory of Human Genetics and Genomics, The Rockefeller University.

Abstract

Background: Nonsyndromic craniosynostosis is one of the most common anomalies treated by craniofacial surgeons. Despite optimal surgical management, nearly half of affected children have subtle neurocognitive deficits. Whereas timing and type of surgical intervention have been studied, the possibility of genetic influence on neurodevelopment in nonsyndromic craniosynostosis patients remains unexplored.

Methods: The authors performed whole-exome sequencing for 404 case-parent trios with sporadic nonsyndromic craniosynostosis. Statistical analyses were performed to assess the burden of de novo mutations in cases compared to both expectation and 1789 healthy control trios. Individuals with and without each mutation class were analyzed, and the presence or absence of various types of neurodevelopmental delay were recorded alongside demographic information.

Results: The authors identified a highly significant burden of damaging de novo mutations in mutation-intolerant [probability of loss of function intolerance (pLI) >0.9] genes in nonsyndromic craniosynostosis probands (p = 5.9 × 10-6). Children with these mutations had a two-fold higher incidence of neurodevelopmental delay (p = 0.001) and a more than 20-fold greater incidence of intellectual disability (p = 7.2 × 10-7), and were 3.6-fold more likely to have delays that persisted past 5 years of age (p = 4.4 × 10-4) in comparison with children with nonsyndromic craniosynostosis without these mutations. Transmitted loss of function mutations in high-pLI genes also conferred a 1.9-fold greater risk of neurodevelopmental delay (p = 4.5 ×10-4).

Conclusions: These findings implicate genetic lesions concurrently impacting neurodevelopment and cranial morphogenesis in the pathoetiology of nonsyndromic craniosynostosis and identify a strong genetic influence on neurodevelopmental outcomes in affected children. These findings may eventually prove useful in determining which children with nonsyndromic craniosynostosis are most likely to benefit from surgical intervention.

Clinical question/level of evidence: Risk, III.

MeSH terms

Child
Craniosynostoses* / complications
Craniosynostoses* / genetics
Craniosynostoses* / pathology
Exome Sequencing
Humans
Incidence
Mutation
Skull / pathology

Grants and funding

UM1 HG006504/HG/NHGRI NIH HHS/United States