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2. A recurrent SHANK3 frameshift variant in Autism Spectrum Disorder

Author

Loureiro, Livia O., Howe, Jennifer L., Reuter, Miriam S., Iaboni, Alana, Calli, Kristina, Roshandel, Delnaz, Pritišanac, Iva, Moses, Alan, Forman-Kay, Julie D., Trost, Brett, Zarrei, Mehdi, Rennie, Olivia, Lau, Lynette Y. S., Marshall, Christian R., Srivastava, Siddharth, Godlewski, Brianna, Buttermore, Elizabeth D., Sahin, Mustafa, Hartley, Dean, Frazier, Thomas, Vorstman, Jacob, Georgiades, Stelios, Lewis, Suzanne M. E., Szatmari, Peter, Bradley, Clarrisa A. (Lisa), Tabet, Anne-Claude, Willems, Marjolaine, Lumbroso, Serge, Piton, Amélie, Lespinasse, James, Delorme, Richard, Bourgeron, Thomas, Anagnostou, Evdokia, and Scherer, Stephen W.

Published
2021
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3. Genetic and metabolic investigations for neurodevelopmental disorders: position statement of the Canadian College of Medical Geneticists (CCMG)

Author

Carter, Melissa T, primary, Srour, Myriam, additional, Au, Ping-Yee Billie, additional, Buhas, Daniela, additional, Dyack, Sarah, additional, Eaton, Alison, additional, Inbar-Feigenberg, Michal, additional, Howley, Heather, additional, Kawamura, Anne, additional, Lewis, Suzanne M E, additional, McCready, Elizabeth, additional, Nelson, Tanya N, additional, and Vallance, Hilary, additional

Published
2023
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4. Trends in Special Education Code Assignment for Autism: Implications for Prevalence Estimates

Author

Ouellette-Kuntz, Helene, Coo, Helen, Lloyd, Jennifer E. V., Kasmara, Liza, Holden, Jeanette J. A., and Lewis, Suzanne M. E.

Abstract

There is considerable controversy over reasons for observed increases in the prevalence of autism spectrum disorders. We examined trends in British Columbia education database coding of children with autism from 1996 to 2004. There was a significant linear increase in autism prevalence. The proportion of children identified by age 6 increased significantly from 1996 to 1999. When we calculated prevalence assuming onset prior to age 3, previously unidentified cases, particularly among girls in 1996 and 1997, accounted for substantial increases in estimated prevalence. The magnitude of under-identification decreased from 1996 to 2000, and rose slightly in 2001. Analyses of prevalence trends must take into account effects of earlier age at identification and inclusion of previously undetected cases on prevalence estimates.

Published
2007
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6. Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes

Author

Qiao, Ying, Mondal, Kajari, Trapani, Valentina, Wen, Jiadi, Carpenter, Gillian, Wildin, Robert, Price, Magda E., Gibbons, Richard J., Eichmeyer, Jennifer, Jiang, Ruby, DuPont, Barbara, Martell, Sally, Lewis, Suzanne M. E., Robinson, Wendy P., OʼDriscoll, Mark, Wolf, Federica I., Zwick, Michael E., and Rajcan-Separovic, Evica

Published
2014
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10. Sex differences in conditioned orienting and the role of estradiol in addiction-related behaviors.

Author

Hilz, Emily N., Lewis, Suzanne M., Olshavsky, Megan E., Khoury, Elizabeth S., Gore, Andrea C., Monfils, Marie H., and Lee, Hongjoo J.

