Your search keyword '"Swieten, John C van"' showing total 27 results

1. Connecting dementia risk loci to the CSF proteome identifies pathophysiological leads for dementia.

Author

Reus, Lianne M, Jansen, Iris E, Tijms, Betty M, Visser, Pieter Jelle, Tesi, Niccoló, Lee, Sven J van der, Vermunt, Lisa, Peeters, Carel F W, Groot, Lisa A De, Hok-A-Hin, Yanaika S, Chen-Plotkin, Alice, Irwin, David J, Hu, William T, Meeter, Lieke H, Swieten, John C van, Holstege, Henne, Hulsman, Marc, Lemstra, Afina W, Pijnenburg, Yolande A L, and Flier, Wiesje M van der

Subjects

LEWY body dementia, FRONTOTEMPORAL dementia, LOCUS (Genetics), ALZHEIMER'S disease, DISEASE risk factors

Abstract

Genome-wide association studies have successfully identified many genetic risk loci for dementia, but exact biological mechanisms through which genetic risk factors contribute to dementia remains unclear. Integrating CSF proteomic data with dementia risk loci could reveal intermediate molecular pathways connecting genetic variance to the development of dementia. We tested to what extent effects of known dementia risk loci can be observed in CSF levels of 665 proteins [proximity extension-based (PEA) immunoassays] in a deeply-phenotyped mixed memory clinic cohort [ n = 502, mean age (standard deviation, SD) = 64.1 (8.7) years, 181 female (35.4%)], including patients with Alzheimer's disease (AD, n = 213), dementia with Lewy bodies (DLB, n = 50) and frontotemporal dementia (FTD, n = 93), and controls (n = 146). Validation was assessed in independent cohorts (n = 99 PEA platform, n = 198, mass reaction monitoring-targeted mass spectroscopy and multiplex assay). We performed additional analyses stratified according to diagnostic status (AD, DLB, FTD and controls separately), to explore whether associations between CSF proteins and genetic variants were specific to disease or not. We identified four AD risk loci as protein quantitative trait loci (pQTL): CR1 -CR2 (rs3818361, P = 1.65 × 10−8), ZCWPW1 -PILRB (rs1476679, P = 2.73 × 10−32), CTSH -CTSH (rs3784539, P = 2.88 × 10−24) and HESX1 -RETN (rs186108507, P = 8.39 × 10−8), of which the first three pQTLs showed direct replication in the independent cohorts. We identified one AD-specific association between a rare genetic variant of TREM2 and CSF IL6 levels (rs75932628, P = 3.90 × 10−7). DLB risk locus GBA showed positive trans effects on seven inter-related CSF levels in DLB patients only. No pQTLs were identified for FTD loci, either for the total sample as for analyses performed within FTD only. Protein QTL variants were involved in the immune system, highlighting the importance of this system in the pathophysiology of dementia. We further identified pQTLs in stratified analyses for AD and DLB, hinting at disease-specific pQTLs in dementia. Dissecting the contribution of risk loci to neurobiological processes aids in understanding disease mechanisms underlying dementia. [ABSTRACT FROM AUTHOR]

Published

2024

2. Impaired glymphatic system in genetic frontotemporal dementia: a GENFI study.

Author

Premi, Enrico, Diano, Matteo, Mattioli, Irene, Altomare, Daniele, Cantoni, Valentina, Bocchetta, Martina, Gasparotti, Roberto, Buratti, Emanuele, Pengo, Marta, Bouzigues, Arabella, Russell, Lucy L, Foster, Phoebe H, Ferry-Bolder, Eve, Heller, Carolin, Swieten, John C van, Jiskoot, Lize C, Seelaar, Harro, Moreno, Fermin, Sanchez-Valle, Raquel, and Galimberti, Daniela

Published

2024

3. CSF proteomics in autosomal dominant Alzheimer's disease highlights parallels with sporadic disease.

Author

Ende, Emma L van der, Veld, Sjors G J G In 't, Hanskamp, Iris, van der Lee, Sven, Dijkstra, Janna I R, Hok-A-Hin, Yanaika S, Blujdea, Elena R, Swieten, John C van, Irwin, David J, Chen-Plotkin, Alice, Hu, William T, Lemstra, Afina W, Pijnenburg, Yolande A L, Flier, Wiesje M van der, Campo, Marta del, Teunissen, Charlotte E, and Vermunt, Lisa

Subjects

ALZHEIMER'S disease, PROTEOMICS, BLOOD proteins, TISSUE remodeling, PROTEIN folding

Abstract

Autosomal dominant Alzheimer's disease (ADAD) offers a unique opportunity to study pathophysiological changes in a relatively young population with few comorbidities. A comprehensive investigation of proteome changes occurring in ADAD could provide valuable insights into AD-related biological mechanisms and uncover novel biomarkers and therapeutic targets. Furthermore, ADAD might serve as a model for sporadic AD, but in-depth proteome comparisons are lacking. We aimed to identify dysregulated CSF proteins in ADAD and determine the degree of overlap with sporadic AD. We measured 1472 proteins in CSF of PSEN1 or APP mutation carriers (n = 22) and age- and sex-matched controls (n = 20) from the Amsterdam Dementia Cohort using proximity extension-based immunoassays (PEA). We compared protein abundance between groups with two-sided t -tests and identified enriched biological pathways. Using the same protein panels in paired plasma samples, we investigated correlations between CSF proteins and their plasma counterparts. Finally, we compared our results with recently published PEA data from an international cohort of sporadic AD (n = 230) and non-AD dementias (n = 301). All statistical analyses were false discovery rate-corrected. We detected 66 differentially abundant CSF proteins (65 increased, 1 decreased) in ADAD compared to controls (q < 0.05). The most strongly upregulated proteins (fold change >1.8) were related to immunity (CHIT1, ITGB2, SMOC2), cytoskeletal structure (MAPT, NEFL) and tissue remodelling (TMSB10, MMP-10). Significant CSF-plasma correlations were found for the upregulated proteins SMOC2 and LILR1B. Of the 66 differentially expressed proteins, 36 had been measured previously in the sporadic dementias cohort, 34 of which (94%) were also significantly upregulated in sporadic AD, with a strong correlation between the fold changes of these proteins in both cohorts (rs = 0.730, P < 0.001). Twenty-nine of the 36 proteins (81%) were also upregulated among non-AD patients with suspected AD co-pathology. This CSF proteomics study demonstrates substantial biochemical similarities between ADAD and sporadic AD, suggesting involvement of the same biological processes. Besides known AD-related proteins, we identified several relatively novel proteins, such as TMSB10, MMP-10 and SMOC2, which have potential as novel biomarkers. With shared pathophysiological CSF changes, ADAD study findings might be translatable to sporadic AD, which could greatly expedite therapy development. [ABSTRACT FROM AUTHOR]

