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1. iSeeNumbers project report:main findings and recommendations for practice

Author

Mononen, R. (Riikka), Korhonen, J. (Johan), Niemivirta, M. (Markku), Rawling, A. M. (Anna Maria), Tapola, A. (Anna), Tuominen, H. (Heta), Mononen, R. (Riikka), Korhonen, J. (Johan), Niemivirta, M. (Markku), Rawling, A. M. (Anna Maria), Tapola, A. (Anna), and Tuominen, H. (Heta)

Abstract

This report gives an overview of the main findings from the iSeeNumbers project, (Eye) Tracking individual differences in numeracy development. Interplay between skills, motivation and well-being (2018–2022), and some recommendations that could be considered in early grades mathematics teaching.

Published
2023

2. Achievement emotions and arithmetic fluency:development and parallel processes during the early school years

Author

Rawlings, A. M. (Anna Maria), Niemivirta, M. (Markku), Korhonen, J. (Johan), Lindskog, M. (Marcus), Tuominen, H. (Heta), Mononen, R. (Riikka), Rawlings, A. M. (Anna Maria), Niemivirta, M. (Markku), Korhonen, J. (Johan), Lindskog, M. (Marcus), Tuominen, H. (Heta), and Mononen, R. (Riikka)

Abstract

This study investigated the developmental trajectories and interrelationships of mathematics-related achievement emotions and arithmetic fluency from first to third grade, and the effects of these on third grade mathematics performance. Participants were 232 Norwegian students. Students’ emotions and arithmetic fluency were measured four times and mathematics performance once. Applying latent growth curve modeling, developmental patterns of decreasing enjoyment and increasing boredom were observed over time. The mean level of enjoyment remained fairly high, and of both boredom and anxiety quite low. Individual differences were observed in both the initial levels and development of all emotions and arithmetic fluency, indicating differences in developmental trajectories. Only the initial levels and rate of change in arithmetic fluency predicted mathematics performance at the third grade.

Published
2023

3. Novel human lymph node-derived matrix supports the adhesion of metastatic oral carcinoma cells

Author

Naakka, E. (Erika), Wahbi, W. (Wafa), Tiikkaja, R. (Riia), Juurikka, K. (Krista), Sandvik, T. (Toni), Koivunen, P. (Petri), Autio, T. (Timo), Tikanto, J. (Jukka), Väisänen, J. (Janne), Tuominen, H. (Hannu), Talvensaari-Mattila, A. (Anne), Al-Samadi, A. (Ahmed), Soliymani, R. (Rabah), Åström, P. (Pirjo), Risteli, M. (Maija), Salo, T. (Tuula), Naakka, E. (Erika), Wahbi, W. (Wafa), Tiikkaja, R. (Riia), Juurikka, K. (Krista), Sandvik, T. (Toni), Koivunen, P. (Petri), Autio, T. (Timo), Tikanto, J. (Jukka), Väisänen, J. (Janne), Tuominen, H. (Hannu), Talvensaari-Mattila, A. (Anne), Al-Samadi, A. (Ahmed), Soliymani, R. (Rabah), Åström, P. (Pirjo), Risteli, M. (Maija), and Salo, T. (Tuula)

Abstract

Background: 3D culture is increasingly used in cancer research, as it allows the growth of cells in an environment that mimics in vivo conditions. Metastases are the primary cause of morbidity and mortality in cancer patients, and solid tumour metastases are mostly located in lymph nodes. Currently, there are no techniques that model the pre-metastatic lymph node microenvironment in vitro. In this study, we prepared a novel extracellular matrix, Lymphogel, which is derived from lymph nodes, mimicking the tumour microenvironment (TME) of metastatic carcinoma cells. We tested the suitability of the new matrix in various functional experiments and compared the results with those obtained using existing matrices. Methods: We used both commercial and patient-derived primary and metastatic oral tongue squamous cell carcinoma (OTSCC) cell lines. We characterized the functional differences of these cells using three different matrices (human uterine leiomyoma-derived Myogel, human pre-metastatic neck lymph node-derived Lymphogel (h-LG), porcine normal neck lymph node-derived Lymphogel (p-LG) in proliferation, adhesion, migration and invasion assays. We also performed proteomic analyses to compare the different matrices in relation to their functional properties. Results: OTSCC cells exhibited different adhesion and invasion patterns depending on the matrix. Metastatic cell lines showed improved ability to adhere to h-LG, but the effects of the matrices on cell invasion fluctuated non-significantly between the cell lines. Proteomic analyses showed that the protein composition between matrices was highly variable; Myogel contained 618, p-LG 1823 and h-LG 1520 different proteins. The comparison of all three matrices revealed only 120 common proteins. Analysis of cellular pathways and processes associated with proteomes of each matrix revealed similarities of Myogel with h-LG but less with p-LG. Similarly, p-LG contained the least adhesion-related proteins compared wit

Published
2023

4. Novel patients with NHLRC2 variants expand the phenotypic spectrum of FINCA disease

Author

Tallgren, A. (Antti), Kager, L. (Leo), O’Grady, G. (Gina), Tuominen, H. (Hannu), Körkkö, J. (Jarmo), Kuismin, O. (Outi), Feucht, M. (Martha), Wilson, C. (Callum), Behunova, J. (Jana), England, E. (Eleina), Kurki, M. I. (Mitja I.), Palotie, A. (Aarno), Hallman, M. (Mikko), Kaarteenaho, R. (Riitta), Laccone, F. (Franco), Boztug, K. (Kaan), Hinttala, R. (Reetta), Uusimaa, J. (Johanna), Tallgren, A. (Antti), Kager, L. (Leo), O’Grady, G. (Gina), Tuominen, H. (Hannu), Körkkö, J. (Jarmo), Kuismin, O. (Outi), Feucht, M. (Martha), Wilson, C. (Callum), Behunova, J. (Jana), England, E. (Eleina), Kurki, M. I. (Mitja I.), Palotie, A. (Aarno), Hallman, M. (Mikko), Kaarteenaho, R. (Riitta), Laccone, F. (Franco), Boztug, K. (Kaan), Hinttala, R. (Reetta), and Uusimaa, J. (Johanna)

