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1. Taksi Jukka Moilanen secures contract for Transport services (excl. Waste transport)

Subjects
Transportation industry -- Contracts, Contract agreement, News, opinion and commentary
Abstract

Finland based Taksi Jukka Moilanen has secured contract from Suomussalmen kunta for Transport services (excl. Waste transport). The contract is valued approximately 65 000.00 EUR. Copyright © 2011-2021 pivotalsources.com. All [...]

Published
2021

2. Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility.

Author

Timo A Kumpula, Sandra Vorimo, Taneli T Mattila, Luke O'Gorman, Galuh Astuti, Anna Tervasmäki, Susanna Koivuluoma, Tiina M Mattila, Mervi Grip, Robert Winqvist, Outi Kuismin, Jukka Moilanen, Alexander Hoischen, Christian Gilissen, Tuomo Mantere, and Katri Pylkäs

Subjects
Genetics, QH426-470
Abstract

Copy number variants (CNVs) are a major source of genetic variation and can disrupt genes or affect gene dosage. They are known to be causal or underlie predisposition to various diseases. However, the role of CNVs in inherited breast cancer susceptibility has not been thoroughly investigated. To address this, we performed whole-exome sequencing based analysis of rare CNVs in 98 high-risk Northern Finnish breast cancer cases. After filtering, selected candidate alleles were validated and characterized with a combination of orthogonal methods, including PCR-based approaches, optical genome mapping and long-read sequencing. This revealed three recurrent alterations: a 31 kb deletion co-occurring with a retrotransposon insertion (delins) in RAD52, a 13.4 kb deletion in HSD17B14 and a 64 kb partial duplication of RAD51C. Notably, all these genes encode proteins involved in pathways previously identified as essential for breast cancer development. Variants were genotyped in geographically matched cases and controls (altogether 278 hereditary and 1983 unselected breast cancer cases, and 1229 controls). The RAD52 delins and HSD17B14 deletion both showed significant enrichment among cases with indications of hereditary disease susceptibility. RAD52 delins was identified in 7/278 cases (2.5%, P = 0.034, OR = 2.86, 95% CI = 1.10-7.45) and HSD17B14 deletion in 8/278 cases (2.9%, P = 0.014, OR = 3.28, 95% CI = 1.31-8.23), the frequency of both variants in the controls being 11/1229 (0.9%). This suggests a role for RAD52 and HSD17B14 in hereditary breast cancer susceptibility. The RAD51C duplication was very rare, identified only in 2/278 of hereditary cases and 2/1229 controls (P = 0.157, OR = 4.45, 95% CI = 0.62-31.70). The identification of recurrent CNVs in these genes, and especially the relatively high frequency of RAD52 and HSD17B14 alterations in the Finnish population, highlights the importance of studying CNVs alongside single nucleotide variants when searching for genetic factors underlying hereditary disease predisposition.

Published
2023
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3. Predisposition to childhood acute lymphoblastic leukemia caused by a constitutional translocation disrupting ETV6

Author

Tekla Järviaho, Benedicte Bang, Vasilios Zachariadis, Fulya Taylan, Jukka Moilanen, Merja Möttönen, C.I. Edvard Smith, Arja Harila-Saari, Riitta Niinimäki, and Ann Nordgren

Subjects
Specialties of internal medicine, RC581-951
Abstract

Pathogenic germline variants in ETV6 have been associated with familial predisposition to thrombocytopenia and hematological malignancies, predominantly childhood B-cell precursor acute lymphoblastic leukemia (BCP-ALL). In addition, overrepresentation of a high hyperdiploid subtype and older age at diagnosis have been reported among sporadic BCP-ALL cases with germline variants in ETV6. We studied a family with 2 second-degree relatives who developed childhood high hyperdiploid BCP-ALL at ages 8 and 12 years, respectively. A constitutional balanced reciprocal translocation t(12;14)(p13.2;q23.1) was discovered in both patients by routine karyotyping at diagnosis and, subsequently, in 7 healthy family members who had not experienced hematological malignancies. No carriers had thrombocytopenia. Whole-genome sequencing confirmed the translocation, resulting in 2 actively transcribed but nonfunctional fusion genes, causing heterozygous loss and consequently monoallelic expression of ETV6. Whole-genome sequencing analysis of the affected female subjects' leukemia excluded additional somatic aberrations in ETV6 and RTN1 as well as shared somatic variants in other genes. Expression studies, performed to confirm decreased expression of ETV6, were not conclusive. We suggest that germline aberrations resulting in monoallelic expression of ETV6 contribute to leukemia susceptibility, whereas more severe functional deficiency of ETV6 is required for developing THC5. To our knowledge, this report is the first of a constitutional translocation disrupting ETV6 causing predisposition to childhood ALL.

Published
2019
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4. Exome sequencing in routine diagnostics: a generic test for 254 patients with primary immunodeficiencies

Author

Peer Arts, Annet Simons, Mofareh S. AlZahrani, Elanur Yilmaz, Eman AlIdrissi, Koen J. van Aerde, Njood Alenezi, Hamza A. AlGhamdi, Hadeel A. AlJubab, Abdulrahman A. Al-Hussaini, Fahad AlManjomi, Alaa B. Alsaad, Badr Alsaleem, Abdulrahman A. Andijani, Ali Asery, Walid Ballourah, Chantal P. Bleeker-Rovers, Marcel van Deuren, Michiel van der Flier, Erica H. Gerkes, Christian Gilissen, Murad K. Habazi, Jayne Y. Hehir-Kwa, Stefanie S. Henriet, Esther P. Hoppenreijs, Sarah Hortillosa, Chantal H. Kerkhofs, Riikka Keski-Filppula, Stefan H. Lelieveld, Khurram Lone, Marius A. MacKenzie, Arjen R. Mensenkamp, Jukka Moilanen, Marcel Nelen, Jaap ten Oever, Judith Potjewijd, Pieter van Paassen, Janneke H. M. Schuurs-Hoeijmakers, Anna Simon, Tomasz Stokowy, Maartje van de Vorst, Maaike Vreeburg, Anja Wagner, Gijs T. J. van Well, Dimitra Zafeiropoulou, Evelien Zonneveld-Huijssoon, Joris A. Veltman, Wendy A. G. van Zelst-Stams, Eissa A. Faqeih, Frank L. van de Veerdonk, Mihai G. Netea, and Alexander Hoischen

Subjects
Routine diagnostics, Genetic diagnosis, Exome sequencing, Primary immunodeficiencies, Medicine, Genetics, QH426-470
Abstract

Abstract Background Diagnosis of primary immunodeficiencies (PIDs) is complex and cumbersome yet important for the clinical management of the disease. Exome sequencing may provide a genetic diagnosis in a significant number of patients in a single genetic test. Methods In May 2013, we implemented exome sequencing in routine diagnostics for patients suffering from PIDs. This study reports the clinical utility and diagnostic yield for a heterogeneous group of 254 consecutively referred PID patients from 249 families. For the majority of patients, the clinical diagnosis was based on clinical criteria including rare and/or unusual severe bacterial, viral, or fungal infections, sometimes accompanied by autoimmune manifestations. Functional immune defects were interpreted in the context of aberrant immune cell populations, aberrant antibody levels, or combinations of these factors. Results For 62 patients (24%), exome sequencing identified pathogenic variants in well-established PID genes. An exome-wide analysis diagnosed 10 additional patients (4%), providing diagnoses for 72 patients (28%) from 68 families altogether. The genetic diagnosis directly indicated novel treatment options for 25 patients that received a diagnosis (34%). Conclusion Exome sequencing as a first-tier test for PIDs granted a diagnosis for 28% of patients. Importantly, molecularly defined diagnoses indicated altered therapeutic options in 34% of cases. In addition, exome sequencing harbors advantages over gene panels as a truly generic test for all genetic diseases, including in silico extension of existing gene lists and re-analysis of existing data.

