Hotspots of missense mutation identify neurodevelopmental disorder genes and functional domains

Madeleine R. Geisheker,Gabriel Heymann,Tianyun Wang,Bradley P. Coe,Tychele N. Turner,Holly A. F. Stessman,Kendra Hoekzema,Malin Kvarnung,Marie Shaw,Kathryn Friend,Jan Liebelt,Christopher Barnett,Elizabeth Thompson,Eric Haan,Hui Guo,Britt-Marie Anderlid,Ann Nordgren,Anna Lindstrand,Geert Vandeweyer,Antonino Alberti,Emanuela Avola,Mirella Vinci,Stefania Giusto,Tiziano Pramparo,Karen Pierce,Srinivasa Nalabolu,Jacob J. Michaelson,Zdenek Sedlacek,Gijs W.E. Santen,Hilde Peeters,Hakon Hakonarson,Eric Courchesne,Corrado Romano,R. Frank Kooy,Raphael Bernier,Magnus Nordenskjöld,Jozef Gecz,Kun Xia,Larry S. Zweifel,Evan E. Eichler

Hotspots of missense mutation identify neurodevelopmental disorder genes and functional domains

2017

This study characterizes the properties of disease-causing mutations that produce sporadic amino acid replacements in proteins of people with autism and developmental delay. The mutations tend to cluster and reoccur at specific regions important to protein function, highlighting for future follow-up ∼200 candidate genes, many involved in neuronal signaling.

Keywords:

Candidate gene
Neuroscience
Autism
Missense mutation
Exome
Neurodevelopmental disorder
Gene
Amino acid
Peptide sequence
Genetics
Biology

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