Functional characterization of novel <i>MFSD8</i> pathogenic variants anticipates neurological involvement in juvenile isolated maculopathy

Bauwens, Miriam; Storch, Stephan; Weisschuh, Nicole; Groote, Chantal Ceuterick‐de; Rycke, Riet De; Guillemyn, Brecht; Jaegere, Sarah De; Coppieters, Frauke; Coster, Rudy Van; Leroy, Bart P.; Baere, Elfride De

doi:10.1111/cge.13673

Cited by 10 publications

(4 citation statements)

References 34 publications

(98 reference statements)

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“…Remarkably, a similar situation has been described for other genes causative for lysosomal storage diseases. While variants in genes associated with neuronal ceroid lipofuscinosis ( CLN3 (OMIM 607042), CLN5 (OMIM 608102), and MFSD8 / CLN7 (OMIM611124)) typically lead to severe neuronal dysfunction and lysosomal storage in neurons and the peripheral tissues, some variants present with isolated retina disease (Bauwens et al 2020 ; Khan et al 2017 ; Ku et al 2017 ; Magliyah et al 2021 ). Similarly, variants in HGSNAT (OMIM 610453) are associated with mucopolysaccharidosis in the vast majority of patients, but isolated retina degeneration has also been described (Haer-Wigman et al 2015 ).…”

Section: Discussionmentioning

confidence: 99%

Usher syndrome type IV: clinically and molecularly confirmed by novel ARSG variants

et al. 2022

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Usher syndrome (USH) is an autosomal recessively inherited disease characterized by sensorineural hearing loss (SNHL) and retinitis pigmentosa (RP) with or without vestibular dysfunction. It is highly heterogeneous both clinically and genetically. Recently, variants in the arylsulfatase G (ARSG) gene have been reported to underlie USH type IV. This distinct type of USH is characterized by late-onset RP with predominantly pericentral and macular changes, and late onset SNHL without vestibular dysfunction. In this study, we describe the USH type IV phenotype in three unrelated subjects. We identified three novel pathogenic variants, two novel likely pathogenic variants, and one previously described pathogenic variant in ARSG. Functional experiments indicated a loss of sulfatase activity of the mutant proteins. Our findings confirm that ARSG variants cause the newly defined USH type IV and support the proposed extension of the phenotypic USH classification.

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Section: Discussionmentioning

confidence: 99%

Usher syndrome type IV: clinically and molecularly confirmed by novel ARSG variants

et al. 2022

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“…There is emerging evidence for gain-of-function caused by CLN7 mutation in other neurodegenerative spectrum diseases where CLN7/MFSD8 mutation has been shown to contribute to ALS/FTD (20,36). Some allelic mutations in CLN7 can contribute to retinopathies including retinitis pigmentosa and macular dystrophy (37)(38)(39). CLN7 has been shown to co-localize with post-synaptic density marker 95 (PSD-95) in the mouse retina indicating that it may play more complex roles in specialist neural cell-types (39).…”

Section: Discussionmentioning

confidence: 99%

CLN7 mutation causes aberrant redistribution of protein isoforms and contributes to Batten disease pathobiology

Sharaireh

Guevara-Ferrer

Herranz-Martín

et al. 2022

Preprint

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The variant late infantile form of the inherited neurodegenerative Batten disease (BD) is caused by mutations in the CLN7/MFSD8 gene and represents a strong candidate for gene therapy. Post-natal intracerebral administration of AAV9-hCLN7 to Cln7Δex2 knockout mice resulted in extended lifespan but dose escalation resulted in reduced acuity in neurophysiology tests, cerebral atrophy and elevated neuroinflammation. Comparing patient and control iPSC-derived neural progenitor cells (iNPC) we discovered that CLN7 localizes to the nucleus as well as the endolysosomal network and is differentially distributed in BD iNPC. Proteomics identified a profound nuclear defect in BD iNPC that compounds with mitochondrial and lysosomal metabolic defects resulting in elevated apoptosis. We further identified a 50kDa common nuclear CLN7 isoform and a 37kDa isoform that accumulates only in BD iNPC nuclei. Our findings suggest that successful treatment of CLN7 BD will require combinatorial therapies addressing both loss and aberrant gain of protein function.

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“…Whether maculopathy precedes cognitive impairment in CLN3 disease, or if both visual impairment and mild cognitive failure occur at around the same time ( 98 ) is still the subject of discussion. Biallelic variants of the MFSD8 gene may be associated with isolated juvenile maculopathy, evolving into a slowly progressive encephalopathy with protracted course ( 99 ). Conversely, late visual impairment, or even long lasting preservation of visual function can occur in CLN5 and CLN6 diseases ( 92 , 100 ).…”

Section: Selected Clinical Featuresmentioning

confidence: 99%

Neuronal Ceroid Lipofuscinosis: The Multifaceted Approach to the Clinical Issues, an Overview

Simonati

Williams

2022

Front. Neurol.

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The main aim of this review is to summarize the current state-of-art in the field of childhood Neuronal Ceroid Lipofuscinosis (NCL), a group of rare neurodegenerative disorders. These are genetic diseases associated with the formation of toxic endo-lysosomal storage. Following a brief historical review of the evolution of NCL definition, a clinically-oriented approach is used describing how the early symptoms and signs affecting motor, visual, cognitive domains, and including seizures, may lead clinicians to a rapid molecular diagnosis, avoiding the long diagnostic odyssey commonly observed. We go on to focus on recent advances in NCL research and summarize contributions to knowledge of the pathogenic mechanisms underlying NCL. We describe the large variety of experimental models which have aided this research, as well as the most recent technological developments which have shed light on the main mechanisms involved in the cellular pathology, such as apoptosis and autophagy. The search for innovative therapies is described. Translation of experimental data into therapeutic approaches is being established for several of the NCLs, and one drug is now commercially available. Lastly, we show the importance of palliative care and symptomatic treatments which are still the main therapeutic interventions.

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Functional characterization of novel MFSD8 pathogenic variants anticipates neurological involvement in juvenile isolated maculopathy

Cited by 10 publications

References 34 publications

Usher syndrome type IV: clinically and molecularly confirmed by novel ARSG variants

Usher syndrome type IV: clinically and molecularly confirmed by novel ARSG variants

CLN7 mutation causes aberrant redistribution of protein isoforms and contributes to Batten disease pathobiology

Neuronal Ceroid Lipofuscinosis: The Multifaceted Approach to the Clinical Issues, an Overview

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