Cited by Alzheimer’s disease: Insights and new prospects in disease pathophysiology, biomarkers and disease-modifying drugs

Donanemab in Early Symptomatic Alzheimer Disease DOI

John R. Sims,

Jennifer A. Zimmer,

Cynthia Evans

и другие.

JAMA, Год журнала: 2023, Номер 330(6), С. 512 - 512

Опубликована: Июль 17, 2023

Importance There are limited efficacious treatments for Alzheimer disease. Objective To assess efficacy and adverse events of donanemab, an antibody designed to clear brain amyloid plaque. Design, Setting, Participants Multicenter (277 medical research centers/hospitals in 8 countries), randomized, double-blind, placebo-controlled, 18-month phase 3 trial that enrolled 1736 participants with early symptomatic disease (mild cognitive impairment/mild dementia) low/medium or high tau pathology based on positron emission tomography imaging from June 2020 November 2021 (last patient visit primary outcome April 2023). Interventions were randomized a 1:1 ratio receive donanemab (n = 860) placebo 876) intravenously every 4 weeks 72 weeks. the group switched blinded manner if dose completion criteria met. Main Outcomes Measures The was change integrated Disease Rating Scale (iADRS) score baseline 76 (range, 0-144; lower scores indicate greater impairment). 24 gated outcomes (primary, secondary, exploratory), including secondary sum boxes Clinical Dementia (CDR-SB) 0-18; higher Statistical testing allocated α .04 population outcomes, remainder (.01) combined outcomes. Results Among (mean age, 73.0 years; 996 [57.4%] women; 1182 [68.1%] 552 [31.8%] pathology), 1320 (76%) completed trial. Of 23 statistically significant. least-squares mean (LSM) iADRS at −6.02 (95% CI, −7.01 −5.03) −9.27 −10.23 −8.31) (difference, 3.25 [95% 1.88-4.62]; P &lt; .001) −10.2 −11.22 −9.16) −13.1 −14.10 −12.13) 2.92 1.51-4.33]; population. LSM CDR-SB 1.20 1.00-1.41) 1.88 1.68-2.08) −0.67 −0.95 −0.40]; 1.72 1.53-1.91) 2.42 2.24-2.60) −0.7 −0.45]; Amyloid-related abnormalities edema effusion occurred 205 (24.0%; 52 symptomatic) 18 (2.1%; 0 during study) infusion-related reactions 74 (8.7%) (0.5%) placebo. Three deaths 1 considered treatment related. Conclusions Relevance pathology, significantly slowed clinical progression those Trial Registration ClinicalTrials.gov Identifier: NCT04437511

Язык: Английский

Процитировано

1130

Two Randomized Phase 3 Studies of Aducanumab in Early Alzheimer’s Disease DOI

Samantha Budd Haeberlein,

Paul Aisen,

Frederik Barkhof

и другие.

The Journal of Prevention of Alzheimer s Disease, Год журнала: 2022, Номер unknown

Опубликована: Янв. 1, 2022

Alzheimer's disease is a progressive, irreversible, and fatal for which accumulation of amyloid beta thought to play key role in pathogenesis. Aducanumab human monoclonal antibody directed against aggregated soluble insoluble forms beta.We evaluated the efficacy safety aducanumab early disease.EMERGE ENGAGE were two randomized, double-blind, placebo-controlled, global, phase 3 studies patients with disease.These involved 348 sites 20 countries.Participants included 1638 (EMERGE) 1647 (ENGAGE) (aged 50-85 years, confirmed pathology) who met clinical criteria mild cognitive impairment due or dementia, 1812 (55.2%) completed study.Participants randomly assigned 1:1:1 receive low dose (3 6 mg/kg target dose), high (10 placebo via IV infusion once every 4 weeks over 76 weeks.The primary outcome measure was change from baseline week 78 on Clinical Dementia Rating Sum Boxes (CDR-SB), an integrated scale that assesses both function cognition. Other measures assessments; secondary tertiary outcomes assessed cognition, function, behavior; biomarker endpoints.EMERGE halted based futility analysis data pooled first approximately 50% enrolled patients; subsequent analyses larger set collected up declaration followed prespecified statistical analyses. The endpoint EMERGE (difference -0.39 high-dose vs [95% CI, -0.69 -0.09; P=.012; 22% decrease]) but not 0.03, -0.26 0.33; P=.833; 2% increase]). Results substudies engagement dose-dependent reduction markers pathophysiology. most common adverse event amyloid-related imaging abnormalities-edema.Data demonstrated statistically significant across all four endpoints. did meet its A dose- time-dependent pathophysiological observed trials.

Язык: Английский

Процитировано

776

The amyloid hypothesis in Alzheimer disease: new insights from new therapeutics DOI

Eric Karran, Bart De Strooper

Nature Reviews Drug Discovery, Год журнала: 2022, Номер 21(4), С. 306 - 318

Опубликована: Фев. 17, 2022

Язык: Английский

Процитировано

485

Revised criteria for diagnosis and staging of Alzheimer's disease: Alzheimer's Association Workgroup DOI

Clifford R. Jack,

J. Scott Andrews,

Thomas G. Beach

и другие.

