Prevalence Estimates of Amyloid Abnormality Across the Alzheimer Disease Clinical Spectrum

Jansen, Willemijn J.; Janssen, Olin; Tijms, Betty M.; Vos, Stephanie J.B.; Ossenkoppele, Rik; Visser, Pieter Jelle; Aarsland, Dag; Alcolea, Daniel; Altomare, Daniele; Arnim, Christine von; Baiardi, Simone; Baldeiras, Inês; Barthel, Henryk; Bateman, Randall J.; Berckel, Bart van; Binette, Alexa Pichet; Blennow, Kaj; Boada, Merçé; Boecker, Henning; Bottlaender, Michel; Braber, Anouk den; Brooks, David J.; Buchem, Mark A. van; Camus, Vincent; Carill, Jose Manuel; Cerman, Jiří; Chen, Kewei; Chételat, Gaël; Chipi, Elena; Cohen, Ann D.; Daniels, Alisha; Delarue, Marion; Didic, Mira; Drzezga, Alexander; Dubois, Bruno; Eckerström, Marie; Ekblad, Laura L.; Engelborghs, Sebastiaan; Epelbaum, Stéphane; Fagan, Anne M.; Fan, Yong; Fladby, Tormod; Fleisher, Adam; Flier, Wiesje M. van der; Förster, Stefan; Fortea, Juan; Frederiksen, Kristian Steen; Freund‐Levi, Yvonne; Frings, Lars; Frisoni, Giovanni B.; Fröhlich, L.; Gabryelewicz, Tomasz; Gertz, Hermann‐Josef; Gill, Kiran Dip; Gkatzima, Olymbia; Gómez‐Tortosa, Estrella; Grimmer, Timo; Guedj, Éric; Habeck, Christian; Hampel, Harald; Handels, Ron; Hansson, Oskar; Hausner, Lucrezia; Hellwig, Sabine; Heneka, Michael T.; Herukka, Sanna‐Kaisa; Hildebrandt, Helmut; Hodges, John R.; Hort, Jakub; Huang, Chin‐Chang; Iriondo, Ane; Itoh, Yoshiaki; Ivanoiu, Adrian; Jagust, William J.; Jessen, Frank; Johannsen, Peter; Johnson, Keith A.; Kandimalla, Ramesh; Kapaki, Elisabeth; Kern, Silke; Kilander, Lena; Klimkowicz‐Mrowiec, Aleksandra; Klunk, William E.; Koglin, Norman; Kornhuber, Johannes; Kramberger, Milica G.; Kuo, Hung‐Chou; Laere, Koen Van; Landau, Susan; Landeau, Brigitte; Lee, Dong Hoon; Leon, Mony J. de; Leyton, Cristian E.; Lin, Kun‐Ju; Lleó, Alberto; Löwenmark, Malin; Madsen, Karine; Maier, Wolfgang; Marcusson, Jan; Marquié, Marta; Martínez-Lage, Pablo; Maserejian, Nancy N.; Mattsson, Niklas; Mendonça, Alexandre de; Meyer, Philipp T.; Miller, Bruce L.; Minatani, Shinobu; Mintun, Mark A.; Mok, Vincent Chung Tong; Molinuevo, José Luís; Morbelli, Silvia; Morris, John C.; Mroczko, Barbara; Na, Duk L.; Newberg, Andrew B.; Nobili, Flavio; Nordberg, Agneta; Rikkert, Marcel G M Olde; Oliveira, Catarina; Olivieri, Pauline; Orellana, Adela; Paraskevas, George P.; Parchi, Piero; Pardini, Matteo; Parnetti, Lucilla; Peters, Oliver; Poirier, Judes; Popp, Julius; Prabhakar, Sudesh; Rabinovici, Gil D.; Ramakers, Inez; Rami, Lorena; Reiman, Eric M.; Rodrigue, Karen M.; Rodríguez-Rodríguez, Eloy; Roe, Catherine M.; Rosa‐Neto, Pedro; Rosen, Howard J.; Rot, Uroš; Rowe, Christopher C.; Rüther, Eckart; Ruiz, Agustín; Sabri, Osama; Sakhardande, Jayant; Sánchez‐Juan, Pascual; Sando, Sigrid Botne; Santana, Isabel; Sarazin, Marie; Scheltens, Philip; Schröder, Johannes; Selnes, Per; Seo, Sang Won; Silva, Dina; Skoog, Ingmar; Snyder, Peter J.; Soininen, Hilkka; Sollberger, Marc; Sperling, Reisa A.; Spiru, L.; Stern, Yaakov; Stomrud, Erik; Takeda, Akitoshi; Teichmann, Marc; Teunissen, Charlotte E.; Thompson, Louisa I.; Tomassen, Jori; Tsolaki, Magda; Vandenberghe, Rik; Verbeek, Marcel M.; Verhey, Frans R.J.; Villemagne, Victor L.; Villeneuve, Sylvia; Vogelgsang, Jonathan; Waldemar, Gunhild; Wallin, Anders; Wallin, Åsa; Wiltfang, Jens; Wolk, David A.; Yen, Tzu‐Chen; Zboch, Marzena; Zetterberg, Henrik