Abstract

Purpose: FINCA disease (Fibrosis, Neurodegeneration and Cerebral Angiomatosis, OMIM 618278) is an infantile-onset neurodevelopmental and multiorgan disease. Since our initial report in 2018, additional patients have been described. FINCA is the first human disease caused by recessive variants in the highly conserved NHLRC2 gene. Our previous studies have shown that Nhlrc2-null mouse embryos die during gastrulation, indicating the essential role of the protein in embryonic development. Defect in NHLRC2 leads to cerebral neurodegeneration and severe pulmonary, hepatic and cardiac fibrosis. Despite having a structure suggestive of an enzymatic role and the clinical importance of NHLRC2 in multiple organs, the specific physiological role of the protein is unknown. Methods: The clinical histories of five novel FINCA patients diagnosed with whole exome sequencing were reviewed. Segregation analysis of the biallelic, potentially pathogenic NHLRC2 variants was performed using Sanger sequencing. Studies on neuropathology and NHLRC2 expression in different brain regions were performed on autopsy samples of three previously described deceased FINCA patients. Results: One patient was homozygous for the pathogenic variant c.442G > T, while the other four were compound heterozygous for this variant and two other pathogenic NHLRC2 gene variants. All five patients presented with multiorgan dysfunction with neurodevelopmental delay, recurrent infections and macrocytic anemia as key features. Interstitial lung disease was pronounced in infancy but often stabilized. Autopsy samples revealed widespread, albeit at a lower intensity than the control, NHLRC2 expression in the brain. Conclusion: This report expands on the characteristic clinical features of FINCA disease. Presentation is typically in infancy, and although patients can live to late adulthood, the key clinical and histopathological features are fibrosis, infection susceptibility/immunodeficiency/intellectual disa

Published
2023

5. PIN3 regulates the weight-induced radial growth in plants

Author

Carrió-Seguí, A, Brunot-Garau, P, Miskolczi, P, Vera-Sirera, Francisco, Tuominen, H, Agusti, J., Carrió-Seguí, A, Brunot-Garau, P, Miskolczi, P, Vera-Sirera, Francisco, Tuominen, H, and Agusti, J.

Published
2023

6. Spinal cord injury during selective cerebral perfusion and segmental artery occlusion:an experimental study

Author

Honkanen, H.-P. (Hannu-Pekka), Mustonen, C. (Caius), Tuominen, H. (Hannu), Kiviluoma, K. (Kai), Anttila, V. (Vesa), Juvonen, T. (Tatu), Honkanen, H.-P. (Hannu-Pekka), Mustonen, C. (Caius), Tuominen, H. (Hannu), Kiviluoma, K. (Kai), Anttila, V. (Vesa), and Juvonen, T. (Tatu)

Abstract

Objectives: Since selective cerebral perfusion (SCP) has been used in aortic arch surgical procedures, the core temperature during lower body circulatory arrest (LBCA) has been steadily rising. Simultaneously, the use of a frozen elephant trunk (FET) graft has been increasing. The safe period of LBCA in relation to spinal cord ischaemic tolerance in combination with segmental artery occlusion by the FET procedure has not been defined. Methods: Sixteen pigs were assigned to undergo 65 (n = 10) or 90 min (n = 6) of SCP at 28°C with LBCA in combination with occlusion of the 8 uppermost segmental arteries in the thoracic (Th) aorta (15–20 cm FET, Th8-level). The follow-up period consisted of a 6-h intensive period and a 5-day observation period. Near-infrared spectroscopy of the collateral network was used to determine spinal cord oxygenation. The neurological status of the patients was evaluated daily, and the brain and the spinal cord were harvested for a histopathological analysis. Results: Five out of 6 pigs after 90 min and 1 out of 10 pigs after 65 min of LBCA died within 48 h of multiorgan failure. Of the survivors in the 65-min group, 6 out of 9 had paraparesis/paraplegia; the remaining 3 reached normal function. The lone survivor after 90 min of LBCA was paraplegic. Nadir near-infrared spectroscopy of the collateral network values at Th8 and Th10 were 34 (±5) and 39 (±4), and they were reached within 35 min of SCP in both groups. Conclusions: An extended FET graft with LBCA and SCP durations >65 min at 28°C results in a poor outcome.

Published
2022

7. Regulation of PaRBOH1-mediated ROS production in Norway spruce by Ca²⁺ binding and phosphorylation

Author

Nickolov, K. (Kaloian), Gauthier, A. (Adrien), Hashimoto, K. (Kenji), Laitinen, T. (Teresa), Väisänen, E. (Enni), Paasela, T. (Tanja), Soliymani, R. (Rabah), Kurusu, T. (Takamitsu), Himanen, K. (Kristiina), Blokhina, O. (Olga), Fagerstedt, K. V. (Kurt V.), Jokipii-Lukkari, S. (Soile), Tuominen, H. (Hannele), Häggman, H. (Hely), Wingsle, G. (Gunnar), Teeri, T. H. (Teemu H.), Kuchitsu, K. (Kazuyuki), Kärkönen, A. (Anna), Nickolov, K. (Kaloian), Gauthier, A. (Adrien), Hashimoto, K. (Kenji), Laitinen, T. (Teresa), Väisänen, E. (Enni), Paasela, T. (Tanja), Soliymani, R. (Rabah), Kurusu, T. (Takamitsu), Himanen, K. (Kristiina), Blokhina, O. (Olga), Fagerstedt, K. V. (Kurt V.), Jokipii-Lukkari, S. (Soile), Tuominen, H. (Hannele), Häggman, H. (Hely), Wingsle, G. (Gunnar), Teeri, T. H. (Teemu H.), Kuchitsu, K. (Kazuyuki), and Kärkönen, A. (Anna)

Abstract

Plant respiratory burst oxidase homologs (RBOHs) are plasma membrane-localized NADPH oxidases that generate superoxide anion radicals, which then dismutate to H₂O₂, into the apoplast using cytoplasmic NADPH as an electron donor. PaRBOH1 is the most highly expressed RBOH gene in developing xylem as well as in a lignin-forming cell culture of Norway spruce (Picea abies L. Karst.). Since no previous information about regulation of gymnosperm RBOHs exist, our aim was to resolve how PaRBOH1 is regulated with a focus on phosphorylation. The N-terminal part of PaRBOH1 was found to contain several putative phosphorylation sites and a four-times repeated motif with similarities to the Botrytis-induced kinase 1 target site in Arabidopsis AtRBOHD. Phosphorylation was indicated for six of the sites in in vitro kinase assays using 15 amino-acid-long peptides for each of the predicted phosphotarget site in the presence of protein extracts of developing xylem. Serine and threonine residues showing positive response in the peptide assays were individually mutated to alanine (kinase-inactive) or to aspartate (phosphomimic), and the wild type PaRBOH1 and the mutated constructs transfected to human kidney embryogenic (HEK293T) cells with a low endogenous level of extracellular ROS production. ROS-producing assays with HEK cells showed that Ca²⁺ and phosphorylation synergistically activate the enzyme and identified several serine and threonine residues that are likely to be phosphorylated including a novel phosphorylation site not characterized in other plant species. These were further investigated with a phosphoproteomic study. Results of Norway spruce, the first gymnosperm species studied in relation to RBOH regulation, show that regulation of RBOH activity is conserved among seed plants.

