PLoS Genetics (Mar 2017)

COLEC10 is mutated in 3MC patients and regulates early craniofacial development.

  • Mustafa M Munye,
  • Anna Diaz-Font,
  • Louise Ocaka,
  • Maiken L Henriksen,
  • Melissa Lees,
  • Angela Brady,
  • Dagan Jenkins,
  • Jenny Morton,
  • Soren W Hansen,
  • Chiara Bacchelli,
  • Philip L Beales,
  • Victor Hernandez-Hernandez

DOI
https://doi.org/10.1371/journal.pgen.1006679
Journal volume & issue
Vol. 13, no. 3
p. e1006679

Abstract

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3MC syndrome is an autosomal recessive heterogeneous disorder with features linked to developmental abnormalities. The main features include facial dysmorphism, craniosynostosis and cleft lip/palate; skeletal structures derived from cranial neural crest cells (cNCC). We previously reported that lectin complement pathway genes COLEC11 and MASP1/3 are mutated in 3MC syndrome patients. Here we define a new gene, COLEC10, also mutated in 3MC families and present novel mutations in COLEC11 and MASP1/3 genes in a further five families. The protein products of COLEC11 and COLEC10, CL-K1 and CL-L1 respectively, form heteromeric complexes. We show COLEC10 is expressed in the base membrane of the palate during murine embryo development. We demonstrate how mutations in COLEC10 (c.25C>T; p.Arg9Ter, c.226delA; p.Gly77Glufs*66 and c.528C>G p.Cys176Trp) impair the expression and/or secretion of CL-L1 highlighting their pathogenicity. Together, these findings provide further evidence linking the lectin complement pathway and complement factors COLEC11 and COLEC10 to morphogenesis of craniofacial structures and 3MC etiology.