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1. JARID2 haploinsufficiency is associated with a clinically distinct neurodevelopmental syndrome

Author

Verberne, Eline A., Goh, Shuxiang, England, Jade, van Ginkel, Manon, Rafael-Croes, Louise, Maas, Saskia, Polstra, Abeltje, Zarate, Yuri A., Bosanko, Katherine A., Pechter, Kieran B., Bedoukian, Emma, Izumi, Kosuke, Chaudhry, Ayeshah, Robin, Nathaniel H., Boothe, Megan, Lippa, Natalie C., Aggarwal, Vimla, De Vivo, Darryl C., Lehman, Anna, Study, Causes, Stockler, Sylvia, Bruel, Ange-Line, Isidor, Bertrand, Lemons, Jennifer, Rodriguez-Buritica, David F., Richmond, Christopher M., Stark, Zornitza, Agrawal, Pankaj B., Kooy, R. Frank, Meuwissen, Marije E. C., Koolen, David A., Pfundt, Rolf, Lieden, Agne, Anderlid, Britt-Marie, Glatz, Dagmar, Mannens, Marcel M. A. M., Bakshi, Madhura, Mallette, Frédérick A., van Haelst, Mieke M., and Campeau, Philippe M.

Published
2021
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2. From cytogenetics to cytogenomics: whole-genome sequencing as a first-line test comprehensively captures the diverse spectrum of disease-causing genetic variation underlying intellectual disability

Author

Anna Lindstrand, Jesper Eisfeldt, Maria Pettersson, Claudia M. B. Carvalho, Malin Kvarnung, Giedre Grigelioniene, Britt-Marie Anderlid, Olof Bjerin, Peter Gustavsson, Anna Hammarsjö, Patrik Georgii-Hemming, Erik Iwarsson, Maria Johansson-Soller, Kristina Lagerstedt-Robinson, Agne Lieden, Måns Magnusson, Marcel Martin, Helena Malmgren, Magnus Nordenskjöld, Ameli Norling, Ellika Sahlin, Henrik Stranneheim, Emma Tham, Josephine Wincent, Sofia Ygberg, Anna Wedell, Valtteri Wirta, Ann Nordgren, Johanna Lundin, and Daniel Nilsson

Subjects
Whole-genome sequencing, Intellectual disability, Monogenic disease, Copy number variation, Structural variation, Single nucleotide variant, Medicine, Genetics, QH426-470
Abstract

Abstract Background Since different types of genetic variants, from single nucleotide variants (SNVs) to large chromosomal rearrangements, underlie intellectual disability, we evaluated the use of whole-genome sequencing (WGS) rather than chromosomal microarray analysis (CMA) as a first-line genetic diagnostic test. Methods We analyzed three cohorts with short-read WGS: (i) a retrospective cohort with validated copy number variants (CNVs) (cohort 1, n = 68), (ii) individuals referred for monogenic multi-gene panels (cohort 2, n = 156), and (iii) 100 prospective, consecutive cases referred to our center for CMA (cohort 3). Bioinformatic tools developed include FindSV, SVDB, Rhocall, Rhoviz, and vcf2cytosure. Results First, we validated our structural variant (SV)-calling pipeline on cohort 1, consisting of three trisomies and 79 deletions and duplications with a median size of 850 kb (min 500 bp, max 155 Mb). All variants were detected. Second, we utilized the same pipeline in cohort 2 and analyzed with monogenic WGS panels, increasing the diagnostic yield to 8%. Next, cohort 3 was analyzed by both CMA and WGS. The WGS data was processed for large (> 10 kb) SVs genome-wide and for exonic SVs and SNVs in a panel of 887 genes linked to intellectual disability as well as genes matched to patient-specific Human Phenotype Ontology (HPO) phenotypes. This yielded a total of 25 pathogenic variants (SNVs or SVs), of which 12 were detected by CMA as well. We also applied short tandem repeat (STR) expansion detection and discovered one pathologic expansion in ATXN7. Finally, a case of Prader-Willi syndrome with uniparental disomy (UPD) was validated in the WGS data. Important positional information was obtained in all cohorts. Remarkably, 7% of the analyzed cases harbored complex structural variants, as exemplified by a ring chromosome and two duplications found to be an insertional translocation and part of a cryptic unbalanced translocation, respectively. Conclusion The overall diagnostic rate of 27% was more than doubled compared to clinical microarray (12%). Using WGS, we detected a wide range of SVs with high accuracy. Since the WGS data also allowed for analysis of SNVs, UPD, and STRs, it represents a powerful comprehensive genetic test in a clinical diagnostic laboratory setting.

Published
2019
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3. Ataxia in Patients With Bi-Allelic NFASC Mutations and Absence of Full-Length NF186

Author

Malin Kvarnung, Mansoureh Shahsavani, Fulya Taylan, Mohsen Moslem, Nicole Breeuwsma, Loora Laan, Jens Schuster, Zhe Jin, Daniel Nilsson, Agne Lieden, Britt-Marie Anderlid, Magnus Nordenskjöld, Elisabeth Syk Lundberg, Bryndis Birnir, Niklas Dahl, Ann Nordgren, Anna Lindstrand, and Anna Falk

Subjects
neurofascin, neuronal isoform NF186, ataxia, patient-specific induced pluripotent stem cells, neuroepithelial stem cells, neurites, Genetics, QH426-470
Abstract

The etiology of hereditary ataxia syndromes is heterogeneous, and the mechanisms underlying these disorders are often unknown. Here, we utilized exome sequencing in two siblings with progressive ataxia and muscular weakness and identified a novel homozygous splice mutation (c.3020-1G > A) in neurofascin (NFASC). In RNA extracted from fibroblasts, we showed that the mutation resulted in inframe skipping of exon 26, with a deprived expression of the full-length transcript that corresponds to NFASC isoform NF186. To further investigate the disease mechanisms, we reprogrammed fibroblasts from one affected sibling to induced pluripotent stem cells, directed them to neuroepithelial stem cells and finally differentiated to neurons. In early neurogenesis, differentiating cells with selective depletion of the NF186 isoform showed significantly reduced neurite outgrowth as well as fewer emerging neurites. Furthermore, whole-cell patch-clamp recordings of patient-derived neuronal cells revealed a lower threshold for openings, indicating altered Na+ channel kinetics, suggesting a lower threshold for openings as compared to neuronal cells without the NFASC mutation. Taken together, our results suggest that loss of the full-length NFASC isoform NF186 causes perturbed neurogenesis and impaired neuronal biophysical properties resulting in a novel early-onset autosomal recessive ataxia syndrome.