Alzheimer s & Dementia, Год журнала: 2024, Номер 20(8), С. 5143 - 5169

Опубликована: Июнь 27, 2024

Abstract The National Institute on Aging and the Alzheimer's Association convened three separate work groups in 2011 single 2012 2018 to create recommendations for diagnosis characterization of disease (AD). present document updates research framework response several recent developments. Defining diseases biologically, rather than based syndromic presentation, has long been standard many areas medicine (e.g., oncology), is becoming a unifying concept common all neurodegenerative diseases, not just AD. consistent with this principle. Our intent objective criteria staging AD, incorporating advances biomarkers, serve as bridge between clinical care. These are intended provide step‐by‐step practice guidelines workflow or specific treatment protocols, but general principles inform AD that reflect current science. Highlights We define (AD) be biological process begins appearance neuropathologic change (ADNPC) while people asymptomatic. Progression burden leads later progression symptoms. Early‐changing Core 1 biomarkers (amyloid positron emission tomography [PET], approved cerebrospinal fluid accurate plasma [especially phosphorylated tau 217]) map onto either amyloid beta tauopathy pathway; however, these presence ADNPC more generally (i.e., both neuritic plaques tangles). An abnormal biomarker result sufficient establish decision making throughout continuum. Later‐changing 2 (biofluid PET) can prognostic information, when abnormal, will increase confidence contributing integrated scheme described accommodates fact copathologies, cognitive reserve, resistance may modify relationships stages.

Язык: Английский

Процитировано

464

The Alzheimer's Association appropriate use recommendations for blood biomarkers in Alzheimer's disease DOI

Oskar Hansson, Rebecca M. Edelmayer, Adam L. Boxer

и другие.

Alzheimer s & Dementia, Год журнала: 2022, Номер 18(12), С. 2669 - 2686

Опубликована: Июль 31, 2022

Abstract Blood‐based markers (BBMs) have recently shown promise to revolutionize the diagnostic and prognostic work‐up of Alzheimer's disease (AD), as well improve design interventional trials. Here we discuss in detail further research needed be performed before widespread use BBMs. We already now recommend BBMs (pre‐)screeners identify individuals likely AD pathological changes for inclusion trials evaluating disease‐modifying therapies, provided status is confirmed with positron emission tomography (PET) or cerebrospinal fluid (CSF) testing. also encourage studying longitudinal BBM ongoing future However, should not yet used primary endpoints pivotal Further, cautiously start using specialized memory clinics part patients cognitive symptoms results whenever possible CSF PET. Additional data are stand‐alone markers, considering care.

Язык: Английский

Процитировано

361

Blood-based biomarkers for Alzheimer's disease: towards clinical implementation DOI

Charlotte E. Teunissen, Inge M.W. Verberk, Elisabeth H. Thijssen

и другие.

The Lancet Neurology, Год журнала: 2021, Номер 21(1), С. 66 - 77

Опубликована: Ноя. 25, 2021

Язык: Английский

Процитировано

354

Head-to-Head Comparison of 8 Plasma Amyloid-β 42/40 Assays in Alzheimer Disease DOI

Shorena Janelidze,

Charlotte E. Teunissen, Henrik Zetterberg

и другие.

JAMA Neurology, Год журнала: 2021, Номер 78(11), С. 1375 - 1375

Опубликована: Сен. 20, 2021

Blood-based tests for brain amyloid-β (Aβ) pathology are needed widespread implementation of Alzheimer disease (AD) biomarkers in clinical care and to facilitate patient screening monitoring treatment responses trials.To compare the performance plasma Aβ42/40 measured using 8 different Aβ assays when detecting abnormal status patients with early AD.This study included 182 cognitively unimpaired participants 104 mild cognitive impairment from BioFINDER cohort who were enrolled at 3 hospitals Sweden underwent positron emission tomography (PET) imaging cerebrospinal fluid (CSF) collection 2010 2014. Plasma was an immunoprecipitation-coupled mass spectrometry developed Washington University (IP-MS-WashU), antibody-free liquid chromatography MS by Araclon (LC-MS-Arc), immunoassays Roche Diagnostics (IA-Elc); Euroimmun (IA-EI); Amsterdam Medical Center, ADx Neurosciences, Quanterix (IA-N4PE). also IP-MS-based method Shimadzu 200 (IP-MS-Shim) Gothenburg (IP-MS-UGOT) another immunoassay (IA-Quan) among 227 participants. For validation, 122 (51 normal, 51 impairment, 20 AD dementia) Disease Neuroimaging Initiative Aβ-PET assessments IP-MS-WashU, IP-MS-Shim, IP-MS-UGOT, IA-Elc, IA-N4PE, IA-Quan assays.Discriminative accuracy quantified CSF status.A total 408 this study. In cohort, mean (SD) age 71.6 (5.6) years 49.3% women. When identifying whole IP-MS-WashU showed significantly higher (area under receiver operating characteristic curve [AUC], 0.86; 95% CI, 0.81-0.90) than LC-MS-Arc Aβ42/40, IA-Elc IA-EI IA-N4PE (AUC range, 0.69-0.78; P < .05). performed better IP-MS-UGOT (AUC, 0.84 vs 0.68 0.64, respectively; .001), while there no difference AUCs between IP-MS-Shim (0.87 0.83; = .16) 2 subcohorts where these available. The results similar as outcome. IPMS-WashU IPMS-Shim highest coefficients correlations (r 0.56-0.65). replicated (mean [SD] age, 72.4 [5.4] years; 43.4% women), assay but not assay.The independent cohorts indicate that certain MS-based methods most pathology.