doi:10.1001/jamaneurol.2021.5216

Cited by 127 publications

(86 citation statements)

References 43 publications

(76 reference statements)

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“…CSF Aβ 42 /Aβ 40 is an early AD biomarker, often becoming abnormal ahead of Aβ-PET [ 40 ]. The accessibility, cost-effectiveness, and simplicity advantages of blood make it a highly attractive biofluid for clinical chemistry evaluation of biological changes in disease.…”

Section: Discussionmentioning

confidence: 99%

Diagnostic value of serum versus plasma phospho-tau for Alzheimer’s disease

et al. 2022

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Background Blood phosphorylated tau (p-tau) forms are promising Alzheimer’s disease (AD) biomarkers, but validation in matrices other than ethylenediaminetetraacetic acid (EDTA) plasma is limited. Firstly, we assessed the diagnostic potential of p-tau231 and p-tau181 in paired plasma and serum samples. Secondly, we compared serum and cerebrospinal fluid (CSF) samples from biomarker-positive AD and biomarker-negative control participants. Methods We studied three independent cohorts (n=115 total): cohorts 1 and 2 included individuals with paired plasma and serum, while cohort 3 included paired serum and CSF. Blood-based p-tau231 and p-tau181 were measured using in-house or commercial single molecule array (Simoa) methods. Results Serum and plasma p-tau231 and p-tau181 were two- to three-fold increased in biomarker-positive AD versus biomarker-negative controls (P≤0.0008). Serum p-tau231 separated diagnostic groups with area under the curve (AUC) of 82.2% (cohort 3) to 88.2% (cohort 1) compared with 90.2% (cohort 1) for plasma. Similarly, p-tau181 showed AUC of 89.6% (cohort 1) to 89.8% (cohort 3) in serum versus 85.4% in plasma (cohort 1). P-tau231 and p-tau181 correlated slightly better in serum (rho=0.92 for cohort 1, 0.93 for cohort 3) than in plasma (rho=0.88, cohort 1). Within-individual p-tau181 (Quanterix) and p-tau231 concentrations were twice higher in plasma versus serum, but p-tau181 (in-house, Gothenburg) levels were not statistically different. Bland-Altman plots revealed that the relative difference between serum/plasma was larger in the lower range. P-tau levels in paired plasma and serum correlated strongly with each other (rho=0.75–0.93) as well as with CSF Aβ42 (rho= −0.56 to −0.59), p-tau and total-tau (rho=0.53–0.73). Based on the results, it seems possible that serum p-tau reflects the same pool of brain-secreted p-tau as in CSF; we estimated that less than 2% of CSF p-tau is found in serum, being same for both controls and AD. Conclusions Comparable diagnostic performances and strong correlations between serum versus plasma pairs suggest that p-tau analyses can be expanded to research cohorts and hospital systems that prefer serum to other blood matrices. However, absolute biomarker concentrations may not be interchangeable, indicating that plasma and serum samples should be used independently. These results should be validated in independent cohorts.

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Section: Discussionmentioning

confidence: 99%

Diagnostic value of serum versus plasma phospho-tau for Alzheimer’s disease

et al. 2022

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“…In a recent study of 747 individuals, subtle cognitive difficulties associated with entorhinal cortex atrophy were present prior to amyloid plaque formation ( Thomas et al, 2020 ). Recent estimates show that more than a third of cognitively normal people over the age of 70 and more than a half of individuals over the age of 95 have elevated Aβ 42 in their CSF ( Jansen et al, 2022 ). Most disappointingly, more than 30 Phase three clinical trials of drugs targeting Aβ have failed to slow cognitive decline in AD ( Ayton and Bush, 2020 ).…”

Section: An Accelerated Historical Perspective Of Alzheimer’s Disease...mentioning

confidence: 99%

Peripheral Pathways to Neurovascular Unit Dysfunction, Cognitive Impairment, and Alzheimer’s Disease

Nelson

2022

Front. Aging Neurosci.

