GM1 Gangliosidosis: Mechanisms and Management

Rha, Allisandra K; Maguire, Anne; Martin, Douglas R.

doi:10.2147/tacg.s206076

Cited by 34 publications

(44 citation statements)

References 183 publications

(585 reference statements)

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“…Biomarkers are also essential for monitoring and assessing outcomes in ongoing clinical trials [ 6 ]. Currently, FDA-approved treatments for patients with GM1 gangliosidosis and sialidosis [ 31 , 32 ] are limited to supportive care. The efficacy of substrate reduction therapy, pharmacological chaperones, enzyme replacement therapy, stem cell transplantation, and gene therapy for GM1 gangliosidosis is currently being evaluated [ 6 , 33 ].…”

Section: Discussionmentioning

confidence: 99%

Fluorescent In Situ Staining and Flow Cytometric Procedures as New Pre-Diagnostic Tests for Sialidosis, GM1 Gangliosidosis and Niemann–Pick Type C

et al. 2022

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Background: Early diagnosis is essential in the field of lysosomal storage disorders for the proper management of patients and for starting therapies before irreversible damage occurs, particularly in neurodegenerative conditions. Currently, specific biomarkers for the diagnosis of lysosomal storage disorders are lacking in routine laboratory practice, except for enzymatic tests, which are available only in specialized metabolic centers. Recently, we established a method for measuring and verifying changes in GM1 ganglioside levels in peripheral blood lymphocytes in patients with GM1 gangliosidosis. However, fresh blood is not always available, and using frozen/thawed lymphocytes can lead to inaccurate results. Methods: We used frozen/thawed fibroblasts obtained from stored biopsies to explore the feasibility of fluorescent imaging and flow-cytometric methods to track changes in storage materials in fibroblasts from patients with three lysosomal neurodegenerative conditions: GM1 gangliosidosis, Sialidosis, and Niemann–Pick type C. We used specific markers for each pathology. Results and Conclusions: We demonstrated that with our methods, it is possible to clearly distinguish the levels of accumulated metabolites in fibroblasts from affected and unaffected patients for all the three pathologies considered. Our methods proved to be rapid, sensitive, unbiased, and potentially applicable to other LSDs.

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Section: Discussionmentioning

confidence: 99%

Fluorescent In Situ Staining and Flow Cytometric Procedures as New Pre-Diagnostic Tests for Sialidosis, GM1 Gangliosidosis and Niemann–Pick Type C

et al. 2022

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“…The progressive nature of the neurological disease in GM1 gangliosidosis requires close monitoring. Biomarkers in blood, urine, and CSF biomarkers may be potentially useful in this regard (Gray-Edwards et al, 2017a,b;Rha et al, 2021). Disease progression can also be monitored using minimally invasive neuroimaging.…”

Section: Clinical Manifestationsmentioning

confidence: 99%

“…Generalizations based on crystallographic structure of the β-GAL enzyme have been attempted (Ohto et al, 2012). Mutations associated with type I/infantile onset GM1 gangliosidosis, for the most part, are located in the core protein region causing β-gal instability, whereas mutations associated with milder phenotypes, such as types II and III GM1 gangliosidosis, tend to be on the protein surface (Morita et al, 2009;Ohto et al, 2012;Rha et al, 2021). Recently, the determination of the 3D structure of murine β-gal in complex with PPCA has revealed that some mutations at conserved amino acid residues found in GM1 gangliosidosis patients affect formation of the complex (Gorelik et al, 2021).…”

Section: Genotypesmentioning

confidence: 99%

“…Bi-allelic mutations in GLB1 result in a reduction in β-GAL activity and the build-up of GM1 ganglioside in multiple tissues including the brain (Brunetti-Pierri and Scaglia, 2008;Karimzadeh et al, 2017;Rha et al, 2021) leading to severe neurodegeneration resulting in morbidity and premature mortality (Ferreira and Gahl, 2017). More than 200 diseasecausing mutations have been identified across the GLB1 gene, particularly in exons 2, 6, 15, and 16 (Figure 2).…”

