Ovine congenital progressive muscular dystrophy (OCPMD) is a model of TNNT1 congenital myopathy

Joshua S Clayton,Gianina Ravenscroft,Keren Muthsam,Alison C Testa,Nigel G Laing,David Groth,David Coote,Rhonda L Taylor,Amanda J O’Hara,Kristen J Nowak,Elyshia L Mcnamara,Hayley Goullee,James Kijas,Gabrielle C Musk,Coen Ottenheijm,Stefan Conijn

doi:10.1186/s40478-020-01017-1

Abstract

Ovine congenital progressive muscular dystrophy (OCPMD) was first described in Merino sheep flocks in Queensland and Western Australia in the 1960s and 1970s. The most prominent feature of the disease is a distinctive gait with stiffness of the hind limbs that can be seen as early as 3 weeks after birth. The disease is progressive. Histopathological examination had revealed dystrophic changes specifically in type I (slow) myofibres, while electron microscopy had demonstrated abundant nemaline bodies. Therefore, it was never certain whether the disease was a dystrophy or a congenital myopathy with dystrophic features. In this study, we performed whole genome sequencing of OCPMD sheep and identified a single base deletion at the splice donor site (+ 1) of intron 13 in the type I myofibre-specific TNNT1 gene (KT218690 c.614 + 1delG). All affected sheep were homozygous for this variant. Examination of TNNT1 splicing by RT-PCR showed intron retention and premature termination, which disrupts the highly conserved 14 amino acid C-terminus. The variant did not reduce TNNT1 protein levels or affect its localization but impaired its ability to modulate muscle contraction in response to Ca2+ levels. Identification of the causative variant in TNNT1 finally clarifies that the OCPMD sheep is in fact a large animal model of TNNT1 congenital myopathy. This model could now be used for testing molecular or gene therapies.

Highlights

Ovine congenital progressive muscular dystrophy (OCPMD) was first described in a Merino sheep flock in Queensland, Australia in 1969 [1]
Gross observation and histochemical analysis confirmed type I myofibres are predominantly affected in OCPMD sheep The skeletal muscle histopathology and myofibre morphometry of OCPMD sheep was characterized in detail in the 1970s and 1980s [2, 4, 5]
Here, we identify the genetic cause of the well-characterized model of ovine congenital progressive muscular dystrophy from Western Australia and re-classify it as a congenital myopathy with dystrophic features

Summary

Introduction

Ovine congenital progressive muscular dystrophy (OCPMD) was first described in a Merino sheep flock in Queensland, Australia in 1969 [1]. Further cases were subsequently characterized in Merino sheep in Western Australia in 1979 [2]. The clinical and pathological features of both flocks are highly similar, there is no known breeding connection between these. Clayton et al acta neuropathol commun (2020) 8:142 myofibre-predominant [3]. Skeletal muscle wasting continues throughout life and skeletal muscles, especially those with high proportions of type I myofibres, are gradually replaced by fat [3]. Histopathology [4] and myofibre morphometry [5] indicated confinement of OCPMD pathology to type I myofibres. Electron microscopy showed large numbers of nemaline bodies in the affected myofibres [6]

Methods

Results

Discussion

Conclusion