Association of Plasma Clusterin Concentration With Severity, Pathology, and Progression in Alzheimer Disease

Thambisetty, Madhav; Simmons, Andrew; Velayudhan, Latha; Hye, Abdul; Campbell, James; Zhang, Yi; Wahlund, Lars‐Olof; Westman, Eric; Kinsey, Anna; Güntert, Andreas; Proitsi, Petroula; Powell, John; Čaušević, Mirsada; Killick, Richard; Lunnon, Katie; Lynham, Steven; Broadstock, Martin; Choudhry, Fahd; Howlett, David; Williams, Robert J.; Sharp, Sally I.; Mitchelmore, Cathy; Tunnard, Catherine; Leung, Rufina; Foy, Catherine; O’Brien, Darragh P.; Breen, Gerome; Furney, Simon J.; Ward, Malcolm; Kłoszewska, Iwona; Mecocci, Patrizia; Soininen, Hilkka; Tsolaki, Magda; Vellas, Bruno; Hodges, Angela; Murphy, Declan; Parkins, Sue; Richardson, Jill C.; Resnick, Susan M.; Ferrucci, Luigi; Wong, Dean F.; Zhou, Yun; Muehlboeck, Sebastian; Evans, Alan C.; Francis, Paul T.; Spenger, Christian; Lovestone, Simon

doi:10.1001/archgenpsychiatry.2010.78

Cited by 363 publications

(372 citation statements)

References 46 publications

(55 reference statements)

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“…Carbonyl reductase is elevated in hippocampi of 3xTg‐AD mice, which have markedly elevated levels of protein carbonylation (Shen et al ., 2015). Clusterin (ApoJ) polymorphism is associated with AD (Lambert et al ., 2009), and its circulating levels predict AD progression (Thambisetty et al ., 2010). Other apolipoproteins are also strongly linked to AD risk: ApoD catalyzes reduction of peroxidized lipids and its levels increase with age and AD, while ApoE has allele‐specific effects on Aβ levels and AD risk (Tai et al ., 2013; Dassati et al ., 2014).…”

Section: Discussionmentioning

confidence: 99%

Proteins that mediate protein aggregation and cytotoxicity distinguish Alzheimer's hippocampus from normal controls

et al. 2016

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SummaryNeurodegenerative diseases are distinguished by characteristic protein aggregates initiated by disease‐specific ‘seed’ proteins; however, roles of other co‐aggregated proteins remain largely unexplored. Compact hippocampal aggregates were purified from Alzheimer's and control‐subject pools using magnetic‐bead immunoaffinity pulldowns. Their components were fractionated by electrophoretic mobility and analyzed by high‐resolution proteomics. Although total detergent‐insoluble aggregates from Alzheimer's and controls had similar protein content, within the fractions isolated by tau or Aβ1–42 pulldown, the protein constituents of Alzheimer‐derived aggregates were more abundant, diverse, and post‐translationally modified than those from controls. Tau‐ and Aβ‐containing aggregates were distinguished by multiple components, and yet shared >90% of their protein constituents, implying similar accretion mechanisms. Alzheimer‐specific protein enrichment in tau‐containing aggregates was corroborated for individuals by three analyses. Five proteins inferred to co‐aggregate with tau were confirmed by precise in situ methods, including proximity ligation amplification that requires co‐localization within 40 nm. Nematode orthologs of 21 proteins, which showed Alzheimer‐specific enrichment in tau‐containing aggregates, were assessed for aggregation‐promoting roles in C. elegans by RNA‐interference ‘knockdown’. Fifteen knockdowns (71%) rescued paralysis of worms expressing muscle Aβ, and 12 (57%) rescued chemotaxis disrupted by neuronal Aβ expression. Proteins identified in compact human aggregates, bound by antibody to total tau, were thus shown to play causal roles in aggregation based on nematode models triggered by Aβ1–42. These observations imply shared mechanisms driving both types of aggregation, and/or aggregate‐mediated cross‐talk between tau and Aβ. Knowledge of protein components that promote protein accrual in diverse aggregate types implicates common mechanisms and identifies novel targets for drug intervention.