Published
2022

11. Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction

Author

Kaustio, M. (Meri), Nayebzadeh, N. (Naemeh), Hinttala, R. (Reetta), Tapiainen, T. (Terhi), Åström, P. (Pirjo), Mamia, K. (Katariina), Pernaa, N. (Nora), Lehtonen, J. (Johanna), Glumoff, V. (Virpi), Rahikkala, E. (Elisa), Honkila, M. (Minna), Olsén, P. (Päivi), Hassinen, A. (Antti), Polso, M. (Minttu), Al Sukaiti, N. (Nashat), Al Shekaili, J. (Jalila), Al Kindi, M. (Mahmood), Al Hashmi, N. (Nadia), Almusa, H. (Henrikki), Bulanova, D. (Daria), Haapaniemi, E. (Emma), Chen, P. (Pu), Suo-Palosaari, M. (Maria), Vieira, P. (Päivi), Tuominen, H. (Hannu), Kokkonen, H. (Hannaleena), Al Macki, N. (Nabil), Al Habsi, H. (Huda), Löppönen, T. (Tuija), Rantala, H. (Heikki), Pietiäinen, V. (Vilja), Zhang, S.-Y. (Shen-Ying), Renko, M. (Marjo), Hautala, T. (Timo), Al Farsi, T. (Tariq), Uusimaa, J. (Johanna), Saarela, J. (Janna), Kaustio, M. (Meri), Nayebzadeh, N. (Naemeh), Hinttala, R. (Reetta), Tapiainen, T. (Terhi), Åström, P. (Pirjo), Mamia, K. (Katariina), Pernaa, N. (Nora), Lehtonen, J. (Johanna), Glumoff, V. (Virpi), Rahikkala, E. (Elisa), Honkila, M. (Minna), Olsén, P. (Päivi), Hassinen, A. (Antti), Polso, M. (Minttu), Al Sukaiti, N. (Nashat), Al Shekaili, J. (Jalila), Al Kindi, M. (Mahmood), Al Hashmi, N. (Nadia), Almusa, H. (Henrikki), Bulanova, D. (Daria), Haapaniemi, E. (Emma), Chen, P. (Pu), Suo-Palosaari, M. (Maria), Vieira, P. (Päivi), Tuominen, H. (Hannu), Kokkonen, H. (Hannaleena), Al Macki, N. (Nabil), Al Habsi, H. (Huda), Löppönen, T. (Tuija), Rantala, H. (Heikki), Pietiäinen, V. (Vilja), Zhang, S.-Y. (Shen-Ying), Renko, M. (Marjo), Hautala, T. (Timo), Al Farsi, T. (Tariq), Uusimaa, J. (Johanna), and Saarela, J. (Janna)

Abstract

Background: Homozygous loss of DIAPH1 results in seizures, cortical blindness, and microcephaly syndrome (SCBMS). We studied 5 Finnish and 2 Omani patients with loss of DIAPH1 presenting with SCBMS, mitochondrial dysfunction, and immunodeficiency. Objective: We sought to further characterize phenotypes and disease mechanisms associated with loss of DIAPH1. Methods: Exome sequencing, genotyping and haplotype analysis, B- and T-cell phenotyping, in vitro lymphocyte stimulation assays, analyses of mitochondrial function, immunofluorescence staining for cytoskeletal proteins and mitochondria, and CRISPR-Cas9 DIAPH1 knockout in heathy donor PBMCs were used. Results: Genetic analyses found all Finnish patients homozygous for a rare DIAPH1 splice-variant (NM_005219:c.684+1G>A) enriched in the Finnish population, and Omani patients homozygous for a previously described pathogenic DIAPH1 frameshift-variant (NM_005219:c.2769delT;p.F923fs). In addition to microcephaly, epilepsy, and cortical blindness characteristic to SCBMS, the patients presented with infection susceptibility due to defective lymphocyte maturation and 3 patients developed B-cell lymphoma. Patients’ immunophenotype was characterized by poor lymphocyte activation and proliferation, defective B-cell maturation, and lack of naive T cells. CRISPR-Cas9 knockout of DIAPH1 in PBMCs from healthy donors replicated the T-cell activation defect. Patient-derived peripheral blood T cells exhibited impaired adhesion and inefficient microtubule-organizing center repositioning to the immunologic synapse. The clinical symptoms and laboratory tests also suggested mitochondrial dysfunction. Experiments with immortalized, patient-derived fibroblasts indicated that DIAPH1 affects the amount of complex IV of the mitochondrial respiratory chain. Conclusions: Our data demonstrate that individuals with SCBMS can have combined immune deficiency and implicate defective cytoskeletal organization and mitochondrial dysfunction in

Published
2021

13. 'När män är förtryckta är det tragedi, när kvinnor är förtryckta är det tradition':stilfigurer och stil i Jessica Hallbäcks Girls just wanna have fundamental human rights

Author

Tuominen, H. (Heta)

Abstract

t. Detta arbete behandlar stilfigurer och stil i Jessica Hallbäcks Girls just wanna have fundamental human rights (2018). Syftet med avhandlingen är att beskriva hur stilfigurer används i samband med talspråklig stil för att skapa en tydlig, slående och humoristisk helhet. Syftet är också att förklara effekten stilfigurerna har på texten och hur de stödjer argumenteringen. Metoden som används är kvalitativ och den valdes utifrån behovet av att förklara ett fenomen. Stilfigurerna analyseras med att förklara deras syfte, kontext och effekt. Stilen analyseras med att klassificera olika stildrag som är frekventa. Jag hänvisar till teori i Stilistiken (2015) av Peter Cassirer och Retorik idag (2013) av Jens Elmelund Kjeldsen. Resultatet av arbetet visar att stilfigurer som används frekvent i Hallbäcks bok är hyperbol, ironi och upprepning. Andra stilfigurer som förekommer mindre frekvent är metafor, liknelse, allusion och retoriska fråga. Stilfigurerna används för att underhålla, väcka intresse och för att tydliggöra. Ironi är en stilfigur som också uttrycker samhällskritik. Stilfigurerna fungerar som ethos- och pathosargument. Stilen är vardaglig och präglas av språkbruk på sociala medier. Texten innehåller informella stildrag som ordförlängning, överflödiga skiljetecken och svärande. Stilen har också likadana drag med kåseristil och polemisk och propagandistisk stil. Detta syns i stildrag som upprepningar, överdrifter, ironi, enkla meningar och talspråkligt språk samt i användningen av värdeladdade ord.Tiivistelmä. Tämä lopputyö käsittelee kielikuvien ja tyylin käyttöä Jessica Hallbäckin kirjassa Girls just wanna have fundamental human rights (2018). Tavoitteena on kuvata, miten kielikuvat yhdessä tyylivalintojen kanssa luo selkeän, humoristisen ja vetävän kokonaisuuden. Pyrkimyksenä on myös kuvata kielikuvien vaikutus tekstiin ja argumentointiin. Tutkielmani metodi on kvalitatiivinen, koska tarkoituksena on selventää kielellistä ilmiötä. Kielikuvia analysoidaan selittämällä niiden tarkoitukset, asiayhteydet ja vaikutukset. Tyyliä analysoidaan luokittelemalla toistuvia piirteitä. Viittaan Peter Cassirerin teokseen Stilistiken (2015) ja Jens Elmelund Kjeldsenin teokseen Retorik idag (2013). Työn tulokset osoittavat, että yleisimmät kielikuvat ovat hyperbola, ironia ja toisto. Muita vähemmän yleisiä kielikuvia ovat metafora, vertaus, alluusio ja retorinen kysymys. Kielikuvien käytöllä pyritään viihdyttämään, herättämään mielenkiintoa ja selventämään. Ironialla ilmaistaan myös yhteiskuntakritiikkiä. Kielikuvat tukevat argumentaatiota vetoamalla eetokseen ja paatokseen. Tyyli on epämuodollista ja on saanut vaikutteita sosiaalisen median kielenkäytöstä. Teksti sisältää epämuodollisia piirteitä, kuten sanojen pidentämistä, ylimääräisiä välimerkkejä ja kirosanoja. Tyyli on myös yhteneväinen pakinatyylin sekä poleemisen ja propagandistisen tyylin kanssa. Tämä ilmenee piirteissä, kuten toistossa, liioittelussa, ironiassa ja yksinkertaisten lauseiden sekä arvoväritteisten sanojen käytössä.

