Sequential distribution of pTDP-43 pathology in behavioral variant frontotemporal dementia (bvFTD)

Brettschneider, Johannes; Tredici, Kelly Del; Irwin, David J.; Grossman, Murray; Robinson, John; Toledo, Jon B.; Fang, Lubin; Deerlin, Vivianna M. Van; Ludolph, Albert C.; Lee, Virginia M.‐Y.; Braak, Heiko; Trojanowski, John Q.

doi:10.1007/s00401-013-1238-y

Cited by 242 publications

(290 citation statements)

References 110 publications

(165 reference statements)

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“…Family history for ALS was more prevalent in pure bvFTD cases with TDP-43 in the hypoglossal nucleus, but this did not reach significance compared to other bvFTD cohorts (p = 0.06). The recent topographical staging of TDP-43 pathology in bvFTD and ALS [6,7] demonstrated that TDP-43 initiated in the motor system network in ALS is also seen in the majority of bvFTD cases, despite the absence of ALS in over 50% of these [6,21]. In a recent analysis [21], we identified the hypoglossal nucleus as a key brain region in discriminating between cases with and without ALS and the present study corroborates this finding in bvFTD cases.…”

Section: Demographic Featuressupporting

confidence: 88%

“…The TAR DNA-binding protein 43 (TDP-43) in behavioral variant frontotemporal dementia (bvFTD) was recently proposed to have a regional distribution, initiated in the orbitofrontal cortex and amygdala before progressing to the frontal and temporal cortices, eventually involving the motor system, visual cortex and cerebellum [5]. Although the majority of bvFTD cases were found to have TDP-43 pathology in motor system regions, less than half of these demonstrated clinical features suggestive or diagnostic of amyotrophic lateral sclerosis (ALS) [5].…”

Section: Introductionmentioning

confidence: 99%

“…Although the majority of bvFTD cases were found to have TDP-43 pathology in motor system regions, less than half of these demonstrated clinical features suggestive or diagnostic of amyotrophic lateral sclerosis (ALS) [5].…”

Section: Introductionmentioning

confidence: 99%

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TDP-43 in the hypoglossal nucleus identifies amyotrophic lateral sclerosis in behavioral variant frontotemporal dementia

Halliday

Kiernan

Kril

et al. 2016

Journal of the Neurological Sciences

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The hypoglossal nucleus was recently identified as a key brain region in which the presence of TDP-43 pathology could accurately discriminate TDP-43 proteinopathy cases with clinical amyotrophic lateral sclerosis (ALS). The objective of the present study was to assess the hypoglossal nucleus in behavioral variant frontotemporal dementia (bvFTD), and determine whether TDP-43 in this region is associated with clinical ALS. Twenty-nine cases with neuropathological FTLD-TDP and clinical bvFTD that had not been previously assessed for hypoglossal TDP-43 pathology were included in this study. Of these 29 cases, 41% (n=12) had a dual diagnosis of bvFTD-ALS at presentation, all 100% (n=12) of which demonstrated hypoglossal TDP-43 pathology. Of the 59% (n=17) cohort that presented with pure bvFTD, 35% (n=6) were identified with hypoglossal TDP-43 pathology. Review of the case files of all pure bvFTD cases revealed evidence of possible or probable ALS in 5 of the 6 hypoglossal-positive cases (83%) towards the end of disease, and this was absent from all cases without such pathology. In conclusion, the present study validates grading the presence of TDP-43 in the hypoglossal nucleus for the pathological identification of bvFTD cases with clinical ALS, and extends this to include the identification of cases with possible ALS at end-stage.

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Section: Demographic Featuressupporting

confidence: 88%

Section: Introductionmentioning

confidence: 99%

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TDP-43 in the hypoglossal nucleus identifies amyotrophic lateral sclerosis in behavioral variant frontotemporal dementia

Halliday

Kiernan

Kril

et al. 2016

Journal of the Neurological Sciences

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“…Indeed, PSP and other forms of FTLD-tau have significant WM oligodendritic pathology 28,29 that is more prominent than in FTLD-TDP. [30][31][32] While animal-and cell-model experiments are needed to clarify the normal function of MOBP and the association of the rs1768208 polymorphism with neurodegeneration in FTLD, our neuroimaging findings are consistent with the possibility that degeneration particularly involving WM myelin may be contributing to poorer prognosis in MOBP RA1 patients. Specifically, we found increased RD in the WM of the midbrain and SCR, and additional decrease in FA in the SLF and ILF ( figure 2, A and B) in MOBP RA1 patients.…”

