A Mouse Model with a Frameshift Mutation in the Nuclear Factor I/X (NFIX) Gene Has Phenotypic Features of Marshall-Smith Syndrome

Kreepa G Kooblall; Mark Stevenson; Michelle Stewart; Lachlan Harris; Oressia Zalucki; Hannah Dewhurst; Natalie Butterfield; Houfu Leng; Tertius A Hough; Da Ma; Bernard Siow; Paul Potter; Roger D Cox; Stephen D M Brown; Nicole Horwood; Benjamin Wright; Helen Lockstone; David Buck; Tonia L Vincent; Fadil M Hannan; J H Duncan Bassett; Graham R Williams; Kate E Lines; Michael Piper; Sara Wells; Lydia Teboul; Raoul C Hennekam; Rajesh V Thakker

doi:10.1002/jbm4.10739

A Mouse Model with a Frameshift Mutation in the Nuclear Factor I/X (NFIX) Gene Has Phenotypic Features of Marshall-Smith Syndrome

JBMR Plus. 2023 Mar 30;7(6):e10739. doi: 10.1002/jbm4.10739. eCollection 2023 Jun.

Authors

Kreepa G Kooblall¹, Mark Stevenson¹, Michelle Stewart², Lachlan Harris³, Oressia Zalucki⁴, Hannah Dewhurst⁵, Natalie Butterfield⁵, Houfu Leng⁶, Tertius A Hough², Da Ma⁷, Bernard Siow³, Paul Potter², Roger D Cox², Stephen D M Brown², Nicole Horwood⁶, Benjamin Wright⁸, Helen Lockstone⁸, David Buck⁸, Tonia L Vincent⁶, Fadil M Hannan^{1

9}, J H Duncan Bassett⁵, Graham R Williams⁵, Kate E Lines¹, Michael Piper⁴, Sara Wells², Lydia Teboul², Raoul C Hennekam¹⁰, Rajesh V Thakker¹

Affiliations

¹ Academic Endocrine Unit, Radcliffe Department of Medicine, Oxford Centre for Diabetes, Endocrinology and Metabolism (OCDEM) University of Oxford Oxford UK.
² MRC Harwell, Mary Lyon Centre Harwell Science and Innovation Campus Oxfordshire UK.
³ The Francis Crick Institute London UK.
⁴ The School of Biomedical Sciences and The Queensland Brain Institute The University of Queensland Brisbane Australia.
⁵ Molecular Endocrinology Laboratory, Department of Metabolism, Digestion and Reproduction, Imperial College London Hammersmith Hospital London UK.
⁶ Centre for OA Pathogenesis Versus Arthritis, The Kennedy Institute of Rheumatology, Nuffield Department of Orthopaedics, Rheumatology and Musculoskeletal Sciences (NDORMS) Medical Sciences Division University of Oxford Oxford UK.
⁷ Department of Internal Medicine Wake Forest University School of Medicine Winston-Salem NC USA.
⁸ Oxford Genomics Centre, The Wellcome Centre for Human Genetics University of Oxford Oxford UK.
⁹ Nuffield Department of Women's and Reproductive Health University of Oxford Oxford UK.
¹⁰ Department of Pediatrics, Amsterdam UMC University of Amsterdam Amsterdam The Netherlands.

Abstract

The nuclear factor I/X (NFIX) gene encodes a ubiquitously expressed transcription factor whose mutations lead to two allelic disorders characterized by developmental, skeletal, and neural abnormalities, namely, Malan syndrome (MAL) and Marshall-Smith syndrome (MSS). NFIX mutations associated with MAL mainly cluster in exon 2 and are cleared by nonsense-mediated decay (NMD) leading to NFIX haploinsufficiency, whereas NFIX mutations associated with MSS are clustered in exons 6-10 and escape NMD and result in the production of dominant-negative mutant NFIX proteins. Thus, different NFIX mutations have distinct consequences on NFIX expression. To elucidate the in vivo effects of MSS-associated NFIX exon 7 mutations, we used CRISPR-Cas9 to generate mouse models with exon 7 deletions that comprised: a frameshift deletion of two nucleotides (Nfix Del2); in-frame deletion of 24 nucleotides (Nfix Del24); and deletion of 140 nucleotides (Nfix Del140). Nfix ^+/Del2, Nfix ^+/Del24, Nfix ^+/Del140, Nfix ^Del24/Del24, and Nfix ^{Del140/Del140} mice were viable, normal, and fertile, with no skeletal abnormalities, but Nfix ^Del2/Del2 mice had significantly reduced viability (p < 0.002) and died at 2-3 weeks of age. Nfix Del2 was not cleared by NMD, and Nfix^Del2/Del2 mice, when compared to Nfix ^+/+ and Nfix ^+/Del2 mice, had: growth retardation; short stature with kyphosis; reduced skull length; marked porosity of the vertebrae with decreased vertebral and femoral bone mineral content; and reduced caudal vertebrae height and femur length. Plasma biochemistry analysis revealed Nfix ^Del2/Del2 mice to have increased total alkaline phosphatase activity but decreased C-terminal telopeptide and procollagen-type-1-N-terminal propeptide concentrations compared to Nfix ^+/+ and Nfix ^+/Del2 mice. Nfix ^Del2/Del2 mice were also found to have enlarged cerebral cortices and ventricular areas but smaller dentate gyrus compared to Nfix ^+/+ mice. Thus, Nfix ^Del2/Del2 mice provide a model for studying the in vivo effects of NFIX mutants that escape NMD and result in developmental abnormalities of the skeletal and neural tissues that are associated with MSS. © 2023 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.

Keywords: NFIX; brain abnormalities; frameshift mutation; kyphosis; osteopenia.

Abstract

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