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Alzheimer’s disease (AD) is the most common form of dementia. It was first described more than a century ago, and scientists are acquiring new data and learning novel information about the disease every day. Although there are nuances and details continuously being unraveled, many key players were identified in the early 1900’s by Dr. Oskar Fischer and Dr. Alois Alzheimer, including amyloid-beta (Aβ), tau, vascular abnormalities, gliosis, and a possible role of infections. More recently, there has been growing interest in and appreciation for neurovascular unit dysfunction that occurs early in mild cognitive impairment (MCI) before and independent of Aβ and tau brain accumulation. In the last decade, evidence that Aβ and tau oligomers are antimicrobial peptides generated in response to infection has expanded our knowledge and challenged preconceived notions. The concept that pathogenic germs cause infections generating an innate immune response (e.g., Aβ and tau produced by peripheral organs) that is associated with incident dementia is worthwhile considering in the context of sporadic AD with an unknown root cause. Therefore, the peripheral amyloid hypothesis to cognitive impairment and AD is proposed and remains to be vetted by future research. Meanwhile, humans remain complex variable organisms with individual risk factors that define their immune status, neurovascular function, and neuronal plasticity. In this focused review, the idea that infections and organ dysfunction contribute to Alzheimer’s disease, through the generation of peripheral amyloids and/or neurovascular unit dysfunction will be explored and discussed. Ultimately, many questions remain to be answered and critical areas of future exploration are highlighted.

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“…Although brain Aβ load is associated with AD-related cognitive decline (25), Aβ pathology alone seems not to be not sufficient to cause it (25). For example, it is well established that around 30% of CU individuals older than 55 years of age present brain Aβ pathology and that a large portion of these individuals remains cognitively intact during their lives (26). This supports that the association between Aβ accumulation and cognitive deterioration depends on patients’ intrinsic resilience and susceptibility mechanisms.…”

Section: Discussionmentioning

confidence: 99%

Genetic Risk for Attention-Deficit/Hyperactivity Disorder Predicts Cognitive Decline and Development of Alzheimer’s Disease Pathophysiology in Cognitively Unimpaired Older Adults

Leffa

Ferrari‐Souza

Bellaver

et al. 2022

Preprint

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Background: Attention-Deficit/Hyperactivity Disorder (ADHD) persists in older age and is postulated to be a risk factor for cognitive impairment and Alzheimer's Disease (AD). However, this notion relies exclusively on epidemiological associations, and no previous study has linked ADHD with a decline in cognitive performance in older adults or with AD progression. Therefore, this study aimed to determine whether genetic liability for ADHD, as measured by a well-validated ADHD polygenic risk score (ADHD-PRS), is associated with longitudinal cognitive decline and the development of AD pathophysiology in cognitively unimpaired (CU) older adults. Methods: We calculated a weighted ADHD-PRS in 212 CU individuals without a clinical diagnosis of ADHD (55-90 years) using whole-genome information. These individuals had baseline amyloid-β (Aβ) positron emission tomography, as well as longitudinal cerebrospinal fluid (CSF) phosphorylated tau at threonine 181, structural magnetic resonance imaging, and cognitive assessments for up to 6 years. Linear mixed-effects models were used to test the association of ADHD-PRS with cognition and AD biomarkers. Outcomes: Higher ADHD-PRS was associated with greater cognitive decline over 6 years. The combined effect between high ADHD-PRS and brain Aβ deposition on cognitive deterioration was more significant than each individually. Additionally, higher ADHD-PRS was associated with increased CSF p-tau181 levels and frontoparietal atrophy in CU Aβ-positive individuals. Interpretation: Our results suggest that genetic liability for ADHD is associated with cognitive deterioration and the development of AD pathophysiology in the CU elderly. These findings indicate that ADHD-PRS might inform the risk of developing cognitive decline in this population. Funding: National Institute of Health and Brain & Behavioral Research Foundation.

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Prevalence Estimates of Amyloid Abnormality Across the Alzheimer Disease Clinical Spectrum

Cited by 127 publications

References 43 publications

Diagnostic value of serum versus plasma phospho-tau for Alzheimer’s disease

Diagnostic value of serum versus plasma phospho-tau for Alzheimer’s disease

Peripheral Pathways to Neurovascular Unit Dysfunction, Cognitive Impairment, and Alzheimer’s Disease

Genetic Risk for Attention-Deficit/Hyperactivity Disorder Predicts Cognitive Decline and Development of Alzheimer’s Disease Pathophysiology in Cognitively Unimpaired Older Adults

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