Expanding the clinical spectrum associated with defects in CNTNAP2 and NRXN1

Anne Gregor; Beate Albrecht; Ingrid Bader; Emilia K Bijlsma; Arif B Ekici; Hartmut Engels; Karl Hackmann; Denise Horn; Juliane Hoyer; Jakub Klapecki; Jürgen Kohlhase; Isabelle Maystadt; Sandra Nagl; Eva Prott; Sigrid Tinschert; Reinhard Ullmann; Eva Wohlleber; Geoffrey Woods; André Reis; Anita Rauch; Christiane Zweier

doi:10.1186/1471-2350-12-106

Expanding the clinical spectrum associated with defects in CNTNAP2 and NRXN1

BMC Med Genet. 2011 Aug 9:12:106. doi: 10.1186/1471-2350-12-106.

Affiliation

¹ Institute of Human Genetics, Friedrich-Alexander-University Erlangen-Nuremberg, Erlangen, Germany.

Abstract

Background: Heterozygous copy-number and missense variants in CNTNAP2 and NRXN1 have repeatedly been associated with a wide spectrum of neuropsychiatric disorders such as developmental language and autism spectrum disorders, epilepsy and schizophrenia. Recently, homozygous or compound heterozygous defects in either gene were reported as causative for severe intellectual disability.

Methods: 99 patients with severe intellectual disability and resemblance to Pitt-Hopkins syndrome and/or suspected recessive inheritance were screened for mutations in CNTNAP2 and NRXN1. Molecular karyotyping was performed in 45 patients. In 8 further patients with variable intellectual disability and heterozygous deletions in either CNTNAP2 or NRXN1, the remaining allele was sequenced.

Results: By molecular karyotyping and mutational screening of CNTNAP2 and NRXN1 in a group of severely intellectually disabled patients we identified a heterozygous deletion in NRXN1 in one patient and heterozygous splice-site, frameshift and stop mutations in CNTNAP2 in four patients, respectively. Neither in these patients nor in eight further patients with heterozygous deletions within NRXN1 or CNTNAP2 we could identify a defect on the second allele. One deletion in NRXN1 and one deletion in CNTNAP2 occurred de novo, in another family the deletion was also identified in the mother who had learning difficulties, and in all other tested families one parent was shown to be healthy carrier of the respective deletion or mutation.

Conclusions: We report on patients with heterozygous defects in CNTNAP2 or NRXN1 associated with severe intellectual disability, which has only been reported for recessive defects before. These results expand the spectrum of phenotypic severity in patients with heterozygous defects in either gene. The large variability between severely affected patients and mildly affected or asymptomatic carrier parents might suggest the presence of a second hit, not necessarily located in the same gene.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Alleles
Calcium-Binding Proteins
Cell Adhesion Molecules, Neuronal / genetics*
Child
Child Development Disorders, Pervasive / genetics
Child, Preschool
Codon, Terminator
Facies
Female
Frameshift Mutation
Gene Deletion
Heterozygote
Humans
Hyperventilation / genetics
Intellectual Disability / genetics*
Karyotyping
Male
Membrane Proteins / genetics*
Nerve Tissue Proteins / genetics*
Neural Cell Adhesion Molecules
RNA Splice Sites
Young Adult

Substances

CNTNAP2 protein, human
Calcium-Binding Proteins
Cell Adhesion Molecules, Neuronal
Codon, Terminator
Membrane Proteins
NRXN1 protein, human
Nerve Tissue Proteins
Neural Cell Adhesion Molecules
RNA Splice Sites

Supplementary concepts

Pitt-Hopkins syndrome