Your search keyword '"Kushner S.A."' showing total 73 results

1. Dysfunctional parvalbumin interneurons in a genetic mouse model of schizophrenia

Author

Hijazi, S., primary, Pascual-García, M., additional, Tolido, A., additional, Pham, A., additional, and Kushner, S.A., additional

Published

2023

2. Association between prenatal alcohol exposure and children's facial shape:: a prospective population-based cohort study

Author

Liu, X. (author), Kayser, Manfred (author), Kushner, S.A. (author), Tiemeier, H (author), Rivadeneira, F (author), Jaddoe, Vincent (author), Niessen, W.J. (author), Wolvius, E.B. (author), Roshchupkin, G.V. (author), Liu, X. (author), Kayser, Manfred (author), Kushner, S.A. (author), Tiemeier, H (author), Rivadeneira, F (author), Jaddoe, Vincent (author), Niessen, W.J. (author), Wolvius, E.B. (author), and Roshchupkin, G.V. (author)

Abstract

STUDY QUESTION: Is there an association between low-to-moderate levels of prenatal alcohol exposure (PAE) and children's facial shape? SUMMARY ANSWER: PAE before and during pregnancy, even at low level (<12 g of alcohol per week), was found associated with the facial shape of children, and these associations were found attenuated as children grow older. WHAT IS KNOWN ALREADY: High levels of PAE during pregnancy can have significant adverse associations with a child's health development resulting in recognizably abnormal facial development. STUDY DESIGN, SIZE, DURATION: This study was based on the Generation R Study, a prospective cohort from fetal life onwards with maternal and offspring data. We analyzed children 3-dimensional (3D) facial images taken at ages 9 (n = 3149) and 13 years (n = 2477) together with the data of maternal alcohol consumption. PARTICIPANTS/MATERIALS, SETTING, METHODS: We defined six levels of PAE based on the frequency and dose of alcohol consumption and defined three tiers based on the timing of alcohol exposure of the unborn child. For the image analysis, we used 3D graph convolutional networks for non-linear dimensionality reduction, which compressed the high-dimensional images into 200 traits representing facial morphology. These 200 traits were used for statistical analysis to search for associations with PAE. Finally, we generated heatmaps to display the facial phenotypes associated with PAE. MAIN RESULTS AND THE ROLE OF CHANCE: The results of the linear regression in the 9-year-old children survived correction for multiple testing with false discovery rate (FDR). In Tier 1 where we examined PAE only before pregnancy (exposed N = 278, unexposed N = 760), we found three traits survived FDR correction. The lowest FDR-P is 1.7e-05 (beta = 0.021, SE = 0.0040) in Trait #29; In Tier 2b where we examine any PAE during first trimester (exposed N = 756; unexposed N = 760), we found eight traits survived FDR correction. The lowest FDR-P is, ImPhys/Vos group, ImPhys/Computational Imaging

Published

2023

3. Plasticity of visual evoked potentials in patients with neurofibromatosis type 1

Author

Castricum, J., primary, Tulen, J.H.M., additional, Heuvelmans, A.M., additional, Geleijnse, G., additional, Straver, D.C.G., additional, Taal, W., additional, Kushner, S.A., additional, and Elgersma, Y., additional

Published

2022

4. Rapid specification of human pluripotent stem cells to functional astrocytes

Author

Lendemeijer, B., primary, Unkel, M., additional, Mossink, B., additional, Hijazi, S., additional, Sampedro, S.G., additional, Shpak, G., additional, Slump, D.E., additional, van den Hout, M.C.G.N., additional, van IJcken, W.F.J., additional, Bindels, E.M.J., additional, Hoogendijk, W.J.G., additional, Nadif Kasri, N., additional, de Vrij, F.M.S., additional, and Kushner, S.A., additional

Published

2022

5. Schizophrenia polygenic risk is associated with child mental health problems through early childhood adversity

Author

Bolhuis, K., Steenkamp, L.R., Blanken, L.M.E., Neumann, A., Jansen, P.R., Hillegers, M.H.J., Cecil, C.A.M., Tiemeier, H., and Kushner, S.A.

Subjects

Stressful life events, Generation R, Gene–environment, Population-based, Psychosis

Abstract

Previous studies have shown that schizophrenia polygenic risk predicts a multitude of mental health problems in the general population. Yet it is unclear by which mechanisms these associations arise. Here, we explored a possible gene-environment correlation in the association of schizophrenia polygenic risk with mental health problems via childhood adversity. This study was embedded in the population-based Generation R Study, including N = 1901 participants with genotyping for schizophrenia polygenic risk, maternal reporting of childhood adversity, and Child Behaviour Checklist measurement of mental health problems. Independent replication was attempted in the Avon Longitudinal Study of Parents and Children (ALSPAC; N = 3641). Associations were analysed with Poisson regression and statistical mediation analysis. Higher burden of schizophrenia polygenic risk was associated with greater exposure to childhood adversity (P-value threshold < 0.5: Generation R Study, OR = 1.08, 95%CI 1.02-1.15, P = 0.01; ALSPAC, OR = 1.02, 95%CI 1.01-1.03, P < 0.01). Childhood adversities partly explained the relationship of schizophrenia polygenic risk with emotional, attention, and thought problems (proportion explained, range 5-23%). Direct effects of schizophrenia polygenic risk and adversity on mental health outcomes were also observed. In summary, genetic liability to schizophrenia increased the risk for mental health problems in the general paediatric population through childhood adversity. Although this finding could result from a mediated causal relationship between genotype and mental health, we argue that these observations most likely reflect a gene-environment correlation, i.e. adversities are a marker for the genetic risk that parents transmit to children. These and similar recent findings raise important conceptual questions about preventative interventions aimed at reducing childhood adversities.

Published

2021

6. Genome-wide association study of more than 40,000 bipolar disorder cases provides new insights into the underlying biology

Author

Mullins, N. Forstner, A.J. O’Connell, K.S. Coombes, B. Coleman, J.R.I. Qiao, Z. Als, T.D. Bigdeli, T.B. Børte, S. Bryois, J. Charney, A.W. Drange, O.K. Gandal, M.J. Hagenaars, S.P. Ikeda, M. Kamitaki, N. Kim, M. Krebs, K. Panagiotaropoulou, G. Schilder, B.M. Sloofman, L.G. Steinberg, S. Trubetskoy, V. Winsvold, B.S. Won, H.-H. Abramova, L. Adorjan, K. Agerbo, E. Al Eissa, M. Albani, D. Alliey-Rodriguez, N. Anjorin, A. Antilla, V. Antoniou, A. Awasthi, S. Baek, J.H. Bækvad-Hansen, M. Bass, N. Bauer, M. Beins, E.C. Bergen, S.E. Birner, A. Bøcker Pedersen, C. Bøen, E. Boks, M.P. Bosch, R. Brum, M. Brumpton, B.M. Brunkhorst-Kanaan, N. Budde, M. Bybjerg-Grauholm, J. Byerley, W. Cairns, M. Casas, M. Cervantes, P. Clarke, T.-K. Cruceanu, C. Cuellar-Barboza, A. Cunningham, J. Curtis, D. Czerski, P.M. Dale, A.M. Dalkner, N. David, F.S. Degenhardt, F. Djurovic, S. Dobbyn, A.L. Douzenis, A. Elvsåshagen, T. Escott-Price, V. Ferrier, I.N. Fiorentino, A. Foroud, T.M. Forty, L. Frank, J. Frei, O. Freimer, N.B. Frisén, L. Gade, K. Garnham, J. Gelernter, J. Giørtz Pedersen, M. Gizer, I.R. Gordon, S.D. Gordon-Smith, K. Greenwood, T.A. Grove, J. Guzman-Parra, J. Ha, K. Haraldsson, M. Hautzinger, M. Heilbronner, U. Hellgren, D. Herms, S. Hoffmann, P. Holmans, P.A. Huckins, L. Jamain, S. Johnson, J.S. Kalman, J.L. Kamatani, Y. Kennedy, J.L. Kittel-Schneider, S. Knowles, J.A. Kogevinas, M. Koromina, M. Kranz, T.M. Kranzler, H.R. Kubo, M. Kupka, R. Kushner, S.A. Lavebratt, C. Lawrence, J. Leber, M. Lee, H.-J. Lee, P.H. Levy, S.E. Lewis, C. Liao, C. Lucae, S. Lundberg, M. MacIntyre, D.J. Magnusson, S.H. Maier, W. Maihofer, A. Malaspina, D. Maratou, E. Martinsson, L. Mattheisen, M. McCarroll, S.A. McGregor, N.W. McGuffin, P. McKay, J.D. Medeiros, H. Medland, S.E. Millischer, V. Montgomery, G.W. Moran, J.L. Morris, D.W. Mühleisen, T.W. O’Brien, N. O’Donovan, C. Olde Loohuis, L.M. Oruc, L. Papiol, S. Pardiñas, A.F. Perry, A. Pfennig, A. Porichi, E. Potash, J.B. Quested, D. Raj, T. Rapaport, M.H. DePaulo, J.R. Regeer, E.J. Rice, J.P. Rivas, F. Rivera, M. Roth, J. Roussos, P. Ruderfer, D.M. Sánchez-Mora, C. Schulte, E.C. Senner, F. Sharp, S. Shilling, P.D. Sigurdsson, E. Sirignano, L. Slaney, C. Smeland, O.B. Smith, D.J. Sobell, J.L. Søholm Hansen, C. Soler Artigas, M. Spijker, A.T. Stein, D.J. Strauss, J.S. Świątkowska, B. Terao, C. Thorgeirsson, T.E. Toma, C. Tooney, P. Tsermpini, E.-E. Vawter, M.P. Vedder, H. Walters, J.T.R. Witt, S.H. Xi, S. Xu, W. Yang, J.M.K. Young, A.H. Young, H. Zandi, P.P. Zhou, H. Zillich, L. Adolfsson, R. Agartz, I. Alda, M. Alfredsson, L. Babadjanova, G. Backlund, L. Baune, B.T. Bellivier, F. Bengesser, S. Berrettini, W.H. Blackwood, D.H.R. Boehnke, M. Børglum, A.D. Breen, G. Carr, V.J. Catts, S. Corvin, A. Craddock, N. Dannlowski, U. Dikeos, D. Esko, T. Etain, B. Ferentinos, P. Frye, M. Fullerton, J.M. Gawlik, M. Gershon, E.S. Goes, F.S. Green, M.J. Grigoroiu-Serbanescu, M. Hauser, J. Henskens, F. Hillert, J. Hong, K.S. Hougaard, D.M. Hultman, C.M. Hveem, K. Iwata, N. Jablensky, A.V. Jones, I. Jones, L.A. Kahn, R.S. Kelsoe, J.R. Kirov, G. Landén, M. Leboyer, M. Lewis, C.M. Li, Q.S. Lissowska, J. Lochner, C. Loughland, C. Martin, N.G. Mathews, C.A. Mayoral, F. McElroy, S.L. McIntosh, A.M. McMahon, F.J. Melle, I. Michie, P. Milani, L. Mitchell, P.B. Morken, G. Mors, O. Mortensen, P.B. Mowry, B. Müller-Myhsok, B. Myers, R.M. Neale, B.M. Nievergelt, C.M. Nordentoft, M. Nöthen, M.M. O’Donovan, M.C. Oedegaard, K.J. Olsson, T. Owen, M.J. Paciga, S.A. Pantelis, C. Pato, C. Pato, M.T. Patrinos, G.P. Perlis, R.H. Posthuma, D. Ramos-Quiroga, J.A. Reif, A. Reininghaus, E.Z. Ribasés, M. Rietschel, M. Ripke, S. Rouleau, G.A. Saito, T. Schall, U. Schalling, M. Schofield, P.R. Schulze, T.G. Scott, L.J. Scott, R.J. Serretti, A. Shannon Weickert, C. Smoller, J.W. Stefansson, H. Stefansson, K. Stordal, E. Streit, F. Sullivan, P.F. Turecki, G. Vaaler, A.E. Vieta, E. Vincent, J.B. Waldman, I.D. Weickert, T.W. Werge, T. Wray, N.R. Zwart, J.-A. Biernacka, J.M. Nurnberger, J.I. Cichon, S. Edenberg, H.J. Stahl, E.A. McQuillin, A. Di Florio, A. Ophoff, R.A. Andreassen, O.A. HUNT All-In Psychiatry

Abstract

Bipolar disorder is a heritable mental illness with complex etiology. We performed a genome-wide association study of 41,917 bipolar disorder cases and 371,549 controls of European ancestry, which identified 64 associated genomic loci. Bipolar disorder risk alleles were enriched in genes in synaptic signaling pathways and brain-expressed genes, particularly those with high specificity of expression in neurons of the prefrontal cortex and hippocampus. Significant signal enrichment was found in genes encoding targets of antipsychotics, calcium channel blockers, antiepileptics and anesthetics. Integrating expression quantitative trait locus data implicated 15 genes robustly linked to bipolar disorder via gene expression, encoding druggable targets such as HTR6, MCHR1, DCLK3 and FURIN. Analyses of bipolar disorder subtypes indicated high but imperfect genetic correlation between bipolar disorder type I and II and identified additional associated loci. Together, these results advance our understanding of the biological etiology of bipolar disorder, identify novel therapeutic leads and prioritize genes for functional follow-up studies. © 2021, The Author(s), under exclusive licence to Springer Nature America, Inc.

