Objectives. Cerebral Amyloid Angiopathy-related inflammation (CAA-ri) is a rare meningoencephalitis characterized by vasogenic edema and multiple cortical/subcortical microbleeds, shearing several aspects with the recently defined Amyloid-Related Imaging Abnormalities (ARIA) occurring in Alzheimer's disease (AD) passive immunization therapies. Here, we investigated the specific role of autologous anti-Aβ antibodies and Tissue Factor Pathway Inhibitor (TFPI) in order to identify novel biomarkers for ARIA. Methods. By a multicenter case-control study in 100 subjects, using a novel ultra-sensitive technique (patent application pending), we evaluated the anti-Aβ autoantibodies and TFPI, as a marker of cerebrovascular impairment, in the CSF of CAA-ri, CAA, AD, MS and controls. Levels of circulating Aβ40 (cAβ40), cAβ42, tau, P-181 tau and APOE4 genotype were also investigated. Results. We demonstrated a direct involvement of anti-Aβ autoantibodies during the occurrence of ARIA, showing that their concentration is specifically increased during the acute phase of CAA-ri (apCAA-ri) and progressively reduced with clinical and radiological remission. Moreover, a strong correlation with the increased mobilization of cAβ40 and cAβ42 during apCAA-ri was shown, followed by their return to control levels and reduced tau and P-181 tau after remission. A parallel increase of the endothelial impairment marker TFPI was also confirmed both in AD and apCAA-ri, in particular in those patients carrying the APOE4 allele . Conclusions. Our data strongly support the hypothesis that the pathogenesis of CAA-ri is mediated by a selective autoimmune reaction against cerebro-vascular Aβ, directly related to autoantibodies concentration and cAβ overloading. The parallel increase of TFPI during apCAA-ri may finally allows to speculate that ARIA is a temporary but necessary event preceding the downstream beneficial Aß-clearance effects of disease modifying therapies (DMTs), further strengthening the increased susceptibility to vascular damage by the therapeutically-administered antibodies. Given the similarities between spontaneous ARIA which develops in CAA-ri and that induced through immunization strategies, CSF anti-Aβ autoantibodies and TFPI may be proposed as useful biomarkers for the diagnosis of CAA-ri, and for a better stratification (at baseline) and the monitoring of ARIA during the upcoming DMTs prevention trials
Piazza, F., Greenberg, S., Savoiardo, M., Nitrini, R., Sakaguchi, H., Giaccone, G., et al. (2013). Anti-AB autoantibodies and endothelial damage during amyloid-related imaging abnormalities (ARIA): report from the Inflammatory Cerebral Amyloid Angiopathy and Alzheimer's disease Biomarkers Collaborative Network. NEUROLOGICAL SCIENCES, 34(supplemento), 97-98.
Anti-AB autoantibodies and endothelial damage during amyloid-related imaging abnormalities (ARIA): report from the Inflammatory Cerebral Amyloid Angiopathy and Alzheimer's disease Biomarkers Collaborative Network
PIAZZA, FABRIZIOPrimo
;FERRARESE, CARLO;DiFrancesco, J;
2013
Abstract
Objectives. Cerebral Amyloid Angiopathy-related inflammation (CAA-ri) is a rare meningoencephalitis characterized by vasogenic edema and multiple cortical/subcortical microbleeds, shearing several aspects with the recently defined Amyloid-Related Imaging Abnormalities (ARIA) occurring in Alzheimer's disease (AD) passive immunization therapies. Here, we investigated the specific role of autologous anti-Aβ antibodies and Tissue Factor Pathway Inhibitor (TFPI) in order to identify novel biomarkers for ARIA. Methods. By a multicenter case-control study in 100 subjects, using a novel ultra-sensitive technique (patent application pending), we evaluated the anti-Aβ autoantibodies and TFPI, as a marker of cerebrovascular impairment, in the CSF of CAA-ri, CAA, AD, MS and controls. Levels of circulating Aβ40 (cAβ40), cAβ42, tau, P-181 tau and APOE4 genotype were also investigated. Results. We demonstrated a direct involvement of anti-Aβ autoantibodies during the occurrence of ARIA, showing that their concentration is specifically increased during the acute phase of CAA-ri (apCAA-ri) and progressively reduced with clinical and radiological remission. Moreover, a strong correlation with the increased mobilization of cAβ40 and cAβ42 during apCAA-ri was shown, followed by their return to control levels and reduced tau and P-181 tau after remission. A parallel increase of the endothelial impairment marker TFPI was also confirmed both in AD and apCAA-ri, in particular in those patients carrying the APOE4 allele . Conclusions. Our data strongly support the hypothesis that the pathogenesis of CAA-ri is mediated by a selective autoimmune reaction against cerebro-vascular Aβ, directly related to autoantibodies concentration and cAβ overloading. The parallel increase of TFPI during apCAA-ri may finally allows to speculate that ARIA is a temporary but necessary event preceding the downstream beneficial Aß-clearance effects of disease modifying therapies (DMTs), further strengthening the increased susceptibility to vascular damage by the therapeutically-administered antibodies. Given the similarities between spontaneous ARIA which develops in CAA-ri and that induced through immunization strategies, CSF anti-Aβ autoantibodies and TFPI may be proposed as useful biomarkers for the diagnosis of CAA-ri, and for a better stratification (at baseline) and the monitoring of ARIA during the upcoming DMTs prevention trials
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