Section: Introductionmentioning

confidence: 99%

“…Comprehensive reviews of GM1 gangliosidosis have been recently published (Regier et al, 1993;Breiden and Sandhoff, 2019;Lawrence et al, 2019;Lang et al, 2020;Rha et al, 2021). In this mini review, we will focus on the clinical spectrum of disease and genetic variants, our current understanding of disease pathogenesis, the utility of available animal models and approaches to therapy for these devastating disorders.…”

Section: Introductionmentioning

confidence: 99%

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GM1 Gangliosidosis—A Mini-Review

et al. 2021

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GM1 gangliosidosis is a progressive, neurosomatic, lysosomal storage disorder caused by mutations in the GLB1 gene encoding the enzyme β-galactosidase. Absent or reduced β-galactosidase activity leads to the accumulation of β-linked galactose-containing glycoconjugates including the glycosphingolipid (GSL) GM1-ganglioside in neuronal tissue. GM1-gangliosidosis is classified into three forms [Type I (infantile), Type II (late-infantile and juvenile), and Type III (adult)], based on the age of onset of clinical symptoms, although the disorder is really a continuum that correlates only partially with the levels of residual enzyme activity. Severe neurocognitive decline is a feature of Type I and II disease and is associated with premature mortality. Most of the disease-causing β-galactosidase mutations reported in the literature are clustered in exons 2, 6, 15, and 16 of the GLB1 gene. So far 261 pathogenic variants have been described, missense/nonsense mutations being the most prevalent. There are five mouse models of GM1-gangliosidosis reported in the literature generated using different targeting strategies of the Glb1 murine locus. Individual models differ in terms of age of onset of the clinical, biochemical, and pathological signs and symptoms, and overall lifespan. However, they do share the major abnormalities and neurological symptoms that are characteristic of the most severe forms of GM1-gangliosidosis. These mouse models have been used to study pathogenic mechanisms, to identify biomarkers, and to evaluate therapeutic strategies. Three GLB1 gene therapy trials are currently recruiting Type I and Type II patients (NCT04273269, NCT03952637, and NCT04713475) and Type II and Type III patients are being recruited for a trial utilizing the glucosylceramide synthase inhibitor, venglustat (NCT04221451).

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Glycosphingolipids within membrane contact sites influence their function as signaling hubs in neurodegenerative diseases

et al. 2023

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Intracellular organelles carry out many of their functions by engaging in extensive interorganellar communication through specialized membrane contact sites (MCSs) formed where two organelles tether to each other or to the plasma membrane (PM) without fusing. In recent years, these ubiquitous membrane structures have emerged as central signaling hubs that control a multitude of cellular pathways, ranging from lipid metabolism/transport to the exchange of metabolites and ions (i.e., Ca2+), and general organellar biogenesis. The functional crosstalk between juxtaposed membranes at MCSs relies on a defined composite of proteins and lipids that populate these microdomains in a dynamic fashion. This is particularly important in the nervous system, where alterations in the composition of MCSs have been shown to affect their functions and have been implicated in the pathogenesis of neurodegenerative diseases. In this review, we focus on the MCSs that are formed by the tethering of the endoplasmic reticulum (ER) to the mitochondria, the ER to the endo‐lysosomes and the mitochondria to the lysosomes. We highlight how glycosphingolipids that are aberrantly processed/degraded and accumulate ectopically in intracellular membranes and the PM change the topology of MCSs, disrupting signaling pathways that lead to neuronal demise and neurodegeneration. In particular, we focus on neurodegenerative lysosomal storage diseases linked to altered glycosphingolipid catabolism.

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GM1 Gangliosidosis: Mechanisms and Management

Cited by 34 publications

References 183 publications

Fluorescent In Situ Staining and Flow Cytometric Procedures as New Pre-Diagnostic Tests for Sialidosis, GM1 Gangliosidosis and Niemann–Pick Type C

Fluorescent In Situ Staining and Flow Cytometric Procedures as New Pre-Diagnostic Tests for Sialidosis, GM1 Gangliosidosis and Niemann–Pick Type C

GM1 Gangliosidosis—A Mini-Review

Glycosphingolipids within membrane contact sites influence their function as signaling hubs in neurodegenerative diseases

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