Developmental Neuropathology 2018
DOI: 10.1002/9781119013112.ch29
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Sphingolipidoses and Related Disorders

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Cited by 3 publications
(4 citation statements)
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“…This could at least in part explain why GALC represents a major risk locus for MS. As outlined, Krabbe's disease manifests when two copies of mutated alleles are inherited, an event that occurs with an incidence of 1:100,000-200,000 births. The carrier frequency is 1:150 (Laquerriere et al, 2018). GALC ± animals have been demonstrated to be clinically similar to WT animals at 3 months of age, exhibiting no accumulation of psychosine.…”
Section: Common G Ene Ti C Alter Ati On S Among Ms and Inborn S Phimentioning
confidence: 96%
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“…This could at least in part explain why GALC represents a major risk locus for MS. As outlined, Krabbe's disease manifests when two copies of mutated alleles are inherited, an event that occurs with an incidence of 1:100,000-200,000 births. The carrier frequency is 1:150 (Laquerriere et al, 2018). GALC ± animals have been demonstrated to be clinically similar to WT animals at 3 months of age, exhibiting no accumulation of psychosine.…”
Section: Common G Ene Ti C Alter Ati On S Among Ms and Inborn S Phimentioning
confidence: 96%
“…In any case, GALC deficiency impairs psychosine catabolism provoking its accumulation that is deeply toxic for oligodendrocytes and also for neurons. Over 100 mutations affecting GALC, that spans 60.2 kb, have been discovered; in Europe, the most common is a 30 kb deletion mapped from 11th to 17th exon (502T/del) (Laquerriere et al, 2018). Different mutations affect GALC functionality in different way: by impairing the conformation of the catalytic site, by altering the enzyme folding, processing or localization, or by distorting its ability to associate with coactivators (Spratley et al, 2016).…”
Section: Common G Ene Ti C Alter Ati On S Among Ms and Inborn S Phimentioning
confidence: 99%
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“…Despite the very low incidence of KD [1:100,000 live births in the United States and Europe, with a pick of incidence recorded in Sweden (1:39,000)] [ 19 , 20 ], heterozygous carriers are estimated to be frequent in Caucasians (1:150) [ 21 ] and are suggested to carry a risk for neurological disorder onset [ 5 ]. In fact, despite carriers of recessive disorders not being clinically ill, they may present non-physiological biochemical and molecular traits that may predispose them to develop a disease state [ 16 ].…”
Section: Introductionmentioning
confidence: 99%