Published
2019
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4. From cytogenetics to cytogenomics: whole-genome sequencing as a first-line test comprehensively captures the diverse spectrum of disease-causing genetic variation underlying intellectual disability

Author

Lindstrand, Anna, Eisfeldt, Jesper, Pettersson, Maria, Carvalho, Claudia M. B., Kvarnung, Malin, Grigelioniene, Giedre, Anderlid, Britt-Marie, Bjerin, Olof, Gustavsson, Peter, Hammarsjö, Anna, Georgii-Hemming, Patrik, Iwarsson, Erik, Johansson-Soller, Maria, Lagerstedt-Robinson, Kristina, Lieden, Agne, Magnusson, Måns, Martin, Marcel, Malmgren, Helena, Nordenskjöld, Magnus, Norling, Ameli, Sahlin, Ellika, Stranneheim, Henrik, Tham, Emma, Wincent, Josephine, Ygberg, Sofia, Wedell, Anna, Wirta, Valtteri, Nordgren, Ann, Lundin, Johanna, and Nilsson, Daniel

Published
2019
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5. Genome sequencing is a sensitive first-line test to diagnose individuals with intellectual disability

Author

Lindstrand, Anna, primary, Ek, Marlene, additional, Kvarnung, Malin, additional, Anderlid, Britt-Marie, additional, Björck, Erik, additional, Carlsten, Jonas, additional, Eisfeldt, Jesper, additional, Grigelioniene, Giedre, additional, Gustavsson, Peter, additional, Hammarsjö, Anna, additional, Helgadottir, Hafdís T., additional, Hellström-Pigg, Maritta, additional, Kuchinskaya, Ekaterina, additional, Lagerstedt-Robinson, Kristina, additional, Levin, Lars-Åke, additional, Lieden, Agne, additional, Lindelöf, Hillevi, additional, Malmgren, Helena, additional, Nilsson, Daniel, additional, Svensson, Eva, additional, Paucar, Martin, additional, Sahlin, Ellika, additional, Tesi, Bianca, additional, Tham, Emma, additional, Winberg, Johanna, additional, Winerdal, Max, additional, Wincent, Josephine, additional, Soller, Maria Johansson, additional, Pettersson, Maria, additional, and Nordgren, Ann, additional

Published
2023
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7. Replicative and non-replicative mechanisms in the formation of clustered CNVs are indicated by whole genome characterization.

Author

Lusine Nazaryan-Petersen, Jesper Eisfeldt, Maria Pettersson, Johanna Lundin, Daniel Nilsson, Josephine Wincent, Agne Lieden, Lovisa Lovmar, Jesper Ottosson, Jelena Gacic, Outi Mäkitie, Ann Nordgren, Francesco Vezzi, Valtteri Wirta, Max Käller, Tina Duelund Hjortshøj, Cathrine Jespersgaard, Rayan Houssari, Laura Pignata, Mads Bak, Niels Tommerup, Elisabeth Syk Lundberg, Zeynep Tümer, and Anna Lindstrand

Subjects
Genetics, QH426-470
Abstract

Clustered copy number variants (CNVs) as detected by chromosomal microarray analysis (CMA) are often reported as germline chromothripsis. However, such cases might need further investigations by massive parallel whole genome sequencing (WGS) in order to accurately define the underlying complex rearrangement, predict the occurrence mechanisms and identify additional complexities. Here, we utilized WGS to delineate the rearrangement structure of 21 clustered CNV carriers first investigated by CMA and identified a total of 83 breakpoint junctions (BPJs). The rearrangements were further sub-classified depending on the patterns observed: I) Cases with only deletions (n = 8) often had additional structural rearrangements, such as insertions and inversions typical to chromothripsis; II) cases with only duplications (n = 7) or III) combinations of deletions and duplications (n = 6) demonstrated mostly interspersed duplications and BPJs enriched with microhomology. In two cases the rearrangement mutational signatures indicated both a breakage-fusion-bridge cycle process and haltered formation of a ring chromosome. Finally, we observed two cases with Alu- and LINE-mediated rearrangements as well as two unrelated individuals with seemingly identical clustered CNVs on 2p25.3, possibly a rare European founder rearrangement. In conclusion, through detailed characterization of the derivative chromosomes we show that multiple mechanisms are likely involved in the formation of clustered CNVs and add further evidence for chromoanagenesis mechanisms in both "simple" and highly complex chromosomal rearrangements. Finally, WGS characterization adds positional information, important for a correct clinical interpretation and deciphering mechanisms involved in the formation of these rearrangements.

Published
2018
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8. Genome sequencing is a sensitive first-line test to diagnose individuals with intellectual disability

Author

Lindstrand, Anna, primary, Ek, Marlene, additional, Kvarnung, Malin, additional, Anderlid, Britt-Marie, additional, Björck, Erik, additional, Carlsten, Jonas, additional, Eisfeldt, Jesper, additional, Grigelioniene, Giedre, additional, Gustavsson, Peter, additional, Hammarsjö, Anna, additional, Helgadóttir, Hafdís T., additional, Hellström-Pigg, Maritta, additional, Kuchinskaya, Ekaterina, additional, Lagerstedt-Robinson, Kristina, additional, Levin, Lars-Åke, additional, Lieden, Agne, additional, Lindelöf, Hillevi, additional, Malmgren, Helena, additional, Nilsson, Daniel, additional, Svensson, Eva, additional, Paucar, Martin, additional, Sahlin, Ellika, additional, Tesi, Bianca, additional, Tham, Emma, additional, Winberg, Johanna, additional, Winerdal, Max, additional, Wincent, Josephine, additional, Johansson Soller, Maria, additional, Pettersson, Maria, additional, and Nordgren, Ann, additional

Published
2022
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9. DNA Methylation Signature for

Author

Eline A, Verberne, Liselot, van der Laan, Sadegheh, Haghshenas, Kathleen, Rooney, Michael A, Levy, Mariëlle, Alders, Saskia M, Maas, Sandra, Jansen, Agne, Lieden, Britt-Marie, Anderlid, Louise, Rafael-Croes, Philippe M, Campeau, Ayeshah, Chaudhry, David A, Koolen, Rolph, Pfundt, Anna C E, Hurst, Frederic, Tran-Mau-Them, Ange-Line, Bruel, Laetitia, Lambert, Bertrand, Isidor, Marcel M A M, Mannens, Bekim, Sadikovic, Peter, Henneman, and Mieke M, van Haelst

Subjects
Phenotype, Polycomb Repressive Complex 2, Humans, Syndrome, DNA Methylation, Nucleotide Motifs, Protein Processing, Post-Translational
Published
2022

10. DNA Methylation Signature for JARID2-Neurodevelopmental Syndrome

Author

Verberne, Eline A., primary, van der Laan, Liselot, additional, Haghshenas, Sadegheh, additional, Rooney, Kathleen, additional, Levy, Michael A., additional, Alders, Mariëlle, additional, Maas, Saskia M., additional, Jansen, Sandra, additional, Lieden, Agne, additional, Anderlid, Britt-Marie, additional, Rafael-Croes, Louise, additional, Campeau, Philippe M., additional, Chaudhry, Ayeshah, additional, Koolen, David A., additional, Pfundt, Rolph, additional, Hurst, Anna C. E., additional, Tran-Mau-Them, Frederic, additional, Bruel, Ange-Line, additional, Lambert, Laetitia, additional, Isidor, Bertrand, additional, Mannens, Marcel M. A. M., additional, Sadikovic, Bekim, additional, Henneman, Peter, additional, and van Haelst, Mieke M., additional

Published
2022
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11. Genome sequencing is a sensitive first-line test to diagnose individuals with intellectual disability

Author

Lindstrand, Anna, Ek, Marlene, Kvarnung, Malin, Anderlid, Britt-Marie, Bjoerck, Erik, Carlsten, Jonas, Eisfeldt, Jesper, Grigelioniene, Giedre, Gustavsson, Peter, Hammarsjoe, Anna, Helgadottir, Hafdis T., Hellstroem-Pigg, Maritta, Kuchinskaya, Ekaterina, Lagerstedt-Robinson, Kristina, Levin, Lars-Åke, Lieden, Agne, Lindeloef, Hillevi, Malmgren, Helena, Nilsson, Daniel, Svensson, Eva, Paucar, Martin, Sahlin, Ellika, Tesi, Bianca, Tham, Emma, Winberg, Johanna, Winerdal, Max, Wincent, Josephine, Soller, Maria Johansson, Pettersson, Maria, Nordgren, Ann, Lindstrand, Anna, Ek, Marlene, Kvarnung, Malin, Anderlid, Britt-Marie, Bjoerck, Erik, Carlsten, Jonas, Eisfeldt, Jesper, Grigelioniene, Giedre, Gustavsson, Peter, Hammarsjoe, Anna, Helgadottir, Hafdis T., Hellstroem-Pigg, Maritta, Kuchinskaya, Ekaterina, Lagerstedt-Robinson, Kristina, Levin, Lars-Åke, Lieden, Agne, Lindeloef, Hillevi, Malmgren, Helena, Nilsson, Daniel, Svensson, Eva, Paucar, Martin, Sahlin, Ellika, Tesi, Bianca, Tham, Emma, Winberg, Johanna, Winerdal, Max, Wincent, Josephine, Soller, Maria Johansson, Pettersson, Maria, and Nordgren, Ann