Abstract

Conditioned orienting response (OR) is a form of cue-directed behavior thought to indicate increased attentional and/or motivational processing of reward-associated stimuli. OR as a phenotype has been shown to predict both direct drug proclivity in female rats and behaviors indirectly related to drug proclivity in male rats, but no extant research has compared males and females in terms of their OR behavior or its notable substrates. As females are at increased risk for substance abuse, and the ovarian hormone estradiol is often cited as a driving factor for this predilection, it is important to characterize sex differences between males and females and explore what, if any, contribution estradiol has in behaviors which predict substance abuse. In these experiments, male and female rats [intact or ovariectomized (OVX) with/without estradiol replacement] were compared on a battery of behavioral tasks, including OR, novelty-seeking, attentional set-shifting, and ultrasonic vocalizations (USVs) to amphetamine treatment. Female rats, regardless of estradiol replacement, had higher OR scores than males. OR score was a predictor of attention impairments, and estradiol availability contributed to this relationship in females. Sex differences were not observed in novelty-seeking, attentional set-shifting, or USV response to amphetamine; however, estradiol replacement did alter the presentation of these behaviors. [ABSTRACT FROM AUTHOR]

Published
2022
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14. Open Content Licensing: Cultivating the Creative Commons

Author

Fitzgerald, Brian F., Coates, Jessica M., and Lewis, Suzanne M.

Subjects
Machinima, Morpheus, Lawrence Lessig, US Free Trade Agreement Implementation Act 2004, Creative Commons, Blogs, User Generated Content, open source, Technological Protection Measure, AEShareNet, Second Life, Warner Entertainment Co Ltd v Channel 4 Television Corp PLC, BitTorrent, The Future of Ideas, EULA, Digital Sampling, Wired CD, Code and Other Laws of Cyberspace, Creative Industries, open access licensing, US v Thomas, Conger, 160510 Public Policy, Kahle v Ashcroft, Remixing, Universal Music Australia Pty Ltd v Cooper, Virtual Worlds, Fair Dealing/Fair Use, Open Content licensing, Lucasfilm Ltd v High Frontier, Intellectual Property Law, Network Ten Pty Ltd v TCN Channel Nine Pty Ltd, SFAA v USOC, Eldred v Ashcroft, CLRC, Sonny Bono Copyright Term Extension Act 1998, Read My Lips, Crown Copyright, Australasian Performing Right Association, Digital Agenda, Bridgeport Music Inc v Dimension Films Inc, MP3, 190000 STUDIES IN CREATIVE ARTS AND WRITING, Massive Multi, copyright, Australia, San Francisco Arts and Athletic Inc v US Olympics Committee, Autodesk Inc v Dyason, Digital Rights Management, Michelin Case, intellectual property, Copyright Law Review Committee, Digital Agenda Act, Universal Music Australia Pty Ltd v Miyamoto, My Life, The Internet Archive, MMOG, Social Capital, 220204 History and Philosophy of Law and Justice, Trainz, US Free Trade Agreement, Open Digital Rights Language, Davidson & Associates v Jung, Internet and Innovation, Miller v Taylor, Trade Marks, ccPublisher, APRA, Australasian Mechanical Copyright Owners’ Society, Marvel v NCSoft, Uncovered, Auran, Flickr, Blizzard v bnetd, Copyright Amendment (Digital Agenda) Act 2000, OpenCourseware, iCommons, Linux, Creative Commons Licence, Law and Legal Studies, 180115 Intellectual Property Law, Copyright Act 1968, Universal Music Australia Pty Ltd v Sharman, How Big Media Uses Technology and the Law to Lock Down Culture and Control Creativity, Public Library of Science, Culture Jamming, Copyright Amendment Act 2006, Smart State Strategy, Blog, Queensland, copyright history, Statute of Anne, Games, Ladbroke (Football) Ltd v William Hill (Football) Ltd, Magnatune, 160511 Research Science and Technology Policy, TPM, End User Licence Agreement, 160600 POLITICAL SCIENCE, 160805 Social Change, 180000 LAW AND LEGAL STUDIES, copyleft, Open Access to knowledge, ACRO, Moral Rights, Science Commons, Oz Magazine, Outfoxed, Youth Internet Radio Network, copyright term, free culture, copyright and contract, Digital Agenda Reforms, DRM, AMCOS, SoundClick, The Corporation, Australian Creative Resources Online, user Online Games, 180100 LAW, Australian copyright, Law
Abstract

