Biallelic variants in<i>HMGCS1</i>are a novel cause of rare rigid spine syndrome

Dofash, Lein NH; Miles, Lee B; Saito, Yoshihiko; Rivas, Eloy; Calcinotto, Vanessa; Oveissi, Sara; Serrano, Rita J; Templin, Rachel; Ramm, Georg; Rodger, Alison; Haywood, Joel; Ingley, Evan; Clayton, Joshua S; Taylor, Rhonda L; Folland, Chiara L; Groth, David; Hock, Daniella H; Stroud, David A; Gorokhova, Svetlana; Donkervoort, Sandra; Bönnemann, Carsten G; Sud, Malika; VanNoy, Grace; Mangilog, Brian E; Pais, Lynn; Madruga-Garrido, Marcos; Scala, Marcello; Fiorillo, Chiara; Baratto, Serena; Traverso, Monica; Bruno, Claudio; Zara, Federico; Paradas, Carmen; Ogata, Katsuhisa; Nishino, Ichizo; Laing, Nigel G; Bryson-Richardson, Robert J; Cabrera-Serrano, Macarena; Ravenscroft, Gianina

doi:10.1101/2023.10.25.23297129

Cited by 2 publications

(1 citation statement)

References 98 publications

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“…Other inherited muscle diseases involving the mevalonate pathway include those associated with variants in HMGCS1 related to rare form of rigid spine syndrome 33 and those associated with variants in GGPS1 , which is associated with a rare form of muscular dystrophy represented with hearing loss and ovarian insufficiency 34,35 . HMG-CoA synthase 1 (encoded by HMGCS1 ) catalyzes a reaction immediately upstream of HMGCR, whereas geranylgeranyl diphosphate synthase 1 (encoded by GGPS1 ) catalyzes a reaction in a different downstream pathway than cholesterol synthesis 5 , suggesting that the myopathic effects of HMGCR deficiency may be due in part to protein geranyl geranylation (Figure 1).…”

Section: Discussionmentioning

confidence: 99%

Effects of HMGCR deficiency on skeletal muscle development

Gunasekaran,

Littel,

Wells

et al. 2024

Preprint

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Pathogenic variants in HMGCR were recently linked to a limb-girdle muscular dystrophy (LGMD) phenotype. The protein product HMG CoA reductase (HMGCR) catalyzes a key component of the cholesterol synthesis pathway. The two other muscle diseases associated with HMGCR, statin-associated myopathy (SAM) and autoimmune anti-HMGCR myopathy, are not inherited in a Mendelian pattern. The mechanism linking pathogenic variants in HMGCR with skeletal muscle dysfunction is unclear. We knocked down Hmgcr in mouse skeletal myoblasts, knocked down hmgcr in Drosophila, and expressed three pathogenic HMGCR variants (c.1327C>T, p.Arg443Trp; c.1522_1524delTCT, p.Ser508del; and c.1621G>A, p.Ala541Thr) in Hmgcr knockdown mouse myoblasts. Hmgcr deficiency was associated with decreased proliferation, increased apoptosis, and impaired myotube fusion. Transcriptome sequencing of Hmgcr knockdown versus control myoblasts revealed differential expression involving mitochondrial function, with corresponding differences in cellular oxygen consumption rates. Both ubiquitous and muscle-specific knockdown of hmgcr in Drosophila led to lethality. Overexpression of reference HMGCR cDNA rescued myotube fusion in knockdown cells, whereas overexpression of the pathogenic variants of HMGCR cDNA did not. These results suggest that the three HMGCR-related muscle diseases share disease mechanisms related to skeletal muscle development.

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Section: Discussionmentioning

confidence: 99%

Effects of HMGCR deficiency on skeletal muscle development

Gunasekaran,

Littel,

Wells

et al. 2024

Preprint

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Untargeted proteomics enables ultra-rapid variant prioritization in mitochondrial and other rare diseases

Hock,

Caruana,

Semcesen

et al. 2024

Preprint

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Only half of individuals with suspected rare diseases receive a definitive genetic diagnosis following genomic testing. A genetic diagnosis allows access to appropriate patient care and reduces the number of potentially unnecessary interventions and related healthcare costs. Here, we demonstrate that an untargeted quantitative mass-spectrometry approach quantifying >6,000 proteins in primary fibroblasts representing >80% of known mitochondrial disease genes can provide functional evidence for 88% of individuals in a cohort of known primary mitochondrial diseases. We profiled >90 individuals, including 28 with confirmed disease and diagnosed 6 individuals with variants in both nuclear and mitochondrial genes. Lastly, we developed an ultra-rapid proteomics pipeline using minimally invasive peripheral blood mononuclear cells to support upgrade of variant pathogenicity in as little as 54 hours in critically ill infants with suspected mitochondrial disorders. This study supports the integration of a single untargeted proteomics test into routine diagnostic practice for the diagnosis of rare genetic disorders in clinically actionable timelines, offering a paradigm shift for the functional validation of genetic variants.

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Biallelic variants inHMGCS1are a novel cause of rare rigid spine syndrome

Cited by 2 publications

References 98 publications

Effects of HMGCR deficiency on skeletal muscle development

Effects of HMGCR deficiency on skeletal muscle development

Untargeted proteomics enables ultra-rapid variant prioritization in mitochondrial and other rare diseases

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