Published

2023

4. Differential Impairment Of Cerebrospinal Fluid Synaptic Biomarkers In The Genetic Forms Of Frontotemporal Dementia

Author

Sogorb-Esteve, Aitana, primary, Nilsson, Johanna, additional, Swift, Imogen J, additional, Heller, Carolin, additional, Russell, Lucy L., additional, Peakman, Georgia, additional, Convery, Rhian S., additional, Swieten, John C. van, additional, Seelaar, Harro, additional, Borroni, Barbara, additional, Galimberti, Daniela, additional, Sanchez-Valle, Raquel, additional, Laforce, Robert, additional, Moreno, Fermin, additional, Synofzik, Matthis, additional, Graff, Caroline, additional, Masellis, Mario, additional, Tartaglia, Maria Carmela, additional, Rowe, James B., additional, Vandenberghe, Rik, additional, Finger, Elizabeth, additional, Tagliavini, Fabrizio, additional, Santana, Isabel, additional, Butler, Chris R., additional, Ducharme, Simon, additional, Gerhard, Alexander, additional, Danek, Adrian, additional, Levin, Johannes, additional, Otto, Markus, additional, Sorbi, Sandro, additional, Ber, Isabelle Le, additional, Pasquier, Florence, additional, Gobom, Johan, additional, Brinkmalm, Ann, additional, Blennow, Kaj, additional, Zetterberg, Henrik, additional, and Rohrer, Jonathan D, additional

Published

2022

5. Language Impairment in the Genetic Forms of Behavioural Variant Frontotemporal Dementia

Author

Samra, Kiran, primary, MacDougall, Amy M, additional, Bouzigues, Arabella, additional, Bocchetta, Martina, additional, Cash, David M., additional, Greaves, Caroline V., additional, Convery, Rhian S., additional, Swieten, John C. van, additional, Jiskoot, Lize, additional, Moreno, Fermin, additional, Sanchez-Valle, Raquel, additional, Laforce, Robert, additional, Graff, Caroline, additional, Masellis, Mario, additional, Tartaglia, Carmela, additional, Rowe, James B., additional, Borroni, Barbara, additional, Finger, Elizabeth, additional, Synofzik, Matthis, additional, Otto, Markus, additional, Sorbi, Sandro, additional, Rohrer, Jonathan D., additional, Russell, Lucy L, additional, Galimberti, Daniela, additional, Vandenberge, Rik, additional, de Mendonça, Alexandre, additional, Butler, Chris R, additional, Gerhard, Alexander, additional, Ducharme, Simon, additional, Ber, Isabelle Le, additional, Tiraboschi, Pietro, additional, Santana, Isabel, additional, Pasquier, Florence, additional, and Levin, Johannes, additional

Published

2022

6. Apolipoprotein L1 is Increased in Frontotemporal Lobar Degeneration Post-mortem Brain but Not in Ante-mortem Cerebrospinal Fluid

Author

Hok-A-Hin, Yanaika Sylvana, primary, Dijkstra, Anke A, additional, Rábano, Alberto, additional, Hoozemans, Jeroen J, additional, Castillo, Lucia, additional, Seelaar, Harro, additional, Swieten, John C van, additional, Pijnenburg, Yolanda A.L., additional, Teunissen, Charlotte E, additional, and Campo, Marta Del, additional

Published

2022

7. Psychiatric symptoms of frontotemporal dementia and subcortical (co-)pathology burden: new insights.

Author

Scarioni, Marta, Gami-Patel, Priya, Peeters, Carel F W, Koning, Florianne de, Seelaar, Harro, Mol, Merel O, Swieten, John C van, Bank, Netherlands Brain, Rozemuller, Annemieke J M, Hoozemans, Jeroen J M, Pijnenburg, Yolande A L, and Dijkstra, Anke A

Subjects

FRONTOTEMPORAL dementia, DELUSIONS, BRAIN diseases, DNA-binding proteins, PATHOLOGY, LOCUS coeruleus, FRONTOTEMPORAL lobar degeneration

Abstract

Three subtypes of distinct pathological proteins accumulate throughout multiple brain regions and shape the heterogeneous clinical presentation of frontotemporal lobar degeneration (FTLD). Besides the main pathological subtypes, co-occurring pathologies are common in FTLD brain donors. The objective of this study was to investigate how the location and burden of (co-)pathology correlate to early psychiatric and behavioural symptoms of FTLD. Eighty-seven brain donors from The Netherlands Brain Bank cohort (2008–2017) diagnosed with FTLD were included: 46 FTLD-TAR DNA-binding protein 43 (FTLD-TDP), 34 FTLD-tau, and seven FTLD-fused-in-sarcoma (FTLD-FUS). Post-mortem brain tissue was dissected into 20 standard regions and stained for phosphorylated TDP-43, phosphorylated tau, FUS, amyloid-β, and α-synuclein. The burden of each pathological protein in each brain region was assessed with a semi-quantitative score. Clinical records were reviewed for early psychiatric and behavioural symptoms. Whole-brain clinico-pathological partial correlations were calculated (local false discovery rate threshold = 0.01). Elaborating on the results, we validated one finding using a quantitative assessment of TDP-43 pathology in the granular layer of the hippocampus in FTLD-TDP brain donors with (n = 15) and without (n = 15) hallucinations. In subcortical regions, the presence of psychiatric symptoms showed positive correlations with increased hippocampal pathology burden: hallucinations with TDP-43 in the granular layer (R = 0.33), mania with TDP-43 in CA1 (R = 0.35), depression with TDP-43 in CA3 and with parahippocampal tau (R = 0.30 and R = 0.23), and delusions with CA3 tau (R = 0.26) and subicular amyloid-β (R = 0.25). Behavioural disinhibition showed positive correlations with tau burden in the thalamus (R = 0.29) and with both TDP-43 and amyloid-β burden in the subthalamus (R = 0.23 and R = 0.24). In the brainstem, the presence of α-synuclein co-pathology in the substantia nigra correlated with disinhibition (R = 0.24), tau pathology in the substantia nigra correlated with depression (R = 0.25) and in the locus coeruleus with both depression and perseverative/compulsive behaviour (R = 0.26 and R = 0.32). The quantitative assessment of TDP-43 in the granular layer validated the higher burden of TDP-43 pathology in brain donors with hallucinations compared to those without hallucinations (P = 0.007). Our results show that psychiatric symptoms of FTLD are linked to subcortical pathology burden in the hippocampus, and hallucinations are linked to a higher burden of TDP-43 in the granular layer. Co-occurring non-FTLD pathologies in subcortical regions could contribute to configuring the clinical phenotype of FTLD. [ABSTRACT FROM AUTHOR]

