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2. Endoscopic third ventriculostomy for adults with hydrocephalus:creating a prognostic model for success: protocol for a retrospective multicentre study (Nordic ETV)

Author

Tefre, S. (Sondre), Lilja-Cyron, A. (Alexander), Arvidsson, L. (Lisa), Bartek, J. (Jiri), Corell, A. (Alba), Forsse, A. (Axel), Glud, A. N. (Andreas Nørgaard), Hamdeh, S. A. (Sami Abu), Hansen, F. L. (Frederik Lundgaard), Huotarinen, A. (Antti), Johansson, C. (Conny), Kämäräinen, O.-P. (Olli-Pekka), Korhonen, T. (Tommi), Kotkansalo, A. (Anna), Mansoor, N. M. (Nadia Mauland), Mireles, E. E. (Eduardo Erasmo Mendoza), Miscov, R. (Rares), Munthe, S. (Sune), Nittby-Redebrandt, H. (Henrietta), Obad, N. (Nina), Pedersen, L. K. (Lars Kjelsberg), Posti, J. (Jussi), Raj, R. (Rahul), Satopää, J. (Jarno), Ståhl, N. (Nils), Tetri, S. (Sami), Tobieson, L. (Lovisa), Juhler, M. (Marianne), Tefre, S. (Sondre), Lilja-Cyron, A. (Alexander), Arvidsson, L. (Lisa), Bartek, J. (Jiri), Corell, A. (Alba), Forsse, A. (Axel), Glud, A. N. (Andreas Nørgaard), Hamdeh, S. A. (Sami Abu), Hansen, F. L. (Frederik Lundgaard), Huotarinen, A. (Antti), Johansson, C. (Conny), Kämäräinen, O.-P. (Olli-Pekka), Korhonen, T. (Tommi), Kotkansalo, A. (Anna), Mansoor, N. M. (Nadia Mauland), Mireles, E. E. (Eduardo Erasmo Mendoza), Miscov, R. (Rares), Munthe, S. (Sune), Nittby-Redebrandt, H. (Henrietta), Obad, N. (Nina), Pedersen, L. K. (Lars Kjelsberg), Posti, J. (Jussi), Raj, R. (Rahul), Satopää, J. (Jarno), Ståhl, N. (Nils), Tetri, S. (Sami), Tobieson, L. (Lovisa), and Juhler, M. (Marianne)

Abstract

Introduction: Endoscopic third ventriculostomy (ETV) is becoming an increasingly widespread treatment for hydrocephalus, but research is primarily based on paediatric populations. In 2009, Kulkarni et al created the ETV Success score to predict the outcome of ETV in children. The purpose of this study is to create a prognostic model to predict the success of ETV for adult patients with hydrocephalus. The ability to predict who will benefit from an ETV will allow better primary patient selection both for ETV and shunting. This would reduce additional second procedures due to primary treatment failure. A success score specific for adults could also be used as a communication tool to provide better information and guidance to patients. Methods and analysis: The study will adhere to the Transparent Reporting of a multivariable prediction model for Individual Prognosis Or Diagnosis reporting guidelines and conducted as a retrospective chart review of all patients≥18 years of age treated with ETV at the participating centres between 1 January 2010 and 31 December 2018. Data collection is conducted locally in a standardised database. Univariate analysis will be used to identify several strong predictors to be included in a multivariate logistic regression model. The model will be validated using K-fold cross validation. Discrimination will be assessed using area under the receiver operating characteristic curve (AUROC) and calibration with calibration belt plots. Ethics and dissemination: The study is approved by appropriate ethics or patient safety boards in all participating countries.

Published
2022

4. Alterations in mitochondria-endoplasmic reticulum connectivity in human brain biopsies from idiopathic normal pressure hydrocephalus patients

Author

Leal, N. S. (Nuno Santos), Dentoni, G. (Giacomo), Schreiner, B. (Bernadette), Kämäräinen, O.-P. (Olli-Pekka), Partanen, N. (Nelli), Herukka, S.-K. (Sanna-Kaisa), Koivisto, A. M. (Anne M), Hiltunen, M. (Mikko), Rauramaa, T. (Tuomas), Leinonen, V. (Ville), Ankarcrona, M. (Maria), Leal, N. S. (Nuno Santos), Dentoni, G. (Giacomo), Schreiner, B. (Bernadette), Kämäräinen, O.-P. (Olli-Pekka), Partanen, N. (Nelli), Herukka, S.-K. (Sanna-Kaisa), Koivisto, A. M. (Anne M), Hiltunen, M. (Mikko), Rauramaa, T. (Tuomas), Leinonen, V. (Ville), and Ankarcrona, M. (Maria)

