Author: "Remes, A. M. (Anne M.)" - Searchworks@Jio Institute Digital Library Search Results

Your search keyword '"Remes, A. M. (Anne M.)"' showing total 65 results

Start Over Author "Remes, A. M. (Anne M.)"

65 results on '"Remes, A. M. (Anne M.)"'

1. The Cognitive Function at Work Questionnaire (CFWQ):a new scale for measuring cognitive complaints in occupational population

Author: Heikkinen, A.-L. (Anna-Leena), Hänninen, T. (Tuomo), Kuikka, P. (Pekka), Akila, R. (Ritva), Savolainen, A. (Aslak), Valtonen, T. (Teppo), Umer, A. (Adil), Lötjönen, J. (Jyrki), Hublin, C. (Christer), Remes, A. M. (Anne M.), Paajanen, T. (Teemu), Heikkinen, A.-L. (Anna-Leena), Hänninen, T. (Tuomo), Kuikka, P. (Pekka), Akila, R. (Ritva), Savolainen, A. (Aslak), Valtonen, T. (Teppo), Umer, A. (Adil), Lötjönen, J. (Jyrki), Hublin, C. (Christer), Remes, A. M. (Anne M.), and Paajanen, T. (Teemu)
Abstract: Cognitive functioning is a relevant work and health related topic, however, validated methods to assess subjective cognitive complaints (SCC) at work are lacking. We introduce the Cognitive Function at Work Questionnaire (CFWQ) for measuring SCC in occupational settings. 1-year follow-up data of 418 employees from a Finnish public media service company was analyzed. Participants completed web-based CFWQ, cognitive tests and a broad set of questionnaires for evaluating depression, anxiety, insomnia, daytime sleepiness, burnout, stress, mental job burden, work ability, cognitive errors, and perceived health. The factor analysis yielded a model with the CFWQ subdomains: Memory, Language, Executive Function, Speed of Processing, Cognitive Control and Name Memory. The internal consistency (Cronbach’s alpha = 0.87) and the test-retest constancy (ICC = 0.84) reflected good reliability. Correlation between the CFWQ and cognitive errors at work ranged from 0.25 to 0.64 indicating adequate concurrent validity. Employees with depression, insomnia and burnout symptoms had higher (p < 0.001) CFWQ scores than participants without these symptoms. Depression and burnout symptom severity as well as accumulation of mood, sleep, and psychosocial stressors were associated with higher CFWQ scores (p < 0.001 in all). The CFWQ appears psychometrically sound measure for the assessment of SCC in occupational population.
Published: 2023

2. Fatigue and health-related quality of life depend on the disability status and clinical course in RRMS

Author: Ahvenjärvi, H. (Henrik), Niiranen, M. (Marja), Simula, S. (Sakari), Hämäläinen, P. (Päivi), Surcel, H.-M. (Heljä-Marja), Remes, A. M. (Anne M.), Ryytty, M. (Mervi), Krüger, J. (Johanna), Ahvenjärvi, H. (Henrik), Niiranen, M. (Marja), Simula, S. (Sakari), Hämäläinen, P. (Päivi), Surcel, H.-M. (Heljä-Marja), Remes, A. M. (Anne M.), Ryytty, M. (Mervi), and Krüger, J. (Johanna)
Abstract: Background: Fatigue is a prominent and disabling symptom of multiple sclerosis (MS), impairing quality of life. The disease course of relapsing remitting MS (RRMS) is individual. Objectives: We aimed to study the effects of demographic and clinical characteristics, as well as lifestyle risk factors on experienced fatigue and health-related quality of life (HRQoL) among RRMS patients, comparing benign and severe disease types. Methods: Altogether 198 Finnish RRMS patients were recruited for this real-life cross-sectional study. Self-reported questionnaires were used to evaluate fatigue and HRQoL by using Fatigue Scale for Motor and Cognitive Functions and 15D health-related quality of life questionnaires. Patients were categorized into subgroups based on the current disability status measured by the Expanded Disability Status Scale (EDSS) cut-off value of 4.5, and by retrospective clinical course divided into benign and aggressive RRMS. Results: All in all, 73% of the RRMS patients suffered from fatigue. Lower HRQoL had a strong correlation with more prominent fatigue (r = -0.719). Higher EDSS was associated with more prominent fatigue and lower HRQoL in the whole RRMS cohort. Older age at the disease onset was associated with more prominent fatigue and decreased HRQoL in the groups of aggressive RRMS and EDSS > 4.5. In the groups of EDSS ≤ 4.5 and benign RRMS, a higher number of used disease-modifying treatments (DMTs) was associated with more pronounced fatigue and reduced HRQoL. In addition, higher BMI was associated with lower HRQoL in patients with benign RRMS. Side effects (45 %) and lack of efficacy (26 %) were the most common reasons for discontinuing a DMT. Cessation due to side effects was the only reason that was significantly associated with more prominent fatigue and lower HRQoL. Use of nicotine products, gender, or disease duration were not associated with fatigue or HRQoL. Conclusions: Individuals with severe RRMS and higher EDSS scores are
Published: 2023

3. Correlation of fatigue with disability and accelerometer-measured daily physical activity in patients with relapsing-remitting MS

Author: Luostarinen, M. (Marko), Remes, A. M. (Anne M), Urpilainen, P. (Pirjo), Takala, S. (Saara), Venojärvi, M. (Mika), Luostarinen, M. (Marko), Remes, A. M. (Anne M), Urpilainen, P. (Pirjo), Takala, S. (Saara), and Venojärvi, M. (Mika)
Abstract: Background: Fatigue is one of the most common symptoms in patients with multiple sclerosis (MS). Furthermore, measuring its effects on patients in daily life is challenging. This study aimed to discover the association between relapsing-remitting MS (RRMS) patients’ disability, fatigue, and accelerometer-measured physical activity. Methods: A total of 41 patients with RRMS with an Expanded Disability Status Scale (EDSS) level of 0–5.5 and 20 healthy controls completed the Modified Fatigue Impact Scale (MFIS) and the Fatigue Severity Scale (FSS) questionnaires. The EDSS was evaluated for all patients with RRMS, and all participants performed the MS Functional Composite (MSFC) test and six-min walk test and wore an accelerometer for seven days. Results: Patients with an EDSS level of 0–2.5 were found to have higher fatigue levels (p < 0.001) than healthy controls but lower levels than patients with an EDSS level of 3–5.5 (p < 0.001). A significant correlation was found to exist between fatigue and disability level measured by the EDSS (EDSS/FSS, r=0.750/p=0.001; EDSS/MFIS, r=0.661/p=0.001) and with the MSFC test in the patient group (MSFC/FSS, r = −0.350 p=0.025; MSFC/MFIS, r = −0.423/p=0.007). Total daily activity correlated with fatigue as measured by the FSS (MVPS/FSS r = −0.357/p=0.028, step count/FSS r = −0.463/p=0.003), but no correlation was found between the EDSS or the MSFC. Conclusion: A lower disability rate, better physical condition, and higher daily-living activity were found to predict lower fatigue levels.
Published: 2023

4. Psychopharmacological medication use in frontotemporal dementia at the time of diagnosis:comparison with Alzheimer’s disease

Author: Katisko, K. (Kasper), Krüger, J. (Johanna), Soppela, H. (Helmi), Hartikainen, P. (Päivi), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), Solje, E. (Eino), Katisko, K. (Kasper), Krüger, J. (Johanna), Soppela, H. (Helmi), Hartikainen, P. (Päivi), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), and Solje, E. (Eino)
Abstract: Background: Due to the significant presence of neuropsychiatric symptoms in patients with frontotemporal dementia (FTD) spectrum disorders, psychiatric misdiagnoses, diagnostic delay, and use of psychiatric treatments are common prior to the FTD diagnosis. Furthermore, treatment of diagnosed FTD patients mainly relies on off-label psychopharmacological approaches. Currently, limited real-world data are available regarding the actual use of psychopharmacological medications in FTD. Objective: To evaluate psychopharmacological medication use at the time of FTD diagnosis. Methods: Psychopharmacological medication use was evaluated in a Finnish FTD cohort containing 222 FTD patients, including the major clinical disease phenotypes (behavioral, language, and motor variants) and genetic patients carrying the C9orf72 repeat expansion. A cohort of 214 Alzheimer’s disease (AD) patients was used as a neurodegenerative disease reference group. Results: Active use of psychopharmacological medications at the time of diagnosis was significantly more common in FTD compared to AD, especially in the case of antidepressants (26.1% versus 15.0%, OR = 2.01, p = 0.008), antipsychotics (23.9% versus 9.3%, OR = 3.15, p < 0.001), and mood-stabilizers (6.3% versus 1.9%, OR = 2.93, p = 0.085; not statistically significant), whereas the use of cholinesterase inhibitors or memantine was nearly nonexistent in FTD patients. Female gender and behavioral variant of FTD phenotype alongside with depressive and psychotic symptoms were the most prominent factors associating with the use of these medications among the FTD spectrum patients. Conclusions: Use of off-label psychopharmacological medication and polypharmacy is substantially common at the time of FTD diagnosis. This likely reflects the challenges in using symptom-driven treatment approaches, especially prior to the eventual diagnosis.
Published: 2023

5. Traumatic brain injury associates with an earlier onset in sporadic frontotemporal dementia

Author: Soppela, H. (Helmi), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Koivisto, A. (Anne), Haapasalo, A. (Annakaisa), Borroni, B. (Barbara), Remes, A. M. (Anne M), Katisko, K. (Kasper), Solje, E. (Eino), Soppela, H. (Helmi), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Koivisto, A. (Anne), Haapasalo, A. (Annakaisa), Borroni, B. (Barbara), Remes, A. M. (Anne M), Katisko, K. (Kasper), and Solje, E. (Eino)
Abstract: Background: Currently, there are few studies considering possible modifiable risk factors of frontotemporal dementia (FTD). Objectives: In this retrospective case-control study, we evaluated whether a history of traumatic brain injury (TBI) associates with a diagnosis of FTD or modulates the clinical phenotype or onset age in FTD patients. Methods: We compared the prevalence of prior TBI between individuals with FTD (N = 218) and age and sex-matched AD patients (N = 214) or healthy controls (HC; N = 100). Based on the patient records, an individual was categorized to the TBI+ group if they were reported to have suffered from TBI during lifetime. The possible associations of TBI with age of onset and disease duration were also evaluated in the whole FTD patient group or separately in the sporadic and genetic FTD groups. Results: The prevalence of previous TBI was the highest in the FTD group (19.3%) when compared to the AD group (13.1%, p = 0.050) or HC group (12%, p = 0.108, not significant). Preceding TBI was more often associated with the sporadic FTD cases than the C9orf72 repeat expansion-carrying FTD cases (p = 0.003). Furthermore, comparison of the TBI+ and TBI- FTD groups indicated that previous TBI was associated with an earlier onset age in the FTD patients (B = 3.066, p = 0.010). Conclusions: A preceding TBI associates especially with sporadic FTD and with earlier onset of symptoms. The results of this study suggest that TBI may be a triggering factor for the neurodegenerative processes in FTD. However, understanding the precise underlying mechanisms still needs further studies.
Published: 2023

6. Cognitive impairment is not uncommon in patients with biallelic RFC1 AAGGG repeat expansion, but the expansion is rare in patients with cognitive disease

Author: Korpioja, A. (Anita), Krüger, J. (Johanna), Hurme-Niiranen, A. (Anri), Solje, E. (Eino), Katisko, K. (Kasper), Lipponen, J. (Joonas), Lehtilahti, M. (Maria), Remes, A. M. (Anne M.), Majamaa, K. (Kari), Kytövuori, L. (Laura), Korpioja, A. (Anita), Krüger, J. (Johanna), Hurme-Niiranen, A. (Anri), Solje, E. (Eino), Katisko, K. (Kasper), Lipponen, J. (Joonas), Lehtilahti, M. (Maria), Remes, A. M. (Anne M.), Majamaa, K. (Kari), and Kytövuori, L. (Laura)
Abstract: Introduction: The biallelic repeat expansion (AAGGG)exp in RFC1 causes cerebellar ataxia, neuropathy, and vestibular areflexia syndrome (CANVAS). Recently, cognitive impairment has been reported in patients with CANVAS and a broader neurodegenerative process associated with RFC1 has been suggested. Furthermore, rare cases of multiple system atrophy, Parkinson’s disease, amyotrophic lateral sclerosis or CANVAS with features of dementia with Lewy bodies have been found. Objective: We hypothesized that the biallelic (AAGGG)exp is associated with neurodegeneration manifested as cognitive symptoms and that atypical RFC1 disease may be found among patients with cognitive disorder. Methods: Clinical data on nine patients with biallelic (AAGGG)exp were reviewed and 564 patients with Alzheimer’s disease or frontotemporal dementia (FTD) were investigated for biallelic RFC1 (AAGGG)exp. Results: Five patients with biallelic (AAGGG)exp were found with a cognitive impairment and in four of them the phenotype resembled FTD. However, biallelic (AAGGG)exp was not detected among patients with Alzheimer’s disease or FTD. Conclusions: Cognitive impairment is a feature in patients with the biallelic (AAGGG)exp, but the pathogenic expansion seems to be rare in patients with dementia. Studies on patients with diverse phenotypes would be useful to further explore the involvement of RFC1 in neuronal degeneration and to identify atypical phenotypes, which should be taken into account in clinical practice.
Published: 2022

