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1. KIF1A variants are a frequent cause of autosomal dominant hereditary spastic paraplegia

Author

Pennings, Maartje, Schouten, Meyke I., van Gaalen, Judith, Meijer, Rowdy P. P., de Bot, Susanne T., Kriek, Marjolein, Saris, Christiaan G. J., van den Berg, Leonard H., van Es, Michael A., Zuidgeest, Dick M. H., Elting, Mariet W., van de Kamp, Jiddeke M., van Spaendonck-Zwarts, Karin Y., Die-Smulders, Christine de, Brilstra, Eva H., Verschuuren, Corien C., de Vries, Bert B. A., Bruijn, Jacques, Sofou, Kalliopi, Duijkers, Floor A., Jaeger, B., Schieving, Jolanda H., van de Warrenburg, Bart P., and Kamsteeg, Erik-Jan

Published
2020
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5. Ultrasound and MR muscle imaging in new onset idiopathic inflammatory myopathies at diagnosis and after treatment: a comparative pilot study

Author

Walter, Anne W, primary, Lim, Johan, additional, Raaphorst, Joost, additional, Smithuis, Frank F, additional, den Harder, J Michiel, additional, Eftimov, Filip, additional, Potters, Wouter, additional, Saris, Christiaan G J, additional, de Visser, Marianne, additional, van Schaik, Ivo N, additional, de Haan, Rob J, additional, van der Kooi, Anneke J, additional, and Verhamme, Camiel, additional

Published
2022
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6. Reduced Expression of the Kinesin-Associated Protein 3 (KIFAP3) Gene Increases Survival in Sporadic Amyotrophic Lateral Sclerosis

Author

Landers, John E., Melki, Judith, Meininger, Vincent, Glass, Jonathan D., van den Berg, Leonard H., van Es, Michael A., Sapp, Peter C., van Vught, Paul W. J., McKenna-Yasek, Diane M., Blauw, Hylke M., Cho, Ting-Jan, Polak, Meraida, Shi, Lijia, Wills, Anne-Marie, Broom, Wendy J., Ticozzi, Nicola, Silani, Vincenzo, Ozoguz, Aslihan, Rodriguez-Leyva, Ildefonso, Veldink, Jan H., Ivinson, Adrian J., Saris, Christiaan G. J., Hosier, Betsy A., Bames-Nessa, Alayna, Couture, Nicole, Wokke, John H. J., Kwiatkowski,, Thomas J., Ophoff, Roel A., Cronin, Simon, Hardiman, Orla, Diekstra, Frank P., Leigh, P. Nigel, Shaw, Christopher E., Simpson, Claire L., Hansen, Valerie K., Powell, John F., Corcia, Philippe, Salachas, François, Heath, Simon, Galan, Pilar, Georges, Franck, Horvitz, H. Robert, Lathrop, Mark, Purcell, Shaun, Al-Chalabi, Ammar, Brown,, Robert H., and Housman, David E.

Published
2009
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8. Ultrasound and MR muscle imaging in new onset idiopathic inflammatory myopathies at diagnosis and after treatment: a comparative pilot study.

Author

Walter, Anne W, Lim, Johan, Raaphorst, Joost, Smithuis, Frank F, Harder, J Michiel den, Eftimov, Filip, Potters, Wouter, Saris, Christiaan G J, Visser, Marianne de, Schaik, Ivo N van, Haan, Rob J de, Kooi, Anneke J van der, and Verhamme, Camiel

Subjects
DIAGNOSIS of muscle diseases, MUSCLE diseases, PILOT projects, ULTRASONIC imaging, SKELETAL muscle, IMMUNOGLOBULINS, INTRAVENOUS therapy, MAGNETIC resonance imaging, QUANTITATIVE research, COMPARATIVE studies, QUALITATIVE research, DESCRIPTIVE statistics, SENSITIVITY & specificity (Statistics)
Abstract

Objectives To prospectively compare ultrasound (US) and whole-body MRI for detection of muscle abnormalities compatible with idiopathic inflammatory myopathies (IIM). Methods Newly diagnosed IIM patients underwent US (14 muscles) and MRI (36 muscles) at diagnosis and after nine weeks monotherapy with intravenous immunoglobulin. Muscles were compatible with IIM when quantitative US echo-intensity (EI) z scores was ≥1.5, semi-quantitative US Heckmatt score was ≥2, qualitative US was abnormal, or when MRI showed oedema on T2-weighted images. At patient level, findings were classified as abnormal when quantitative US EI z scores was >1.5 (n  = 3 muscles), >2.5 (n  = 2 muscles) or >3.5 (n  = 1 muscle), or if ≥3 muscles showed abnormalities as described above for the other diagnostic methods. Results At diagnosis, in 18 patients US of 252 muscles revealed abnormalities in 36 muscles (14%) with quantitative, in 153 (61%) with semi-quantitative and in 168 (67%) with qualitative analysis. MRI showed oedema in 476 out of 623 muscles (76%). Five patients (28%) reached abnormal classification with quantitative US, 16 (89%) with semi-quantitative and qualitative US, and all patients (100%) with MRI. Nine-week follow-up of 12 patients showed no change over time with quantitative US or MRI, and a decrease in abnormalities with semi-quantitative US (P  <0.01), and qualitative US (P  <0.01). Conclusion At diagnosis, MRI was more sensitive than US to detect muscle abnormalities compatible with IIM. Semi-quantitative US and qualitative US detected abnormalities in the majority of the patients while evaluating fewer muscles than MRI and showed change over time after nine weeks of treatment. [ABSTRACT FROM AUTHOR]

Published
2023
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9. Intravenous immunoglobulins as first-line treatment in idiopathic inflammatory myopathies: a pilot study

Author

Lim, Johan, primary, Eftimov, Filip, additional, Verhamme, Camiel, additional, Brusse, Esther, additional, Hoogendijk, Jessica E, additional, Saris, Christiaan G J, additional, Raaphorst, Joost, additional, De Haan, Rob J, additional, van Schaik, Ivo N, additional, Aronica, Eleonora, additional, de Visser, Marianne, additional, and van der Kooi, Anneke J, additional

Published
2020
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11. Nerve ultrasound for diagnosing chronic inflammatory neuropathy: a multicenter validation study

Author

Projectafdeling ALS, ZL Neuromusculaire Ziekten Medisch, Brain, Regenerative Medicine and Stem Cells, Herraets, Ingrid J T, Goedee, H Stephan, Telleman, Johan A, van Eijk, Ruben P A, Verhamme, Camiel, Saris, Christiaan G J, Eftimov, Filip, van Alfen, Nens, van Asseldonk, J Thies, Visser, Leo H, van den Berg, Leonard H, van der Pol, W Ludo, Projectafdeling ALS, ZL Neuromusculaire Ziekten Medisch, Brain, Regenerative Medicine and Stem Cells, Herraets, Ingrid J T, Goedee, H Stephan, Telleman, Johan A, van Eijk, Ruben P A, Verhamme, Camiel, Saris, Christiaan G J, Eftimov, Filip, van Alfen, Nens, van Asseldonk, J Thies, Visser, Leo H, van den Berg, Leonard H, and van der Pol, W Ludo

Published
2020

12. KIF1A variants are a frequent cause of autosomal dominant hereditary spastic paraplegia

Author

Pennings, Maartje, primary, Schouten, Meyke I., additional, van Gaalen, Judith, additional, Meijer, Rowdy P. P., additional, de Bot, Susanne T., additional, Kriek, Marjolein, additional, Saris, Christiaan G. J., additional, van den Berg, Leonard H., additional, van Es, Michael A., additional, Zuidgeest, Dick M. H., additional, Elting, Mariet W., additional, van de Kamp, Jiddeke M., additional, van Spaendonck-Zwarts, Karin Y., additional, Die-Smulders, Christine de, additional, Brilstra, Eva H., additional, Verschuuren, Corien C., additional, de Vries, Bert B. A., additional, Bruijn, Jacques, additional, Sofou, Kalliopi, additional, Duijkers, Floor A., additional, Jaeger, B., additional, Schieving, Jolanda H., additional, van de Warrenburg, Bart P., additional, and Kamsteeg, Erik-Jan, additional

Published
2019
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14. Intravenous immunoglobulins as first-line treatment in idiopathic inflammatory myopathies: a pilot study.