Published

2023

8. Cognitive Composites for Genetic Frontotemporal Dementia: GENFI-Cog

Author

Poos, Jackie M., primary, Moore, Katrina M., additional, Nicholas, Jennifer, additional, Russell, Lucy L., additional, Peakman, Georgia, additional, Convery, Rhian S., additional, Jiskoot, Lize C., additional, Ende, Emma L. van der, additional, Berg, Esther van den, additional, Papma, Janne M., additional, Seelaar, Harro, additional, Pijnenburg, Yolande A.L., additional, Moreno, Fermin, additional, Sanchez-Valle, Raquel, additional, Borroni, Barbara, additional, Laforce, Robert, additional, Masellis, Mario, additional, Tartaglia, Carmela, additional, Graff, Caroline, additional, Galimberti, Daniela, additional, Rowe, James, additional, Finger, Elizabeth, additional, Synofzik, Matthis, additional, Vandenberghe, Rik, additional, Mendonça, Alexandre, additional, Tiraboschi, Pietro, additional, Santana, Isabel, additional, Ducharme, Simon, additional, Butler, Chris, additional, Gerhard, Alexander, additional, Levin, Johannes, additional, Danek, Adrian, additional, Otto, Markus, additional, Ber, Isabel Le, additional, Pasquier, Florence, additional, Swieten, John C. van, additional, and Rohrer, Jonathan D., additional

Published

2021

9. Apathy in presymptomatic genetic frontotemporal dementia predicts cognitive decline and is driven by structural brain changes

Author

Malpetti, M., Simon Jones, P., Tsvetanov, Kamen A., Rittman, Timothy, Swieten, John C. van, Borroni, Barbara, Kievit, R., Rowe, James B., Malpetti, M., Simon Jones, P., Tsvetanov, Kamen A., Rittman, Timothy, Swieten, John C. van, Borroni, Barbara, Kievit, R., and Rowe, James B.

Abstract

Contains fulltext : 240522.pdf (Publisher’s version ) (Open Access)

Published

2021

10. Differential early subcortical involvement in genetic FTD within the GENFI cohort

Author

Alzheimer's Research UK, Alzheimer Society, Brain Research UK, Wolfson Foundation, National Institute for Health Research (UK), University College London, Dementia Research Institute (UK), Medical Research Council (UK), Ministero della Salute, Canadian Institutes of Health Research, NVIDIA Corporation, Association for Frontotemporal Degeneration (US), European Research Council, European Commission, National Institutes of Health (US), Wellcome Trust, German Research Foundation, Munich Cluster for Systems Neurology, Bocchetta, Martina, Todd, Emily G., Peakman, Georgia, Cash, David M., Convery, Rhian S., Russell, Lucy L., Thomas, David L., Iglesias, Juan Eugenio, Swieten, John C. van, Jiskoot, Lize C., Seelaar, Harro, Borroni, Barbara, Galimberti, Daniela, Sánchez-Valle, Raquel, Laforce, Robert, Moreno, Fermín, Synofzik, Matthis, Graff, Caroline, Masellis, Mario, Tartaglia, Maria Carmela, Rowe, James, Vandenberghe, Rik, Finger, Elizabeth, Tagliavini, Fabrizio, Mendonça, Alexandre de, Santana, Isabel, Butler, Christopher, Ducharme, Simon, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Sorbi, Sandro, Le Ber, Isabelle, Pasquier, Florence, Rohrer, Jonathan D., Genetic Frontotemporal dementia Initiative, Alzheimer's Research UK, Alzheimer Society, Brain Research UK, Wolfson Foundation, National Institute for Health Research (UK), University College London, Dementia Research Institute (UK), Medical Research Council (UK), Ministero della Salute, Canadian Institutes of Health Research, NVIDIA Corporation, Association for Frontotemporal Degeneration (US), European Research Council, European Commission, National Institutes of Health (US), Wellcome Trust, German Research Foundation, Munich Cluster for Systems Neurology, Bocchetta, Martina, Todd, Emily G., Peakman, Georgia, Cash, David M., Convery, Rhian S., Russell, Lucy L., Thomas, David L., Iglesias, Juan Eugenio, Swieten, John C. van, Jiskoot, Lize C., Seelaar, Harro, Borroni, Barbara, Galimberti, Daniela, Sánchez-Valle, Raquel, Laforce, Robert, Moreno, Fermín, Synofzik, Matthis, Graff, Caroline, Masellis, Mario, Tartaglia, Maria Carmela, Rowe, James, Vandenberghe, Rik, Finger, Elizabeth, Tagliavini, Fabrizio, Mendonça, Alexandre de, Santana, Isabel, Butler, Christopher, Ducharme, Simon, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Sorbi, Sandro, Le Ber, Isabelle, Pasquier, Florence, Rohrer, Jonathan D., and Genetic Frontotemporal dementia Initiative

Abstract

Background: Studies have previously shown evidence for presymptomatic cortical atrophy in genetic FTD. Whilst initial investigations have also identified early deep grey matter volume loss, little is known about the extent of subcortical involvement, particularly within subregions, and how this differs between genetic groups. Methods: 480 mutation carriers from the Genetic FTD Initiative (GENFI) were included (198 GRN, 202 C9orf72, 80 MAPT), together with 298 non-carrier cognitively normal controls. Cortical and subcortical volumes of interest were generated using automated parcellation methods on volumetric 3 T T1-weighted MRI scans. Mutation carriers were divided into three disease stages based on their global CDR® plus NACC FTLD score: asymptomatic (0), possibly or mildly symptomatic (0.5) and fully symptomatic (1 or more). Results: In all three groups, subcortical involvement was seen at the CDR 0.5 stage prior to phenoconversion, whereas in the C9orf72 and MAPT mutation carriers there was also involvement at the CDR 0 stage. In the C9orf72 expansion carriers the earliest volume changes were in thalamic subnuclei (particularly pulvinar and lateral geniculate, 9–10%) cerebellum (lobules VIIa-Crus II and VIIIb, 2–3%), hippocampus (particularly presubiculum and CA1, 2–3%), amygdala (all subregions, 2–6%) and hypothalamus (superior tuberal region, 1%). In MAPT mutation carriers changes were seen at CDR 0 in the hippocampus (subiculum, presubiculum and tail, 3–4%) and amygdala (accessory basal and superficial nuclei, 2–4%). GRN mutation carriers showed subcortical differences at CDR 0.5 in the presubiculum of the hippocampus (8%). Conclusions: C9orf72 expansion carriers show the earliest and most widespread changes including the thalamus, basal ganglia and medial temporal lobe. By investigating individual subregions, changes can also be seen at CDR 0 in MAPT mutation carriers within the limbic system. Our results suggest that subcortical brain volumes may be used as