Published
2020

14. Medulloblastoma, macrocephaly, and a pathogenic germline PTEN variant:cause or coincidence?

Author

Tolonen, J.-P. (Jussi-Pekka), Hekkala, A. (Anne), Kuismin, O. (Outi), Tuominen, H. (Hannu), Suo-Palosaari, M. (Maria), Tynninen, O. (Olli), and Niinimäki, R. (Riitta)

Subjects
megalencephaly, magnetic resonance imaging, disease susceptibility, medulloblastoma, carcinogenesis
Abstract

Background: Medulloblastomas (MBs) are a heterogeneous group of childhood brain tumors with four consensus subgroups, namely MBSHH, MBWNT, MBGroup 3, and MBGroup 4, representing the second most common type of pediatric brain cancer after high‐grade gliomas. They suffer from a high prevalence of genetic predisposition with up to 20% of MBSHH caused by germline mutations in only six genes. However, the spectrum of germline mutations in MBSHH remains incomplete. Methods: Comprehensive Next‐Generation Sequencing panels of both tumor and patient blood samples were performed as molecular genetic characterization. The panels cover genes that are known to predispose to cancer. Results: Here, we report on a patient with a pathogenic germline PTEN variant resulting in an early stop codon p.(Glu7Argfs*4) (ClinVar ID: 480383). The patient developed macrocephaly and MBSHH, but reached remission with current treatment protocols. Conclusions: We propose that pathogenic PTEN variants may predispose to medulloblastoma, and show that remission was reached with current treatment protocols. The PTEN gene should be included in the genetic testing provided to patients who develop medulloblastoma at an early age. We recommend brain magnetic resonance imaging upon an unexpected acceleration of growth of head circumference for pediatric patients harboring pathogenic germline PTEN variants.

Published
2020

15. Brain tight junction protein expression in sepsis in an autopsy series

Author

Erikson, K. (Kristo), Tuominen, H. (Hannu), Vakkala, M. (Merja), Liisanantti, J. H. (Janne Henrik), Karttunen, T. (Tuomo), Syrjälä, H. (Hannu), Ala-Kokko, T. I. (Tero Ilmari), Erikson, K. (Kristo), Tuominen, H. (Hannu), Vakkala, M. (Merja), Liisanantti, J. H. (Janne Henrik), Karttunen, T. (Tuomo), Syrjälä, H. (Hannu), and Ala-Kokko, T. I. (Tero Ilmari)

Abstract

Background: Neuroinflammation often develops in sepsis along with increasing permeability of the blood-brain barrier (BBB), which leads to septic encephalopathy. The barrier is formed by tight junction structures between the cerebral endothelial cells. We investigated the expression of tight junction proteins related to endothelial permeability in brain autopsy specimens in critically ill patients deceased with sepsis and analyzed the relationship of BBB damage with measures of systemic inflammation and systemic organ dysfunction. Methods: The case series included all (385) adult patients deceased due to sepsis in the years 2007–2015 with available brain specimens taken at autopsy. Specimens were categorized according to anatomical location (cerebrum, cerebellum). The immunohistochemical stainings were performed for occludin, ZO-1, and claudin. Patients were categorized as having BBB damage if there was no expression of occludin in the endothelium of cerebral microvessels. Results: Brain tissue samples were available in 47 autopsies, of which 38% (18/47) had no expression of occludin in the endothelium of cerebral microvessels, 34% (16/47) developed multiple organ failure before death, and 74.5% (35/47) had septic shock. The deceased with BBB damage had higher maximum SOFA scores (16 vs. 14, p = 0.04) and more often had procalcitonin levels above 10 μg/L (56% vs. 28%, p = 0.045) during their ICU stay. BBB damage in the cerebellum was more common in cases with C-reactive protein (CRP) above 100 mg/L as compared with CRP less than 100 (69% vs. 25%, p = 0.025). Conclusions: In fatal sepsis, damaged BBB defined as a loss of cerebral endothelial expression of occludin is related with severe organ dysfunction and systemic inflammation.

Published
2020

16. Variant in NHLRC2 leads to increased hnRNP C2 in developing neurons and the hippocampus of a mouse model of FINCA disease

Author

Hiltunen, A. E. (Anniina E.), Kangas, S. M. (Salla M.), Ohlmeier, S. (Steffen), Pietilä, I. (Ilkka), Hiltunen, J. (Jori), Tanila, H. (Heikki), McKerlie, C. (Colin), Govindan, S. (Subashika), Tuominen, H. (Hannu), Kaarteenaho, R. (Riitta), Hallman, M. (Mikko), Uusimaa, J. (Johanna), Hinttala, R. (Reetta), Hiltunen, A. E. (Anniina E.), Kangas, S. M. (Salla M.), Ohlmeier, S. (Steffen), Pietilä, I. (Ilkka), Hiltunen, J. (Jori), Tanila, H. (Heikki), McKerlie, C. (Colin), Govindan, S. (Subashika), Tuominen, H. (Hannu), Kaarteenaho, R. (Riitta), Hallman, M. (Mikko), Uusimaa, J. (Johanna), and Hinttala, R. (Reetta)

Abstract

Background: FINCA disease is a pediatric cerebropulmonary disease caused by variants in the NHL repeat-containing 2 (NHLRC2) gene. Neurological symptoms are among the first manifestations of FINCA disease, but the consequences of NHLRC2 deficiency in the central nervous system are currently unexplored. Methods: The orthologous mouse gene is essential for development, and its complete loss leads to early embryonic lethality. In the current study, we used CRISPR/Cas9 to generate an Nhlrc2 knockin (KI) mouse line, harboring the FINCA patient missense mutation (c.442G > T, p.Asp148Tyr). A FINCA mouse model, resembling the compound heterozygote genotype of FINCA patients, was obtained by crossing the KI and Nhlrc2 knockout mouse lines. To reveal NHLRC2-interacting proteins in developing neurons, we compared cortical neuronal precursor cells of E13.5 FINCA and wild-type mouse embryos by two-dimensional difference gel electrophoresis. Results: Despite the significant decrease in NHLRC2, the mice did not develop severe early onset multiorgan disease in either sex. We discovered 19 altered proteins in FINCA neuronal precursor cells; several of which are involved in vesicular transport pathways and actin dynamics which have been previously reported in other cell types including human to have an association with dysfunctional NHLRC2. Interestingly, isoform C2 of hnRNP C1/C2 was significantly increased in both developing neurons and the hippocampus of adult female FINCA mice, connecting NHLRC2 dysfunction with accumulation of RNA binding protein. Conclusions: We describe here the first NHLRC2-deficient mouse model to overcome embryonic lethality, enabling further studies on predisposing and causative mechanisms behind FINCA disease. Our novel findings suggest that disrupted RNA metabolism may contribute to the neurodegeneration observed in FINCA patients.

