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            Ganglioside Lysosomal Storage Disease in Cats with α-Hexosaminidase Deficiency

Cork, Linda C.; Munnell, J. F.; Lorenz, Michael D.; Murphy, Jerome V.; Baker, Henry J.; Rattazzi, Mario C.

doi:10.1126/science.404709

Cited by 154 publications

(64 citation statements)

References 8 publications

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“…In contrast to a previous study, which showed that GM2 was about 42% of the total brain ganglioside distribution in the SD cat, we show that GM2 accounts for 67% of the total ganglioside distribution in the SD cat (19). The ganglioside distribution in the SD cat in the previous study was analyzed at an earlier age (11 weeks), which could account for the lower GM2 distribution (19). For our study, we analyzed the total brain ganglioside distribution at a similar time-point in disease progression in the SD mouse, cat, and human, and we showed that GM2 accumulation in the SD cat is intermediate between the SD mouse and the SD patient.…”

Section: Discussioncontrasting

confidence: 53%

“…The SD cats were obtained from the fG M2 Baker colony and have been previously described (17,19). Sequence analysis determined that the causative mutation in this domestic shorthair SD cat resulted from a 25-base-pair inversion at the 3' end of the Hexb gene (16).…”

Section: Catsmentioning

confidence: 99%

“…While the CNS GM2 accumulation has been reported for the mouse and cat models of SD and in the patient (11,(19)(20)(21)(22), the comparative total lipid analysis has never been done. In particular, our objective was to analyze similar brain regions, at a similar phenotypic timepoint, using the same methodology to compare the total lipid distribution between mice, cats, and humans with SD.…”

Section: Introductionmentioning

confidence: 99%

“…The brain weight of the mouse is around 0.4 grams while an infantile human brain weighs around 400 grams, representing a 1000-fold difference in size (13)(14)(15). A naturally occurring, authentic model of SD in cats (fG M2 Baker) has been previously characterized and could potentially serve as an intermediate model between mouse and man (16)(17)(18)(19). Although the feline brain is closer in size and complexity to the human brain, it is not clear how the mouse and the cat animal models of SD compare to the human patient.…”

Section: Introductionmentioning

confidence: 99%

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126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

Seyfried

Baek

Martin

et al. 2009

Molecular Genetics and Metabolism

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Sandhoff disease (SD) is a glycosphingolipid (GSL) storage disease that arises from an autosomal recessive mutation in the gene for the β-subunit of β-Hexosaminidase A (Hexb gene), which catabolizes ganglioside GM2 within lysosomes. Accumulation of GM2 and asialo-GM2 (GA2) occurs primarily in the CNS, leading to neurodegeneration and brain dysfunction. We analyzed the total lipids in the brains of SD mice, cats, and humans. GM2 and GA2 were mostly undetectable in the normal mouse, cat, and human brain. The lipid abnormalities in the SD cat brain were generally intermediate to those observed in the SD mouse and the SD human brains. GM2 comprised 38%, 67%, and 87% of the total brain ganglioside distribution in the SD mice, cats, and humans, respectively. The ratio of GA2 to GM2 was 0.93, 0.13, and 0.27 in the SD mice, cats, and humans, respectively, suggesting that the relative storage of GA2 is greater in the SD mouse than in the SD cat or human. Finally, the myelin-enriched lipids, cerebrosides and sulfatides, were significantly lower in the SD brains than in the control brains. This study is the first comparative analysis of brain lipids in mice, cats, and humans with SD and will be important for designing therapies for Sandhoff disease patients.

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Section: Discussioncontrasting

confidence: 53%

Section: Catsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

Seyfried

Baek

Martin

et al. 2009

Molecular Genetics and Metabolism

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“…Therefore, deleterious mutations in the HEXB gene encoding the b-subunit of Hex molecules affect both Hex A and Hex B, producing the null (0) variant of GM2 gangliosidosis (human Sandhoff disease) and lysosomal storage of undegraded GM2 ganglioside in neurons as a major storage material. 5 In domestic animals, naturally occurring Sandhoff-like disease has been reported in only 2 canine breeds (i.e., a Golden Retriever 18 and toy Poodles 16 ) and 4 feline breeds or families (i.e., domestic cats in the United States, 4 Korat cats, 13 Japanese domestic cats, 19 and European Burmese cats 3 ). At present, the pathogenic mutations in all 4 feline families have been identified, 3,8,11,12 but not in canine breeds.…”