Published
2019
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5. Evaluating the role of CHEK2 p.(Asp438Tyr) allele in inherited breast cancer predisposition

Author

Timo A. Kumpula, Susanna Koivuluoma, Leila Soikkonen, Sandra Vorimo, Jukka Moilanen, Robert Winqvist, Tuomo Mantere, Outi Kuismin, and Katri Pylkäs

Subjects
Cancer Research, Breast cancer, Oncology, p.(Asp438Tyr) variant, Genetics, Hereditary predisposition, Cohort study, CHEK2, Genetics (clinical)
Abstract

CHEK2 is a well-established breast cancer susceptibility gene. The most frequent pathogenic CHEK2 variant is 1100delC, a loss-of-function mutation conferring 2-fold risk for breast cancer. This gene also harbors other rare variants encountered in the clinical gene panels for hereditary cancer. One of these is CHEK2 c.1312 G > T, p.(Asp438Tyr) in the kinase domain of the protein, but due to its rarity its clinical significance for breast cancer predisposition has remained unclear. Here, we tested the prevalence of CHEK2 p.(Asp438Tyr) allele showing enrichment in the Northern Finnish population, in a total of 2284 breast cancer patients from this geographical region. Genotyping was performed for DNA samples extracted from peripheral blood using high-resolution melt analysis. Fourteen CHEK2 p.(Asp438Tyr) carriers were identified (14/2284, 0.6%, P = 0.67): two in the cohort of breast cancer cases with the indication of inherited disease susceptibility (2/281, 0.7%, P = 1.00) and twelve in the breast cancer cohort unselected for the family history of disease and age at disease onset (12/2003, 0.6%, P = 0.66). This frequency did not differ from the frequency in the general population (10/1299, 0.8%). No CHEK2 p.(Asp438Tyr) homozygotes were identified. Our results indicate that CHEK2 p.(Asp438Tyr) carriers do not have an increased risk for breast cancer and the classification of the CHEK2 p.(Asp438Tyr) variant can be changed from the variant of uncertain significance (VUS) to likely benign for breast cancer.

Published
2023
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6. Truncating TINF2 p.Tyr312Ter variant and inherited breast cancer susceptibility

Author

Susanna Koivuluoma, Sandra Vorimo, Tiina M. Mattila, Anna Tervasmäki, Timo Kumpula, Outi Kuismin, Robert Winqvist, Jukka Moilanen, Tuomo Mantere, and Katri Pylkäs

Subjects
Cancer Research, Breast cancer, Oncology, Genetics, Hereditary predisposition, Dyskeratosis congenita, TINF2, Genetics (clinical)
Abstract

TINF2 is a critical subunit of the shelterin complex, which protects and maintains the length of telomeres. Pathogenic missense and truncating TINF2 mutations are causative for dyskeratosis congenita (DC), a rare, dominantly inherited bone marrow failure syndrome characterized by mucocutaneous abnormalities and cancer predisposition. Recent reports indicate that specific TINF2 truncating mutations act as high penetrance cancer predisposition alleles outside DC context, including breast cancer in their tumor spectrum. Here, we have evaluated the role of germline mutations in TINF2 and other shelterin genes in inherited breast cancer susceptibility using exome sequencing data from 98 Northern Finnish breast cancer cases with indication of inherited disease predisposition as a discovery cohort. A single protein truncating variant, TINF2 p.Tyr312Ter, was identified in one of the cases (1/98), and four more carriers were observed in the subsequently genotyped unselected breast cancer cohort (4/1904). None of the carriers were reported to have DC. TINF2 p.Tyr312Ter resulted in stable short form of mRNA transcript, and normal telomere length has been indicated by a recent report. Although recurrent in cases (total of 5/2095), TINF2 p.Tyr312Ter is also present in Finnish population controls (8/12,517), and the observed 4-fold higher frequency in cases falls at most into the range of moderate breast cancer risk alleles (OR 3.74, 95% CI 1.22–11.45, p = 0.029). Current results indicate that not all TINF2 truncating variants are high cancer risk alleles and add further evidence that different TINF2 mutations can have very diverse effects on the disease phenotype.

Published
2023

7. Contributors

Author

Steve A. Arshinoff, Bjorn Alvar Johansson, Charles Claoué, David Pérez Silguero, Susan Riyu Qi, Mike Yuan Chen, Mélanie Hébert, David Chang, Ike Iqbal Ahmed, Edna Almodin, Jean-Marie Andre, Haripriya Aravind, Ehud I. Assia, Charles Bekibele, John Bolger, Lisandro Carnielli, James A. Carolan, Dalibor Cholevik, Faye Dance, Petra Davidova, Erin L. Dohaney, Kristen A. Eckert, Bob Edwards, Jeronimo Fabiani Beng, Ivo Ferreira Rios, Oliver Findl, Oliver Yañez Garcia, Ivo Guber, Josef Guber, Rishi Gupta, Warren Hill, Huck A. Holz, Thomas Kohnen, Kari Krootila, Johann Kruger, Laurent Lalonde, Van Charles Lansingh, Michael Lawless, Mun Wai Lee, Y.C. Lee, Marie Eve Légaré, Francisco Sánchez Leon, Christopher Liu, Bita Manzouri, Samuel Masket, Keiki R. Mehta, Cyres Mehta, Syed Farzad Mohammadi, Jukka Moilanen, Magdalena Nenning, Rudy M.M.A. Nuits, Tom Oetting, Saif Bani Oraba, Madhavi Panchamia, Austin Pereira, Miguel Angel Pérez Silguero, R.D. Ravindran, Sloan Rush, Amulya Sahu, Chinmaya Sahu, Rocio Sánchez Sanoja, Steve Schallhorn, Dr. Ahmed Shalaby Bardan, Sewa Singal, Kevin Smith, Lindsay S. Spekreijse, Kent Stiverson, Pavel Stodulka, Yi Ning J. Strube, Jörg Stürmer, Ronit Yagev, Eunice You, and Mehran Zarei-Ghanavati

Published
2023
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10. Psychiatric symptoms in Salla disease

Author

Ida Aulanko, Elisa Rahikkala, and Jukka Moilanen

Subjects
Psychiatry and Mental health, Pediatrics, Perinatology and Child Health, Developmental and Educational Psychology, General Medicine
Abstract

Salla disease (SD) is a rare lysosomal storage disorder characterised by intellectual disability ataxia, athetosis, nystagmus, and central nervous system demyelination. Although the neurological spectrum of SD’s clinical phenotype is well defined, psychotic symptoms in SD remain unreported. We reviewed the presence of psychiatric symptoms in patients diagnosed with SD. Medical records of all SD patients at Oulu University Hospital during the years 1982–2015 were systematically reviewed to evaluate the presence of psychiatric symptoms. Psychiatric symptoms were frequently associated with SD (10/24, 42%), and two patients were described as developing psychosis as adolescents. We reported their clinical characteristics in detail and assessed the prevalence of psychiatric symptoms in a cohort of 24 patients. Other psychiatric factors associated with SD were sleeping disorders (8/24, 32%), aggressive behaviour disorders or restlessness (6/24, 25%), and off-label antipsychotic medication (4/24, 17%). This report expands the knowledge of the phenotypic spectrum of SD and demonstrates the importance of recognising the possibility of psychiatric symptoms, including psychosis, in persons with SD.

Published
2021

11. Tear Film Lipid Layer Structure: Self-Assembly of

Author

Tuomo, Viitaja, Jukka, Moilanen, Kirsi Johanna, Svedström, Filip S, Ekholm, and Riku O, Paananen

Subjects
Tears, Fatty Acids, Biophysics, Esters, Lipids
Abstract

In healthy eyes, the tear film lipid layer (TFLL) is considered to act as an evaporation resistant barrier, which prevents eyes from drying. Seeking to understand the mechanisms behind the evaporation resistance of the TFLL, we studied mixtures of lipid layer wax esters and

Published
2021

13. A novel variant in SMG9 causes intellectual disability, confirming a role for nonsense-mediated decay components in neurocognitive development

Author

Elisa Rahikkala, Lea Urpa, Bishwa Ghimire, Hande Topa, Mitja I. Kurki, Maryna Koskela, Mikko Airavaara, Eija Hämäläinen, Katri Pylkäs, Jarmo Körkkö, Helena Savolainen, Anu Suoranta, Aida Bertoli-Avella, Arndt Rolfs, Pirkko Mattila, Mark Daly, Aarno Palotie, Olli Pietiläinen, Jukka Moilanen, Outi Kuismin, Institute for Molecular Medicine Finland, Genomics of Neurological and Neuropsychiatric Disorders, Faculty of Medicine, Neuroscience Center, Statistical and population genetics, Helsinki Institute of Life Science HiLIFE, Helsinki Institute of Sustainability Science (HELSUS), Drug Research Program, Division of Pharmacology and Pharmacotherapy, Divisions of Faculty of Pharmacy, and Research Programs Unit

Subjects
EXPRESSION, Genetics of the nervous system, MUTATIONS, Disease genetics, Homozygote, 1184 Genetics, developmental biology, physiology, Intracellular Signaling Peptides and Proteins, GENE, Nonsense Mediated mRNA Decay, Intellectual Disability, BINDING, Genetics, Humans, 3111 Biomedicine, Gene expression, RNA, Messenger, RNA SURVEILLANCE COMPLEX, TRANSCRIPTOME, Genetics (clinical), Alleles
Abstract

Biallelic loss-of-function variants in the SMG9 gene, encoding a regulatory subunit of the mRNA nonsense-mediated decay (NMD) machinery, are reported to cause heart and brain malformation syndrome. Here we report five patients from three unrelated families with intellectual disability (ID) and a novel pathogenic SMG9 c.551 T > C p.(Val184Ala) homozygous missense variant, identified using exome sequencing. Sanger sequencing confirmed recessive segregation in each family. SMG9 c.551T > C p.(Val184Ala) is most likely an autozygous variant identical by descent. Characteristic clinical findings in patients were mild to moderate ID, intention tremor, pyramidal signs, dyspraxia, and ocular manifestations. We used RNA sequencing of patients and age- and sex-matched healthy controls to assess the effect of the variant. RNA sequencing revealed that the SMG9 c.551T > C variant did not affect the splicing or expression level of SMG9 gene products, and allele-specific expression analysis did not provide evidence that the nonsense mRNA-induced NMD was affected. Differential gene expression analysis identified prevalent upregulation of genes in patients, including the genes SMOX, OSBP2, GPX3, and ZNF155. These findings suggest that normal SMG9 function may be involved in transcriptional regulation without affecting nonsense mRNA-induced NMD. In conclusion, we demonstrate that the SMG9 c.551T > C missense variant causes a neurodevelopmental disorder and impacts gene expression. NMD components have roles beyond aberrant mRNA degradation that are crucial for neurocognitive development.