supporting

confidence: 76%

Myelin oligodendrocyte basic protein and prognosis in behavioral-variant frontotemporal dementia

et al. 2014

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Objective: To determine the prognostic utility of tauopathy-associated single nucleotide polymorphisms (SNPs) in sporadic behavioral-variant frontotemporal dementia (bvFTD).Methods: Eighty-one patients with sporadic bvFTD were genotyped for tauopathy-associated SNPs at rs8070723 (microtubule-associated protein tau [MAPT]) and rs1768208 (myelin-associated oligodendrocyte basic protein [MOBP]). We performed a retrospective case-control study comparing age at onset and disease duration between carriers of $1 polymorphism allele and noncarriers for these SNPs. Subanalyses were performed for autopsied subgroups with tauopathy (n 5 20) and TDP-43 proteinopathy (n 5 12). To identify a potential biological basis for disease duration, neuroimaging measures of white matter integrity were evaluated (n 5 37).Results: Carriers of risk allele (T) in rs1768208 (i.e., MOBP RA1) had a shorter median disease duration (TC/TT 5 5.5 years, CC 5 9.5 years; p 5 0.02). This was also found in the subset of cases with autopsy-confirmed tauopathies (p 5 0.04) but not with TDP-43 proteinopathies (p . 0.1). By comparison, polymorphisms at rs8070723 (MAPT) had no effect on disease duration (p . 0.1), although carriers of protective allele (G) in rs8070723 had a younger median age at onset (AG/GG 5 54.5 years, AA 5 58 years; p , 0.01). MOBP RA1 patients had increased radial diffusivity in the superior corona radiata and midbrain, and reduced fractional anisotropy in the superior corona radiata as well as superior and inferior longitudinal fasciculi compared with noncarriers (p , 0.01). Conclusions:The rs1768208 risk polymorphism in MOBP may have prognostic value in bvFTD.MOBP RA1 patients have more severe white matter degeneration in bvFTD that may contribute to shorter disease duration. Future studies are needed to help confirm these findings. Neurology ® 2014;83:502-509 GLOSSARY AD 5 Alzheimer disease; ALS 5 amyotrophic lateral sclerosis; bvFTD 5 behavioral-variant frontotemporal dementia; FA 5 fractional anisotropy; FTD 5 frontotemporal dementia; FTLD 5 frontotemporal lobar degeneration; GM 5 gray matter; GMD 5 gray matter density; ILF 5 inferior longitudinal fasciculus; MAPT 5 microtubule-associated protein tau; MOBP 5 myelin-associated oligodendrocyte basic protein; PA 5 protective allele; PSP 5 progressive supranuclear palsy; RA 5 risk allele; RD 5 radial diffusion; SCR 5 superior corona radiata; SLF 5 superior longitudinal fasciculus; SNP 5 single nucleotide polymorphism; STG 5 superior temporal gyrus; TDP-43 5 TAR DNA-binding protein 43; WM 5 white matter.Significant heterogeneity exists in the natural history of behavioral-variant frontotemporal dementia (bvFTD), the most common clinical phenotype in frontotemporal lobar degeneration (FTLD) spectrum pathology. Approximately equal numbers of cases appear to be attributable to the 2 main broad categories of proteinopathies 1,2 : those containing pathologic aggregations of the microtubule-associated protein, tau (i.e., FTLD-tau), 3 and those with inclusions composed of the RNA-b...

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“…In contrast, our data in FTLD-TDPC finds similar disease burden in STG and ACG compared with a lower amount of TDP-43 pathology in MFG. However, we previously found MFG, STG and ACG affected in the same early phase of pathology through examination of 70-µm-thick sections (Brettschneider et al 2014); that study included other FTLD-TDP subtypes (i.e., A, B) and ordinal ratings of both STG and MTG combined, in comparison to our present focused study of STG, which may explain this partial discrepancy. Further study is needed to determine the exact nature of associations between staging and quantitative measures of pathological burden in FTLD.…”

Section: Discussionmentioning

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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Sequential distribution of pTDP-43 pathology in behavioral variant frontotemporal dementia (bvFTD)

Cited by 242 publications

References 110 publications

TDP-43 in the hypoglossal nucleus identifies amyotrophic lateral sclerosis in behavioral variant frontotemporal dementia

TDP-43 in the hypoglossal nucleus identifies amyotrophic lateral sclerosis in behavioral variant frontotemporal dementia

Myelin oligodendrocyte basic protein and prognosis in behavioral-variant frontotemporal dementia

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

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