Abstract

Purpose: Individuals with intellectual disability (ID) and/or neurodevelopment disorders (NDDs) are currently investigated with several different approaches in clinical genetic diagnostics. Methods: We compared the results from 3 diagnostic pipelines in patients with ID/NDD: genome sequencing (GS) first (N = 100), GS as a secondary test (N = 129), or chromosomal microarray (CMA) with or without FMR1 analysis (N = 421). Results: The diagnostic yield was 35% (GS -first), 26% (GS as a secondary test), and 11% (CMA/FMR1). Notably, the age of diagnosis was delayed by 1 year when GS was performed as a secondary test and the cost per diagnosed individual was 36% lower with GS first than with CMA/FMR1. Furthermore, 91% of those with a negative result after CMA/FMR1 analysis (338 individuals) have not yet been referred for additional genetic testing and remain undiagnosed. Conclusion: Our findings strongly suggest that genome analysis outperforms other testing strategies and should replace traditional CMA and FMR1 analysis as a first-line genetic test in individuals with ID/NDD. GS is a sensitive, time-and cost-effective method that results in a confirmed molecular diagnosis in 35% of all referred patients. (c) 2022 The Authors. Published by Elsevier Inc. on behalf of American College of Medical Genetics and Genomics. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

Published
2022
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12. Genome sequencing is a sensitive first-line test to diagnose individuals with intellectual disability

Author

Anna Lindstrand, Marlene Ek, Malin Kvarnung, Britt-Marie Anderlid, Erik Björck, Jonas Carlsten, Jesper Eisfeldt, Giedre Grigelioniene, Peter Gustavsson, Anna Hammarsjö, Hafdís T. Helgadóttir, Maritta Hellström-Pigg, Ekaterina Kuchinskaya, Kristina Lagerstedt-Robinson, Lars-Åke Levin, Agne Lieden, Hillevi Lindelöf, Helena Malmgren, Daniel Nilsson, Eva Svensson, Martin Paucar, Ellika Sahlin, Bianca Tesi, Emma Tham, Johanna Winberg, Max Winerdal, Josephine Wincent, Maria Johansson Soller, Maria Pettersson, and Ann Nordgren

Subjects
Fragile X Mental Retardation Protein, Neurodevelopmental Disorders, Chromosomal microarray, Clinical diagnostics, FMR1 analysis, Genome sequencing, Intellectual disability, Intellectual Disability, Developmental Disabilities, Humans, Genetic Testing, Child, Microarray Analysis, Medical Genetics, Genetics (clinical), Medicinsk genetik, Pathology and Forensic Medicine
Abstract

Purpose: Individuals with intellectual disability (ID) and/or neurodevelopment disorders (NDDs) are currently investigated with several different approaches in clinical genetic diagnostics. Methods: We compared the results from 3 diagnostic pipelines in patients with ID/NDD: genome sequencing (GS) first (N = 100), GS as a secondary test (N = 129), or chromosomal microarray (CMA) with or without FMR1 analysis (N = 421). Results: The diagnostic yield was 35% (GS -first), 26% (GS as a secondary test), and 11% (CMA/FMR1). Notably, the age of diagnosis was delayed by 1 year when GS was performed as a secondary test and the cost per diagnosed individual was 36% lower with GS first than with CMA/FMR1. Furthermore, 91% of those with a negative result after CMA/FMR1 analysis (338 individuals) have not yet been referred for additional genetic testing and remain undiagnosed. Conclusion: Our findings strongly suggest that genome analysis outperforms other testing strategies and should replace traditional CMA and FMR1 analysis as a first-line genetic test in individuals with ID/NDD. GS is a sensitive, time-and cost-effective method that results in a confirmed molecular diagnosis in 35% of all referred patients. (c) 2022 The Authors. Published by Elsevier Inc. on behalf of American College of Medical Genetics and Genomics. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

Published
2022

13. Skin Barrier Function and Staphylococcus aureus Colonization in Vestibulum Nasi and Fauces in Healthy Infants and Infants with Eczema: A Population-Based Cohort Study.

Author

Teresa Løvold Berents, Karin Cecilie Lødrup Carlsen, Petter Mowinckel, Håvard Ove Skjerven, Bente Kvenshagen, Leif Bjarte Rolfsjord, Maria Bradley, Agne Lieden, Kai-Håkon Carlsen, Peter Gaustad, and Petter Gjersvik

Subjects
Medicine, Science
Abstract

Atopic eczema (AE) is associated with Staphylococcus aureus (S. aureus) colonization and skin barrier dysfunction, often measured by increased transepidermal water loss (TEWL). In the present study, the primary aim was to see whether S. aureus colonization in the vestibulum nasi and/or fauces was associated with increased TEWL in infants with healthy skin and infants with eczema. Secondarily, we aimed to investigate whether TEWL measurements on non-lesional skin on the lateral upper arm is equivalent to volar forearm in infants. In 167 of 240 infants, recruited from the general population, TEWL measurements on the lateral upper arm and volar forearm, using a DermaLab USB, fulfilled our environmental requirements. The mean of three TEWL measurements from each site was used for analysis. The infants were diagnosed with no eczema (n = 110), possible AE (n = 28) or AE (n = 29). DNA samples were analysed for mutations in the filaggrin gene (FLG). Bacterial cultures were reported positive with the identification of at least one culture with S. aureus from vestibulum nasi and/or fauces. S. aureus colonization, found in 89 infants (53%), was not associated with increased TEWL (i.e. TEWL in the upper quartile), neither on the lateral upper arm or volar forearm (p = 0.08 and p = 0.98, respectively), nor with AE (p = 0.10) or FLG mutation (p = 0.17). TEWL was significantly higher on both measuring sites in infants with AE compared to infants with possible AE and no eczema. FLG mutation was significantly associated with increased TEWL, with a 47% difference in TEWL. We conclude that S. aureus in vestibulum nasi and/or fauces was not associated with TEWL, whereas TEWL measurements on the lateral upper arm and volar forearm appear equally appropriate in infants.