7. Modifiable potential risk factors in familial and sporadic frontotemporal dementia

Author: Soppela, H. (Helmi), Katisko, K. (Kasper), Gadola, Y. (Yasmine), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Alberici, A. (Antonella), Benussi, A. (Alberto), Koivisto, A. (Anne), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), Borroni, B. (Barbara), Solje, E. (Eino), Soppela, H. (Helmi), Katisko, K. (Kasper), Gadola, Y. (Yasmine), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Alberici, A. (Antonella), Benussi, A. (Alberto), Koivisto, A. (Anne), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), Borroni, B. (Barbara), and Solje, E. (Eino)
Abstract: Objective: Only a few studies have evaluated modifiable risk factors for frontotemporal dementia (FTD). Here, we evaluated several modifiable factors and their association with disease phenotype, genotype, and prognosis in a large study population including Finnish and Italian patients with FTD and control groups. Methods: In this case–control study, we compared the presence of several cardiovascular and other lifestyle-related diseases and education between Finnish and Italian patients with familial (n = 376) and sporadic (n = 654) FTD, between different phenotypes of FTD, and between a subgroup of Finnish FTD patients (n = 221) and matched Finnish patients with Alzheimer’s disease (AD) (n = 214) and cognitively healthy controls (HC) (n = 100). Results: Patients with sporadic FTD were less educated (p = 0.042, B = -0.560, 95% CI −1.101 to −0.019) and had more heart diseases (p < 0.001, OR = 2.265, 95% CI 1.502–3.417) compared to patients with familial FTD. Finnish FTD patients were less educated (p = 0.032, B = 0.755, 95% CI 0.064–1.466) compared with AD patients. The Finnish FTD group showed lower prevalence of hypertension than the HC group (p = 0.003, OR = 2.162, 95% CI 1.304–3.583) and lower prevalence of hypercholesterolemia than in the HC group (p < 0.001, OR = 2.648, 95%CI 1.548–4.531) or in the AD group (p < 0.001, OR = 1.995, 95% CI 1.333–2.986). Within the FTD group, clinical phenotypes also differed regarding education and lifestyle-related factors. Interpretation: Our study suggests distinct profiles of several modifiable factors in the FTD group depending on the phenotype and familial inheritance history and that especially sporadic FTD may be associated with modifiable risk factors.
Published: 2022

8. Serum total TDP-43 levels are decreased in frontotemporal dementia patients with C9orf72 repeat expansion or concomitant motoneuron disease phenotype

Author: Katisko, K. (Kasper), Huber, N. (Nadine), Kokkola, T. (Tarja), Hartikainen, P. (Päivi), Krüger, J. (Johanna), Heikkinen, A.-L. (Anna-Leena), Paananen, V. (Veera), Leinonen, V. (Ville), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Herukka, S.-K. (Sanna-Kaisa), Cantoni, V. (Valentina), Gadola, Y. (Yasmine), Archetti, S. (Silvana), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), Borroni, B. (Barbara), Solje, E. (Eino), Katisko, K. (Kasper), Huber, N. (Nadine), Kokkola, T. (Tarja), Hartikainen, P. (Päivi), Krüger, J. (Johanna), Heikkinen, A.-L. (Anna-Leena), Paananen, V. (Veera), Leinonen, V. (Ville), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Herukka, S.-K. (Sanna-Kaisa), Cantoni, V. (Valentina), Gadola, Y. (Yasmine), Archetti, S. (Silvana), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), Borroni, B. (Barbara), and Solje, E. (Eino)
Abstract: Background: Frontotemporal dementia (FTD) covers a spectrum of neurodegenerative disorders with various clinical and neuropathological subtypes. The two major pathological proteins accumulating in the brains of FTD patients, depending on their genetic background, are TDP-43 and tau. We aimed to evaluate whether total TDP-43 levels measured from the serum associate with the genotype or clinical phenotype of the FTD patients and whether serum TDP-43 provides prognostic or diagnostic value in the FTD spectrum disorders. Methods: The study cohort included 254 participants with a clinical diagnosis of FTD (including all major genotypes and clinical phenotypes) and 105 cognitively healthy controls. Serum total TDP-43 levels measured with a single-molecule array (Simoa) were compared within the FTD group according to the genotype, clinical phenotype, and predicted neuropathological subtype of the patients. We also evaluated the associations between the TDP-43 levels and disease severity or survival in FTD. Results: Total TDP-43 levels in the serum were significantly lower in the FTD group as compared to the healthy control group (275.3 pg/mL vs. 361.8 pg/mL, B = 0.181, 95%CI = 0.014–0.348, p = 0.034). The lowest TDP-43 levels were observed in the subgroup of FTD patients harboring predicted TDP-43 brain pathology (FTD-TDP, 241.4 pg/mL). The low levels in the FTD-TDP group were especially driven by C9orf72 repeat expansion carriers (169.2 pg/mL) and FTD patients with concomitant motoneuron disease (FTD-MND, 113.3 pg/mL), whereas GRN mutation carriers did not show decreased TDP-43 levels (328.6 pg/mL). Serum TDP-43 levels showed no correlation with disease severity nor progression in FTD. Conclusions: Our results indicate that the total levels of TDP-43 in the serum are decreased especially in FTD patients with the C9orf72 repeat expansion or FTD-MND phenotype, both subtypes strongly associated with TDP-43 type B brain pathology. Serum-based measurement of TDP-43 co
Published: 2022

9. Grey matter atrophy in patients with benign multiple sclerosis

Author: Niiranen, M. (Marja), Koikkalainen, J. (Juha), Lötjönen, J. (Jyrki), Selander, T. (Tuomas), Cajanus, A. (Antti), Hartikainen, P. (Päivi), Simula, S. (Sakari), Vanninen, R. (Ritva), Remes, A. M. (Anne M.), Niiranen, M. (Marja), Koikkalainen, J. (Juha), Lötjönen, J. (Jyrki), Selander, T. (Tuomas), Cajanus, A. (Antti), Hartikainen, P. (Päivi), Simula, S. (Sakari), Vanninen, R. (Ritva), and Remes, A. M. (Anne M.)
Abstract: Background: Brain atrophy appears during the progression of multiple sclerosis (MS) and is associated with the disability caused by the disease. Methods: We investigated global and regional grey matter (GM) and white matter (WM) volumes, WM lesion load, and corpus callosum index (CCI), in benign relapsing-remitting MS (BRRMS, n = 35) with and without any treatment and compared those to aggressive relapsing-remitting MS (ARRMS, n = 46). Structures were analyzed by using an automated MRI quantification tool (cNeuro®). Results: The total brain and cerebral WM volumes were larger in BRRMS than in ARRMS (p = .014, p = .017 respectively). In BRRMS, total brain volumes, regional GM volumes, and CCI were found similar whether or not disease-modifying treatment (DMT) was used. The total (p = .033), as well as subcortical (p = .046) and deep WM (p = .041) lesion load volumes were larger in BRRMS patients without DMT. Cortical GM volumes did not differ between BRRMS and ARRMS, but the volumes of total brain tissue (p = .014) and thalami (p = .003) were larger in patients with BRRMS compared to ARRMS. A positive correlation was found between CCI and whole-brain volume in both BRRMS (r = .73, p < .001) and ARRMS (r = .80, p < .01). Conclusions: Thalamic volume is the most prominent measure to differentiate BRRMS and ARRMS. Validation of automated quantification of CCI provides an additional applicable MRI biomarker to detect brain atrophy in MS.
Published: 2022

10. Deficient neurotransmitter systems and synaptic function in frontotemporal lobar degeneration:insights into disease mechanisms and current therapeutic approaches

Author: Huber, N. (Nadine), Korhonen, S. (Sonja), Hoffmann, D. (Dorit), Leskelä, S. (Stina), Rostalski, H. (Hannah), Remes, A. M. (Anne M.), Honkakoski, P. (Paavo), Solje, E. (Eino), Haapasalo, A. (Annakaisa), Huber, N. (Nadine), Korhonen, S. (Sonja), Hoffmann, D. (Dorit), Leskelä, S. (Stina), Rostalski, H. (Hannah), Remes, A. M. (Anne M.), Honkakoski, P. (Paavo), Solje, E. (Eino), and Haapasalo, A. (Annakaisa)
Abstract: Frontotemporal lobar degeneration (FTLD) comprises a heterogenous group of fatal neurodegenerative diseases and, to date, no validated diagnostic or prognostic biomarkers or effective disease-modifying therapies exist for the different clinical or genetic subtypes of FTLD. Current treatment strategies rely on the off-label use of medications for symptomatic treatment. Changes in several neurotransmitter systems including the glutamatergic, GABAergic, dopaminergic, and serotonergic systems have been reported in FTLD spectrum disease patients. Many FTLD-related clinical and neuropsychiatric symptoms such as aggressive and compulsive behaviour, agitation, as well as altered eating habits and hyperorality can be explained by disturbances in these neurotransmitter systems, suggesting that their targeting might possibly offer new therapeutic options for treating patients with FTLD. This review summarizes the present knowledge on neurotransmitter system deficits and synaptic dysfunction in model systems and patients harbouring the most common genetic causes of FTLD, the hexanucleotide repeat expansion in C9orf72 and mutations in the granulin (GRN) and microtubule-associated protein tau (MAPT) genes. We also describe the current pharmacological treatment options for FLTD that target different neurotransmitter systems.
Published: 2022

11. NDUFA1 p.Gly32Arg variant in early-onset dementia

Author: Huttula, S. (Samuli), Väyrynen, H. (Henri), Helisalmi, S. (Seppo), Kytövuori, L. (Laura), Luukkainen, L. (Laura), Hiltunen, M. (Mikko), Remes, A. M. (Anne M.), Krüger, J. (Johanna), Huttula, S. (Samuli), Väyrynen, H. (Henri), Helisalmi, S. (Seppo), Kytövuori, L. (Laura), Luukkainen, L. (Laura), Hiltunen, M. (Mikko), Remes, A. M. (Anne M.), and Krüger, J. (Johanna)
Abstract: Early-onset dementia (EOD) is highly heritable. However, in many EOD cases the genetic etiology remains unknown. Mitochondrial dysfunction is associated with neurodegeneration and the complex I (CI) deficiency is the most common enzyme deficiency in diseases related to oxidative phosphorylation. The X-chromosomal NDUFA1 gene is essential for the activity of CI. Mutations in NDUFA1 are associated with mitochondrial diseases especially with Leigh syndrome. CI deficiency is also associated with neurodegenerative diseases, such as Alzheimer’s disease (AD). The aim of this study was to evaluate the role of NDUFA1 variants in EOD patients. Next-generation sequencing panel was used to screen NDUFA1 variants in a cohort of 37 EOD patients with a family history of dementia or an atypical or rapidly progressive course of disease. We identified a hemizygous p.Gly32Arg variant in two brothers with AD. Subsequent screening of the variant in a larger cohort of EOD patients (n = 279) revealed three additional variant carriers (one male and two heterozygote females), suggesting that NDUFA1 variant p.Gly32Arg may play a role in neurodegenerative dementia.
Published: 2022

12. Brainstem atrophy is linked to extrapyramidal symptoms in frontotemporal dementia

Author: Heikkinen, S. (Sami), Cajanus, A. (Antti), Katisko, K. (Kasper), Hartikainen, P. (Päivi), Vanninen, R. (Ritva), Haapasalo, A. (Annakaisa), Krüger, J. (Johanna), Remes, A. M. (Anne M.), Solje, E. (Eino), Heikkinen, S. (Sami), Cajanus, A. (Antti), Katisko, K. (Kasper), Hartikainen, P. (Päivi), Vanninen, R. (Ritva), Haapasalo, A. (Annakaisa), Krüger, J. (Johanna), Remes, A. M. (Anne M.), and Solje, E. (Eino)
Abstract: Extrapyramidal (EP) symptoms are a known feature in a subpopulation of patients with behavioral variant frontotemporal dementia (bvFTD). Concomitant EP symptoms with FTD-like neuropsychiatric symptoms are also core features in progressive supranuclear palsy (PSP) and corticobasal degeneration (CBD). This complicates the early diagnosis of these disorders. Our retrospective register study aimed to discover imaging (MRI and FDG-PET) biomarkers to differentiate PSP, CBD, and bvFTD patients with extrapyramidal symptoms (EP +) from bvFTD patients without EP symptoms (EP-). The records of 2751 patients were screened for the diagnoses and presence of EP symptoms. A total of 222 patients were submitted to imaging analysis and applicable imaging data were recovered from 139 patients. Neuroimaging data were analyzed using Freesurfer software. In the whole cohort, EP + patients showed lower volumes of gray matter compared to EP- patients in the putamen (p = 0.002), bilateral globus pallidum (p = 0.002, p = 0.042), ventral diencephalon (p = 0.002) and brain stem (p < 0.001). In the bvFTD subgroup, there was volumetric difference between EP + and EP− patients in the brain stem. FDG-PET scans in the bvFTD patient subgroup showed that EP + patients had comparative hypometabolism of the superior cerebellar peduncle (SCP) and the frontal lobes. We discovered that EP symptoms are linked to brainstem atrophy in bvFTD patients and the whole cohort. Also, evident hypometabolism in the SCP of bvFTD EP + patients was detected as compared to bvFTD EP− patients. This could indicate that the EP symptoms in these diseases have a more caudal origin in the brainstem than in Parkinson’s disease.
Published: 2022

13. C9orf72 hexanucleotide repeat expansion leads to altered neuronal and dendritic spine morphology and synaptic dysfunction

Author: Huber, N. (Nadine), Hoffmann, D. (Dorit), Giniatullina, R. (Raisa), Rostalski, H. (Hannah), Leskelä, S. (Stina), Takalo, M. (Mari), Natunen, T. (Teemu), Solje, E. (Eino), Remes, A. M. (Anne M.), Giniatullin, R. (Rashid), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Huber, N. (Nadine), Hoffmann, D. (Dorit), Giniatullina, R. (Raisa), Rostalski, H. (Hannah), Leskelä, S. (Stina), Takalo, M. (Mari), Natunen, T. (Teemu), Solje, E. (Eino), Remes, A. M. (Anne M.), Giniatullin, R. (Rashid), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: Frontotemporal lobar degeneration (FTLD) comprises a heterogenous group of progressive neurodegenerative syndromes. To date, no validated biomarkers or effective disease-modifying therapies exist for the different clinical or genetic subtypes of FTLD. The most common genetic cause underlying FTLD and amyotrophic lateral sclerosis (ALS) is a hexanucleotide repeat expansion in the C9orf72 gene (C9-HRE). FTLD is accompanied by changes in several neurotransmitter systems, including the glutamatergic, GABAergic, dopaminergic, and serotonergic systems and many clinical symptoms can be explained by disturbances in these systems. Here, we aimed to elucidate the effects of the C9-HRE on synaptic function, molecular composition of synapses, and dendritic spine morphology. We overexpressed the pathological C9-HRE in cultured E18 mouse primary hippocampal neurons and characterized the pathological, morphological, and functional changes by biochemical methods, confocal microscopy, and live cell calcium imaging. The C9-HRE-expressing neurons were confirmed to display the pathological RNA foci and DPR proteins. C9-HRE expression led to significant changes in dendritic spine morphologies, as indicated by decreased number of mushroom-type spines and increased number of stubby and thin spines, as well as diminished neuronal branching. These morphological changes were accompanied by concomitantly enhanced susceptibility of the neurons to glutamate-induced excitotoxicity as well as augmented and prolonged responses to excitatory stimuli by glutamate and depolarizing potassium chloride as compared to control neurons. Mechanistically, the hyperexcitation phenotype in the C9-HRE-expressing neurons was found to be underlain by increased activity of extrasynaptic GluN2B-containing N-methyl-d-aspartate (NMDA) receptors. Our results are in accordance with the idea suggesting that C9-HRE is associated with enhanced excitotoxicity and synaptic dysfunction. Thus, therapeutic interventio
Published: 2022

