Genetic ablation of acid ceramidase in Krabbe disease confirms the psychosine hypothesis and identifies a new therapeutic target

Li, Yedda; Xu, Yilin; Benitez, Bruno A.; Nagree, Murtaza S.; Dearborn, Joshua T.; Jiang, Xuntian; Guzmán, Miguel A.; Woloszynek, Josh C.; Giaramita, Alex; Yip, Bryan K.; Elsbernd, Joseph; Babcock, Michael; Lo, Melanie J.; Fowler, Stephen C.; Wozniak, David F.; Vogler, Carole; Medin, Jeffrey A.; Crawford, Brett E.; Sands, Mark S.

doi:10.1073/pnas.1912108116

Cited by 72 publications

(92 citation statements)

References 30 publications

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“…The next step in the breakdown pathway is release of the fatty acyl group from ceramide by acid ceramidase (Figure 1). Recent studies have suggested that when GALC is deficient, acid ceramidase removes the fatty acyl chain from galactosylceramide to 2 of 7 generate psychosine ( Figure 1) [4]. Psychosine is thought to be a key cytotoxic agent that is responsible for loss of oligodendrocytes and Schwann cells that is the hallmark of Krabbe disease [4].…”

Section: Introductionmentioning

confidence: 99%

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Achieving Congruence among Reference Laboratories for Absolute Abundance Measurement of Analytes for Rare Diseases: Psychosine for Diagnosis and Prognosis of Krabbe Disease

Herbst

Turgeon

Biski

et al. 2020

IJNS

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Measurement of the absolute concentration of the biomarker psychosine in dried blood spots (DBS) is useful for diagnosis and prognosis of Krabbe disease and to support newborn screening of this leukodystrophy. As for assays for more common diseases, it is important to achieve congruence when multiple clinical laboratories provide testing. Four clinical laboratories, one research laboratory, and a commercial vendor collaborated with the goal to achieve congruence in quantitative psychosine measurement in DBS. A set of DBS calibrators was prepared by a single vendor and used in each reference laboratory to make a standard curve of measured psychosine in DBS versus the stated calibrator psychosine level. Congruence between the participating five laboratories was achieved using the psychosine DBS calibrators. This allowed application of disease-specific reference ranges obtained by the reference laboratory with the most extensive data by the other reference laboratories. Congruence between multiple reference laboratories in the measurement of the absolute concentration of biomarkers in DBS (and by extension other samples) is possible by the use of a common set of DBS calibrators.

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Section: Introductionmentioning

confidence: 99%

“…Galactocerebrosidase (GALC)-catalyzed reaction and direct conversion of galactosylceramide to psychosine when GALC is deficient as proposed[4].…”

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confidence: 99%

Achieving Congruence among Reference Laboratories for Absolute Abundance Measurement of Analytes for Rare Diseases: Psychosine for Diagnosis and Prognosis of Krabbe Disease

Herbst

Turgeon

Biski

et al. 2020

IJNS

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“…In support of this hypothesis, in vitro studies show that treating cells with psychosine increases proapoptotic factors and kills oligodendrocytes (OL) 5 , Schwann cells 6,7 and neurons 8 . The long-held psychosine hypothesis was recently confirmed, in vivo, which demonstrated that the abnormal accumulation of psychosine is toxic and is generated catabolically through the deacylation of galactosylceramide by acid ceramidase 9 More than 85% of KD patients exhibit the rapidly progressive infantile-onset form of disease, which leads to death by two years of age. Although there is no cure for Krabbe disease, hematopoietic stem cell therapy (HSCT) attenuates neurologic deterioration and improves developmental gains 10 .…”

Section: Introductionmentioning

confidence: 94%

Brainstem development requires galactosylceramidase and is critical for the pathogenesis of Krabbe Disease

Weinstock

Kreher

Favret

et al. 2020

Preprint

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Krabbe disease (KD) is caused by a deficiency of galactosylceramidase (GALC), which induces demyelination and neurodegeneration due to accumulation of cytotoxic psychosine. Hematopoietic stem cell transplantation (HSCT) improves clinical outcomes in KD patients only if delivered pre-symptomatically. We hypothesized that the restricted temporal efficacy of HSCT reflects a requirement for GALC in early brain development. Using a novel Galc floxed allele, we induced ubiquitous GALC ablation (Galc-iKO) at various postnatal timepoints and identified a critical period of vulnerability to GALC ablation between P4-6. Early Galc-iKO induction caused a worse KD phenotype, higher psychosine levels, and a significantly shorter life-span. Intriguingly, GALC expression peaks during this critical developmental period. Further analysis revealed a novel cell autonomous role for GALC in the development and maturation of immature T-box-brain-1 positive brainstem neurons. These data identify a perinatal developmental period, in which neuronal GALC expression influences brainstem development that is critical for KD pathogenesis.

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“…3. Krabbe disease (OMIM #245200) is caused by a deficiency of GALC (Galactosylceramidase), which leads to the accumulation of psychosine (galactosylsphingosine), a metabolite of galactosylceramide (Li et al, 2019). Clinical symptoms often present in the 1st year of life including irritability, spasticity and developmental delay.…”

Section: Metachromatic Leukodystrophy (Mld Omim #250100)mentioning

confidence: 99%

“…Clinical symptoms often present in the 1st year of life including irritability, spasticity and developmental delay. Underlying pathology includes widespread demyelination and neurodegeneration (Li et al, 2019). HSCT appears to be of some benefit in cases of later onset or in infantile patients who have been diagnosed before symptoms begin (Wright et al, 2017).…”

Section: Metachromatic Leukodystrophy (Mld Omim #250100)mentioning

confidence: 99%

Pre-clinical Mouse Models of Neurodegenerative Lysosomal Storage Diseases

Favret

Weinstock

Feltri

et al. 2020

Front. Mol. Biosci.

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There are over 50 lysosomal hydrolase deficiencies, many of which cause neurodegeneration, cognitive decline and death. In recent years, a number of broad innovative therapies have been proposed and investigated for lysosomal storage diseases (LSDs), such as enzyme replacement, substrate reduction, pharmacologic chaperones, stem cell transplantation, and various forms of gene therapy. Murine models that accurately reflect the phenotypes observed in human LSDs are critical for the development, assessment and implementation of novel translational therapies. The goal of this review is to summarize the neurodegenerative murine LSD models available that recapitulate human disease, and the pre-clinical studies previously conducted. We also describe some limitations and difficulties in working with mouse models of neurodegenerative LSDs.

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Genetic ablation of acid ceramidase in Krabbe disease confirms the psychosine hypothesis and identifies a new therapeutic target

Cited by 72 publications

References 30 publications

Achieving Congruence among Reference Laboratories for Absolute Abundance Measurement of Analytes for Rare Diseases: Psychosine for Diagnosis and Prognosis of Krabbe Disease

Achieving Congruence among Reference Laboratories for Absolute Abundance Measurement of Analytes for Rare Diseases: Psychosine for Diagnosis and Prognosis of Krabbe Disease

Brainstem development requires galactosylceramidase and is critical for the pathogenesis of Krabbe Disease

Pre-clinical Mouse Models of Neurodegenerative Lysosomal Storage Diseases

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