Published
2021

14. On the importance of chain branching in tear film lipid layer wax and cholesteryl esters

Author

Tuomo Viitaja, Jan-Erik Raitanen, Antti Hynynen, Jukka Moilanen, Kirsi Svedström, Riku O. Paananen, Filip S. Ekholm, Department of Chemistry, Silmäklinikka, HUS Head and Neck Center, Faculty of Science, Department of Physics, and Clinicum

Subjects
Structural elucidation, HUMAN MEIBUM, 116 Chemical sciences, Biophysics, PHYSICAL-PROPERTIES, MONOLAYERS, Esters, Surfaces and Interfaces, General Medicine, Lipids, EVAPORATION, HYDROXY FATTY-ACIDS, Colloid and Surface Chemistry, X-RAY-DIFFRACTION, SURFACE PHASE, Tears, Tear film lipid layer, MEIBOMIAN GLAND, WATER, lipids (amino acids, peptides, and proteins), Chemical synthesis, Cholesterol Esters, Physical and Theoretical Chemistry, BEHAVIOR, Biotechnology
Abstract

The tear film lipid layer (TFLL) is important to the maintenance of ocular surface health. Surprisingly, information on the individual roles of the myriad of unique lipids found therein is limited. The most abundant lipid species are the wax esters (WE) and cholesteryl esters (CE), and, especially their branched analogs. The isolation of these lipid species from the TFLL has proved to be tedious, and as a result, insights on their biophysical profiles and role in the TFLL is currently lacking. Herein, we circumvent these issues by a total synthesis of the most abundant iso-methyl branched WEs and CEs found in the TFLL. Through a detailed characterization of the biophysical properties, by the use of Langmuir monolayer and wide-angle X-ray scattering techniques, we demonstrate that chain branching alters the behavior of these lipid species on multiple levels. Taken together, our results fill an important knowledge gap concerning the structure and function of the TFLL on the whole.

Published
2022
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15. Correction to The Properties and Role of O-Acyl-ω-hydroxy Fatty Acids and Type I-St and Type II Diesters in the Tear Film Lipid Layer Revealed by a Combined Chemistry and Biophysics Approach

Author

Tuomo Viitaja, Jan-Erik Raitanen, Jukka Moilanen, Riku O. Paananen, and Filip S. Ekholm

Subjects
Tears, Organic Chemistry, Fatty Acids, Biophysics, Lipids, Addition/Correction
Abstract

The tear film lipid layer (TFLL) that covers the ocular surface contains several unique lipid classes, including

Published
2021

16. Cancer Risks Associated With Germline

Author

Xin, Yang, Goska, Leslie, Alicja, Doroszuk, Sandra, Schneider, Jamie, Allen, Brennan, Decker, Alison M, Dunning, James, Redman, James, Scarth, Inga, Plaskocinska, Craig, Luccarini, Mitul, Shah, Karen, Pooley, Leila, Dorling, Andrew, Lee, Muriel A, Adank, Julian, Adlard, Kristiina, Aittomäki, Irene L, Andrulis, Peter, Ang, Julian, Barwell, Jonine L, Bernstein, Kristie, Bobolis, Åke, Borg, Carl, Blomqvist, Kathleen B M, Claes, Patrick, Concannon, Adeline, Cuggia, Julie O, Culver, Francesca, Damiola, Antoine, de Pauw, Orland, Diez, Jill S, Dolinsky, Susan M, Domchek, Christoph, Engel, D Gareth, Evans, Florentia, Fostira, Judy, Garber, Lisa, Golmard, Ellen L, Goode, Stephen B, Gruber, Eric, Hahnen, Christopher, Hake, Tuomas, Heikkinen, Judith E, Hurley, Ramunas, Janavicius, Zdenek, Kleibl, Petra, Kleiblova, Irene, Konstantopoulou, Anders, Kvist, Holly, Laduca, Ann S G, Lee, Fabienne, Lesueur, Eamonn R, Maher, Arto, Mannermaa, Siranoush, Manoukian, Rachel, McFarland, Wendy, McKinnon, Alfons, Meindl, Kelly, Metcalfe, Nur Aishah, Mohd Taib, Jukka, Moilanen, Katherine L, Nathanson, Susan, Neuhausen, Pei Sze, Ng, Tu, Nguyen-Dumont, Sarah M, Nielsen, Florian, Obermair, Kenneth, Offit, Olufunmilayo I, Olopade, Laura, Ottini, Judith, Penkert, Katri, Pylkäs, Paolo, Radice, Susan J, Ramus, Vilius, Rudaitis, Lucy, Side, Rachel, Silva-Smith, Valentina, Silvestri, Anne-Bine, Skytte, Thomas, Slavin, Jana, Soukupova, Carlo, Tondini, Alison H, Trainer, Gary, Unzeitig, Lydia, Usha, Thomas, van Overeem Hansen, James, Whitworth, Marie, Wood, Cheng Har, Yip, Sook-Yee, Yoon, Amal, Yussuf, George, Zogopoulos, David, Goldgar, John L, Hopper, Georgia, Chenevix-Trench, Paul, Pharoah, Sophia H L, George, Judith, Balmaña, Claude, Houdayer, Paul, James, Zaki, El-Haffaf, Hans, Ehrencrona, Marketa, Janatova, Paolo, Peterlongo, Heli, Nevanlinna, Rita, Schmutzler, Soo-Hwang, Teo, Mark, Robson, Tuya, Pal, Fergus, Couch, Jeffrey N, Weitzel, Aaron, Elliott, Melissa, Southey, Robert, Winqvist, Douglas F, Easton, William D, Foulkes, Antonis C, Antoniou, and Marc, Tischkowitz

Subjects
Adult, Aged, 80 and over, Male, Ovarian Neoplasms, Risk, Internationality, Age Factors, Middle Aged, Breast Neoplasms, Male, Pancreatic Neoplasms, Neoplasms, RAPID COMMUNICATIONS, Humans, Female, Genetic Predisposition to Disease, Fanconi Anemia Complementation Group N Protein, Germ-Line Mutation, Aged
Abstract

PURPOSE: To estimate age-specific relative and absolute cancer risks of breast cancer and to estimate risks of ovarian, pancreatic, male breast, prostate, and colorectal cancers associated with germline PALB2 pathogenic variants (PVs) because these risks have not been extensively characterized. METHODS: We analyzed data from 524 families with PALB2 PVs from 21 countries. Complex segregation analysis was used to estimate relative risks (RRs; relative to country-specific population incidences) and absolute risks of cancers. The models allowed for residual familial aggregation of breast and ovarian cancer and were adjusted for the family-specific ascertainment schemes. RESULTS: We found associations between PALB2 PVs and risk of female breast cancer (RR, 7.18; 95% CI, 5.82 to 8.85; P = 6.5 × 10(−76)), ovarian cancer (RR, 2.91; 95% CI, 1.40 to 6.04; P = 4.1 × 10(−3)), pancreatic cancer (RR, 2.37; 95% CI, 1.24 to 4.50; P = 8.7 × 10(−3)), and male breast cancer (RR, 7.34; 95% CI, 1.28 to 42.18; P = 2.6 × 10(−2)). There was no evidence for increased risks of prostate or colorectal cancer. The breast cancer RRs declined with age (P for trend = 2.0 × 10(−3)). After adjusting for family ascertainment, breast cancer risk estimates on the basis of multiple case families were similar to the estimates from families ascertained through population-based studies (P for difference = .41). On the basis of the combined data, the estimated risks to age 80 years were 53% (95% CI, 44% to 63%) for female breast cancer, 5% (95% CI, 2% to 10%) for ovarian cancer, 2%-3% (95% CI females, 1% to 4%; 95% CI males, 2% to 5%) for pancreatic cancer, and 1% (95% CI, 0.2% to 5%) for male breast cancer. CONCLUSION: These results confirm PALB2 as a major breast cancer susceptibility gene and establish substantial associations between germline PALB2 PVs and ovarian, pancreatic, and male breast cancers. These findings will facilitate incorporation of PALB2 into risk prediction models and optimize the clinical cancer risk management of PALB2 PV carriers.

