YKL-40: A Novel Prognostic Fluid Biomarker for Preclinical Alzheimer's Disease

Craig‐Schapiro, Rebecca; Perrin, Richard J.; Roe, Catherine M.; Xiong, Chengjie; Carter, Deborah; Cairns, Nigel J.; Mintun, Mark A.; Peskind, Elaine R.; Li, Ge; Galasko, Douglas; Clark, Christopher M.; Quinn, Joseph F.; D’Angelo, Gina; Malone, James P.; Townsend, R. Reid; Morris, John C.; Fagan, Anne M.; Holtzman, David M.

doi:10.1016/j.biopsych.2010.08.025

Cited by 397 publications

(444 citation statements)

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“…In agreement with previous studies, CSF YKL40 was increased in FTLD and AD compared to controls 35, 36, 37. FTLD‐TDP had the highest YKL‐40 values, which were comparable to those observed in AD patients, but different to those observed in CON, FTLD‐Tau, or DLB.…”

Section: Discussionsupporting

confidence: 91%

Novel CSF biomarkers to discriminate FTLD and its pathological subtypes

Campo

Galimberti

Elias

et al. 2018

Ann Clin Transl Neurol

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ObjectiveFrontotemporal lobar degeneration (FTLD) is the second most prevalent dementia in young patients and is characterized by the presence of two main protein aggregates in the brain, tau (FTLD‐Tau) or TDP43 (FTLD‐TDP), which likely require distinct pharmacological therapy. However, specific diagnosis of FTLD and its subtypes remains challenging due to largely overlapping clinical phenotypes. Here, we aimed to assess the clinical performance of novel cerebrospinal fluid (CSF) biomarkers for discrimination of FTLD and its pathological subtypes.Methods YKL40, FABP4, MFG‐E8, and the activities of catalase and specific lysosomal enzymes were analyzed in patients with FTLD‐TDP (n = 30), FTLD‐Tau (n = 20), AD (n = 30), DLB (n = 29), and nondemented controls (n = 29) obtained from two different centers. Models were validated in an independent CSF cohort (n = 188).Results YKL40 and catalase activity were increased in FTLD‐TDP cases compared to controls. YKL40 levels were also higher in FTLD‐TDP compared to FTLD‐Tau. We identified biomarker models able to discriminate FTLD from nondemented controls (MFG‐E8, tTau, and Aβ 42; 78% sensitivity and 83% specificity) and non‐FTLD dementia (YKL40, pTau, p/tTau ratio, and age; 90% sensitivity, 78% specificity), which were validated in an independent cohort. In addition, we identified a biomarker model differentiating FTLD‐TDP from FTLD‐Tau (YKL40, MFGE‐8, βHexA together with βHexA/tHex and p/tTau ratios and age) with 80% sensitivity and 82% specificity.InterpretationThis study identifies CSF protein signatures distinguishing FTLD and the two main pathological subtypes with optimal accuracy (specificity/sensitivity > 80%). Validation of these models may allow appropriate selection of cases for clinical trials targeting the accumulation of Tau or TDP43, thereby increasing their efficiency and facilitating the development of successful therapies.

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Section: Discussionsupporting

confidence: 91%

Novel CSF biomarkers to discriminate FTLD and its pathological subtypes

Campo

Galimberti

Elias

et al. 2018

Ann Clin Transl Neurol

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“…The expression of YKL-40 in the CSF is elevated in early AD. The ratio of YKL-40 to Aβ42 predicts cognitive impairment as well as the best CSF biomarkers (Aβ42, t-tau, and p-tau) [83] , suggesting potential as a biomarker for preclinical AD. dementias, and that CSF VILIP-1/Aβ42 predicts cognitive impairment as well as tau/Aβ42 and p-tau181/Aβ42 [84,85] .…”

Section: Infl Ammationmentioning

confidence: 99%

Cerebrospinal fluid biomarkers of Alzheimer’s disease

Sui

Yang

2014

Neurosci. Bull.

