Your search keyword '"Polvikoski, Tuomo"' showing total 8 results

1. TDP-43 Related Neuropathologies and Phosphorylation State: Associations with Age and Clinical Dementia in the Cambridge City over-75s Cohort.

Author

Hunter, Sally, Hokkanen, Suvi R.K., Keage, Hannah A.D., Fleming, Jane, Minett, Thais, Polvikoski, Tuomo, Allinson, Kieren, Brayne, Carol, and Cambridge City over 75s Cohort collaboration

Subjects

DEMENTIA, NEUROLOGICAL disorders, PHOSPHORYLATION, CARRIER proteins, PHYSIOLOGICAL control systems, BIOLOGICAL classification, CELL metabolism, RESEARCH, HIPPOCAMPUS (Brain), NEURONS, AGE distribution, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, AGING, CELLS, RESEARCH funding, TDP-43 proteinopathies, NEURODEGENERATION

Abstract

Pathologies associated with the Tar-DNA binding protein 43 KDa (TDP-43) are associated with neurodegenerative diseases and aging. Phosphorylation of cellular proteins is a well-accepted mechanism of biological control and can be associated with disease pathways. Phosphorylation state associated with TDP-43 associated pathology has not been investigated with respect to dementia status in a population representative sample. TDP-43 immunohistochemistry directed toward phosphorylated (TDP-43P) and unphosphorylated (TDP-43U) was assessed in sections of hippocampus and temporal cortex from 222 brains donated to the population representative Cambridge City over-75s Cohort. Relationships between dementia status and age at death for TDP-43 immunoreactive pathologies by phosphorylation state were investigated. TDP-43 pathologies are common in the oldest old in the population and often do not conform to MacKenzie classification. Increasing age is associated with glial (TDP-43P) and neuronal inclusions (TDP-43P and TDP-43U), neurites, and granulovacuolar degeneration (GVD). Dementia status is associated with GVD and glial (TDP-43 P) and neural inclusions (TDP-43 P and U). Dementia severity was associated with glial (TDP-43P) and neuronal inclusions (TDP-43U and TDP-43P), GVD, and neurites. The associations between dementia severity and both glial cytoplasmic inclusions and GVD were independent from other pathologies and TDP-43 neuronal cytoplasmic inclusions. TDP-43 pathology contributes to dementia status and progression in a variety of ways in different phosphorylation states involving both neurons and glia, independently from age and from classic Alzheimer-related pathologies. TDP-43 pathologies as cytoplasmic inclusions in neurons or glia or as GVD contribute independently to dementia. [ABSTRACT FROM AUTHOR]

Published

2020

2. Hippocampal Sclerosis in the Oldest Old: A Finnish Population-Based Study

Author

Kero, Mia, primary, Raunio, Anna, additional, Polvikoski, Tuomo, additional, Tienari, Pentti J., additional, Paetau, Anders, additional, and Myllykangas, Liisa, additional

Published

2018

3. Amygdala α-Synuclein Pathology in the Population-Based Vantaa 85+ Study

Author

Raunio, Anna, primary, Myllykangas, Liisa, additional, Kero, Mia, additional, Polvikoski, Tuomo, additional, Paetau, Anders, additional, and Oinas, Minna, additional

Published

2017

4. Capillary Amyloid-β Protein Deposition in a Population-Based Study (Vantaa 85+)

Author

Mäkelä, Mira, primary, Paetau, Anders, additional, Polvikoski, Tuomo, additional, Myllykangas, Liisa, additional, and Tanskanen, Maarit, additional

Published

2015

5. APOE and AβPP Gene Variation in Cortical and Cerebrovascular Amyloid-β Pathology and Alzheimer's Disease: A Population-Based Analysis

Author

Peuralinna, Terhi, primary, Tanskanen, Maarit, additional, Mäkelä, Mira, additional, Polvikoski, Tuomo, additional, Paetau, Anders, additional, Kalimo, Hannu, additional, Sulkava, Raimo, additional, Hardy, John, additional, Lai, Shiao-Lin, additional, Arepalli, Sampath, additional, Hernandez, Dena, additional, Traynor, Bryan J., additional, Singleton, Andrew, additional, Tienari, Pentti J., additional, and Myllykangas, Liisa, additional

Published

2011

6. Capillary amyloid-β protein deposition in a population-based study (Vantaa 85+).

Author

Mäkelä, Mira, Paetau, Anders, Polvikoski, Tuomo, Myllykangas, Liisa, and Tanskanen, Maarit

Subjects

CEREBRAL amyloid angiopathy, NEUROLOGICAL disorders, APOLIPOPROTEIN E genetics, AMYLOID beta-protein, IMMUNOHISTOCHEMISTRY, ALZHEIMER'S disease, APOLIPOPROTEINS, AUTOPSY, CAPILLARIES, LONGITUDINAL method, MULTIVARIATE analysis, OCCIPITAL lobe, PEPTIDES, LOGISTIC regression analysis, SEVERITY of illness index, GENOTYPES