Open Content Licensing: Cultivating the Creative Commons brings together papers from some of the most prominent thinkers of our time on the internet, law and the importance of open content licensing in the digital age. Drawing on material presented at the Queensland University of Technology conference of the same name in January 2005, the text provides a snapshot of the thoughts of over 30 Australian and international experts – including Professor Lawrence Lessig, Futurist Richard Neville and the Hon Justice Ronald Sackville – on topics surrounding the international Creative Commons, from the landmark Eldred v Ashcroft copyright term decision to the legalities of digital sampling in a remix world. Edited book: Contributors include: Richard Neville, Professor Arun Sharma, Mark Fallu, Professor Barry Conyngham AM, Greg Lane, Professor Brian Fitzgerald, Nic Suzor, Professor Lawrence Lessig, Professor Richard Jones, Professor Greg Hearn, Professor John Quiggin, Dr David Rooney, Neeru Paharia, Michael Lavarch, Stuart Cunningha, Dr Terry Cutler, Damien O’Brien, Renato Ianella, Carol Fripp, Dennis MacNamara, Jean Burgess, The Hon Justice James Douglas, The Hon Justice Ronald Sackville, Linda Lavarch MP, Tom Cochrane, Ian Oi, Dr Anne Fitzgerald, Neale Hooper, Keith Done, Sal Humphreys, John Banks

Published
2007

15. Variant ATRX Syndrome with Dysfunction ofATRXandMAGT1Genes

Author

Qiao, Ying, primary, Mondal, Kajari, additional, Trapani, Valentina, additional, Wen, Jiadi, additional, Carpenter, Gillian, additional, Wildin, Robert, additional, Price, E. Magda, additional, Gibbons, Richard J., additional, Eichmeyer, Jennifer, additional, Jiang, Ruby, additional, DuPont, Barbara, additional, Martell, Sally, additional, Lewis, Suzanne M. E., additional, Robinson, Wendy P., additional, O'Driscoll, Mark, additional, Wolf, Federica I., additional, Zwick, Michael E., additional, and Rajcan-Separovic, Evica, additional

Published
2013
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18. Functional consequences of copy number variants in miscarriage.

Author

Jiadi Wen, Hanna, Courtney W., Martell, Sally, Leung, Peter C. K., Lewis, Suzanne M. E., Robinson, Wendy P., Stephenson, Mary D., and Rajcan-Separovic, Evica

Subjects
DNA copy number variations, GENETIC polymorphisms, GENOMIC imprinting, MISCARRIAGE, ALLELES, GENETICS
Abstract

Background: The presence of unique copy number variations (CNVs) in miscarriages suggests that their integral genes have a role in maintaining early pregnancy. In our previous work, we identified 19 unique CNVs in ~40% of studied euploid miscarriages, which were predominantly familial in origin. In our current work, we assessed their relevance to miscarriage by expression analysis of 14 genes integral to CNVs in available miscarriage chorionic villi. As familial CNVs could cause miscarriage due to imprinting effect, we investigated the allelic expression of one of the genes (TIMP2) previously suggested to be maternally expressed in placenta and involved in placental remodelling and embryo development. Results: Six out of fourteen genes had detectable expression in villi and for three genes the RNA and protein expression was altered due to maternal CNVs. These genes were integral to duplication on Xp22.2 (TRAPPC2 and OFD!) or disrupted by a duplication mapping to 17q25.3 (TIMP2). RNA and protein expression was increased for TRAPPC2 and OFD! and reduced for TIMP2 in carrier miscarriages. The three genes have roles in processes important for pregnancy development such as extracellular matrix homeostasis (TIMP2 and TRAPPC2) and cilia function (OFD!). TIMP2 allelic expression was not affected by the CNV in miscarriages in comparison to control elective terminations. Conclusion: We propose that functional studies of CNVs could help determine if and how the miscarriage CNVs affect the expression of integral genes. In case of parental CNVs, assessment of the function of their integral genes in parental reproductive tissues should be also considered in the future, especially if they affect processes relevant for pregnancy development and support. [ABSTRACT FROM AUTHOR]

Published
2015
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20. miRNA and miRNA target genes in copy number variations occurring in individuals with intellectual disability.

