Your search keyword '"Kia K. Kemppainen"' showing total 9 results

1. Ligand-Bound GeneSwitch Causes Developmental Aberrations in Drosophila that Are Alleviated by the Alternative Oxidase

Author

Ana Andjelković, Kia K. Kemppainen, and Howard T. Jacobs

Subjects

inducible transgenes, nuclear receptor, Drosophila, cleft thorax, notched wings, Genetics, QH426-470

Abstract

Culture of Drosophila expressing the steroid-dependent GeneSwitch transcriptional activator under the control of the ubiquitous α-tubulin promoter was found to produce extensive pupal lethality, as well as a range of dysmorphic adult phenotypes, in the presence of high concentrations of the inducing drug RU486. Prominent among these was cleft thorax, seen previously in flies bearing mutant alleles of the nuclear receptor Ultraspiracle and many other mutants, as well as notched wings, leg malformations, and bristle abnormalities. Neither the α-tubulin-GeneSwitch driver nor the inducing drug on their own produced any of these effects. A second GeneSwitch driver, under the control of the daughterless promoter, which gave much lower and more tissue-restricted transgene expression, exhibited only mild bristle abnormalities in the presence of high levels of RU486. Coexpression of the alternative oxidase (AOX) from Ciona intestinalis produced a substantial shift in the developmental outcome toward a wild-type phenotype, which was dependent on the AOX expression level. Neither an enzymatically inactivated variant of AOX, nor GFP, or the alternative NADH dehydrogenase Ndi1 from yeast gave any such rescue. Users of the GeneSwitch system should be aware of the potential confounding effects of its application in developmental studies.

Published

2016

2. Ligand-Bound GeneSwitch Causes Developmental Aberrations inDrosophilathat Are Alleviated by the Alternative Oxidase

Author

Ana Andjelković, Howard T. Jacobs, Kia K. Kemppainen, Institute of Biotechnology, and Research Programme for Molecular Neurology

Subjects

0301 basic medicine, METAMORPHOSIS, Mutant, PROTEIN, QH426-470, Ligands, inducible transgenes, notched wings, Gene expression, Drosophila Proteins, Wings, Animal, nuclear receptor, Transgenes, THORAX CLOSURE, Genetics (clinical), Plant Proteins, LIFE-SPAN, GENE-EXPRESSION, Genetics, MELANOGASTER, cleft thorax, biology, Pupa, 1184 Genetics, developmental biology, physiology, Thorax, Ciona intestinalis, Cell biology, DNA-Binding Proteins, DEFICIENCY, Mifepristone, Drosophila melanogaster, Phenotype, Drosophila, Oxidoreductases, Drosophila Protein, Alternative oxidase, Saccharomyces cerevisiae Proteins, Genotype, Transgene, Embryonic Development, Investigations, JNK PATHWAY, Bristle, Mitochondrial Proteins, 03 medical and health sciences, Animals, Molecular Biology, Electron Transport Complex I, biology.organism_classification, 030104 developmental biology, FEMALE DROSOPHILA, Mutation, NUCLEAR RECEPTORS, Transcription Factors

Abstract

Culture of Drosophila expressing the steroid-dependent GeneSwitch transcriptional activator under the control of the ubiquitous α-tubulin promoter was found to produce extensive pupal lethality, as well as a range of dysmorphic adult phenotypes, in the presence of high concentrations of the inducing drug RU486. Prominent among these was cleft thorax, seen previously in flies bearing mutant alleles of the nuclear receptor Ultraspiracle and many other mutants, as well as notched wings, leg malformations, and bristle abnormalities. Neither the α-tubulin-GeneSwitch driver nor the inducing drug on their own produced any of these effects. A second GeneSwitch driver, under the control of the daughterless promoter, which gave much lower and more tissue-restricted transgene expression, exhibited only mild bristle abnormalities in the presence of high levels of RU486. Coexpression of the alternative oxidase (AOX) from Ciona intestinalis produced a substantial shift in the developmental outcome toward a wild-type phenotype, which was dependent on the AOX expression level. Neither an enzymatically inactivated variant of AOX, nor GFP, or the alternative NADH dehydrogenase Ndi1 from yeast gave any such rescue. Users of the GeneSwitch system should be aware of the potential confounding effects of its application in developmental studies.