Abstract

Background: Capillary amyloid-β (capAβ) deposition in the cerebral cortex is the neuropathological feature providing the basis for categorizing cerebral amyloid angiopathy (CAA) into two distinct types, CAA-Type1 with capAβ and CAA-Type2 without capAβ.Objective: We investigated the neuropathological and clinical characteristics of capAβ deposition in a prospective population-based study.Methods: Vantaa 85+ includes 601 individuals aged ≥85 years, of which 300 were studied clinically and neuropathologically. 278 subjects were analyzed for the apolipoprotein E (APOE) genotype. The diagnosis of capAβ was determined using immunohistochemistry against Aβ, and of CAA using Congo red confirmed by Aβ immunohistochemistry, both analyzed in six brain areas. The severity of capAβ was graded semi-quantitatively, and the severity of CAA was based on the percentage of affected vessels. Alzheimer's disease (AD)-type neuropathology (CERAD score and Braak stage) was analyzed using standard methods.Results: CAA-Type1 was present in 86/300, CAA-Type2 in 135/300, and 79/300 had no CAA. CapAβ was most frequent in the occipital lobe (79/86). CAA-Type1 was associated with the severity of CAA (p <  0.001), dementia (p <  0.001), severe AD-type neuropathology (p-value 0.09 for CERAD C and 0.017 for Braak stages V-VI), and APOE ɛ4 allele carrier status (p <  0.001).Conclusions: This population-based study confirmed the presence of distinct CAA-Type1 and its association with the severity of CAA, severe AD-type neuropathology, and the APOE ɛ4 carrier status. Both the severity and localization of the deposition seemed to determine the clinical significance of capAβ. [ABSTRACT FROM AUTHOR]

Published

2016

7. Neuropathologic Findings of Dementia with Lewy Bodies (DLB) in a Population-based Vantaa 85+ Study.

Author

Oinas, Minna, Polvikoski, Tuomo, Sulkava, Raimo, Myllykangas, Liisa, Juva, Kati, Notkola, Irma-Leena, Rastas, Sari, Niinistö, Leena, Kalimo, Hannu, and Paetau, Anders

Subjects

*MEDICAL research, *LEWY body dementia, *NEUROLOGICAL disorders, *EXTRAPYRAMIDAL disorders, *DISEASES in older people, *GUIDELINES

Abstract

The consortium on dementia with Lewy bodies has established consensus guidelines for the neuropathologic diagnosis of dementia with Lewy bodies (DLB) including the likelihood that the neuropathologic findings associate with the clinical syndrome. Nevertheless, clinico-pathological correlations remain controversial. We applied the consensus guidelines for determining Lewy-related pathology (LRP) and evaluated the clinical presentation in the prospective, population-based Vantaa 85+ study consisting of individuals at least 85 years of age. LRP was seen in 36% of 304 subjects and categorized as follows: 3% brainstem-predominant, 14% limbic, 15% diffuse neocortical type (4% could not be categorized). The likelihood that the neuropathology predicts the DLB clinical syndrome was low in 6%, intermediate in 13%, and high in 13% of all 304 subjects. In the latter two groups, 77% were demented, 35% had at least one extrapyramidal symptom, and 15% had visual hallucinations. Surprisingly, DLB clinical features associated better with high neurofibrillary stage than with diffuse neocortical LRP. Moreover, the neurofibrillary stage, substantia nigra neuron loss, and grade of Lewy neurites in hippocampal CA2-3 region, each showed a significant association with the extent of LRP. In conclusion, the neuropathologic DLB in this very elderly population was common, but the clinical symptoms tended to associate better with severe neurofibrillary pathology than with extensive LRP. [ABSTRACT FROM AUTHOR]

Published

2009

8. Cohort profile: Epidemiological Clinicopathological Studies in Europe (EClipSE)

Author

Hannah Keage, Carol Brayne, Fiona Matthews, Brayne, Carol, Ince, Paul, Keage, Hannah, McKeith, ian, Matthews, Fiona, Polvikoski, Tuomo, and Sulkava, R

Subjects

Male, Gerontology, medicine.medical_specialty, Pathology, brain, Population, population, Neuropathology, Cohort Studies, Epidemiology, Prevalence, medicine, Humans, Dementia, education, Aged, Eclipse, Aged, 80 and over, education.field_of_study, business.industry, General Neuroscience, aging, Brain, health, Cognition, General Medicine, medicine.disease, Tissue Donors, Europe, Psychiatry and Mental health, Clinical Psychology, Cohort, Other Psychology and Cognitive Sciences, epidemiology, Female, Geriatrics and Gerontology, business, dementia

Abstract

Epidemiological Clinicopathological Studies in Europe (EClipSE) is the harmonization of neuropathological and longitudinal clinical data from three population-based prospective longitudinal studies of aging. The EClipSE database (Version 1.0) comprises data from the first 970 people who donated their brain at death and this number will increase. EClipSE enables sociodemographic, health, cognitive, and genetic measures collected during life to be related to neuropathology at death, testing hypotheses which require more power than has been previously possible. EClipSE aims to help throw light on relationships between biological, health and psychological factors underlying ageing and the manifestation of clinical dementia.

Published

2009