Decreased β-Amyloid<sub>1-42</sub>and Increased Tau Levels in Cerebrospinal Fluid of Patients With Alzheimer Disease

Sunderland, Trey; Linker, Gary; Mirza, Nadeem Q.; Putnam, Karen; Friedman, D. L.; Kimmel, Lida H.; Bergeson, Judy; Manetti, G.; Zimmermann, Matthew; Tang, Brian; Bartko, John J.; Cohen, Robert M.

doi:10.1001/jama.289.16.2094

Cited by 602 publications

(440 citation statements)

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“…The diagnostic performance of the three biomarkers, total tau, phospho-tau, and the 42 amino acid form of ␤-amyloid have been evaluated in numerous studies and their ability to identify incipient AD in MCI cases has also been studied. Some candidate AD biomarkers including ubiquitin, neurofilament proteins, growth-associated protein 43 (neuromodulin), and neuronal thread protein (AD7c) show interesting results but have been less extensively studied. It is concluded that CSF biomarkers may have clinical utility in the differentiation between AD and several important differential diagnoses, including normal aging, depression, alcohol dementia, and Parkinson's disease, and also in the identification of Creutzfeldt-Jakob disease in cases with rapidly progressive dementia.…”

Section: Resultsmentioning

confidence: 99%

“…A moderate to marked decrease in CSF A␤42 in AD to about 50% of control levels has been found using the majority of these methods (Table 1). 35,39,[41][42][43][44][45]47,48 An increase in CSF A␤42 in AD was found in one study. 46 This finding may be attributable to methodological differences (e.g., assay specificity for aggregated or truncated A␤ variants).…”

Section: ␤-Amyloidmentioning

confidence: 88%

“…However, in a large study on 131 AD cases in which the diagnosis was confirmed at autopsy in 31 cases, the performance of CSF T-tau and A␤42 was similar in both groups. 43 Since CSF T-tau reflects neuronal and axonal degeneration, it is not specific for AD; high CSF T-tau levels will be found in all CNS disorders with neuronal degeneration or damage. The highest levels are found in acute stroke 18 and in CJD.…”

Section: Csf T-taumentioning

confidence: 99%

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Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

2004

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Summary:The introduction of acetylcholine esterase (AChE) inhibitors as a symptomatic treatment of Alzheimer's disease (AD) has made patients seek medical advice at an earlier stage of the disease. This has highlighted the importance of diagnostic markers for early AD. However, there is no clinical method to determine which of the patients with mild cognitive impairment (MCI) will progress to AD with dementia, and which have a benign form of MCI without progression. In this paper, the performance of cerebrospinal fluid (CSF) protein biomarkers for AD is reviewed. The diagnostic performance of the three biomarkers, total tau, phospho-tau, and the 42 amino acid form of ␤-amyloid have been evaluated in numerous studies and their ability to identify incipient AD in MCI cases has also been studied. Some candidate AD biomarkers including ubiquitin, neurofilament proteins, growth-associated protein 43 (neuromodulin), and neuronal thread protein (AD7c) show interesting results but have been less extensively studied. It is concluded that CSF biomarkers may have clinical utility in the differentiation between AD and several important differential diagnoses, including normal aging, depression, alcohol dementia, and Parkinson's disease, and also in the identification of Creutzfeldt-Jakob disease in cases with rapidly progressive dementia. Early diagnosis of AD is not only of importance to be able to initiate symptomatic treatment with AChE inhibitors, but will be the basis for initiation of treatment with drugs aimed at slowing down or arresting the degenerative process, such as ␥-secretase inhibitors, if these prove to affect AD pathology and to have a clinical effect.

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Section: Resultsmentioning

confidence: 99%

Section: ␤-Amyloidmentioning

confidence: 88%

Section: Csf T-taumentioning

confidence: 99%

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Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

2004

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“…CSF biomarkers have proven to be the most accurate of the biomarkers investigated to date, with AD being shown to be associated with decreased Aβ42 levels and increased tau levels in the CSF [33]. However the latter procedure is invasive and patient compliance is anticipated to be low.…”

Section: Diagnosismentioning

confidence: 99%

Ocular Biomarkers for Early Detection of Alzheimer's Disease

Frost

Martins

Kanagasingam

2010

JAD

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Alzheimer's disease (AD) is the most common form of dementia and is characterized clinically by a progressive decline in memory, learning and executive function and neuropathologically by the presence of cerebral amyloid deposits. Despite a century of research, there is still no cure or conclusive pre-mortem diagnosis for the disease. A number of symptom-modifying drugs for AD have been developed, but their efficacy is minimal and short-lived. AD cognitive symptoms arise only after significant, irreversible neural deterioration has occurred, hence there is an urgent need to detect AD early, before the onset of cognitive symptoms. An accurate, early diagnostic test for AD would enable current and future treatments to be more effective, as well as contribute to the development of new treatments.While most AD related pathology occurs in the brain, the disease has also been reported to affect the eye, which is more accessible for imaging than the brain. AD-related proteins exist in the normal human eye and may produce ocular pathology in AD. There is some homology between the retinal and cerebral vasculatures and the retina also contains nerve cells and fibers that form a sensory extension of the brain. The eye is the only place in the body where vasculature or neural tissue is available for non-invasive optical imaging. This article presents a review of current literature on ocular morphology in AD and discusses the potential for an ocular based screening test for AD.