Author

Lim, Johan, Eftimov, Filip, Verhamme, Camiel, Brusse, Esther, Hoogendijk, Jessica E, Saris, Christiaan G J, Raaphorst, Joost, Haan, Rob J De, Schaik, Ivo N van, Aronica, Eleonora, Visser, Marianne de, and Kooi, Anneke J van der

Subjects
THERAPEUTIC use of immunoglobulins, PILOT projects, IMMUNOGLOBULINS, CONFIDENCE intervals, DISEASE duration, DESCRIPTIVE statistics, MYOSITIS, DRUG side effects
Abstract

Objectives We explored efficacy and safety of IVIg as first-line treatment in patients with an idiopathic inflammatory myopathy. Methods In this investigator-initiated phase 2 open-label study, we included 20 adults with a newly diagnosed, biopsy-proven idiopathic inflammatory myopathy, and a disease duration of less than 9 months. Patients with IBM and prior use of immunosuppressants were excluded. The standard treatment regimen consisted of IVIg (Privigen) monotherapy for 9 weeks: a loading dose (2 g/kg body weight) and two subsequent maintenance doses (1 g/kg body weight) with a 3-week interval. The primary outcome was the number of patients with at least moderate improvement on the 2016 ACR/EULAR Total Improvement Score. Secondary outcomes included time to improvement, the number of patients requiring rescue medication and serious adverse events. Results We included patients with DM (n  = 9), immune-mediated necrotizing myopathy (n  = 6), non-specific myositis/overlap myositis (n  = 4) and anti-synthetase syndrome (n  = 1). One patient was excluded from analyses because of minimal weakness resulting in a ceiling effect. Eight patients (8/19 = 42.0%; Clopper–Pearson 95% CI: 19.6, 64.6) had at least moderate improvement by 9 weeks. Of these, six reached improvement by 3 weeks. Seven patients required rescue medication due to insufficient efficacy and prematurely ended the study. Three serious adverse events occurred, of which one was pulmonary embolism. Conclusion First-line IVIg monotherapy led to at least moderate improvement in nearly half of patients with a fast clinical response in the majority of responders. Trial registration Netherlands Trial Register identifier, NTR6160. [ABSTRACT FROM AUTHOR]

Published
2021
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16. Effect of Mexiletine on Muscle Stiffness in Patients With Nondystrophic Myotonia Evaluated Using Aggregated N-of-1 Trials

Author

Stunnenberg, Bas C., primary, Raaphorst, Joost, additional, Groenewoud, Hans M., additional, Statland, Jeffrey M., additional, Griggs, Robert C., additional, Woertman, Willem, additional, Stegeman, Dick F., additional, Timmermans, Janneke, additional, Trivedi, Jaya, additional, Matthews, Emma, additional, Saris, Christiaan G. J., additional, Schouwenberg, Bas J., additional, Drost, Gea, additional, van Engelen, Baziel G. M., additional, and van der Wilt, Gert Jan, additional

Published
2018
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17. Whole blood transcriptome analysis in amyotrophic lateral sclerosis: A biomarker study

Author

van Rheenen, Wouter, primary, Diekstra, Frank P., additional, Harschnitz, Oliver, additional, Westeneng, Henk-Jan, additional, van Eijk, Kristel R., additional, Saris, Christiaan G. J., additional, Groen, Ewout J. N., additional, van Es, Michael A., additional, Blauw, Hylke M., additional, van Vught, Paul W. J., additional, Veldink, Jan H., additional, and van den Berg, Leonard H., additional

Published
2018
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18. Autoantibodies to Cytosolic 5′-Nucleotidase 1A in Primary Sjögren’s Syndrome and Systemic Lupus Erythematosus

Author

Rietveld, Anke, primary, van den Hoogen, Luuk L., additional, Bizzaro, Nicola, additional, Blokland, Sofie L. M., additional, Dähnrich, Cornelia, additional, Gottenberg, Jacques-Eric, additional, Houen, Gunnar, additional, Johannsen, Nora, additional, Mandl, Thomas, additional, Meyer, Alain, additional, Nielsen, Christoffer T., additional, Olsson, Peter, additional, van Roon, Joel, additional, Schlumberger, Wolfgang, additional, van Engelen, Baziel G. M., additional, Saris, Christiaan G. J., additional, and Pruijn, Ger J. M., additional

Published
2018
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20. KIF1Avariants are a frequent cause of autosomal dominant hereditary spastic paraplegia

Author

Pennings, Maartje, Schouten, Meyke I., van Gaalen, Judith, Meijer, Rowdy P. P., de Bot, Susanne T., Kriek, Marjolein, Saris, Christiaan G. J., van den Berg, Leonard H., van Es, Michael A., Zuidgeest, Dick M. H., Elting, Mariet W., van de Kamp, Jiddeke M., van Spaendonck-Zwarts, Karin Y., Die-Smulders, Christine de, Brilstra, Eva H., Verschuuren, Corien C., de Vries, Bert B. A., Bruijn, Jacques, Sofou, Kalliopi, Duijkers, Floor A., Jaeger, B., Schieving, Jolanda H., van de Warrenburg, Bart P., and Kamsteeg, Erik-Jan

Abstract

Variants in the KIF1Agene can cause autosomal recessive spastic paraplegia 30, autosomal recessive hereditary sensory neuropathy, or autosomal (de novo) dominant mental retardation type 9. More recently, variants in KIF1Ahave also been described in a few cases with autosomal dominant spastic paraplegia. Here, we describe 20 KIF1Avariants in 24 patients from a clinical exome sequencing cohort of 347 individuals with a mostly ‘pure’ spastic paraplegia. In these patients, spastic paraplegia was slowly progressive and mostly pure, but with a highly variable disease onset (0–57 years). Segregation analyses showed a de novo occurrence in seven cases, and a dominant inheritance pattern in 11 families. The motor domain of KIF1A is a hotspot for disease causing variants in autosomal dominant spastic paraplegia, similar to mental retardation type 9 and recessive spastic paraplegia type 30. However, unlike these allelic disorders, dominant spastic paraplegia was also caused by loss-of-function variants outside this domain in six families. Finally, three missense variants were outside the motor domain and need further characterization. In conclusion, KIF1Avariants are a frequent cause of autosomal dominant spastic paraplegia in our cohort (6–7%). The identification of KIF1Aloss-of-function variants suggests haploinsufficiency as a possible mechanism in autosomal dominant spastic paraplegia.

Published
2020
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21. Analysis of the KIFAP3 gene in amyotrophic lateral sclerosis : a multicenter survival study

Author

Van Doormaal, Perry T. C., Ticozzi, Nicola, Gellera, Cinzia, Ratti, Antonia, Taroni, Franco, Chio, Adriano, Calvo, Andrea, Mora, Gabriele, Restagno, Gabriella, Traynor, Bryan J., Birve, Anna, Lemmens, Robin, Van Es, Michael A., Saris, Christiaan G. J., Blauw, Hylke M., Van Vught, Paul W. J., Groen, Ewout J. N., Corrado, Lucia, Mazzini, Letizia, Del Bo, Roberto, Corti, Stefania, Waibel, Stefan, Meyer, Thomas, Ludolph, Albert C., Goris, An, Van Damme, Philip, Robberecht, Wim, Shatunov, Aleksey, Fogh, Isabella, Andersen, Peter M., D'Alfonso, Sandra, Hardiman, Orla, Cronin, Simon, Rujescu, Dan, Al-Chalabi, Ammar, Landers, John E., Silani, Vincenzo, Van den Berg, Leonard H., Veldink, Jan H., Van Doormaal, Perry T. C., Ticozzi, Nicola, Gellera, Cinzia, Ratti, Antonia, Taroni, Franco, Chio, Adriano, Calvo, Andrea, Mora, Gabriele, Restagno, Gabriella, Traynor, Bryan J., Birve, Anna, Lemmens, Robin, Van Es, Michael A., Saris, Christiaan G. J., Blauw, Hylke M., Van Vught, Paul W. J., Groen, Ewout J. N., Corrado, Lucia, Mazzini, Letizia, Del Bo, Roberto, Corti, Stefania, Waibel, Stefan, Meyer, Thomas, Ludolph, Albert C., Goris, An, Van Damme, Philip, Robberecht, Wim, Shatunov, Aleksey, Fogh, Isabella, Andersen, Peter M., D'Alfonso, Sandra, Hardiman, Orla, Cronin, Simon, Rujescu, Dan, Al-Chalabi, Ammar, Landers, John E., Silani, Vincenzo, Van den Berg, Leonard H., and Veldink, Jan H.

Published
2014
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22. Mapping of Gene Expression Reveals CYP27A1 as a Susceptibility Gene for Sporadic ALS

Author

Diekstra, Frank P., Saris, Christiaan G. J., van Rheenen, Wouter, Franke, Lude, Jansen, Ritsert C., van Es, Michael A., van Vught, Paul W. J., Blauw, Hylke M., Groen, Ewout J. N., Horvath, Steve, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G., Robberecht, Wim, Andersen, Peter M., Melki, Judith, Meininger, Vincent, Hardiman, Orla, Landers, John E., Brown, Robert H., Jr., Shatunov, Aleksey, Shaw, Christopher E., Leigh, P. Nigel, Al-Chalabi, Ammar, Ophoff, Roel A., van den Berg, Leonard H., Veldink, Jan H., Diekstra, Frank P., Saris, Christiaan G. J., van Rheenen, Wouter, Franke, Lude, Jansen, Ritsert C., van Es, Michael A., van Vught, Paul W. J., Blauw, Hylke M., Groen, Ewout J. N., Horvath, Steve, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G., Robberecht, Wim, Andersen, Peter M., Melki, Judith, Meininger, Vincent, Hardiman, Orla, Landers, John E., Brown, Robert H., Jr., Shatunov, Aleksey, Shaw, Christopher E., Leigh, P. Nigel, Al-Chalabi, Ammar, Ophoff, Roel A., van den Berg, Leonard H., and Veldink, Jan H.

