Literature DB >> 30375152

Using human sequencing to guide craniofacial research.

Ryan P Liegel1, Erin Finnerty1, Lauren Blizzard1, Andrew DiStasio1, Robert B Hufnagel1, Howard M Saal1,2, Kristen L Sund1,2, Cynthia A Prows1,3,2, Rolf W Stottmann1,4,2.   

Abstract

A recent convergence of technological innovations has re-energized the ability to apply genetics to research in human craniofacial development. Next-generation exome and whole genome sequencing have significantly dropped in price, making it relatively trivial to sequence and analyze patients and families with congenital craniofacial anomalies. A concurrent revolution in genome editing with the use of the CRISPR-Cas9 system enables the rapid generation of animal models, including mouse, which can precisely recapitulate human variants. Here, we summarize the choices currently available to the research community. We illustrate this approach with the study of a family with a novel craniofacial syndrome with dominant inheritance pattern. The genomic analysis suggested a causal variant in AMOTL1 which we modeled in mice. We also made a novel deletion allele of Amotl1. Our results indicate that Amotl1 is not required in the mouse for survival to weaning. Mice carrying the variant identified in the human sequencing studies, however, do not survive to weaning in normal ratios. The cause of death is not understood for these mice complicating our conclusions about the pathogenicity in the index patient. Thus, we highlight some of the powerful opportunities and confounding factors confronting current craniofacial genetic research.
© 2018 Wiley Periodicals, Inc.

Entities:  

Keywords:  birth defects; mammal; organism; process, genetics; process, neural crest; process, organogenesis; tissue; tissue, other

Mesh:

Substances:

Year:  2018        PMID: 30375152      PMCID: PMC8796141          DOI: 10.1002/dvg.23259

Source DB:  PubMed          Journal:  Genesis        ISSN: 1526-954X            Impact factor:   2.487


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