Published

2021

11. Brain functional network integrity sustains cognitive function despite atrophy in presymptomatic genetic frontotemporal dementia

Author

British Academy, Wellcome Trust, Medical Research Council (UK), German Research Foundation, University of Cambridge, Instituto de Salud Carlos III, Fundació La Marató de TV3, Canadian Institutes of Health Research, Ministero della Salute, National Institute for Health Research (UK), Association for Frontotemporal Degeneration (US), Munich Cluster for Systems Neurology, Swedish Research Council, Swedish Brain Foundation, Swedish Alzheimer Foundation, Stockholm County Council, Tsvetanov, Kamen A., Gazzina, Stefano, Jones, P. Simon, Swieten, John C. van, Borroni, Barbara, Sánchez-Valle, Raquel, Moreno, Fermín, Laforce, Robert, Graff, Caroline, Synofzik, Matthis, Galimberti, Daniela, Masellis, Mario, Tartaglia, Maria Carmela, Finger, Elizabeth, Vandenberghe, Rik, Mendonça, Alexandre de, Tagliavini, Fabrizio, Santana, Isabel, Ducharme, Simon, Butler, Christopher, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Frisoni, Giovanni, Ghidoni, Roberta, Sorbi, Sandro, Rohrer, Jonathan D., Rowe, James, The Genetic FTD Initiative GENFI, British Academy, Wellcome Trust, Medical Research Council (UK), German Research Foundation, University of Cambridge, Instituto de Salud Carlos III, Fundació La Marató de TV3, Canadian Institutes of Health Research, Ministero della Salute, National Institute for Health Research (UK), Association for Frontotemporal Degeneration (US), Munich Cluster for Systems Neurology, Swedish Research Council, Swedish Brain Foundation, Swedish Alzheimer Foundation, Stockholm County Council, Tsvetanov, Kamen A., Gazzina, Stefano, Jones, P. Simon, Swieten, John C. van, Borroni, Barbara, Sánchez-Valle, Raquel, Moreno, Fermín, Laforce, Robert, Graff, Caroline, Synofzik, Matthis, Galimberti, Daniela, Masellis, Mario, Tartaglia, Maria Carmela, Finger, Elizabeth, Vandenberghe, Rik, Mendonça, Alexandre de, Tagliavini, Fabrizio, Santana, Isabel, Ducharme, Simon, Butler, Christopher, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Frisoni, Giovanni, Ghidoni, Roberta, Sorbi, Sandro, Rohrer, Jonathan D., Rowe, James, and The Genetic FTD Initiative GENFI

Abstract

Introduction: The presymptomatic phase of neurodegenerative disease can last many years, with sustained cognitive function despite progressive atrophy. We investigate this phenomenon in familial frontotemporal dementia (FTD). Methods: We studied 121 presymptomatic FTD mutation carriers and 134 family members without mutations, using multivariate data-driven approach to link cognitive performance with both structural and functional magnetic resonance imaging. Atrophy and brain network connectivity were compared between groups, in relation to the time from expected symptom onset. Results: There were group differences in brain structure and function, in the absence of differences in cognitive performance. Specifically, we identified behaviorally relevant structural and functional network differences. Structure-function relationships were similar in both groups, but coupling between functional connectivity and cognition was stronger for carriers than for non-carriers, and increased with proximity to the expected onset of disease. Discussion: Our findings suggest that the maintenance of functional network connectivity enables carriers to maintain cognitive performance.

Published

2021

12. Dietary intake of antioxidants and risk of Alzheimer disease. (Original Contribution)

Author

Engelhart, Marianne J., Geerlings, Mirjam I., Ruitenberg, Annemieke, Swieten, John C. van, Hofman, Albert, Witteman, Jacqueline C.M., and Breteler, Monique M.B.

Subjects

Alzheimer's disease -- Prevention, Vitamin C -- Health aspects, Vitamin E -- Health aspects, Antioxidants -- Health aspects

Abstract

High levels of vitamins C and E in the diet may lower the risk of Alzheimer's disease, according to a study of 5,395 people. Vitamins C and E are anti-oxidants, and researchers believe free radical damage may be a risk factor for Alzheimer's disease., Context Laboratory findings have suggested that oxidative stress may contribute to the pathogenesis of Alzheimer disease. Therefore, the risk of Alzheimer disease might be reduced by intake of antioxidants that counteract the detrimental effects of oxidative stress. Objective To determine whether dietary intake of antioxidants is related to risk of Alzheimer disease. Design and Setting The Rotterdam Study, a population-based, prospective cohort study conducted in the Netherlands. Participants A total of 5395 participants who, at baseline (1990-1993), were aged at least 55 years, free of dementia, and noninstitutionalized and had reliable dietary assessment. Participants were reexamined in 1993-1994 and 1997-1999 and were continuously monitored for incident dementia. Main Outcome Measures Incidence of Alzheimer disease, based on Diagnostic and Statistical Manual of Mental Disorders, Revised Third Edition (DSM-III-R) criteria and National Institute of Neurological and Communicative Disorders and Stroke and Alzheimer Disease and Related Disorders Association (NINCDS-ADRDA) criteria, associated with dietary intake of beta carotene, flavonoids, vitamin C, and vitamin E. Results After a mean follow-up of 6 years, 197 participants developed dementia, of whom 146 had Alzheimer disease. When adjustments were made for age, sex, baseline Mini-Mental State Examination score, alcohol intake, education, smoking habits, pack-years of smoking, body mass index, total energy intake, presence of carotid plaques, and use of antioxidative supplements, high intake of vitamin C and vitamin E was associated with lower risk of Alzheimer disease (rate ratios [RRs] per 1-SD increase in intake were 0.82 [95% confidence interval {CI}, 0.68-0.99) and 0.82 [95% CI, 0.661.00], respectively). Among current smokers, this relationship was most pronounced (RRs, 0.65 [95% CI, 0.37-1.14] and 0.58 [95% CI, 0.30-1.12), respectively) and also was present for intake of beta carotene (RR, 0.49 [95% CI, 0.27-0.92]) and flavonoids (RR, 0.54 [95% CI, 0.31-0.96]). The associations did not vary by education or apolipoprotein E genotype. Conclusion High dietary intake of vitamin C and vitamin E may lower the risk of Alzheimer disease.