Published
2020

17. Human myoma tissue-based extracellular matrix models for testing the effects of irradiation on the HPV positive cells

Author

Tuominen, H. (Heidi), Al-Samadi, A. (Ahmed), Salo, T. (Tuula), Rautava, J. (Jaana), Tuominen, H. (Heidi), Al-Samadi, A. (Ahmed), Salo, T. (Tuula), and Rautava, J. (Jaana)

Abstract

Background/Objectives: This study was designed to investigate the invasion of human papillomavirus (HPV) positive human cervical carcinoma cell lines in human leiomyoma-based extracellular matrices in vitro, and to test the suitability of the model for studying the irradiation effects on the cancer cell invasion. Methods: HPV positive cervical carcinoma cell lines SiHa and CaSki, and HPV negative squamous cell carcinoma cell line HSC-3 were used. CaSki cells contain around 600 copies of HPV 16 virus in the genome, whereas SiHa have only 1–2 copies per cell. Cells were analyzed using two different human tumor derived extracellular matrix methods (3D myoma disc model, and Myogel Transwell invasion assay). Cultures were irradiated with 4 Gy. Myoma invasion area and the depth of invasion were measured with ImageJ 1.51j8 software. Statistical analyses were performed with SPSS Statistics (IBM SPSS® Statistics 25). Results: All cells invaded through Myogel coated Transwell membranes and within myoma discs. In myoma discs, a difference in the invasion depth (p = 0.0001) but not in invasion area (p = 0.310) between the HPV positive cell lines was seen, since SiHa (less HPV) invaded slightly better than CaSki (more HPV). HSC-3 cells (HPV negative) invaded deepest (p = 0.048) than either of the HPV positive cell line cells. No difference was detected in the invasion area (p = 0.892) between HPV positive and HPV negative cells. The ionized radiation significantly reduced the invasion depth of HSC-3 (p = 0.008), SiHa (p = 0.0001) and CaSki (p = 0.005). No significant effect on the invasion area was detected in any of the cell lines. However, a significant difference was observed between SiHa and CaSki in the reduction of the invasion depth after radiation (p = 0.013) as the reduction was greater with SiHa than CaSki. Conclusions: Both solid and gelatinous human leiomyoma-based extracellular matrix models were suitable platforms to study the invasion of HPV positive cerv

Published
2020

23. High spatial resolution profiling in tree species

Author

Giacomello, Stefania, Delhomme, N., Niittylä, T., Tuominen, H., Street, N. R., Giacomello, Stefania, Delhomme, N., Niittylä, T., Tuominen, H., and Street, N. R.

Abstract

Until recently, the majority of genomics assays have been performed on bulk tissue samples containing multiple cell types. Tissues such as the wood formation zone in trees contain a complex mix of cell types organised in three-dimensional space. Moreover, cells within the wood formation zone represent a continual developmental progression from meristematic cambial initials through to cell death. This spatiotemporal developmental gradient and cell type information are not assayed by bulk samples. New and improved sampling methods coupled to next-generation sequencing assays are enabling the generation of high spatial resolution and single-cell transcriptomics data, offering unprecedented insight into the biology of unique cell types and cell developmental programs.We overview the application of these approaches to the study of wood development, in particular, and highlight challenges associated with the analysis of such data., Export Date: 8 September 2021; Article; Funding details: FR-2017/0009; Funding details: VINNOVA; Funding details: Knut och Alice Wallenbergs Stiftelse; Funding text 1: S.G. is supported by Formas Research Council grant FR-2017/0009. N.R.S. is supported by the Trees and Crop for the Future (TC4F) project. T.N. is supported by the Bio4Energy project. H.T., N.R.S., T.N. and N.D. acknowledge funding support from Vinnova (the Swedish Governmental Agency for Innovation Systems) and KAW (The Knut and Alice Wallenberg Foundation). We thank Juan Inda (Chalmers) and Dr Saeed Omidi (Sophia Genetics) for insightful discussion regarding single-cell computational challenges.; Funding text 2: S.G. is supported by Formas Research Council grant FR-2017/0009. N.R.S. is supported by the Trees and Crop for the Future (TC4F) project. T.N. is supported by the Bio4Energy project. H.T., N.R.S., T.N. and N.D. acknowledge funding support from Vinnova (the Swedish Governmental Agency for Innovation Systems) and KAW(The Knut and AliceWallenberg Foundation). We thank Juan Inda (Chalmers) and Dr Saeed Omidi (Sophia Genetics) for insightful discussion regarding single-cell computational challenges. QC 20210915

Published
2019
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24. Biallelic loss-of-function P4HTM gene variants cause hypotonia, hypoventilation, intellectual disability, dysautonomia, epilepsy, and eye abnormalities (HIDEA syndrome)

Author

Rahikkala, E. (Elisa), Myllykoski, M. (Matti), Hinttala, R. (Reetta), Vieira, P. (Päivi), Nayebzadeh, N. (Naemeh), Weiss, S. (Simone), Plomp, A. S. (Astrid S.), Bittner, R. E. (Reginald E.), Kurki, M. I. (Mitja I.), Kuismin, O. (Outi), Lewis, A. M. (Andrea M.), Väisänen, M.-L. (Marja-Leena), Kokkonen, H. (Hannaleena), Westermann, J. (Jonne), Bernert, G. (Günther), Tuominen, H. (Hannu), Palotie, A. (Aarno), Aaltone, L. (Lauri), Yang, Y. (Yaping), Potocki, L. (Lorraine), Moilanen, J. (Jukka), van Koningsbruggen, S. (Silvana), Wang, X. (Xia), Schmidt, W. M. (Wolfgang M.), Koivunen, P. (Peppi), Uusimaa, J. (Johanna), Rahikkala, E. (Elisa), Myllykoski, M. (Matti), Hinttala, R. (Reetta), Vieira, P. (Päivi), Nayebzadeh, N. (Naemeh), Weiss, S. (Simone), Plomp, A. S. (Astrid S.), Bittner, R. E. (Reginald E.), Kurki, M. I. (Mitja I.), Kuismin, O. (Outi), Lewis, A. M. (Andrea M.), Väisänen, M.-L. (Marja-Leena), Kokkonen, H. (Hannaleena), Westermann, J. (Jonne), Bernert, G. (Günther), Tuominen, H. (Hannu), Palotie, A. (Aarno), Aaltone, L. (Lauri), Yang, Y. (Yaping), Potocki, L. (Lorraine), Moilanen, J. (Jukka), van Koningsbruggen, S. (Silvana), Wang, X. (Xia), Schmidt, W. M. (Wolfgang M.), Koivunen, P. (Peppi), and Uusimaa, J. (Johanna)