Published
2019

17. The conflictual sense of commercialisation and academic entrepreneurship

Author

Tero Montonen, Jukka Moilanen, and Päivi Eriksson

Subjects
Power (social and political), Organizational Behavior and Human Resource Management, Empirical data, Entrepreneurship, Power dynamics, Work (electrical), Engineering ethics, Formative context, Sociology, Sensemaking
Abstract

This article draws attention to how scientists make sense of commercialisation activities at the university. Using the critical sensemaking lens (CSM), it illustrates how the juxtaposition of the dominant discourse of academic research and the emerging discourse of commercialisation in academic work (re)produces a tensioned and conflictual sense of commercialisation and academic entrepreneurship (AE). The article is based on empirical data gathered from a two-year study of scientists working on a project that included both research and commercialisation activities. The contribution of this article is twofold; it argues that commercialisation is not only about organising and funding, but also about power dynamics and it demonstrates how hybrid projects that aim to integrate research with commercialisation activities offer rich data for the researchers of AE.

Published
2021
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18. Where does it lead to? Nowhere! Problematic sensemaking concerning commercialisation

Author

Päivi Eriksson, Tero Montonen, and Jukka Moilanen

Subjects
Organizational Behavior and Human Resource Management, Entrepreneurship, University spin-off, Action (philosophy), business.industry, Process (engineering), Sociology, Sensemaking, Public relations, Construct (philosophy), business, Business development, Centrality
Abstract

This study utilised Weick's sensemaking framework to understand academic entrepreneurship as a social process. This paper presents an analysis of the sensemaking process of a group of scientists, assisted by a university business advisor, who aimed to establish a university spin-off company. The case study shows how the scientists failed to construct a new sense of commercialisation in their business development project. Analysing personal interviews with the scientists, this study investigated problematic sensemaking concerning commercialisation activities and academic entrepreneurship. In addition to showing how problems in sensemaking produced hesitation rather than action in business development, the findings emphasise the centrality of identities, enactments, salient cues and social contexts in organising commercialisation activities at universities.

Published
2019
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20. Erratum

Author

Jean-Marie Robine and Jukka Moilanen

Subjects
Aged, 80 and over, Male, Aging, Longevity, Mutation, Humans, Female, Cell Biology, Erratum, DNA, Mitochondrial, Oxidative Phosphorylation
Abstract

To re-examine the correlation between mtDNA variability and longevity, we examined mtDNAs from samples obtained from over 2200 ultranonagenarians (and an equal number of controls) collected within the framework of the GEHA EU project. The samples were categorized by high-resolution classification, while about 1300 mtDNA molecules (650 ultranonagenarians and an equal number of controls) were completely sequenced. Sequences, unlike standard haplogroup analysis, made possible to evaluate for the first time the cumulative effects of specific, concomitant mtDNA mutations, including those that per se have a low, or very low, impact. In particular, the analysis of the mutations occurring in different OXPHOS complex showed a complex scenario with a different mutation burden in 90+ subjects with respect to controls. These findings suggested that mutations in subunits of the OXPHOS complex I had a beneficial effect on longevity, while the simultaneous presence of mutations in complex I and III (which also occurs in J subhaplogroups involved in LHON) and in complex I and V seemed to be detrimental, likely explaining previous contradictory results. On the whole, our study, which goes beyond haplogroup analysis, suggests that mitochondrial DNA variation does affect human longevity, but its effect is heavily influenced by the interaction between mutations concomitantly occurring on different mtDNA genes.

Published
2015

21. Analysis of variants in the complement factor H, the elongation of very long chain fatty acids-like 4 and the hemicentin 1 genes of age-related macular degeneration in the Finnish population

Author

Seitsonen, Sanna P., Susanna Lemmelä, Juha Holopainen, Petri Tommila, Päivi Ranta, Antti Kotamies, Jukka Moilanen, Tapani Palosaari, Kai Kaarniranta, Seppo Meri, Ilkka Immonen, and Irma Järvelä

Subjects
Extracellular Matrix Proteins, Genotype, Genetic Variation, Immunoglobulins, Membrane Proteins, Blood Donors, Macular Degeneration, Gene Frequency, Case-Control Studies, Complement Factor H, Humans, Eye Proteins, Finland, Aged
Abstract

A strong association of a Tyr402His polymorphism in the complement factor H (CFH) gene and a Met299Val polymorphism in the elongation of very long chain fatty acids-like 4 (ELOVL4) gene with age-related macular degeneration (AMD) has been identified in Caucasian populations in the United States. Earlier a Gln5345Arg variant in the hemicentin 1 (HMCN1) gene was reported in a large AMD family in the United States. We wanted to investigate whether the polymorphisms of the CFH and the ELOVL4 genes or the mutation of the HMCN1 gene are associated with AMD in patients originating from the Finnish population with characteristics of a genetic isolate.The material consisted of familial (n=181) and sporadic cases (n=154) with AMD, a control group with no AMD (non-AMD controls, n=105), and a control group of anonymous blood donors (blood donor controls, n =350). The DNA of the subjects was sequenced to analyze the variants of the three genes.We detected a strong association between the C/C-genotype compared to the T/T-genotype of Tyr402His polymorphism (first base of the Tyr-codon changes) of the CFH gene and AMD in the AMD cases compared to the non-AMD (p=8.86x10(-12)) or to blood donor controls (p=2.02x10(-13)). The frequency of the C/C genotype was significantly increased in both familial cases compared to non-AMD controls with non-adjusted odds ratio (OR) 10.1 (confidence intervals [CI] 95% 4.64-22.2) or compared to blood donor controls with non-adjusted OR 5.50 (CI 95% 3.17-9.55) and in sporadic cases with non-adjusted OR 9.33 (CI 95% 4.10-21.3; non-AMD-controls), OR 5.06 (CI 95% 2.75-9.28; blood donor controls). Frequency of C allele differed significantly between cases and controls (p=1.32x10(-11); non-AMD-controls and p=3.94x10(-14); blood donor controls). No association with AMD was detected with Met299Val polymorphism in the ELOVL4 gene in the familial or sporadic cases compared to non-AMD or blood donor controls. None of our subjects (258 AMD cases, 72 non-AMD controls) had the Gln5345Arg variant in the HMCN1 gene.The CFH gene polymorphism seems to be an important etiologic factor for AMD also in the isolated Finnish population.

Published
2006

22. DR-GPT: A large language model for medical report analysis of diabetic retinopathy patients.

Author

Jaskari, Joel, Sahlsten, Jaakko, Summanen, Paula, Moilanen, Jukka, Lehtola, Erika, Aho, Marjo, Säpyskä, Elina, Hietala, Kustaa, and Kaski, Kimmo

Subjects
LANGUAGE models, DIABETIC retinopathy, ETIOLOGY of diabetes, MEDICAL databases, EYE examination
Abstract

Diabetic retinopathy (DR) is a sight-threatening condition caused by diabetes. Screening programmes for DR include eye examinations, where the patient's fundi are photographed, and the findings, including DR severity, are recorded in the medical report. However, statistical analyses based on DR severity require structured labels that calls for laborious manual annotation process if the report format is unstructured. In this work, we propose a large language model DR-GPT for classification of the DR severity from unstructured medical reports. On a clinical set of medical reports, DR-GPT reaches 0.975 quadratic weighted Cohen's kappa using truncated Early Treatment Diabetic Retinopathy Study scale. When DR-GPT annotations for unlabeled data are paired with corresponding fundus images, the additional data improves image classifier performance with statistical significance. Our analysis shows that large language models can be applied for unstructured medical report databases to classify diabetic retinopathy with a variety of applications. [ABSTRACT FROM AUTHOR]

Published
2024
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24. Psychiatric symptoms in Salla disease.

Author

Aulanko, Ida, Rahikkala, Elisa, and Moilanen, Jukka

Subjects
ACADEMIC medical centers, PSYCHOSES, PASSIVE-aggressive personality, RETROSPECTIVE studies, ACQUISITION of data, LYSOSOMAL storage diseases, RISK assessment, SLEEP disorders, MEDICAL records, DESCRIPTIVE statistics, PSYCHOMOTOR disorders, DATA analysis software, RARE diseases, PHENOTYPES, ANTIPSYCHOTIC agents, CHILDREN, ADOLESCENCE
Abstract

Salla disease (SD) is a rare lysosomal storage disorder characterised by intellectual disability ataxia, athetosis, nystagmus, and central nervous system demyelination. Although the neurological spectrum of SD's clinical phenotype is well defined, psychotic symptoms in SD remain unreported. We reviewed the presence of psychiatric symptoms in patients diagnosed with SD. Medical records of all SD patients at Oulu University Hospital during the years 1982–2015 were systematically reviewed to evaluate the presence of psychiatric symptoms. Psychiatric symptoms were frequently associated with SD (10/24, 42%), and two patients were described as developing psychosis as adolescents. We reported their clinical characteristics in detail and assessed the prevalence of psychiatric symptoms in a cohort of 24 patients. Other psychiatric factors associated with SD were sleeping disorders (8/24, 32%), aggressive behaviour disorders or restlessness (6/24, 25%), and off-label antipsychotic medication (4/24, 17%). This report expands the knowledge of the phenotypic spectrum of SD and demonstrates the importance of recognising the possibility of psychiatric symptoms, including psychosis, in persons with SD. [ABSTRACT FROM AUTHOR]

Published
2023
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25. Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility.