Published

2002

13. High prevalence of mutations in the microtubule-associated protein tau in a population study of frontotemporal dementia in the Netherlands

Author

Rizzu, Patrizia, Swieten, John C. Van, Joosse, Marijke, Hasegawa, Masato, Stevens, Martijn, Tibben, Aad, Niermeijer, Martinus F., Hillebrand, Marcel, Ravid, Rivka, Oostra, Ben A., Goedert, Michel, Duijn, Cornelia M. van, and Heutink, Peter

Subjects

Genetic disorders -- Research, Chromosome mapping -- Usage, Population genetics -- Research, Presenile dementia -- Genetic aspects, Brain -- Abnormalities, Biological sciences

Abstract

Genetic aspects of frontotemporal dementia (FTD) have been studied in the Netherlands. High prevalence of mutations has been found in the microtubule-associated protein tau in a population study. Thirty-seven patients had one or more first-degree relatives with dementia. Mutation in the tau gene existed in 17.8% of the patients with FTD and in 43% of patients with both FTD and a positive family FTD history. Three missense mutations were responsible for 15.6% of the mutations. Tau mutations are the source of a large fraction of familial FTD cases; families with FTD and no mutations in tau exist.

Published

1999

14. Comparison of clinical rating scales in genetic frontotemporal dementia within the GENFI cohort.

Author

Peakman, Georgia, Russell, Lucy L., Convery, Rhian S., Nicholas, Jennifer M., Swieten, John C. Van, Jiskoot, Lize C., Moreno, Fermin, Sanchez-Valle, Raquel, Laforce, Robert, Graff, Caroline, Masellis, Mario, Tartaglia, Maria Carmela, Rowe, James B., Borroni, Barbara, Finger, Elizabeth, Synofzik, Matthis, Galimberti, Daniela, Vandenberghe, Rik, de Mendonça, Alexandre, and Butler, Chris R.

Subjects

FRONTOTEMPORAL dementia, FRONTOTEMPORAL lobar degeneration, MEDICAL sciences, PARKINSONIAN disorders, MEDICAL genetics, DISEASE progression, RESEARCH, GENETIC mutation, NERVE tissue proteins, CROSS-sectional method, RESEARCH methodology, EVALUATION research, COMPARATIVE studies, RESEARCH funding, LONGITUDINAL method

Abstract

Background: Therapeutic trials are now underway in genetic forms of frontotemporal dementia (FTD) but clinical outcome measures are limited. The two most commonly used measures, the Clinical Dementia Rating (CDR)+National Alzheimer's Disease Coordinating Center (NACC) Frontotemporal Lobar Degeneration (FTLD) and the FTD Rating Scale (FRS), have yet to be compared in detail in the genetic forms of FTD.Methods: The CDR+NACC FTLD and FRS were assessed cross-sectionally in 725 consecutively recruited participants from the Genetic FTD Initiative: 457 mutation carriers (77 microtubule-associated protein tau (MAPT), 187 GRN, 193 C9orf72) and 268 family members without mutations (non-carrier control group). 231 mutation carriers (51 MAPT, 92 GRN, 88 C9orf72) and 145 non-carriers had available longitudinal data at a follow-up time point.Results: Cross-sectionally, the mean FRS score was lower in all genetic groups compared with controls: GRN mutation carriers mean 83.4 (SD 27.0), MAPT mutation carriers 78.2 (28.8), C9orf72 mutation carriers 71.0 (34.0), controls 96.2 (7.7), p<0.001 for all comparisons, while the mean CDR+NACC FTLD Sum of Boxes was significantly higher in all genetic groups: GRN mutation carriers mean 2.6 (5.2), MAPT mutation carriers 3.2 (5.6), C9orf72 mutation carriers 4.2 (6.2), controls 0.2 (0.6), p<0.001 for all comparisons. Mean FRS score decreased and CDR+NACC FTLD Sum of Boxes increased with increasing disease severity within each individual genetic group. FRS and CDR+NACC FTLD Sum of Boxes scores were strongly negatively correlated across all mutation carriers (rs=-0.77, p<0.001) and within each genetic group (rs=-0.67 to -0.81, p<0.001 in each group). Nonetheless, discrepancies in disease staging were seen between the scales, and with each scale and clinician-judged symptomatic status. Longitudinally, annualised change in both FRS and CDR+NACC FTLD Sum of Boxes scores initially increased with disease severity level before decreasing in those with the most severe disease: controls -0.1 (6.0) for FRS, -0.1 (0.4) for CDR+NACC FTLD Sum of Boxes, asymptomatic mutation carriers -0.5 (8.2), 0.2 (0.9), prodromal disease -2.3 (9.9), 0.6 (2.7), mild disease -10.2 (18.6), 3.0 (4.1), moderate disease -9.6 (16.6), 4.4 (4.0), severe disease -2.7 (8.3), 1.7 (3.3). Sample sizes were calculated for a trial of prodromal mutation carriers: over 180 participants per arm would be needed to detect a moderate sized effect (30%) for both outcome measures, with sample sizes lower for the FRS.Conclusions: Both the FRS and CDR+NACC FTLD measure disease severity in genetic FTD mutation carriers throughout the timeline of their disease, although the FRS may be preferable as an outcome measure. However, neither address a number of key symptoms in the FTD spectrum, for example, motor and neuropsychiatric deficits, which future scales will need to incorporate. [ABSTRACT FROM AUTHOR]

Published

2022

15. The inner fluctuations of the brain in presymptomatic Frontotemporal Dementia: The chronnectome fingerprint

Author

National Institutes of Health (US), National Science Foundation (US), Wellcome Trust, Premi, Enrico, Calhoun, Vince, D., Matteo, Gazzina, Stefano, Cosseddu, Maura, Alberici, Antonella, Archetti, Silvana, Paternicò, Donata, Gasparotti, Roberto, Swieten, John C. van, Galimberti, Daniela, Sánchez-Valle, Raquel, Laforce, Robert, Moreno, Fermín, Synofzik, Matthis, Graff, Caroline, Masellis, Mario, Tartaglia, Maria Carmela, Rowe, James, Vandenberghe, Rik, Finger, Elizabeth, Tagliavini, Fabrizio, Mendonça, Alexandre de, Santana, Isabel, Butler, Christopher, Ducharme, Simon, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Frisoni, Giovanni, Cappa, Stefano, Sorbi, Sandro, Padovani, Alessandro, Rohrer, Jonathan D., Borroni, Barbara, National Institutes of Health (US), National Science Foundation (US), Wellcome Trust, Premi, Enrico, Calhoun, Vince, D., Matteo, Gazzina, Stefano, Cosseddu, Maura, Alberici, Antonella, Archetti, Silvana, Paternicò, Donata, Gasparotti, Roberto, Swieten, John C. van, Galimberti, Daniela, Sánchez-Valle, Raquel, Laforce, Robert, Moreno, Fermín, Synofzik, Matthis, Graff, Caroline, Masellis, Mario, Tartaglia, Maria Carmela, Rowe, James, Vandenberghe, Rik, Finger, Elizabeth, Tagliavini, Fabrizio, Mendonça, Alexandre de, Santana, Isabel, Butler, Christopher, Ducharme, Simon, Gerhard, Alex, Danek, Adrian, Levin, Johannes, Otto, Markus, Frisoni, Giovanni, Cappa, Stefano, Sorbi, Sandro, Padovani, Alessandro, Rohrer, Jonathan D., and Borroni, Barbara