Author

Qiao, Ying, Badduke, Chansonette, Mercier, Eloi, Lewis, Suzanne M. E., Pavlidis, Paul, and Rajcan-Separovic, Evica

Subjects
MICRORNA, DNA copy number variations, NON-coding RNA, HUMAN proteins, GENE expression, NUCLEOTIDES
Abstract

Background: MicroRNAs (miRNAs) are a family of short, non-coding RNAs modulating expression of human protein coding genes (miRNA target genes). Their dysfunction is associated with many human diseases, including neurodevelopmental disorders. It has been recently shown that genomic copy number variations (CNVs) can cause aberrant expression of integral miRNAs and their target genes, and contribute to intellectual disability (ID). Results: To better understand the CNV-miRNA relationship in ID, we investigated the prevalence and function of miRNAs and miRNA target genes in five groups of CNVs. Three groups of CNVs were from 213 probands with ID (24 de novo CNVs, 46 familial and 216 common CNVs), one group of CNVs was from a cohort of 32 cognitively normal subjects (67 CNVs) and one group of CNVs represented 40 ID related syndromic regions listed in DECIPHER (30 CNVs) which served as positive controls for CNVs causing or predisposing to ID. Our results show that 1). The number of miRNAs is significantly higher in de novo or DECIPHER CNVs than in familial or common CNV subgroups (P < 0.01). 2). miRNAs with brain related functions are more prevalent in de novo CNV groups compared to common CNV groups. 3). More miRNA target genes are found in de novo, familial and DECIPHER CNVs than in the common CNV subgroup (P < 0.05). 4). The MAPK signaling cascade is found to be enriched among the miRNA target genes from de novo and DECIPHER CNV subgroups. Conclusions: Our findings reveal an increase in miRNA and miRNA target gene content in de novo versus common CNVs in subjects with ID. Their expression profile and participation in pathways support a possible role of miRNA copy number change in cognition and/or CNV-mediated developmental delay. Systematic analysis of expression/ function of miRNAs in addition to coding genes integral to CNVs could uncover new causes of IDE. [ABSTRACT FROM AUTHOR]

Published
2013
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21. DRD2 and PPP1R1B (DARPP-32) polymorphisms independently confer increased risk for autism spectrum disorders and additively predict affected status in male-only affected sib-pair families.

Author

Hettinger, Joe A., Liu, Hudson, Melissa L., Lee, Alana, Cohen, Ira L., Michaelis, Ron C., Schwartz, Charles E., Lewis, Suzanne M. E., and Holden, Jeanette J. A.

Subjects
GENETIC polymorphisms, DOPAMINE, AUTISM spectrum disorders, COHORT analysis, SOCIAL interaction
Abstract

Background: The neurotransmitter dopamine (DA) modulates executive functions, learning, and emotional processing, all of which are impaired in individuals with autism spectrum disorders (ASDs). Our previous findings suggest a role for dopamine-related genes in families with only affected males. Methods: We examined two additional genes which affect DA function, the DRD2 and PPP1R1B (DARPP-32) genes, in a cohort of 112 male-only affected sib-pair families. Selected polymorphisms spanning these genes were genotyped and both family-based and population-based tests were carried out for association analysis. General discriminant analysis was used to examine the gene-gene interactions in predicting autism susceptibility. Results: There was a significantly increased frequency of the DRD2 rs1800498TT genotype (P = 0.007) in affected males compared to the comparison group, apparently due to over-transmission of the T allele (P = 0.0003). The frequency of the PPP1R1B rs1495099CC genotype in affected males was also higher than that in the comparison group (P = 0.002) due to preferential transmission of the C allele from parents to affected children (P = 0.0009). Alleles rs1800498T and rs1495099C were associated with more severe problems in social interaction (P = 0.0002 and P = 0.0016, respectively) and communication (P = 0.0004 and P = 0.0046), and increased stereotypic behaviours (P = 0.0021 and P = 0.00072). General discriminant analysis found that the DRD2 and PPP1R1B genes additively predicted ASDs (P = 0.00011; Canonical R = 0.26) and explain ~7% of the variance in our families. All findings remained significant following corrections for multiple testing. Conclusion: Our findings support a role for the DRD2 and PPP1R1B genes in conferring risk for autism in families with only affected males and show an additive effect of these genes towards prediction of affected status in our families. [ABSTRACT FROM AUTHOR]

Published
2012
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22. Understanding the impact of 1q21.1 copy number variant.

