2015
DOI: 10.1016/j.expneurol.2015.04.020
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Enzyme replacement therapy of a novel humanized mouse model of globoid cell leukodystrophy

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Cited by 32 publications
(36 citation statements)
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References 45 publications
(54 reference statements)
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“…(Graziano & Cardile, 2015) and only in pre-symptomatic patients (Matthes et al, 2015), we propose to investigate in deeper detail, the PN alterations in the brain of TW mouse, by proteomics coupled with bioinformatics. ER lumen is swollen and poorly decorated of ribosomes which appear slightly electron-densed.…”
Section: Analysis Of Protein Synthesis and Degradation Markersmentioning
confidence: 99%
See 1 more Smart Citation
“…(Graziano & Cardile, 2015) and only in pre-symptomatic patients (Matthes et al, 2015), we propose to investigate in deeper detail, the PN alterations in the brain of TW mouse, by proteomics coupled with bioinformatics. ER lumen is swollen and poorly decorated of ribosomes which appear slightly electron-densed.…”
Section: Analysis Of Protein Synthesis and Degradation Markersmentioning
confidence: 99%
“…Even if mutant GALC reaches lysosomes, its residual enzymatic activity would account for the catabolism of only a minimal part of GalCers. Currently, the standard of care for infant with Krabbe disease is nonspecific therapies, such as hematopoietic stem cell transplantation; positive effects have been obtained only in pre-symptomatic patients (Matthes et al, 2015) and little evidence has been observed in remyelination and reversion of neurological impairment (Graziano & Cardile, 2015). For all these reasons, mismanagement of protein folding and trafficking, proteasome impairment and ER stress are in the spotlight as a transversal key process in several neurodegenerative conditions (Freeman & Mallucci, 2016;Halliday & Mallucci, 2014;Irahara-Miyana et al, 2018).…”
mentioning
confidence: 99%
“…In cell culture studies, GALC‐deficient OLs were able to take up exogenous GALC enzyme (Luddi et al, ; Kondo et al, ). In addition, systemic GALC treatments of twi mice as well as human mutant GALC knockin mice were reported to reduce the CNS PSY accumulation (Lee et al, ; Matthes et al, ). However, current ERT therapy based on recombinant GALC ERT was not successful in stopping the death of animals from KD pathologies (Lee et al, ; Matthes et al, ).…”
Section: Therapeutic Approaches For Kdmentioning
confidence: 99%
“…In addition, systemic GALC treatments of twi mice as well as human mutant GALC knockin mice were reported to reduce the CNS PSY accumulation (Lee et al, ; Matthes et al, ). However, current ERT therapy based on recombinant GALC ERT was not successful in stopping the death of animals from KD pathologies (Lee et al, ; Matthes et al, ). The reasons for the limited efficacy of recombinant GALC ERT are reported to be its inability to cross the BBB and low cross‐correction efficiency of recombinant wild‐type (WT) GALC (Wenger et al, ; Meng et al, ; Kim, ).…”
Section: Therapeutic Approaches For Kdmentioning
confidence: 99%
“…After the success of ERT for non‐CNS LSDs, such as Gaucher's disease (Shayman, ; Marshal et al, ), a significant advance has been the development of a “humanized” mouse model of KD by inserting a human GALC cDNA containing an adult‐onset patient mutation into the murine GALC gene. Such mice were found to exhibit all the pathological hallmarks of KD, including psychosine accumulation, neuroinflammation, CNS infiltration of macrophages, astrogliosis, and demyelination (Matthes et al, ). Residual GALC activities in mouse tissues were low, and the mice had a reduced life span of 46 days.…”
Section: Current Status Of Therapy For Kdmentioning
confidence: 99%