14. FRONTotemporal dementia Incidence European Research Study—FRONTIERS:rationale and design

Author: Borroni, B. (Barbara), Graff, C. (Caroline), Hardiman, O. (Orla), Ludolph, A. C. (Albert C.), Moreno, F. (Fermin), Otto, M. (Markus), Piccininni, M. (Marco), Remes, A. M. (Anne M), Rowe, J. B. (James B), Seelaar, H. (Harro), Stefanova, E. (Elka), Traykov, L. (Latchezar), Logroscino, G. (Giancarlo), and F. (FRONTIERS)
Subjects: frontotemporal lobar degeneration, incidence, rare diseases, epidemiology, registry, frontotemporal dementia
Abstract: Introduction: The incidence of Frontotemporal Lobar Degeneration (FTLD)–related disorders and their characteristics are not well known. The “FRONTotemporal dementia Incidence European Research Study” (FRONTIERS) is designed to fill this gap. Methods: FRONTIERS is a European prospective, observational population study based on multinational registries. FRONTIERS comprises 11 tertiary referral centers across Europe with long-lasting experience in FTLD-related disorders and comprehensive regional referral networks, enabling incidence estimation over well-defined geographical areas. Endpoints: The primary endpoints are (1) the incidence of FTLD-related disorders across Europe; (2) geographic trends of FTLD-related disorders; (3) the distribution of FTLD phenotypes in different populations and ethnicities in Europe; (4) inheritance of FTLD-related disorders, including the frequencies of monogenic FTLD as compared to overall disease burden; and (5) implementation of data banking for clinical and biological material. Expected impacts: FRONTIERS will improve the understanding of FTLD-related disorders and their epidemiology, promoting appropriate public health service policies and treatment strategies.
Published: 2021

15. Otsa-ohimolohkorappeumat:miten tunnistan ja hoidan?

Author: Krüger, J. (Johanna), Katisko, K. (Kasper), Suhonen, N.-M. (Noora-Maria), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), and Solje, E. (Eino)
Abstract: Tiivistelmä Otsa-ohimolohkorappeumat ovat työikäisten toiseksi yleisin etenevän muistisairauden aiheuttaja. Yleisin tämän ryhmän oireyhtymistä on otsalohkodementia, jolle ovat tyypillisiä persoonallisuuden ja käyttäytymisen muutokset. Toisen ryhmän muodostavat primaariset etenevät afasiat, joihin liittyy etupäässä kielellisiä ongelmia. Otsa-ohimolohkorappeumien diagnosointi on vaativaa, sillä ensioireet voivat herättää epäilyn esimerkiksi psykiatrisesta sairaudesta eikä taudille spesifisiä biomarkkereita tai kognitiivisia seulontatestejä ole kliinisessä käytössä. Siksi laaja neuropsykologinen tutkimus on tarpeen osana diagnostiikkaa. Näköpiirissä olevien uusien biomarkkerien käyttöönotto helpottaa jatkossa varhaista diagnostiikkaa. Toistaiseksi otsa-ohimolohkorappeumiin ei ole käytettävissä taudinkulkuun vaikuttavaa hoitoa, mutta varhaisen tunnistamisen ja oikean diagnoosin merkitys korostuvat, kun kehitteillä olevat lääkkeet tulevat saataville.
Published: 2021

16. Cardiovascular brain impulses in Alzheimer’s disease

Author: Rajna, Z. (Zalán), Mattila, H. (Heli), Huotari, N. (Niko), Tuovinen, T. (Timo), Krüger, J. (Johanna), Holst, S. C. (Sebastian C.), Korhonen, V. (Vesa), Remes, A. M. (Anne M.), Seppänen, T. (Tapio), Hennig, J. (Jürgen), Nedergaard, M. (Maiken), Kiviniemi, V. (Vesa), Rajna, Z. (Zalán), Mattila, H. (Heli), Huotari, N. (Niko), Tuovinen, T. (Timo), Krüger, J. (Johanna), Holst, S. C. (Sebastian C.), Korhonen, V. (Vesa), Remes, A. M. (Anne M.), Seppänen, T. (Tapio), Hennig, J. (Jürgen), Nedergaard, M. (Maiken), and Kiviniemi, V. (Vesa)
Abstract: Accumulation of amyloid-β is a key neuropathological feature in brain of Alzheimer’s disease patients. Alterations in cerebral haemodynamics, such as arterial impulse propagation driving the (peri)vascular CSF flux, predict future Alzheimer’s disease progression. We now present a non-invasive method to quantify the three-dimensional propagation of cardiovascular impulses in human brain using ultrafast 10 Hz magnetic resonance encephalography. This technique revealed spatio-temporal abnormalities in impulse propagation in Alzheimer’s disease. The arrival latency and propagation speed both differed in patients with Alzheimer’s disease. Our mapping of arterial territories revealed Alzheimer’s disease-specific modifications, including reversed impulse propagation around the hippocampi and in parietal cortical areas. The findings imply that pervasive abnormality in (peri)vascular CSF impulse propagation compromises vascular impulse propagation and subsequently glymphatic brain clearance of amyloid-β in Alzheimer’s disease.
Published: 2021

17. State-of-the-art methods and emerging fluid biomarkers in the diagnostics of dementia:a short review and diagnostic algorithm

Author: Solje, E. (Eino), Benussi, A. (Alberto), Buratti, E. (Emanuele), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), Borroni, B. (Barbara), Solje, E. (Eino), Benussi, A. (Alberto), Buratti, E. (Emanuele), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), and Borroni, B. (Barbara)
Abstract: The most common neurodegenerative dementias include Alzheimer’s disease (AD), dementia with Lewy bodies (DLB), and frontotemporal dementia (FTD). The correct etiology-based diagnosis is pivotal for clinical management of these diseases as well as for the suitable timing and choosing the accurate disease-modifying therapies when these become available. Enzyme-linked immunosorbent assay (ELISA)-based methods, detecting altered levels of cerebrospinal fluid (CSF) Tau, phosphorylated Tau, and Aβ-42 in AD, allowed the wide use of this set of biomarkers in clinical practice. These analyses demonstrate a high diagnostic accuracy in AD but suffer from a relatively restricted usefulness due to invasiveness and lack of prognostic value. In recent years, the development of novel advanced techniques has offered new state-of-the-art opportunities in biomarker discovery. These include single molecule array technology (SIMOA), a tool for non-invasive analysis of ultra-low levels of central nervous system-derived molecules from biofluids, such as CSF or blood, and real-time quaking (RT-QuIC), developed to analyze misfolded proteins. In the present review, we describe the history of methods used in the fluid biomarker analyses of dementia, discuss specific emerging biomarkers with translational potential for clinical use, and suggest an algorithm for the use of new non-invasive blood biomarkers in clinical practice.
Published: 2021

18. A novel genetic marker for the C9orf72 repeat expansion in the Finnish population

Author: Rostalski, H. (Hannah), Korhonen, V. (Ville), Kuulasmaa, T. (Teemu), Solje, E. (Eino), Krüger, J. (Johanna), Kaivola, K. (Karri), Eide, P. K. (Per Kristian), Lambert, J.-C. (Jean-Charles), Julkunen, V. (Valtteri), Tienari, P. J. (Pentti J.), Remes, A. M. (Anne M.), Leinonen, V. (Ville), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Rostalski, H. (Hannah), Korhonen, V. (Ville), Kuulasmaa, T. (Teemu), Solje, E. (Eino), Krüger, J. (Johanna), Kaivola, K. (Karri), Eide, P. K. (Per Kristian), Lambert, J.-C. (Jean-Charles), Julkunen, V. (Valtteri), Tienari, P. J. (Pentti J.), Remes, A. M. (Anne M.), Leinonen, V. (Ville), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: Background: C9orf72 repeat expansion (C9exp) is the most common genetic cause underlying frontotemporal lobar degeneration (FTLD) and amyotrophic lateral sclerosis (ALS). However, detection of the C9exprequires elaborative methods. Objective: Identification of C9exp carriers from genotyped cohorts could be facilitated by using single nucleotide polymorphisms (SNPs) as markers for the C9exp. Methods: We elucidated the potential of the previously described Finnish risk haplotype, defined by the SNP rs3849942, to identify potential C9exp carriers among 218,792 Finns using the FinnGen database. The haplotype approach was first tested in an idiopathic normal pressure hydrocephalus (iNPH) patient cohort (European Alzheimer’s Disease DNA BioBank) containing C9exp carriers by comparing intermediate (15–30) and full-length (> 60 repeats) C9exp carriers (n = 41) to C9exp negative patients (< 15 repeats, n = 801). Results: In this analysis, rs3849942 was associated with carriership of C9exp (OR 8.44, p < 2 × 10–15), while the strongest association was found with rs139185008 (OR 39.4, p < 5 × 10–18). Unbiased analysis of rs139185008 in FinnGen showed the strongest association with FTLD (OR 4.38, 3 × 10–15) and motor neuron disease ALS (OR 5.19, 3 × 10–21). rs139185008 was the top SNP in all diseases (iNPH, FTLD, ALS), and further showed a strong association with ALS in the UK Biobank (p = 9.0 × 10–8). Conclusions: Our findings suggest that rs139185008 is a useful marker to identify potential C9exp carriers in the genotyped cohorts and biobanks originating from Finland.
Published: 2021

19. FTLD patient–derived fibroblasts show defective mitochondrial function and accumulation of p62

Author: Leskelä, S. (Stina), Hoffmann, D. (Dorit), Rostalski, H. (Hannah), Huber, N. (Nadine), Wittrahm, R. (Rebekka), Hartikainen, P. (Päivi), Korhonen, V. (Ville), Leinonen, V. (Ville), Hiltunen, M. (Mikko), Solje, E. (Eino), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), Leskelä, S. (Stina), Hoffmann, D. (Dorit), Rostalski, H. (Hannah), Huber, N. (Nadine), Wittrahm, R. (Rebekka), Hartikainen, P. (Päivi), Korhonen, V. (Ville), Leinonen, V. (Ville), Hiltunen, M. (Mikko), Solje, E. (Eino), Remes, A. M. (Anne M.), and Haapasalo, A. (Annakaisa)
Abstract: Frontotemporal lobar degeneration (FTLD) is a clinically, genetically, and neuropathologically heterogeneous group of neurodegenerative syndromes, leading to progressive cognitive dysfunction and frontal and temporal atrophy. C9orf72 hexanucleotide repeat expansion (C9-HRE) is the most common genetic cause of FTLD, but pathogenic mechanisms underlying FTLD are not fully understood. Here, we compared cellular features and functional properties, especially related to protein degradation pathways and mitochondrial function, of FTLD patient–derived skin fibroblasts from C9-HRE carriers and non-carriers and healthy donors. Fibroblasts from C9-HRE carriers were found to produce RNA foci, but no dipeptide repeat proteins, and they showed unchanged levels of C9orf72 mRNA transcripts. The main protein degradation pathways, the ubiquitin–proteasome system and autophagy, did not show alterations between the fibroblasts from C9-HRE-carrying and non-carrying FTLD patients and compared to healthy controls. An increase in the number and size of p62-positive puncta was evident in fibroblasts from both C9-HRE carriers and non-carriers. In addition, several parameters of mitochondrial function, namely, basal and maximal respiration and respiration linked to ATP production, were significantly reduced in the FTLD patient–derived fibroblasts from both C9-HRE carriers and non-carriers. Our findings suggest that FTLD patient–derived fibroblasts, regardless of whether they carry the C9-HRE expansion, show unchanged proteasomal and autophagic function, but significantly impaired mitochondrial function and increased accumulation of p62 when compared to control fibroblasts. These findings suggest the possibility of utilizing FTLD patient–derived fibroblasts as a platform for biomarker discovery and testing of drugs targeted to specific cellular functions, such as mitochondrial respiration..
Published: 2021

20. Safety of alemtuzumab in a nationwide cohort of Finnish multiple sclerosis patients

Author: Rauma, I. (Ilkka), Mustonen, T. (Tiina), Seppä, J. M. (Juha Matti), Ukkonen, M. (Maritta), Männikkö, M. (Marianne), Verkkoniemi-Ahola, A. (Auli), Kartau, M. (Marge), Saarinen, J. T. (Jukka T.), Luostarinen, L. (Liisa), Simula, S. (Sakari), Ryytty, M. (Mervi), Ahmasalo, R. (Riitta), Sipilä, J. O. (Jussi O. T.), Pieninkeroinen, I. (Ilkka), Tapiola, T. (Tero), Remes, A. M. (Anne M.), Kuusisto, H. (Hanna), Rauma, I. (Ilkka), Mustonen, T. (Tiina), Seppä, J. M. (Juha Matti), Ukkonen, M. (Maritta), Männikkö, M. (Marianne), Verkkoniemi-Ahola, A. (Auli), Kartau, M. (Marge), Saarinen, J. T. (Jukka T.), Luostarinen, L. (Liisa), Simula, S. (Sakari), Ryytty, M. (Mervi), Ahmasalo, R. (Riitta), Sipilä, J. O. (Jussi O. T.), Pieninkeroinen, I. (Ilkka), Tapiola, T. (Tero), Remes, A. M. (Anne M.), and Kuusisto, H. (Hanna)
Abstract: Background: Alemtuzumab is an effective disease-modifying therapy (DMT) for highly active multiple sclerosis (MS). However, safety concerns limit its use in clinical practice. Objectives: To evaluate the safety of alemtuzumab in a nationwide cohort of Finnish MS patients. Methods: In this retrospective case series study, we analyzed the data of all but two MS patients who had received alemtuzumab in Finland until 2019. Data were systematically collected from patient files. Results: Altogether 121 patients were identified, most of whom had received previous DMTs (82.6%). Median follow-up time after treatment initiation was 30.3 months and exceeded 24 months in 78 patients. Infusion-associated reactions (IARs) were observed in 84.3%, 57.3%, and 57.1% of patients during alemtuzumab courses 1–3, respectively. Serious adverse events (SAEs) were observed in 32.2% of patients, serious IARs in 12.4% of patients, and SAEs other than IARs in 23.1% of patients. Autoimmune adverse events were observed in 30.6% of patients. One patient died of hemophagocytic lymphohistiocytosis, and one patient died of pneumonia. A previously unreported case of thrombotic thrombocytopenic purpura was documented. Conclusions: SAEs were more frequent in the present cohort than in previous studies. Even though alemtuzumab is a highly effective therapy for MS, vigorous monitoring with a long enough follow-up time is advised.
Published: 2021