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Alzheimer's disease (AD) is a fatal neurodegenerative disorder that takes about a decade to develop, making early diagnosis possible. Clinically, the diagnosis of AD is complicated, costly, and inaccurate, so it is urgent to fi nd specifi c biomarkers. Due to its multifactorial nature, a panel of biomarkers for the multiple pathologies of AD, such as cerebral amyloidogenesis, neuronal dysfunction, synapse loss, oxidative stress, and infl ammation, are most promising for accurate diagnosis. Highly sensitive and high-throughput proteomic techniques can be applied to develop a panel of novel biomarkers for AD. In this review, we discuss the metabolism and diagnostic performance of the well-established core candidate cerebrospinal fl uid (CSF) biomarkers (β-amyloid, total tau, and hyperphosphorylated tau). Meanwhile, novel promising CSF biomarkers, especially those identifi ed by proteomics, updated in the last fi ve years are also extensively discussed. Furthermore, we provide perspectives on how biomarker discovery for AD is evolving.Keywords: Alzheimer's disease; biomarker; cerebrospinal fl uid; β-amyloid; tau; proteomics ·Review· Introduction Alzheimer's disease (AD) is becoming more prevalent due to the increasing population of people aged over 65 [1] .It is estimated that it will affect 66 million by 2030 and 115 million by 2050 worldwide if no effective therapeutic strategies are found [2] . Clinically, AD is characterized by cognitive impairment, progressive disturbance of daily activities, many neuropsychiatric symptoms, and behavioral deterioration [3][4][5][6][7][8] . Pathologically, it is characterized by deposition of extracellular neuritic plaques composed of β-amyloid (Aβ) [9] and intracellular neurofibrillary tangles (NFTs) consisting of a hyperphosphorylated form of the microtubule-associated protein tau [10][11][12] . Besides, loss of neurons and synapses is also a pathological hallmark of AD [13][14][15] . The worldwide cost of dementia is huge and expected to skyrocket in the next few years. AD may become one of the most marked social, health, and economic challenges in the twenty-fi rst century [16] .Clinically, the procedure for the diagnosis of AD is diffi cult and complex. Neuropsychological tests, such as the mini-mental state examination, magnetic resonance imaging of hippocampal volume, and clinical assessment, are used to aid in diagnosis. However, a defi nitive diagnosis of AD requires confirmation at autopsy. It is estimated to take 8-10 years or longer before mild cognitive impairment (MCI) develops into AD [17,18] . Meanwhile, intervention therapies work most effectively in the early stage of AD. Thus, it is urgent and feasible to seek novel specifi c biomarkers to aid in diagnosis and the evaluation of treatments [19] . Surrounding the brain and spinal cord, cerebrospinal fluid (CSF) is an ideal source refl ecting biochemical changes in the brain of the AD patient [20] . Extensive studies have focused on seeking AD biomarkers in CSF.A comprehensive search of the Web of Science (Janua...

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“…Furthermore, to simplify the clinical diagnosis, several peripheral biomarkers have already been chosen as supportive indicators, including the level of Aβ1‐42 and p‐tau181 within the CSF (cerebrospinal fluid) and the rate of glucose uptake by FDG‐PET (fluorodeoxyglucose‐positron emission tomography) (Ballard, Gauthier, Corbett, Brayne, & Aarsland, 2011; Cohen & Klunk, 2017; Khan & Alkon, 2015; Lista, Garaci, Ewers, Teipel, & Zetterberg, 2014). Moreover, other biomarkers are believed to have potential diagnostic values based on preliminary analyses, including ApoE4 level in the blood, YKL‐40 (chitinase‐3 like‐1) level in the CSF, and NTP (neuronal thread protein) level in the urine, despite insufficient confirmatory evidence (Craig‐Schapiro, Perrin, Roe, Xiong, & Carter, 2010; Farrer, 1997; Lonneborg, 2008). The combination of these diagnostic biomarkers could largely increase the accuracy and potential early diagnosis and thus benefit the prognosis of patients (Table 1).…”

Section: Introductionmentioning

confidence: 99%

The emerging roles of protein homeostasis‐governing pathways in Alzheimer's disease

et al. 2018

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Pathways governing protein homeostasis are involved in maintaining the structural, quantitative, and functional stability of intracellular proteins and involve the ubiquitin–proteasome system, autophagy, endoplasmic reticulum, and mTOR pathway. Due to the broad physiological implications of protein homeostasis pathways, dysregulation of proteostasis is often involved in the development of multiple pathological conditions, including Alzheimer's disease (AD). Similar to other neurodegenerative diseases that feature pathogenic accumulation of misfolded proteins, Alzheimer's disease is characterized by two pathological hallmarks, amyloid‐β (Aβ) plaques and tau aggregates. Knockout or transgenic overexpression of various proteostatic components in mice results in AD‐like phenotypes. While both Aβ plaques and tau aggregates could in turn enhance the dysfunction of these proteostatic pathways, eventually leading to apoptotic or necrotic neuronal death and pathogenesis of Alzheimer's disease. Therefore, targeting the components of proteostasis pathways may be a promising therapeutic strategy against Alzheimer's disease.

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YKL-40: A Novel Prognostic Fluid Biomarker for Preclinical Alzheimer's Disease

Cited by 397 publications

References 50 publications

Novel CSF biomarkers to discriminate FTLD and its pathological subtypes

Novel CSF biomarkers to discriminate FTLD and its pathological subtypes

Cerebrospinal fluid biomarkers of Alzheimer’s disease

The emerging roles of protein homeostasis‐governing pathways in Alzheimer's disease

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