Язык: Английский

Процитировано

320

Head-to-head comparison of 10 plasma phospho-tau assays in prodromal Alzheimer’s disease DOI

Shorena Janelidze,

Divya Bali, Nicholas J. Ashton

и другие.

Brain, Год журнала: 2022, Номер 146(4), С. 1592 - 1601

Опубликована: Сен. 10, 2022

Plasma phospho-tau (p-tau) species have emerged as the most promising blood-based biomarkers of Alzheimer's disease. Here, we performed a head-to-head comparison p-tau181, p-tau217 and p-tau231 measured using 10 assays to detect abnormal brain amyloid-β (Aβ) status predict future progression dementia. The study included 135 patients with baseline diagnosis mild cognitive impairment (mean age 72.4 years; 60.7% women) who were followed for an average 4.9 years. Seventy-one participants had Aβ-status (i.e. CSF Aβ42/40) at baseline; 45 these Aβ-positive progressed dementia during follow-up. P-tau concentrations determined in plasma CSF. P-tau217 p-tau181 both immunoassays developed by Lilly Research Laboratories (Lilly) mass spectrometry Washington University (WashU). was also analysed Simoa immunoassay Janssen Development (Janss). P-tau181 from ADxNeurosciences (ADx), Lumipulse Fujirebio (Fuji) Splex Mesoscale Discovery (Splex). Both quantified Gothenburg (UGOT). We found that spectrometry-based (p-tau217WashU) exhibited significantly better performance than all other p-tau when detecting Aβ [area under curve (AUC) = 0.947; Pdiff < 0.015] or (AUC 0.932; 0.027). Among immunoassays, p-tau217Lilly highest AUCs (0.886-0.889), which not different p-tau217Janss, p-tau181ADx p-tau181WashU (AUCrange 0.835-0.872; > 0.09), but higher compared AUC p-tau231UGOT, p-tau181Lilly, p-tau181UGOT, p-tau181Fuji p-tau181Splex 0.642-0.813; ≤ 0.029). Correlations between values strongest p-tau217WashU (R 0.891) 0.755; 0.003 versus p-tau217WashU) weak moderate rest (Rrange 0.320-0.669). In conclusion, our findings suggest among tested assays, measures perform best identifying those will subsequently progress Several (p-tau217Lilly, p-tau181WashU) showed relatively high consistent accuracy across outcomes. results further indicate performing metrics rival gold standards Aβ-PET If validated, significant impacts diagnosis, screening treatment future.

Язык: Английский

Процитировано

282

Tau biomarkers in Alzheimer's disease: towards implementation in clinical practice and trials DOI

Rik Ossenkoppele, Rik van der Kant, Oskar Hansson

и другие.

The Lancet Neurology, Год журнала: 2022, Номер 21(8), С. 726 - 734

Опубликована: Май 25, 2022

Язык: Английский

Процитировано

279

Differential roles of Aβ42/40, p-tau231 and p-tau217 for Alzheimer’s trial selection and disease monitoring DOI

Nicholas J. Ashton, Shorena Janelidze, Niklas Mattsson

и другие.

Nature Medicine, Год журнала: 2022, Номер 28(12), С. 2555 - 2562

Опубликована: Дек. 1, 2022

Abstract Blood biomarkers indicative of Alzheimer’s disease (AD) pathology are altered in both preclinical and symptomatic stages the disease. Distinctive may be optimal for identification AD or monitoring progression. that correlate with changes cognition atrophy during course could used clinical trials to identify successful interventions thereby accelerate development efficient therapies. When disease-modifying treatments become approved use, blood-based might also inform on treatment implementation management practice. In BioFINDER-1 cohort, plasma phosphorylated (p)-tau231 amyloid-β42/40 ratio were more changed at lower thresholds amyloid pathology. Longitudinally, however, only p-tau217 demonstrated marked amyloid-dependent over 4–6 years disease, no such observed p-tau231, p-tau181, amyloid-β42/40, glial acidic fibrillary protein neurofilament light. Only longitudinal increases associated deterioration brain AD. The selective increase its associations cognitive decline was confirmed an independent cohort (Wisconsin Registry Prevention). These findings support differential association strongly highlight as a surrogate marker progression prodromal AD, impact new treatments.

Язык: Английский

Процитировано

246