Journal Article10.1212/01.WNL.0000295996.54210.69
Disease-modifying therapies for Alzheimer disease: challenges to early intervention.
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TL;DR: Enrichment strategies for clinical trials with MCI include use of biomarkers such as amyloid imaging, MRI with demonstration of medial temporal lobe atrophy, bilateral parietal hypometabolism on PET, and reduced amyloids beta peptide and increased tau protein in CSF.
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Abstract: Prevention of Alzheimer disease (AD) is a national and global imperative. Therapy is optimally initiated when individuals are asymptomatic or exhibit mild cognitive impairment (MCI). Development of therapeutically beneficial compounds requires the creation of clinical trial methodologies for primary and secondary prevention. Populations in primary prevention trials selected only on the basis of age will have low rates of emergent MCI or AD. Epidemiologically based risk factors or biomarkers can be used to enrich trials and increase the likelihood of disease occurrence during the trial. Enrichment strategies for clinical trials with MCI include use of biomarkers such as amyloid imaging, MRI with demonstration of medial temporal lobe atrophy, bilateral parietal hypometabolism on PET, and reduced amyloid beta peptide and increased tau protein in CSF. Neuropsychological measures appropriate for trials of MCI may not be identical to those measures most suited for AD trials. Attention to these and other features of trial design, clinical assessment, and use of biomarkers is critical to improving the detection of disease-modifying effects of emerging therapies in presymptomatic or minimally symptomatic populations. The neurologic health of the growing aging population demands disease-modifying therapies and the development of methods to identify and test promising candidate agents.
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Citations
Principal component analysis of FDG PET in amnestic MCI.
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Ultraviolet–visible–near-infrared optical properties of amyloid fibrils shed light on amyloidogenesis
Jonathan Pansieri,Jonathan Pansieri,Véronique Josserand,Sun-Jae Lee,Anaëlle Rongier,Daniel Imbert,M. Sallanon,M. Sallanon,Eniko Veronika Kovari,Thomas G. Dane,Charlotte Vendrely,Charlotte Vendrely,Odette Chaix-Pluchery,Mélanie Guidetti,Julien Vollaire,Arnold Fertin,Yves Usson,Patrice Rannou,Jean-Luc Coll,C. Marquette,Vincent Forge +20 more
TL;DR: Two optical signatures of amyloid fibres—luminescence in the blue and a near-infrared signal, which can be observed in in vitro and in vivo tissues—are reported and could open the door to innovative diagnostic strategies for neurodegenerative diseases.
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Design, synthesis and evaluation of novel tacrine-multialkoxybenzene hybrids as dual inhibitors for cholinesterases and amyloid beta aggregation.
Wen Luo,Yan-Ping Li,Yan He,Shi-Liang Huang,Jia-Heng Tan,Tian-Miao Ou,Ding Li,Lian-Quan Gu,Zhi-Shu Huang +8 more
TL;DR: A new series of tacrine-multialkoxybenzene hybrids (9a-9n) were designed, synthesized and evaluated as dual inhibitors of cholinesterases (ChEs) and self-induced β-amyloid aggregation and showed higher self- induced Aβ aggregation inhibitory activity than a reference compound, curcumin.
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CSF biomarkers, impairment of cerebral hemodynamics and degree of cognitive decline in Alzheimer's and mixed dementia
Alessandro Stefani,Giuseppe Sancesario,Mariangela Pierantozzi,Giorgia Leone,Salvatore Galati,Atticus H. Hainsworth,Marina Diomedi +6 more
TL;DR: It is indicated that hemodynamic impairment is a critical marker of cognitive decline and supports once more the hypothesis of a significant pathigenic role of vascular damage in AD.
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