Published
2015
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15. JARID2 haploinsufficiency is associated with a clinically distinct neurodevelopmental syndrome

Author

Verberne, E.A., Goh, S., England, J., Ginkel, M. van, Rafael-Croes, L., Maas, S., Polstra, A., Zarate, Y.A., Bosanko, K.A., Pechter, K.B., Bedoukian, E., Izumi, K., Chaudhry, A., Robin, N.H., Boothe, M., Lippa, N.C., Aggarwal, V., Vivo, D.C. De, Lehman, A., Study, C., Stockler, S., Bruel, A.L., Isidor, B., Lemons, J., Rodriguez-Buritica, D.F., Richmond, C.M., Stark, Z., Agrawal, P.B., Kooy, R.F., Meuwissen, M.E.C., Koolen, D.A., Pfundt, R.P., Lieden, A., Anderlid, B.M., Glatz, D., Mannens, M., Bakshi, M., Mallette, F.A., Haelst, M.M. van, Campeau, P.M., Verberne, E.A., Goh, S., England, J., Ginkel, M. van, Rafael-Croes, L., Maas, S., Polstra, A., Zarate, Y.A., Bosanko, K.A., Pechter, K.B., Bedoukian, E., Izumi, K., Chaudhry, A., Robin, N.H., Boothe, M., Lippa, N.C., Aggarwal, V., Vivo, D.C. De, Lehman, A., Study, C., Stockler, S., Bruel, A.L., Isidor, B., Lemons, J., Rodriguez-Buritica, D.F., Richmond, C.M., Stark, Z., Agrawal, P.B., Kooy, R.F., Meuwissen, M.E.C., Koolen, D.A., Pfundt, R.P., Lieden, A., Anderlid, B.M., Glatz, D., Mannens, M., Bakshi, M., Mallette, F.A., Haelst, M.M. van, and Campeau, P.M.

Abstract

Item does not contain fulltext, PURPOSE: JARID2, located on chromosome 6p22.3, is a regulator of histone methyltransferase complexes that is expressed in human neurons. So far, 13 individuals sharing clinical features including intellectual disability (ID) were reported with de novo heterozygous deletions in 6p22-p24 encompassing the full length JARID2 gene (OMIM 601594). However, all published individuals to date have a deletion of at least one other adjoining gene, making it difficult to determine if JARID2 is the critical gene responsible for the shared features. We aim to confirm JARID2 as a human disease gene and further elucidate the associated clinical phenotype. METHODS: Chromosome microarray analysis, exome sequencing, and an online matching platform (GeneMatcher) were used to identify individuals with single-nucleotide variants or deletions involving JARID2. RESULTS: We report 16 individuals in 15 families with a deletion or single-nucleotide variant in JARID2. Several of these variants are likely to result in haploinsufficiency due to nonsense-mediated messenger RNA (mRNA) decay. All individuals have developmental delay and/or ID and share some overlapping clinical characteristics such as facial features with those who have larger deletions involving JARID2. CONCLUSION: We report that JARID2 haploinsufficiency leads to a clinically distinct neurodevelopmental syndrome, thus establishing gene-disease validity for the purpose of diagnostic reporting.

Published
2021

16. A genome-wide association study of atopic dermatitis identifies loci with overlapping effects on asthma and psoriasis

Author

Weidinger, Stephan, Willis-Owen, Saffron A.G., Kamatani, Yoichiro, Baurecht, Hansjörg, Morar, Nilesh, Liang, Liming, Edser, Pauline, Street, Teresa, Rodriguez, Elke, OʼRegan, Grainne M., Beattie, Paula, Fölster-Holst, Regina, Franke, Andre, Novak, Natalija, Fahy, Caoimhe M., Winge, Mårten C.G., Kabesch, Michael, Illig, Thomas, Heath, Simon, Söderhäll, Cilla, Melén, Erik, Pershagen, Göran, Kere, Juha, Bradley, Maria, Lieden, Agne, Nordenskjold, Magnus, Harper, John I., Mclean, W.H. Irwin, Brown, Sara J., Cookson, William O.C., Lathrop, G. Mark, Irvine, Alan D., and Moffatt, Miriam F.

Published
2013
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18. Ataxia in Patients With Bi-Allelic NFASC Mutations and Absence of Full-Length NF186

Author

Kvarnung, Malin, Shahsavani, Mansoureh, Taylan, Fulya, Moslem, Mohsen, Breeuwsma, Nicole, Laan, Loora, Schuster, Jens, Jin, Zhe, Nilsson, Daniel, Lieden, Agne, Anderlid, Britt-Marie, Nordenskjold, Magnus, Lundberg, Elisabeth Syk, Birnir, Bryndis, Dahl, Niklas, Nordgren, Ann, Lindstrand, Anna, Falk, Anna, Kvarnung, Malin, Shahsavani, Mansoureh, Taylan, Fulya, Moslem, Mohsen, Breeuwsma, Nicole, Laan, Loora, Schuster, Jens, Jin, Zhe, Nilsson, Daniel, Lieden, Agne, Anderlid, Britt-Marie, Nordenskjold, Magnus, Lundberg, Elisabeth Syk, Birnir, Bryndis, Dahl, Niklas, Nordgren, Ann, Lindstrand, Anna, and Falk, Anna

Abstract

The etiology of hereditary ataxia syndromes is heterogeneous, and the mechanisms underlying these disorders are often unknown. Here, we utilized exome sequencing in two siblings with progressive ataxia and muscular weakness and identified a novel homozygous splice mutation (c.3020-1G > A) in neurofascin (NFASC). In RNA extracted from fibroblasts, we showed that the mutation resulted in inframe skipping of exon 26, with a deprived expression of the full-length transcript that corresponds to NFASC isoform NF186. To further investigate the disease mechanisms, we reprogrammed fibroblasts from one affected sibling to induced pluripotent stem cells, directed them to neuroepithelial stem cells and finally differentiated to neurons. In early neurogenesis, differentiating cells with selective depletion of the NF186 isoform showed significantly reduced neurite outgrowth as well as fewer emerging neurites. Furthermore, whole-cell patch-clamp recordings of patient-derived neuronal cells revealed a lower threshold for openings, indicating altered Na+ channel kinetics, suggesting a lower threshold for openings as compared to neuronal cells without the NFASC mutation. Taken together, our results suggest that loss of the full-length NFASC isoform NF186 causes perturbed neurogenesis and impaired neuronal biophysical properties resulting in a novel early-onset autosomal recessive ataxia syndrome.

Published
2019
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19. From cytogenetics to cytogenomics : whole genome sequencing as a comprehensive genetic test in rare disease diagnostics

Author

Nilsson, D., Eisfeldt, J., Lundin, J., Pettersson, M., Kvarnung, M., Lieden, A., Sahlin, E., Lagerstedt, K., Martin, M., Ygberg, S., Bjerin, O., Stranneheim, H., Wedell, A., Nordenskjold, M., Soller, M. Johansson, Nordgren, A., Wirta, Valtteri, Lindstrand, A., Nilsson, D., Eisfeldt, J., Lundin, J., Pettersson, M., Kvarnung, M., Lieden, A., Sahlin, E., Lagerstedt, K., Martin, M., Ygberg, S., Bjerin, O., Stranneheim, H., Wedell, A., Nordenskjold, M., Soller, M. Johansson, Nordgren, A., Wirta, Valtteri, and Lindstrand, A.

