2009
DOI: 10.1177/1352458508100031
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Reduced cerebrospinal fluid BACE1 activity in multiple sclerosis

Abstract: These results suggest an involvement of BACE1 in the MS disease process.

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Cited by 58 publications
(52 citation statements)
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References 34 publications
(41 reference statements)
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“…In fact, CSF Ab42 is the earliest nongenetic biomarker we know of in AD. Low CSF Ab42 concentrations in the absence of senile plaques have been reported in neuroinflammatory conditions, for example, bacterial meningitis [63], multiple sclerosis [64], human immunodeficiency virus (HIV)-associated dementia [65], and Lyme neuroborreliosis [66], and are often accompanied by biomarker evidence of a general reduction in APP metabolites, for example, secreted forms of APP, which is not typical of AD [50]. Besides Ab42, several other Ab isoforms are present in CSF.…”
Section: Csf Ab42mentioning
confidence: 96%
“…In fact, CSF Ab42 is the earliest nongenetic biomarker we know of in AD. Low CSF Ab42 concentrations in the absence of senile plaques have been reported in neuroinflammatory conditions, for example, bacterial meningitis [63], multiple sclerosis [64], human immunodeficiency virus (HIV)-associated dementia [65], and Lyme neuroborreliosis [66], and are often accompanied by biomarker evidence of a general reduction in APP metabolites, for example, secreted forms of APP, which is not typical of AD [50]. Besides Ab42, several other Ab isoforms are present in CSF.…”
Section: Csf Ab42mentioning
confidence: 96%
“…Interestingly, cerebrospinal fluid (CSF) from MS patients exhibits decreased BACE1 activity, suggesting decreased β2 cleavage and consequent alterations in normal VGSC α expression and localization. Low BACE1 activity in MS is linked to worsened disease severity and longer disease duration, and BACE1 expression continues to decrease throughout disease progression (132). …”
Section: Channelopathies and Pathophysiology Of Vgsc β Subunitsmentioning
confidence: 99%
“…APP is cleaved by an integral membrane aspartyl protease ( β -site APP-cleaving enzyme 1, BACE1), which results in the release of N-terminal β -cleaved soluble APP ( β -sAPP). The C-terminal fragment is further processed by γ -secretase to yield the amyloid beta (A β 42) and the APP intracellular domain [122]. APP can also undergo α -secretase-mediated cleavage, which results in the release of the solubile α -sAPP [123].…”
Section: Biomarkers Of Neuroaxonal Damage In Multiple Sclerosismentioning
confidence: 99%