18F-Flortaucipir in TDP-43 associated frontotemporal dementia

Smith, Ruben; Santillo, Alexander; Waldö, María Landqvist; Strandberg, Olof; Berron, David; Vestberg, Susanna; Westen, Danielle van; Swieten, John van; Honer, Michael; Hansson, Oskar

doi:10.1038/s41598-019-42625-9

Cited by 31 publications

(34 citation statements)

References 40 publications

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“…The absence of binding in the vitro autoradiography images of FTLD-TDP cases is in line with a recent study in which in vitro [ 3 H]AV1451 autoradiography on frontal and temporal cortical cryosections of SV PPA cases as well as C9orf72 TDP-43 type B cases also showed no binding [12]. Another independent study demonstrated the absence of in vivo [ 18 F]AV1451 PET signal during life in a patient with the C9orf72 mutation who was neuropathologically diagnosed as TDP-43 type B [21].…”

Section: Discussionsupporting

confidence: 90%

“…This made the authors conclude that MAO-B does not appear to be a significant binding target of [ 18 F]AV1451, despite tau levels being low in this patient group in the first place. Similarly, we also could not reveal any binding in vitro while in vivo, a strong signal has been consistently shown [9][10][11][12]14]. On the other hand, for [ 18 F]THK5351, in vivo reduction of tracer uptake has been demonstrated in AD and PSP using an oral dose of selegiline [25].…”

Section: Discussionmentioning

confidence: 47%

“…We and others have previously demonstrated strong PET signal of the first-generation tau-PET tracers in the anterior temporal lobe that was consistently present in patients with SV PPA [9][10][11][12][13][14][15][16]. In an effort to explain this unexpected but highly consistent finding, we conducted an in vitro autoradiography binding study with [ 18 F]AV1451 in SV PPA cases, constituting the range of underlying pathologies.…”

Section: Discussionmentioning

confidence: 64%

“…Currently, a positron emission tomography (PET) tracer to visualize TDP-43 in vivo is not available yet. However, firstgeneration tau-PET tracers such as [ 18 F]AV1451 [7] and [ 18 F]THK5351 [8] have consistently shown strong in vivo tracer retention in the anterior temporal lobe of SV PPA patients [9][10][11][12][13][14][15][16]. At the individual patient level, evidence for consistently elevated [ 18 F]AV1451 binding has been found in the anterior temporal lobe of all seven SV PPA cases and all seven "right" semantic dementia cases [10,11].…”

Section: Introductionmentioning

confidence: 98%

“…In vitro binding studies with fluorine-18 labeled and tritiated AV1451 on sections with FTLD pathology have shown heterogeneous results [12,[17][18][19][20][21]. [ 3 H]AV1451 autoradiography indicated no binding to TDP-43 type C in SV PPA nor to C9orf72 gene mutation carriers with underlying TDP-43 type B pathology [12].…”

Section: Introductionmentioning

confidence: 99%

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Binding of [18F]AV1451 in post mortem brain slices of semantic variant primary progressive aphasia patients

Schaeverbeke

Celen

Cornelis

et al. 2019

Eur J Nucl Med Mol Imaging

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Purpose In vivo tau-PET tracer retention in the anterior temporal lobe of patients with semantic variant primary progressive aphasia (SV PPA) has consistently been reported. This is unexpected as the majority of these patients have frontotemporal lobar degeneration TDP (FTLD-TDP). Methods We conducted an in vitro [ 18 F]AV1451 autoradiography binding study in five cases with a clinical diagnosis of SV PPA constituting the range of pathologies (i.e., three FTLD-TDP, one Alzheimer's disease (AD), and one Pick's disease (PiD)). Binding was compared with two controls without neurodegeneration, two typical AD, one corticobasal syndrome with underlying AD, and one frontotemporal dementia behavioral variant with FTLD-TDP. The effect of blocking with the authentic reference material and with the MAO-B inhibitor deprenyl was assessed. Immunohistochemistry was performed on adjacent cryosections. Results Absence of specific [ 18 F]AV1451 binding was observed for all three SV PPA FTLD-TDP cases. The absence of binding in controls as well as the successful blocking with authentic AV1451 in cases with tauopathy demonstrated specificity of the [ 18 F]AV1451 signal for tau. The specific [ 18 F]AV1451 binding was highest in AD, followed by PiD. This binding colocalized with the respective tau lesions and could not be blocked by deprenyl. Similar pilot findings were obtained with [ 18 F]THK5351. Conclusion In vitro autoradiography showed no [ 18 F]AV1451 binding in SV PPA due to FTLD-TDP, while specific binding was present in SV PPA due to AD and PiD. The discrepancy between in vitro and in vivo findings remains to be explained. The discordance is not related to [ 18 F]AV1451 idiosyncrasies as [ 18 F]THK5351 findings were similar.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 47%