Abstract

Rare genetic diseases are caused by different types of genetic variants, from single nucleotide variants (SNVs) to large chromosomal rearrangements. Recent data indicates that whole genome sequencing (WGS) may be used as a comprehensive test to identify multiple types of pathologic genetic aberrations in a single analysis. We present FindSV, a bioinformatic pipeline for detection of balanced (inversions and translocations) and unbalanced (deletions and duplications) structural variants (SVs). First, FindSV was tested on 106 validated deletions and duplications with a median size of 850 kb (min: 511 bp, max: 155 Mb). All variants were detected. Second, we demonstrated the clinical utility in 138 monogenic WGS panels. SV analysis yielded 11 diagnostic findings (8%). Remarkably, a complex structural rearrangement involving two clustered deletions disrupting SCN1A, SCN2A, and SCN3A was identified in a three months old girl with epileptic encephalopathy. Finally, 100 consecutive samples referred for clinical microarray were also analyzed by WGS. The WGS data was screened for large (>2 kbp) SVs genome wide, processed for visualization in our clinical routine arrayCGH workflow with the newly developed tool vcf2cytosure, and for exonic SVs and SNVs in a panel of 700 genes linked to intellectual disability. We also applied short tandem repeat (STR) expansion detection and discovered one pathologic expansion in ATXN7. The diagnostic rate (29%) was doubled compared to clinical microarray (12%). In conclusion, using WGS we have detected a wide range of structural variation with high accuracy, confirming it a powerful comprehensive genetic test in a clinical diagnostic laboratory setting., QC 20191104

Published
2019
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20. From cytogenetics to cytogenomics whole genome sequencing as a comprehensive genetic test in rare disease diagnostics

Author

Eisfeldt, Jesper, Lundin, Johanna, Pettersson, Maria, Kvarnung, Malin, Lieden, Agne, Sahlin, Ellika, Lagerstedt, Kristina, Martin, Marcel, Ygberg, Sofia, Bjerin, Olof, Stranneheim, Henrik, Wedell, Anna, Nordenskjold, Magnus, Soller, Maria Johansson, Nordgren, Ann, Wirta, Valtteri, Nilsson, Daniel, Lindstrand, Anna, Eisfeldt, Jesper, Lundin, Johanna, Pettersson, Maria, Kvarnung, Malin, Lieden, Agne, Sahlin, Ellika, Lagerstedt, Kristina, Martin, Marcel, Ygberg, Sofia, Bjerin, Olof, Stranneheim, Henrik, Wedell, Anna, Nordenskjold, Magnus, Soller, Maria Johansson, Nordgren, Ann, Wirta, Valtteri, Nilsson, Daniel, and Lindstrand, Anna

Abstract

QC 20190731

Published
2019

21. Identification of putative pathogenic single nucleotide variants (SNVs) in genes associated with heart disease in 290 cases of stillbirth

Author

Sahlin, Ellika, Gréen, Anna, Gustavsson, Peter, Lieden, Agne, Nordenskjold, Magnus, Papadogiannakis, Nikos, Pettersson, Karin, Nilsson, Daniel, Jonasson, Jon, Iwarsson, Erik, Sahlin, Ellika, Gréen, Anna, Gustavsson, Peter, Lieden, Agne, Nordenskjold, Magnus, Papadogiannakis, Nikos, Pettersson, Karin, Nilsson, Daniel, Jonasson, Jon, and Iwarsson, Erik

Abstract

The incidence of stillbirth in Sweden has essentially remained constant since the 1980s, and despite thorough investigation, many cases remain unexplained. It has been suggested that a proportion of stillbirth cases is caused by heart disease, mainly channelopathies. The aim of this study was to analyze DNA from 290 stillbirth cases without chromosomal abnormalities for pathogenic single nucleotide variants (SNVs) in 70 genes associated with cardiac channelopathies and cardiomyopathies. The HaloPlex Target Enrichment System (Agilent Technologies) was utilized to prepare sequencing libraries which were sequenced on the Illumina NextSeq platform. We found that 12.1% of the 290 investigated stillbirth cases had one (n = 31) or two (n = 4) variants with evidence supporting pathogenicity, i.e. loss-of-function variants (nonsense, frameshift, splice site substitutions), evidence from functional studies, or previous identification of the variants in affected individuals. Regarding identified putative pathogenic variants in genes associated with channelopathies, the prevalence was significantly higher in the stillbirth cohort (n = 23, 7.93%) than the corresponding prevalence of the same variants in the non-Finnish European population of the Exome Aggregation Consortium (2.70%, pamp;lt;0.001) and SweGen, (2.30%, pamp;lt;0.001). Our results give further support to the hypothesis that cardiac channelopathies might contribute to stillbirth. Screening for pathogenic SNVs in genes associated with heart disease might be a valuable complement for stillbirth cases where todays conventional investigation does not reveal the underlying cause of fetal demise., Funding Agencies|FORSS, Forskningsradet i sydostra Sverige (the Medical Research Council of Southeast Sweden) [FORSS-307961]; Stockholms Ians landsting (Stockholm County Council) [SLL20160339]

Published
2019
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22. Ataxia in Patients With Bi-Allelic NFASC Mutations and Absence of Full-Length NF186

Author

Kvarnung, Malin, primary, Shahsavani, Mansoureh, additional, Taylan, Fulya, additional, Moslem, Mohsen, additional, Breeuwsma, Nicole, additional, Laan, Loora, additional, Schuster, Jens, additional, Jin, Zhe, additional, Nilsson, Daniel, additional, Lieden, Agne, additional, Anderlid, Britt-Marie, additional, Nordenskjöld, Magnus, additional, Syk Lundberg, Elisabeth, additional, Birnir, Bryndis, additional, Dahl, Niklas, additional, Nordgren, Ann, additional, Lindstrand, Anna, additional, and Falk, Anna, additional

Published
2019
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23. Whole genome characterization of array defined clustered CNVs reveals two distinct complex rearrangement subclasses generated through either non-homologous repair or template switching

Author

Nazaryan-Petersen, L., Eisfeldt, J., Lundin, J., Pettersson, M., Nilsson, D., Wincent, J., Lieden, A., Vezzi, F., Wirta, Valtteri, Käller, Max, Duelund, T., Houssari, R., Pignata, L., Bak, M., Tommerup, N., Lundberg, E. S., Tumer, Z., Lindstrand, A., Nazaryan-Petersen, L., Eisfeldt, J., Lundin, J., Pettersson, M., Nilsson, D., Wincent, J., Lieden, A., Vezzi, F., Wirta, Valtteri, Käller, Max, Duelund, T., Houssari, R., Pignata, L., Bak, M., Tommerup, N., Lundberg, E. S., Tumer, Z., and Lindstrand, A.

Abstract

QC 20200312

Published
2018

24. Replicative and non-replicative mechanisms in the formation of clustered CNVs are indicated by whole genome characterization

Author

Nazaryan-Petersen, Lusine, Eisfeldt, Jesper, Pettersson, Maria, Lundin, Johanna, Nilsson, Daniel, Wincent, Josephine, Lieden, Agne, Lovmar, Lovisa, Ottosson, Jesper, Gacic, Jelena, Makitie, Outi, Nordgren, Ann, Vezzi, Francesco, Wirta, Valtteri, Käller, Max, Hjortshoj, Tina Duelund, Jespersgaard, Cathrine, Houssari, Rayan, Pignata, Laura, Bak, Mads, Tommerup, Niels, Lundberg, Elisabeth Syk, Tumer, Zeynep, Lindstrand, Anna, Nazaryan-Petersen, Lusine, Eisfeldt, Jesper, Pettersson, Maria, Lundin, Johanna, Nilsson, Daniel, Wincent, Josephine, Lieden, Agne, Lovmar, Lovisa, Ottosson, Jesper, Gacic, Jelena, Makitie, Outi, Nordgren, Ann, Vezzi, Francesco, Wirta, Valtteri, Käller, Max, Hjortshoj, Tina Duelund, Jespersgaard, Cathrine, Houssari, Rayan, Pignata, Laura, Bak, Mads, Tommerup, Niels, Lundberg, Elisabeth Syk, Tumer, Zeynep, and Lindstrand, Anna