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, neurodegenerative disease characterized by loss of upper and lower motor neurons. ALS is considered to be a complex trait and genome-wide association studies (GWAS) have implicated a few susceptibility loci. However, many more causal loci remain to be discovered. Since it has been shown that genetic variants associated with complex traits are more likely to be eQTLs than frequency-matched variants from GWAS platforms, we conducted a two-stage genome-wide screening for eQTLs associated with ALS. In addition, we applied an eQTL analysis to finemap association loci. Expression profiles using peripheral blood of 323 sporadic ALS patients and 413 controls were mapped to genome-wide genotyping data. Subsequently, data from a two-stage GWAS (3,568 patients and 10,163 controls) were used to prioritize eQTLs identified in the first stage (162 ALS, 207 controls). These prioritized eQTLs were carried forward to the second sample with both gene-expression and genotyping data (161 ALS, 206 controls). Replicated eQTL SNPs were then tested for association in the second-stage GWAS data to find SNPs associated with disease, that survived correction for multiple testing. We thus identified twelve cis eQTLs with nominally significant associations in the second-stage GWAS data. Eight SNP-transcript pairs of highest significance (lowest p = 1.27 x 10(-51)) withstood multiple-testing correction in the second stage and modulated CYP27A1 gene expression. Additionally, we show that C9orf72 appears to be the only gene in the 9p21.2 locus that is regulated in cis, showing the potential of this approach in identifying causative genes in association loci in ALS. This study has identified candidate genes for sporadic ALS, most notably CYP27A1. Mutations in CYP27A1 are causal to cerebrotendinous xanthomatosis which can present as a clinical mimic of ALS with progressive upper motor neuron loss, making it a plausible susceptibility gene for ALS

Published
2012
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23. Mapping of Gene Expression Reveals CYP27A1 as a Susceptibility Gene for Sporadic ALS

Author

Brug, Marcel P. van der, Diekstra, Frank P., Saris, Christiaan G. J., van Rheenen, Wouter, Franke, Lude, Jansen, Ritsert C., van Es, Michael A., van Vught, Paul W. J., Blauw, Hylke M., Groen, Ewout J. N., Horvath, Steve, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G., Robberecht, Wim, Andersen, Peter M., Melki, Judith, Meininger, Vincent, Hardiman, Orla, Landers, John E., Brown, Robert H., Shatunov, Aleksey, Shaw, Christopher E., Leigh, P. Nigel, Al-Chalabi, Ammar, Ophoff, Roel A., van den Berg, Leonard H., Veldink, Jan H., Brown Jr., Robert H., Brug, Marcel P. van der, Diekstra, Frank P., Saris, Christiaan G. J., van Rheenen, Wouter, Franke, Lude, Jansen, Ritsert C., van Es, Michael A., van Vught, Paul W. J., Blauw, Hylke M., Groen, Ewout J. N., Horvath, Steve, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G., Robberecht, Wim, Andersen, Peter M., Melki, Judith, Meininger, Vincent, Hardiman, Orla, Landers, John E., Brown, Robert H., Shatunov, Aleksey, Shaw, Christopher E., Leigh, P. Nigel, Al-Chalabi, Ammar, Ophoff, Roel A., van den Berg, Leonard H., Veldink, Jan H., and Brown Jr., Robert H.

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, neurodegenerative disease characterized by loss of upper and lower motor neurons. ALS is considered to be a complex trait and genome-wide association studies (GWAS) have implicated a few susceptibility loci. However, many more causal loci remain to be discovered. Since it has been shown that genetic variants associated with complex traits are more likely to be eQTLs than frequency-matched variants from GWAS platforms, we conducted a two-stage genome-wide screening for eQTLs associated with ALS. In addition, we applied an eQTL analysis to finemap association loci. Expression profiles using peripheral blood of 323 sporadic ALS patients and 413 controls were mapped to genome-wide genotyping data. Subsequently, data from a two-stage GWAS (3,568 patients and 10,163 controls) were used to prioritize eQTLs identified in the first stage (162 ALS, 207 controls). These prioritized eQTLs were carried forward to the second sample with both gene-expression and genotyping data (161 ALS, 206 controls). Replicated eQTL SNPs were then tested for association in the second-stage GWAS data to find SNPs associated with disease, that survived correction for multiple testing. We thus identified twelve cis eQTLs with nominally significant associations in the second-stage GWAS data. Eight SNP-transcript pairs of highest significance (lowest p = 1.27 x 10(-51)) withstood multiple-testing correction in the second stage and modulated CYP27A1 gene expression. Additionally, we show that C9orf72 appears to be the only gene in the 9p21.2 locus that is regulated in cis, showing the potential of this approach in identifying causative genes in association loci in ALS. This study has identified candidate genes for sporadic ALS, most notably CYP27A1. Mutations in CYP27A1 are causal to cerebrotendinous xanthomatosis which can present as a clinical mimic of ALS with progressive upper motor neuron loss, making it a plausible susceptibility gene for

Published
2012

24. A large genome scan for rare CNVs in amyotrophic lateral sclerosis

Author

Blauw, Hylke M, Al-Chalabi, Ammar, Andersen, Peter M, van Vught, Paul W J, Diekstra, Frank P, van Es, Michael A, Saris, Christiaan G J, Groen, Ewout J N, van Rheenen, Wouter, Koppers, Max, Van't Slot, Ruben, Strengman, Eric, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G, Kiemeney, Lambertus A, Vermeulen, Sita H M, Birve, Anna, Waibel, Stefan, Meyer, Thomas, Cronin, Simon, McLaughlin, Russell L, Hardiman, Orla, Sapp, Peter C, Tobin, Martin D, Wain, Louise V, Tomik, Barbara, Slowik, Agnieszka, Lemmens, Robin, Rujescu, Dan, Schulte, Claudia, Gasser, Thomas, Brown, Robert H, Landers, John E, Robberecht, Wim, Ludolph, Albert C, Ophoff, Roel A, Veldink, Jan H, van den Berg, Leonard H, Blauw, Hylke M, Al-Chalabi, Ammar, Andersen, Peter M, van Vught, Paul W J, Diekstra, Frank P, van Es, Michael A, Saris, Christiaan G J, Groen, Ewout J N, van Rheenen, Wouter, Koppers, Max, Van't Slot, Ruben, Strengman, Eric, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Uitterlinden, Andre G, Kiemeney, Lambertus A, Vermeulen, Sita H M, Birve, Anna, Waibel, Stefan, Meyer, Thomas, Cronin, Simon, McLaughlin, Russell L, Hardiman, Orla, Sapp, Peter C, Tobin, Martin D, Wain, Louise V, Tomik, Barbara, Slowik, Agnieszka, Lemmens, Robin, Rujescu, Dan, Schulte, Claudia, Gasser, Thomas, Brown, Robert H, Landers, John E, Robberecht, Wim, Ludolph, Albert C, Ophoff, Roel A, Veldink, Jan H, and van den Berg, Leonard H

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease selectively affecting motor neurons in the brain and spinal cord. Recent genome-wide association studies (GWASs) have identified several common variants which increase disease susceptibility. In contrast, rare copy-number variants (CNVs), which have been associated with several neuropsychiatric traits, have not been studied for ALS in well-powered study populations. To examine the role of rare CNVs in ALS susceptibility, we conducted a CNV association study including over 19,000 individuals. In a genome-wide screen of 1875 cases and 8731 controls, we did not find evidence for a difference in global CNV burden between cases and controls. In our association analyses, we identified two loci that met our criteria for follow-up: the DPP6 locus (OR = 3.59, P = 6.6 × 10(-3)), which has already been implicated in ALS pathogenesis, and the 15q11.2 locus, containing NIPA1 (OR = 12.46, P = 9.3 × 10(-5)), the gene causing hereditary spastic paraparesis type 6 (HSP 6). We tested these loci in a replication cohort of 2559 cases and 5887 controls. Again, results were suggestive of association, but did not meet our criteria for independent replication: DPP6 locus: OR = 1.92, P = 0.097, pooled results: OR = 2.64, P = 1.4 × 10(-3); NIPA1: OR = 3.23, P = 0.041, pooled results: OR = 6.20, P = 2.2 × 10(-5)). Our results highlight DPP6 and NIPA1 as candidates for more in-depth studies. Unlike other complex neurological and psychiatric traits, rare CNVs with high effect size do not play a major role in ALS pathogenesis.

