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Divergent CSF τ alterations in two common tauopathies: Alzheimers disease and progressive supranuclear palsy.
- Wagshal, Dana;
- Sankaranarayanan, Sethu;
- Guss, Valerie;
- Hall, Tracey;
- Berisha, Flora;
- Lobach, Iryna;
- Karydas, Anna;
- Voltarelli, Lisa;
- Scherling, Carole;
- Heuer, Hilary;
- Tartaglia, Maria;
- Ahlijanian, Michael;
- Soares, Holly;
- Meredith, Jere;
- Kramer, Joel;
- Coppola, Giovanni;
- Boxer, Adam;
- Miller, Bruce;
- Rabinovici, Gil;
- Rosen, Howard;
- Miller, Zachary
- et al.
Published Web Location
https://doi.org/10.1136/jnnp-2014-308004Abstract
BACKGROUND: Elevated CSF τ is considered a biomarker of neuronal injury in newly developed Alzheimers disease (AD) and mild cognitive impairment (MCI) criteria. However, previous studies have failed to detect alterations of τ species in other primary tauopathies. We assessed CSF τ protein abnormalities in AD, a tauopathy with prominent Aβ pathology, and progressive supranuclear palsy (PSP), a primary tauopathy characterised by deposition of four microtubule-binding repeat (4R) τ with minimal Aβ pathology. METHODS: 26 normal control (NC), 37 AD, and 24 patients with PSP participated in the study. AD and PSP were matched for severity using the clinical dementia rating sum of boxes (CDR-sb) scores. The INNO BIA AlzBio3 multiplex immunoassay was used to measure CSF Aβ, total τ, and ptau181. Additional, novel ELISAs targeting different N-terminal and central τ epitopes were developed to examine CSF τ components and to investigate interactions between diagnostic group, demographics and genetic variables. RESULTS: PSP had lower CSF N-terminal and C-terminal τ concentrations than NC and AD measured with the novel τ ELISAs and the standard AlzBio3 τ and ptau assays. AD had higher total τ and ptau levels than NC and PSP. There was a gender by diagnosis interaction in AD and PSP for most τ species, with lower concentrations for male compared to female patients. CONCLUSIONS: CSF τ fragment concentrations are different in PSP compared with AD despite the presence of severe τ pathology and neuronal injury in both disorders. CSF τ concentration likely reflects multiple factors in addition to the degree of neuronal injury.
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