Published

2021

7. GenNet framework: interpretable deep learning for predicting phenotypes from genetic data

Author

Hilten, A. van, Kushner, S.A., Kayser, M., Ikram, M.Arfan, Adams, H.H.H., Klaver, C.C.W., Niessen, W.J., Roshchupkin, G.V., Hilten, A. van, Kushner, S.A., Kayser, M., Ikram, M.Arfan, Adams, H.H.H., Klaver, C.C.W., Niessen, W.J., and Roshchupkin, G.V.

Abstract

Contains fulltext : 243996.pdf (Publisher’s version ) (Open Access), Applying deep learning in population genomics is challenging because of computational issues and lack of interpretable models. Here, we propose GenNet, a novel open-source deep learning framework for predicting phenotypes from genetic variants. In this framework, interpretable and memory-efficient neural network architectures are constructed by embedding biologically knowledge from public databases, resulting in neural networks that contain only biologically plausible connections. We applied the framework to seventeen phenotypes and found well-replicated genes such as HERC2 and OCA2 for hair and eye color, and novel genes such as ZNF773 and PCNT for schizophrenia. Additionally, the framework identified ubiquitin mediated proteolysis, endocrine system and viral infectious diseases as most predictive biological pathways for schizophrenia. GenNet is a freely available, end-to-end deep learning framework that allows researchers to develop and use interpretable neural networks to obtain novel insights into the genetic architecture of complex traits and diseases.

Published

2021

8. The continued need for animals to advance brain research

Author

Homberg, J.R., Adan, R.A., Alenina, N., Asiminas, A., Bader, M., Beckers, T., Begg, D.P., Blokland, A., Burger, M.E., Dijk, G. Van, Eisel, U.L., Elgersma, Y., Englitz, B., Fernandez-Ruiz, A., Fitzsimons, C.P., Dam, A.M.W. van, Gass, P., Grandjean, J., Havekes, R., Henckens, M.J.A.G., Herden, C., Hut, R.A., Jarrett, W., Jeffrey, K., Jezova, D., Kalsbeek, A., Kamermans, M., Kas, M.J., Nadif Kasri, N., Kiliaan, A.J., Kolk, S.M., Korosi, A., Korte, S.M., Kozicz, T., Kushner, S.A., Leech, K., Lesch, K.P., Lesscher, H., Lucassen, P.J., Luthi, A., Ma, L., Mallien, A.S., Meerlo, P., Mejias, J.F., Meye, F.J., Mitchell, A.S., Mul, J.D., Olcese, U., González, A.O., Olivier, J.D., Pasqualetti, M., Pennartz, C.M.A., Popik, P., Prickaerts, J., Prida, L.M. de la, Ribeiro, S., Roozendaal, B., Rossato, J.I., Salari, A.A., Schoemaker, R.G., Smit, A.B., Vanderschuren, L., Takeuchi, T., Veen, R. van der, Smidt, M.P., Vyazovskiy, V.V., Wiesmann, M., Wierenga, C.J., Williams, B., Willuhn, I., Wöhr, M., Wolvekamp, M., Zee, E.A. van der, Genzel, L., Homberg, J.R., Adan, R.A., Alenina, N., Asiminas, A., Bader, M., Beckers, T., Begg, D.P., Blokland, A., Burger, M.E., Dijk, G. Van, Eisel, U.L., Elgersma, Y., Englitz, B., Fernandez-Ruiz, A., Fitzsimons, C.P., Dam, A.M.W. van, Gass, P., Grandjean, J., Havekes, R., Henckens, M.J.A.G., Herden, C., Hut, R.A., Jarrett, W., Jeffrey, K., Jezova, D., Kalsbeek, A., Kamermans, M., Kas, M.J., Nadif Kasri, N., Kiliaan, A.J., Kolk, S.M., Korosi, A., Korte, S.M., Kozicz, T., Kushner, S.A., Leech, K., Lesch, K.P., Lesscher, H., Lucassen, P.J., Luthi, A., Ma, L., Mallien, A.S., Meerlo, P., Mejias, J.F., Meye, F.J., Mitchell, A.S., Mul, J.D., Olcese, U., González, A.O., Olivier, J.D., Pasqualetti, M., Pennartz, C.M.A., Popik, P., Prickaerts, J., Prida, L.M. de la, Ribeiro, S., Roozendaal, B., Rossato, J.I., Salari, A.A., Schoemaker, R.G., Smit, A.B., Vanderschuren, L., Takeuchi, T., Veen, R. van der, Smidt, M.P., Vyazovskiy, V.V., Wiesmann, M., Wierenga, C.J., Williams, B., Willuhn, I., Wöhr, M., Wolvekamp, M., Zee, E.A. van der, and Genzel, L.

Abstract

Item does not contain fulltext, Policymakers aim to move toward animal-free alternatives for scientific research and have introduced very strict regulations for animal research. We argue that, for neuroscience research, until viable and translational alternatives become available and the value of these alternatives has been proven, the use of animals should not be compromised.

Published

2021

9. Peer-reported bullying, rejection and hallucinatory experiences in childhood

Author

Steenkamp, L.R. (Lisa R.), Tiemeier, H.W. (Henning), Bolhuis, K. (Koen), Hillegers, M.H.J. (Manon), Kushner, S.A. (Steven A.), Blanken, L.M.E. (Laura), Steenkamp, L.R. (Lisa R.), Tiemeier, H.W. (Henning), Bolhuis, K. (Koen), Hillegers, M.H.J. (Manon), Kushner, S.A. (Steven A.), and Blanken, L.M.E. (Laura)

Abstract

Objective: Psychotic experiences, such as hallucinations, occur commonly in children and have been related to bullying victimization. However, whether bullying perpetration, peer rejection, or peer acceptance are related to hallucinatory experiences has remained under-examined. We used a novel peer nomination method to examine whether (i) bullying perpetration and (ii) social positions within peer networks were associated with future hallucinatory experiences. Methods: This prospective study was embedded in the population-based Generation R Study. Bullying perpetration, peer rejection, and peer acceptance were assessed using peer nominations at age 7 years (N = 925). Using a social network analysis, we estimated social positions within peer rejection and acceptance networks. Bullying victimization was assessed using self-reports. Self-reported hallucinatory experiences were assessed at age 10 years. Analyses were adjusted for sociodemographic covariates. Results: Higher levels of bullying perpetration were prospectively associated with an increased burden of hallucinatory experiences (OR = 1.22, 95% CI 1.05–1.43, p = 0.011). Bullies had a 50% higher, and bully-victims had a 89% higher odds, of endorsing hallucinatory experiences three years later than children who were not involved in bullying (ORbully = 1.50, 95% CI 1.01–2.24, p = 0.045; ORbully-victim = 1.89, 95% CI 1.15–3.10, p = 0.012). Unfavorable positions within peer rejection networks, but not peer acceptance networks, were associated with an increased risk for hallucinatory experiences (ORpeer rejection = 1.24, 95% CI 1.07–1.44, pFDR-corrected = 0.024). Conclusion: Using peer reports, we observed that bullies and socially rejected children have a higher likelihood to report hallucinatory experiences in pre-adolescence. Children who are both a bully and a victim of bullying (ie, bully-victims) may be particularly vulnerable for psychotic experiences.

Published

2021

10. Prolonged surgical duration in open craniofacial surgery: Detrimental to cognitive functioning?

Author

Vlugt, J.J.B. van der, Coebergh van den Braak, R.R.J., Meulen, J.J.M.N. van der, Hovius, S.E.R., Verhulst, F.C., Okkerse, J.M., Wierdsma, A.I., Kushner, S.A., Klimek, M., Vlugt, J.J.B. van der, Coebergh van den Braak, R.R.J., Meulen, J.J.M.N. van der, Hovius, S.E.R., Verhulst, F.C., Okkerse, J.M., Wierdsma, A.I., Kushner, S.A., and Klimek, M.

Abstract

Item does not contain fulltext

Published

2021

11. The continued need for animals to advance brain research

Author

University of Toronto, Homberg, J.R., Adan, R.A.H., Alenina, N., Asiminas, A., Bader, M., Beckers, T., Begg, D.P., Blokland, A., Burger, M.E., van Dijk, G., Eisel, U.L.M., Elgersma, Y., Englitz, B., Fernández-Ruiz, Antonio, Fitzsimons, C.P., van Dam, A.M., Gass, P., Grandjean, J., Havekes, R., Henckens, M.J.A.G., Herden, C., Hut, R.A., Jarrett, W., Jeffrey, K., Jezova, D., Kalsbeek, A., Kamermans, M., Kas, Martien J. H., Kasri, N.N., Kiliaan, A.J, Kolk, S.M., Korosi, A., Korte, S.M., Kozicz, T., Kushner, S.A., Leech, Kirk, Lesch, K.P., Lesscher, H., Lucassen, P.J., Luthi, A., Ma, L., Mallien, A.S., Meerlo, P., Mejías, Jorge F., Meye, F.J., Mitchell, A.S., Mul, J.D, Olcese, U., González, A.O., Olivier, Jocelien D.A., Pasqualetti, Massimo, Pennartz, Cyriel M.A., Popik, Piotr, Prickaerts, Jos, Menéndez de la Prida, Liset, Ribeiro, S., Roozendaal, B, Rossato, J.I., Salari, Ali-Akbar, Schoemaker, R.G., Smit, A.B., Vanderschuren, L.J.M.J., Takeuchi, T., van der Veen, Rixt, Smidt, M.P., Vyazovskiy, V.V., Wiesmann, M., Wierenga, C.J., Williams, B., Willuhn, I., Wo¨hr, M., Wolvekamp, M., van der Zee, E.A., Genzel, L., University of Toronto, Homberg, J.R., Adan, R.A.H., Alenina, N., Asiminas, A., Bader, M., Beckers, T., Begg, D.P., Blokland, A., Burger, M.E., van Dijk, G., Eisel, U.L.M., Elgersma, Y., Englitz, B., Fernández-Ruiz, Antonio, Fitzsimons, C.P., van Dam, A.M., Gass, P., Grandjean, J., Havekes, R., Henckens, M.J.A.G., Herden, C., Hut, R.A., Jarrett, W., Jeffrey, K., Jezova, D., Kalsbeek, A., Kamermans, M., Kas, Martien J. H., Kasri, N.N., Kiliaan, A.J, Kolk, S.M., Korosi, A., Korte, S.M., Kozicz, T., Kushner, S.A., Leech, Kirk, Lesch, K.P., Lesscher, H., Lucassen, P.J., Luthi, A., Ma, L., Mallien, A.S., Meerlo, P., Mejías, Jorge F., Meye, F.J., Mitchell, A.S., Mul, J.D, Olcese, U., González, A.O., Olivier, Jocelien D.A., Pasqualetti, Massimo, Pennartz, Cyriel M.A., Popik, Piotr, Prickaerts, Jos, Menéndez de la Prida, Liset, Ribeiro, S., Roozendaal, B, Rossato, J.I., Salari, Ali-Akbar, Schoemaker, R.G., Smit, A.B., Vanderschuren, L.J.M.J., Takeuchi, T., van der Veen, Rixt, Smidt, M.P., Vyazovskiy, V.V., Wiesmann, M., Wierenga, C.J., Williams, B., Willuhn, I., Wo¨hr, M., Wolvekamp, M., van der Zee, E.A., and Genzel, L.