Abstract

Purpose: A new syndrome with hypotonia, intellectual disability, and eye abnormalities (HIDEA) was previously described in a large consanguineous family. Linkage analysis identified the recessive disease locus, and genome sequencing yielded three candidate genes with potentially pathogenic biallelic variants: transketolase (TKT), transmembrane prolyl 4-hydroxylase (P4HTM), and ubiquitin specific peptidase 4 (USP4). However, the causative gene remained elusive. Methods: International collaboration and exome sequencing were used to identify new patients with HIDEA and biallelic, potentially pathogenic, P4HTM variants. Segregation analysis was performed using Sanger sequencing. P4H-TM wild-type and variant constructs without the transmembrane region were overexpressed in insect cells and analyzed using sodium dodecyl sulfate–polyacrylamide gel electrophoresis and western blot. Results: Five different homozygous or compound heterozygous pathogenic P4HTM gene variants were identified in six new and six previously published patients presenting with HIDEA. Hypoventilation, obstructive and central sleep apnea, and dysautonomia were identified as novel features associated with the phenotype. Characterization of three of the P4H-TM variants demonstrated yielding insoluble protein products and, thus, loss-of-function. Conclusions: Biallelic loss-of-function P4HTM variants were shown to cause HIDEA syndrome. Our findings enable diagnosis of the condition, and highlight the importance of assessing the need for noninvasive ventilatory support in patients.

Published
2019

25. The role of study engagement in university students' daily experiences:a multilevel test of moderation

Author

Ketonen, E. E. (Elina E.), Malmberg, L.-E. (Lars-Erik), Salmela-Aro, K. (Katariina), Muukkonen, H. (Hanni), Tuominen, H. (Heta), Lonka, K. (Kirsti), Ketonen, E. E. (Elina E.), Malmberg, L.-E. (Lars-Erik), Salmela-Aro, K. (Katariina), Muukkonen, H. (Hanni), Tuominen, H. (Heta), and Lonka, K. (Kirsti)

Abstract

The present study investigated the dynamic nature of students’ daily experiences and general study engagement using intra-individual assessment. More specifically, we examined individual differences in the relationship between university students’ task-specific value and situational emotions and, further, whether first-year study engagement would moderate this association during the first two years of studies. Intra-individual state assessments were conducted via mobile phone-based experience sampling method (ESM) during participants’ first (N = 72) and second (N = 56) academic years, resulting in 3089 and 2912 fully completed state questionnaires. In both years, students were asked five times a day over two weeks how important they perceived their current activity and their positive and negative emotions. Using multilevel structural equation modeling, we found that, on average, a higher perception of task-specific value was associated with higher positive emotions and lower negative emotions within individuals. However, individual differences were detected in the value-emotion relations especially during the second academic year. Finally, the findings indicated that overall study engagement, measured at the beginning of the first academic year, predicted between-person differences in these within-person relationships both years.

Published
2019

28. Neonatal Alexander disease:novel GFAP mutation and comparison to previously published cases

Author

Knuutinen, O. (Oula), Kousi, M. (Maria), Suo-Palosaari, M. (Maria), Moilanen, J. S. (Jukka S.), Tuominen, H. (Hannu), Vainionpää, L. (Leena), Joensuu, T. (Tarja), Anttonen, A.-K. (Anna-Kaisa), Uusimaa, J. (Johanna), Lehesjoki, A.-E. (Anna-Elina), and Vieira, P. (Päivi)

Subjects
leukodystrophy, neuroimaging, drug-resistant seizures, hydrocephalus
Abstract

Alexander disease (AxD) is a genetic leukodystrophy caused by GFAP mutations leading to astrocyte dysfunction. Neonatal AxD is a rare phenotype with onset in the first month of life. The proband, belonging to a large pedigree with dominantly inherited benign familial neonatal epilepsy (BFNE), had a phenotype distinct from the rest of the family, with hypotonia and macrocephaly in addition to drug-resistant neonatal seizures. The patient deteriorated and passed away at 6 weeks of age. The pathological and neuroimaging data were consistent with the diagnosis of AxD. Genetic analysis of the proband identified a novel de novo GFAP missense mutation and a KCNQ2 splice site mutation segregating with the BFNE phenotype in the family. The GFAP mutation was located in the coil 2B region of GFAP protein, similar to most neonatal-onset AxD cases with an early death. The clinical and neuroradiological features of the previously published neonatal AxD patients are presented. This study further supports the classification of neonatal-onset AxD as a distinct phenotype based on the age of onset.

Published
2018

31. A novel intrinsically disordered outer membrane lipoprotein of Aggregatibacter actinomycetemcomitans binds various cytokines and plays a role in biofilm response to interleukin-1β and interleukin-8

Author

Ahlstrand, T. (Tuuli), Tuominen, H. (Heidi), Beklen, A. (Arzu), Torittu, A. (Annamari), Oscarsson, J. (Jan), Sormunen, R. (Raija), Pöllänen, M. T. (Marja T.), Permi, P. (Perttu), Ihalin, R. (Riikka), Ahlstrand, T. (Tuuli), Tuominen, H. (Heidi), Beklen, A. (Arzu), Torittu, A. (Annamari), Oscarsson, J. (Jan), Sormunen, R. (Raija), Pöllänen, M. T. (Marja T.), Permi, P. (Perttu), and Ihalin, R. (Riikka)

Abstract

Intrinsically disordered proteins (IDPs) do not have a well-defined and stable 3-dimensional fold. Some IDPs can function as either transient or permanent binders of other proteins and may interact with an array of ligands by adopting different conformations. A novel outer membrane lipoprotein, bacterial interleukin receptor I (BilRI) of the opportunistic oral pathogen Aggregatibacter actinomycetemcomitans binds a key gatekeeper proinflammatory cytokine interleukin (IL)-1β. Because the amino acid sequence of the novel lipoprotein resembles that of fibrinogen binder A of Haemophilus ducreyi, BilRI could have the potential to bind other proteins, such as host matrix proteins. However, from the tested host matrix proteins, BilRI interacted with neither collagen nor fibrinogen. Instead, the recombinant non-lipidated BilRI, which was intrinsically disordered, bound various pro/anti-inflammatory cytokines, such as IL-8, tumor necrosis factor (TNF)-α, interferon (IFN)-γ and IL-10. Moreover, BilRI played a role in the in vitro sensing of IL-1β and IL-8 because low concentrations of cytokines did not decrease the amount of extracellular DNA in the matrix of bilRI− mutant biofilm as they did in the matrix of wild-type biofilm when the biofilms were exposed to recombinant cytokines for 22 hours. BilRI played a role in the internalization of IL-1β in the gingival model system but did not affect either IL-8 or IL-6 uptake. However, bilRI deletion did not entirely prevent IL-1β internalization, and the binding of cytokines to BilRI was relatively weak. Thus, BilRI might sequester cytokines on the surface of A. actinomycetemcomitans to facilitate the internalization process in low local cytokine concentrations.