Abstract

Clustered copy number variants (CNVs) as detected by chromosomal microarray analysis (CMA) are often reported as germline chromothripsis. However, such cases might need further investigations by massive parallel whole genome sequencing (WGS) in order to accurately define the underlying complex rearrangement, predict the occurrence mechanisms and identify additional complexities. Here, we utilized WGS to delineate the rearrangement structure of 21 clustered CNV carriers first investigated by CMA and identified a total of 83 breakpoint junctions (BPJs). The rearrangements were further sub-classified depending on the patterns observed: I) Cases with only deletions (n = 8) often had additional structural rearrangements, such as insertions and inversions typical to chromothripsis; II) cases with only duplications (n = 7) or III) combinations of deletions and duplications (n = 6) demonstrated mostly interspersed duplications and BPJs enriched with microhomology. In two cases the rearrangement mutational signatures indicated both a breakage-fusion-bridge cycle process and haltered formation of a ring chromosome. Finally, we observed two cases with Alu- and LINE-mediated rearrangements as well as two unrelated individuals with seemingly identical clustered CNVs on 2p25.3, possibly a rare European founder rearrangement. In conclusion, through detailed characterization of the derivative chromosomes we show that multiple mechanisms are likely involved in the formation of clustered CNVs and add further evidence for chromoanagenesis mechanisms in both "simple" and highly complex chromosomal rearrangements. Finally, WGS characterization adds positional information, important for a correct clinical interpretation and deciphering mechanisms involved in the formation of these rearrangements., QC 20190110

Published
2018
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25. Replicative and non-replicative mechanisms in the formation of clustered CNVs are indicated by whole genome characterization

Author

Nazaryan-Petersen, Lusine, primary, Eisfeldt, Jesper, additional, Pettersson, Maria, additional, Lundin, Johanna, additional, Nilsson, Daniel, additional, Wincent, Josephine, additional, Lieden, Agne, additional, Lovmar, Lovisa, additional, Ottosson, Jesper, additional, Gacic, Jelena, additional, Mäkitie, Outi, additional, Nordgren, Ann, additional, Vezzi, Francesco, additional, Wirta, Valtteri, additional, Käller, Max, additional, Hjortshøj, Tina Duelund, additional, Jespersgaard, Cathrine, additional, Houssari, Rayan, additional, Pignata, Laura, additional, Bak, Mads, additional, Tommerup, Niels, additional, Lundberg, Elisabeth Syk, additional, Tümer, Zeynep, additional, and Lindstrand, Anna, additional

Published
2018
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28. Whole genome characterization of array defined clustered CNVs reveals two distinct complex rearrangement subclasses generated through either non homologous repair or template switching

Author

Eisfeldt, Jesper, Nazaryan-Petersen, Lusine, Lundin, Johanna Lundin, Pettersson, Maria, Nilsson, Daniel, Wincent, Josephine, Lieden, Agne, Vezzi, Francesco, Wirta, Valteri, Käller, Max, Duelund, Tina, Houssari, Rayan, Pignata, Laura, Bak, Mads, Tommerup, Niels, Lundberg, Elisabeth Syk, Tumer, Zeynep, Lindstrand, Anna, Eisfeldt, Jesper, Nazaryan-Petersen, Lusine, Lundin, Johanna Lundin, Pettersson, Maria, Nilsson, Daniel, Wincent, Josephine, Lieden, Agne, Vezzi, Francesco, Wirta, Valteri, Käller, Max, Duelund, Tina, Houssari, Rayan, Pignata, Laura, Bak, Mads, Tommerup, Niels, Lundberg, Elisabeth Syk, Tumer, Zeynep, and Lindstrand, Anna

Abstract

QC 20171013

Published
2017

30. Deletion of Wiskott-Aldrich syndrome protein triggers Rac2 activity and increased cross-presentation by dendritic cells

Author

Baptista, Marisa A. P., Keszei, Marton, Oliveira, Mariana, Sunahara, Karen K. S., Andersson, John, Dahlberg, Carin I. M., Worth, Austen J., Lieden, Agne, Kuo, I-Chun, Wallin, Robert P. A., Snapper, Scott B., Eidsmo, Liv, Scheynius, Annika, Karlsson, Mikael C. I., Bouma, Gerben, Burns, Siobhan O., Forsell, Mattias N. E., Thrasher, Adrian J., Nylén, Susanne, Westerberg, Lisa S., Baptista, Marisa A. P., Keszei, Marton, Oliveira, Mariana, Sunahara, Karen K. S., Andersson, John, Dahlberg, Carin I. M., Worth, Austen J., Lieden, Agne, Kuo, I-Chun, Wallin, Robert P. A., Snapper, Scott B., Eidsmo, Liv, Scheynius, Annika, Karlsson, Mikael C. I., Bouma, Gerben, Burns, Siobhan O., Forsell, Mattias N. E., Thrasher, Adrian J., Nylén, Susanne, and Westerberg, Lisa S.

Abstract

Wiskott-Aldrich syndrome (WAS) is caused by loss-of-function mutations in the WASp gene. Decreased cellular responses in WASp-deficient cells have been interpreted to mean that WASp directly regulates these responses in WASp-sufficient cells. Here, we identify an exception to this concept and show that WASp-deficient dendritic cells have increased activation of Rac2 that support cross-presentation to CD8(+) T cells. Using two different skin pathology models, WASp-deficient mice show an accumulation of dendritic cells in the skin and increased expansion of IFN gamma-producing CD8(+) T cells in the draining lymph node and spleen. Specific deletion of WASp in dendritic cells leads to marked expansion of CD8(+) T cells at the expense of CD4(+) T cells. WASp-deficient dendritic cells induce increased cross-presentation to CD8(+) T cells by activating Rac2 that maintains a near neutral pH of phagosomes. Our data reveals an intricate balance between activation of WASp and Rac2 signalling pathways in dendritic cells.

Published
2016
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31. Small 6q16.1 deletions encompassing POU3F2 cause susceptibility to obesity and variable developmental delay with intellectual disability

Author

Kasher, Paul R., Shertz, Katherine E., Thomas, Megan, Jackson, Adam, Annunziata, Silvia, Ballesta-Martinez, Maria J., Campeau, Philippe M., Clayton, Peter E., Eaton, Jennifer L., Granata, Tiziana, Guille-Navarro, Encarna, Hernando, Cristina, Laverriere, Caroline E., Lieden, Agne, Villa-Marcos, Olaya, McEntagart, Meriel, Nordgren, Ann, Pantaleonie, Chiara, Prebel-Richard, Celine, Sarret, Catherine, Sciacca, Francesca L., Wright, Ronnie, Kerr, Bronwyn, Glasgow, Eric, Banka, Siddharth, Kasher, Paul R., Shertz, Katherine E., Thomas, Megan, Jackson, Adam, Annunziata, Silvia, Ballesta-Martinez, Maria J., Campeau, Philippe M., Clayton, Peter E., Eaton, Jennifer L., Granata, Tiziana, Guille-Navarro, Encarna, Hernando, Cristina, Laverriere, Caroline E., Lieden, Agne, Villa-Marcos, Olaya, McEntagart, Meriel, Nordgren, Ann, Pantaleonie, Chiara, Prebel-Richard, Celine, Sarret, Catherine, Sciacca, Francesca L., Wright, Ronnie, Kerr, Bronwyn, Glasgow, Eric, and Banka, Siddharth

Abstract

Genetic studies of intellectual disability and identification of monogenic causes of obesity in humans have made immense contribution toward the understanding of the brain and control of body mass. The leptin > melanocortin > SIM1 pathway is dysregulated in multiple monogenic human obesity syndromes but its downstream targets are still unknown. In ten individuals from six families, with overlapping 6q16.1 deletions, we describe a disorder of variable developmental delay, intellectual disability, and susceptibility to obesity and hyperphagia. The 6q16.1 deletions segregated with the phenotype in multiplex families and were shown to be de novo in four families, and there was dramatic phenotypic overlap among affected individuals who were independently ascertained without bias from clinical features. Analysis of the deletions revealed a ∼350 kb critical region on chromosome 6q16.1 that encompasses a gene for proneuronal transcription factor POU3F2, which is important for hypothalamic development and function. Using morpholino and mutant zebrafish models, we show that POU3F2 lies downstream of SIM1 and controls oxytocin expression in the hypothalamic neuroendocrine preoptic area. We show that this finding is consistent with the expression patterns of POU3F2 and related genes in the human brain. Our work helps to further delineate the neuro-endocrine control of energy balance/body mass and demonstrates that this molecular pathway is conserved across multiple species.