Abstract

Policymakers aim to move toward animal-free alternatives for scientific research and have introduced very strict regulations for animal research. We argue that, for neuroscience research, until viable and translational alternatives become available and the value of these alternatives has been proven, the use of animals should not be compromised.

Published

2021

12. Conserved UBE3A subcellular distribution between human and mice is facilitated by non-homologous isoforms

Author

Zampeta, F. Isabella, Sonzogni, Monica, Niggl, Eva, Lendemeijer, B. (Bas), Smeenk, H.G., Vrij, F.M.S. (Femke), Kushner, S.A. (Steven), Distel, Ben, Elgersma, Y. (Ype), Zampeta, F. Isabella, Sonzogni, Monica, Niggl, Eva, Lendemeijer, B. (Bas), Smeenk, H.G., Vrij, F.M.S. (Femke), Kushner, S.A. (Steven), Distel, Ben, and Elgersma, Y. (Ype)

Abstract

The human UBE3A gene, which is essential for normal neurodevelopment, encodes three Ubiquitin E3 ligase A (UBE3A) protein isoforms. However, the subcellular localization and relative abundance of these human UBE3A isoforms are unknown. We found, as previously reported in mice, that UBE3A is predominantly nuclear in human neurons. However, this conserved subcellular distribution is achieved by strikingly distinct cis-acting mechanisms. A single amino-acid deletion in the N-terminus of human hUBE3A-Iso3, which is homologous to cytosolic mouse mUBE3A-Iso2, results in its translocation to the nucleus. This singe amino-acid deletion is shared with apes and Old World monkeys and was preceded by the appearance of the cytosolic hUBE3A-Iso2 isoform. This hUBE3A-Iso2 isoform arose after the lineage of New World monkeys and Old World monkeys separated from the Tarsiers (Tarsiidae). Due to the loss of a si

Published

2020

13. Motor cortical excitability and plasticity in patients with neurofibromatosis type 1

Author

Castricum, J., Tulen, J.H.M. (Joke), Taal, W. (Walter), Ottenhoff, M.J. (Myrthe), Kushner, S.A. (Steven), Elgersma, Y. (Ype), Castricum, J., Tulen, J.H.M. (Joke), Taal, W. (Walter), Ottenhoff, M.J. (Myrthe), Kushner, S.A. (Steven), and Elgersma, Y. (Ype)

Abstract

Objective: Neurofibromatosis type 1 (NF1) is an autosomal dominant genetic disorder that is associated with cognitive disabilities. Based on studies involving animals, the hypothesized cause of these disabilities results from increased activity of inhibitory interneurons that decreases synaptic plasticity. We obtained transcranial magnetic stimulation (TMS)-based measures of cortical

Published

2020

14. Psychotic experiences and future school performance in childhood: a population-based cohort study

Author

Steenkamp, L.R. (Lisa R.), Bolhuis, K. (Koen), Blanken, L.M.E. (Laura), Luijk, P.C.M. (Maartje), Hillegers, M.H.J. (Manon), Kushner, S.A. (Steven), Tiemeier, H.W. (Henning), Steenkamp, L.R. (Lisa R.), Bolhuis, K. (Koen), Blanken, L.M.E. (Laura), Luijk, P.C.M. (Maartje), Hillegers, M.H.J. (Manon), Kushner, S.A. (Steven), and Tiemeier, H.W. (Henning)

Abstract

BACKGROUND: Psychotic experiences are common in childhood and an important risk indicator of adverse mental health outcomes. However, little is known about the association of psychotic experiences with functional outcomes in childhood, particularly regarding school performance. The aim of the present study was to examine whether psychotic experiences were prospectively related to school performance in childhood. METHODS: This study was embedded in the population-based Generation R Study (N = 2,362). Psychotic experiences were assessed using self-reports on hallucinations at age 10 years. School performance was assessed using a standardized national school performance test at age 12 years. We considered the total school performance score, as well as language and mathematics subscales. Analyses were adjusted for sociodemographic characteristics, maternal nonverbal IQ, nonverbal IQ at age 6 years and co-occurring psychopathology at age 10 years. RESULTS: Psychotic experiences were prospectively associated with poorer school performance scores (B = -0.61, 95% CI [-0.98;-0.25], p = .001), as well as poorer language (Bpercentile rank score = -2.00, 95% CI [-3.20;-0.79], p = .001) and mathematical ability (Bpercentile rank score = -1.75, 95% CI [-2.99;-0.51], p = .006). These associations remained after additional adjustment for nonverbal IQ at age 6 years (B = -0.51, 95% CI [-0.86;-0.16], p = .005), and co-occurring internalizing (B = -0.40, 95% CI [-0.77;-0.03], p = .036) and externalizing problems (B = -0.40, 95% CI [-0.75;-0.04], p = .029), but not attention problems (B = -0.10, 95% CI [-0.47;0.26], p = .57). CONCLUSIONS: Children with psychotic experiences had lower school performance scores than their nonaffected peers. The finding was independent of sociodemographic characteristics, intelligence and co-occurring internalizing and externalizing problems, but not attention problems. This study suggests that psychotic experiences are associated with childhood functio

Published

2020

15. Genetic risk for Alzheimer disease in children: Evidence from early-life IQ and brain white-matter microstructure

Author

Vinueza Veloz, M.F. (Maria), Martín-Román, C. (Carlos), Robalino-Valdivieso, M.P. (María Paulina), White, T.J.H. (Tonya), Kushner, S.A. (Steven), Zeeuw, C.I. (Chris) de, Vinueza Veloz, M.F. (Maria), Martín-Román, C. (Carlos), Robalino-Valdivieso, M.P. (María Paulina), White, T.J.H. (Tonya), Kushner, S.A. (Steven), and Zeeuw, C.I. (Chris) de

Abstract

It remains unclear whether the genetic risk for late-onset Alzheimer disease (AD) is linked to premorbid individual differences in general cognitive ability and brain structure. The objective of the present study was to determine whether the genetic risk of late-onset AD is related to premorbid individual differences in intelligence quotient (IQ) and characteristics of the cerebral white-matter in children. The study sample included children of the Generation R Study from Rotterdam, The Netherlands. IQ was measured using a well-validated Dutch nonverbal IQ test (n = 1908) at ages 5 to 9 years. White-matter microstructure was assessed by measuring fractional anisotropy (FA) of whit

Published

2020

16. Synthetic Polymers Provide a Robust Substrate for Functional Neuron Culture

Author

Zhang, Y. (Yichuan), Venkateswaran, S. (Seshasailam), Higuera, G.A. (Gustavo A.), Nath, S. (Suvra), Shpak, G. (Guy), Matray, J. (Jeffrey), Fratila-Apachitei, L.E. (L.), Zadpoor, A.A. (Amir Abbas), Kushner, S.A. (Steven), Bradley, M. (Mark), Zeeuw, C.I. (Chris) de, Zhang, Y. (Yichuan), Venkateswaran, S. (Seshasailam), Higuera, G.A. (Gustavo A.), Nath, S. (Suvra), Shpak, G. (Guy), Matray, J. (Jeffrey), Fratila-Apachitei, L.E. (L.), Zadpoor, A.A. (Amir Abbas), Kushner, S.A. (Steven), Bradley, M. (Mark), and Zeeuw, C.I. (Chris) de

Abstract

Substrates for neuron culture and implantation are required to be both biocompatible and display surface compositions that support cell attachment, growth, differentiation, and neural activity. Laminin, a naturally occurring extracellular matrix protein is the most widely used substrate for neuron culture and fulfills some of these requirements, however, it is expensive, unstable (compared to synthetic materials), and prone to batch-to-batch variation. This study uses a high-throughput polymer screening approach to identify synthetic polymers that supports the in vitro culture of primary mouse cerebellar neurons. This allows the identification of materials that enable primary c

Published

2020

17. How the COVID-19 pandemic highlights the necessity of animal research

Author

Genzel, L., Adan, R., Berns, A., Beucken, J.J.J.P van den, Blokland, A., Boddeke, E., Bogers, W.M., Bontrop, R., Bulthuis, R., Bousema, T., Clevers, H., Coenen, T., Dam, A.V., Deen, P.M.T., Dijk, K.W. van, Eggen, B.J.L., Elgersma, Y., Erdogan, I., Englitz, B., Fentener van Vlissingen, J.M., Fleur, S. la, Fouchier, R., Fitzsimons, C.P., Frieling, W., Haagmans, B., Heesters, B.A., Henckens, M.J.A.G., Herfst, S., Hol, E., Hove, D. van den, Jonge, M.I. de, Jonkers, J., Joosten, L.A.B., Kalsbeek, A., Kamermans, M., Kampinga, H.H., Kas, M.J., Keijer, J., Kersten, Sander, Kiliaan, A.J., Kooij, T.W., Kooijman, S., Koopman, W.J.H., Korosi, A., Krugers, H.J., Kuiken, T., Kushner, S.A., Langermans, J.A., Lesscher, H., Lucassen, P.J., Lutgens, E., Netea, M.G., Noldus, L.P.J.J., Meer, J.W.M. van der, Meye, F.J., Mul, J.D., Oers, K. van, Olivier, J.D., Pasterkamp, R.J., Philippens, I., Prickaerts, J., Pullox, B.J.A., Rensen, P.C., Rheenen, J. van, Rij, R.P. van, Ritsma, L., Rockx, B.H.G., Roozendaal, B., Schothorst, E.M. van, Stittelaar, K., Stockhofe, N., Swaab, D.F., Swart, R.L. de, Vanderschuren, L., Vries, T. de, Vrij, F. de, Wezel, R.J.A. van, Wierenga, C.J., Wiesmann, M., Willuhn, I., Zeeuw, C.I. de, Homberg, J.R., Genzel, L., Adan, R., Berns, A., Beucken, J.J.J.P van den, Blokland, A., Boddeke, E., Bogers, W.M., Bontrop, R., Bulthuis, R., Bousema, T., Clevers, H., Coenen, T., Dam, A.V., Deen, P.M.T., Dijk, K.W. van, Eggen, B.J.L., Elgersma, Y., Erdogan, I., Englitz, B., Fentener van Vlissingen, J.M., Fleur, S. la, Fouchier, R., Fitzsimons, C.P., Frieling, W., Haagmans, B., Heesters, B.A., Henckens, M.J.A.G., Herfst, S., Hol, E., Hove, D. van den, Jonge, M.I. de, Jonkers, J., Joosten, L.A.B., Kalsbeek, A., Kamermans, M., Kampinga, H.H., Kas, M.J., Keijer, J., Kersten, Sander, Kiliaan, A.J., Kooij, T.W., Kooijman, S., Koopman, W.J.H., Korosi, A., Krugers, H.J., Kuiken, T., Kushner, S.A., Langermans, J.A., Lesscher, H., Lucassen, P.J., Lutgens, E., Netea, M.G., Noldus, L.P.J.J., Meer, J.W.M. van der, Meye, F.J., Mul, J.D., Oers, K. van, Olivier, J.D., Pasterkamp, R.J., Philippens, I., Prickaerts, J., Pullox, B.J.A., Rensen, P.C., Rheenen, J. van, Rij, R.P. van, Ritsma, L., Rockx, B.H.G., Roozendaal, B., Schothorst, E.M. van, Stittelaar, K., Stockhofe, N., Swaab, D.F., Swart, R.L. de, Vanderschuren, L., Vries, T. de, Vrij, F. de, Wezel, R.J.A. van, Wierenga, C.J., Wiesmann, M., Willuhn, I., Zeeuw, C.I. de, and Homberg, J.R.