Abstract

Frontotemporal Dementia (FTD) is preceded by a long period of subtle brain changes, occurring in the absence of overt cognitive symptoms, that need to be still fully characterized. Dynamic network analysis based on resting-state magnetic resonance imaging (rs-fMRI) is a potentially powerful tool for the study of preclinical FTD. In the present study, we employed a “chronnectome” approach (recurring, time-varying patterns of connectivity) to evaluate measures of dynamic connectivity in 472 at-risk FTD subjects from the Genetic Frontotemporal dementia research Initiative (GENFI) cohort. We considered 249 subjects with FTD-related pathogenetic mutations and 223 mutation non-carriers (HC). Dynamic connectivity was evaluated using independent component analysis and sliding-time window correlation to rs-fMRI data, and meta-state measures of global brain flexibility were extracted. Results show that presymptomatic FTD exhibits diminished dynamic fluidity, visiting less meta-states, shifting less often across them, and travelling through a narrowed meta-state distance, as compared to HC. Dynamic connectivity changes characterize preclinical FTD, arguing for the desynchronization of the inner fluctuations of the brain. These changes antedate clinical symptoms, and might represent an early signature of FTD to be used as a biomarker in clinical trials.

Published

2019

16. Somatic TARDBP variants as a cause of semantic dementia.

Author

Rooij, Jeroen van, Mol, Merel O, Melhem, Shamiram, van der Wal, Pelle, Arp, Pascal, Paron, Francesca, Kaat, Laura Donker, Seelaar, Harro, Bank, Netherlands Brain, Miedema, Suzanne S M, Oshima, Takuya, Eggen, Bart J L, Uitterlinden, André, Meurs, Joyce van, Kesteren, Ronald E van, Smit, August B, Buratti, Emanuele, Swieten, John C van, van Rooij, Jeroen, and Donker Kaat, Laura

Subjects

DEMENTIA, DENTATE gyrus, MUTANT proteins, NEURODEGENERATION, NEURAL development, SENILE dementia, SEMANTICS, BIOCHEMISTRY, GENETICS, DNA, GENETIC mutation, RNA, PHENOMENOLOGY, COMPARATIVE studies, GENOMES, GENES, DNA-binding proteins, TDP-43 proteinopathies, FRONTOTEMPORAL dementia, DISEASE complications

Abstract

The aetiology of late-onset neurodegenerative diseases is largely unknown. Here we investigated whether de novo somatic variants for semantic dementia can be detected, thereby arguing for a more general role of somatic variants in neurodegenerative disease. Semantic dementia is characterized by a non-familial occurrence, early onset (<65 years), focal temporal atrophy and TDP-43 pathology. To test whether somatic variants in neural progenitor cells during brain development might lead to semantic dementia, we compared deep exome sequencing data of DNA derived from brain and blood of 16 semantic dementia cases. Somatic variants observed in brain tissue and absent in blood were validated using amplicon sequencing and digital PCR. We identified two variants in exon one of the TARDBP gene (L41F and R42H) at low level (1-3%) in cortical regions and in dentate gyrus in two semantic dementia brains, respectively. The pathogenicity of both variants is supported by demonstrating impaired splicing regulation of TDP-43 and by altered subcellular localization of the mutant TDP-43 protein. These findings indicate that somatic variants may cause semantic dementia as a non-hereditary neurodegenerative disease, which might be exemplary for other late-onset neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2020

17. Refining the Spectrum of Neuronal Intranuclear Inclusion Disease: A Case Report.

Author

Cupidi, Chiara, Dijkstra, Anke A, Melhem, Shami, Vernooij, Meike W, Severijnen, Lies-Anne, Hukema, Renate K, Rozemuller, Annemieke J M, Neumann, Manuela, Swieten, John C van, and Seelaar, Harro

Published

2019

18. Longitudinal multimodal MRI as prognostic and diagnostic biomarker in presymptomatic familial frontotemporal dementia.

Author

Jiskoot, Lize C, Panman, Jessica L, Meeter, Lieke H, Dopper, Elise G P, Kaat, Laura Donker, Franzen, Sanne, Ende, Emma L van der, Minkelen, Rick van, Rombouts, Serge A R B, Papma, Janne M, Swieten, John C van, Donker Kaat, Laura, van der Ende, Emma L, van Minkelen, Rick, and van Swieten, John C

Abstract

Developing and validating sensitive biomarkers for the presymptomatic stage of familial frontotemporal dementia is an important step in early diagnosis and for the design of future therapeutic trials. In the longitudinal Frontotemporal Dementia Risk Cohort, presymptomatic mutation carriers and non-carriers from families with familial frontotemporal dementia due to microtubule-associated protein tau (MAPT) and progranulin (GRN) mutations underwent a clinical assessment and multimodal MRI at baseline, 2-, and 4-year follow-up. Of the cohort of 73 participants, eight mutation carriers (three GRN, five MAPT) developed clinical features of frontotemporal dementia ('converters'). Longitudinal whole-brain measures of white matter integrity (fractional anisotropy) and grey matter volume in these converters (n = 8) were compared with healthy mutation carriers ('non-converters'; n = 35) and non-carriers (n = 30) from the same families. We also assessed the prognostic performance of decline within white matter and grey matter regions of interest by means of receiver operating characteristic analyses followed by stepwise logistic regression. Longitudinal whole-brain analyses demonstrated lower fractional anisotropy values in extensive white matter regions (genu corpus callosum, forceps minor, uncinate fasciculus, and superior longitudinal fasciculus) and smaller grey matter volumes (prefrontal, temporal, cingulate, and insular cortex) over time in converters, present from 2 years before symptom onset. White matter integrity loss of the right uncinate fasciculus and genu corpus callosum provided significant classifiers between converters, non-converters, and non-carriers. Converters' within-individual disease trajectories showed a relatively gradual onset of clinical features in MAPT, whereas GRN mutations had more rapid changes around symptom onset. MAPT converters showed more decline in the uncinate fasciculus than GRN converters, and more decline in the genu corpus callosum in GRN than MAPT converters. Our study confirms the presence of spreading predominant frontotemporal pathology towards symptom onset and highlights the value of multimodal MRI as a prognostic biomarker in familial frontotemporal dementia. [ABSTRACT FROM AUTHOR]

