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Precision mouse models of <i>Yars</i>/dominant intermediate Charcot‐Marie‐Tooth disease type C and <i>Sptlc1</i>/hereditary sensory and autonomic neuropathy type 1

Timothy J. Hines, Abigail L. D. Tadenev, Museer A. Lone, Courtney L. Hatton, Inseyah Bagasrawala, Morgane Stum, Kathy E. Miers, Thorsten Hornemann, Robert W. Burgess

2021Journal of Anatomy22 citationsDOIOpen Access PDF

Abstract

Abstract Animal models of neurodegenerative diseases such as inherited peripheral neuropathies sometimes accurately recreate the pathophysiology of the human disease, and sometimes accurately recreate the genetic perturbations found in patients. Ideally, models achieve both, but this is not always possible; nonetheless, such models are informative. Here we describe two animal models of inherited peripheral neuropathy: mice with a mutation in tyrosyl tRNA‐synthetase, Yars E196K , modeling dominant intermediate Charcot‐Marie‐Tooth disease type C (diCMTC), and mice with a mutation in serine palmitoyltransferase long chain 1, Sptlc1 C133W , modeling hereditary sensory and autonomic neuropathy type 1 (HSAN1). Yars E196K mice develop disease‐relevant phenotypes including reduced motor performance and reduced nerve conduction velocities by 4 months of age. Peripheral motor axons are reduced in size, but there is no reduction in axon number and plasma neurofilament light chain levels are not increased. Unlike the dominant human mutations, the Yars E196K mice only show these phenotypes as homozygotes, or as compound heterozygotes with a null allele, and no phenotype is observed in E196K or null heterozygotes. The Sptlc1 C133W mice carry a knockin allele and show the anticipated increase in 1‐deoxysphingolipids in circulation and in a variety of tissues. They also have mild behavioral defects consistent with HSAN1, but do not show neurophysiological defects or axon loss in peripheral nerves or in the epidermis of the hind paw or tail. Thus, despite the biochemical phenotype, the Sptlc1 C133W mice do not show a strong neuropathy phenotype. Surprisingly, these mice were lethal as homozygotes, but the heterozygous genotype studied corresponds to the dominant genetics seen in humans. Thus, Yars E196K homozygous mice have a relevant phenotype, but imprecisely reproduce the human genetics, whereas the Sptlc1 C133W mice precisely reproduce the human genetics, but do not recreate the disease phenotype. Despite these shortcomings, both models are informative and will be useful for future research.

Topics & Concepts

PhenotypeNull alleleAlleleBiologyHeterozygote advantageHereditary motor and sensory neuropathyPeripheral neuropathyAxonMutationGeneticsNeuroscienceEndocrinologyGeneDiabetes mellitusHereditary Neurological DisordersRNA Research and SplicingNeurological diseases and metabolism
Precision mouse models of <i>Yars</i>/dominant intermediate Charcot‐Marie‐Tooth disease type C and <i>Sptlc1</i>/hereditary sensory and autonomic neuropathy type 1 | Litcius