Abstract

Contains fulltext : 225123.pdf (publisher's version ) (Closed access), Recently, a petition was offered to the European Commission calling for an immediate ban on animal testing. Although a Europe-wide moratorium on the use of animals in science is not yet possible, there has been a push by the non-scientific community and politicians for a rapid transition to animal-free innovations. Although there are benefits for both animal welfare and researchers, advances on alternative methods have not progressed enough to be able to replace animal research in the foreseeable future. This trend has led first and foremost to a substantial increase in the administrative burden and hurdles required to make timely advances in research and treatments for human and animal diseases. The current COVID-19 pandemic clearly highlights how much we actually rely on animal research. COVID-19 affects several organs and systems, and the various animal-free alternatives currently available do not come close to this complexity. In this Essay, we therefore argue that the use of animals is essential for the advancement of human and veterinary health.

Published

2020

18. Novel genetic loci affecting facial shape variation in humans

Author

Xiong, Z. (Ziyi), Dankova, G. (Gabriela), Howe, L.J. (Laurence J.), Lee, M.K. (Myoung Keun), Hysi, P.G. (Pirro G.), Jong, M.A. (Markus) de, Zhu, G. (Gu), Adhikari, K. (Kaustubh), Li, D. (Dan), Li, Y. (Yi), Pan, B. (Bo), Feingold, E. (Eleanor), Marazita, M.L. (Mary), Shaffer, J.R. (John R), McAloney, K. (Kerrie), Xu, S. (Shuhua), Jin, L. (Li), Wang, S. (Sijia), Vrij, F.M.S. (Femke), Lendemeijer, B. (Bas), Richmond, S. (Stephen), Zhurov, A. (Alexei), Lewis, S. (Sarah), Sharp, G.C. (Gemma C.), Paternoster, L. (Lavinia), Thompson, H. (Holly), Gonzalez-Jose, R. (Rolando), Bortolini, M.C. (Maria Catira), Canizales-Quinteros, S. (Samuel), Gallo, C. (Carla), Poletti, G. (Giovanni), Bedoya, E.G. (Elsie), Rothhammer, F. (Francisco), Uitterlinden, A.G. (André), Ikram, M.A. (Arfan), Wolvius, E.B. (Eppo), Kushner, S.A. (Steven), Nijsten, T.E.C. (Tamar), Palstra, R.-J.T.S. (Robert-Jan), Boehringer, S. (Stefan), Medland, S.E. (Sarah), Tang, K. (Kun), Ruiz-Linares, A. (Andres), Martin, N.G. (Nicholas), Spector, T.D. (Timothy), Stergiakouli, E. (Evie), Weinberg, S.M. (Seth M.), Liu, F. (Fan), Kayser, M.H. (Manfred), Xiong, Z. (Ziyi), Dankova, G. (Gabriela), Howe, L.J. (Laurence J.), Lee, M.K. (Myoung Keun), Hysi, P.G. (Pirro G.), Jong, M.A. (Markus) de, Zhu, G. (Gu), Adhikari, K. (Kaustubh), Li, D. (Dan), Li, Y. (Yi), Pan, B. (Bo), Feingold, E. (Eleanor), Marazita, M.L. (Mary), Shaffer, J.R. (John R), McAloney, K. (Kerrie), Xu, S. (Shuhua), Jin, L. (Li), Wang, S. (Sijia), Vrij, F.M.S. (Femke), Lendemeijer, B. (Bas), Richmond, S. (Stephen), Zhurov, A. (Alexei), Lewis, S. (Sarah), Sharp, G.C. (Gemma C.), Paternoster, L. (Lavinia), Thompson, H. (Holly), Gonzalez-Jose, R. (Rolando), Bortolini, M.C. (Maria Catira), Canizales-Quinteros, S. (Samuel), Gallo, C. (Carla), Poletti, G. (Giovanni), Bedoya, E.G. (Elsie), Rothhammer, F. (Francisco), Uitterlinden, A.G. (André), Ikram, M.A. (Arfan), Wolvius, E.B. (Eppo), Kushner, S.A. (Steven), Nijsten, T.E.C. (Tamar), Palstra, R.-J.T.S. (Robert-Jan), Boehringer, S. (Stefan), Medland, S.E. (Sarah), Tang, K. (Kun), Ruiz-Linares, A. (Andres), Martin, N.G. (Nicholas), Spector, T.D. (Timothy), Stergiakouli, E. (Evie), Weinberg, S.M. (Seth M.), Liu, F. (Fan), and Kayser, M.H. (Manfred)

Abstract

The human face represents a combined set of highly heritable phenotypes, but knowledge on its genetic architecture remains limited, despite the relevance for various fields. A series of genome-wide association studies on 78 facial shape phenotypes quantified from 3-dimensional facial images of 10,115 Europeans identified 24 genetic loci reaching study-wide suggestive association (p < 5 × 10-8), among which 17 were previously unreported. A follow-up multi-ethnic study in additional 7917 individuals confirmed 10 loci including six unreported ones (padjusted < 2.1 × 10-3). A global map of derived polygenic face scores assembled facial features in major continental groups consistent with anthropological knowledge. Analyses of epigenomic datasets from cranial neural crest cells revealed abundant cis-regulatory activities at the face-associated genetic loci. Luciferase reporter assays in neural crest progenitor cells highlighted enhancer activities of several face-associated DNA variants. These results substantially advance our understanding of the genetic basis underlying human facial variation and provide candidates for future in-vivo functional studies.

Published

2019

19. Local axonal morphology guides the topography of interneuron myelination in mouse and human neocortex

Author

Stedehouder, J. (Jeffrey), Brizee, D. (D.), Slotman, J.A. (Johan A.), Pascual-García, M. (M.), Leyrer, M.L. (M. L.), Bouwen, B.L.J. (B. L.J.), Dirven, C.M.F. (Clemens), Gao, Z. (Z.), Berson, D.M. (D. M.), Houtsmuller, A.B. (Adriaan), Kushner, S.A. (Steven), Stedehouder, J. (Jeffrey), Brizee, D. (D.), Slotman, J.A. (Johan A.), Pascual-García, M. (M.), Leyrer, M.L. (M. L.), Bouwen, B.L.J. (B. L.J.), Dirven, C.M.F. (Clemens), Gao, Z. (Z.), Berson, D.M. (D. M.), Houtsmuller, A.B. (Adriaan), and Kushner, S.A. (Steven)

Abstract

GABAergic fast-spiking parvalbumin-positive (PV) interneurons are frequently myelinated in the cerebral cortex. However, the factors governing the topography of cortical interneuron myelination remain incompletely understood. Here, we report that segmental myelination along neocortical interneuron axons is strongly predicted by the joint combination of interbranch distance and local axon caliber. Enlargement of PV+ interneurons increased axonal myelination, while reduced cell size led to decreased myelination. Next, we considered regular-spiking SOM+ cells, which normally have relatively shorter interbranch distances and thinner axon diameters than PV+ cells, and are rarely myelinated. Consistent with the importance of axonal morphology for guiding interneuron myelination, enlargement of SOM+ cell size dramatically increased the frequency of myelinated axonal segments. Lastly, we confirm that these findings also extend to human neocortex by quantifying interneuron axonal myelination from ex vivo surgical tissue. Together, these findings establish a predictive model of neocortical GABAergic interneuron myelination determined by 42 local axonal morphology.

Published

2019

20. Engram-specific transcriptome profiling of contextual memory consolidation

Author

Rao-Ruiz, P. (Priyanka), Couey, J.J., Marcelo, IM, Bouwkamp, C.G. (Christian), Zee, R. (Ruurd) van der, Matos, M.R., van der Loo, RJ, Martins, G.J., Hout, M. (Marcel) van den, IJcken, W.F.J. (Wilfred) van, Costa, R.M. (Rui), van den Oever, M.C., Kushner, S.A. (Steven), Rao-Ruiz, P. (Priyanka), Couey, J.J., Marcelo, IM, Bouwkamp, C.G. (Christian), Zee, R. (Ruurd) van der, Matos, M.R., van der Loo, RJ, Martins, G.J., Hout, M. (Marcel) van den, IJcken, W.F.J. (Wilfred) van, Costa, R.M. (Rui), van den Oever, M.C., and Kushner, S.A. (Steven)

Abstract

Sparse populations of neurons in the dentate gyrus (DG) of the hippocampus are causally implicated in the encoding of contextual fear memories. However, engram-specific molecular mechanisms underlying memory consolidation remain largely unknown. Here we perform unbiased RNA sequencing of DG engram neurons 24 h after contextual fear conditioning to identify transcriptome changes specific to memory consolidation. DG engram neurons exhibit a highly distinct pattern of gene expression, in which CREB-dependent transcription features prominently (P = 6.2 × 10−13), including Atf3 (P = 2.4 × 10−41), Penk (P = 1.3 × 10−15), and Kcnq3 (P = 3.1 × 10−12). Moreover, we validate the functional relevance of the RNAseq findings by establishing the causal requirement of intact CREB function specifically within the DG engram during memory consolidation, and identify a novel group of CREB target genes involved in the encoding of long-term memory.

Published

2019

21. Interaction of schizophrenia polygenic risk and cortisol level on pre-adolescent brain structure

Author

Bolhuis, K. (Koen), Tiemeier, H.W. (Henning), Jansen, P.R. (Philip), Muetzel, R.L. (Ryan), Neumann, A. (Alexander), Hillegers, M.H.J. (Manon), van den Akker, E.T.L. (Erica T.L.), Rossum, E.F.C. (Liesbeth) van, Jaddoe, V.W.V. (Vincent), Vernooij, M.W. (Meike W.), White, T. (Tonya), Kushner, S.A. (Steven A.), Bolhuis, K. (Koen), Tiemeier, H.W. (Henning), Jansen, P.R. (Philip), Muetzel, R.L. (Ryan), Neumann, A. (Alexander), Hillegers, M.H.J. (Manon), van den Akker, E.T.L. (Erica T.L.), Rossum, E.F.C. (Liesbeth) van, Jaddoe, V.W.V. (Vincent), Vernooij, M.W. (Meike W.), White, T. (Tonya), and Kushner, S.A. (Steven A.)

Abstract

The etiology of schizophrenia is multi-factorial with early neurodevelopmental antecedents, likely to result from a complex interaction of genetic and environmental risk. However, few studies have examined how schizophrenia polygenic risk scores (PRS) are moderated by environmental factors in shaping neurodevelopmental brain structure, prior to the onset of psychotic symptoms. Here, we examined whether hair cortisol, a quantitative metric of chronic stress, moderated the association between genetic risk for schizophrenia and pre-adolescent brain structure. This study was embedded within the Generation R Study, involving pre-adolescents of European ancestry assessed regarding schizophrenia PRS, hair cortisol, and brain imaging (n = 498 structural; n = 526 diffusion tensor imaging). Linear regression was performed to determine the association between schizophrenia PRS, hair cortisol level, and brain imaging outcomes. Although no single measure exceeded the multiple testing threshold, nominally significant interactions were observed for total ventricle volume (P interaction = 0.02) and global white matter microstructure (P interaction = 0.01) – two of the most well replicated brain structural findings in schizophrenia. These findings provide suggestive evidence for the joint effects of schizophrenia liability and cortisol levels on brain correlates in the pediatric general population. Given the widely replicated finding of ventricular enlargement and lower white matter integrity among schizophrenia patients, our findings generate novel hypotheses for future research on ge

Published

2019

22. The intellectual disability-associated CAMK2G p.Arg292Pro mutation acts as a pathogenic gain-of-function

Author

Proietti-Onori, M. (Martina), Koopal, B. (Balwina), Everman, D.B. (David B.), Worthington, J.D. (Jessica D.), Jones, J.R. (Julie R.), Ploeg, M.A. (Melissa), Mientjes, E.J. (Edwin), Bon, B. (Bregje) van, Kleefstra, T. (Tjitske), Schulman, H. (Howard), Kushner, S.A. (Steven), Küry, S. (Sébastien), Elgersma, Y. (Ype), Woerden, G.M. (Geeske) van, Proietti-Onori, M. (Martina), Koopal, B. (Balwina), Everman, D.B. (David B.), Worthington, J.D. (Jessica D.), Jones, J.R. (Julie R.), Ploeg, M.A. (Melissa), Mientjes, E.J. (Edwin), Bon, B. (Bregje) van, Kleefstra, T. (Tjitske), Schulman, H. (Howard), Kushner, S.A. (Steven), Küry, S. (Sébastien), Elgersma, Y. (Ype), and Woerden, G.M. (Geeske) van

Abstract

The abundantly expressed calcium/calmodulin-dependent protein kinase II (CAMK2), alpha (CAMK2A), and beta (CAMK2B) isoforms are essential for learning and memory formation. Recently, a de novo candidate mutation (p.Arg292Pro) in the gamma isoform of CAMK2 (CAMK2G) was identified in a patient with severe intellectual disability (ID), but the mechanism(s) by which this mutation causes ID is unknown. Here, we identified a second, unrelated individual, with a de novo CAMK2G p.Arg292Pro mutation, and used in vivo and in vitro assays to assess the impact of this mutation on CAMK2G and neuronal function. We found that knockdown of CAMK2G results in inappropriate precocious neuronal maturation. We further found that the CAMK2G p.Arg292Pro mutation acts as a highly pathogenic gain-of-function mutation, leading to increased phosphotransferase activity and impaired neuronal maturation as well as impaired targeting of the nuclear CAMK2G isoform. Silencing the catalytic site of the CAMK2G p.Arg292Pro protein reversed the pathogenic effect of the p.Arg292Pro mutation on neuronal maturation, without rescuing its nuclear targeting. Taken together, our results reveal an indispensable function of CAMK2G in neurodevelopment and indicate that the CAMK2G p.Arg292Pro protein acts as a pathogenic gain-of-function mutation, through constitutive activity toward cytosolic targets, rather than impaired targeting to the nucleus.