Published
2010
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25. Genome-wide association study identifies 19p13.3 (UNC13A) and 9p21.2 as susceptibility loci for sporadic amyotrophic lateral sclerosis

Author

van Es, Michael A, Veldink, Jan H, Saris, Christiaan G J, Blauw, Hylke M, van Vught, Paul W J, Birve, Anna, Lemmens, Robin, Schelhaas, Helenius J, Groen, Ewout J N, Huisman, Mark H B, van der Kooi, Anneke J, de Visser, Marianne, Dahlberg, Caroline, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Zwarts, Machiel J, van Doormaal, Perry T C, Rujescu, Dan, Strengman, Eric, Giegling, Ina, Muglia, Pierandrea, Tomik, Barbara, Slowik, Agnieszka, Uitterlinden, Andre G, Hendrich, Corinna, Waibel, Stefan, Meyer, Thomas, Ludolph, Albert C, Glass, Jonathan D, Purcell, Shaun, Cichon, Sven, Nöthen, Markus M, Wichmann, H-Erich, Schreiber, Stefan, Vermeulen, Sita H H M, Kiemeney, Lambertus A, Wokke, John H J, Cronin, Simon, McLaughlin, Russell L, Hardiman, Orla, Fumoto, Katsumi, Pasterkamp, R Jeroen, Meininger, Vincent, Melki, Judith, Leigh, P Nigel, Shaw, Christopher E, Landers, John E, Al-Chalabi, Ammar, Brown, Robert H, Robberecht, Wim, Andersen, Peter M, Ophoff, Roel A, van den Berg, Leonard H, van Es, Michael A, Veldink, Jan H, Saris, Christiaan G J, Blauw, Hylke M, van Vught, Paul W J, Birve, Anna, Lemmens, Robin, Schelhaas, Helenius J, Groen, Ewout J N, Huisman, Mark H B, van der Kooi, Anneke J, de Visser, Marianne, Dahlberg, Caroline, Estrada, Karol, Rivadeneira, Fernando, Hofman, Albert, Zwarts, Machiel J, van Doormaal, Perry T C, Rujescu, Dan, Strengman, Eric, Giegling, Ina, Muglia, Pierandrea, Tomik, Barbara, Slowik, Agnieszka, Uitterlinden, Andre G, Hendrich, Corinna, Waibel, Stefan, Meyer, Thomas, Ludolph, Albert C, Glass, Jonathan D, Purcell, Shaun, Cichon, Sven, Nöthen, Markus M, Wichmann, H-Erich, Schreiber, Stefan, Vermeulen, Sita H H M, Kiemeney, Lambertus A, Wokke, John H J, Cronin, Simon, McLaughlin, Russell L, Hardiman, Orla, Fumoto, Katsumi, Pasterkamp, R Jeroen, Meininger, Vincent, Melki, Judith, Leigh, P Nigel, Shaw, Christopher E, Landers, John E, Al-Chalabi, Ammar, Brown, Robert H, Robberecht, Wim, Andersen, Peter M, Ophoff, Roel A, and van den Berg, Leonard H

Abstract

We conducted a genome-wide association study among 2,323 individuals with sporadic amyotrophic lateral sclerosis (ALS) and 9,013 control subjects and evaluated all SNPs with P < 1.0 x 10(-4) in a second, independent cohort of 2,532 affected individuals and 5,940 controls. Analysis of the genome-wide data revealed genome-wide significance for one SNP, rs12608932, with P = 1.30 x 10(-9). This SNP showed robust replication in the second cohort (P = 1.86 x 10(-6)), and a combined analysis over the two stages yielded P = 2.53 x 10(-14). The rs12608932 SNP is located at 19p13.3 and maps to a haplotype block within the boundaries of UNC13A, which regulates the release of neurotransmitters such as glutamate at neuromuscular synapses. Follow-up of additional SNPs showed genome-wide significance for two further SNPs (rs2814707, with P = 7.45 x 10(-9), and rs3849942, with P = 1.01 x 10(-8)) in the combined analysis of both stages. These SNPs are located at chromosome 9p21.2, in a linkage region for familial ALS with frontotemporal dementia found previously in several large pedigrees.

Published
2009
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26. Genetic variation in DPP6 is associated with susceptibility to amyotrophic lateral sclerosis.

Author

van Es, Michael A, van Vught, Paul W J, Blauw, Hylke M, Franke, Lude, Saris, Christiaan G J, Van den Bosch, Ludo, de Jong, Sonja W, de Jong, Vianney, Baas, Frank, van't Slot, Ruben, Lemmens, Robin, Schelhaas, Helenius J, Birve, Anna, Sleegers, Kristel, Van Broeckhoven, Christine, Schymick, Jennifer C, Traynor, Bryan J, Wokke, John H J, Wijmenga, Cisca, Robberecht, Wim, Andersen, Peter M, Veldink, Jan H, Ophoff, Roel A, van den Berg, Leonard H, van Es, Michael A, van Vught, Paul W J, Blauw, Hylke M, Franke, Lude, Saris, Christiaan G J, Van den Bosch, Ludo, de Jong, Sonja W, de Jong, Vianney, Baas, Frank, van't Slot, Ruben, Lemmens, Robin, Schelhaas, Helenius J, Birve, Anna, Sleegers, Kristel, Van Broeckhoven, Christine, Schymick, Jennifer C, Traynor, Bryan J, Wokke, John H J, Wijmenga, Cisca, Robberecht, Wim, Andersen, Peter M, Veldink, Jan H, Ophoff, Roel A, and van den Berg, Leonard H

Abstract

We identified a SNP in the DPP6 gene that is consistently strongly associated with susceptibility to amyotrophic lateral sclerosis (ALS) in different populations of European ancestry, with an overall P value of 5.04 x 10(-8) in 1,767 cases and 1,916 healthy controls and with an odds ratio of 1.30 (95% confidence interval (CI) of 1.18-1.43). Our finding is the first report of a genome-wide significant association with sporadic ALS and may be a target for future functional studies.

Published
2008
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29. Mapping of Gene Expression Reveals CYP27A1 as a Susceptibility Gene for Sporadic ALS

Author

Diekstra, Frank P., primary, Saris, Christiaan G. J., additional, van Rheenen, Wouter, additional, Franke, Lude, additional, Jansen, Ritsert C., additional, van Es, Michael A., additional, van Vught, Paul W. J., additional, Blauw, Hylke M., additional, Groen, Ewout J. N., additional, Horvath, Steve, additional, Estrada, Karol, additional, Rivadeneira, Fernando, additional, Hofman, Albert, additional, Uitterlinden, Andre G., additional, Robberecht, Wim, additional, Andersen, Peter M., additional, Melki, Judith, additional, Meininger, Vincent, additional, Hardiman, Orla, additional, Landers, John E., additional, Brown, Robert H., additional, Shatunov, Aleksey, additional, Shaw, Christopher E., additional, Leigh, P. Nigel, additional, Al-Chalabi, Ammar, additional, Ophoff, Roel A., additional, van den Berg, Leonard H., additional, and Veldink, Jan H., additional

Published
2012
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30. Trans-eQTLs Reveal That Independent Genetic Variants Associated with a Complex Phenotype Converge on Intermediate Genes, with a Major Role for the HLA

Author

Fehrmann, Rudolf S. N., primary, Jansen, Ritsert C., additional, Veldink, Jan H., additional, Westra, Harm-Jan, additional, Arends, Danny, additional, Bonder, Marc Jan, additional, Fu, Jingyuan, additional, Deelen, Patrick, additional, Groen, Harry J. M., additional, Smolonska, Asia, additional, Weersma, Rinse K., additional, Hofstra, Robert M. W., additional, Buurman, Wim A., additional, Rensen, Sander, additional, Wolfs, Marcel G. M., additional, Platteel, Mathieu, additional, Zhernakova, Alexandra, additional, Elbers, Clara C., additional, Festen, Eleanora M., additional, Trynka, Gosia, additional, Hofker, Marten H., additional, Saris, Christiaan G. J., additional, Ophoff, Roel A., additional, van den Berg, Leonard H., additional, van Heel, David A., additional, Wijmenga, Cisca, additional, te Meerman, Gerard J., additional, and Franke, Lude, additional

Published
2011
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31. Genome-wide association study identifies 19p13.3 (UNC13A) and 9p21.2 as susceptibility loci for sporadic amyotrophic lateral sclerosis