Author

Kumpula, Timo A., Vorimo, Sandra, Mattila, Taneli T., O'Gorman, Luke, Astuti, Galuh, Tervasmäki, Anna, Koivuluoma, Susanna, Mattila, Tiina M., Grip, Mervi, Winqvist, Robert, Kuismin, Outi, Moilanen, Jukka, Hoischen, Alexander, Gilissen, Christian, Mantere, Tuomo, and Pylkäs, Katri

Subjects
DNA copy number variations, CANCER susceptibility, BREAST cancer, DNA repair, SINGLE nucleotide polymorphisms, BRCA genes
Abstract

Copy number variants (CNVs) are a major source of genetic variation and can disrupt genes or affect gene dosage. They are known to be causal or underlie predisposition to various diseases. However, the role of CNVs in inherited breast cancer susceptibility has not been thoroughly investigated. To address this, we performed whole-exome sequencing based analysis of rare CNVs in 98 high-risk Northern Finnish breast cancer cases. After filtering, selected candidate alleles were validated and characterized with a combination of orthogonal methods, including PCR-based approaches, optical genome mapping and long-read sequencing. This revealed three recurrent alterations: a 31 kb deletion co-occurring with a retrotransposon insertion (delins) in RAD52, a 13.4 kb deletion in HSD17B14 and a 64 kb partial duplication of RAD51C. Notably, all these genes encode proteins involved in pathways previously identified as essential for breast cancer development. Variants were genotyped in geographically matched cases and controls (altogether 278 hereditary and 1983 unselected breast cancer cases, and 1229 controls). The RAD52 delins and HSD17B14 deletion both showed significant enrichment among cases with indications of hereditary disease susceptibility. RAD52 delins was identified in 7/278 cases (2.5%, P = 0.034, OR = 2.86, 95% CI = 1.10–7.45) and HSD17B14 deletion in 8/278 cases (2.9%, P = 0.014, OR = 3.28, 95% CI = 1.31–8.23), the frequency of both variants in the controls being 11/1229 (0.9%). This suggests a role for RAD52 and HSD17B14 in hereditary breast cancer susceptibility. The RAD51C duplication was very rare, identified only in 2/278 of hereditary cases and 2/1229 controls (P = 0.157, OR = 4.45, 95% CI = 0.62–31.70). The identification of recurrent CNVs in these genes, and especially the relatively high frequency of RAD52 and HSD17B14 alterations in the Finnish population, highlights the importance of studying CNVs alongside single nucleotide variants when searching for genetic factors underlying hereditary disease predisposition. Author summary: For breast cancer susceptibility, CNVs represent an inadequately studied class of genetic variation that could explain a part of the inherited risk. Here, we performed whole-exome sequencing based analysis of rare CNVs in 98 hereditary breast cancer cases and identified recurrent alterations in RAD52, RAD51C and HSD17B14 genes. Of these, RAD52 and RAD51C are involved in DNA damage response pathway, whereas HSD17B14 encodes a protein involved in steroid hormone metabolism. These CNVs were characterized at nucleotide level and genotyped in additional Northern Finnish case-control cohorts. The CNVs that disrupted RAD52 and HSD17B14 genes showed enrichment among cases with a family history of the disease and/or early disease onset, suggesting a role for these alterations in breast cancer susceptibility. Overall, the identification of these gene-disrupting recurrent CNVs emphasizes the need to consider CNV detection in the analysis pipelines when searching for novel predisposing alleles for breast cancer. [ABSTRACT FROM AUTHOR]

Published
2023
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26. Evaluating the role of CHEK2 p.(Asp438Tyr) allele in inherited breast cancer predisposition.

Author

Kumpula, Timo A., Koivuluoma, Susanna, Soikkonen, Leila, Vorimo, Sandra, Moilanen, Jukka, Winqvist, Robert, Mantere, Tuomo, Kuismin, Outi, and Pylkäs, Katri

Subjects
CHECKPOINT kinase 2, BREAST cancer, BRCA genes, AGE of onset, FAMILY history (Medicine)
Abstract

CHEK2 is a well-established breast cancer susceptibility gene. The most frequent pathogenic CHEK2 variant is 1100delC, a loss-of-function mutation conferring 2-fold risk for breast cancer. This gene also harbors other rare variants encountered in the clinical gene panels for hereditary cancer. One of these is CHEK2 c.1312 G > T, p.(Asp438Tyr) in the kinase domain of the protein, but due to its rarity its clinical significance for breast cancer predisposition has remained unclear. Here, we tested the prevalence of CHEK2 p.(Asp438Tyr) allele showing enrichment in the Northern Finnish population, in a total of 2284 breast cancer patients from this geographical region. Genotyping was performed for DNA samples extracted from peripheral blood using high-resolution melt analysis. Fourteen CHEK2 p.(Asp438Tyr) carriers were identified (14/2284, 0.6%, P = 0.67): two in the cohort of breast cancer cases with the indication of inherited disease susceptibility (2/281, 0.7%, P = 1.00) and twelve in the breast cancer cohort unselected for the family history of disease and age at disease onset (12/2003, 0.6%, P = 0.66). This frequency did not differ from the frequency in the general population (10/1299, 0.8%). No CHEK2 p.(Asp438Tyr) homozygotes were identified. Our results indicate that CHEK2 p.(Asp438Tyr) carriers do not have an increased risk for breast cancer and the classification of the CHEK2 p.(Asp438Tyr) variant can be changed from the variant of uncertain significance (VUS) to likely benign for breast cancer. [ABSTRACT FROM AUTHOR]

Published
2023
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27. Truncating TINF2 p.Tyr312Ter variant and inherited breast cancer susceptibility.

Author

Koivuluoma, Susanna, Vorimo, Sandra, Mattila, Tiina M., Tervasmäki, Anna, Kumpula, Timo, Kuismin, Outi, Winqvist, Robert, Moilanen, Jukka, Mantere, Tuomo, and Pylkäs, Katri

Subjects
CANCER susceptibility, BREAST cancer, BRCA genes, DISEASE susceptibility, DISEASE risk factors
Abstract

TINF2 is a critical subunit of the shelterin complex, which protects and maintains the length of telomeres. Pathogenic missense and truncating TINF2 mutations are causative for dyskeratosis congenita (DC), a rare, dominantly inherited bone marrow failure syndrome characterized by mucocutaneous abnormalities and cancer predisposition. Recent reports indicate that specific TINF2 truncating mutations act as high penetrance cancer predisposition alleles outside DC context, including breast cancer in their tumor spectrum. Here, we have evaluated the role of germline mutations in TINF2 and other shelterin genes in inherited breast cancer susceptibility using exome sequencing data from 98 Northern Finnish breast cancer cases with indication of inherited disease predisposition as a discovery cohort. A single protein truncating variant, TINF2 p.Tyr312Ter, was identified in one of the cases (1/98), and four more carriers were observed in the subsequently genotyped unselected breast cancer cohort (4/1904). None of the carriers were reported to have DC. TINF2 p.Tyr312Ter resulted in stable short form of mRNA transcript, and normal telomere length has been indicated by a recent report. Although recurrent in cases (total of 5/2095), TINF2 p.Tyr312Ter is also present in Finnish population controls (8/12,517), and the observed 4-fold higher frequency in cases falls at most into the range of moderate breast cancer risk alleles (OR 3.74, 95% CI 1.22–11.45, p = 0.029). Current results indicate that not all TINF2 truncating variants are high cancer risk alleles and add further evidence that different TINF2 mutations can have very diverse effects on the disease phenotype. [ABSTRACT FROM AUTHOR]

Published
2023
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28. A comprehensive model for measuring real‐life cost‐effectiveness in eyecare: automation in care and evaluation of system (aces‐rwm™).