Author

Harvard, Chansonette, Strong, Emma, Mercier, Eloi, Colnaghi, Rita, Alcantara, Diana, Chow, Eva, Martell, Sally, Tyson, Christine, Hrynchak, Monica, McGillivray, Barbara, Hamilton, Sara, Marles, Sandra, Mhanni, Aziz, Dawson, Angelika J, Pavlidis, Paul, Qiao, Ying, Holden, Jeanette J, Lewis, Suzanne M E, O'Driscoll, Mark, and Rajcan-Separovic, Evica

Subjects
GENETIC regulation, GENE expression, GENOMES, CELL lines, DISEASE complications
Abstract

Background: 1q21.1 Copy Number Variant (CNV) is associated with a highly variable phenotype ranging from congenital anomalies, learning deficits/intellectual disability (ID), to a normal phenotype. Hence, the clinical significance of this CNV can be difficult to evaluate. Here we described the consequences of the 1q21.1 CNV on genome-wide gene expression and function of selected candidate genes within 1q21.1 using cell lines from clinically well described subjects.Methods and Results: Eight subjects from 3 families were included in the study: six with a 1q21.1 deletion and two with a 1q21.1 duplication. High resolution Affymetrix 2.7M array was used to refine the 1q21.1 CNV breakpoints and exclude the presence of secondary CNVs of pathogenic relevance. Whole genome expression profiling, studied in lymphoblast cell lines (LBCs) from 5 subjects, showed enrichment of genes from 1q21.1 in the top 100 genes ranked based on correlation of expression with 1q21.1 copy number. The function of two top genes from 1q21.1, CHD1L/ALC1 and PRKAB2, was studied in detail in LBCs from a deletion and a duplication carrier. CHD1L/ALC1 is an enzyme with a role in chromatin modification and DNA damage response while PRKAB2 is a member of the AMP kinase complex, which senses and maintains systemic and cellular energy balance. The protein levels for CHD1L/ALC1 and PRKAB2 were changed in concordance with their copy number in both LBCs. A defect in chromatin remodeling was documented based on impaired decatenation (chromatid untangling) checkpoint (DCC) in both LBCs. This defect, reproduced by CHD1L/ALC1 siRNA, identifies a new role of CHD1L/ALC1 in DCC. Both LBCs also showed elevated levels of micronuclei following treatment with a Topoisomerase II inhibitor suggesting increased DNA breaks. AMP kinase function, specifically in the deletion containing LBCs, was attenuated.Conclusion: Our studies are unique as they show for the first time that the 1q21.1 CNV not only causes changes in the expression of its key integral genes, associated with changes at the protein level, but also results in changes in their known function, in the case of AMPK, and newly identified function such as DCC activation in the case of CHD1L/ALC1. Our results support the use of patient lymphoblasts for dissecting the functional sequelae of genes integral to CNVs in carrier cell lines, ultimately enhancing understanding of biological processes which may contribute to the clinical phenotype. [ABSTRACT FROM AUTHOR]

Published
2011
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23. The DLX1and DLX2 genes and susceptibility to autism spectrum disorders.

Author

Xudong Liu, Novosedlik, Natalia, Wang, Ami, Hudson, Melissa L., Cohen, Ira L., Chudley, Albert E., Forster-Gibson, Cynthia J., Lewis, Suzanne M. E., and Holden, Jeanette J. A.