Author

van Es, Michael A, primary, Veldink, Jan H, additional, Saris, Christiaan G J, additional, Blauw, Hylke M, additional, van Vught, Paul W J, additional, Birve, Anna, additional, Lemmens, Robin, additional, Schelhaas, Helenius J, additional, Groen, Ewout J N, additional, Huisman, Mark H B, additional, van der Kooi, Anneke J, additional, de Visser, Marianne, additional, Dahlberg, Caroline, additional, Estrada, Karol, additional, Rivadeneira, Fernando, additional, Hofman, Albert, additional, Zwarts, Machiel J, additional, van Doormaal, Perry T C, additional, Rujescu, Dan, additional, Strengman, Eric, additional, Giegling, Ina, additional, Muglia, Pierandrea, additional, Tomik, Barbara, additional, Slowik, Agnieszka, additional, Uitterlinden, Andre G, additional, Hendrich, Corinna, additional, Waibel, Stefan, additional, Meyer, Thomas, additional, Ludolph, Albert C, additional, Glass, Jonathan D, additional, Purcell, Shaun, additional, Cichon, Sven, additional, Nöthen, Markus M, additional, Wichmann, H-Erich, additional, Schreiber, Stefan, additional, Vermeulen, Sita H H M, additional, Kiemeney, Lambertus A, additional, Wokke, John H J, additional, Cronin, Simon, additional, McLaughlin, Russell L, additional, Hardiman, Orla, additional, Fumoto, Katsumi, additional, Pasterkamp, R Jeroen, additional, Meininger, Vincent, additional, Melki, Judith, additional, Leigh, P Nigel, additional, Shaw, Christopher E, additional, Landers, John E, additional, Al-Chalabi, Ammar, additional, Brown, Robert H, additional, Robberecht, Wim, additional, Andersen, Peter M, additional, Ophoff, Roel A, additional, and van den Berg, Leonard H, additional

Published
2009
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32. N-of-1 trial of salbutamol in hyperkalaemic periodic paralysis.

Author

Stunnenberg, Bas C., Merkus, Esther C., Raaphorst, Joost, Saris, Christiaan G. J., Groenewoud, Hans, Statland, Jeffrey, Weijma, Robyn, van Vlijmen, Bas, Griggs, Robert, van Engelen, Baziel G. M., van der Wilt, Gert Jan, and Saris, Christiaan Gj

Subjects
ALBUTEROL, HYPOKALEMIA, MEDICAL research, PARALYSIS, PHYSICIANS
Published
2021
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33. Weighted gene co-expression network analysis of the peripheral blood from Amyotrophic Lateral Sclerosis patients.

Author

Saris, Christiaan G. J., Horvath, Steve, van Vught, Paul W. J., van Es, Michael A., Blauw, Hylke M., Fuller, Tova F., Langfelder, Peter, DeYoung, Joseph, Wokke, John H. J., Veldink, Jan H., van den Berg, Leonard H., and Ophoff, Roel A.

Subjects
*AMYOTROPHIC lateral sclerosis, *GENETIC disorders, *GENE expression, *GENETIC regulation, *GENES
Abstract

Background: Amyotrophic Lateral Sclerosis (ALS) is a lethal disorder characterized by progressive degeneration of motor neurons in the brain and spinal cord. Diagnosis is mainly based on clinical symptoms, and there is currently no therapy to stop the disease or slow its progression. Since access to spinal cord tissue is not possible at disease onset, we investigated changes in gene expression profiles in whole blood of ALS patients. Results: Our transcriptional study showed dramatic changes in blood of ALS patients; 2,300 probes (9.4%) showed significant differential expression in a discovery dataset consisting of 30 ALS patients and 30 healthy controls. Weighted gene co-expression network analysis (WGCNA) was used to find disease-related networks (modules) and disease related hub genes. Two large co-expression modules were found to be associated with ALS. Our findings were replicated in a second (30 patients and 30 controls) and third dataset (63 patients and 63 controls), thereby demonstrating a highly significant and consistent association of two large co-expression modules with ALS disease status. Ingenuity Pathway Analysis of the ALS related module genes implicates enrichment of functional categories related to genetic disorders, neurodegeneration of the nervous system and inflammatory disease. The ALS related modules contain a number of candidate genes possibly involved in pathogenesis of ALS. Conclusion: This first large-scale blood gene expression study in ALS observed distinct patterns between cases and controls which may provide opportunities for biomarker development as well as new insights into the molecular mechanisms of the disease. [ABSTRACT FROM AUTHOR]

Published
2009
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34. Genetic variation in DPP6 is associated with susceptibility to amyotrophic lateral sclerosis.

Author

van Es, Michael A., van Vught, Paul W. J., Blauw, Hylke M., Franke, Lude, Saris, Christiaan G. J., Van Den Bosch, Ludo, de Jong, Sonja W., de Jong, Vianney, Baas, Frank, van't Slot, Ruben, Lemmens, Robin, Schelhaas, Helenius J., Birve, Anna, Sleegers, Kristel, Van Broeckhoven, Christine, Schymick, Jennifer C., Traynor, Bryan J., Wokke, John H. J., Wijmenga, Cisca, and Robberecht, Wim

Subjects
AMYOTROPHIC lateral sclerosis, GENES, EUROPEANS, MOTOR neuron diseases, GENETICS, MEDICAL genetics
Abstract

We identified a SNP in the DPP6 gene that is consistently strongly associated with susceptibility to amyotrophic lateral sclerosis (ALS) in different populations of European ancestry, with an overall P value of 5.04 × 10−8 in 1,767 cases and 1,916 healthy controls and with an odds ratio of 1.30 (95% confidence interval (CI) of 1.18–1.43). Our finding is the first report of a genome-wide significant association with sporadic ALS and may be a target for future functional studies. [ABSTRACT FROM AUTHOR]

Published
2008
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35. Ketogenic diet in adult patients with mitochondrial myopathy.

Author

Zweers HEE, Kroesen SH, Beerlink G, Buit E, Gerrits K, Dorhout A, van Wegberg AMJ, Janssen MCH, Wortmann SB, Timmers S, and Saris CGJ

Subjects
Humans, Male, Female, Adult, Middle Aged, DNA, Mitochondrial genetics, Treatment Outcome, Young Adult, Muscle Weakness diet therapy, Muscle Weakness genetics, Muscle Weakness etiology, Mitochondrial Myopathies diet therapy, Mitochondrial Myopathies genetics, Diet, Ketogenic adverse effects
Abstract

Background: This study aimed to explore the feasibility, safety and efficacy of a Modified Atkins Diet (MAD) in patients with mitochondrial myopathy (MM)., Methods: Patients with genetically proven mitochondrial disorder and exercise intolerance or muscle weakness followed a twelve week MAD. Feasibility was measured by diet duration and ketone levels. Safety was assessed by monitoring adverse events (AE). Efficacy was assessed by a maximal incremental test and a muscle performance test., Results: Eight out of twenty patients completed the twelve week intervention. Reasons to discontinue were the occurrence of AE: rhabdomyolysis (n = 3), vomiting (n = 1), fatigue (n = 6), constipation (n = 1), in combination with a lack of improvement and adherence difficulties. On an individual level, various positive effects were reported including improvements in VO 2peak (n = 6), anaerobic threshold (n = 9), muscle fatigue resistance (n = 5), muscle strength (n = 7), fatigue (n = 6), glucose tolerance (n = 7), migraine (n = 3), sleep (n = 3), and gastrointestinal complaints (n = 2). Lipid profile improved and thirteen patients lost weight. All patients with mitochondrial DNA (mtDNA) deletions, experienced muscle related AE. The five patients with the m.3243A>G mutation achieved the longest diet duration., Discussion/conclusion: MAD feasibility, safety and efficacy is variable in MD patients. MAD appears to be unsuitable for MD patients with mtDNA deletions. All patients should be monitored closely for adverse events when initiating the diet. Further research should focus on predictive factors to consider the diet, effectiveness of less stringent carbohydrate restricted diets., Competing Interests: Declaration of competing interest SW and HZ received a travel grants From Nutricia., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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36. 272nd ENMC international workshop: 10 Years of progress - revision of the ENMC 2013 diagnostic criteria for inclusion body myositis and clinical trial readiness. 16-18 June 2023, Hoofddorp, The Netherlands.

Author

Lilleker JB, Naddaf E, Saris CGJ, Schmidt J, de Visser M, and Weihl CC

Subjects
Humans, Consensus, Magnetic Resonance Imaging, Netherlands, Outcome Assessment, Health Care, Myositis diagnosis, Myositis, Inclusion Body therapy, Myositis, Inclusion Body drug therapy
Abstract

Since the publication of the 2013 European Neuromuscular Center (ENMC) diagnostic criteria for Inclusion Body Myositis (IBM), several advances have been made regarding IBM epidemiology, pathogenesis, diagnostic tools, and clinical trial readiness. Novel diagnostic tools include muscle imaging techniques such as MRI and ultrasound, and serological testing for cytosolic 5'-nucleotidase-1A antibodies. The 272nd ENMC workshop aimed to develop new diagnostic criteria, discuss clinical outcome measures and clinical trial readiness. The workshop started with patient representatives highlighting several understudied symptoms and the urge for a timely diagnosis. This was followed by presentations from IBM experts highlighting the new developments in the field. This report is composed of two parts, the first part providing new diagnostic criteria on which consensus was achieved. The second part focuses on the use of outcome measures in clinical practice and clinical trials, highlighting current limitations and outlining the goals for future studies., Competing Interests: Declaration of competing interest The authors have no conflicts of interest., (Copyright © 2024.)