21. Expression of C9orf72 hexanucleotide repeat expansion leads to formation of RNA foci and dipeptide repeat proteins but does not influence autophagy or proteasomal function in neuronal cells

Author: Leskelä, S. (Stina), Huber, N. (Nadine), Hoffmann, D. (Dorit), Rostalski, H. (Hannah), Remes, A. M. (Anne M.), Takalo, M. (Mari), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Leskelä, S. (Stina), Huber, N. (Nadine), Hoffmann, D. (Dorit), Rostalski, H. (Hannah), Remes, A. M. (Anne M.), Takalo, M. (Mari), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: C9orf72 hexanucleotide repeat expansion (HRE) is the major genetic cause underpinning frontotemporal lobar degeneration (FLTD) and amyotrophic lateral sclerosis (ALS). C9orf72 HRE-associated pathogenesis involves both loss-of-function, through reduced C9orf72 levels, and gain-of-function mechanisms, including formation of RNA foci and generation of dipeptide repeat (DPR) proteins. In addition, dysfunctional protein degradation pathways, i.e. autophagy and ubiquitin-proteasome system (UPS), are suggested. Our aim was to study the gain-of-function mechanisms in the context of the function of protein degradation pathways as well as the regulation of the DPR proteins through these pathways. To this end, we expressed the pathological HRE in neuronal N2a cells and mouse primary cortical neurons. Protein degradation pathways were modulated to induce or block autophagy or to inhibit UPS. In addition, proteasomal activity was assessed. The C9orf72 HRE-expressing N2a cells and neurons were confirmed to produce RNA foci and DPR proteins, predominantly the Poly-GP proteins. However, the presence of these pathological hallmarks did not result in alterations in autophagy or proteasomal activity in either of the studied cell types. In N2a cells, Poly-GP proteins appeared in soluble forms and Lactacystin-mediated UPS inhibition increased their levels, indicating proteasomal regulation. Similar effects were not observed in cortical neurons, where the Poly-GP proteins formed also higher molecular weight forms. These results suggest a cell type-specific morphology and regulation of the DPR proteins. Further studies in other model systems may shed additional light onto the effects of the C9orf72 HRE on cellular protein degradation pathways and the regulation of the DPR protein levels.
Published: 2021

22. Cerebrospinal fluid and MRI biomarkers in neurodegenerative diseases:a retrospective memory clinic-based study

Author: Kaipainen, A. (Aku), Jääskeläinen, O. (Olli), Liu, Y. (Yawu), Haapalinna, F. (Fanni), Nykänen, N. (Niko), Vanninen, R. (Ritva), Koivisto, A. M. (Anne M.), Julkunen, V. (Valtteri), Remes, A. M. (Anne M.), and Herukka, S.-K. (Sanna-Kaisa)
Subjects: diagnostic imaging, amyloid, magnetic resonance imaging, neurodegenerative diseases, tau proteins, Alzheimer’s disease, cerebrospinal fluid
Abstract: Background: Cerebrospinal fluid (CSF) and magnetic resonance imaging (MRI) biomarkers of neurodegenerative diseases are relatively sensitive and specific in highly curated research cohorts, but proper validation for clinical use is mostly missing. Objective: We studied these biomarkers in a novel memory clinic cohort with a variety of different neurodegenerative diseases. Methods: This study consisted of 191 patients with subjective or objective cognitive impairment who underwent neurological, CSF biomarker (Aβ42, p-tau, and tau) and T1-weighted MRI examinations at Kuopio University Hospital. We assessed CSF and imaging biomarkers, including structural MRI focused on volumetric and cortical thickness analyses, across groups stratified based on different clinical diagnoses, including Alzheimer’s disease (AD), frontotemporal dementia, dementia with Lewy bodies, Parkinson’s disease, vascular dementia, and mild cognitive impairment (MCI), and subjects with no evidence of neurodegenerative disease underlying the cognitive symptoms. Imaging biomarkers were also studied by profiling subjects according to the novel amyloid, tau, and, neurodegeneration (AT(N)) classification. Results: Numerous imaging variables differed by clinical diagnosis, including hippocampal, amygdalar and inferior lateral ventricular volumes and entorhinal, lingual, inferior parietal and isthmus cingulate cortical thicknesses, at a false discovery rate (FDR)-corrected threshold for significance (analysis of covariance; p
Published: 2020

23. C9orf72 repeat expansion does not affect the phenotype in primary progressive aphasia

Author: Haapanen, M. (Marjut), Katisko, K. (Kasper), Hänninen, T. (Tuomo), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M), and Solje, E. (Eino)
Subjects: frontotemporal lobar degeneration, C9orf72, primary progressive aphasia, respiratory system, frontotemporal dementia
Abstract: Primary progressive aphasia (PPA) forms the spectrum of language variants of frontotemporal lobar degeneration (FTLD), including three subtypes each consisting of distinctive speech and language features. Repeat expansion in C9orf72 gene is the most common genetic cause of FTLD. However, thus far only little is known about the effects of the C9orf72 repeat expansion on the phenotype of PPA. This retrospective study aimed at determining the differences between the PPA phenotypes of the C9orf72 expansion carriers and non-carriers. Our results demonstrated no significant differences between these groups, indicating that the C9orf72 repeat expansion does not substantially affect the phenotype of PPA.
Published: 2020

24. Selection of memory clinic patients for CSF biomarker assessment can be restricted to a quarter of cases by using computerized decision support, without compromising diagnostic accuracy

Author: Rhodius-Meester, H. F. (Hanneke F. M.), van Maurik, I. S. (Ingrid S.), Koikkalainen, J. (Juha), Tolonen, A. (Antti), Frederiksen, K. S. (Kristian S.), Hasselbalch, S. G. (Steen G.), Soininen, H. (Hilkka), Herukka, S.-K. (Sanna-Kaisa), Remes, A. M. (Anne M.), Teunissen, C. E. (Charlotte E.), Barkhof, F. (Frederik), Pijnenburg, Y. A. (Yolande A. L.), Scheltens, P. (Philip), Lötjönen, J. (Jyrki), and van der Flier, W. M. (Wiesje M.)
Abstract: Introduction: An accurate and timely diagnosis for Alzheimer’s disease (AD) is important, both for care and research. The current diagnostic criteria allow the use of CSF biomarkers to provide pathophysiological support for the diagnosis of AD. How these criteria should be operationalized by clinicians is unclear. Tools that guide in selecting patients in which CSF biomarkers have clinical utility are needed. We evaluated computerized decision support to select patients for CSF biomarker determination. Methods: We included 535 subjects (139 controls, 286 Alzheimer’s disease dementia, 82 frontotemporal dementia and 28 vascular dementia) from three clinical cohorts. Positive (AD like) and negative (normal) CSF biomarker profiles were simulated to estimate whether knowledge of CSF biomarkers would impact (confidence in) diagnosis. We applied these simulated CSF values and combined them with demographic, neuropsychology and MRI data to initiate CSF testing (computerized decision support approach). We compared proportion of CSF measurements and patients diagnosed with sufficient confidence (probability of correct class ≥0.80) based on an algorithm with scenarios without CSF (only neuropsychology, MRI and APOE), CSF according to the appropriate use criteria (AUC) and CSF for all patients. Results: The computerized decision support approach recommended CSF testing in 140 (26%) patients, which yielded a diagnosis with sufficient confidence in 379 (71%) of all patients. This approach was more efficient than CSF in none (0% CSF, 308 (58%) diagnosed), CSF selected based on AUC (295 (55%) CSF, 350 (65%) diagnosed) or CSF in all (100% CSF, 348 (65%) diagnosed). Conclusions: We used a computerized decision support with simulated CSF results in controls and patients with different types of dementia. This approach can support clinicians in making a balanced decision in ordering additional biomarker testing. Computer-supported prediction restricts CSF testing to only 26% of cases, without compromising diagnostic accuracy.
Published: 2020

25. Serum neurofilament light chain in FTLD:association with C9orf72, clinical phenotype, and prognosis

Author: Cajanus, A. (Antti), Katisko, K. (Kasper), Kontkanen, A. (Aleksi), Jääskeläinen, O. (Olli), Hartikainen, P. (Päivi), Haapasalo, A. (Annakaisa), Herukka, S. (Sanna‐Kaisa), Vanninen, R. (Ritva), Solje, E. (Eino), Hall, A. (Anette), and Remes, A. M. (Anne M.)
Subjects: disease, hexanucleotide repeat expansion, biomarker, severity, system, mutations, protein, frontotemporal dementia
Abstract: Objective: The aim of the present study was to compare the levels of serum neurofilament light chain (sNfL) in frontotemporal lobar degeneration (FTLD) patients of different clinical subtypes (bvFTD, PPA, and FTLD‐MND) and with or without the C9orf72 repeat expansion, and to correlate sNfL levels to disease progression, assessed by the brain atrophy rate and survival time. Methods: The sNfL levels were determined from 78 FTLD patients (C9orf72 repeat expansion carriers [n = 26] and non‐carriers [n = 52]) with Single Molecule Array (SIMOA). The progression of brain atrophy was evaluated using repeated T1‐weighted MRI scans and the survival time from medical records. Results: In the total FTLD cohort, sNfL levels were significantly higher in C9orf72 repeat expansion carriers compared to non‐carriers. Considering clinical phenotypes, sNfL levels were higher in the C9orf72 repeat expansion carriers than in the non‐carriers in bvFTD and PPA groups. Furthermore, sNfL levels were the highest in the FTLD‐MND group (median 105 pg/mL) and the lowest in the bvFTD group (median 27 pg/mL). Higher sNfL levels significantly correlated with frontal cortical atrophy rate and subcortical grey matter atrophy rate. The higher sNfL levels also associated with shorter survival time. Interpretation: Our results indicate that the C9orf72 repeat expansion carriers show elevated sNFL levels compared to non‐carriers and that the levels differ among different clinical phenotypes of FTLD. Higher sNfL levels correlated with a shorter survival time and cortical and subcortical atrophy rates. Thus, sNfL could prove as a potential prognostic biomarker in FTLD.
Published: 2020

26. Peripheral inflammatory markers and clinical correlations in patients with frontotemporal lobar degeneration with and without the C9orf72 repeat expansion

Author: Katisko, K. (Kasper), Solje, E. (Eino), Korhonen, P. (Paula), Jääskeläinen, O. (Olli), Loppi, S. (Sanna), Hartikainen, P. (Päivi), Koivisto, A. M. (Anne M.), Kontkanen, A. (Aleksi), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Malm, T. (Tarja), Herukka, S. (Sanna‑Kaisa), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), Katisko, K. (Kasper), Solje, E. (Eino), Korhonen, P. (Paula), Jääskeläinen, O. (Olli), Loppi, S. (Sanna), Hartikainen, P. (Päivi), Koivisto, A. M. (Anne M.), Kontkanen, A. (Aleksi), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Malm, T. (Tarja), Herukka, S. (Sanna‑Kaisa), Remes, A. M. (Anne M.), and Haapasalo, A. (Annakaisa)
Abstract: In this study, our aim was to evaluate potential peripheral inflammatory changes in frontotemporal lobar degeneration (FTLD) patients carrying or not the C9orf72 repeat expansion. To this end, levels of several inflammatory markers (MCP-1, RANTES, IL-10, IL-17A, IL-12p, IFN-γ, IL-1β, IL-8, and hs-CRP) and blood cells counts in plasma and/or serum of FTLD patients (N = 98) with or without the C9orf72 repeat expansion were analyzed. In addition, we evaluated whether the analyzed peripheral inflammatory markers correlated with disease progression or distinct clinical phenotypes under the heterogenous FTLD spectrum. Elevated levels of pro-inflammatory RANTES or MCP-1 and decreased levels of anti-inflammatory IL-10 were found to associate with Parkinsonism and a more rapid disease progression, indicated by longitudinal measurements of either MMSE or ADCS-ADL decline. These findings were observed in the total cohort in general, whereas the C9orf72 repeat expansion carriers showed only slight differences in IL-10 and hemoglobin levels compared to non-carriers. Furthermore, these C9orf72 repeat expansion-associated differences were observed mostly in male subjects. The females in general showed elevated levels of several pro-inflammatory markers compared to males regardless of the C9orf72 genotype. Our study suggests that pro-inflammatory changes observed in the early symptomatic phase of FTLD are associated with distinct clinical profiles and a more rapid disease progression, and that the C9orf72 repeat expansion and gender may also affect the inflammatory profile in FTLD.
Published: 2020

27. The variability of functional MRI brain signal increases in Alzheimer’s disease at cardiorespiratory frequencies

Author: Tuovinen, T. (Timo), Kananen, J. (Janne), Rajna, Z. (Zalan), Lieslehto, J. (Johannes), Korhonen, V. (Vesa), Rytty, R. (Riikka), Mattila, H. (Heli), Huotari, N. (Niko), Raitamaa, L. (Lauri), Helakari, H. (Heta), Elseoud, A. A. (Ahmed Abou), Krüger, J. (Johanna), LeVan, P. (Pierre), Tervonen, O. (Osmo), Hennig, J. (Juergen), Remes, A. M. (Anne M.), Nedergaard, M. (Maiken), Kiviniemi, V. (Vesa), Tuovinen, T. (Timo), Kananen, J. (Janne), Rajna, Z. (Zalan), Lieslehto, J. (Johannes), Korhonen, V. (Vesa), Rytty, R. (Riikka), Mattila, H. (Heli), Huotari, N. (Niko), Raitamaa, L. (Lauri), Helakari, H. (Heta), Elseoud, A. A. (Ahmed Abou), Krüger, J. (Johanna), LeVan, P. (Pierre), Tervonen, O. (Osmo), Hennig, J. (Juergen), Remes, A. M. (Anne M.), Nedergaard, M. (Maiken), and Kiviniemi, V. (Vesa)
Abstract: Biomarkers sensitive to prodromal or early pathophysiological changes in Alzheimer’s disease (AD) symptoms could improve disease detection and enable timely interventions. Changes in brain hemodynamics may be associated with the main clinical AD symptoms. To test this possibility, we measured the variability of blood oxygen level-dependent (BOLD) signal in individuals from three independent datasets (totaling 80 AD patients and 90 controls). We detected a replicable increase in brain BOLD signal variability in the AD populations, which constituted a robust biomarker for clearly differentiating AD cases from controls. Fast BOLD scans showed that the elevated BOLD signal variability in AD arises mainly from cardiovascular brain pulsations. Manifesting in abnormal cerebral perfusion and cerebrospinal fluid convection, present observation presents a mechanism explaining earlier observations of impaired glymphatic clearance associated with AD in humans.
Published: 2020