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Section: Discussionmentioning

confidence: 99%

Proteins that mediate protein aggregation and cytotoxicity distinguish Alzheimer's hippocampus from normal controls

et al. 2016

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“…Moreover, CLU was reported to be present in amyloid plaques (Giannakopoulos et al 1998). In addition, recent studies have revealed that the concentration of CLU in the CSF and plasma of AD patients is significantly elevated (Sihlbom et al 2008;Thambisetty et al 2010). Interestingly, as a chaperone protein, CLU has been proven to interact with Ab peptides and this interaction plays an important role in Ab aggregation, toxicity and clearance (Baig et al 2012;DeMattos et al 2002;Narayan et al 2012;Yerbury et al 2007).…”

Section: Clusterinmentioning

confidence: 99%

Inflammation in Alzheimer’s Disease and Molecular Genetics: Recent Update

Zhang

et al. 2015

Arch. Immunol. Ther. Exp.

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Alzheimer's disease (AD) is a complex agerelated neurodegenerative disorder of the central nervous system. Since the first description of AD in 1907, many hypotheses have been established to explain its causes. The inflammation theory is one of them. Pathological and biochemical studies of brains from AD individuals have provided solid evidence of the activation of inflammatory pathways. Furthermore, people with long-term medication of anti-inflammatory drugs have shown a reduced risk to develop the disease. After three decades of genetic study in AD, dozens of loci harboring genetic variants influencing inflammatory pathways in AD patients has been identified through genome-wide association studies (GWAS). The most well-known GWAS risk factor that is responsible for immune response and inflammation in AD development should be APOE e4 allele. However, a growing number of other GWAS risk AD candidate genes in inflammation have recently been discovered. In the present study, we try to review the inflammation in AD and immunity-associated GWAS risk genes like HLA-DRB5/DRB1, INPP5D, MEF2C, CR1, CLU and TREM2.

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“…Later, a systematic review and meta-analysis in 2012 by Koyama et al [31] concluded that plasma A␤ 42 :A␤ 40 ratio may predict development of AD, however, significant heterogeneity in the meta-analysis underlines the need for substantial further investigation of plasma A␤ levels as a preclinical biomarker. Thambisetty et al have identified plasma clusterin as a potential biomarker for AD [32] and present data that suggests that plasma clusterin is associated with rate of atrophy in MCI [33].…”

Section: Introductionmentioning

confidence: 61%

Prediction of Mild Cognitive Impairment that Evolves into Alzheimer's Disease Dementia within Two Years using a Gene Expression Signature in Blood: A Pilot Study

Roed

Grave

Lindahl

et al. 2013

JAD

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Background: The focus on Alzheimer's disease (AD) is shifting from dementia to the prodromal stage of the disorder, to a large extent due to increasing efforts in trying to develop disease modifying treatment for the disorder. For development of diseasemodifying drugs, a reliable and accurate test for identification of mild cognitive impairment (MCI) due to AD is essential. Objective: In the present study, MCI progressing to AD will be predicted using blood-based gene expression. Material and Methods: Gene expression analysis using qPCR was performed on blood RNA from a cohort of patients with amnestic MCI (aMCI; n = 66). Within the aMCI cohort, patients progressing to AD within 1 to 2 years were grouped as MCI converters (n = 34) and the patients remaining at the MCI stage after 2 years were grouped as stable MCI (n = 32). AD and control populations were also included in the study. Results: Multivariate statistical method partial least square regression was used to develop predictive models which later were tested using leave-one-out cross validation. Gene expression signatures that identified aMCI subjects that progressed to AD within 2 years with a prediction accuracy of 74%-77% were identified for the complete dataset and subsets thereof. Conclusion:The present pilot study demonstrates for the first time that MCI that evolves into AD dementia within 2 years may be predicted by analyzing gene expression in blood. Further studies will be needed to validate this gene signature as a potential test for AD in the predementia stage.

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Association of Plasma Clusterin Concentration With Severity, Pathology, and Progression in Alzheimer Disease

Cited by 363 publications

References 46 publications

Proteins that mediate protein aggregation and cytotoxicity distinguish Alzheimer's hippocampus from normal controls

Proteins that mediate protein aggregation and cytotoxicity distinguish Alzheimer's hippocampus from normal controls

Inflammation in Alzheimer’s Disease and Molecular Genetics: Recent Update

Prediction of Mild Cognitive Impairment that Evolves into Alzheimer's Disease Dementia within Two Years using a Gene Expression Signature in Blood: A Pilot Study

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