Published

2016

3. Engineering the alternative oxidase gene to better understand and counteract mitochondrial defects: state of the art and perspectives

Author

Kia K. Kemppainen, Howard T. Jacobs, Eric Dufour, Marten Szibor, Pierre Rustin, and Riyad El-Khoury

Subjects

Pharmacology, Genetics, Alternative oxidase, Mitochondrial disease, Respiratory chain, Context (language use), Disease, Computational biology, Biology, medicine.disease, 3. Good health, mitochondrial fusion, medicine, Identification (biology), Gene

Abstract

Mitochondrial disorders are nowadays recognized as impinging on most areas of medicine. They include specific and widespread organ involvement, including both tissue degeneration and tumour formation. Despite the spectacular progresses made in the identification of their underlying molecular basis, effective therapy remains a distant goal. Our still rudimentary understanding of the pathophysiological mechanisms by which these diseases arise constitutes an obstacle to developing any rational treatments. In this context, the idea of using a heterologous gene, encoding a supplemental oxidase otherwise absent from mammals, potentially bypassing the defective portion of the respiratory chain, was proposed more than 10 years ago. The recent progress made in the expression of the alternative oxidase in a wide range of biological systems and disease conditions reveals great potential benefit, considering the broad impact of mitochondrial diseases. This review addresses the state of the art and the perspectives that can be now envisaged by using this strategy.

Published

2014

4. Expression of the yeast NADH dehydrogenase Ndi1 in Drosophila confers increased lifespan independently of dietary restriction

Author

Pierre Rustin, Bettina Hutz, Manuel Portero-Otin, Alba Naudí, Takao Yagi, Akemi Matsuno-Yagi, George D. Mcilroy, Howard T. Jacobs, Alberto Sanz, Angela M. Wilson, Essi Kiviranta, Simo Ellilä, Reineld Pamplona, Eric Dufour, Mikko Soikkeli, Matti Lakanmaa, Esko Kemppainen, Mariona Jové, Rhoda Stefanatos, Suvi Vartiainen, Kia K. Kemppainen, Akbar Zeb, and Tea Tuomela

Subjects

Aging, Saccharomyces cerevisiae Proteins, Blotting, Western, Longevity, Respiratory chain, Oxidative phosphorylation, Mitochondrion, medicine.disease_cause, NADH dehydrogenase activity, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Caloric Restriction, 030304 developmental biology, 2. Zero hunger, 0303 health sciences, Electron Transport Complex I, Multidisciplinary, biology, Histocytochemistry, Reverse Transcriptase Polymerase Chain Reaction, NADH dehydrogenase, Biological Sciences, Mitochondria, Oxidative Stress, Drosophila melanogaster, Biochemistry, Sirtuin, biology.protein, RNA Interference, Reactive Oxygen Species, 030217 neurology & neurosurgery, Oxidative stress

Abstract

Mutations in mitochondrial oxidative phosphorylation complex I are associated with multiple pathologies, and complex I has been proposed as a crucial regulator of animal longevity. In yeast, the single-subunit NADH dehydrogenase Ndi1 serves as a non-proton-translocating alternative enzyme that replaces complex I, bringing about the reoxidation of intramitochondrial NADH. We have created transgenic strains of Drosophila that express yeast NDI1 ubiquitously. Mitochondrial extracts from NDI1 -expressing flies displayed a rotenone-insensitive NADH dehydrogenase activity, and functionality of the enzyme in vivo was confirmed by the rescue of lethality resulting from RNAi knockdown of complex I. NDI1 expression increased median, mean, and maximum lifespan independently of dietary restriction, and with no change in sirtuin activity. NDI1 expression mitigated the aging associated decline in respiratory capacity and the accompanying increase in mitochondrial reactive oxygen species production, and resulted in decreased accumulation of markers of oxidative damage in aged flies. Our results support a central role of mitochondrial oxidative phosphorylation complex I in influencing longevity via oxidative stress, independently of pathways connected to nutrition and growth signaling.