28. Risk factors for reactivation of clinical disease activity in multiple sclerosis after natalizumab cessation

Author: Mustonen, T. (Tiina), Rauma, I. (Ilkka), Hartikainen, P. (Päivi), Krüger, J. (Johanna), Niiranen, M. (Marja), Selander, T. (Tuomas), Simula, S. (Sakari), Remes, A. M. (Anne M.), Kuusisto, H. (Hanna), Mustonen, T. (Tiina), Rauma, I. (Ilkka), Hartikainen, P. (Päivi), Krüger, J. (Johanna), Niiranen, M. (Marja), Selander, T. (Tuomas), Simula, S. (Sakari), Remes, A. M. (Anne M.), and Kuusisto, H. (Hanna)
Abstract: Background: Natalizumab (NTZ) is widely used for highly active relapsing-remitting multiple sclerosis (MS). Inflammatory disease activity often returns after NTZ treatment discontinuation. We aimed to identify predictive factors for such reactivation in a real-life setting. Methods: We conducted a retrospective survey in four Finnish hospitals. A computer-based search was used to identify all patients who had received NTZ for multiple sclerosis. Patients were included if they had received at least six NTZ infusions, had discontinued treatment for at least three months, and follow-up data was available for at least 12 months after discontinuation. Altogether 89 patients were analyzed with Cox regression model to identify risk factors for reactivation, defined as having a corticosteroid-treated relapse. Results: At 6 and 12 months after discontinuation of NTZ, a relapse was documented in 27.0% and 35.6% of patients, whereas corticosteroid-treated relapses were documented in 20.2% and 30.3% of patients, respectively. A higher number of relapses during the year prior to the introduction of NTZ was associated with a significantly higher risk for reactivation at 6 months (Hazard Ratio [HR] 1.65, p < 0.001) and at 12 months (HR 1.53, p < 0.001). Expanded Disability Status Scale (EDSS) of 5.5 or higher before NTZ initiation was associated with a higher reactivation risk at 6 months (HR 3.70, p = 0.020). Subsequent disease-modifying drugs (DMDs) failed to prevent reactivation of MS in this cohort. However, when subsequent DMDs were used, a washout time longer than 3 months was associated with a higher reactivation risk at 6 months regardless of whether patients were switched to first-line (HR 7.69, p = 0.019) or second-line therapies (HR 3.94, p = 0.035). Gender, age, time since diagnosis, and the number of NTZ infusions were not associated with an increased risk for reactivation. Conclusion: High disease activity and a high level of disability prior to NTZ tr
Published: 2020

29. BV-2 microglial cells overexpressing C9orf72 hexanucleotide repeat expansion produce DPR proteins and show normal functionality but no RNA foci

Author: Rostalski, H. (Hannah), Hietanen, T. (Tomi), Leskelä, S. (Stina), Behánová, A. (Andrea), Abdollahzadeh, A. (Ali), Wittrahm, R. (Rebekka), Mäkinen, P. (Petra), Huber, N. (Nadine), Hoffmann, D. (Dorit), Solje, E. (Eino), Remes, A. M. (Anne M.), Natunen, T. (Teemu), Takalo, M. (Mari), Tohka, J. (Jussi), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Rostalski, H. (Hannah), Hietanen, T. (Tomi), Leskelä, S. (Stina), Behánová, A. (Andrea), Abdollahzadeh, A. (Ali), Wittrahm, R. (Rebekka), Mäkinen, P. (Petra), Huber, N. (Nadine), Hoffmann, D. (Dorit), Solje, E. (Eino), Remes, A. M. (Anne M.), Natunen, T. (Teemu), Takalo, M. (Mari), Tohka, J. (Jussi), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: Hexanucleotide repeat expansion (HRE) in the chromosome 9 open-reading frame 72 (C9orf72) gene is the most common genetic cause underpinning frontotemporal lobar degeneration (FTLD) and amyotrophic lateral sclerosis (ALS). It leads to the accumulation of toxic RNA foci and various dipeptide repeat (DPR) proteins into cells. These C9orf72 HRE-specific hallmarks are abundant in neurons. So far, the role of microglia, the immune cells of the brain, in C9orf72 HRE-associated FTLD/ALS is unclear. In this study, we overexpressed C9orf72 HRE of a pathological length in the BV-2 microglial cell line and used biochemical methods and fluorescence imaging to investigate its effects on their phenotype, viability, and functionality. We found that BV-2 cells expressing the C9orf72 HRE presented strong expression of specific DPR proteins but no sense RNA foci. Transiently increased levels of cytoplasmic TAR DNA-binding protein 43 (TDP-43), slightly altered levels of p62 and lysosome-associated membrane protein (LAMP) 2A, and reduced levels of polyubiquitinylated proteins, but no signs of cell death were detected in HRE overexpressing cells. Overexpression of the C9orf72 HRE did not affect BV-2 cell phagocytic activity or response to an inflammatory stimulus, nor did it shift their RNA profile toward disease-associated microglia. These findings suggest that DPR proteins do not affect microglial cell viability or functionality in BV-2 cells. However, additional studies in other models are required to further elucidate the role of C9orf72 HRE in microglia.
Published: 2020

30. Diabetes is associated with familial idiopathic normal pressure hydrocephalus:a case–control comparison with family members

Author: Räsänen, J. (Joel), Huovinen, J. (Joel), Korhonen, V. E. (Ville E.), Junkkari, A. (Antti), Kastinen, S. (Sami), Komulainen, S. (Simo), Oinas, M. (Minna), Avellan, C. (Cecilia), Frantzen, J. (Janek), Rinne, J. (Jaakko), Ronkainen, A. (Antti), Kauppinen, M. (Mikko), Lönnrot, K. (Kimmo), Perola, M. (Markus), Koivisto, A. M. (Anne M.), Remes, A. M. (Anne M.), Soininen, H. (Hilkka), Hiltunen, M. (Mikko), Helisalmi, S. (Seppo), Kurki, M. I. (Mitja I.), Jääskeläinen, J. E. (Juha E.), Leinonen, V. (Ville), Räsänen, J. (Joel), Huovinen, J. (Joel), Korhonen, V. E. (Ville E.), Junkkari, A. (Antti), Kastinen, S. (Sami), Komulainen, S. (Simo), Oinas, M. (Minna), Avellan, C. (Cecilia), Frantzen, J. (Janek), Rinne, J. (Jaakko), Ronkainen, A. (Antti), Kauppinen, M. (Mikko), Lönnrot, K. (Kimmo), Perola, M. (Markus), Koivisto, A. M. (Anne M.), Remes, A. M. (Anne M.), Soininen, H. (Hilkka), Hiltunen, M. (Mikko), Helisalmi, S. (Seppo), Kurki, M. I. (Mitja I.), Jääskeläinen, J. E. (Juha E.), and Leinonen, V. (Ville)
Abstract: Background: The pathophysiological basis of idiopathic normal pressure hydrocephalus (iNPH) is still unclear. Previous studies have shown a familial aggregation and a potential heritability when it comes to iNPH. Our aim was to conduct a novel case-controlled comparison between familial iNPH (fNPH) patients and their elderly relatives, involving multiple different families. Methods: Questionnaires and phone interviews were used for collecting the data and categorising the iNPH patients into the familial (fNPH) and the sporadic groups. Identical questionnaires were sent to the relatives of the potential fNPH patients. Venous blood samples were collected for genetic studies. The disease histories of the probable fNPH patients (n = 60) were compared with their ≥ 60-year-old relatives with no iNPH (n = 49). A modified Charlson Comorbidity Index (CCI) was used to measure the overall disease burden. Fisher’s exact test (two-tailed), the Mann–Whitney U test (two-tailed) and a multivariate binary logistic regression analysis were used to perform the statistical analyses. Results: Diabetes (32% vs. 14%, p = 0.043), arterial hypertension (65.0% vs. 43%, p = 0.033), cardiac insufficiency (16% vs. 2%, p = 0.020) and depressive symptoms (32% vs. 8%, p = 0.004) were overrepresented among the probable fNPH patients compared to their non-iNPH relatives. In the age-adjusted multivariate logistic regression analysis, diabetes remained independently associated with fNPH (OR = 3.8, 95% CI 1.1–12.9, p = 0.030). Conclusions: Diabetes is associated with fNPH and a possible risk factor for fNPH. Diabetes could contribute to the pathogenesis of iNPH/fNPH, which motivates to further prospective and gene-environmental studies to decipher the disease modelling of iNPH/fNPH.
Published: 2020

31. Serum neurofilament light chain is a discriminative biomarker between frontotemporal lobar degeneration and primary psychiatric disorders

Author: Katisko, K. (Kasper), Cajanus, A. (Antti), Jääskeläinen, O. (Olli), Kontkanen, A. (Aleksi), Hartikainen, P. (Päivi), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Haapasalo, A. (Annakaisa), Koivumaa‑Honkanen, H. (Heli), Herukka, S. (Sanna‑Kaisa), Remes, A. M. (Anne M.), Solje, E. (Eino), Katisko, K. (Kasper), Cajanus, A. (Antti), Jääskeläinen, O. (Olli), Kontkanen, A. (Aleksi), Hartikainen, P. (Päivi), Korhonen, V. E. (Ville E.), Helisalmi, S. (Seppo), Haapasalo, A. (Annakaisa), Koivumaa‑Honkanen, H. (Heli), Herukka, S. (Sanna‑Kaisa), Remes, A. M. (Anne M.), and Solje, E. (Eino)
Abstract: Due to the significant clinical overlap between frontotemporal lobar degeneration (FTLD) spectrum disorders and late-onset primary psychiatric disorders (PPD), diagnostic biomarkers reflecting the different underlying pathophysiologies are urgently needed. Thus far, elevated cerebrospinal fluid (CSF) levels of neurofilament light chain (NfL) have been reported in various neurological conditions. Furthermore, recent advancements in ultrasensitive analytical methods (e.g., single molecule array, Simoa) have enabled sensitive and less invasive NfL detection also from blood samples. In this study, we evaluated the potential of serum NfL (sNfL) as a diagnostic tool between FTLD and PPD. We analyzed sNfL levels with Simoa from 125 participants including patients from FTLD (n = 91) and PPD (n = 34) spectra. Our results show that sNfL levels are higher in the FTLD group compared to the PPD group as well as in separate clinical subtypes of FTLD compared to different psychiatric manifestations (i.e., mood or psychotic disorders). At single-subject level, discrimination between FTLD and PPD was possible with 80% sensitivity and 85% specificity (AUC = 0.850, 95% CI 0.776–0.923), and between behavioral variant frontotemporal dementia (bvFTD) and PPD with 79% sensitivity and 85% specificity (AUC = 0.830, 95% CI 0.732–0.908). These findings highlight the potential of sNfL as a discriminating biomarker for FTLD over PPD in patients with wide-ranging behavioral, psychiatric and cognitive symptoms.
Published: 2020

32. Mutation analysis of the genes linked to early onset Alzheimer's disease and frontotemporal lobar degeneration

Author: Luukkainen, L. (Laura), Helisalmi, S. (Seppo), Kytövuori, L. (Laura), Ahmasalo, R. (Riitta), Solje, E. (Eino), Haapasalo, A. (Annakaisa), Hiltunen, M. (Mikko), Remes, A. M. (Anne M.), and Krüger, J. (Johanna)
Subjects: presenilin-1, missense, frontotemporal lobar degeneration, mental disorders, early onset, genetics, human, microtubule-associated protein tau, mutation, Alzheimer’s disease, frontotemporal dementia
Abstract: A lot of effort has been done to unravel the genetics underlying early-onset Alzheimer’s disease (AD) and frontotemporal lobar degeneration (FTLD). However, many familial early-onset dementia (EOD) cases still show an unclear genetic background. The aim of this study was to evaluate the role of the known causative mutations and possible pathogenic variants associated with AD and FTLD in a Finnish EOD cohort. The cohort consisted of 39 patients (mean age at onset 54.8 years, range 39–65) with a positive family history of dementia or an atypical or rapidly progressive course of the disease. None of the patients carried the C9orf72 hexanucleotide repeat expansion. Mutations and variants in APP, PSEN1, PSEN2, MAPT, GRN, VCP, CHMP2B, FUS, TARDBP, TREM2, TMEM106B, UBQLN2, SOD1, PRNP, UBQLN1, and BIN1 were screened by using a targeted next generation sequencing panel. Two previously reported pathogenic mutations (PSEN1 p.His163Arg and MAPT p.Arg406Trp) were identified in the cohort. Both patients had familial dementia with an atypical early onset phenotype. In addition, a heterozygous p.Arg71Trp mutation in PSEN2 with an uncertain pathogenic nature was identified in a patient with neuropathologically confirmed AD. In conclusion, targeted investigation of the known dementia-linked genes is worthwhile in patients with onset age under 55 and a positive family history, as well as in patients with atypical features.
Published: 2019

