Frontotemporal lobar degeneration: defining phenotypic diversity through personalized medicine

Irwin, David J.; Cairns, Nigel J.; Grossman, Murray; McMillan, Corey T.; Lee, Edward B.; Deerlin, Vivianna M. Van; Lee, Virginia M.‐Y.; Trojanowski, John Q.

doi:10.1007/s00401-014-1380-1

Cited by 221 publications

(259 citation statements)

References 228 publications

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“…A direct comparison of the percent of total pathological burden finds a double-dissociation, where PiD has a lower percent of total pathology in STG whereas FTLD-TDPC has a lower total percent in MFG (Table 2). These preliminary associations in our pilot study suggest that FTLD neuropathological subtypes may have subtle differences in the pattern of disease in bvFTD, which could have potential clinical implications for improved diagnostics of underlying neuropathology (i.e., development of endophenotypes) (Irwin et al 2015). Future studies in larger samples of bvFTD, including other forms of FTLD-Tau and FTLD-TDP, will help to confirm these observations.…”

Section: Discussionsupporting

confidence: 54%

Semi-Automated Digital Image Analysis of Pick’s Disease and TDP-43 Proteinopathy

Irwin

Byrne²,

McMillan³

et al. 2015

J Histochem Cytochem.

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102

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SummaryDigital image analysis of histology sections provides reliable, high-throughput methods for neuropathological studies but data is scant in frontotemporal lobar degeneration (FTLD), which has an added challenge of study due to morphologically diverse pathologies. Here, we describe a novel method of semi-automated digital image analysis in FTLD subtypes including: Pick's disease (PiD, n=11) with tau-positive intracellular inclusions and neuropil threads, and TDP-43 pathology type C (FTLD-TDPC, n=10), defined by TDP-43-positive aggregates predominantly in large dystrophic neurites. To do this, we examined three FTLD-associated cortical regions: mid-frontal gyrus (MFG), superior temporal gyrus (STG) and anterior cingulate gyrus (ACG) by immunohistochemistry. We used a color deconvolution process to isolate signal from the chromogen and applied both object detection and intensity thresholding algorithms to quantify pathological burden. We found object-detection algorithms had good agreement with gold-standard manual quantification of tau-and TDP-43-positive inclusions. Our sampling method was reliable across three separate investigators and we obtained similar results in a pilot analysis using open-source software. Regional comparisons using these algorithms finds differences in regional anatomic disease burden between PiD and FTLD-TDP not detected using traditional ordinal scale data, suggesting digital image analysis is a powerful tool for clinicopathological studies in morphologically diverse FTLD syndromes. (J Histochem Cytochem 64:54-66, 2016)

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Section: Discussionsupporting

confidence: 54%

Semi-Automated Digital Image Analysis of Pick’s Disease and TDP-43 Proteinopathy

Irwin

Byrne²,

McMillan³

et al. 2015

J Histochem Cytochem.

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102

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“…Biomarkers discriminating FTLD pathological subtypes are strongly needed for the selection of patients in drug trials targeting the specific proteinopathies 6, 7. We have assessed and validated the clinical performance of novel CSF biomarkers identified previously12 for discrimination of FTLD pathological subtypes and nondemented controls using two independent CSF cohorts coming from different centers.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, the FTLD‐TDP group was enriched with FTLD patients with amyotrophic lateral sclerosis (FTLD‐ALS, n = 7), associated with TDP43 pathology 15. FTLD cases with tau neuropathology (FTLD‐Tau, n = 20) were selected based on autopsy ( n = 2), MAPT mutations ( n = 2),6 and familial history of autopsy confirmed FTLD‐Tau ( n = 1). The FTLD‐Tau group was also enriched with CSF from patients with FTLD‐Plus syndromes related to tau pathology such as progressive supranuclear palsy (FTLD‐PSP, n = 10) or corticobasal syndrome (FTLD‐CBS, n = 5) 16, 17.…”

Section: Methodsmentioning

confidence: 99%

“…However, the clinical presentation of the FTLD pathological subtypes is heterogeneous and overlapping 5. So far, there are still no effective early biomarkers available to discriminate FTLD and its two main pathological subtypes, hampering the selection of appropriate patients for clinical trials targeting the specific proteinopathy (i.e., Tau or TDP43) 6, 7…”

