Canine Brachycephaly Is Associated with a Retrotransposon-Mediated Missplicing of SMOC2.

Authors

Thomas W Marchant
Edward J Johnson
Lynn McTeir
Craig I Johnson
Adam Gow
Tiziana Liuti
Dana Kuehn
Karen L. Svenson, The Jackson LaboratoryFollow
Mairead L Bermingham
Michaela Drögemüller
Marc Nussbaumer
Megan G Davey
David J Argyle
Roger M Powell
Sérgio Guilherme
Johann Lang
Gert Ter Haar
Tosso Leeb
Tobias Schwarz
Richard J Mellanby
Dylan N Clements
Jeffrey J Schoenebeck

Document Type

Article

Publication Date

6-5-2017

JAX Source

Curr Biol 2017 Jun 5; 27(11):1573-1584

Volume

27

Issue

11

First Page

1573

Last Page

1584

ISSN

1879-0445

PMID

28552356

DOI

https://doi.org/10.1016/j.cub.2017.04.057

Abstract

In morphological terms, "form" is used to describe an object's shape and size. In dogs, facial form is stunningly diverse. Facial retrusion, the proximodistal shortening of the snout and widening of the hard palate is common to brachycephalic dogs and is a welfare concern, as the incidence of respiratory distress and ocular trauma observed in this class of dogs is highly correlated with their skull form. Progress to identify the molecular underpinnings of facial retrusion is limited to association of a missense mutation in BMP3 among small brachycephalic dogs. Here, we used morphometrics of skull isosurfaces derived from 374 pedigree and mixed-breed dogs to dissect the genetics of skull form. Through deconvolution of facial forms, we identified quantitative trait loci that are responsible for canine facial shapes and sizes. Our novel insights include recognition that the FGF4 retrogene insertion, previously associated with appendicular chondrodysplasia, also reduces neurocranium size. Focusing on facial shape, we resolved a quantitative trait locus on canine chromosome 1 to a 188-kb critical interval that encompasses SMOC2. An intronic, transposable element within SMOC2 promotes the utilization of cryptic splice sites, causing its incorporation into transcripts, and drastically reduces SMOC2 gene expression in brachycephalic dogs. SMOC2 disruption affects the facial skeleton in a dose-dependent manner. The size effects of the associated SMOC2 haplotype are profound, accounting for 36% of facial length variation in the dogs we tested. Our data bring new focus to SMOC2 by highlighting its clinical implications in both human and veterinary medicine. Curr Biol 2017 Jun 5; 27(11):1573-1584.

Recommended Citation

Marchant T, Johnson E, McTeir L, Johnson C, Gow A, Liuti T, Kuehn D, Svenson KL, Bermingham M, Drögemüller M, Nussbaumer M, Davey M, Argyle D, Powell R, Guilherme S, Lang J, Ter Haar G, Leeb T, Schwarz T, Mellanby R, Clements D, Schoenebeck J. Canine Brachycephaly Is Associated with a Retrotransposon-Mediated Missplicing of SMOC2. Curr Biol 2017 Jun 5; 27(11):1573-1584