Published

2019

19. Identification of common variants influencing risk of the tauopathy progressive supranuclear palsy.

Author

Novartis, Federal Ministry of Education and Research (Germany), Helmholtz Association, European Commission, Höglinger, Günter U., Melhem, Nadine M., Dickson, Dennis W., Sleiman, Patrick M. A., Wang, Li-San, Klei, Lambertus, Rademakers, Rosa, Silva, Rohan de, Litvan, Irene, Riley, David E., Swieten, John C. van, Heutink, Peter, Wszolek, Zbigniew K., Uitti, Ryan J., Vandrovcova, Jana, Hurtig, Howard I., Gross, Rachel G., Maetzler, Walter, Goldwurm, Stefano, Tolosa, Eduardo, Borroni, Barbara, Pastor, Pau, Cantwell, Laura B., Han, Mi Ryung, Dillman, Allissa, Brug, Marcel P. van der, Gibbs, J. Raphael, Cookson, Mark R., Hernández, Dena G., Singleton, Andrew B., Farrer, Matthew J., Yu, Chang-En, Golbe, Lawrence I., Revesz, Tamas, Hardy, John, Lees, Andrew J., Devlin, Bernie, Hakonarson, Hakon, Müller, Ulrich, Schellenberg, Gerard D., Gerard D., Novartis, Federal Ministry of Education and Research (Germany), Helmholtz Association, European Commission, Höglinger, Günter U., Melhem, Nadine M., Dickson, Dennis W., Sleiman, Patrick M. A., Wang, Li-San, Klei, Lambertus, Rademakers, Rosa, Silva, Rohan de, Litvan, Irene, Riley, David E., Swieten, John C. van, Heutink, Peter, Wszolek, Zbigniew K., Uitti, Ryan J., Vandrovcova, Jana, Hurtig, Howard I., Gross, Rachel G., Maetzler, Walter, Goldwurm, Stefano, Tolosa, Eduardo, Borroni, Barbara, Pastor, Pau, Cantwell, Laura B., Han, Mi Ryung, Dillman, Allissa, Brug, Marcel P. van der, Gibbs, J. Raphael, Cookson, Mark R., Hernández, Dena G., Singleton, Andrew B., Farrer, Matthew J., Yu, Chang-En, Golbe, Lawrence I., Revesz, Tamas, Hardy, John, Lees, Andrew J., Devlin, Bernie, Hakonarson, Hakon, Müller, Ulrich, Schellenberg, Gerard D., and Gerard D.

Abstract

Progressive supranuclear palsy (PSP) is a movement disorder with prominent tau neuropathology. Brain diseases with abnormal tau deposits are called tauopathies, the most common being Alzheimer’s disease. Environmental causes of tauopathies include repetitive head trauma associated with some sports. To identify common genetic variation contributing to risk for tauopathies, we carried out a genome-wide association study of 1,114 PSP cases and 3,247 controls (Stage 1) followed up by a second stage where 1,051 cases and 3,560 controls were genotyped for Stage 1 SNPs that yielded P ≤ 10−3. We found significant novel signals (P < 5 × 10−8) associated with PSP risk at STX6, EIF2AK3, and MOBP. We confirmed two independent variants in MAPT affecting risk for PSP, one of which influences MAPT brain expression. The genes implicated encode proteins for vesicle-membrane fusion at the Golgi-endosomal interface, for the endoplasmic reticulum unfolded protein response, and for a myelin structural component.

Published

2011

20. Structural and functional brain connectivity in presymptomatic familial frontotemporal dementia

Author

Dopper, Elise G.P., Rombouts, Serge A.R.B., Jiskoot, Lize C., den Heijer, Tom, Graaf, J. Roos A. de, de Koning, Inge, Hammerschlag, Anke R., Seelaar, Harro, Seeley, William W., Veer, Ilya M., Buchem, Mark A. van, Rizzu, Patrizia, and Swieten, John C. van

Abstract

We aimed to investigate whether cognitive deficits and structural and functional connectivity changes can be detected before symptom onset in a large cohort of carriers of MAPT(microtubule-associated protein tau) or GRN(progranulin) mutations.

Published

2014

21. Structural and functional brain connectivity in presymptomatic familial frontotemporal dementia

Author

Dopper, Elise G.P., Rombouts, Serge A.R.B., Jiskoot, Lize C., Heijer, Tom den, Graaf, J. Roos A. de, Koning, Inge de, Hammerschlag, Anke R., Seelaar, Harro, Seeley, William W., Veer, Ilya M., Buchem, Mark A. van, Rizzu, Patrizia, and Swieten, John C. van

Abstract

We aimed to investigate whether cognitive deficits and structural and functional connectivity changes can be detected before symptom onset in a large cohort of carriers of microtubule-associated protein tauand progranulinmutations.

Published

2013

22. The ALS-FTD-Q

Author

Raaphorst, Joost, Beeldman, Emma, Schmand, Ben, Berkhout, Joris, Linssen, Wim H.J.P., Berg, Leonard H. van den, Pijnenburg, Yolande A., Grupstra, Hepke F., Weikamp, Janneke G., Schelhaas, H. Jurgen, Papma, Janne M., Swieten, John C. van, de Visser, Marianne, and Haan, Rob J. de

Abstract

The assessment of behavioral disturbances in amyotrophic lateral sclerosis (ALS) is important because of the overlap with the behavioral variant of frontotemporal dementia (ALS-bvFTD). Motor symptoms and dysarthria are not taken into account in currently used behavioral questionnaires. We examined the clinimetric properties of a new behavioral questionnaire for patients with ALS (Amyotrophic Lateral Sclerosis-Frontotemporal Dementia-Questionnaire ALS-FTD-Q).

Published

2012

23. Endogenous estradiol and risk of dementia in women and men: The Rotterdam Study

Author

Geerlings, Mirjam I., Launer, Lenore J., Jong, Frank H. De, Ruitenberg, Annemieke, Stijnen, Theo, Swieten, John C. Van, Hofman, Albert, Witteman, Jacqueline C. M., Pols, Huibert A. P., and Breteler, Monique M. B.