Published

2010

5. Expression of the Ciona intestinalis Alternative Oxidase (AOX) in Drosophila Complements Defects in Mitochondrial Oxidative Phosphorylation

Author

Howard T. Jacobs, Kia K. Kemppainen, Eero Mustalahti, Jongkyeong Chung, Massimo Zeviani, Tea Tuomela, Suvi Vartiainen, Daniel J. M. Fernández-Ayala, Marek Babusiak, Rodolfo Costa, Pierre Rustin, Kevin M.C. O'Dell, Alberto Sanz, Academy of Finland, Tampere University Hospital, Sigrid Juselius Foundation, Fondation Leducq, Centre National de la Recherche Scientifique (France), Institut National de la Santé et de la Recherche Médicale (France), EMBO, Junta de Andalucía, and Telethon

Subjects

Mitochondrial ROS, Alternative oxidase, Physiology, Protein Deglycase DJ-1, HUMDISEASE, Antimycin A, Nerve Tissue Proteins, Mitochondrion, Oxidative Phosphorylation, Electron Transport Complex IV, Mitochondrial Proteins, Animals, Drosophila Proteins, Cytochrome c oxidase, SURF1, Ciona intestinalis, Enzyme Inhibitors, Potassium Cyanide, Molecular Biology, Plant Proteins, biology, fungi, Membrane Proteins, Cell Biology, biology.organism_classification, Mitochondria, Phenotype, Biochemistry, Gene Knockdown Techniques, biology.protein, Drosophila, Drosophila melanogaster, Oxidoreductases, Reactive Oxygen Species, Drosophila Protein

Abstract

Defects in mitochondrial OXPHOS are associated with diverse and mostly intractable human disorders. The single-subunit alternative oxidase (AOX) found in many eukaryotes, but not in arthropods or vertebrates, offers a potential bypass of the OXPHOS cytochrome chain under conditions of pathological OXPHOS inhibition. We have engineered Ciona intestinalis AOX for conditional expression in Drosophila melanogaster. Ubiquitous AOX expression produced no detrimental phenotype in wild-type flies. However, mitochondrial suspensions from AOX-expressing flies exhibited a significant cyanide-resistant substrate oxidation, and the flies were partially resistant to both cyanide and antimycin. AOX expression was able to complement the semilethality of partial knockdown of both cyclope (COXVIc) and the complex IV assembly factor Surf1. It also rescued the locomotor defect and excess mitochondrial ROS production of flies mutated in dj-1β, a Drosophila homolog of the human Parkinson's disease gene DJ1. AOX appears to offer promise as a wide-spectrum therapeutic tool in OXPHOS disorders., This research was funded by Academy of Finland, Tampere University Hospital Medical Research Fund, Sigrid Juselius Foundation, CNRS, INSERM, Leducq Foundation, AMMi, Telethon multicenter grant GGP07019, the Government of Andalucia (Postdoctoral Fellowship to D.J.M.F.-A.), and EMBO (Long-Term Fellowship to A.S.).

Published

2009

6. The alternative oxidase AOX does not rescue the phenotype of tko25t mutant flies

Author

Kia K. Kemppainen, Howard T. Jacobs, and Esko Kemppainen

Subjects

Male, Ribosomal Proteins, Alternative oxidase, Genotype, Mitochondrial translation, Transgene, Mutant, Respiratory chain, oxidative phosphorylation, Embryonic Development, Biology, Mitochondrion, Investigations, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Adenosine Triphosphate, Hormone Antagonists, Genetics, Animals, Drosophila Proteins, Molecular Biology, Genetics (clinical), 030304 developmental biology, Plant Proteins, seizures, 0303 health sciences, Gene knockdown, Electron Transport Complex I, NADH Dehydrogenase, beta Carotene, Phenotype, gene therapy, Ciona intestinalis, Mitochondria, developmental delay, Mifepristone, mitochondrial disease, Drosophila, Female, Oxidoreductases, Reactive Oxygen Species, 030217 neurology & neurosurgery