Published
2016

32. Plasma Fibronectin Deficiency during Chemotherapy of Acute Myeloid Leukaemia

Author

Gudrun Lieden, Brodin B, Olle Vikrot, and Claes Malm

Subjects
Adult, Male, Fever, medicine.medical_treatment, hemic and lymphatic diseases, Plasma fibronectin deficiency, Bronchopneumonia, medicine, Humans, Thioguanine, Aged, Chemotherapy, Innate immune system, biology, business.industry, Daunorubicin, Cytarabine, Normal level, Hematology, Middle Aged, Fibronectins, Fibronectin, Leukemia, Myeloid, Acute, Immunology, biology.protein, Female, Myeloid leukaemia, business
Abstract

Plasma fibronectin was determined using a laser nephelometric method in 10 patients with acute myeloid leukaemia undergoing chemotherapy. There was a continuous fall during the first 3 weeks to about 50% of the normal level. The decrease of fibronectin may contribute to the lowered resistance against infection characteristic of these patients.

Published
2009
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33. Vitamin D levels and atopic eczema in infancy and early childhood in Norway: a cohort study

Author

Berents, T.L., primary, Lødrup Carlsen, K.C., additional, Mowinckel, P., additional, Sandvik, L., additional, Skjerven, H.O., additional, Rolfsjord, L.B., additional, Kvenshagen, B., additional, Hunderi, J.O.G., additional, Bradley, M., additional, Lieden, A., additional, Carlsen, K.‐H., additional, Thorsby, P.M., additional, and Gjersvik, P., additional

Published
2016
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34. Rare copy number variants are common in young children with autism spectrum disorder

Author

Eriksson, Mats Anders, Lieden, Agne, Westerlund, Joakim, Bremer, Anna, Wincent, Josephine, Sahlin, Ellika, Gillberg, Christopher, Fernell, Elisabeth, Anderlid, Britt-Marie, Eriksson, Mats Anders, Lieden, Agne, Westerlund, Joakim, Bremer, Anna, Wincent, Josephine, Sahlin, Ellika, Gillberg, Christopher, Fernell, Elisabeth, and Anderlid, Britt-Marie

Abstract

AimSeveral studies have suggested that rare copy number variants (CNVs) are an important genetic contributor to autism spectrum disorders. The aims of the study were to use chromosomal microarray to investigate the presence of rare copy number variants in a population-based cohort of well-characterised young children with autism spectrum disorders and to relate the genetic results to neurodevelopmental profiles and medical conditions. MethodsWe performed chromosomal microarray on samples from 162 children who had been referred to the Stockholm Autism Centre for Young Children in Sweden after being diagnosed with autism spectrum disorder between 20 and 54months of age. ResultsPathogenic aberrations were detected in 8.6% of the children and variants of uncertain significance were present in another 8.6%. CNVs were more frequent in children with congenital malformations or dysmorphic features as well as in the subgroup with intellectual disability. ConclusionOur results support the use of chromosomal microarray methods for the first tier genetic analysis of autism spectrum disorder. However, it is likely in the near future that chromosomal microarray methods will probably be replaced by whole-exome and whole-genome sequencing technologies in clinical genetic testing.

Published
2015
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35. Rare copy number variants are common in young children with autism spectrum disorder

Author

Anders Eriksson, Mats, Lieden, Agne, Westerlund, Joakim, Bremer, Anna, Wincent, Josephine, Sahlin, Ellika, Gillberg, Christopher, Fernell, Elisabeth, Anderlid, Britt-Marie, Anders Eriksson, Mats, Lieden, Agne, Westerlund, Joakim, Bremer, Anna, Wincent, Josephine, Sahlin, Ellika, Gillberg, Christopher, Fernell, Elisabeth, and Anderlid, Britt-Marie

Abstract

AimSeveral studies have suggested that rare copy number variants (CNVs) are an important genetic contributor to autism spectrum disorders. The aims of the study were to use chromosomal microarray to investigate the presence of rare copy number variants in a population-based cohort of well-characterised young children with autism spectrum disorders and to relate the genetic results to neurodevelopmental profiles and medical conditions. MethodsWe performed chromosomal microarray on samples from 162 children who had been referred to the Stockholm Autism Centre for Young Children in Sweden after being diagnosed with autism spectrum disorder between 20 and 54months of age. ResultsPathogenic aberrations were detected in 8.6% of the children and variants of uncertain significance were present in another 8.6%. CNVs were more frequent in children with congenital malformations or dysmorphic features as well as in the subgroup with intellectual disability. ConclusionOur results support the use of chromosomal microarray methods for the first tier genetic analysis of autism spectrum disorder. However, it is likely in the near future that chromosomal microarray methods will probably be replaced by whole-exome and whole-genome sequencing technologies in clinical genetic testing., Funding Agencies|Swedish Research Council; Stockholm City Council; Frimurare Barnhuset Foundation; Linnea and Josef Carlsson Foundation; Kronprinsessan Lovisas Foundation; Sunnerdahls Foundation; Samariten Foundation; Karolinska Institutet Center of Neurodevelopmental Disorders; Gillberg Neuropsychiatry Centre, Sahlgrenska Academy, University of Gothenburg

Published
2015
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36. The goitrogenic effect of two Sudanese pearl millet cultivars in rats

Author

Leif Hambraeus, Sami A. Khalid, M Eltom, Pierre Bourdoux, A Elnour, and S.-A. Lieden

Subjects
endocrine system, medicine.medical_specialty, Nutrition and Dietetics, Goiter, endocrine system diseases, biology, business.industry, Endocrinology, Diabetes and Metabolism, Thyroid, food and beverages, medicine.disease, biology.organism_classification, Iodine deficiency, Endocrinology, Animal science, Blood serum, medicine.anatomical_structure, Internal medicine, medicine, Cultivar, Thyroid function, Goitrogen, business, Pennisetum
Abstract

Pearl millet ( Pennisetum americanum L. Lecke) is the staple food in many goiter areas in the west of Sudan while wheat is an additional staple food in low goiter areas. Epidemiological evidence from these areas suggests that although iodine deficiency is the major cause of goiter, millet consumption may play a role in goiter causation. This study was designed to determine in rats the possible goitrogenic and antithyroid effects of two millet cultivars, Bayoda and Balady, consumed in two endemic goiter areas with different goiter prevalence rates in the west of Sudan. Both fermented and unfermented forms of the two cultivars of millet were included in the study. Whole grain millet and wheat used in this experiment were only fortified with iodine with an amount supplying recommended dietary requirements. Feeding the two millet cultivars unfermented was associated with serum thyroid hormones comparable with the wheat reference while feeding the Balady cultivar (consumed in the area of low goiter prevalence) unfermented was associated with significant enlargement of the thyroid gland. Fermentation, was associated with the same trend of changes in both cultivars: enlargement of the thyroid gland and increased serum T4, T3 and TSH. Compared to the wheat reference group, fermentation of the cultivars was associated with increased serum T3 and T4 (only Bayoda) and significant further enlargement of the thyroid gland (only Balady). Among the animals that consumed millet (two way analysis), those receiving fermented millet showed increased serum T4, T3 and TSH compared to those which received unfermented millet. Nutritional inadequacies reflected in impaired growth, and enlarged heart and kidneys were more pronounced in animals fed millet diets than in those fed the wheat reference diet. In conclusion, in rats, the consumption of millet interferes with thyroid function; the consumption of Balady seems to induce an enlargement of the gland whereas the consumption of Bayoda causes modifications in the pattern of thyroid hormones.