Published

2018

23. The 5-HTTLPR genotype, early life adversity and cortisol responsivity to psychosocial stress in women

Author

Aleknavičiūtė, J. (Jūratė), Tulen, J.H.M. (Joke), Rijke, Y.B. (Yolanda) de, van der Kroeg, M., Kooiman, C.G., Kushner, S.A. (Steven), Aleknavičiūtė, J. (Jūratė), Tulen, J.H.M. (Joke), Rijke, Y.B. (Yolanda) de, van der Kroeg, M., Kooiman, C.G., and Kushner, S.A. (Steven)

Abstract

Background The serotonin transporter gene-linked polymorphic region (5-HTTLPR) has previously been associated with hypothalamus–pituitary–adrenal axis function. Moreover, it has been suggested that this association is moderated by an interaction with stressful life experiences. Aims To investigate the moderation of cortisol response to psychosocial stress by 5-HTTLPR genotype, either directly or through an interaction with early life stress. Method A total of 151 women, 85 of which had personality psychopathology, performed the Trier Social Stress Test while cortisol responsivity was assessed. Results The results demonstrate a main effect of genotype on cortisol responsivity. Women carrying two copies of the long version of 5-HTTLPR exhibited stronger cortisol responses to psychosocial stress than women with at least one copy of the short allele (P = 0.03). However, the proportion of the variance of stress-induced cortisol responsivity explained by 5-HTTLPR genotype was not further strengthened by including early life adversity as a moderating factor (P = 0.52). Conclusions Our results highlight the need to clarify gender-specific biological factors influencing the serotonergic system. Furthermore, our results suggest that childhood maltreatment, specifically during the first 15 years of life, is unlikely to exert a moderating influence of large effect on the relationship between the 5-HTTLPR genotype and cortisol responsivity to psychosocial stress. Declaration of interest None.

Published

2018

24. The zinc transporter SLC39A7 (ZIP7) is essential for regulation of cytosolic zinc levels s

Author

Woodruff, G. (Grace), Bouwkamp, C.G. (Christian), Vrij, F.M.S. (Femke), Lovenberg, T. (Timothy), Bonaventure, P. (Pascal), Kushner, S.A. (Steven A.), Harrington, A.W. (Anthony W.), Woodruff, G. (Grace), Bouwkamp, C.G. (Christian), Vrij, F.M.S. (Femke), Lovenberg, T. (Timothy), Bonaventure, P. (Pascal), Kushner, S.A. (Steven A.), and Harrington, A.W. (Anthony W.)

Abstract

Zinc homeostasis is a highly regulated process in mammalian cells that is critical for normal growth and development. Movement of zinc across cell compartments is controlled by two classes of transporters: Slc39a family members transport zinc into the cytosol from either the extracellular space or intracellular stores such as the endoplasmic reticulum (ER), whereas the SLC30A family mediates zinc efflux from the cytosol. In this study, we report that genetic ablation of SLC39A7 (ZIP7) results in decreased cytosolic zinc levels, increased ER zinc levels, impaired cell prolife

Published

2018

25. Long-term neurodevelopmental consequences of intrauterine exposure to lithium and antipsychotics: a systematic review and meta-analysis

Author

Poels, E.M.P. (Eline M. P.), Schrijver, L. (Lisanne), Kamperman, A.M. (Astrid), Hillegers, M.H.J. (Manon), Hoogendijk, W.J.G. (Witte), Kushner, S.A. (Steven), Roza, S.J. (Sabine), Poels, E.M.P. (Eline M. P.), Schrijver, L. (Lisanne), Kamperman, A.M. (Astrid), Hillegers, M.H.J. (Manon), Hoogendijk, W.J.G. (Witte), Kushner, S.A. (Steven), and Roza, S.J. (Sabine)

Abstract

Lithium and antipsychotics are often prescribed to treat bipolar disorder or psychotic disorders in women of childbearing age. Little is known about the consequences of these medications during pregnancy for the developing child. The objective of this article is to systematically review findings from preclinical and clinical studies that have examined the neurodevelopmental consequences of intrauterine exposure to lithium and antipsychotics. A systematic search was performed in Embase, Medline, Web of Science, PsychINFO, Cochrane, and Google Scholar. Clinical and experimental studies were selected if they investigated neurodevelopment of offspring exposed to lithium or antipsychotics during gestation. Quality of clinical and preclinical studies was assessed by the Newcastle–Ottawa Scale and the SYRCLE’s risk of Bias tool, respectively. In total, 73 studies were selected for qualitative synthesis and three studies were selected for quantitative synthesis. Of preclinical studies, 93% found one or more adverse effects of prenatal exposure to antipsychotics or lithium on neurodevelopment or behaviour. Only three clinical cohort studies have investigated the consequences of lithium exposure, all of which reported normal development. In 66% of clinical studies regarding antipsychotic exposure, a transient delay in neurodevelopment was observed. The relative risk for neuromotor deficits after in utero exposure to antipsychotics was estimated to be 1.63 (95% CI 1.22–2.19; I2 = 0%). Preclinical studies suggest long-term adverse neurodevelopmental consequences of intrauterine exposure to either lithium or antipsychotics. However, there is a lack of high-quality clinical studies. Interpretation is difficult, since most studies have compared exposed children with their peers from the unaffected population, which did not allow correction for potential influences regarding genetic predisposition or parental psychiatric illness.

Published

2018

26. ACO2 homozygous missense mutation associated with complicated hereditary spastic paraplegia

Author

Bouwkamp, C.G. (Christian), Afawi, Z. (Zaid), Fattal-Valevski, A. (Aviva), Krabbendam, I.E. (Inge E.), Rivetti, S. (Stefano), Masalha, R. (Rafik), Quadri, M. (Marialuisa), Breedveld, G.J. (Guido), Mandel, H., Tailakh, M.A. (Muhammad Abu), Beverloo, H.B. (Berna), Stevanin, G. (Giovanni), Brice, A., IJcken, W.F.J. (Wilfred) van, Vernooij, M.W. (Meike), Dolga, A.M. (Amalia), Vrij, F.M.S. (Femke), Bonifati, V. (Vincenzo), Kushner, S.A. (Steven), Bouwkamp, C.G. (Christian), Afawi, Z. (Zaid), Fattal-Valevski, A. (Aviva), Krabbendam, I.E. (Inge E.), Rivetti, S. (Stefano), Masalha, R. (Rafik), Quadri, M. (Marialuisa), Breedveld, G.J. (Guido), Mandel, H., Tailakh, M.A. (Muhammad Abu), Beverloo, H.B. (Berna), Stevanin, G. (Giovanni), Brice, A., IJcken, W.F.J. (Wilfred) van, Vernooij, M.W. (Meike), Dolga, A.M. (Amalia), Vrij, F.M.S. (Femke), Bonifati, V. (Vincenzo), and Kushner, S.A. (Steven)

Abstract

Objective: To identify the clinical characteristics and genetic etiology of a family affected with hereditary

Published

2018

27. Candidate CSPG4 mutations and induced pluripotent stem cell modeling implicate oligodendrocyte progenitor cell dysfunction in familial schizophrenia

Author

Vrij, F.M.S. (Femke), Bouwkamp, C.G. (Christian), Gunhanlar, N. (Nilhan), Shpak, G. (Guy), Lendemeijer, B. (Bas), Baghdadi, M. (Maarouf), Gopalakrishna, S. (Shreekara), Ghazvini, M. (Mehrnaz), Li, T. (Tracy), Quadri, M. (Marialuisa), Olgiati, S. (Simone), Breedveld, G.J. (Guido), Coesmans, M.P.H. (Michiel), Mientjes, E.J. (Edwin), de Wit, T. (Ton), Verheijen, F.W. (Frans), Beverloo, H.B. (Berna), Cohen, D. (Dan), Kok, R.M. (Rob M.), Bakker, P.R. (Roberto), Nijburg, A. (Aviva), Spijker, A.T. (Anne), Haffmans, P.M.J. (P.M. Judith), Hoencamp, E. (Erik), Bergink, V. (Veerle), Vorstman, J.A.S., Wu, T. (Timothy), Olde Loohuis, L.M. (Loes M.), Amin, N. (Najaf), Langen, C.D. (Carolyn), Hofman, A. (Albert), Hoogendijk, W.J.G. (Witte), van Duijn, C.M. (Cornelia M.), Ikram, M.A. (M. A.), Vernooij, M.W. (Meike), Tiemeier, H.W. (Henning), Uitterlinden, A.G. (André G.), Elgersma, Y. (Ype), Distel, B. (Ben), Gribnau, J.H. (Joost), White, T.J.H. (Tonya), Bonifati, V. (Vincenzo), Kushner, S.A. (Steven A.), Vrij, F.M.S. (Femke), Bouwkamp, C.G. (Christian), Gunhanlar, N. (Nilhan), Shpak, G. (Guy), Lendemeijer, B. (Bas), Baghdadi, M. (Maarouf), Gopalakrishna, S. (Shreekara), Ghazvini, M. (Mehrnaz), Li, T. (Tracy), Quadri, M. (Marialuisa), Olgiati, S. (Simone), Breedveld, G.J. (Guido), Coesmans, M.P.H. (Michiel), Mientjes, E.J. (Edwin), de Wit, T. (Ton), Verheijen, F.W. (Frans), Beverloo, H.B. (Berna), Cohen, D. (Dan), Kok, R.M. (Rob M.), Bakker, P.R. (Roberto), Nijburg, A. (Aviva), Spijker, A.T. (Anne), Haffmans, P.M.J. (P.M. Judith), Hoencamp, E. (Erik), Bergink, V. (Veerle), Vorstman, J.A.S., Wu, T. (Timothy), Olde Loohuis, L.M. (Loes M.), Amin, N. (Najaf), Langen, C.D. (Carolyn), Hofman, A. (Albert), Hoogendijk, W.J.G. (Witte), van Duijn, C.M. (Cornelia M.), Ikram, M.A. (M. A.), Vernooij, M.W. (Meike), Tiemeier, H.W. (Henning), Uitterlinden, A.G. (André G.), Elgersma, Y. (Ype), Distel, B. (Ben), Gribnau, J.H. (Joost), White, T.J.H. (Tonya), Bonifati, V. (Vincenzo), and Kushner, S.A. (Steven A.)