Author

Tuulonen, Anja, Kataja, Marko, Aaltonen, Vesa, Kinnunen, Kati, Moilanen, Jukka, Saarela, Ville, Linna, Miika, Malmivaara, Antti, and Uusitalo‐Jarvinen, Hannele

Subjects
COST effectiveness, QUALITY of life, AUTOMATION, HOLISTIC nursing, VISION, CLINICAL trials monitoring
Abstract

This paper describes a holistic, yet simple and comprehensible, ecosystem model to deal with multiple and complex challenges in eyecare. It aims at producing the best possible wellbeing and eyesight with the available resources. When targeting to improve the real‐world cost‐effectiveness, what gets done in everyday practice needs be measured routinely, efficiently and unselectively. Collection of all real‐world data of all patients will enable evaluation and comparison of eyecare systems and departments between themselves nationally and internationally. The concept advocates a strategy to optimize real‐life effectiveness, sustainability and outcomes of the service delivery in ophthalmology. The model consists of three components: (1) resource‐governing principles (i.e., to deal with increasing demand and limited resources), (2) real‐world monitoring (i.e., to collect structured real‐world data utilizing automation and visualization of clinical parameters, health‐related quality of life and costs), and (3) digital innovation strategy (i.e., to evaluate and benchmark real‐world outcomes and cost‐effectiveness). The core value and strength of the model lies in the consensus and collaboration of all Finnish university eye clinics to collect and evaluate the uniformly structured real‐world outcomes data. In addition to ophthalmology, the approach is adaptable to any medical discipline to efficiently generate real‐world insights and resilience in health systems. [ABSTRACT FROM AUTHOR]

Published
2022
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29. The ethical implications of genetic testing in neurodegenerative diseases: A systematic review.

Author

Nurmi, Sanna-Maria, Halkoaho, Arja, Moilanen, Jukka, Remes, Anne M., and Solje, Eino

Subjects
CINAHL database, ONLINE information services, ETHICS, SYSTEMATIC reviews, GENETIC testing, DECISION making, MEDLINE, CONTENT analysis, NEURODEGENERATION
Abstract

Background: Availability of genetic testing in neurodegenerative disorders has developed rapidly. This growing ability is providing specific genetic information to individuals and, in turn, their families, raising ethical concerns. However, family members' perspective is a seldom-studied phenomenon. Aim: The aim of this systematic review was to describe the ethical aspect of genetic testing in neurodegenerative diseases from the perspective of at-risk family members. Method: A systematic review of data was performed in accordance with the PRISMA statement. The data search was conducted using the CINAHL, PubMed and Scopus databases to identify original peer-reviewed studies published between January 2009 and April 2019. A total of 24 articles were selected. The data were analysed using inductive content analysis. Findings: On the basis of the analysis, four central ethical implications were identified: (i) decision-making in genetic testing as a dilemma: balance between autonomy and responsibility, (ii) the individual's right to make a voluntary and informed decision for genetic testing, (iii) conflicting emotions after knowing one's genetic status and (iv) privacy and confidentiality of genetic information: the fear of genetic discrimination and stigma. Conclusions: The findings of this review increase understanding about the central ethical implications of genetic testing in neurodegenerative diseases from the perspective of family members, and identify and underline outstanding needs for further research. [ABSTRACT FROM AUTHOR]

Published
2021
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31. Alternative genomic diagnoses for individuals with a clinical diagnosis of Dubowitz syndrome.

Author

Dyment, David A., O'Donnell‐Luria, Anne, Agrawal, Pankaj B., Coban Akdemir, Zeynep, Aleck, Kyrieckos A., Antaki, Danny, Al Sharhan, Hind, Au, Ping‐Yee B., Aydin, Hatip, Beggs, Alan H., Bilguvar, Kaya, Boerwinkle, Eric, Brand, Harrison, Brownstein, Catherine A., Buyske, Steve, Chodirker, Bernard, Choi, Jungmin, Chudley, Albert E., Clericuzio, Carol L., and Cox, Gerald F.

Abstract

Dubowitz syndrome (DubS) is considered a recognizable syndrome characterized by a distinctive facial appearance and deficits in growth and development. There have been over 200 individuals reported with Dubowitz or a "Dubowitz‐like" condition, although no single gene has been implicated as responsible for its cause. We have performed exome (ES) or genome sequencing (GS) for 31 individuals clinically diagnosed with DubS. After genome‐wide sequencing, rare variant filtering and computational and Mendelian genomic analyses, a presumptive molecular diagnosis was made in 13/27 (48%) families. The molecular diagnoses included biallelic variants in SKIV2L, SLC35C1, BRCA1, NSUN2; de novo variants in ARID1B, ARID1A, CREBBP, POGZ, TAF1, HDAC8, and copy‐number variation at1p36.11(ARID1A), 8q22.2(VPS13B), Xp22, and Xq13(HDAC8). Variants of unknown significance in known disease genes, and also in genes of uncertain significance, were observed in 7/27 (26%) additional families. Only one gene, HDAC8, could explain the phenotype in more than one family (N = 2). All but two of the genomic diagnoses were for genes discovered, or for conditions recognized, since the introduction of next‐generation sequencing. Overall, the DubS‐like clinical phenotype is associated with extensive locus heterogeneity and the molecular diagnoses made are for emerging clinical conditions sharing characteristic features that overlap the DubS phenotype. [ABSTRACT FROM AUTHOR]

Published
2021
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32. Recessive MYH3 variants cause "Contractures, pterygia, and variable skeletal fusions syndrome 1B" mimicking Escobar variant multiple pterygium syndrome.

Author

Hakonen, Anna H., Lehtonen, Johanna, Kivirikko, Sirpa, Keski‐Filppula, Riikka, Moilanen, Jukka, Kivisaari, Reetta, Almusa, Henrikki, Jakkula, Eveliina, Saarela, Janna, Avela, Kristiina, and Aittomäki, Kristiina

Abstract

The multiple pterygium syndromes (MPS) are rare disorders with disease severity ranging from lethal to milder forms. The nonlethal Escobar variant MPS (EVMPS) is characterized by multiple pterygia and arthrogryposis, as well as various additional features including congenital anomalies. The genetic etiology of EVMPS is heterogeneous and the diagnosis has been based either on the detection of pathogenic CHRNG variants (~23% of patients), or suggestive clinical features. We describe four patients with a clinical suspicion of EVMPS who manifested with multiple pterygia, mild flexion contractures of several joints, and vertebral anomalies. We revealed recessively inherited MYH3 variants as the underlying cause in all patients: two novel variants, c.1053C>G, p.(Tyr351Ter) and c.3102+5G>C, as compound heterozygous with the hypomorphic MYH3 variant c.‐9+1G>A. Recessive MYH3 variants have been previously associated with spondylocarpotarsal synostosis syndrome. Our findings now highlight multiple pterygia as an important feature in patients with recessive MYH3 variants. Based on all patients with recessive MYH3 variants reported up to date, we consider that this disease entity should be designated as "Contractures, pterygia, and variable skeletal fusions syndrome 1B," as recently suggested by OMIM. Our findings underline the importance of analyzing MYH3 in the differential diagnosis of EVMPS, particularly as the hypomorphic MYH3 variant might remain undetected by routine exome sequencing. [ABSTRACT FROM AUTHOR]

Published
2020
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34. HOLDEN AWARDS VANNAS MEDAL.

Subjects
SCHOLARSHIPS, EYE care
Abstract

The article reports on the inaugural Vannas Fellowship for research in international eye care excellence awarded to scientist and ophthalmologist Jukka Moilanen in Helsinki, Finland. It mentions that the fellowship medal and $20,000 prize was awarded by Scientia Professor Brien Holden of the Institute for Eye Research Sydney.

Published
2006

35. Reduced Cancer Incidence in Huntington’s Disease: Analysis in the Registry Study.

Author

McNulty, Paul, Pilcher, Richard, Ramesh, Raviram, Necuiniate, Renata, Hughes, Alis, REGISTRY Investigators of the European Huntington's Disease Network, Bonelli, Raphael M., Hecht, Karen, Herranhof, Brigitte, Holl, Anna, Kapfhammer, Hans-Peter, Koppitz, Michael, Lilek, Sabine, Magnet, Markus, Müller, Nicole, Otti, Daniela, Painold, Annamaria, Reisinger, Karin, Scheibl, Monika, and Schöggl, Helmut

Subjects
HUNTINGTON disease, CANCER diagnosis, AGE of onset, TRINUCLEOTIDE repeats, DISEASE incidence, NEURODEGENERATION
Abstract

Background: People with Huntington’s disease (HD) have been observed to have lower rates of cancers. Objective: To investigate the relationship between age of onset of HD, CAG repeat length, and cancer diagnosis. Methods: Data were obtained from the European Huntington’s disease network REGISTRY study for 6540 subjects. Population cancer incidence was ascertained from the GLOBOCAN database to obtain standardised incidence ratios of cancers in the REGISTRY subjects. Results: 173/6528 HD REGISTRY subjects had had a cancer diagnosis. The age-standardised incidence rate of all cancers in the REGISTRY HD population was 0.26 (CI 0.22–0.30). Individual cancers showed a lower age-standardised incidence rate compared with the control population with prostate and colorectal cancers showing the lowest rates. There was no effect of CAG length on the likelihood of cancer, but a cancer diagnosis within the last year was associated with a greatly increased rate of HD onset (Hazard Ratio 18.94, p < 0.001). Conclusions: Cancer is less common than expected in the HD population, confirming previous reports. However, this does not appear to be related to CAG length in HTT. A recent diagnosis of cancer increases the risk of HD onset at any age, likely due to increased investigation following a cancer diagnosis. [ABSTRACT FROM AUTHOR]

Published
2018
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36. Does arterial hypertension influence the onset of Huntington's disease?