Published
2017

32. Case report:a novel frameshift mutation in the mitochondrial cytochrome c oxidase II gene causing mitochondrial disorder

Author

Kytövuori, L. (Laura), Kärppä, M. (Mikko), Tuominen, H. (Hannu), Uusimaa, J. (Johanna), Saari, M. (Markku), Hinttala, R. (Reetta), Majamaa, K. (Kari), Kytövuori, L. (Laura), Kärppä, M. (Mikko), Tuominen, H. (Hannu), Uusimaa, J. (Johanna), Saari, M. (Markku), Hinttala, R. (Reetta), and Majamaa, K. (Kari)

Abstract

Background: Mitochondrial cytochrome c oxidase 2, MT-CO2, encodes one of the three subunits, which form the catalytic core of cytochrome c oxidase (COX), complex IV. Mutations in MT-CO2 are rare and the associated phenotypes are variable including nonsyndromic and syndromic forms of mitochondrial diseases. Case presentation: We describe a 30-year-old man with cognitive decline, epilepsy, psychosis, exercise intolerance, sensorineural hearing impairment, retinitis pigmentosa, cataract and lactic acidosis. COX-deficient fibers and ragged red fibers were abundant in the muscle. Sequencing of mitochondrial DNA (mtDNA) revealed a novel frameshift mutation m.8156delG that was predicted to cause altered C-terminal amino acid sequence and to lead to truncation of the COX subunit 2. The deletion was heteroplasmic being present in 26% of the mtDNA in blood, 33% in buccal mucosa and 95% in muscle. Deletion heteroplasmy correlated with COX-deficiency in muscle histochemistry. The mother and the siblings of the proband did not harbor the deletion. Conclusions: The clinical features and muscle histology of the proband suggested a mitochondrial disorder. The m.8156delG deletion is a new addition to the short list of pathogenic mutations in the mtDNA-encoded subunits of COX. This case illustrates the importance of mtDNA sequence analysis in patients with an evident mitochondrial disorder.

Published
2017

34. A bHLH-Based Feedback Loop Restricts Vascular Cell Proliferation in Plants

Author

Universitat Politècnica de València. Instituto Universitario Mixto de Biología Molecular y Celular de Plantas - Institut Universitari Mixt de Biologia Molecular i Cel·lular de Plantes, Ministerio de Ciencia e Innovación, Fundació Bancària Caixa d'Estalvis i Pensions de Barcelona, Netherlands Organization for Scientific Research, Agencia Estatal de Investigación, European Commission, Vera Sirera, Francisco José, De Rybel, B, Urbez Lagunas, Cristina, Kouklas, E, Pesquera, M, Álvarez Mahecha, Juan Camilo, Minguet, E.G., Tuominen, H, Carbonell Gisbert, Juan, Borst, JW, Weijers, D, Blazquez Rodriguez, Miguel Angel, Universitat Politècnica de València. Instituto Universitario Mixto de Biología Molecular y Celular de Plantas - Institut Universitari Mixt de Biologia Molecular i Cel·lular de Plantes, Ministerio de Ciencia e Innovación, Fundació Bancària Caixa d'Estalvis i Pensions de Barcelona, Netherlands Organization for Scientific Research, Agencia Estatal de Investigación, European Commission, Vera Sirera, Francisco José, De Rybel, B, Urbez Lagunas, Cristina, Kouklas, E, Pesquera, M, Álvarez Mahecha, Juan Camilo, Minguet, E.G., Tuominen, H, Carbonell Gisbert, Juan, Borst, JW, Weijers, D, and Blazquez Rodriguez, Miguel Angel

Abstract

Control of tissue dimensions in multicellular organisms requires the precise quantitative regulation of mitotic activity. In plants, where cells are immobile, tissue size is achieved through control of both cell division orientation and mitotic rate. The bHLH transcription factor heterodimer formed by TARGET OF MONOPTEROS5 (TMO5) and LONESOME HIGHWAY (LHVV) is a central regulator of vascular width-increasing divisions. An important unanswered question is how its activity is limited to specify vascular tissue dimensions. Here we identify a regulatory network that restricts TMO5/LHW activity. We show that thermospermine synthase ACAULIS5 antagonizes TMO5/LHW activity by promoting the accumulation of SAC51-LIKE (SACL) bHLH transcription factors. SACL proteins heterodimerize with LHW therefore likely competing with TMO5/LHW interactions prevent activation of TMO5/LHW target genes, and suppress the over-proliferation caused by excess TMO5/LHW activity. These findings connect two thus-far disparate pathways and provide a mechanistic understanding of the quantitative control of vascular tissue growth.

Published
2015

35. OP46 – 2969: Novel phenotypes of childhood encephalomyopathies with mitochondrial DNA depletion or deletions

Author

Hautakangas, M.R., primary, Komulainen, T., additional, Hinttala, R., additional, Pakanen, S., additional, Vähäsaija, V., additional, Lehenkari, P., additional, Olsen, P., additional, Vieira, P., additional, Saarenpää-Heikkilä, O., additional, Palmio, J., additional, Tuominen, H., additional, Kinnunen, P., additional, Majamaa, K., additional, Rantala, H., additional, and Uusimaa, J., additional

Published
2015
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36. PIRIN2 stabilizes cysteine protease XCP2 and increases susceptibility to the vascular pathogen Ralstonia solanacearum in Arabidopsis

Author

Zhang, B., Tremousaygue, D., Denancé, N., van Esse, H.P., Hörger, A.C., Dabos, P., Goffner, D., Thomma, B.P.H.J., van der Hoorn, R.A.L., Tuominen, H., Zhang, B., Tremousaygue, D., Denancé, N., van Esse, H.P., Hörger, A.C., Dabos, P., Goffner, D., Thomma, B.P.H.J., van der Hoorn, R.A.L., and Tuominen, H.

Abstract

PIRIN (PRN) is a member of the functionally diverse cupin protein superfamily. There are four members of the Arabidopsis thaliana PRN family, but the roles of these proteins are largely unknown. Here we describe a function of the Arabidopsis PIRIN2 (PRN2) that is related to susceptibility to the bacterial plant pathogen Ralstonia solanacearum. Two prn2 mutant alleles displayed decreased disease development and bacterial growth in response to R. solanacearum infection. We elucidated the underlying molecular mechanism by analyzing PRN2 interactions with the papain-like cysteine proteases (PLCPs) XCP2, RD21A, and RD21B, all of which bound to PRN2 in yeast two-hybrid assays and in Arabidopsis protoplast co-immunoprecipitation assays. We show that XCP2 is stabilized by PRN2 through inhibition of its autolysis on the basis of PLCP activity profiling assays and enzymatic assays with recombinant protein. The stabilization of XCP2 by PRN2 was also confirmed in planta. Like prn2 mutants, an xcp2 single knockout mutant and xcp2 prn2 double knockout mutant displayed decreased susceptibility to R. solanacearum, suggesting that stabilization of XCP2 by PRN2 underlies susceptibility to R. solanacearum in Arabidopsis.