33. Prevalence of C9ORF72 expansion in a large series of patients with idiopathic normal-pressure hydrocephalus

Author: Korhonen, V. E. (Ville E.), Remes, A. M. (Anne M.), Helisalmi, S. (Seppo), Rauramaa, T. (Tuomas), Sutela, A. (Anna), Vanninen, R. (Ritva), Suhonen, N.-M. (Noora-Maria), Haapasalo, A. (Annakaisa), Hiltunen, M. (Mikko), Jääskeläinen, J. E. (Juha E.), Soininen, H. (Hilkka), Koivisto, A. M. (Anne M.), and Leinonen, V. (Ville)
Abstract: Background/Aims: The C9ORF72 expansion is known to cause frontotemporal lobar degeneration (FTLD) and amyotrophic lateral sclerosis (ALS). We aim to identify the prevalence of the C9ORF72 expansion in idiopathic normal pressure hydrocephalus (iNPH). Methods: We analysed the C9ORF72 expansion in a large cohort of patients with possible iNPH (n = 487) and cognitively intact elderly controls (n = 432; age > 65 years). Results: While the C9ORF72 expansion was detected in 1.6% (n = 8/487) of cases with possible iNPH, no control subject was found to carry the mutation. The mean age at onset of symptoms of C9ORF72 expansion carriers was 59 years (range: 52–67 years), 11 years less than non-carriers (p = 0.0002). The most frequent initial/main symptom pertained to gait difficulties. Despite identified mutation, only 3 of the patients fulfilled the criteria for the FTLD-ALS spectrum. Clinically significant shunt response was detected in 6 out of 7 shunted C9ORF72 expansion carriers. Conclusion: This is the first study cohort identifying the underlying C9ORF72 expansion in patients with iNPH providing evidence for the potential comorbidity between iNPH and the FTLD-ALS spectrum. Analysis of the C9ORF72 expansion should be considered for patients with probable iNPH presenting with frontal atrophy and personality changes or other severe psychiatric symptoms.
Published: 2019

34. Prodromal and early bvFTD:evaluating clinical features and current biomarkers

Author: Katisko, K. (Kasper), Cajanus, A. (Antti), Korhonen, T. (Titta), Remes, A. M. (Anne M.), Haapasalo, A. (Annakaisa), and Solje, E. (Eino)
Subjects: differential diagnostics, neuroimaging, frontotemporal lobar degeneration, C9orf72, diagnostics, biomarker, frontotemporal dementia, GRN
Abstract: Despite the current diagnostic criteria, early diagnostics of behavioral variant of frontotemporal dementia (bvFTD) has remained challenging. Patients with bvFTD often present with misleading psychiatric phenotype, and, on the other hand, impairment in memory functions have increasingly been reported. However, impaired episodic memory is currently considered as an exclusion criterion for bvFTD. Single biofluid-based or imaging biomarkers do not currently provide sufficient sensitivity or specificity for early bvFTD diagnosis at single-subject level, although studies have suggested improved accuracy with different biomarker combinations. In this mini review, we evaluate the core clinical features of early bvFTD and summarize the most potential imaging and fluid biomarkers for bvFTD diagnostics.
Published: 2019

35. Normaalipaineisen hydrokefaluksen kliininen kuva, diagnostiset tutkimukset ja hoito

Author: Leinonen, V. (Ville), Junkkari, A. (Antti), Rauramaa, T. (Tuomas), Jääskeläinen, J. E. (Juha E.), Vanninen, R. (Ritva), Savolainen, S. (Sakari), Hiltunen, M. (Mikko), Remes, A. M. (Anne M.), and Koivisto, A. M. (Anne M.)
Subjects: muistisairaudet, hydrokefalia, kävelyvaikeudet, diagnostiikka, normaalipaineinen hydrokefalia, hoito
Abstract: Acute hydrocephalus is a life-threatening emergency. Primary diagnosis and suspected shunt malfunction requires immediate CT or MR imaging and neurosurgical consultation. Normal pressure hydrocephalus (NPH) is a chronic degenerative disease but requires prompt diagnosis and treatment due to progressive nature. Recent studies indicate apparent specific disease mechanisms of idiopathic NPH including potential genetic risk factors. CSF shunt may significantly improve gait, urinary incontinence and cognitive symptoms in selected patients. Noteworthy, iNPH seems to progress frequently despite of shunt emphasizing the need for active follow-up. Recognition and appropriate treatment of potential comorbid neurodegenerative diseases like vascular dementia and Alzheimer’s disease are needed in case of cognitive deterioration. Tiivistelmä Akuutti hydrokefalia on henkeä uhkaava tila kaikenikäisillä. Mikäli sunttiriippuvaisella potilaalla epäillään suntin toimintahäiriötä, on pään TT (tai MK) tehtävä viipymättä ja tarvitessa konsultoitava päivystävää neurokirurgista yksikköä välittömästi. Normaalipaineinen hydrokefalia (NPH) on harvoin päivystyksellinen ongelma, mutta tauti on selkeästi etenevä ja hoidon viivästyminen heikentää ennustetta. Tuoreet tutkimukset avaavat idiopaattisen NPH-taudin (iNPH) etiologiaa ja patofysiologisia mekanismeja sekä ennustetta. Osalla potilaista likvorisuntti voi merkittävästi lievittää oireita, erityisesti liikkumisvaikeuksia mutta myös inkontinenssia ja tiedonkäsittelyn ongelmia. Suntista huolimatta tauti pyrkii vuosien myötä etenemään, korostaen seurannan merkitystä. iNPH potilailla on usein myös samanaikainen vaskulaarinen kognitiivinen heikkenemä, Alzheimerin tauti tai muu aivorappeumasairaus, joka on myös diagnosoitava ja hoidettava.
Published: 2019

36. The association between distinct frontal brain volumes and behavioral symptoms in mild cognitive impairment, Alzheimer's disease, and frontotemporal dementia

Author: Cajanus, A. (Antti), Solje, E. (Eino), Koikkalainen, J. (Juha), Lötjönen, J. (Jyrki), Suhonen, N.-M. (Noora-Maria), Hallikainen, I. (Ilona), Vanninen, R. (Ritva), Hartikainen, P. (Päivi), de Marco, M. (Matteo), Venneri, A. (Annalena), Soininen, H. (Hilkka), Remes, A. M. (Anne M.), Hall, A. (Anette), Cajanus, A. (Antti), Solje, E. (Eino), Koikkalainen, J. (Juha), Lötjönen, J. (Jyrki), Suhonen, N.-M. (Noora-Maria), Hallikainen, I. (Ilona), Vanninen, R. (Ritva), Hartikainen, P. (Päivi), de Marco, M. (Matteo), Venneri, A. (Annalena), Soininen, H. (Hilkka), Remes, A. M. (Anne M.), and Hall, A. (Anette)
Abstract: Our aim was to investigate the association between behavioral symptoms of agitation, disinhibition, irritability, elation, and aberrant motor behavior to frontal brain volumes in a cohort with various neurodegenerative diseases. A total of 121 patients with mild cognitive impairment (MCI, n = 58), Alzheimer's disease (AD, n = 45) and behavioral variant frontotemporal dementia (bvFTD, n = 18) were evaluated with a Neuropsychiatric Inventory (NPI). A T1-weighted MRI scan was acquired for each participant and quantified with a multi-atlas segmentation method. The volumetric MRI measures of the frontal lobes were associated with neuropsychiatric symptom scores with a linear model. In the regression model, we included CDR score and TMT B time as covariates to account for cognitive and executive functions. The brain volumes were corrected for age, gender and head size. The total behavioral symptom score of the five symptoms of interest was negatively associated with the volume of the subcallosal area (β = −0.32, p = 0.002). High disinhibition scores were associated with reduced volume in the gyrus rectus (β = −0.30, p = 0.002), medial frontal cortex (β = −0.30, p = 0.002), superior frontal gyrus (β = −0.28, p = 0.003), inferior frontal gyrus (β = −0.28, p = 0.005) and subcallosal area (β = −0.28, p = 0.005). Elation scores were associated with reduced volumes of the medial orbital gyrus (β = −0.30, p = 0.002) and inferior frontal gyrus (β = −0.28, p = 0.004). Aberrant motor behavior was associated with atrophy of frontal pole (β = −0.29, p = 0.005) and the subcallosal area (β = −0.39, p < 0.001). No significant associations with frontal brain volumes were found for agitation and irritability. We conclude that the subcallosal area may be common neuroanatomical area for behavioral symptoms in neurodegenerative diseases, and it appears to be independent of disease etiology.
Published: 2019

37. CSF biomarkers distinguish idiopathic normal pressure hydrocephalus from its mimics

Author: Jeppsson, A. (Anna), Wikkelsö, C. (Carsten), Blennow, K. (Kaj), Zetterberg, H. (Henrik), Constantinescu, R. (Radu), Remes, A. M. (Anne M), Herukka, S.-K. (Sanna-Kaisa), Rauramaa, T. (Tuomas), Nagga, K. (Katarina), Leinonen, V. (Ville), Tullberg, M. (Mats), Jeppsson, A. (Anna), Wikkelsö, C. (Carsten), Blennow, K. (Kaj), Zetterberg, H. (Henrik), Constantinescu, R. (Radu), Remes, A. M. (Anne M), Herukka, S.-K. (Sanna-Kaisa), Rauramaa, T. (Tuomas), Nagga, K. (Katarina), Leinonen, V. (Ville), and Tullberg, M. (Mats)
Abstract: Objective: To examine the differential diagnostic significance of cerebrospinal fluid (CSF) biomarkers reflecting Alzheimer’s disease-related amyloid β (Aβ) production and aggregation, cortical neuronal damage, tau pathology, damage to long myelinated axons and astrocyte activation, which hypothetically separates patients with idiopathic normal pressure hydrocephalus (iNPH) from patients with other neurodegenerative disorders. Methods: The study included lumbar CSF samples from 82 patients with iNPH, 75 with vascular dementia, 70 with Parkinson’s disease, 34 with multiple system atrophy, 34 with progressive supranuclear palsy, 15 with corticobasal degeneration, 50 with Alzheimer’s disease, 19 with frontotemporal lobar degeneration and 54 healthy individuals (HIs). We analysed soluble amyloid precursor protein alpha (sAPPα) and beta (sAPPβ), Aβ species (Aβ38, Aβ40 and Aβ42), total tau (T-tau), phosphorylated tau, neurofilament light and monocyte chemoattractant protein 1 (MCP-1). Results: Patients with iNPH had lower concentrations of tau and APP-derived proteins in combination with elevated MCP-1 compared with HI and the non-iNPH disorders. T-tau, Aβ40 and MCP-1 together yielded an area under the curve of 0.86, differentiating iNPH from the other disorders. A prediction algorithm consisting of T-tau, Aβ40 and MCP-1 was designed as a diagnostic tool using CSF biomarkers. Conclusions: The combination of the CSF biomarkers T-tau, Aβ40 and MCP-1 separates iNPH from cognitive and movement disorders with good diagnostic sensitivity and specificity. This may have important implications for diagnosis and clinical research on disease mechanisms for iNPH.
Published: 2019

38. Astrocytes and microglia as potential contributors to the pathogenesis of C9orf72 repeat expansion-associated FTLD and ALS

Author: Rostalski, H. (Hannah), Leskelä, S. (Stina), Huber, N. (Nadine), Katisko, K. (Kasper), Cajanus, A. (Antti), Solje, E. (Eino), Marttinen, M. (Mikael), Natunen, T. (Teemu), Remes, A. M. (Anne M.), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Rostalski, H. (Hannah), Leskelä, S. (Stina), Huber, N. (Nadine), Katisko, K. (Kasper), Cajanus, A. (Antti), Solje, E. (Eino), Marttinen, M. (Mikael), Natunen, T. (Teemu), Remes, A. M. (Anne M.), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: Frontotemporal lobar degeneration (FTLD) and amyotrophic lateral sclerosis (ALS) are neurodegenerative diseases with a complex, but often overlapping, genetic and pathobiological background and thus they are considered to form a disease spectrum. Although neurons are the principal cells affected in FTLD and ALS, increasing amount of evidence has recently proposed that other central nervous system-resident cells, including microglia and astrocytes, may also play roles in neurodegeneration in these diseases. Therefore, deciphering the mechanisms underlying the disease pathogenesis in different types of brain cells is fundamental in order to understand the etiology of these disorders. The major genetic cause of FTLD and ALS is a hexanucleotide repeat expansion (HRE) in the intronic region of the C9orf72 gene. In neurons, specific pathological hallmarks, including decreased expression of the C9orf72 RNA and proteins and generation of toxic RNA and protein species, and their downstream effects have been linked to C9orf72 HRE-associated FTLD and ALS. In contrast, it is still poorly known to which extent these pathological changes are presented in other brain cells. Here, we summarize the current literature on the potential role of astrocytes and microglia in C9orf72 HRE-linked FTLD and ALS and discuss their possible phenotypic alterations and neurotoxic mechanisms that may contribute to neurodegeneration in these diseases.
Published: 2019

39. Impact of a clinical decision support tool on prediction of progression in early-stage dementia:a prospective validation study

Author: Bruun, M. (Marie), Frederiksen, K. S. (Kristian S.), Rhodius-Meester, H. F. (Hanneke F. M.), Baroni, M. (Marta), Gjerum, L. (Le), Koikkalainen, J. (Juha), Urhemaa, T. (Timo), Tolonen, A. (Antti), van Gils, M. (Mark), Rueckert, D. (Daniel), Dyremose, N. (Nadia), Andersen, B. B. (Birgitte B.), Lemstra, A. W. (Afina W.), Hallikainen, M. (Merja), Kurl, S. (Sudhir), Herukka, S.-K. (Sanna-Kaisa), Remes, A. M. (Anne M.), Waldemar, G. (Gunhild), Soininen, H. (Hilkka), Mecocci, P. (Patrizia), van der Flier, W. M. (Wiesje M.), Lötjönen, J. (Jyrki), Hasselbalch, S. G. (Steen G.), Bruun, M. (Marie), Frederiksen, K. S. (Kristian S.), Rhodius-Meester, H. F. (Hanneke F. M.), Baroni, M. (Marta), Gjerum, L. (Le), Koikkalainen, J. (Juha), Urhemaa, T. (Timo), Tolonen, A. (Antti), van Gils, M. (Mark), Rueckert, D. (Daniel), Dyremose, N. (Nadia), Andersen, B. B. (Birgitte B.), Lemstra, A. W. (Afina W.), Hallikainen, M. (Merja), Kurl, S. (Sudhir), Herukka, S.-K. (Sanna-Kaisa), Remes, A. M. (Anne M.), Waldemar, G. (Gunhild), Soininen, H. (Hilkka), Mecocci, P. (Patrizia), van der Flier, W. M. (Wiesje M.), Lötjönen, J. (Jyrki), and Hasselbalch, S. G. (Steen G.)
Abstract: Background: In clinical practice, it is often difficult to predict which patients with cognitive complaints or impairment will progress or remain stable. We assessed the impact of using a clinical decision support system, the PredictND tool, to predict progression in patients with subjective cognitive decline (SCD) and mild cognitive impairment (MCI) in memory clinics. Methods: In this prospective multicenter study, we included 429 patients with SCD (n = 230) and MCI (n = 199) (female 54%, age 67 ± 9, MMSE 28 ± 2) and followed them for at least 12 months. Based on all available patient baseline data (demographics, cognitive tests, cerebrospinal fluid biomarkers, and MRI), the PredictND tool provides a comprehensive overview of the data and a classification defining the likelihood of progression. At baseline, a clinician defined an expected follow-up diagnosis and estimated the level of confidence in their prediction using a visual analogue scale (VAS, 0–100%), first without and subsequently with the PredictND tool. As outcome measure, we defined clinical progression as progression from SCD to MCI or dementia, and from MCI to dementia. Correspondence between the expected and the actual clinical progression at follow-up defined the prognostic accuracy. Results: After a mean follow-up time of 1.7 ± 0.4 years, 21 (9%) SCD and 63 (32%) MCI had progressed. When using the PredictND tool, the overall prognostic accuracy was unaffected (0.4%, 95%CI − 3.0%; + 3.9%; p = 0.79). However, restricting the analysis to patients with more certain classifications (n = 203), we found an increase of 3% in the accuracy (95%CI − 0.6%; + 6.5%; p = 0.11). Furthermore, for this subgroup, the tool alone showed a statistically significant increase in the prognostic accuracy compared to the evaluation without tool (6.4%, 95%CI 2.1%; 10.7%; p = 0.004). Specifically, the negative predictive value was high. Moreover, confidence in the prediction increased significantly (∆VAS = 4%, p
Published: 2019