Abstract

Schizophrenia is highly heritable, yet its underlying pathophysiology remains largely unknown. Among the most well-replicated findings in neurobiological studies of schizophrenia are deficits in myelination and white matter integrity; however, direct etiological genetic and cellular evidence has thus far been lacking. Here, we implement a family-based approach for genetic discovery in schizophrenia combined with functional analysis using induced pluripotent stem cells (iPSCs). We observed familial segregation of two rare missense mutations in Chondroitin Sulfate Proteoglycan 4 (CSPG4) (c.391G > A [p.A131T], MAF 7.79 × 10−5 and c.2702T > G [p.V901G], MAF 2.51 × 10−3). The CSPG4A131T mutation was absent from the Swedish Schizophrenia Exome Sequencing Study (2536 cases, 2543 controls), while the CSPG4V901G mutation was nominally enriched in cases (11 cases vs. 3 controls, P = 0.026, OR 3.77, 95% CI 1.05–13.52). CSPG4/NG2 is a hallmark protein of oligodendrocyte progenitor cells (OPCs). iPSC-derived OPCs from CSPG4A131T mutation carriers exhibited abnormal post-translational processing (P = 0.029), subcellular localization of mutant NG2 (P = 0.007), as well as aberrant cellular morphology (P = 3.0 × 10−8), viability (P = 8.9 × 10−7), and myelination potential (P = 0.038). Moreover, transfection of healthy non-carrier sibling OPCs confirmed a pathogenic effect on cell survival of both the CSPG4A131T (P = 0.006) and CSPG4V901G (P = 3.4 × 10−4) mutations. Finally, in vivo diffusion tensor imaging of CSPG4A131T mutation carriers demonstrated a reduction of brain white matter integrity compared to unaffected sibling and matched general population controls (P = 2.2 × 10−5). Together, our findings provide a convergence of genetic and functional evidence to implicate OPC dysfunction as a candidate pathophysiological mechanism of familial schizophrenia.

Published

2018

28. SOX10 Single Transcription Factor-Based Fast and Efficient Generation of Oligodendrocytes from Human Pluripotent Stem Cells

Author

García-León, J.A. (Juan Antonio), Kumar, M. (Manoj), Boon, R. (Ruben), Chau, D. (David), One, J. (Jennifer), Wolfs, E. (Esther), Eggermont, K. (Kristel), Berckmans, P. (Pieter), Gunhanlar, N. (Nilhan), Vrij, F.M.S. (Femke), Lendemeijer, B. (Bas), Pavie, B. (Benjamin), Corthout, N. (Nikky), Kushner, S.A. (Steven A.), Dávila, J.C. (José Carlos), Lambrichts, I. (Ivo), Hu, W.-S. (Wei-Shou), Verfaillie, C.M. (Catherine M.), García-León, J.A. (Juan Antonio), Kumar, M. (Manoj), Boon, R. (Ruben), Chau, D. (David), One, J. (Jennifer), Wolfs, E. (Esther), Eggermont, K. (Kristel), Berckmans, P. (Pieter), Gunhanlar, N. (Nilhan), Vrij, F.M.S. (Femke), Lendemeijer, B. (Bas), Pavie, B. (Benjamin), Corthout, N. (Nikky), Kushner, S.A. (Steven A.), Dávila, J.C. (José Carlos), Lambrichts, I. (Ivo), Hu, W.-S. (Wei-Shou), and Verfaillie, C.M. (Catherine M.)

Abstract

Scarce access to primary samples and lack of efficient protocols to generate oligodendrocytes (OLs) from human pluripotent stem cells (hPSCs) are hampering our understanding of OL biology and the development of novel therapies. Here, we demonstrate that overexpression of the transcription factor SOX10 is sufficient to generate surface antigen O4-positive (O4+) and myelin basic protein-positive OLs from hPSCs in only 22 days, including from patients with multiple sclerosis or amyotrophic lateral sclerosis. The SOX10-induced O4+ population resembles primary human OLs at the transcriptome level and can myelinate neurons in vivo. Using in vitro OL-neuron co-cultures, myelination of neurons by OLs can also be demonstrated, which can be adapted to a high-throughput screening format to test the response of pro-myelinating drugs. In conclusion, we provide an approach to generate OLs in a very rapid and efficient manner, which can be used for disease modeling, drug discovery efforts, and potentially for therapeutic OL transplantation. In this article, García-León JA and colleagues demonstrate the generation of functional oligodendrocytes (OLs) from human pluripotent stem cells in a rapid and efficient manner by the single overexpression of SOX10. Generated OLs resemble primary OLs at the transcriptome level and can myelinate neurons both in vivo and in vitro. Neuron-OL co-cultures, adapted to high-throughput screening formats, responded to drugs affecting myelination.

Published

2018

29. Activity-based protein profiling reveals off-target proteins of the FAAH inhibitor BIA 10-2474

Author

Van Esbroeck, A.C.M. (Annelot C. M.), Janssen, A.P.A. (Antonius P. A.), Cognetta, A.B. (Armand B.), Ogasawara, D. (Daisuke), Shpak, G. (Guy), Kroeg, M. (Mark) van der, Kantae, V. (Vasudev), Baggelaar, M.P. (Marc P.), Vrij, F.M.S. (Femke), Deng, H. (Hui), Allarà, M. (Marco), Fezza, F. (Filomena), Lin, Z. (Zhanmin), Van Der Wel, T. (Tom), Soethoudt, M. (Marjolein), Mock, E.D. (Elliot D.), Dulk, H. (Hans) den, Baak, I.L. (Ilse L.), Florea, B.I. (Bogdan), Hendriks, G. (Giel), De Petrocellis, L. (Luciano), Overkleeft, H.S. (Herman S.), Hankemeier, T. (Thomas), Zeeuw, C.I. (Chris) de, Di Marzo, V. (Vincenzo), Maccarrone, M. (Mauro), Cravatt, B.F. (Benjamin F.), Kushner, S.A. (Steven), Stelt, M. van der (Mario), Van Esbroeck, A.C.M. (Annelot C. M.), Janssen, A.P.A. (Antonius P. A.), Cognetta, A.B. (Armand B.), Ogasawara, D. (Daisuke), Shpak, G. (Guy), Kroeg, M. (Mark) van der, Kantae, V. (Vasudev), Baggelaar, M.P. (Marc P.), Vrij, F.M.S. (Femke), Deng, H. (Hui), Allarà, M. (Marco), Fezza, F. (Filomena), Lin, Z. (Zhanmin), Van Der Wel, T. (Tom), Soethoudt, M. (Marjolein), Mock, E.D. (Elliot D.), Dulk, H. (Hans) den, Baak, I.L. (Ilse L.), Florea, B.I. (Bogdan), Hendriks, G. (Giel), De Petrocellis, L. (Luciano), Overkleeft, H.S. (Herman S.), Hankemeier, T. (Thomas), Zeeuw, C.I. (Chris) de, Di Marzo, V. (Vincenzo), Maccarrone, M. (Mauro), Cravatt, B.F. (Benjamin F.), Kushner, S.A. (Steven), and Stelt, M. van der (Mario)

Abstract

A recent phase 1 trial of the fatty acid amide hydrolase (FAAH) inhibitor BIA 10-2474 led to the death of one volunteer and produced mild-to-severe neurological symptoms in four others. Although the cause of the clinical neurotoxicity is unknown, it has been postulated, given the clinical safety profile of other tested FAAH inhibitors, that off-target activities of BIA 10-2474 may have played a role. Here we use activity-based proteomicmethods to determine the protein interaction landscape of BIA 10-2474 in human cells and tissues. This analysis revealed that the drug inhibits several lipases that are not targeted by PF04457845, a highly selective and clinically tested FAAH inhibitor. BIA 10-2474, but not PF04457845, produced substantial alterations in lipid networks in human cortical neurons, suggesting that promiscuous lipase inhibitors have the potential to cause metabolic dysregulation in the nervous system.

Published

2017

30. Phenotypic differences between Asian and African lineage Zika viruses in human neural progenitor cells

Author

Anfasa, F. (Fatih), Siegers, J.Y. (Jurre), Kroeg, M. (Mark) van der, Mumtaz, N. (Noreen), Stalin Raj, V., Vrij, F.M.S. (Femke), Widagdo, W. (Widagdo), Gabriel, G. (Gülsah), Salinas, S. (Sara), Simonin, Y. (Yannick), Reusken, C.B.E.M. (Chantal), Kushner, S.A. (Steven), Koopmans D.V.M., M.P.G. (Marion), Haagmans, B.L. (Bart), Martina, B.E.E. (Byron), Riel, D.A.J. (Debby) van, Anfasa, F. (Fatih), Siegers, J.Y. (Jurre), Kroeg, M. (Mark) van der, Mumtaz, N. (Noreen), Stalin Raj, V., Vrij, F.M.S. (Femke), Widagdo, W. (Widagdo), Gabriel, G. (Gülsah), Salinas, S. (Sara), Simonin, Y. (Yannick), Reusken, C.B.E.M. (Chantal), Kushner, S.A. (Steven), Koopmans D.V.M., M.P.G. (Marion), Haagmans, B.L. (Bart), Martina, B.E.E. (Byron), and Riel, D.A.J. (Debby) van

Abstract

Recent Zika virus (ZIKV) infections have been associated with a range of neurological complications, in particular congenital microcephaly. Human neural progenitor cells (hNPCs) are thought to play an important role in the pathogenesis of microcephaly, and experimental ZIKV infection of hNPCs has been shown to induce cell death. However, the infection efficiency and rate of cell death have varied between studies, which might be related to intrinsic differences between African and Asian lineage ZIKV strains. Therefore, we determined the replication kinetics, including infection efficiency, burst size, and ability to induce cell death, of two Asian and two African ZIKV strains. African ZIKV strains replicated to higher titers in Vero cells, human glioblastoma (U87MG) cells, human neuroblastoma (SK-N-SH) cells, and hNPCs than Asian ZIKV strains. Furthermore, infection with Asian ZIKV strains did not result in significant cell death early after infection, whereas infection with African ZIKV strains resulted in high percentages of cell death in hNPCs. The differences between African and Asian lineage ZIKV strains highlight the importance of including relevant ZIKV strains to study the pathogenesis of congenital microcephaly and caution against extrapolation of experimental data obtained using historical African ZIKV strains to the current outbreak. Finally, the fact that Asian ZIKV strains infect only a minority of cells with a relatively low burst size together with the lack of early cell death induction might contribute to its ability to cause chronic infections within the central nervous system (CNS).

Published

2017

31. Lithium dosing strategies during pregnancy and the postpartum period

Author

Wesseloo, R. (Richard), Wierdsma, A.I. (André), Kamp, I.L. (Inge) van, Munk-Olsen, T. (Trine), Hoogendijk, W.J.G. (Witte), Kushner, S.A. (Steven), Bergink, V. (Veerle), Wesseloo, R. (Richard), Wierdsma, A.I. (André), Kamp, I.L. (Inge) van, Munk-Olsen, T. (Trine), Hoogendijk, W.J.G. (Witte), Kushner, S.A. (Steven), and Bergink, V. (Veerle)

Abstract

Background Lithium is challenging to dose during pregnancy. Aims To provide guidance for dosing lithium during pregnancy. Method Retrospective observational cohort study. Data on lithium blood level measurements (n = noi), the daily lithium dose, dosing alterations/frequency and creatinine blood levels were obtained from 113 pregnancies of women receiving lithium treatment during pregnancy and the postpartum period. Results Lithium blood levels decreased in the first trimester (-24%, 95% Cl-15 to-35), reached a nadir in the second trimester (-36%, 95% CI-27 to-47), increased in the third trimester (-21%, 95% CI-13 to-30) and were still slightly increased postpartum (+9%, 95% Cl +2 to +15). Delivery itself was not associated with an acute change in lithium and creatinine blood levels. Conclusions We recommend close monitoring of lithium blood levels until 34 weeks of pregnancy, then weekly until delivery and twice weekly for the first

Published

2017

32. The SAC1 domain in synaptojanin is required for autophagosome maturation at presynaptic terminals

Author

Vanhauwaert, R. (Roeland), Kuenen, S. (Sabine), Masius, R.G. (Roy), Bademosi, A. (Adekunle), Manetsberger, J. (Julia), Schoovaerts, N. (Nils), Bounti, L. (Laura), Gontcharenko, S. (Serguei), Swerts, J. (Jef), Vilain, S. (Sven), Picillo, M. (Marina), Barone, P. (Paolo), Munshi, S.T. (Shashini), Vrij, F.M.S. (Femke), Kushner, S.A. (Steven), Gounko, N.V. (Natalia V), Mandemakers, W.J. (Wim), Bonifati, V. (Vincenzo), Meunier, F.A. (Frederic A), Soukup, S.-F. (Sandra-Fausia), Verstreken, P. (Patrik), Vanhauwaert, R. (Roeland), Kuenen, S. (Sabine), Masius, R.G. (Roy), Bademosi, A. (Adekunle), Manetsberger, J. (Julia), Schoovaerts, N. (Nils), Bounti, L. (Laura), Gontcharenko, S. (Serguei), Swerts, J. (Jef), Vilain, S. (Sven), Picillo, M. (Marina), Barone, P. (Paolo), Munshi, S.T. (Shashini), Vrij, F.M.S. (Femke), Kushner, S.A. (Steven), Gounko, N.V. (Natalia V), Mandemakers, W.J. (Wim), Bonifati, V. (Vincenzo), Meunier, F.A. (Frederic A), Soukup, S.-F. (Sandra-Fausia), and Verstreken, P. (Patrik)