Author

Valcárcel-Ocete, Leire, Fullaondo, Asier, Alkorta-Aranburu, Gorka, García-Barcina, María, Roos, Raymund A. C., Hjermind, Lena E., Saft, Carsten, Frontali, Marina, Reilmann, Ralf, Rickards, Hugh, null, null, Zubiaga, Ana M., and Aguirre, Ana

Subjects
HUNTINGTON disease, HUNTINGTIN protein, NEURODEGENERATION, REGRESSION analysis, ANALYSIS of variance
Abstract

Huntington’s disease (HD) age of onset (AO) is mainly determined by the length of the CAG repeat expansion in the huntingtin gene. The remaining AO variability has been attributed to other little-known factors. A factor that has been associated with other neurodegenerative diseases is arterial hypertension (AHT). The aim of this study is to evaluate the contribution of AHT to the AO of HD. We used data from a cohort of 630 European HD patients with adult onset collected by the REGISTRY project of the European Huntington’s Disease Network. Multiple linear regression and ANOVA, controlling for the CAG repeat number of the expanded allele (CAGexp) of each patient, were performed to assess the association between the AHT condition and the AO of the motor symptoms (mAO). The results showed a significant association between AHT and mAO, especially when we only considered the patients diagnosed with AHT prior to manifesting any HD signs (pre-HD AHT). Remarkably, despite the low number of cases, those patients developed motor symptoms 5–8 years later than normotensive patients in the most frequent CAGexp range (40–44). AHT is an age-related condition and consequently, the age of the patient at the time of data collection could be a confounder variable. However, given that most pre-HD AHT patients included in our study had started treatment with antihypertensive drugs prior to the onset of HD, and that antihypertensive drugs have been suggested to confer a neuroprotective effect in other neurodegenerative diseases, raises the interest in elucidating the impact of AHT and/or AHT treatment in HD age of onset in further studies. A confirmation of our results in a larger sample set would open the possibility to significantly improve HD management. [ABSTRACT FROM AUTHOR]

Published
2018
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37. New Eye Diseases and Conditions Study Findings Recently Were Published by a Researcher at University of Helsinki and Helsinki University Hospital (Does Corneal Topography Using 3-Dimensional Optical Coherence Tomography Suggest Different...).

Subjects
OPTICAL coherence tomography, CORNEAL topography, RESEARCH personnel, UNIVERSITY hospitals, EYE diseases
Abstract

A recent study conducted by researchers at the University of Helsinki and Helsinki University Hospital in Finland analyzed corneal topography in patients with Terrien marginal degeneration using 3-dimensional optical coherence tomography. The study classified the topographic axial power maps into four patterns: crab claw, mixed, arcuate, and normal. The researchers found that patients with the crab claw pattern were younger and progressed more rapidly, while those with the mixed pattern were older and progressed slower. The study suggests that there may be different subtypes of Terrien marginal degeneration and that patients with certain patterns may benefit from more frequent monitoring. [Extracted from the article]

Published
2023

38. Topical levofloxacin, nepafenac and prednisolone acetate medication after cataract surgery in the biggest tertiary eye hospital in Finland during 2015–2018.

Author

Loukovaara, Sirpa, Lehtinen, Ville, Nieminen, Risto, and Moilanen, Jukka

Subjects
CATARACT surgery, PHACOEMULSIFICATION, DRUGS, EYE, ACETATES, NONSTEROIDAL anti-inflammatory agents
Abstract

The article offers information on the best topical treatment practice after cataract surgery (CS); and mentions that nonsteroidal antiinflammatory drugs (NSAIDs) such as ketorolac, nepafenac, diclofenac and bromfenac can be used to treat the postoperative anterior chamber inflammation after CS combined to corticosteroids or as monotherapy.

Published
2019
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40. Novel compound heterozygous mutation in SACS gene leads to a milder autosomal recessive spastic ataxia of Charlevoix-Saguenay, ARSACS, in a Finnish family.

Author

Palmio, Johanna, Kärppä, Mikko, Baumann, Peter, Penttilä, Sini, Moilanen, Jukka, and Udd, Bjarne

Subjects
GENETIC mutation, ATAXIA, SPASTICITY, CEREBELLAR ataxia, TREATMENT of peripheral neuropathy, PYRAMIDAL tract, TREATMENT of neurodegeneration, THERAPEUTICS
Abstract

Key Clinical Message Autosomal recessive spastic ataxia of Charlevoix-Saguenay is a rare disorder outside Quebec causing childhood-onset cerebellar ataxia, peripheral neuropathy, and pyramidal tract signs. A Finnish family with milder form of ARSACS was found to harbor three mutations, p.E1100K, p.N1489S, and p.M1359T, in SACS gene. The mutations segregated with the disease. [ABSTRACT FROM AUTHOR]

Published
2016
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41. Genetic aetiology of ophthalmological manifestations in children - a focus on mitochondrial disease-related symptoms.

Author

Widgren, Paula, Hurme, Anri, Falck, Aura, Keski ‐ Filppula, Riikka, Remes, Anne M, Moilanen, Jukka, Majamaa, Kari, Kervinen, Marko, and Uusimaa, Johanna

Subjects
MITOCHONDRIAL DNA abnormalities, MITOCHONDRIAL pathology, NYSTAGMUS, NEUROPATHY, CHILDREN'S health
Abstract

Purpose To investigate the association of mutations in the mitochondrial DNA (mt DNA) or nuclear candidate genes with mitochondrial disease-related ophthalmic manifestations (nystagmus, ptosis, ophthalmoplegia, optic neuropathy and retinopathy) in children. Methods A retrospective cohort of children ( n = 98) was identified from the medical record files of a tertiary care hospital. The entire mt DNA and nuclear genes POLG1, OPA1 and PEO1 were analysed from the available DNA samples ( n = 38). Furthermore, some nuclear candidate genes were investigated based on family history and phenotype. Rare mt DNA mutations were evaluated using in silico predictors and sequence alignment. Results Three patients had previously identified mutations in mt DNA that are associated with optic neuropathy (in MT- ND6 and MT- ND1) and nystagmus (in tRNA Arg). Nine rare mutations in MT- ATP6 were identified in seven patients, of whom four manifested with retinopathy and three had clusters of MT- ATP6 mutations. Nuclear PEO1 and OPA1 were unchanged in all samples, but a patient with nystagmus had a heterozygous POLG1 mutation. The analysis of nuclear candidate genes revealed mutations in NDUF8 (patient with nystagmus), TULP1 (patient with optic neuropathy, nystagmus and retinopathy) and RP2 (patient with retinopathy) genes. Conclusions Children with retinopathy, nystagmus or optic neuropathy, especially together with developmental delay or positive family history, should be considered for mitochondrial disease. MT- ATP6 should be taken into account for children with retinopathy of unknown aetiology. [ABSTRACT FROM AUTHOR]

Published
2016
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43. Rare Copy Number Variants Observed in Hereditary Breast Cancer Cases Disrupt Genes in Estrogen Signaling and TP53 Tumor Suppression Network.

Author

Pylkäs, Katri, Vuorela, Mikko, Otsukka, Meeri, Kallioniemi, Anne, Jukkola-Vuorinen, Arja, and Winqvist, Robert

Subjects
BREAST cancer, CANCER in women, DEVELOPED countries, GENETICS, CANCER patients
Abstract

Breast cancer is the most common cancer in women in developed countries, and the contribution of genetic susceptibility to breast cancer development has been well-recognized. However, a great proportion of these hereditary predisposing factors still remain unidentified. To examine the contribution of rare copy number variants (CNVs) in breast cancer predisposition, high-resolution genome-wide scans were performed on genomic DNA of 103 BRCA1, BRCA2, and PALB2 mutation negative familial breast cancer cases and 128 geographically matched healthy female controls; for replication an independent cohort of 75 similarly mutation negative young breast cancer patients was used. All observed rare variants were confirmed by independent methods. The studied breast cancer cases showed a consistent increase in the frequency of rare CNVs when compared to controls. Furthermore, the biological networks of the disrupted genes differed between the two groups. In familial cases the observed mutations disrupted genes, which were significantly overrepresented in cellular functions related to maintenance of genomic integrity, including DNA double-strand break repair (P = 0.0211). Biological network analysis in the two independent breast cancer cohorts showed that the disrupted genes were closely related to estrogen signaling and TP53 centered tumor suppressor network. These results suggest that rare CNVs represent an alternative source of genetic variation influencing hereditary risk for breast cancer. [ABSTRACT FROM AUTHOR]

Published
2012
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44. Exome sequencing in routine diagnostics: a generic test for 254 patients with primary immunodeficiencies.