Section: Discussionmentioning

confidence: 64%

Section: Introductionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Binding of [18F]AV1451 in post mortem brain slices of semantic variant primary progressive aphasia patients

Schaeverbeke

Celen

Cornelis

et al. 2019

Eur J Nucl Med Mol Imaging

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Association of Cognitive and Behavioral Features Between Adults With Tuberous Sclerosis and Frontotemporal Dementia

et al. 2020

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IMPORTANCE Individuals with tuberous sclerosis complex can develop a progressive neuropsychiatric syndrome known as tuberous sclerosis-associated neuropsychiatric disorders. Tuberous sclerosis-associated neuropsychiatric disorders symptoms overlap with clinical criteria for frontotemporal dementia, yet the association between the 2 has not been explored.OBJECTIVE To investigate the potential association between tuberous sclerosis-associated neuropsychiatric disorders and frontotemporal dementia. DESIGN, SETTING, AND PARTICIPANTSCase-control study that enrolled patients with tuberous sclerosis complex with normal IQs in an observational clinical study at the University of California, San Francisco, from 2017 to 2019 where they underwent a comprehensive clinical evaluation including neuropsychologic testing, cerebral spinal fluid biomarker profiling, and structural neuroimaging. The study included adults who fulfilled the clinical criteria for tuberous sclerosis complex and had normal IQs, had frontotemporal dementia, or were healthy control individuals. MAIN OUTCOMES AND MEASURESTuberous sclerosis-associated neuropsychiatric disorders checklist severity score, neuropsychologic test scores, cerebral spinal fluid concentrations of phosphorylated tau 181 , total tau, amyloid-β 42, and neurofilament light chain. Amyloid and tau positron emission tomography scans were obtained in a subset of patients.RESULTS Eighteen patients with tuberous sclerosis complex (mean [SD] age, 48 years [9.54]; 13 women [72%]), 16 with frontotemporal dementia (60 [6.93] years; 7 women [44%]) and 18 healthy control individuals (63 [3.85] years; 9 women [50%]) were included. The tuberous sclerosis-associated neuropsychiatric disorders checklist and neuropsychological test results were not significantly different when the tuberous sclerosis complex and frontotemporal dementia cohorts were compared. The tuberous sclerosis complex cohort exhibited elevated cerebral spinal fluid phosphorylated tau 181 and neurofilament light chain with a mean of 32 pg/mL and 2300 pg/mL, respectively, when compared to healthy control individuals. All 3 patients with tuberous sclerosis complex who underwent fluorine 1B-labeled flortaucipir tau positron emission tomographic neuroimaging showed punctate foci of elevated [ 18 F]flortaucipir binding in the frontal and temporal regions.CONCLUSIONS AND RELEVANCE Adults with tuberous sclerosis complex showed phenotypic overlap with frontotemporal dementia. The results support a possible clinical continuum between tuberous sclerosis-associated neuropsychiatric disorders and frontotemporal dementia and highlights a potential pathophysiological link between neurodevelopmental and neurodegenerative processes. Quantitative neuropsychological testing and the tuberous sclerosis-associated neuropsychiatric disorders checklist, potentially supplemented by cerebral spinal fluid and imaging biomarkers, could be used to screen and prognosticate for risk of a neurodegenerative process in adult patients with tuberous sclerosis complex.

