LRFN5 locus structure is associated with autism and influenced by the sex of the individual and locus conversions

Helle Lybaek; Michael Robson; Nicole de Leeuw; Jayne Y Hehir-Kwa; Aaron Jeffries; Bjørn Ivar Haukanes; Siren Berland; Diederik de Bruijn; Stefan Mundlos; Malte Spielmann; Gunnar Houge

doi:10.1002/aur.2677

LRFN5 locus structure is associated with autism and influenced by the sex of the individual and locus conversions

Autism Res. 2022 Mar;15(3):421-433. doi: 10.1002/aur.2677. Epub 2022 Jan 28.

Authors

Affiliations

¹ Department of Medical Genetics, Haukeland University Hospital, Bergen, Norway.
² Max Planck Institute for Molecular Genetics, Berlin, Germany.
³ Department of Human Genetics, Radboud University Nijmegen Medical Centre, Nijmegen, Netherlands.
⁴ Princess Máxima Center for Pediatric Oncology, Utrecht, Netherlands.
⁵ University of Exeter, Exeter, UK.
⁶ Institute for Human Genetics, UKSH, Kiel, Germany.
⁷ Institute of Clinical Medicine K2, Faculty of Medicine, University of Bergen, Bergen, Norway.
⁸ Honorary Chair of Evolution and Genomic Sciences, University of Manchester, Manchester, UK.

Abstract

LRFN5 is a regulator of synaptic development and the only gene in a 5.4 Mb mammalian-specific conserved topologically associating domain (TAD); the LRFN5 locus. An association between locus structural changes and developmental delay (DD) and/or autism was suggested by several cases in DECIPHER and own records. More significantly, we found that maternal inheritance of a specific LRFN5 locus haplotype segregated with an identical type of autism in distantly related males. This autism-susceptibility haplotype had a specific TAD pattern. We also found a male/female quantitative difference in the amount histone-3-lysine-9-associated chromatin around the LRFN5 gene itself (p < 0.01), possibly related to the male-restricted autism susceptibility. To better understand locus behavior, the prevalence of a 60 kb deletion polymorphism was investigated. Surprisingly, in three cohorts of individuals with DD (n = 8757), the number of deletion heterozygotes was 20%-26% lower than expected from Hardy-Weinberg equilibrium. This suggests allelic interaction, also because the conversions from heterozygosity to wild-type or deletion homozygosity were of equal magnitudes. Remarkably, in a control group of medical students (n = 1416), such conversions were three times more common (p = 0.00001), suggesting a regulatory role of this allelic interaction. Taken together, LRFN5 regulation appears unusually complex, and LRFN5 dysregulation could be an epigenetic cause of autism. LAY SUMMARY: LRFN5 is involved with communication between brain cells. The gene sits alone in a huge genomic niche, called the LRFN5 locus, of complex structure and high mammalian conservation. We have found that a specific locus structure increases autism susceptibility in males, but we do not yet know how common this epigenetic cause of autism is. It is, however, a cause that potentially could explain why higher-functioning autism is more common in males than females.

Keywords: LRFN5; SALM5; TAD structure; allelic interaction; autism; chromatin structure; epigenetics; epigenomics.

Publication types

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

MeSH terms

Animals
Autism Spectrum Disorder* / genetics
Autistic Disorder* / genetics
Cell Adhesion Molecules, Neuronal / genetics*
Female
Haplotypes
Humans
Male
Mammals
Polymorphism, Genetic

Substances

Cell Adhesion Molecules, Neuronal
LRFN5 protein, human