Abstract

Idiopathic normal pressure hydrocephalus (iNPH) is a neuropathology with unknown cause characterised by gait impairment, cognitive decline and ventriculomegaly. These patients often present comorbidity with Alzheimer’s disease (AD), including AD pathological hallmarks such as amyloid plaques mainly consisting of amyloid β-peptide and neurofibrillary tangles consisting of hyperphosphorylated tau protein. Even though some of the molecular mechanisms behind AD are well described, little is known about iNPH. Several studies have reported that mitochondria-endoplasmic reticulum contact sites (MERCS) regulate amyloid β-peptide metabolism and conversely that amyloid β-peptide can influence the number of MERCS. MERCS have also been shown to be dysregulated in several neurological pathologies including AD. In this study we have used transmission electron microscopy and show, for the first time, several mitochondria contact sites including MERCS in human brain biopsies. These unique human brain samples were obtained during neurosurgery from 14 patients that suffer from iNPH. Three of these 14 patients presented comorbidities with other dementias: one patient with AD, one with AD and vascular dementia and one patient with Lewy body dementia. Furthermore, we report that the numbers of MERCS are increased in biopsies obtained from patients diagnosed with dementia. Moreover, the presence of both amyloid plaques and neurofibrillary tangles correlates with decreased contact length between endoplasmic reticulum and mitochondria, while amyloid plaques alone do not seem to affect endoplasmic reticulum-mitochondria apposition. Interestingly, we report a significant positive correlation between the number of MERCS and ventricular cerebrospinal fluid amyloid β-peptide levels, as well as with increasing age of iNPH patients.

Published
2018

5. Erratum: EMQN Best Practice Guidelines for molecular genetic testing of SCAs (European Journal of Human Genetics)

Author

Giunti P, Kämäräinen O, Volpini V, Weirich H, Christodoulou K, Bazak N, Sinke R, Sulek-Piatkowska A, Garcia-Planells J, Davis M, Frontali M, Hämäläinen P, Wieczorek S, Zühlke C, Saraiva-Pereira ML, Warner J, Leguern E, Thonney F, Quintáns Castro B, Jonasson J, Storm K, Andersson A, Ravani A, Correia L, Silveira I, Alonso I, Martins C, Pinto Basto J, Coutinho P, Perdigão A, Barton D, Davis M and European Molecular Quality Genetics Network .multiple author names added.

Published
2010
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6. The search for susceptibility genes in osteoarthritis

Author

Kämäräinen, O.-P. (Olli-Pekka)

Subjects
Osteoarthritis - genetics, inflammation, linkage analysis
Abstract

This work engaged Finnish females affected with osteoarthritis (OA) of the hand to define the role of common sequence variations within the genes of the important structural protein of cartilage, aggrecan (AGC1), and the genes of inflammatory mediators, the interleukin 1 gene cluster and interleukin 6 (IL6), as possible risk factors for the disease. Also, a genome-wide linkage analysis was performed in a sample consisting of Finnish families with multiple individuals affected with hip and knee OA in order to reveal new chromosomal areas that are likely to contain disease associated variations. OA is a chronic disease that leads to the degeneration of articular cartilage in synovial joints. The etiology of the disease is for the most part unknown. Joints of the hand, hip and knee are most commonly affected, and obesity, trauma and excess mechanical stress are known risk factors for the disease. OA also has a significant genetic component. AGC1 carries a variable number of tandem repeats (VNTR) polymorphism, which may be significant for the biomechanical properties of cartilage. It was shown that the most common allele with 27 tandem repeats is protective against hand OA (HOA) (odds ratio 0.46, 95% confidence interval 0.27–0.78). Also, carrying two copies of any of the shorter or longer alleles increased the risk of the disease. Inflammation seems to play a role in the etiology of OA and certain polymorphisms within the interleukin 1 gene cluster and IL6 have been previously shown to increase the transcription of these molecules and to associate with OA. In this study it was shown that the G alleles in three common IL6 promoter single nucleotide polymorphism (SNP) sites are associated with the risk of more severe forms of HOA (p = 0.001 for GGG haplotype). A SNP in IL1B associated with the bilateral form of the disease (p = 0.006) and two IL1B-IL1RN extended haplotype alleles were associated with the same phenotype. Genome-wide and fine mapping linkage analyses recognized chromosomal locus 2q21 with a multipoint LOD score of 3.96. Despite the association analyses of several candidate genes within the locus, no disease-associating sequence variants were identified.