Published
2024
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37. An attenuated, adult case of AADC deficiency demonstrated by protein characterization.

Author

Bisello G, Saris CGJ, Franchini R, Verbeek MM, Willemsen MAAP, Perduca M, and Bertoldi M

Abstract

A case of an adult with borderline AADC deficiency symptoms is presented here. Genetic analysis revealed that the patient carries two AADC variants (NM&#95;000790.3: c.1040G > A and c.679G > C) in compound heterozygosis, resulting in p.Arg347Gln and p.Glu227Gln amino acid alterations. While p.Arg347Gln is a known pathogenic variant, p.Glu227Gln is unknown. Combining clinical features to bioinformatic and molecular characterization of the AADC protein population of the patient (p.Arg347Gln/p.Arg347Gln homodimer, p.Glu227Gln/p.Glu227Gln homodimer, and p.Glu227Gln/p.Arg347Gln heterodimer), we determined that: i) the p.Arg347Gln/p.Arg347Gln homodimer is inactive since the alteration affects a catalytically essential structural element at the active site, ii) the p.Glu227Gln/p.Glu227Gln homodimer is as active as the wild-type AADC since the alteration occurs at the surface and does not change the chemical nature of the amino acid, and iii) the p.Glu227Gln/p.Arg347Gln heterodimer has a catalytic efficiency 75% that of the wild-type since only one of the two active sites is compromised, thus demonstrating a positive complementation. By this approach, the molecular basis for the mild presentation of the disease is provided, and the experience made can also be useful for personalized therapeutic decisions in other mild AADC deficiency patients. Interestingly, in the last few years, many previously undiagnosed or misdiagnosed patients have been identified as mild cases of AADC deficiency, expanding the phenotype of this neurotransmitter disease., Competing Interests: M.B. received research funding and unconditional support by PTC Therapeutics, Inc., (© 2024 The Authors. Published by Elsevier Inc.)

Published
2024
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38. The Hypoxia Response Pathway: A Potential Intervention Target in Parkinson's Disease?

Author

Janssen Daalen JM, Koopman WJH, Saris CGJ, Meinders MJ, Thijssen DHJ, and Bloem BR

Subjects
Humans, Oxidative Stress, Neuroprotection, Hypoxia, Parkinson Disease therapy, Parkinson Disease metabolism
Abstract

Parkinson's disease (PD) is a progressive neurodegenerative disorder for which only symptomatic treatments are available. Both preclinical and clinical studies suggest that moderate hypoxia induces evolutionarily conserved adaptive mechanisms that enhance neuronal viability and survival. Therefore, targeting the hypoxia response pathway might provide neuroprotection by ameliorating the deleterious effects of mitochondrial dysfunction and oxidative stress, which underlie neurodegeneration in PD. Here, we review experimental studies regarding the link between PD pathophysiology and neurophysiological adaptations to hypoxia. We highlight the mechanistic differences between the rescuing effects of chronic hypoxia in neurodegeneration and short-term moderate hypoxia to improve neuronal resilience, termed "hypoxic conditioning". Moreover, we interpret these preclinical observations regarding the pharmacological targeting of the hypoxia response pathway. Finally, we discuss controversies with respect to the differential effects of hypoxia response pathway activation across the PD spectrum, as well as intervention dosing in hypoxic conditioning and potential harmful effects of such interventions. We recommend that initial clinical studies in PD should focus on the safety, physiological responses, and mechanisms of hypoxic conditioning, as well as on repurposing of existing pharmacological compounds. © 2023 International Parkinson and Movement Disorder Society., (© 2023 International Parkinson and Movement Disorder Society.)

Published
2024
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39. Screening and prevalence of cardiac abnormalities on electro- and echocardiography in a large cohort of patients with mitochondrial disease.

Author

Hendrix CLF, van den Heuvel FMA, Rodwell L, Timmermans J, Nijveldt R, Janssen MCH, and Saris CGJ

Subjects
Deafness, Diabetes Mellitus, Type 2, Echocardiography, Electrocardiography, Female, Humans, Hypertrophy, Left Ventricular diagnosis, Male, Prevalence, Retrospective Studies, Heart Defects, Congenital, MELAS Syndrome genetics, Mitochondrial Diseases diagnostic imaging, Mitochondrial Diseases epidemiology
Abstract

Background: In patients with primary mitochondrial disease (MD), screening with electrocardiogram (ECG) and transthoracic echocardiography (TTE) is warranted according to current guidelines as structural cardiac abnormalities are frequent. This study aims to evaluate the cardiac phenotype of a large Dutch cohort of patients with MD and investigates whether ECG alone is sufficient for predicting structural cardiac abnormalities on TTE., Methods: In this retrospective cohort study, genetically confirmed MD patients >18 years old with an available ECG and TTE were included. Newcastle Mitochondrial Disease Scale for Adults (NMDAS) scores were assessed. ECG's were evaluated for rhythm and conduction disorders, voltage criteria for left ventricular hypertrophy (LVH) and repolarization disorders. Echocardiographic evaluation included left and right ventricular volumes and function, and presence of LVH or concentric remodeling., Results: In total, 200 MD patients were included with a median age of 45 years (IQR; 37-57) of whom 36% were male. Of all MD patients, 35% had abnormalities on ECG and 61% on TTE. Most frequent structural cardiac abnormalities on TTE were: global longitudinal strain > - 18% (54%), concentric remodeling (27%) and left ventricular (LV) ejection fraction <52% (14%). Patients with maternally inherited diabetes and deafness (MIDD) and mitochondrial encephalomyopathy, lactic acidosis and stroke-like episodes (MELAS) had the highest prevalence of ECG abnormalities (50% and 47%). TTE abnormalities were most prevalent in patients with MIDD (75%), followed by mitochondrial myopathy (MM) (55%), MELAS (47%) and Mitochondrial Epilepsy and Ragged Red Fibers (MERRF) (47%). MD patients with a high disease severity (NMDAS ≥21) had a higher prevalence of ECG abnormalities (44%, p = 0.039) and structural cardiac abnormalities (72%, p = 0.004) compared to patients with a NMDAS score of 11-20 and ≤ 10 (ECG: 34% and 19%; TTE: 63% and 39%). ECG abnormalities had a positive predictive value of 74% and a negative predictive value of 53% for structural cardiac abnormalities on TTE., Conclusion: MD patients frequently have cardiac involvement especially patients with MIDD, MELAS or high NMDAS score. ECG as sole screening parameter is insufficient to detect structural cardiac abnormalities., Competing Interests: Declaration of Competing Interest The authors report no conflicts of interest. The authors alone are responsible for the content and writing of the paper. There were no known competing financial conflicts or personal interest that could have influenced the work reported in this paper., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2022
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40. Mitochondrial migraine; a prevalence, impact and treatment efficacy cohort study.

Author

Tiehuis LH, Koene S, Saris CGJ, and Janssen MCH

Subjects
Adolescent, Adult, Cohort Studies, Female, Humans, Male, Middle Aged, Migraine Disorders etiology, Mitochondrial Diseases genetics, Netherlands epidemiology, Prevalence, Quality of Life, Surveys and Questionnaires, Treatment Outcome, Young Adult, Migraine Disorders drug therapy, Migraine Disorders epidemiology, Mitochondrial Diseases complications
Abstract

Mitochondrial respiratory chain dysfunction may be predisposing for the development of migraine, reflected in high migraine prevalence in patients with mitochondrial disease. Prevalence and impact of migraine in patients with proven mitochondrial disease and the current treatment efficacy were studied using online questionnaires. Patients were selected at the Internal Medicine Department. Headache was reported by 34 (55%) out of 62 patients. Migraine-criteria were met by 85% of them. Efficacy of migraine treatment was achieved in 4 patients. Given the high prevalence of migraine and current treatment insufficiency, migraine is a major threat of quality of life patients with mitochondrial disease., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2020
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41. Ultrasound can differentiate inclusion body myositis from disease mimics.