Abstract

Presynaptic terminals are metabolically active and accrue damage through continuous vesicle cycling. How synapses locally regulate protein homeostasis is poorly understood. We show that the presynaptic lipid phosphatase synaptojanin is required for macroautophagy, and this role is inhibited by the Parkinson's disease mutation R258Q. Synaptojanin drives synaptic endocytosis by dephosphorylating PI(4,5)P2, but this function appears normal in SynaptojaninRQ knock-in flies. Instead, R258Q affects the synaptojanin SAC1 domain that dephosphorylates PI(3)P and PI(3,5)P2, two lipids found in autophagosomal membranes. Using advanced imaging, we show that SynaptojaninRQ mutants accumulate the PI(3)P/PI(3,5)P2-binding protein Atg18a on nascent synaptic autophagosomes, blocking autophagosome maturation at fly synapses and in neurites of human patient induced pluripotent stem cell-derived neurons. Additionally, we observe neurodegeneration, including dopaminergic neuron loss, in SynaptojaninRQ flies. Thus, synaptojanin is essential for macroautophagy within presynaptic terminals, coupling protein turnover with synaptic vesicle cycling and linking presynaptic-specific autophagy defects to Parkinson's disease.

Published

2017

33. Mechanisms underlying cognitive deficits in a mouse model for Costello Syndrome are distinct from other RASopathy mouse models

Author

Schreiber, J. (Jadwiga), Grimbergen, L.-A. (Laura-Anne), Overwater, I.E. (Iris), Vaart, M.H.T. (Thijs) van der, Stedehouder, J. (Jeffrey), Schuhmacher, A.J. (Alberto J.), Guerra, C. (Carmen), Kushner, S.A. (Steven), Jaarsma, D. (Dick), Elgersma, Y. (Ype), Schreiber, J. (Jadwiga), Grimbergen, L.-A. (Laura-Anne), Overwater, I.E. (Iris), Vaart, M.H.T. (Thijs) van der, Stedehouder, J. (Jeffrey), Schuhmacher, A.J. (Alberto J.), Guerra, C. (Carmen), Kushner, S.A. (Steven), Jaarsma, D. (Dick), and Elgersma, Y. (Ype)

Abstract

RASopathies, characterized by germline mutations in genes encoding proteins of the RAS-ERK signaling pathway, show overlapping phenotypes, which manifest themselves with a varying severity of intellectual disability. However, it is unclear to what extent they share the same downstream pathophysiology that underlies the cognitive deficits. Costello syndrome (CS) is a rare RASopathy caused by activating mutations in the HRAS gene. Here we investigated the mechanisms underlying the cognitive deficits of HRas G12V/G12V mice. HRas G12V/G12V mice showed robust upregulation of ERK signaling, neuronal hypertrophy, increased brain volume, spatial learning deficits, and impaired mGluR-dependent long-term depression (LTD). In contrast, long-term potentiation (LTP), which is affected in other RASopathy mouse models was unaffected. Treatment with lovastatin, a HMG-CoA-Reductase inhibitor which has been shown to rescue the behavioral phenotypes of mouse models of NF1 and Noonan syndrome, was unable to restore ERK signaling and the cognitive deficits of HRas G12V/G12V mice. Administration of a potent mitogen-activated protein kinase (MEK) inhibitor rescued the ERK upregulation and the mGluR-LTD deficit of HRas G12V/G12V mice, but failed to rescue the cognitive deficits. Taken together, this study indicates that the fundamental molecular and cellular mechanisms underlying the cognitive aspects of different RASopathies are remarkably distinct, and may require disease specific treatments.

Published

2017

34. Myelination of parvalbumin interneurons: a parsimonious locus of pathophysiological convergence in schizophrenia

Author

Stedehouder, J. (Jeffrey), Kushner, S.A. (Steven), Stedehouder, J. (Jeffrey), and Kushner, S.A. (Steven)

Abstract

Schizophrenia is a debilitating psychiatric disorder characterized by positive, negative and cognitive symptoms. Despite more than a century of research, the neurobiological mechanism underlying schizophrenia remains elusive. White matter abnormalities and interneuron dysfunction are the most widely replicated cellular neuropathological alterations in patients with schizophrenia. However, a unifying model incorporating these findings has not yet been established. Here, we propose that myelination of fast-spiking parvalbumin (PV) interneurons could be an important locus of pathophysiological convergence in schizophrenia. Myelination of interneurons has been demonstrated across a wide diversity of brain regions and appears highly specific for the PV interneuron subclass. Given the critical influence of fast-spiking PV interneurons for mediating oscillations in the gamma frequency range (~30–120 Hz), PV myelination is well positioned to optimize action potential fidelity and metabolic homeostasis. We discuss this hypothesis with consideration of data from human postmortem studies, in vivo brain imaging and electrophysiology, and molecular genetics, as well as fundamental and translational studies in rodent models. Together, the parvalbumin interneuron myelination hypothesis provides a falsifiable model for guiding future studies of schizophrenia pathophysiology.Molecular Psychiatry advance online publication, 20 September 2016; doi:10.1038/mp.2016.147.

Published

2017

35. Reduced trigeminovascular cyclicity in patients with menstrually related migraine

Author

Ibrahimi, K., Oosterhout, W.P.J. van, Dorp, W. van, Danser, A.H.J., Garrelds, I.M., Kushner, S.A., Lesaffre, E.M.E.H., Terwindt, G.M., Ferrari, M.D., Meiracker, A.H. van den, and MaassenVanDenBrink, A.

Published

2015

36. A balanced translocation disrupting BCL2L10 and PNLDC1 segregates with affective psychosis

Author

Bouwkamp, C.G. (Christian G.), Kievit, A.J.A. (Anneke J.A.), Olgiati, S. (Simone), Breedveld, G.J. (Guido), Coesmans, M.P.H. (Michiel), Bonifati, V. (Vincenzo), Kushner, S.A. (Steven), Bouwkamp, C.G. (Christian G.), Kievit, A.J.A. (Anneke J.A.), Olgiati, S. (Simone), Breedveld, G.J. (Guido), Coesmans, M.P.H. (Michiel), Bonifati, V. (Vincenzo), and Kushner, S.A. (Steven)

Abstract

Affective psychoses are a group of severe psychiatric disorders, including schizoaffective disorder and bipolar I disorder, together affecting ∼1% of the population. Despite their high heritability, the molecular genetics and neurobiology of affective psychosis remain largely elusive. Here, we describe the identification of a structural genetic variant segregating with affective psychosis in a family with multiple members suffering from bipolar I disorder or schizoaffective disorder, bipolar type. A balanced translocation involving chromosomes 6 and 15 was detected by karyotyping and fluorescence in-situ hybridization (FISH). Using whole-genome sequencing, we rapidly delineated the translocation breakpoints as corresponding intragenic events disrupting BCL2L10 and PNLDC1. These data warrant further consideration for BCL2L10 and PNLDC1 as novel candidates for affective psychosis.

Published

2016

37. Arc expression identifies the lateral amygdala fear memory trace

Author

Gouty-Colomer, L.A., Hosseini, B., Marcelo, I.M., Schreiber, J. (Jadwiga), Slump, D.E. (Denise E.), Yamaguchi, S., Houweling, A.R. (Arthur), Jaarsma, D., Elgersma, Y. (Ype), Kushner, S.A. (Steven), Gouty-Colomer, L.A., Hosseini, B., Marcelo, I.M., Schreiber, J. (Jadwiga), Slump, D.E. (Denise E.), Yamaguchi, S., Houweling, A.R. (Arthur), Jaarsma, D., Elgersma, Y. (Ype), and Kushner, S.A. (Steven)

Abstract

Memories are encoded within sparsely distributed neuronal ensembles. However, the defining cellular properties of neurons within a memory trace remain incompletely understood. Using a fluorescence-based Arc reporter, we were able to visually identify the distinct subset of lateral amygdala (LA) neurons activated during auditory fear conditioning. We found that Arc-expressing neurons have enhanced intrinsic excitability and are preferentially recruited into newly encoded memory traces. Furthermore, synaptic potentiation of thalamic inputs to the LA during fear conditioning is learning-specific, postsynaptically mediated and highly localized to Arc-expressing neurons. Taken together, our findings validate the immediate-early gene Arc as a molecular marker for the LA neuronal ensemble recruited during fear learning. Moreover, these results establish a model of fear memory formation in which intrinsic excitability determines neuronal selection, whereas learning-related encoding is governed by synaptic plasticity.

Published

2016

38. Sex-Specific Mechanism of Social Hierarchy in Mice

Author

van den Berg, W.E., Lamballais, S. (Sander), Kushner, S.A. (Steven), van den Berg, W.E., Lamballais, S. (Sander), and Kushner, S.A. (Steven)

Abstract

The establishment of social hierarchies is a naturally occurring, evolutionarily conserved phenomenon with a well-established impact on fitness and health. Investigations of complex social group dynamics may offer novel opportunities for translational studies of autism spectrum disorder. Here we describe a robust behavioral paradigm using an automated version of the tube test. Isogenic groups of male and female mice establish linear social hierarchies that remain highly stable for at least 14 days, the longest interval tested. Remarkably, however, their social strategy is sex-specific: females primarily utilize intrinsic attributes, whereas males are strongly influenced by prior social experience. Using both genetic and pharmacological manipulations, we identify testosterone as a critical sex-specific factor for determining which social strategy is used. Males inheriting a null mutation of the sex-determining region Y (Sry) gene used a similar social cognitive strategy as females. In contrast, females with transgenic expression of Sry utilized a typically male social strategy. Analogously, castration of males and testosterone supplementation of females yielded similar outcomes, with a reversal of their social cogn

Published

2015

39. Pre-eclampsia and first-onset postpartum psychiatric episodes: A Danish population-based cohort study

Author

Bergink, V. (Veerle), Laursen, T.M., Johannsen, B.M.W., Kushner, S.A. (Steven), Meltzer-Brody, S. (Samantha), Munk-Olsen, T. (Trine), Bergink, V. (Veerle), Laursen, T.M., Johannsen, B.M.W., Kushner, S.A. (Steven), Meltzer-Brody, S. (Samantha), and Munk-Olsen, T. (Trine)

Abstract

Recent evidence suggests that postpartum psychiatric episodes may share similar etiological mechanisms with immune-related disorders. Pre-eclampsia is one of the most prevalent immune-related disorders of pregnancy. Multiple clinical features are shared between pre-eclampsia and postpartum psychiatric disorders, most prominently a strong link to first pregnancies. Therefore, we aimed to study if pre-eclampsia is a risk factor for first-onset postpartum psychiatric episodes. Method. We conducted a cohort study using the Danish population registry, with a total of 400 717 primiparous women with a singleton delivery between 1995 and 2011. First-lifetime childbirth was the main exposure variable and the outcome of interest was first-onset postpartum psychiatric episodes. The main outcome measures were monthly incidence rate ratios (IRRs), with the period 11-12 months after birth as the reference category. Adjustments were made for age, calendar period, reproductive history, and perinatal maternal health including somatic and obstetric co-morbidity. Results. Primiparous women were at particularly high risk of first-onset psychiatric episodes during the first month postpartum [IRR 2.93, 95% confidence interval (CI) 2.53-3.40] and pre-eclampsia added to that risk (IRR 4.21, 95% CI 2.89-6.13). Having both pre-eclampsia and a somatic co-morbidity resulted in the highest risk of psychiatric episodes during the 3-month period after childbirth (IRR 4.81, 95% CI 2.72-8.50). Conclusions. We confirmed an association between pre-eclampsia and pos