Published
2009

7. Capturing the catalytic intermediates of parkin ubiquitination.

Author

Connelly EM, Rintala-Dempsey AC, Gundogdu M, Freeman EA, Koszela J, Aguirre JD, Zhu G, Kämäräinen O, Tadayon R, Walden H, and Shaw GS

Subjects
Humans, Catalytic Domain, Ubiquitin metabolism, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Conjugating Enzymes genetics, Parkinson Disease metabolism, Parkinson Disease genetics, Models, Molecular, Ubiquitin-Protein Ligases metabolism, Ubiquitin-Protein Ligases genetics, Ubiquitination
Abstract

Parkin is an E3 ubiquitin ligase implicated in early-onset forms of Parkinson's disease. It catalyzes a transthiolation reaction by accepting ubiquitin (Ub) from an E2 conjugating enzyme, forming a short-lived thioester intermediate, and transfers Ub to mitochondrial membrane substrates to signal mitophagy. A major impediment to the development of Parkinsonism therapeutics is the lack of structural and mechanistic detail for the essential, short-lived transthiolation intermediate. It is not known how Ub is recognized by the catalytic Rcat domain in parkin that enables Ub transfer from an E2~Ub conjugate to the catalytic site and the structure of the transthiolation complex is undetermined. Here, we capture the catalytic intermediate for the Rcat domain of parkin in complex with ubiquitin (Rcat-Ub) and determine its structure using NMR-based chemical shift perturbation experiments. We show that a previously unidentified α-helical region near the Rcat domain is unmasked as a recognition motif for Ub and guides the C-terminus of Ub toward the parkin catalytic site. Further, we apply a combination of guided AlphaFold modeling, chemical cross-linking, and single turnover assays to establish and validate a model of full-length parkin in complex with UbcH7, its donor Ub, and phosphoubiquitin, trapped in the process of transthiolation. Identification of this catalytic intermediate and orientation of Ub with respect to the Rcat domain provides important structural insights into Ub transfer by this E3 ligase and explains how the previously enigmatic Parkinson's pathogenic mutation T415N alters parkin activity., Competing Interests: Competing interests statement:The authors declare no competing interest.

Published
2024
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8. Allosteric mechanism for site-specific ubiquitination of FANCD2.

Author

Chaugule VK, Arkinson C, Rennie ML, Kämäräinen O, Toth R, and Walden H

Subjects
Allosteric Regulation physiology, Amino Acid Sequence, DNA Damage, DNA Repair, Fanconi Anemia Complementation Group D2 Protein physiology, Fanconi Anemia Complementation Group L Protein physiology, Fanconi Anemia Complementation Group Proteins metabolism, Fanconi Anemia Complementation Group Proteins physiology, Humans, Protein Binding, Substrate Specificity, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Conjugating Enzymes physiology, Ubiquitination, Fanconi Anemia Complementation Group D2 Protein metabolism, Fanconi Anemia Complementation Group L Protein metabolism
Abstract

DNA-damage repair is implemented by proteins that are coordinated by specialized molecular signals. One such signal in the Fanconi anemia (FA) pathway for the repair of DNA interstrand crosslinks is the site-specific monoubiquitination of FANCD2 and FANCI. The signal is mediated by a multiprotein FA core complex (FA-CC) however, the mechanics for precise ubiquitination remain elusive. We show that FANCL, the RING-bearing module in FA-CC, allosterically activates its cognate ubiqutin-conjugating enzyme E2 UBE2T to drive site-specific FANCD2 ubiquitination. Unlike typical RING E3 ligases, FANCL catalyzes ubiquitination by rewiring the intraresidue network of UBE2T to influence the active site. Consequently, a basic triad unique to UBE2T engages a structured acidic patch near the target lysine on FANCD2. This three-dimensional complementarity, between the E2 active site and substrate surface, induced by FANCL is central to site-specific monoubiquitination in the FA pathway. Furthermore, the allosteric network of UBE2T can be engineered to enhance FANCL-catalyzed FANCD2-FANCI di-monoubiquitination without compromising site specificity.

Published
2020
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9. EMQN Best Practice Guidelines for molecular genetic testing of SCAs.

Author

Sequeiros J, Martindale J, Seneca S, Giunti P, Kämäräinen O, Volpini V, Weirich H, Christodoulou K, Bazak N, Sinke R, Sulek-Piatkowska A, Garcia-Planells J, Davis M, Frontali M, Hämäläinen P, Wieczorek S, Zühlke C, Saraiva-Pereira ML, Warner J, Leguern E, Thonney F, Quintáns Castro B, Jonasson J, Storm K, Andersson A, Ravani A, Correia L, Silveira I, Alonso I, Martins C, Pinto Basto J, Coutinho P, Perdigão A, Barton D, and Davis M

Subjects
Humans, Genetic Testing methods, Spinocerebellar Ataxias diagnosis, Spinocerebellar Ataxias genetics
Published
2010
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10. Molecular modeling of prohibitin domains.