Author

Arts, Peer, Simons, Annet, AlZahrani, Mofareh S., Yilmaz, Elanur, AlIdrissi, Eman, van Aerde, Koen J., Alenezi, Njood, AlGhamdi, Hamza A., AlJubab, Hadeel A., Al-Hussaini, Abdulrahman A., AlManjomi, Fahad, Alsaad, Alaa B., Alsaleem, Badr, Andijani, Abdulrahman A., Asery, Ali, Ballourah, Walid, Bleeker-Rovers, Chantal P., van Deuren, Marcel, van der Flier, Michiel, and Gerkes, Erica H.

Subjects
HUMAN chromosome abnormality diagnosis, GENETIC testing, MYCOSES, CELL populations, THERAPEUTICS, MUCORMYCOSIS
Abstract

Background: Diagnosis of primary immunodeficiencies (PIDs) is complex and cumbersome yet important for the clinical management of the disease. Exome sequencing may provide a genetic diagnosis in a significant number of patients in a single genetic test. Methods: In May 2013, we implemented exome sequencing in routine diagnostics for patients suffering from PIDs. This study reports the clinical utility and diagnostic yield for a heterogeneous group of 254 consecutively referred PID patients from 249 families. For the majority of patients, the clinical diagnosis was based on clinical criteria including rare and/or unusual severe bacterial, viral, or fungal infections, sometimes accompanied by autoimmune manifestations. Functional immune defects were interpreted in the context of aberrant immune cell populations, aberrant antibody levels, or combinations of these factors. Results: For 62 patients (24%), exome sequencing identified pathogenic variants in well-established PID genes. An exome-wide analysis diagnosed 10 additional patients (4%), providing diagnoses for 72 patients (28%) from 68 families altogether. The genetic diagnosis directly indicated novel treatment options for 25 patients that received a diagnosis (34%). Conclusion: Exome sequencing as a first-tier test for PIDs granted a diagnosis for 28% of patients. Importantly, molecularly defined diagnoses indicated altered therapeutic options in 34% of cases. In addition, exome sequencing harbors advantages over gene panels as a truly generic test for all genetic diseases, including in silico extension of existing gene lists and re-analysis of existing data. [ABSTRACT FROM AUTHOR]

Published
2019
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45. Holden awards Vannas medal

Subjects
Ophthalmologists -- Achievements and awards, Business, Health care industry, Business, international
Abstract

Finnish scientist and ophthalmologist Jukka Moilanen (left) was recently awarded the inaugural Vannas Fellowship for research in international eye care excellence in Helsinki. The fellowship medal and $20,000 prize was [...]

Published
2006

46. Acute Myeloid Leukemia: Diagnosis, Prognosis, Treatment and Outcomes

Author

Rina Kansal and Rina Kansal

Subjects
Acute myeloid leukemia, Acute myeloid leukemia--Diagnosis, Acute myeloid leukemia--Treatment
Abstract

This book is written by multidisciplinary specialists who diagnose and treat acute myeloid leukemia (AML) patients and is meant for anyone interested in the clinical care of patients with hematologic malignancies, including students and trainees. The 21 contributors for this book include expert clinicians in leukemia and hematologic malignancies, infectious diseases, pharmacological drug administration, pathology, cytogenetics, molecular genetics, and artificial intelligence, and one medical student and advanced trainees. The book comprises nine chapters, starting with a comprehensive overview of the global epidemiology, etiology, prognosis, treatment, and outcomes in patients with AML. Chapter 2 describes the classification of myeloid neoplasms, including AML, with a historical perspective and current diagnostic criteria. This chapter describes the fifth edition of the World Health Organization (WHO) classification and the updates from the revised fourth edition of the WHO classification. It compares the similarities and differences from the International Consensus Classification. Chapter 3 is focused on genetic evaluation in AML, emphasizing cytogenetic techniques, with numerous illustrations depicting genetic abnormalities in AML. Chapter 4 discusses measurable residual disease (MRD) in AML and explains the approaches and current guidelines for MRD detection by multiparametric flow cytometry and molecular techniques, emphasizing the pre-analytical, analytical, and post-analytical factors in evaluating MRD, with illustrations for essential concepts. Chapter 5 describes clonal hematopoiesis and its role in the development of myeloid neoplasms. Chapter 6 discusses inherited germline predisposition to myeloid malignancies, including inherited bone marrow failure syndromes and syndromic and non-syndromic predisposition syndromes for hematologic malignancies. Chapter 7 describes and illustrates novel therapeutic agents in AML, including genetically-targeted therapies, non-genetically targeted therapies, and immunotherapies. Chapter 8 covers the management of infectious complications in patients with AML, and Chapter 9 introduces the reader, with many illustrations, to the emerging applications of artificial intelligence in diagnostic hematopathology.

Published
2024

47. Genome Finland: From Rare Diseases to Data Economy

Author

Ilpo Helén, Karoliina Snell, Heta Tarkkala, Aaro Tupasela, Ilpo Helén, Karoliina Snell, Heta Tarkkala, and Aaro Tupasela

Subjects
Genomes, Medical genetics--Finland
Abstract

Genome Finland tells a story of genomic medicine in Finland from the study of rare Finnish diseases in the 1960s and 1970s to the implementation of personalized medicine in the 2020s. The main focus is on the 21st century - the period after the Human Genome Project - and on the establishment of new infrastructures to support genomic medicine, such as biobanks. The book opens up the reasoning and discussions as well as the settings and events through which Finnish medical genetics reached the top level of international biomedicine in the late 1990s, biobanks and biobank research evolved during the 2000s and 2010s, and large transnational public-private partnership projects utilising massive amounts of genome and patient data started to dominate also Finnish research into the 2020s. In particular, Genome Finland examines and exposes the connections between biomedical science,'knowledge-based'economy and business, and innovation policy in Finland during the past decades.

Published
2024

48. Immediately Sequential Bilateral Cataract Surgery (ISBCS) : Global History and Methodology

Author

Steve A. Arshinoff, Charles Claoue, Bjorn Johansson, David Perez-Silguero, Susan Ruyu Qi, Mike Yuan Chen, Melanie Hebert, Steve A. Arshinoff, Charles Claoue, Bjorn Johansson, David Perez-Silguero, Susan Ruyu Qi, Mike Yuan Chen, and Melanie Hebert

Subjects
Cataract--Surgery
Abstract

Immediately Sequential Bilateral Cataract Surgery (ISBCS): Global History and Methodology is a comprehensive guide for the safe and efficient performance of ISBCS. It provides an overview of the history, recommended protocols, necessary precautions, exclusion criteria, benefits and risks associated with this procedure, organizational standards, and more. Written by the most prominent ISBCS surgeons in the world, chapters recount the arguments for and against bilateral surgery that have been made throughout the ages, up to the present, and deliver achieved and proposed resolutions to all problems discussed. Topics such as ethics and medico-legal issues surrounding ISBCS are also discussed, and a chapter on the global evolution of bilateral cataract surgery provides readers with a complete overview of the development of ISBCS practices in countries from all continents. - Provides a comprehensive history and current status of ISBCS globally - Provides step-by-step recommendations and precautions necessary to perform ISBCS safely, including detailed discussion of surgical infection prophylaxis with antibiotics delivered into the eye at surgery - Reviews and explains the patient benefits associated with ISBCS - Covers development of ISBCS practices worldwide

Published
2023

49. New Movements in Academic Entrepreneurship

Author

Päivi Eriksson, Ulla Hytti, Katri Komulainen, Tero Montonen, Päivi Siivonen, Päivi Eriksson, Ulla Hytti, Katri Komulainen, Tero Montonen, and Päivi Siivonen

Subjects
University-based new business enterprises, Entrepreneurship
Abstract

Focusing on academic entrepreneurship in the university context, the authors explore how researchers, teachers, students, academic managers and administrators make sense of entrepreneurship and of the paradoxes and contradictions involved. The book investigates how these diverse entrepreneurial actors and their stakeholders interpret and analyse entrepreneurial activities within the university ecosystem.New Movements in Academic Entrepreneurship covers research commercialisation, academic start-up companies and entrepreneurship education, as well as university-society relationships more widely. With contributions from Europe, North America and Asia, this book helps to broaden our understanding of academic entrepreneurship using original theoretical insights and rich empirical data.Essential reading for students and researchers of entrepreneurial universities and ecosystems, this book provides fresh theoretical frameworks and an inclusive understanding of academic entrepreneurship.

Published
2021

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