40. C9orf72 proteins regulate autophagy and undergo autophagosomal or proteasomal degradation in a cell type-dependent manner

Author: Leskelä, S. (Stina), Huber, N. (Nadine), Rostalski, H. (Hannah), Natunen, T. (Teemu), Remes, A. M. (Anne M.), Takalo, M. (Mari), Hiltunen, M. (Mikko), Haapasalo, A. (Annakaisa), Leskelä, S. (Stina), Huber, N. (Nadine), Rostalski, H. (Hannah), Natunen, T. (Teemu), Remes, A. M. (Anne M.), Takalo, M. (Mari), Hiltunen, M. (Mikko), and Haapasalo, A. (Annakaisa)
Abstract: Dysfunctional autophagy or ubiquitin-proteasome system (UPS) are suggested to underlie abnormal protein aggregation in neurodegenerative diseases. Frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS)-associated C9orf72 is implicated in autophagy, but whether it activates or inhibits autophagy is partially controversial. Here, we utilized knockdown or overexpression of C9orf72 in mouse N2a neuroblastoma cells or cultured neurons to elucidate the potential role of C9orf72 proteins in autophagy and UPS. Induction of autophagy in C9orf72 knockdown N2a cells led to decreased LC3BI to LC3BII conversion, p62 degradation, and formation of LC3-containing autophagosomes, suggesting compromised autophagy. Proteasomal activity was slightly decreased. No changes in autophagy nor proteasomal activity in C9orf72-overexpressing N2a cells were observed. However, in these cells, autophagy induction by serum starvation or rapamycin led to significantly decreased C9orf72 levels. The decreased levels of C9orf72 in serum-starved N2a cells were restored by the proteasomal inhibitor lactacystin, but not by the autophagy inhibitor bafilomycin A1 (BafA1) treatment. These data suggest that C9orf72 undergoes proteasomal degradation in N2a cells during autophagy. Lactacystin significantly elevated C9orf72 levels in N2a cells and neurons, further suggesting UPS-mediated regulation. In rapamycin and BafA1-treated neurons, C9orf72 levels were significantly increased. Altogether, these findings corroborate the previously suggested regulatory role for C9orf72 in autophagy and suggest cell type-dependent regulation of C9orf72 levels via UPS and/or autophagy.
Published: 2019

41. Low serum high-density lipoprotein cholesterol levels associate with the C9orf72 repeat expansion in frontotemporal lobar degeneration patients

Author: Jääskeläinen, O. (Olli), Solje, E. (Eino), Hall, A. (Anette), Katisko, K. (Kasper), Korhonen, V. (Ville), Tiainen, M. (Mika), Kangas, A. J. (Antti J.), Helisalmi, S. (Seppo), Pikkarainen, M. (Maria), Koivisto, A. (Anne), Hartikainen, P. (Päivi), Hiltunen, M. (Mikko), Ala-Korpela, M. (Mika), Soininen, H. (Hilkka), Soininen, P. (Pasi), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), Herukka, S.-K. (Sanna-Kaisa), Jääskeläinen, O. (Olli), Solje, E. (Eino), Hall, A. (Anette), Katisko, K. (Kasper), Korhonen, V. (Ville), Tiainen, M. (Mika), Kangas, A. J. (Antti J.), Helisalmi, S. (Seppo), Pikkarainen, M. (Maria), Koivisto, A. (Anne), Hartikainen, P. (Päivi), Hiltunen, M. (Mikko), Ala-Korpela, M. (Mika), Soininen, H. (Hilkka), Soininen, P. (Pasi), Haapasalo, A. (Annakaisa), Remes, A. M. (Anne M.), and Herukka, S.-K. (Sanna-Kaisa)
Abstract: Decreased levels of serum high-density lipoprotein (HDL) cholesterol have previously been linked to systemic inflammation and neurodegenerative diseases, such as Alzheimer’s disease. Here, we aimed to analyze the lipoprotein profile and inflammatory indicators, the high-sensitivity C-reactive peptide (hs-CRP) and glycoprotein acetyls (GlycA), in sporadic and C9orf72 repeat expansion-associated frontotemporal lobar degeneration (FTLD) patients. The C9orf72 hexanucleotide repeat expansion is the most frequent genetic etiology underlying FTLD. The concentrations of different lipid measures in the sera of 67 FTLD patients (15 C9orf72 repeat expansion carriers), including GlycA, were analyzed by nuclear magnetic resonance spectroscopy. To verify the state of systemic inflammation, hs-CRP was also quantified from patient sera. We found that the total serum HDL concentration was decreased in C9orf72 repeat expansion carriers when compared to non-carriers. Moreover, decreased concentrations of HDL particles of different sizes and subclass were consistently observed. No differences were detected in the very low- and low-density lipoprotein subclasses between the C9orf72 repeat expansion carriers and non-carriers. Furthermore, hs-CRP and GlycA levels did not differ between the C9orf72 repeat expansion carriers and non-carriers. In conclusion, the HDL-related changes were linked with C9orf72 repeat expansion associated FTLD but were not seen to associate with systemic inflammation. The underlying reason for the HDL changes remains unclear.
Published: 2019

42. BP180 autoantibodies target different epitopes in multiple sclerosis or Alzheimer’s disease than in bullous pemphigoid

Author: Tuusa, J. (Jussi), Lindgren, O. (Outi), Tertsunen, H.-M. (Hanna-Mari), Nishie, W. (Wataru), Kokkonen, N. (Nina), Huilaja, L. (Laura), Izumi, K. (Kentaro), Herukka, S.-K. (Sanna-Kaisa), Miettunen, J. (Jouko), Shimizu, H. (Hiroshi), Remes, A. M. (Anne M.), Tasanen, K. (Kaisa), Tuusa, J. (Jussi), Lindgren, O. (Outi), Tertsunen, H.-M. (Hanna-Mari), Nishie, W. (Wataru), Kokkonen, N. (Nina), Huilaja, L. (Laura), Izumi, K. (Kentaro), Herukka, S.-K. (Sanna-Kaisa), Miettunen, J. (Jouko), Shimizu, H. (Hiroshi), Remes, A. M. (Anne M.), and Tasanen, K. (Kaisa)
Abstract: Neurologic patients have an increased risk for bullous pemphigoid (BP), in which autoantibodies target BP180, a cutaneous basement membrane protein also expressed in the brain. Here we show that 53.6% of sera from patients with multiple sclerosis (MS) (n = 56) had IgG reactivity against full-length BP180 in immunoblotting, while in BP180 non-collagenous 16A ELISA (n = 143), only 7.7% of MS samples studied were positive. Epitope mapping with 13 fusion proteins covering the entire BP180 polypeptide revealed that in MS and Alzheimer’s disease (AD) patients, IgG autoantibodies target regions located in the intracellular and mid-extracellular parts of BP180, but not the well-known BP epitopes located in the non-collagenous 16A domain and the distal part of extracellular domain. In indirect immunofluorescence analysis, 8.1% of MS sera recognized the cutaneous basement membrane and in full-length BP180 ELISA analysis, 7.5% MS and AD sera were positive, indicating that these autoantibodies rarely recognize BP180 in its native conformation. Thus, in MS and AD patients, BP180 autoantibodies have a different epitope profile than in patients with BP, and seldom bind to native BP180. This explains the inability of these autoantibodies to cause skin symptoms. Our results suggest that the autoantibodies against BP180 alone are not sufficient to induce BP in MS and AD patients.
Published: 2019

43. Detecting frontotemporal dementia syndromes using MRI biomarkers

Author: Bruun, M. (Marie), Koikkalainen, J. (Juha), Rhodius-Meester, H. F. (Hanneke F. M.), Baroni, M. (Marta), Gjerum, L. (Le), van Gils, M. (Mark), Soininen, H. (Hilkka), Remes, A. M. (Anne M.), Hartikainen, P. (Päivi), Waldemar, G. (Gunhild), Mecocci, P. (Patrizia), Barkhof, F. (Frederik), Pijnenburg, Y. (Yolande), van der Flier, W. M. (Wiesje M.), Hasselbalch, S. G. (Steen G.), Lötjönen, J. (Jyrki), Frederiksen, K. S. (Kristian S.), Bruun, M. (Marie), Koikkalainen, J. (Juha), Rhodius-Meester, H. F. (Hanneke F. M.), Baroni, M. (Marta), Gjerum, L. (Le), van Gils, M. (Mark), Soininen, H. (Hilkka), Remes, A. M. (Anne M.), Hartikainen, P. (Päivi), Waldemar, G. (Gunhild), Mecocci, P. (Patrizia), Barkhof, F. (Frederik), Pijnenburg, Y. (Yolande), van der Flier, W. M. (Wiesje M.), Hasselbalch, S. G. (Steen G.), Lötjönen, J. (Jyrki), and Frederiksen, K. S. (Kristian S.)
Abstract: Background: Diagnosing frontotemporal dementia may be challenging. New methods for analysis of regional brain atrophy patterns on magnetic resonance imaging (MRI) could add to the diagnostic assessment. Therefore, we aimed to develop automated imaging biomarkers for differentiating frontotemporal dementia subtypes from other diagnostic groups, and from one another. Methods: In this retrospective multicenter cohort study, we included 1213 patients (age 67 ± 9, 48% females) from two memory clinic cohorts: 116 frontotemporal dementia, 341 Alzheimer’s disease, 66 Dementia with Lewy bodies, 40 vascular dementia, 104 other dementias, 229 mild cognitive impairment, and 317 subjective cognitive decline. Three MRI atrophy biomarkers were derived from the normalized volumes of automatically segmented cortical regions: 1) the anterior vs. posterior index, 2) the asymmetry index, and 3) the temporal pole left index. We used the following performance metrics: area under the receiver operating characteristic curve (AUC), sensitivity, and specificity. To account for the low prevalence of frontotemporal dementia we pursued a high specificity of 95%. Cross-validation was used in assessing the performance. The generalizability was assessed in an independent cohort (n = 200). Results: The anterior vs. posterior index performed with an AUC of 83% for differentiation of frontotemporal dementia from all other diagnostic groups (Sensitivity = 59%, Specificity = 95%, positive likelihood ratio = 11.8, negative likelihood ratio = 0.4). The asymmetry index showed highest performance for separation of primary progressive aphasia and behavioral variant frontotemporal dementia (AUC = 85%, Sensitivity = 79%, Specificity = 92%, positive likelihood ratio = 9.9, negative likelihood ratio = 0.2), whereas the temporal pole left index was specific for detection of semantic variant primary progressive aphasia (AUC = 85%, Sensitivity = 82%, Specificity = 80%, positive likelihood ratio = 4.1, neg
Published: 2019

44. Prevalence of schizophrenia in idiopathic normal pressure hydrocephalus

Author: Vanhala, V. (Vasco), Junkkari, A. (Antti), Korhonen, V. E. (Ville E.), Kurki, M. I. (Mitja I.), Hiltunen, M. (Mikko), Rauramaa, T. (Tuomas), Nerg, O. (Ossi), Koivisto, A. M. (Anne M.), Remes, A. M. (Anne M.), Perälä, J. (Jonna), Suvisaari, J. (Jaana), Lehto, S. M. (Soili M.), Viinamäki, H. (Heimo), Soininen, H. (Hilkka), Jääskeläinen, J. E. (Juha E.), Leinonen, V. (Ville), Vanhala, V. (Vasco), Junkkari, A. (Antti), Korhonen, V. E. (Ville E.), Kurki, M. I. (Mitja I.), Hiltunen, M. (Mikko), Rauramaa, T. (Tuomas), Nerg, O. (Ossi), Koivisto, A. M. (Anne M.), Remes, A. M. (Anne M.), Perälä, J. (Jonna), Suvisaari, J. (Jaana), Lehto, S. M. (Soili M.), Viinamäki, H. (Heimo), Soininen, H. (Hilkka), Jääskeläinen, J. E. (Juha E.), and Leinonen, V. (Ville)
Abstract: Background: Idiopathic normal pressure hydrocephalus (iNPH) is a progressive and potentially treatable neurodegenerative disease affecting elderly people, characterized by gait impairment and ventricular enlargement in brain imaging. Similar findings are seen in some patients with schizophrenia (SCZ). Objective: To determine the prevalence of SCZ among patients suffering from probable or possible iNPH and the specific effects of comorbid SCZ on the outcome of the cerebrospinal fluid (CSF) shunting. Methods: All medical records of the 521 iNPH patients in the NPH registry were retrospectively analyzed from 1991 until 2017. The prevalence of comorbidity of SCZ was determined and compared to that of general aged (≥65 yr) population in Finland. Results: We identified a total of 16 (3.1%) iNPH patients suffering from comorbid SCZ. The prevalence of SCZ among the iNPH patients was significantly higher compared to the general population (3.1% vs 0.9%, P < .001). All iNPH patients with comorbid SCZ were CSF shunted and 12 (75%) had a clinically verified shunt response 3 to 12 mo after the procedure. The CSF shunt response rate did not differ between patients with and without comorbid SCZ. Conclusion: SCZ seems to occur 3 times more frequently among iNPH patients compared to the general aged population in Finland. The outcome of the treatment was not affected by comorbid SCZ and therefore iNPH patients suffering from comorbid SCZ should not be left untreated. These results merit validation in other populations. In addition, further research towards the potential connection between these chronic conditions is warranted.
Published: 2019