Author

Winter A, Kämäräinen O, and Hofmann A

Subjects
Amino Acid Sequence, Conserved Sequence genetics, Humans, Molecular Sequence Data, Peptide Hydrolases metabolism, Prohibitins, Repressor Proteins genetics, Repressor Proteins metabolism, Sequence Alignment, Sequence Homology, Models, Molecular, Protein Structure, Secondary, Protein Structure, Tertiary, Repressor Proteins chemistry
Abstract

Prohibitins comprise a family of highly conserved ubiquitous eukaryotic proteins that mainly localize to the mitochondria. They have been implicated in important cellular processes such as cellular signaling and transcriptional control, apoptosis, cellular senescence, and mitochondrial biogenesis. Using molecular modeling techniques, we have generated structural models of human prohibitins BAP32 and BAP37, which have previously been shown to exist as large ringlike oligomers in the membrane-bound state. The middle domain of prohibitins is evolutionary conserved in the family of SPFH (PHB) domain proteins. On the basis of the known structure of flotillin-2, another member of the SPFH-domain family, we have generated homology models for BAP32 and BAP37, and elucidated the implications for formation of high molecular weight oligomers. A model for the dimeric-building block of BAP32: BAP37 for such assemblies was generated and its stability scrutinized by molecular dynamics simulations. The model of BAP32 was also analyzed as to potential ligand-binding sites and the previously identified ligand melanogenin was docked into a membrane-proximal cavity. The results are discussed in the context of prohibitin interactions with mitochondrial AAA-proteases and we suggest two possible interaction interfaces between the BAP32:BAP37 building block and the protease., (2007 Wiley-Liss, Inc.)

Published
2007
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11. Pathological consequences of VCP mutations on human striated muscle.

Author

Hübbers CU, Clemen CS, Kesper K, Böddrich A, Hofmann A, Kämäräinen O, Tolksdorf K, Stumpf M, Reichelt J, Roth U, Krause S, Watts G, Kimonis V, Wattjes MP, Reimann J, Thal DR, Biermann K, Evert BO, Lochmüller H, Wanker EE, Schoser BG, Noegel AA, and Schröder R

Subjects
Adenosine Triphosphatases, Aged, Cardiomyopathy, Dilated metabolism, Cardiomyopathy, Dilated pathology, Cell Cycle Proteins metabolism, Cells, Cultured, Chromosomes, Human, Pair 9 genetics, DNA Mutational Analysis methods, Databases, Genetic, Female, Humans, Ligands, Male, Microscopy, Confocal, Middle Aged, Muscle, Skeletal metabolism, Myoblasts pathology, Myositis, Inclusion Body metabolism, Myositis, Inclusion Body pathology, Osteitis Deformans genetics, Osteitis Deformans pathology, Phenotype, Protein Binding, Protein Structure, Tertiary, Spinal Diseases genetics, Spinal Diseases pathology, Transduction, Genetic, Transfection, Valosin Containing Protein, Cardiomyopathy, Dilated genetics, Cell Cycle Proteins genetics, Muscle, Skeletal ultrastructure, Mutation, Myositis, Inclusion Body genetics
Abstract

Mutations in the valosin-containing protein (VCP, p97) gene on chromosome 9p13-p12 cause a late-onset form of autosomal dominant inclusion body myopathy associated with Paget disease of the bone and frontotemporal dementia (IBMPFD). We report on the pathological consequences of three heterozygous VCP (R93C, R155H, R155C) mutations on human striated muscle. IBMPFD skeletal muscle pathology is characterized by degenerative changes and filamentous VCP- and ubiquitin-positive cytoplasmic and nuclear protein aggregates. Furthermore, this is the first report demonstrating that mutant VCP leads to a novel form of dilatative cardiomyopathy with inclusion bodies. In contrast to post-mitotic striated muscle cells and neurons of IBMPFD patients, evidence of protein aggregate pathology was not detected in primary IBMPFD myoblasts or in transient and stable transfected cells using wild-type-VCP and R93C-, R155H-, R155C-VCP mutants. Glutathione S-transferase pull-down experiments showed that all three VCP mutations do not affect the binding to Ufd1, Npl4 and ataxin-3. Structural analysis demonstrated that R93 and R155 are both surface-accessible residues located in the centre of cavities that may enable ligand-binding. Mutations at R93 and R155 are predicted to induce changes in the tertiary structure of the VCP protein. The search for putative ligands to the R93 and R155 cavities resulted in the identification of cyclic sugar compounds with high binding scores. The latter findings provide a novel link to VCP carbohydrate interactions in the complex pathology of IBMPFD.

Published
2007
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