Author

Leeuwenberg KE, van Alfen N, Christopher-Stine L, Paik JJ, Tiniakou E, Mecoli C, Doorduin J, Saris CGJ, and Albayda J

Subjects
Aged, Aged, 80 and over, Diagnosis, Differential, Female, Humans, Male, Middle Aged, Neuromuscular Diseases diagnostic imaging, Neuromuscular Diseases physiopathology, Retrospective Studies, Ultrasonography, Interventional standards, Myositis, Inclusion Body diagnostic imaging, Myositis, Inclusion Body physiopathology, Ultrasonography, Interventional methods
Abstract

Introduction: The diagnosis of inclusion body myositis (IBM) can be challenging, and its presentation can be confused with other forms of myositis or neuromuscular disorders. In this study we evaluate the ability of quantitative muscle ultrasound to differentiate between IBM and mimicking diseases., Methods: Patients 50 years of age and older were included from two specialty centers. Muscle echogenicity and muscle thickness of four characteristically involved muscles in IBM were measured and compared with polymyositis (PM)/dermatomyositis (DM), other neuromuscular disorders, and healthy controls., Results: Echogenicity was higher and muscle thickness generally lower in all four muscles in IBM compared with PM/DM and normal controls. When comparing IBM with the comparator groups, the flexor digitorum profundus was the most discriminative muscle., Discussion: Ultrasound appears to be a good test to differentiate established IBM from PM/DM and neuromuscular controls, with value as a diagnostic tool for IBM., (© 2020 The Authors. Muscle & Nerve published by Wiley Periodicals, Inc.)

Published
2020
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42. Frequencies and clinical associations of myositis-related antibodies in The Netherlands: A one-year survey of all Dutch patients.

Author

Platteel ACM, Wevers BA, Lim J, Bakker JA, Bontkes HJ, Curvers J, Damoiseaux J, Heron M, de Kort G, Limper M, van Lochem EG, Mulder AHL, Saris CGJ, van der Valk H, van der Kooi AJ, van Leeuwen EMM, Veltkamp M, Schreurs MWJ, Meek B, and Hamann D

Abstract

Idiopathic inflammatory myopathies (IIM) are a heterogeneous group of connective tissue diseases, collectively known as myositis. Diagnosis of IIM is challenging while timely recognition of an IIM is of utter importance considering treatment options and otherwise irreversible (severe) long-term clinical complications. With the EULAR/ACR classification criteria (2017) considerable advancement has been made in the diagnostic workup of IIM. While these criteria take into account clinical parameters as well as presence of one autoantibody, anti-Jo-1, several autoantibodies are associated with IIM and are currently evaluated to be incorporated into classification criteria. As individual antibodies occur at low frequency, the development of line blots allowing multiplex antibody analysis has improved laboratory diagnostics for IIM. The Euroline myositis line-blot assay (Euroimmun) allows screening and semi-quantitative measurement for 15 autoantibodies, i.e . myositis specific antibodies (MSA) to SRP, EJ, OJ, Mi-2α, Mi-2β, TIF1-γ, MDA5, NXP2, SAE1, PL-12, PL-7, Jo-1 and myositis associated antibodies (MAA) to Ku, PM/Scl-75 and PM/Scl-100. To evaluate the clinical significance of detection and levels of these autoantibodies in the Netherlands, a retrospective analysis of all Dutch requests for extended myositis screening within a 1 year period was performed. A total of 187 IIM patients and 632 non-IIM patients were included. We conclude that frequencies of MSA and MAA observed in IIM patients in a routine diagnostic setting are comparable to cohort-based studies. Weak positive antibody levels show less diagnostic accuracy compared to positive antibody levels, except for anti-NXP2. Known associations between antibodies and skin involvement (anti-MDA5, anti-TIF1-γ), lung involvement (anti-Jo-1), and malignancy (anti-TIF1-γ) were confirmed in our IIM study population. The availability of multiplex antibody analyses will facilitate inclusion of additional autoantibodies in clinical myositis guidelines and help to accelerate diagnosing IMM with rare but specific antibodies., (© 2019 The Authors.)

Published
2019
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43. Panel-Based Exome Sequencing for Neuromuscular Disorders as a Diagnostic Service.

Author

Westra D, Schouten MI, Stunnenberg BC, Kusters B, Saris CGJ, Erasmus CE, van Engelen BG, Bulk S, Verschuuren-Bemelmans CC, Gerkes EH, de Geus C, van der Zwaag PA, Chan S, Chung B, Barge-Schaapveld DQCM, Kriek M, Sznajer Y, van Spaendonck-Zwarts K, van der Kooi AJ, Krause A, Schönewolf-Greulich B, de Die-Smulders C, Sallevelt SCEH, Krapels IPC, Rasmussen M, Maystadt I, Kievit AJA, Witting N, Pennings M, Meijer R, Gillissen C, Kamsteeg EJ, and Voermans NC

Subjects
Adolescent, Adult, Aged, Child, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Male, Middle Aged, Young Adult, Neuromuscular Diseases diagnosis, Neuromuscular Diseases genetics, Exome Sequencing methods
Abstract

Background: Neuromuscular disorders (NMDs) are clinically and genetically heterogeneous. Accurate molecular genetic diagnosis can improve clinical management, provides appropriate genetic counseling and testing of relatives, and allows potential therapeutic trials., Objective: To establish the clinical utility of panel-based whole exome sequencing (WES) in NMDs in a population with children and adults with various neuromuscular symptoms., Methods: Clinical exome sequencing, followed by diagnostic interpretation of variants in genes associated with NMDs, was performed in a cohort of 396 patients suspected of having a genetic cause with a variable age of onset, neuromuscular phenotype, and inheritance pattern. Many had previously undergone targeted gene testing without results., Results: Disease-causing variants were identified in 75/396 patients (19%), with variants in the three COL6-genes (COL6A1, COL6A2 and COL6A3) as the most common cause of the identified muscle disorder, followed by variants in the RYR1 gene. Together, these four genes account for almost 25% of cases in whom a definite genetic cause was identified. Furthermore, likely pathogenic variants and/or variants of uncertain significance were identified in 95 of the patients (24%), in whom functional and/or segregation analysis should be used to confirm or reject the pathogenicity. In 18% of the cases with a disease-causing variant of which we received additional clinical information, we identified a genetic cause in genes of which the associated phenotypes did not match that of the patients. Hence, the advantage of panel-based WES is its unbiased approach., Conclusion: Whole exome sequencing, followed by filtering for NMD genes, offers an unbiased approach for the genetic diagnostics of NMD patients. This approach could be used as a first-tier test in neuromuscular disorders with a high suspicion of a genetic cause. With uncertain results, functional testing and segregation analysis are needed to complete the evidence.

Published
2019
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44. Seronegative patients form a distinctive subgroup of immune-mediated necrotizing myopathy.

Author

Lim J, Rietveld A, De Bleecker JL, Badrising UA, Saris CGJ, van der Kooi AJ, and de Visser M

Subjects
Adult, Aged, Aged, 80 and over, Autoimmune Diseases complications, Female, Humans, Male, Middle Aged, Muscle, Skeletal immunology, Myositis complications, Myositis immunology, Myositis pathology, Necrosis, Retrospective Studies, Serologic Tests, Young Adult, Autoimmune Diseases epidemiology, Myositis epidemiology
Abstract

Objectives: To investigate the characteristics of different clinico-serologic subgroups of immune-mediated necrotizing myopathy (IMNM)., Methods: We retrospectively reviewed data from medical charts of 64 patients diagnosed with IMNM between 2012 and 2017 in 3 neuromuscular referral centers in The Netherlands and 1 in Belgium., Results: Seventeen patients had anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR) autoantibodies (Abs), of whom 11 had a history of statin use, 15 had anti-signal recognition particle (SRP) Abs, 2 had anti-melanoma differentiation-associated protein 5 (MDA5) Abs, 22 patients were seronegative, and 9 patients did not have a complete Ab assessment. Moderate to severe disability in HMGCR Ab-positive and anti-SRP Ab-positive IMNM was common (71% and 60%, respectively) despite multimodality treatment. Compared with statin-associated anti-HMGCR Ab-positive IMNM, statin-naive anti-HMGCR Ab-positive IMNM patients were more often men (67% vs 45%), had lower rates of dysphagia (17% vs 45%), and more frequently had third-line therapy (50% vs 9%) and poor to fatal outcome (50% vs 0%). Compared with seropositive IMNM, seronegative IMNM was characterized by female predominance (1:3), frequent occurrence of associated connective tissue disorders (22% vs 9%), and significantly higher rates of extramuscular disease activity (50% vs 16%, p 0.014; 2-sided Fisher exact), also after excluding patients with an associated connective tissue disease (35% vs 7%, p 0.038; 2-sided Fisher exact)., Conclusions: Our findings indicate that seronegative IMNM forms a subgroup with distinctive features from seropositive IMNM.

Published
2018
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45. MT-ND5 Mutation Exhibits Highly Variable Neurological Manifestations at Low Mutant Load.