Abstract

We determined whether higher endogenous estradiol levels were associated with lower risk of dementia in older men and women not using hormonal replacement therapy, using a case-cohort design within the Rotterdam Study, a population-based follow-up study on chronic diseases, including dementia, in 7,983 subjects aged 55 years or older, and ongoing since 1990. The analyses were based on a random subcohort of 508 women and 438 men, and on 76 women and 53 men with incident dementia. Cox proportional hazards models with robustly estimated standard errors showed that in women higher levels of total estradiol were associated with higher risk of dementia (age-adjusted hazard ratio per standard deviation increase 1.38; 95% CI 1.04–1.84). Age-adjusted HR's of Alzheimer's disease and vascular dementia associated with higher levels of total estradiol (per SD increase) were 1.24 (95% CI 0.87–1.76) and 2.19 (95% CI 1.22–3.92), respectively. Similar results were observed for bioavailable estradiol. Additional adjustments for potential confounders did not change the results substantially. In men, no clear association was observed between estradiol levels and risk of dementia or its subtypes. The findings do not support the hypothesis that higher levels of endogenous estradiol reduce risk of dementia, neither in women nor in men. Ann Neurol 2003

Published

2003

24. Variable phenotypic expression and extensive tau pathology in two families with the novel <TOGGLE>tau</TOGGLE> mutation L315R

Author

Herpen, Esther Van, Rosso, Sonia M., Serverijnen, Lies-Anne, Yoshida, Hirotaka, Breedveld, Guido, Graaf, Raoul Van De, Kamphorst, Wouter, Ravid, Rivka, Willemsen, Rob, Dooijes, Dennis, Majoor-Krakauer, Daniëlle, Kros, Johan M., Crowther, R. Anthony, Goedert, Michel, Heutink, Peter, and Swieten, John C. Van

Abstract

Mutations in the tau gene cause familial frontotemporal dementia and parkinsonism linked to chromosome 17. Here, we describe two Dutch families with familial frontotemporal dementia associated with the novel missense mutation L315R in exon 11 of tau. The age at onset of disease showed a large variation within each family, ranging from 25 to 64 years. Incomplete penetrance was established in an 82-year-old mutation carrier with no signs of dementia and appeared probable in two additional subjects. The brains of two affected subjects were studied and showed extensive tau pathology in neurons (Pick-like inclusions) and astroglial cells, particularly in the frontotemporal cortex and the hippocampal formation. Sarkosyl-insoluble tau extracted from the cerebral cortex showed the presence of straight and twisted tau filaments and a pattern of pathological tau bands similar to that of Pick's disease. Upon dephosphorylation, only five of the six brain tau isoforms were observed, with the shortest isoform being undetectable. All six tau isoforms were present in soluble brain tau. Recombinant tau proteins with the L315R mutation showed a reduced ability to promote microtubule assembly. Ann Neurol 2003;54:573–581

Published

2003

25. New developments in frontotemporal dementia and parkinsonism linked to chromosome 17

Author

Rosso, Sonia M. and Swieten, John C. van

Abstract

The identification of taumutations in frontotemporal dementia and parkinsonism linked to chromosome 17 (FTDP-17) has revealed invaluable information regarding the role of the tau protein in neurodegenerative disease. Over the past year several new mutations have been identified, and experimental studies have provided further insight into the mechanism of neurodegeneration due to taumutations and possible interactions with amyloid pathology.

Published

2002

26. FTDALS families are no longer orphaned

Author

Swieten, John C. van and Grossman, Murray

Published

2012

27. Whole-Genome Sequencing Analysis Reveals New Susceptibility Loci and Structural Variants Associated with Progressive Supranuclear Palsy.

Author

Wang H, Chang TS, Dombroski BA, Cheng PL, Patil V, Valiente-Banuet L, Farrell K, Mclean C, Molina-Porcel L, Rajput A, De Deyn PP, Bastard NL, Gearing M, Kaat LD, Swieten JCV, Dopper E, Ghetti BF, Newell KL, Troakes C, de Yébenes JG, Rábano-Gutierrez A, Meller T, Oertel WH, Respondek G, Stamelou M, Arzberger T, Roeber S, Müller U, Hopfner F, Pastor P, Brice A, Durr A, Ber IL, Beach TG, Serrano GE, Hazrati LN, Litvan I, Rademakers R, Ross OA, Galasko D, Boxer AL, Miller BL, Seeley WW, Deerlin VMV, Lee EB, White CL 3rd, Morris H, de Silva R, Crary JF, Goate AM, Friedman JS, Leung YY, Coppola G, Naj AC, Wang LS, Dickson DW, Höglinger GU, Schellenberg GD, Geschwind DH, and Lee WP

Abstract

Background: Progressive supranuclear palsy (PSP) is a rare neurodegenerative disease characterized by the accumulation of aggregated tau proteins in astrocytes, neurons, and oligodendrocytes. Previous genome-wide association studies for PSP were based on genotype array, therefore, were inadequate for the analysis of rare variants as well as larger mutations, such as small insertions/deletions (indels) and structural variants (SVs)., Method: In this study, we performed whole genome sequencing (WGS) and conducted association analysis for single nucleotide variants (SNVs), indels, and SVs, in a cohort of 1,718 cases and 2,944 controls of European ancestry. Of the 1,718 PSP individuals, 1,441 were autopsy-confirmed and 277 were clinically diagnosed., Results: Our analysis of common SNVs and indels confirmed known genetic loci at MAPT , MOBP , S TX6 , SLCO1A2 , DUSP10 , and SP1 , and further uncovered novel signals in APOE , FCHO1/MAP1S, KIF13A, TRIM24, TNXB, and ELOVL1 . Notably, in contrast to Alzheimer's disease (AD), we observed the APOE ε2 allele to be the risk allele in PSP. Analysis of rare SNVs and indels identified significant association in ZNF592 and further gene network analysis identified a module of neuronal genes dysregulated in PSP. Moreover, seven common SVs associated with PSP were observed in the H1/H2 haplotype region (17q21.31) and other loci, including IGH , PCMT1 , CYP2A13 , and SMCP . In the H1/H2 haplotype region, there is a burden of rare deletions and duplications ( P = 6.73×10 -3 ) in PSP., Conclusions: Through WGS, we significantly enhanced our understanding of the genetic basis of PSP, providing new targets for exploring disease mechanisms and therapeutic interventions., Competing Interests: Competing interests Laura Molina-Porcel received income from Biogen as a consultant in 2022. Gesine Respondek is now employed by Roche (Hoffmann-La Roche, Basel, Switzerland) since 2021. Her affiliation whilst completing her contribution to this manuscript was German Center for Neurodegenerative Diseases (DZNE), Munich, Germany. Thomas G Beach is a consultant for Aprinoia Therapeutics and a Scientific Advisor and stock option holder for Vivid Genomics. Huw Morris is employed by UCL. In the last 12 months he reports paid consultancy from Roche, Aprinoia, AI Therapeutics and Amylyx; lecture fees/honoraria - BMJ, Kyowa Kirin, Movement Disorders Society. Huw Morris is a co-applicant on a patent application related to C9ORF72 - Method for diagnosing a neurodegenerative disease (PCT/GB2012/052140). Giovanni Coppola is currently an employee of Regeneron Pharmaceuticals. Alison Goate serves on the SAB for Genentech and Muna Therapeutics.

Published

2024