Published
2014

38. Individuals with mutations in XPNPEP3, which encodes a mitochondrial protein, develop a nephronophthisis-like nephropathy.

Author

O'Toole, J.F., Liu, Y., Davis, E.E., Westlake, C.J., Attanasio, M., Otto, E.A., Seelow, D., Nurnberg, G., Becker, C., Nuutinen, M., Karppa, M., Ignatius, J., Uusimaa, J., Pakanen, S., Jaakkola, E., Heuvel, L.P.W.J. van den, Fehrenbach, H., Wiggins, R., Goyal, M., Zhou, W., Wolf, M.T., Wise, E., Helou, J., Allen, S.J., Murga-Zamalloa, C.A., Ashraf, S., Chaki, M., Heeringa, S., Chernin, G., Hoskins, B.E., Chaib, H., Gleeson, J., Kusakabe, T., Suzuki, T., Isaac, R.E., Quarmby, L.M., Tennant, B., Fujioka, H., Tuominen, H., Hassinen, I., Lohi, H., Houten, J.L. van, Rotig, A., Sayer, J.A., Rolinski, B., Freisinger, P., Madhavan, S.M., Herzer, M., Madignier, F., Prokisch, H., Nurnberg, P., Jackson, P.K., Khanna, H., Katsanis, N., Hildebrandt, F., O'Toole, J.F., Liu, Y., Davis, E.E., Westlake, C.J., Attanasio, M., Otto, E.A., Seelow, D., Nurnberg, G., Becker, C., Nuutinen, M., Karppa, M., Ignatius, J., Uusimaa, J., Pakanen, S., Jaakkola, E., Heuvel, L.P.W.J. van den, Fehrenbach, H., Wiggins, R., Goyal, M., Zhou, W., Wolf, M.T., Wise, E., Helou, J., Allen, S.J., Murga-Zamalloa, C.A., Ashraf, S., Chaki, M., Heeringa, S., Chernin, G., Hoskins, B.E., Chaib, H., Gleeson, J., Kusakabe, T., Suzuki, T., Isaac, R.E., Quarmby, L.M., Tennant, B., Fujioka, H., Tuominen, H., Hassinen, I., Lohi, H., Houten, J.L. van, Rotig, A., Sayer, J.A., Rolinski, B., Freisinger, P., Madhavan, S.M., Herzer, M., Madignier, F., Prokisch, H., Nurnberg, P., Jackson, P.K., Khanna, H., Katsanis, N., and Hildebrandt, F.

Abstract

Contains fulltext : 88043.pdf (publisher's version ) (Closed access), The autosomal recessive kidney disease nephronophthisis (NPHP) constitutes the most frequent genetic cause of terminal renal failure in the first 3 decades of life. Ten causative genes (NPHP1-NPHP9 and NPHP11), whose products localize to the primary cilia-centrosome complex, support the unifying concept that cystic kidney diseases are "ciliopathies". Using genome-wide homozygosity mapping, we report here what we believe to be a new locus (NPHP-like 1 [NPHPL1]) for an NPHP-like nephropathy. In 2 families with an NPHP-like phenotype, we detected homozygous frameshift and splice-site mutations, respectively, in the X-prolyl aminopeptidase 3 (XPNPEP3) gene. In contrast to all known NPHP proteins, XPNPEP3 localizes to mitochondria of renal cells. However, in vivo analyses also revealed a likely cilia-related function; suppression of zebrafish xpnpep3 phenocopied the developmental phenotypes of ciliopathy morphants, and this effect was rescued by human XPNPEP3 that was devoid of a mitochondrial localization signal. Consistent with a role for XPNPEP3 in ciliary function, several ciliary cystogenic proteins were found to be XPNPEP3 substrates, for which resistance to N-terminal proline cleavage resulted in attenuated protein function in vivo in zebrafish. Our data highlight an emerging link between mitochondria and ciliary dysfunction, and suggest that further understanding the enzymatic activity and substrates of XPNPEP3 will illuminate novel cystogenic pathways.

Published
2010

40. A genomic approach to investigate developmental cell death in woody tissues of Populus trees

Author

Moreau, C., Aksenov, N., Lorenzo, M. G., Segerman, B., Funk, C., Nilsson, Peter, Jansson, S., Tuominen, H., Moreau, C., Aksenov, N., Lorenzo, M. G., Segerman, B., Funk, C., Nilsson, Peter, Jansson, S., and Tuominen, H.

Abstract

Background: Poplar ( Populus sp.) has emerged as the main model system for molecular and genetic studies of forest trees. A Populus expressed sequence tag ( EST) database (POPULUSDB) was previously created from 19 cDNA libraries each originating from different Populus tree tissues, and opened to the public in September 2004. We used this dataset for in silico transcript profiling of a particular process in the woody tissues of the Populus stem: the programmed death of xylem fibers. Results: One EST library in POPULUSDB originates from woody tissues of the Populus stem where xylem fibers undergo cell death. Analysis of EST abundances and library distribution within the POPULUSDB revealed a large number of previously uncharacterized transcripts that were unique in this library and possibly related to the death of xylem fibers. The in silico analysis was complemented by a microarray analysis utilizing a novel Populus cDNA array with a unigene set of 25,000 sequences. Conclusions: In silico analysis, combined with the microarray analysis, revealed the usefulness of non-normalized EST libraries in elucidating transcriptional regulation of previously uncharacterized physiological processes. The data suggested the involvement of two novel extracellular serine proteases, nodulin-like proteins and an Arabidopsis thaliana OPEN STOMATA 1 (AtOST1) homolog in signaling fiber-cell death, as well as mechanisms responsible for hormonal control, nutrient remobilization, regulation of vacuolar integrity and autolysis of the dying fibers., QC 20100525

Published
2005
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45. Crystal Structures of the CBS and DRTGG Domains of the Regulatory Region of Clostridium perfringens Pyrophosphatase Complexed with the Inhibitor, AMP, and Activator, Diadenosine Tetraphosphate

Author

Tuominen, H., primary, Salminen, A., additional, Oksanen, E., additional, Jämsen, J., additional, Heikkilä, O., additional, Lehtiö, L., additional, Magretova, N.N., additional, Goldman, A., additional, Baykov, A.A., additional, and Lahti, R., additional

Published
2010
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50. Investigation of LANDSAT imagery on correlations between ore deposits and major shield structures in Finland

Author

Tuominen, H. V and Kuosmanen, V

Subjects
Earth Resources And Remote Sensing
Abstract

The author has identified the following significant results. On the central Baltic Shield, the concept of drainage patterns can be extended to smaller scales in which case many cultural features become involved to the spatial patterns influenced by bedrock structure. Features resulting from agriculture activity and timbering often exaggerate the influence of the bedrock on the image texture.

Published
1975

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