Published

2015

40. P.1.e.010 Tryptophan pathway alterations in the postpartum period and in acute postpartum psychosis and depression

Author

Veen, C., primary, Myint, A.M., additional, Burgerhout, K.M., additional, Schwarz, M.J., additional, Schütze, G., additional, Kushner, S.A., additional, Hoogendijk, W.J., additional, Drexhage, H., additional, and Bergink, V., additional

Published

2015

41. 8D.06

Author

Danser, A. H. J., primary, Slump, D.E., additional, Grefhorst, A., additional, van Veghel, R., additional, Garrelds, I.M., additional, Roks, A.J.M., additional, Kushner, S.A., additional, and van Esch, J.H.M., additional

Published

2015

42. Fragile X mice have robust mGluR5-dependent alterations of social behaviour in the Automated Tube Test

Author

de Esch, C.E.F., primary, van den Berg, W.E., additional, Buijsen, R.A.M., additional, Jaafar, I.A., additional, Nieuwenhuizen-Bakker, I.M., additional, Gasparini, F., additional, Kushner, S.A., additional, and Willemsen, R., additional

Published

2015

43. Neurons Are Recruited to a Memory Trace Based on Relative Neuronal Excitability Immediately before Training

Author

Yiu, A.P. (Adelaide), Mercaldo, V. (Valentina), Yan, C. (Chen), Richards, B. (Blake), Rashid, M.U. (Muhammad), Hsiang, H.L. (Hwa), Pressey, J. (Jessica), Mahadevan, V. (Vivek), Tran, M.M. (Matthew), Kushner, S.A. (Steven), Woodin, M.A. (Melanie), Frankland, P.W. (Paul), Josselyn, S.A. (Sheena), Yiu, A.P. (Adelaide), Mercaldo, V. (Valentina), Yan, C. (Chen), Richards, B. (Blake), Rashid, M.U. (Muhammad), Hsiang, H.L. (Hwa), Pressey, J. (Jessica), Mahadevan, V. (Vivek), Tran, M.M. (Matthew), Kushner, S.A. (Steven), Woodin, M.A. (Melanie), Frankland, P.W. (Paul), and Josselyn, S.A. (Sheena)

Abstract

Memories are thought to be sparsely encoded in neuronal networks, but little is known about why a given neuron is recruited or allocated to a particular memory trace. Previous research shows that in the lateral amygdala (LA), neurons with increased CREB are selectively recruited to a fear memory trace. CREB is a ubiquitous transcription factor implicated in many cellular processes. Which process mediates neuronal memory allocation? One hypothesis is that CREB increases neuronal excitability to bias neuronal recruitment, although this has not been shown experimentally. Here we use several methods to increase neuronal excitability and show this both biases recruitment into the memory trace and enhances memory formation. Moreover, artificial activation of these neurons alone is a sufficient retrieval cue for fear memory expression, showing that these neurons are critical components of the memory trace. These results indicate that neuronal memory allocation is based on relative neuronal excitability immediately before training.

Published

2014

44. Neuroanatomical phenotypes in a mouse model of the 22q11.2 microdeletion

Author

Ellegood, J., Markx, S., Lerch, J.P. (Jason), Steadman, P.E., Genç, C.G. (Cansu), Provenzano, F., Kushner, S.A. (Steven), Henkelman, R.M., Karayiorgou, M., Gogos, J.A., Ellegood, J., Markx, S., Lerch, J.P. (Jason), Steadman, P.E., Genç, C.G. (Cansu), Provenzano, F., Kushner, S.A. (Steven), Henkelman, R.M., Karayiorgou, M., and Gogos, J.A.

Abstract

Recurrent deletions at the 22q11.2 locus have been established as a strong genetic risk factor for the development of schizophrenia and cognitive dysfunction. Individuals with 22q11.2 deletions have a range of well-defined volumetric abnormalities in a number of critical brain structures. A mouse model of the 22q11.2 deletion (Df(16)A+/-) has previously been utilized to characterize disease-associated abnormalities on synaptic, cellular, neurocircuitry, and behavioral levels. We performed a high-resolution MRI analysis of mutant mice compared with wild-type littermates. Our analysis revealed a striking similarity in the specific volumetric changes of Df(16)A+/-mice compared with human 22q11.2 deletion carriers, including in cortico-cerebellar, cortico-striatal and cortico-limbic circuits. In addition, higher resolution magnetic resonance imaging compared with neuroimaging in human subjects allowed the detection of previously unknown subtle local differences. The cerebellar findings in Df(16)A+/-mice are particularly instructive as they are localized to specific areas within both the deep cerebellar nuclei and the cerebellar cortex. Our study indicates that the Df(16)A+/-mouse model recapitulates most of the hallmark neuroanatomical changes observed in 22q11.2 deletion carriers. Our findings will help guide the design and interpretation of additional complementary studies and thereby advance our understanding of the abnormal brain development underlying the emergence of 22q11.2 deletion-associated psychiatric and cognitive symptoms.Molecular Psychiatry advance online publication, 3 September 2013; doi:10.1038/mp.2013.112.

Published

2014

45. Epigenetic characterization of the FMR1 promoter in induced pluripotent stem cells from human fibroblasts carrying an unmethylated full mutation

Author

Esch, C. (Celine) de, Ghazvini, M. (Mehrnaz), Loos, F. (Friedemann), Schelling-Kazaryan, N. (Nune), Widagdo, W. (Widagdo), Munshi, S.T. (Shashini), Wal, E. (Erik) van der, Douben, H. (Hannie), Gunhanlar, N. (Nilhan), Kushner, S.A. (Steven), Pijnappel, W.W.M.P. (Pim), Vrij, F.M.S. (Femke), Geijsen, N. (Niels), Gribnau, J.H. (Joost), Willemsen, R. (Rob), Esch, C. (Celine) de, Ghazvini, M. (Mehrnaz), Loos, F. (Friedemann), Schelling-Kazaryan, N. (Nune), Widagdo, W. (Widagdo), Munshi, S.T. (Shashini), Wal, E. (Erik) van der, Douben, H. (Hannie), Gunhanlar, N. (Nilhan), Kushner, S.A. (Steven), Pijnappel, W.W.M.P. (Pim), Vrij, F.M.S. (Femke), Geijsen, N. (Niels), Gribnau, J.H. (Joost), and Willemsen, R. (Rob)

Abstract

Silencing of the FMR1 gene leads to fragile X syndrome, the most common cause of inherited intellectual disability. To study the epigenetic modifications of the FMR1 gene during silencing in time, we used fibroblasts and induced pluripotent stem cells (iPSCs) of an unmethylated full mutation (uFM) individual with normal intelligence. The uFM fibroblast line carried an unmethylated FMR1 promoter region and expressed normal to slightly increased FMR1 mRNA levels. The FMR1 expression in the uFM line corresponds with the increased H3 acetylation and H3K4 methylation in combination with a reduced H3K9 methylation. After reprogramming, the FMR1 promoter region was methylated in all uFM iPSC clones. Two clones were analyzed further and showed a lack of FMR1 expression, whereas the presence of specific histone modifications also indicated a repressed FMR1 promoter. In conclusion, these findings demonstrate that the standard reprogramming procedure leads to epigenetic silencing of the fully mutated FMR1 gene.

Published

2014

46. Effect of simvastatin on cognitive functioning in children with neurofibromatosis Type 1

Author

Krab, L.C., De Goede-Bolder, A., Aarsen, F.K., Pluijm, S.M.F., Bouman, M.J., van der Geest, J.N., Lequin, M., Catsman, C.E., Arts, W.F.M., Kushner, S.A., Silva, A.J., de Zeeuw, C.I., Moll, H.A., Elgersma, Y., and Netherlands Institute for Neuroscience (NIN)

Published

2008

47. Synaptic transmission and plasticity at inputs to murine cerebellar purkinje cells are largely dispensable for standard nonmotor tasks

Author

Galliano, E. (Elisa), Potters, J.W. (Jan Willem), Elgersma, Y. (Ype), Wisden, W. (William), Kushner, S.A. (Steven), Zeeuw, C.I. (Chris) de, Hoebeek, F.E. (Freek), Galliano, E. (Elisa), Potters, J.W. (Jan Willem), Elgersma, Y. (Ype), Wisden, W. (William), Kushner, S.A. (Steven), Zeeuw, C.I. (Chris) de, and Hoebeek, F.E. (Freek)

Abstract

In addition to its well established role in motor coordination, the cerebellum has been hypothesized to be involved in the control of cognitive and emotional functions. Although a cerebellar contribution to nonmotor functions has been supported by recent studies in human and monkey, it remains to be clarified with an in-depth, systematic approach in mouse mutants. Here we subjected four different cerebellar cell-specific mouse lines whereby the excitatory or inhibitory input to Purkinje cells (PCs) and/or PC postsynaptic plasticity were compromised, to a wide battery of standard cognitive and emotional tests. The four lines, which have all been shown to suffer from impaired motor learning without being ataxic, were tested for social behavior using a sociability task, for spatial navigation using the Morris watermaze, for fear responses using contextual and cued conditioning, and general anxiety using the open-field task. None of the four cerebellum-specific genetic perturbations showed significantly impaired cognitive or emotional behavior. In fact, even without correction for multiple comparisons, only 5 of 154 statistical comparisons showed a marginally significant deficit. Therefore, our data indicate that none of the perturbations of cerebellar functioning studied here affected the cognitive or emotional tests we used. This suggests that there may be a differentia

Published

2013

48. Synaptic transmission and plasticity at inputs to murine cerebellar purkinje cells are largely dispensable for standard nonmotor tasks.

Author

Galliano, E., Potters, J.W., Elgersma, Y., Wisden, W., Kushner, S.A., De Zeeuw, C.I., Hoebeek, F.E., Galliano, E., Potters, J.W., Elgersma, Y., Wisden, W., Kushner, S.A., De Zeeuw, C.I., and Hoebeek, F.E.

Published

2013

49. Prevention of postpartum psychosis and mania in women at high risk

Author

Bergink, V. (Veerle), Bouvy, P.F. (Paul), Vervoort, J. (Jeroen), Koorengevel, K.M. (Kathelijne), Steegers, E.A.P. (Eric), Kushner, S.A. (Steven), Bergink, V. (Veerle), Bouvy, P.F. (Paul), Vervoort, J. (Jeroen), Koorengevel, K.M. (Kathelijne), Steegers, E.A.P. (Eric), and Kushner, S.A. (Steven)

Abstract

Objective: Women with a history of bipolar disorder or postpartum psychosis are at extremely high risk of relapse postpartum. Although lithium prophylaxis has demonstrated efficacy in reducing postpartum relapse, the timing of prophylaxis remains controversial given the balance of risks and benefits for the mother and fetus. The authors compared lithium use during pregnancy to its initiation postpartum in women at high risk for postpartum psychosis. Method: Between 2003 and 2010, 70 pregnant women at high risk for postpartum psychosis were referred to the authors' psychiatric outpatient clinic. Women who were initially medication free were advised to start lithium prophylaxis immediately postpartum. Women already taking maintenance lithium during pregnancy were advised to continue treatment. Results: All women with a history of psychosis limited to the postpartum period

Published

2012

50. Fetal alcohol exposure leads to abnormal olfactory bulb development and impaired odor discrimination in adult mice

Author

Akers, K.G. (Katherine), Kushner, S.A. (Steven), Leslie, A.T. (Ana), Clarke, L. (Laura), Kooy, D. (Derek) van der, Lerch, J.P. (Jason), Frankland, P.W. (Paul), Akers, K.G. (Katherine), Kushner, S.A. (Steven), Leslie, A.T. (Ana), Clarke, L. (Laura), Kooy, D. (Derek) van der, Lerch, J.P. (Jason), and Frankland, P.W. (Paul)

Abstract

Background: Children whose mothers consumed alcohol during pregnancy exhibit widespread brain abnormalities and a complex array of behavioral disturbances. Here, we used a mouse model of fetal alcohol exposure to investigate relationships between brain abnormalities and specific behavioral alterations during adulthood. Results: Mice drank a 10% ethanol sol

Published

2011