Published
1997
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37. Skin Barrier Function and Staphylococcus aureus Colonization in Vestibulum Nasi and Fauces in Healthy Infants and Infants with Eczema: A Population-Based Cohort Study

Author

Berents, Teresa Løvold, primary, Carlsen, Karin Cecilie Lødrup, additional, Mowinckel, Petter, additional, Skjerven, Håvard Ove, additional, Kvenshagen, Bente, additional, Rolfsjord, Leif Bjarte, additional, Bradley, Maria, additional, Lieden, Agne, additional, Carlsen, Kai-Håkon, additional, Gaustad, Peter, additional, and Gjersvik, Petter, additional

Published
2015
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39. Nasal speech and hypothyroidism are common hallmarks of 12q15 microdeletions.

Author

Vergult, S., Krgovic, D., Loeys, B.L., Lyonnet, S., Lieden, A., Anderlid, B.M., Sharkey, F., Joss, S., Mortier, G., Menten, B., Vergult, S., Krgovic, D., Loeys, B.L., Lyonnet, S., Lieden, A., Anderlid, B.M., Sharkey, F., Joss, S., Mortier, G., and Menten, B.

Abstract

Item does not contain fulltext

Published
2011

40. Traditional fermentation increases goitrogenic activity in pearl millet

Author

M Eltom, Leif Hambraeus, A Elnour, Sami A. Khalid, Pierre Bourdoux, and S.-A. Lieden

Subjects
Male, Food intake, medicine.medical_specialty, Thyroid Gland, Medicine (miscellaneous), engineering.material, Biology, Panicum, Weight Gain, Toxicology, Rats, Sprague-Dawley, Calcification, Physiologic, Internal medicine, medicine, Animals, Goitrogen, Minerals, Nutrition and Dietetics, food and beverages, Organ Size, eye diseases, Diet, Rats, Sprague dawley, Endocrinology, Fermentation, engineering, Dietary Proteins, Energy Metabolism, Pearl, Goiter, Endemic, Iodine
Abstract

Epidemiological evidence suggests that millet might play a role in the etiology of endemic goiter. Recently, we showed that a traditional fermentation procedure of two pearl millet (Pennisetum americanum L. Lecke) cultivars grown in Sudan modified their effects on the weight of the thyroid gland and thyroid hormone profile in rats. In the present study, we report that this fermentation procedure reduced the ash contents of millet by about 40% and removed considerable amounts of Mg (>50%), Zn (27–39%) and K (45%). Other minerals (Ca, Fe, Cu) were not affected. Feeding of one fermented cultivar resulted in significant reduction in bone Mg and Zn contents, whereas feeding of the other fermented cultivar resulted in reduction of bone Mg only. Dietary Mg intake and bone Mg contents correlated negatively with serum T3. Groups fed the millet diets had higher serum Se level compared to those fed wheat or casein diets and feeding of fermented millet resulted in a further increase in serum Se level. Thus our data indicate that in rats the enhanced effects of millet on the thyroid induced by fermentation is likely related to removal of minerals from millet and/or chemical transformation of the goitrogens contained in millet.

Published
1999

46. Acknowledgement to the 1998 Reviewers

Author

Masahiro Nomura, Anna Nagyova, Maria Lúcia Zaidan Dagli, Sadaichi Sakamoto, Sami A. Khalid, Leif Hambraeus, P. Barraza, Primavera Borelli, Paweł Maćkowiak, Marica Kudláčková, Riitta Korpela, Yasuharu Niwa, M Eltom, Katarzyna Kandulska, Hideki Matoba, S.-A. Lieden, Masako Iwamoto, I. P. Souza, Tomasz Szkudelski, Leszek Nogowski, Tsutomu Hara, Mariane Lutz, Kazuko Okada, Ulla Teuri, S. Bonilla, Tatiana Magálová, José Alvarado, Pierre Bourdoux, Yutaka Nakaya, Masaharu Ohnaka, Hyen-Wook Kang, Elena Grančičová, Krzysztof W. Nowak, Masataka Kusonoki, J. Concha, A Elnour, Kimiko Nakayasu, and Radovan Borojevic

Subjects
Gerontology, Medical education, medicine.medical_specialty, Nutrition and Dietetics, business.industry, Acknowledgement, Alternative medicine, medicine, Medicine (miscellaneous), business
Published
1998
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48. Plasmapheresis in the initial treatment of insulin-dependent diabetes mellitus in children

Author

L. G. Heding, Åke Lernmark, B. Marner, Johnny Ludvigsson, and G. Lieden

Subjects
Male, medicine.medical_specialty, Time Factors, Adolescent, medicine.medical_treatment, Disease, Gastroenterology, Islets of Langerhans, chemistry.chemical_compound, Internal medicine, Diabetes mellitus, medicine, Humans, Insulin, Child, Autoantibodies, General Environmental Science, geography, geography.geographical_feature_category, C-Peptide, C-peptide, business.industry, General Engineering, Autoantibody, Plasmapheresis, General Medicine, medicine.disease, Islet, Diabetes Mellitus, Type 1, Endocrinology, chemistry, Etiology, General Earth and Planetary Sciences, Female, business, Research Article
Abstract

Several factors indicate that autoimmune mechanisms may play a part in the aetiology of insulin-dependent diabetes mellitus. At the onset of the disease in 10 children (aged 11-16 years) plasmapheresis was performed four times over one to two weeks. Seventeen age-matched children with the same clinical features served as controls. The C-peptide concentrations at onset were the same in the two groups, but after one month the children treated with plasmapheresis had significantly higher values. This difference became even more pronounced after three, nine, and 18 months, both during fasting and at the maximum response to a standardised meal. The study group also had a significantly more stable metabolism, longer partial remission, and no higher insulin requirement. Of the 10 treated children islet-cell cytoplasmic antibodies were present in seven before plasmapheresis and in nine during treatment. The antibodies remained detectable in five and six out of nine patients at one and six months respectively after plasmapheresis. Although the mechanisms are obscure, plasmapheresis performed at the onset of insulin-dependent diabetes mellitus may help to preserve beta-cell function.

Published
1983
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50. Thyroid Function After Thermal Trauma

Author

Smeds, S., Kagedal, B., Lieden, G., and Liljedahl, S. -O.

Abstract

The thyroid function was analyzed for 4-6 weeks in a prospective study on 12 thermally injured patients. The burn size range was 15-90%. Serum concentrations of 3,5,3'-triidothyronine (T3) was suppressed and 3,3',5'-triidothyronine (rT3) was increased. The ratio T3/rT3 was subnormal on the third day after the trauma and normalized after 3 weeks. Thyroxine and the free T4-index were within the normal range. The free T3-index were within the normal range. The TSH concentration was initially low but slowly increasing during the period of study. The concentration of the thyroxine-binding globulin (TBG) varied within the normal range. The T3 resin uptake test varied inversely with the TBG concentration. The concentration of thyroxine-binding prealbumin (TBPA) was subnormal. A control experiment excluded possible interference on the hormone concentrations of administered donor blood and plasma. It is concluded that the thyroid hormones are not responsible for the posttraumatic hypermetabolism in burn injury. The present findings further indicate a depletion of metabolically active thyroid hormones at the cellular level after burn injury.

Published
1981
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