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“…Por meio de uma metanálise, Sunderland et al (2003) examinaram os achados de 17 artigos sobre Aβ42 e 34 artigos sobre tau no LCR de pacientes com DA. Todos os estudos incluídos nessa metanálise relataram aumento de tau total no LCR na DA.…”

Section: Proteína Tau E Suas Formas Fosforiladasunclassified

Trabalho de consenso de força-tarefa da WFSBP sobre marcadores biológicos das demências: contribuição da análise do LCR e do sangue para o diagnóstico precoce e diferencial das demências

Wiltfang¹,

Lewczuk²,

Riederer³

et al. 2009

Rev. psiquiatr. clín.

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RevisãoTrabalho de consenso de força-tarefa da WFSBP # sobre marcadores biológicos das demências: Contribuição da análise do LCR e do sangue para o diagnóstico precoce e diferencial das demências ResumoO envelhecimento da população e o aumento da expectativa de vida resultam em um número cada vez maior de pacientes com demência. Os déficits cognitivos podem ser manifestações de uma doença curável do sistema nervoso central (por exemplo, neuroinflamação), como também de uma doença atualmente considerada irreversível, como a doença de Alzheimer (DA). Tendo em vista as novas abordagens terapêuticas para a DA, em que se avalia o potencial modificador da patogenia, torna-se necessário o estabelecimento de um diagnóstico confiável em vida. Embora a análise do líquido cefalorraquidiano (LCR) e do soro seja realização de rotina em doenças neuroinflamatórias, ainda necessita de padronização para ser usada como instrumento auxiliar no diagnóstico clínico da DA. Vários parâmetros relacionados à DA (tau total, formas fosforiladas de tau, peptídeos Aβ, genótipo ApoE, p97 etc.) podem ser determinados no LCR. A combinação de alguns desses parâmetros proporciona sensibilidade e especificidade na faixa de 85% para o diagnóstico da DA, um valor usualmente atribuído a um bom instrumento de diagnóstico. Nesta revisão, são discutidas as publicações mais recentes sobre os marcadores neuroquímicos para o diagnóstico clínico das demências, com ênfase no diagnóstico precoce e diferencial da DA. Discutem-se brevemente as novas perspectivas oferecidas por tecnologias recentes, tais como a FCS (fluorescence correlation spectroscopy) e a técnica de espectrometria de massa pelo método SELDI-TOF (surface enhanced laser desorption/ionization time-of-flight mass spectrometry). Wiltfang J, et al. / Rev Psiq Clín. 2009;36( Wiltfang J, et al. / Rev Psiq Clín. 2009;36(1):1-16 IntroduçãoEm função do envelhecimento populacional e do aumento da expectativa de vida, os transtornos demenciantes irão se tornar um sério problema para os sistemas de atendimento à saúde. Em relação à doença de Alzheimer (DA), apesar do número cada vez maior de pacientes, poucos progressos foram feitos em direção a um melhor padrão para o diagnóstico em vida. Embora a sensibilidade do diagnóstico clínico seja relativamente alta (93%), a especificidade pode ser mais baixa -55%, conforme relatado por um estudo clínico-patológico multicêntrico (Mayeux, 1998). Em mãos experientes, o diagnóstico clínico de DA pode ser preditivo da confirmação neuropatológica em 80% a 90% dos casos; contudo, o diagnóstico da DA em fases iniciais assim como o diagnóstico diferencial das apresentações demenciais incomuns continuam a ser tarefas difíceis em bases puramente clínicas. A introdução das drogas antidemência, tais como os inibidores da acetilcolinesterase para o tratamento da DA, representou um potencial de benefício terapêutico considerável, ante uma doença até então considerada irreversível (recente revisão de Bullock, 2002;Knopman, 2001). Desse modo, a necessidade de se estabelec...

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Decreased β-Amyloid_1-42and Increased Tau Levels in Cerebrospinal Fluid of Patients With Alzheimer Disease

Cited by 602 publications

References 74 publications

Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

Ocular Biomarkers for Early Detection of Alzheimer's Disease

Trabalho de consenso de força-tarefa da WFSBP sobre marcadores biológicos das demências: contribuição da análise do LCR e do sangue para o diagnóstico precoce e diferencial das demências

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Decreased β-Amyloid1-42and Increased Tau Levels in Cerebrospinal Fluid of Patients With Alzheimer Disease

Cited by 602 publications

References 74 publications

Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

Cerebrospinal fluid protein biomarkers for Alzheimer’s disease

Ocular Biomarkers for Early Detection of Alzheimer's Disease

Trabalho de consenso de força-tarefa da WFSBP sobre marcadores biológicos das demências: contribuição da análise do LCR e do sangue para o diagnóstico precoce e diferencial das demências

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Decreased β-Amyloid_1-42and Increased Tau Levels in Cerebrospinal Fluid of Patients With Alzheimer Disease