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Diagnostic Performance of RO948 F 18 Tau Positron Emission Tomography in the Differentiation of Alzheimer Disease From Other Neurodegenerative Disorders

et al. 2020

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The diagnostic performance of second-generation tau positron emission tomographic (PET) tracers is not yet known. OBJECTIVE To examine the novel tau PET tracer RO948 F 18 ([ 18 F]RO948) performance in discriminating Alzheimer disease (AD) from non-AD neurodegenerative disorders. DESIGN, SETTING, AND PARTICIPANTS In this diagnostic study, 613 participants in the Swedish BioFINDER-2 study were consecutively enrolled in a prospective cross-sectional study from September 4, 2017, to August 28, 2019. Participants included 257 cognitively unimpaired controls, 154 patients with mild cognitive impairment, 100 patients with AD dementia, and 102 with non-AD neurodegenerative disorders. Evaluation included a comparison of tau PET tracer [ 18 F]RO948 with magnetic resonance imaging (MRI) and cerebrospinal fluid and a head-to-head comparison between [ 18 F]RO948 and flortaucipir F 18 ([ 18 F]flortaucipir) in patients with semantic variant primary progressive aphasia (svPPA). EXPOSURES [ 18 F]RO948 (all patients) and [ 18 F]flortaucipir (3 patients with svPPA) tau PET; MRI (hippocampal volume, composite temporal lobe cortical thickness, whole-brain cortical thickness) and cerebrospinal fluid measures (p-tau181 and amyloid Aβ42 and Aβ40 ratio [Aβ42/Aβ40], and Aβ42/p-tau181 ratio). MAIN OUTCOMES AND MEASURES Standard uptake value ratios (SUVRs) in 4 predefined regions of interest (ROIs) reflecting Braak staging scheme for tau pathology and encompass I-II (entorhinal cortex), III-IV (inferior/middle temporal, fusiform gyrus, parahippocampal cortex, and amygdala), I-IV, and V-VI (widespread neocortical areas), area under the receiver operating characteristic curve (AUC) values, and subtraction images between [ 18 F]RO948 and [ 18 F]flortaucipir. RESULTS Diagnostic groups among the 613 participants included cognitively unimpaired (mean [SD] age, 65.8 [12.1] years; 117 men [46%]), mild cognitive impairment (age, 70.8 [8.3] years; 82 men [53%]), AD dementia (age, 73.5 [6.7] years; 57 men [57%]), and non-AD disorders (age, 70.5 [8.6] years; 41 men [40%]). Retention of [ 18 F]RO948 was higher in AD dementia compared with all other diagnostic groups. [ 18 F]RO948 could distinguish patients with AD dementia from individuals without cognitive impairment and those with non-AD disorders, and the highest AUC was obtained using the I-IV ROI (AUC = 0.98; 95% CI, 0.96-0.99 for AD vs no cognitive impairment and AUC = 0.97; 95% CI, 0.95-0.99 for AD vs non-AD disorders), which outperformed MRI (highest AUC = 0.91 for AD vs no cognitive impairment using whole-brain thickness, and AUC = 0.80 for AD vs non-AD disorders using temporal lobe thickness) and cerebrospinal fluid measures (highest AUC = 0.94 for AD vs no cognitive impairment using Aβ42/p-tau181, and AUC = 0.93 for AD vs non-AD disorders using Aβ42/Aβ40). Generally, tau PET positivity using [ 18 F]RO948 was observed only in Aβ-positive cases or in MAPT R406W mutation carriers. Retention of [ 18 F]RO948 was not pronounced in patients with svPPA, and head-to-head comparison revealed lower temp...

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18F-Flortaucipir in TDP-43 associated frontotemporal dementia

Cited by 31 publications

References 40 publications

Binding of [18F]AV1451 in post mortem brain slices of semantic variant primary progressive aphasia patients

Binding of [18F]AV1451 in post mortem brain slices of semantic variant primary progressive aphasia patients

Association of Cognitive and Behavioral Features Between Adults With Tuberous Sclerosis and Frontotemporal Dementia

Diagnostic Performance of RO948 F 18 Tau Positron Emission Tomography in the Differentiation of Alzheimer Disease From Other Neurodegenerative Disorders

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