Abstract

A point mutation [technical knockout25t (tko25t)] in the Drosophila gene coding for mitoribosomal protein S12 generates a phenotype of developmental delay and bang sensitivity. tko25t has been intensively studied as an animal model for human mitochondrial diseases associated with deficiency of mitochondrial protein synthesis and consequent multiple respiratory chain defects. Transgenic expression in Drosophila of the alternative oxidase (AOX) derived from Ciona intestinalis has previously been shown to mitigate the toxicity of respiratory chain inhibitors and to rescue mutant and knockdown phenotypes associated with cytochrome oxidase deficiency. We therefore tested whether AOX expression could compensate the mutant phenotype of tko25t using the GeneSwitch system to activate expression at different times in development. The developmental delay of tko25t was not mitigated by expression of AOX throughout development. AOX expression for 1 d after eclosion, or continuously throughout development, had no effect on the bang sensitivity of tko25t adults, and continued expression in adults older than 30 d also produced no amelioration of the phenotype. In contrast, transgenic expression of the yeast alternative NADH dehydrogenase Ndi1 was synthetically semi-lethal with tko25t and was lethal when combined with both AOX and tko25t. We conclude that AOX does not rescue tko25t and that the mutant phenotype is not solely due to limitations on electron flow in the respiratory chain, but rather to a more complex metabolic defect. The future therapeutic use of AOX in disorders of mitochondrial translation may thus be of limited value.

Published

2014

7. Expression of alternative oxidase in Drosophila ameliorates diverse phenotypes due to cytochrome oxidase deficiency

Author

Pierre Rustin, Juho Rinne, Anna Popplestone, Howard T. Jacobs, Matti Lakanmaa, Ashwin Sriram, Kia K. Kemppainen, Alberto Sanz, Tea Tuomela, Satpal Singh, Akbar Zeb, BioMediTech - BioMediTech, and University of Tampere

Subjects

Male, Alternative oxidase, Developmental Disabilities, Mitochondrial disease, Blotting, Western, Respiratory chain, Cytochrome-c Oxidase Deficiency, Mitochondrion, Biology, Real-Time Polymerase Chain Reaction, Biokemia, solu- ja molekyylibiologia - Biochemistry, cell and molecular biology, Animals, Genetically Modified, Electron Transport Complex IV, Immunoenzyme Techniques, Mitochondrial Proteins, Genetics, medicine, Animals, Humans, Cytochrome c oxidase, RNA, Messenger, Molecular Biology, Cells, Cultured, Infertility, Male, Genetics (clinical), Plant Proteins, Gene knockdown, Oxidase test, Reverse Transcriptase Polymerase Chain Reaction, Neurodegenerative Diseases, Articles, General Medicine, medicine.disease, Molecular biology, Mitochondria, Cell biology, Drosophila melanogaster, Phenotype, Mitochondrial respiratory chain, biology.protein, Female, Oxidoreductases

Abstract

Mitochondrial dysfunction is a significant factor in human disease, ranging from systemic disorders of childhood to cardiomyopathy, ischaemia and neurodegeneration. Cytochrome oxidase, the terminal enzyme of the mitochondrial respiratory chain, is a frequent target. Lower eukaryotes possess alternative respiratory-chain enzymes that provide non-proton-translocating bypasses for respiratory complexes I (single-subunit reduced nicotinamide adenine dinucleotide dehydrogenases, e.g. Ndi1 from yeast) or III + IV [alternative oxidase (AOX)], under conditions of respiratory stress or overload. In previous studies, it was shown that transfer of yeast Ndi1 or Ciona intestinalis AOX to Drosophila was able to overcome the lethality produced by toxins or partial knockdown of complex I or IV. Here, we show that AOX can provide a complete or substantial rescue of a range of phenotypes induced by global or tissue-specific knockdown of different cIV subunits, including integral subunits required for catalysis, as well as peripheral subunits required for multimerization and assembly. AOX was also able to overcome the pupal lethality produced by muscle-specific knockdown of subunit CoVb, although the rescued flies were short lived and had a motility defect. cIV knockdown in neurons was not lethal during development but produced a rapidly progressing locomotor and seizure-sensitivity phenotype, which was substantially alleviated by AOX. Expression of Ndi1 exacerbated the neuronal phenotype produced by cIV knockdown. Ndi1 expressed in place of essential cI subunits produced a distinct residual phenotype of delayed development, bang sensitivity and male sterility. These findings confirm the potential utility of alternative respiratory chain enzymes as tools to combat mitochondrial disease, while indicating important limitations thereof.

