Kif1bp loss in mice leads to defects in the peripheral and central nervous system and perinatal death

CS Hirst; LA Stamp; AJ Bergner; MM Hao; MX Tran; JM Morgan; M Dutschmann; AM Allen; G Paxinos; TM Furlong; SJ McKeown; HM Young

Journal article

Kif1bp loss in mice leads to defects in the peripheral and central nervous system and perinatal death

CS Hirst, LA Stamp, AJ Bergner, MM Hao, MX Tran, JM Morgan, M Dutschmann, AM Allen, G Paxinos, TM Furlong, SJ McKeown, HM Young

Scientific Reports | NATURE PORTFOLIO | Published : 2017

DOI: 10.1038/s41598-017-16965-3

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Abstract

Goldberg-Shprintzen syndrome is a poorly understood condition characterized by learning difficulties, facial dysmorphism, microcephaly, and Hirschsprung disease. GOSHS is due to recessive mutations in KIAA1279, which encodes kinesin family member 1 binding protein (KIF1BP, also known as KBP). We examined the effects of inactivation of Kif1bp in mice. Mice lacking Kif1bp died shortly after birth, and exhibited smaller brains, olfactory bulbs and anterior commissures, and defects in the vagal and sympathetic innervation of the gut. Kif1bp was found to interact with Ret to regulate the development of the vagal innervation of the stomach. Although newborn Kif1bp -/- mice had neurons along the en..

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University of Melbourne Researchers

Lincon Stamp Author

Annette Bergner Author

Marlene Hao Author

Andrew Allen Author

Grants

Awarded by National Health and Medical Research Council

Funding Acknowledgements

This work was supported by NHMRC Australia Project Grant 1047953 to HMY and SMcK. We thank Robert Hofstra and Maria Alves for the KIF1BP antisera, Hideki Enomoto for the PHOX2B antisera, Vanda Lennon for the HuC/D antisera and Piers Emson for the nNOS antisera.