Author

Ng YS, Lax NZ, Maddison P, Alston CL, Blakely EL, Hepplewhite PD, Riordan G, Meldau S, Chinnery PF, Pierre G, Chronopoulou E, Du A, Hughes I, Morris AA, Kamakari S, Chrousos G, Rodenburg RJ, Saris CGJ, Feeney C, Hardy SA, Sakakibara T, Sudo A, Okazaki Y, Murayama K, Mundy H, Hanna MG, Ohtake A, Schaefer AM, Champion MP, Turnbull DM, Taylor RW, Pitceathly RDS, McFarland R, and Gorman GS

Subjects
Adolescent, Adult, Brain diagnostic imaging, Child, Cohort Studies, Female, Humans, Magnetic Resonance Imaging, Male, Syndrome, Young Adult, Brain pathology, Electron Transport Complex I genetics, Mitochondrial Proteins genetics, Mutation genetics
Abstract

Mutations in the m.13094T>C MT-ND5 gene have been previously described in three cases of Leigh Syndrome (LS). In this retrospective, international cohort study we identified 20 clinically affected individuals (13 families) and four asymptomatic carriers. Ten patients were deceased at the time of analysis (median age of death was 10years (range: 5·4months-37years, IQR=17·9years). Nine patients manifested with LS, one with mitochondrial encephalomyopathy, lactic acidosis and stroke-like episodes (MELAS), and one with Leber hereditary optic neuropathy. The remaining nine patients presented with either overlapping syndromes or isolated neurological symptoms. Mitochondrial respiratory chain activity analysis was normal in five out of ten muscle biopsies. We confirmed maternal inheritance in six families, and demonstrated marked variability in tissue segregation, and phenotypic expression at relatively low blood mutant loads. Neuropathological studies of two patients manifesting with LS/MELAS showed prominent capillary proliferation, microvacuolation and severe neuronal cell loss in the brainstem and cerebellum, with conspicuous absence of basal ganglia involvement. These findings suggest that whole mtDNA genome sequencing should be considered in patients with suspected mitochondrial disease presenting with complex neurological manifestations, which would identify over 300 known pathogenic variants including the m.13094T>C., (Copyright © 2018 German Center for Neurodegenerative Diseases (DZNE). Published by Elsevier B.V. All rights reserved.)

Published
2018
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46. Analysis of the KIFAP3 gene in amyotrophic lateral sclerosis: a multicenter survival study.

Author

van Doormaal PT, Ticozzi N, Gellera C, Ratti A, Taroni F, Chiò A, Calvo A, Mora G, Restagno G, Traynor BJ, Birve A, Lemmens R, van Es MA, Saris CG, Blauw HM, van Vught PW, Groen EJ, Corrado L, Mazzini L, Del Bo R, Corti S, Waibel S, Meyer T, Ludolph AC, Goris A, van Damme P, Robberecht W, Shatunov A, Fogh I, Andersen PM, D'Alfonso S, Hardiman O, Cronin S, Rujescu D, Al-Chalabi A, Landers JE, Silani V, van den Berg LH, and Veldink JH

Subjects
Aged, Cohort Studies, Female, Genotype, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Survival Analysis, Adaptor Proteins, Signal Transducing genetics, Amyotrophic Lateral Sclerosis genetics, Amyotrophic Lateral Sclerosis mortality, Cytoskeletal Proteins genetics, Genetic Variation genetics, Genome-Wide Association Study
Abstract

Sporadic amyotrophic lateral sclerosis is a multifactorial disease of environmental and genetic origin. In a previous large multicenter genome wide study, common genetic variation in the Kinesin-Associated Protein 3 (KIFAP3) gene (rs1541160) was reported to have a significant effect on survival in amyotrophic lateral sclerosis patients. However, this could not be replicated in 3 smaller independent cohorts. We conducted a large multicenter multivariate survival analysis (n = 2362) on the effect of genetic variation in rs1541160. The previously reported beneficial genotype did not show a significant improvement in survival in this patient group., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published
2014
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47. A large genome scan for rare CNVs in amyotrophic lateral sclerosis.

Author

Blauw HM, Al-Chalabi A, Andersen PM, van Vught PW, Diekstra FP, van Es MA, Saris CG, Groen EJ, van Rheenen W, Koppers M, Van't Slot R, Strengman E, Estrada K, Rivadeneira F, Hofman A, Uitterlinden AG, Kiemeney LA, Vermeulen SH, Birve A, Waibel S, Meyer T, Cronin S, McLaughlin RL, Hardiman O, Sapp PC, Tobin MD, Wain LV, Tomik B, Slowik A, Lemmens R, Rujescu D, Schulte C, Gasser T, Brown RH Jr, Landers JE, Robberecht W, Ludolph AC, Ophoff RA, Veldink JH, and van den Berg LH

Subjects
Case-Control Studies, Genetic Predisposition to Disease, Genetic Variation, Genome, Human, Humans, Motor Neurons, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Risk Factors, Spastic Paraplegia, Hereditary genetics, Amyotrophic Lateral Sclerosis genetics, DNA Copy Number Variations, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases genetics, Genome-Wide Association Study, Membrane Proteins genetics, Nerve Tissue Proteins genetics, Potassium Channels genetics
Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease selectively affecting motor neurons in the brain and spinal cord. Recent genome-wide association studies (GWASs) have identified several common variants which increase disease susceptibility. In contrast, rare copy-number variants (CNVs), which have been associated with several neuropsychiatric traits, have not been studied for ALS in well-powered study populations. To examine the role of rare CNVs in ALS susceptibility, we conducted a CNV association study including over 19,000 individuals. In a genome-wide screen of 1875 cases and 8731 controls, we did not find evidence for a difference in global CNV burden between cases and controls. In our association analyses, we identified two loci that met our criteria for follow-up: the DPP6 locus (OR = 3.59, P = 6.6 × 10(-3)), which has already been implicated in ALS pathogenesis, and the 15q11.2 locus, containing NIPA1 (OR = 12.46, P = 9.3 × 10(-5)), the gene causing hereditary spastic paraparesis type 6 (HSP 6). We tested these loci in a replication cohort of 2559 cases and 5887 controls. Again, results were suggestive of association, but did not meet our criteria for independent replication: DPP6 locus: OR = 1.92, P = 0.097, pooled results: OR = 2.64, P = 1.4 × 10(-3); NIPA1: OR = 3.23, P = 0.041, pooled results: OR = 6.20, P = 2.2 × 10(-5)). Our results highlight DPP6 and NIPA1 as candidates for more in-depth studies. Unlike other complex neurological and psychiatric traits, rare CNVs with high effect size do not play a major role in ALS pathogenesis.

Published
2010
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48. Copy-number variation in sporadic amyotrophic lateral sclerosis: a genome-wide screen.

Author

Blauw HM, Veldink JH, van Es MA, van Vught PW, Saris CG, van der Zwaag B, Franke L, Burbach JP, Wokke JH, Ophoff RA, and van den Berg LH

Subjects
Adult, Aged, Aged, 80 and over, Chromosome Mapping, Female, Gene Frequency, Genetic Predisposition to Disease, Genetic Testing methods, Humans, Male, Middle Aged, Oligonucleotide Array Sequence Analysis, Amyotrophic Lateral Sclerosis genetics, Gene Dosage physiology, Genetic Variation, Genome physiology
Abstract

Background: Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease characterised by the selective death of motor neurons in the brain and spinal cord. Genetic risk factors have been implicated in susceptibility to ALS. Like single nucleotide polymorphisms (SNPs), copy-number variants (CNVs) are a source of genetic variation that have important effects on gene expression and disease phenotypes, and our aim was to identify CNVs that predispose to sporadic ALS., Methods: We did a genome-wide screen for CNVs by analysis of Illumina 317K SNP arrays for 406 patients with sporadic ALS and 404 controls. We examined CNVs for association with ALS, and used the Kyoto Encyclopedia of Genes and Genomes database and the Gene Ontology database to investigate the functionality of genes that were deleted exclusively in patients with ALS., Findings: We detected 2328 CNVs in 810 individuals. No CNV locus was significantly associated with sporadic ALS. 406 genes were duplicated or deleted exclusively in patients with ALS and have not been reported in previous studies of CNVs. Of the 390 genes heterozygously deleted in patients with sporadic ALS, 155 (40%) deletions were recorded exclusively in patients. By contrast, of the 323 genes heterozygously deleted in control participants, only 51 (16%) were exclusive to the controls (p=2.15 x 10(-12) for difference between groups). Products of the genes deleted specifically in patients with sporadic ALS include proteins involved in oxidative phosphorylation, regulation of the actin cytoskeleton, and interactions between cytokines and their receptors., Interpretation: Common CNVs in the regions of the genome represented on the SNP array are unlikely to be associated with sporadic ALS. However, the high number of genes deleted specifically in patients with ALS strongly suggests that multiple rare deletions might have an important role in ALS pathogenesis.

Published
2008
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