Published

2014

8. Engineering the alternative oxidase gene to better understand and counteract mitochondrial defects: state of the art and perspectives

Author

Riyad, El-Khoury, Kia K, Kemppainen, Eric, Dufour, Marten, Szibor, Howard T, Jacobs, and Pierre, Rustin

Subjects

Mitochondrial Proteins, Mitochondrial Diseases, Animals, Humans, Themed Issue: Mitochondrial Pharmacology: Energy, Injury & Beyond, Genetic Engineering, Oxidoreductases, Mitochondria, Plant Proteins

Abstract

Mitochondrial disorders are nowadays recognized as impinging on most areas of medicine. They include specific and widespread organ involvement, including both tissue degeneration and tumour formation. Despite the spectacular progresses made in the identification of their underlying molecular basis, effective therapy remains a distant goal. Our still rudimentary understanding of the pathophysiological mechanisms by which these diseases arise constitutes an obstacle to developing any rational treatments. In this context, the idea of using a heterologous gene, encoding a supplemental oxidase otherwise absent from mammals, potentially bypassing the defective portion of the respiratory chain, was proposed more than 10 years ago. The recent progress made in the expression of the alternative oxidase in a wide range of biological systems and disease conditions reveals great potential benefit, considering the broad impact of mitochondrial diseases. This review addresses the state of the art and the perspectives that can be now envisaged by using this strategy.

Published

2013

9. Comparison of single bicycle crashes and collisions among severely injured cyclists-A 16-year analysis based on the Helsinki Trauma Registry (HTR).

Author

Airaksinen N, Kemppainen K, Handolin L, Espro C, Virtanen K, and Heinänen M

Subjects

Male, Humans, Middle Aged, Female, Bicycling injuries, Injury Severity Score, Registries, Head Protective Devices, Accidents, Traffic prevention & control, Craniocerebral Trauma prevention & control

Abstract

Objective: The Finnish national Traffic Safety Strategy 2022-2026 seeks to halve the number of road fatalities and serious injuries from 2020 to 2030. The strategy states that better information on bicycle crashes is needed for safety promotion. The aim of this study was to describe the demographics, injury characteristics, alcohol involvement, and helmet use of severely injured cyclists and to compare single bicycle crashes (falling alone or hitting a fixed object) to collisions., Material and Methods: We identified all bicycle crashes between 2006 and 2021 from the Helsinki Trauma Registry (HTR). Variables analysed were basic patient demographics, Abbreviated Injury Scale (AIS) codes, AIS 3+ injuries, injured body regions, patient Injury Severity Score (ISS) and New Injury Severity Score (NISS), 30-day in-hospital mortality, ICU length of stay, injury mechanism, alcohol use by the injured cyclists, and helmet use., Results: Of the 325 severe (NISS >15) cycling injury patients in the HTR, 53.5 % were injured in single crashes and 46.5 % in collisions with a moving object. Most (71.4 %) patients were men and mean age of all patients was 54.1 years (SD 16.7). Alcohol was detected in 23.1 % of cases and more often in single crashes (32.8 %) than in collisions (11.9 %). Less than a third (29.2 %) of all cyclists wore a helmet; those who wore a helmet had fewer serious (AIS 3+) head injuries than those who did not. Cyclists injured in collisions had higher ISS and NISS scores than those injured in single crashes. Serious (AIS 3+) injuries in extremities or in pelvic girdle were more common in collisions than in single crashes., Conclusions: Among severely injured cyclists, single bicycle crashes were more common; alcohol was more often detected in single bicycle crashes than in collisions. Overall injury severity was higher in collisions than in single crashes. Helmet users had less AIS 3+ head injuries than non-users. Attention should be focused on preventing alcohol-related cycling injuries, promoting use of bicycle helmets, and more precise and comprehensive documentation of bicycle crashes in health care units., Competing Interests: Declaration of Competing Interest The authors declare that there are no financial or personal relationships with other people or organizations that could cause conflicts of interest., (Copyright © 2023 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2024