Section: Introductionmentioning

confidence: 99%

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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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“…It is possible that prospective assessments of neuropsychological tests and motor evaluations may yield a deeper endophenotype of CBS that can be used to screen individuals for likely forms of underlying pathology. 30 Future studies are necessary in an independent cohort to evaluate the sensitivity and specificity of asymmetric rigidity, along with our observed dissociation between neuroimaging features, for improving the diagnosis of underlying pathology in CBS.…”

Section: )mentioning

confidence: 97%

Multimodal imaging evidence of pathology-mediated disease distribution in corticobasal syndrome

et al. 2016

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Objective: To use multimodal neuroimaging to evaluate the influence of heterogeneous underlying pathology in corticobasal syndrome (CBS) on the neuroanatomical distribution of disease.Methods: We performed a retrospective evaluation of 35 patients with CBS with T1-weighted MRI, diffusion tensor imaging, and neuropathologic, genetic, or CSF evidence of underlying pathology. Patients were assigned to 2 groups: those with evidence of Alzheimer pathology (CBS-AD) and those without Alzheimer pathology (CBS-non-AD). Group comparisons of CBS-AD and CBS-non-AD assessed clinical features, gray matter (GM) cortical thickness, and white matter (WM) fractional anisotropy.Results: CBS-AD was found in 34% (n 5 12) and CBS-non-AD in 66% (n 5 23) of CBS patients.Clinical evaluations revealed that CBS-non-AD had a higher frequency of asymmetric rigidity compared to CBS-AD, but groups otherwise did not differ in dementia severity, impairments in cognition, or rates of extrapyramidal symptoms. We found frontoparietal GM and WM disease in each group compared to healthy, demographically comparable controls, as well as multimodal neuroimaging evidence of a double dissociation: CBS-non-AD had WM disease in the corpus callosum, corticospinal tract, and superior longitudinal fasciculus relative to CBS-AD, and CBS-AD had reduced temporoparietal GM relative to CBS-non-AD, including the precuneus and posterior cingulate. Conclusions:Patients with CBS have a pathology-mediated dissociation of GM and WM disease.Multimodality neuroimaging may be useful for improving in vivo pathologic diagnosis of CBS. Corticobasal syndrome (CBS) is a neurodegenerative condition characterized by lateralized extrapyramidal features and cortically mediated cognitive dysfunction.1 The underlying pathology of CBS is heterogeneous, and clinical features appear to be insufficient to identify an individual's histopathologic abnormality during life.2,3 The most common neuropathologic causes of CBS include corticobasal degeneration, a 4-repeat form of tau pathology associated with frontotemporal lobar degeneration (FTLD), 4 and Alzheimer disease (AD). 2,5,6 Multimodal neuroimaging studies suggest that AD and FTLD can be dissociated on the basis of gray matter (GM) and white matter (WM) neuroimaging. 7,8 Specifically, GM atrophy was evident in both AD and FTLD in T1-weighted MRI studies, but diffusion tensor imaging (DTI) revealed more WM disease in FTLD than in AD. Additional neuroimaging evidence suggests that tau pathology, the most common form of underlying pathology in CBS, is associated with substantial WM imaging changes 9 and that these findings converge with neuropathologic evidence of WM disease burden in 4-repeat tauopathy.9,10 However, prior evidence of greater WM pathology in FTLD disorders has been based on clinically heterogeneous study samples; therefore, it is not clear whether a dissociation of GM and WM disease is

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Frontotemporal lobar degeneration: defining phenotypic diversity through personalized medicine

Cited by 221 publications

References 228 publications

Semi-Automated Digital Image Analysis of Pick’s Disease and TDP-43 Proteinopathy

Semi-Automated Digital Image Analysis of Pick’s Disease and TDP-43 Proteinopathy

Novel CSF biomarkers to discriminate FTLD and its pathological subtypes

Multimodal imaging evidence of pathology-mediated disease distribution in corticobasal syndrome

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