45. Predicting development of Alzheimer’s disease in patients with shunted idiopathic normal pressure hydrocephalus

Author: Luikku, A. J. (Antti J.), Hall, A. (Anette), Nerg, O. (Ossi), Koivisto, A. M. (Anne M.), Hiltunen, M. (Mikko), Helisalmi, S. (Seppo), Herukka, S.-K. (Sanna-Kaisa), Junkkari, A. (Antti), Sutela, A. (Anna), Kojoukhova, M. (Maria), Korhonen, V. (Ville), Mattila, J. (Jussi), Lötjönen, J. (Jyrki), Rummukainen, J. (Jaana), Alafuzoff, I. (Irina), Jääskeläinen, J. E. (Juha E.), Remes, A. M. (Anne M.), Solomon, A. (Alina), Kivipelto, M. (Miia), Soininen, H. (Hilkka), Rauramaa, T. (Tuomas), Leinonen, V. (Ville), Luikku, A. J. (Antti J.), Hall, A. (Anette), Nerg, O. (Ossi), Koivisto, A. M. (Anne M.), Hiltunen, M. (Mikko), Helisalmi, S. (Seppo), Herukka, S.-K. (Sanna-Kaisa), Junkkari, A. (Antti), Sutela, A. (Anna), Kojoukhova, M. (Maria), Korhonen, V. (Ville), Mattila, J. (Jussi), Lötjönen, J. (Jyrki), Rummukainen, J. (Jaana), Alafuzoff, I. (Irina), Jääskeläinen, J. E. (Juha E.), Remes, A. M. (Anne M.), Solomon, A. (Alina), Kivipelto, M. (Miia), Soininen, H. (Hilkka), Rauramaa, T. (Tuomas), and Leinonen, V. (Ville)
Abstract: Background: Idiopathic normal pressure hydrocephalus (iNPH) patients often develop Alzheimer’s disease (AD) related brain pathology. Disease State Index (DSI) is a method to combine data from various sources for differential diagnosis and progression of neurodegenerative disorders. Objective: To apply DSI to predict clinical AD in shunted iNPH-patients in a defined population. Methods: 335 shunted iNPH-patients (median 74 years) were followed until death (n = 185) or 6/2015 (n = 150). DSI model (including symptom profile, onset age of NPH symptoms, atrophy of medial temporal lobe in CT/MRI, cortical brain biopsy finding, and APOE genotype) was applied. Performance of DSI model was evaluated with receiver operating characteristic (ROC) curve analysis. Results: A total of 70 (21%) patients developed clinical AD during median follow-up of 5.3 years. DSI-model predicted clinical AD with moderate effectiveness (AUC = 0.75). Significant factors were cortical biopsy (0.69), clinical symptoms (0.66), and medial temporal lobe atrophy (0.66). Conclusion: We found increased occurrence of clinical AD in previously shunted iNPH patients as compared with general population. DSI supported the prediction of AD. Cortical biopsy during shunt insertion seems indicated for earlier diagnosis of comorbid AD.
Published: 2019

46. Low prevalence of cancer in patients with frontotemporal lobar degeneration

Author: Katisko, K. (Kasper), Haapasalo, A. (Annakaisa), Koivisto, A. (Anne), Krüger, J. (Johanna), Hartikainen, P. (Päivi), Korhonen, V. (Ville), Helisalmi, S. (Seppo), Herukka, S.-K. (Sanna-Kaisa), Remes, A. M. (Anne M.), and Solje, E. (Eino)
Subjects: comorbidity, frontotemporal lobar degeneration, mental disorders, nutritional and metabolic diseases, C9ORF72, cancer, frontotemporal dementia, nervous system diseases
Abstract: Several studies have reported reduced risk of cancer in patients with Alzheimer’s disease (AD) or Parkinson’s disease. The relationship between cancer and frontotemporal lobar degeneration (FTLD) has not been previously reported. Here, our aim was to evaluate the occurrence of cancer in Finnish FTLD patients with a high proportion of C9ORF72 repeat expansion carriers in comparison to age- and sex-matched group of AD patients and control subjects classified as not cognitively impaired (NCI). The prevalence of cancer was 9.7% in FTLD, 18.7% in AD, and 17.4% in NCI (FTLD versus AD p = 0.012, FTLD versus NCI p = 0.029) groups. No differences were observed between C9ORF72 repeat expansion carriers and non-carriers inside the FTLD group. To our knowledge, this is the first study showing significantly lower prevalence of cancer in FTLD patients compared to patients with AD or NCI subjects. Our data suggest an inverse association between neurodegeneration and cancer and that FTLD-specific mechanisms may underlie the especially strong inverse association observed in this study.
Published: 2018

47. Evaluating combinations of diagnostic tests to discriminate different dementia types

Author: Bruun, M. (Marie), Rhodius-Meester, H. F. (Hanneke F. M.), Koikkalainen, J. (Juha), Baroni, M. (Marta), Gjerum, L. (Le), Lemstra, A. W. (Aﬁna W.), Barkhof, F. (Frederik), Remes, A. M. (Anne M.), Urhemaa, T. (Timo), Tolonen, A. (Antti), Rueckert, D. (Daniel), van Gils, M. (Mark), Frederiksen, K. S. (Kristian S.), Waldemar, G. (Gunhild), Scheltens, P. (Philip), Mecocci, P. (Patrizia), Soininen, H. (Hilkka), Lötjönen, J. (Jyrki), Hasselbalch, S. G. (Steen G.), van der Flier, W. M. (Wiesje M.), Bruun, M. (Marie), Rhodius-Meester, H. F. (Hanneke F. M.), Koikkalainen, J. (Juha), Baroni, M. (Marta), Gjerum, L. (Le), Lemstra, A. W. (Aﬁna W.), Barkhof, F. (Frederik), Remes, A. M. (Anne M.), Urhemaa, T. (Timo), Tolonen, A. (Antti), Rueckert, D. (Daniel), van Gils, M. (Mark), Frederiksen, K. S. (Kristian S.), Waldemar, G. (Gunhild), Scheltens, P. (Philip), Mecocci, P. (Patrizia), Soininen, H. (Hilkka), Lötjönen, J. (Jyrki), Hasselbalch, S. G. (Steen G.), and van der Flier, W. M. (Wiesje M.)
Abstract: Introduction: We studied, using a data-driven approach, how different combinations of diagnostic tests contribute to the differential diagnosis of dementia. Methods: In this multicenter study, we included 356 patients with Alzheimer’s disease, 87 frontotemporal dementia, 61 dementia with Lewy bodies, 38 vascular dementia, and 302 controls. We used a classifier to assess accuracy for individual performance and combinations of cognitive tests, cerebrospinal fluid biomarkers, and automated magnetic resonance imaging features for pairwise differentiation between dementia types. Results: Cognitive tests had good performance in separating any type of dementia from controls. Cerebrospinal fluid optimally contributed to identifying Alzheimer’s disease, whereas magnetic resonance imaging features aided in separating vascular dementia, dementia with Lewy bodies, and frontotemporal dementia. Combining diagnostic tests increased the accuracy, with balanced accuracies ranging from 78% to 97%. Conclusions: Different diagnostic tests have their distinct roles in differential diagnostics of dementias. Our results indicate that combining different diagnostic tests may increase the accuracy further.
Published: 2018

48. Lifetime antipsychotic medication and cognitive performance in schizophrenia at age 43 years in a general population birth cohort

Author: Husa, A. P. (Anja P.), Moilanen, J. (Jani), Murray, G. K. (Graham K.), Marttila, R. (Riikka), Haapea, M. (Marianne), Rannikko, I. (Irina), Barnett, J. H. (Jennifer H.), Jones, P. B. (Peter B.), Isohanni, M. (Matti), Remes, A. M. (Anne M.), Koponen, H. (Hannu), Miettunen, J. (Jouko), Jääskeläinen, E. (Erika), Clinicum, Department of Psychiatry, HUS Psychiatry, School of Medicine / Clinical Medicine, Murray, Graham [0000-0001-8296-1742], Jones, Peter [0000-0002-0387-880X], and Apollo - University of Cambridge Repository
Subjects: Adult, Male, Time Factors, Neuropsychological Tests, Adverse effect, Article, Drug Administration Schedule, 3124 Neurology and psychiatry, Cohort Studies, Cognition, Cross-sectional, DOSE-REDUCTION, DEFICITS, RISPERIDONE, Humans, 1ST-EPISODE PSYCHOSIS, Finland, Biological Psychiatry, METAANALYSIS, Age Factors, Psychosis, Treatment, Psychiatry and Mental health, RELIABILITY, Schizophrenia, Female, Schizophrenic Psychology, NEUROCOGNITION, FOLLOW-UP, OLANZAPINE, Antipsychotic Agents, LONGITUDINAL MRI
Abstract: Article, This naturalistic study analysed the association between cumulative lifetime antipsychotic dose and cognition in schizophrenia after an average of 16.5 years of illness. Sixty participants with schizophrenia and 191 controls from the Northern Finland Birth Cohort 1966 were assessed at age 43 years with a neurocognitive test battery. Cumulative lifetime antipsychotic dose-years were collected from medical records and interviews. The association between antipsychotic dose-years and a cognitive composite score based on principal component analysis was analysed using linear regression. Higher lifetime antipsychotic dose-years were significantly associated with poorer cognitive composite score, when adjusted for gender, onset age and lifetime hospital treatment days. The effects of typical and atypical antipsychotics did not differ. This is the first report of an association between cumulative lifetime antipsychotic dose and global cognition in midlife schizophrenia. Based on these data, higher lifetime antipsychotic dose-years may be associated with poorer cognitive performance at age 43 years. Potential biases related to the naturalistic design may partly explain the results; nonetheless, it is possible that large antipsychotic doses harm cognition in schizophrenia in the long-term., final draft, peerReviewed
Published: 2017

49. Increased levels of the bullous pemphigoid BP180 autoantibody are associated with more severe dementia in Alzheimer's disease

Author: Kokkonen, N. (Nina), Herukka, S.-K. (Sanna-Kaisa), Huilaja, L. (Laura), Kokki, M. (Merja), Koivisto, A. M. (Anne M.), Hartikainen, P. (Päivi), Remes, A. M. (Anne M.), and Tasanen, K. (Kaisa)
Abstract: Bullous pemphigoid (BP) is a subepidermal blistering skin disease, which has shown a strong association with neurological diseases in epidemiological studies. The BP autoantigens BP180 and BP230 are expressed in the cutaneous basement membrane and the central nervous system. Using BP180 and BP230 ELISA assays and immunoblotting against BP180, we analyzed the IgG reactivity in the sera of 115 patients with Alzheimer’s disease (AD) and 40 neurologically healthy controls. BP180 autoantibodies were found in 18% of patients with AD, whereas only 3% of controls had positive results (P = 0.019). BP230 values were higher and more often elevated in patients with AD than controls, but not significantly. None of the positive AD sera that recognized the full-length human BP180 in immunoblotting reacted with the cutaneous basement membrane in indirect immunofluorescence analysis. Moreover, a retrospective evaluation of the hospital records of the patients with AD revealed neither BP diagnosis nor BP-like symptoms. Interestingly, increased BP180-NC16A autoantibody values correlated with cognitive decline measured by mini-mental state examination scores, but not with the concentration of AD biomarkers in cerebrospinal fluid. Our findings further the understanding of the role of BP180 as a shared autoantigen in neurodermatological interactions and the association between BP and neurodegenerative diseases.
Published: 2017

50. The impact of multiple sclerosis onset symptom on cardiac repolarization

Author: Mikkola, A. (Alma), Ojanen, A. (Aku), Hartikainen, J. E. (Juha E. K.), Remes, A. M. (Anne M.), Simula, S. (Sakari), Mikkola, A. (Alma), Ojanen, A. (Aku), Hartikainen, J. E. (Juha E. K.), Remes, A. M. (Anne M.), and Simula, S. (Sakari)
Abstract: Introduction: Multiple sclerosis is associated with prolonged cardiac repolarization but the underlying physiology has remained unknown. In this study, we compared cardiac repolarization during the relapsing- remitting multiple sclerosis (RRMS) disease course in patients with motor and sensory onset symptom. Methods: Twenty- five RRMS patients with motor and 33 RRMS patients with sensory onset symptom having 12- lead electrocardiogram (ECG) recorded at the time of the first demyelinating event (ECG1) as well as at the later disease course (ECG2) were identified from the patient records. The average time interval between ECG1 and ECG2 was 8.6 ± 5.9 y. Heart rate-corrected QT intervals reflecting cardiac repolarization were calculated by Bazett (QTcBaz), Fridericia (QTcFri), and Karjalainen (QTcKar) formulas. Results: Heart rate-corrected QT intervals as well as heart rate were similar in patients with motor and sensory onset symptom in ECG1. However, QTcBaz (p = .002), QTcFri (p = .019), and QTcKar (p = .026) were longer and heart rate was higher (p = .035) in patients with motor than sensory onset symptom in ECG2. Correspondingly, QTcBaz (p = .002), QTcFri (p = .033), and QTcKar (p = .043) prolonged and heart rate tended to increase (p = .060) during the disease course only in the patients with motor onset symptom. Conclusions: Cardiac repolarization prolonged and heart rate increased during the disease course in RRMS patients with motor but not with sensory onset symptom. This suggests different traits in RRMS according to its initial manifestation and also association of motor onset symptom with more unfavorable cardiovascular prognostic determinants.
Published: 2017

Catalog

Books, media, physical & digital resources

See catalog results

Searchworks

Select search scope, currently: Articles Catalog books, media & more in Jio Institute collections Articles journal articles & other e-resources

Search

Search Constraints

Refine your results

Search Limiters

Topic

Publication Year Range

Language

Publication Type

Database

Publisher

65 results on '"Remes, A. M. (Anne M.)"'

Search Results

Catalog

Select search scope, currently: Articles

Catalog

books, media & more in Jio Institute collections

Articles

journal articles & other e-resources