mentioning

confidence: 99%

Rapid and Simple Polymerase Chain Reaction—Based Diagnostic Assays for GM2 Gangliosidosis Variant 0 (Sandhoff-Like Disease) in Japanese Domestic Cats

et al. 2011

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Abstract. Polymerase chain reaction (PCR)-based assays combined with microchip electrophoresis were developed and evaluated for diagnosis and genotyping of GM2 gangliosidosis variant 0 (Sandhoff-like disease) in Japanese domestic cats. A preliminary genotyping survey was carried out in the population of Japanese domestic cats (1,015 cats in total) in southern Japan. Three kinds of assays including PCR primer-induced restriction analysis (PIRA) and mutagenically separated (MS)-PCR were carried out using blood-stained Flinders Technology Associates filter papers (FTA cards) as templates. The PCR products were analyzed by both agarose gel and microchip electrophoreses. All assays were sufficient to determine the genotypes of this disease, but MS-PCR offered the most rapid and simplest test, as it does not need the restriction enzyme step required in PCR-PIRA. The use of microchip electrophoresis in combination with FTA cards for sampling could shorten the time required for genotyping and simplify the procedure as well. The genotyping survey in the current study did not find any cats that possessed the mutant allele, suggesting that the prevalence of this allele is low (,0.1%) in southern Japan.

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Life‐Limiting Peripheral Organ Dysfunction in Feline Sandhoff Disease Emerges after Effective CNS Gene Therapy

Johnson

McCurdy

Gray‐Edwards

et al. 2023

Annals of Neurology

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ObjectiveGM2 gangliosidosis is usually fatal by 5 years of age in its 2 major subtypes, Tay‐Sachs and Sandhoff disease. First reported in 1881, GM2 gangliosidosis has no effective treatment today, and children succumb to the disease after a protracted neurodegenerative course and semi‐vegetative state. This study seeks to further develop adeno‐associated virus (AAV) gene therapy for human translation.MethodsCats with Sandhoff disease were treated by intracranial injection of vectors expressing feline β‐N‐acetylhexosaminidase, the enzyme deficient in GM2 gangliosidosis.ResultsHexosaminidase activity throughout the brain and spinal cord was above normal after treatment, with highest activities at the injection sites (thalamus and deep cerebellar nuclei). Ganglioside storage was reduced throughout the brain and spinal cord, with near complete clearance in many regions. While untreated cats with Sandhoff disease lived for 4.4 ± 0.6 months, AAV‐treated cats lived to 19.1 ± 8.6 months, and 3 of 9 cats lived >21 months. Correction of the central nervous system was so effective that significant increases in lifespan led to the emergence of otherwise subclinical peripheral disease, including megacolon, enlarged stomach and urinary bladder, soft tissue spinal cord compression, and patellar luxation. Throughout the gastrointestinal tract, neurons of the myenteric and submucosal plexuses developed profound pathology, demonstrating that the enteric nervous system was inadequately treated.InterpretationThe vector formulation in the current study effectively treats neuropathology in feline Sandhoff disease, but whole‐body targeting will be an important consideration in next‐generation approaches. ANN NEUROL 2023

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GM ₂ Ganglioside Lysosomal Storage Disease in Cats with α-Hexosaminidase Deficiency

Cited by 154 publications

References 8 publications

126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

Rapid and Simple Polymerase Chain Reaction—Based Diagnostic Assays for GM2 Gangliosidosis Variant 0 (Sandhoff-Like Disease) in Japanese Domestic Cats

Life‐Limiting Peripheral Organ Dysfunction in Feline Sandhoff Disease Emerges after Effective CNS Gene Therapy

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GM 2 Ganglioside Lysosomal Storage Disease in Cats with α-Hexosaminidase Deficiency

Cited by 154 publications

References 8 publications

126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

126. Comparative Analysis of brain lipids in Mice, Cats, and Humans with Sandhoff disease

Rapid and Simple Polymerase Chain Reaction—Based Diagnostic Assays for GM2 Gangliosidosis Variant 0 (Sandhoff-Like Disease) in Japanese Domestic Cats

Life‐Limiting Peripheral Organ Dysfunction in Feline Sandhoff Disease Emerges after Effective CNS Gene Therapy

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GM ₂ Ganglioside Lysosomal Storage Disease in Cats with α-Hexosaminidase Deficiency