Subjects
CEREBRAL cortex, AUTISM, TRANSCRIPTION factors, GABA, EPILEPSY, GENETIC disorders, HUMAN genetics
Abstract

An imbalance between excitation and inhibition in the cerebral cortex has been suggested as a possible etiology of autism. The DLX genes encode homeodomain-containing transcription factors controlling the generation of GABAergic cortical interneurons. The DLX1 and DLX2 genes lie head-to-head in 2q32, a region associated with autism susceptibility. We investigated 6 Tag SNPs within the DLX1/2 genes in two cohorts of multiplex (MPX) and one of simplex (SPX) families for association with autism. Family-based association tests showed strong association with five of the SNPs. The common alleles of rs743605 and rs4519482 were significantly associated with autism (P<0.012) in the first sample of 138 MPX families, with the latter remaining significant after correction for multiple testing (Pcor=0.0046). Findings in a second sample of 169 MPX families not only confirmed the association at rs4519482 (P=0.034) but also showed strong allelic association of the common alleles at rs788172, rs788173 and rs813720 (Pcor=0.0003–0.04). In the combined MPX families, the common alleles were all significantly associated with autism (Pcor=0.0005–0.016). The GGGTG haplotype was over transmitted in the two MPX cohorts and the combined samples [Pcor<0.05: Pcor=0.00007 for the combined MPX families, Odds Ratio: 1.75 (95% CI: 1.33–2.30)]. Further testing in 306 SPX families replicated the association at rs4519482 (P=0.033) and the over transmission of the haplotype GGGTG (P=0.012) although P-values were not significant after correction for multiple testing. The findings support the presence of two functional polymorphisms, one in or near each of the DLX genes that increase susceptibility to, or cause, autism in MPX families where there is a greater genetic component for these conditions.European Journal of Human Genetics (2009) 17, 228–235; doi:10.1038/ejhg.2008.148; published online 27 August 2008 [ABSTRACT FROM AUTHOR]

Published
2009
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25. DRD2 and PPP1R1B (DARPP-32) polymorphisms independently confer increased risk for autism spectrum disorders and additively predict affected status in male-only affected sib-pair families

Author

Hettinger, Joe A, Liu, Xudong, Hudson, Melissa L, Lee, Alana, Cohen, Ira L, Michaelis, Ron C, Schwartz, Charles E, Lewis, Suzanne M, and Holden, Jeanette J

Subjects
10. No inequality
Abstract

Background: The neurotransmitter dopamine (DA) modulates executive functions, learning, and emotional processing, all of which are impaired in individuals with autism spectrum disorders (ASDs). Our previous findings suggest a role for dopamine-related genes in families with only affected males. Methods: We examined two additional genes which affect DA function, the DRD2 and PPP1R1B (DARPP-32) genes, in a cohort of 112 male-only affected sib-pair families. Selected polymorphisms spanning these genes were genotyped and both family-based and population-based tests were carried out for association analysis. General discriminant analysis was used to examine the gene-gene interactions in predicting autism susceptibility. Results: There was a significantly increased frequency of the DRD2 rs1800498TT genotype (P = 0.007) in affected males compared to the comparison group, apparently due to over-transmission of the T allele (P = 0.0003). The frequency of the PPP1R1B rs1495099CC genotype in affected males was also higher than that in the comparison group (P = 0.002) due to preferential transmission of the C allele from parents to affected children (P = 0.0009). Alleles rs1800498T and rs1495099C were associated with more severe problems in social interaction (P = 0.0002 and P = 0.0016, respectively) and communication (P = 0.0004 and P = 0.0046), and increased stereotypic behaviours (P = 0.0021 and P = 0.00072). General discriminant analysis found that the DRD2 and PPP1R1B genes additively predicted ASDs (P = 0.00011; Canonical R = 0.26) and explain ~7% of the variance in our families. All findings remained significant following corrections for multiple testing. Conclusion: Our findings support a role for the DRD2 and PPP1R1B genes in conferring risk for autism in families with only affected males and show an additive effect of these genes towards prediction of affected status in our families.

26. Disruption at the PTCHD1Locus on Xp22.11 in Autism Spectrum Disorder and Intellectual Disability

Author

Noor, Abdul, Whibley, Annabel, Marshall, Christian R., Gianakopoulos, Peter J., Piton, Amelie, Carson, Andrew R., Orlic-Milacic, Marija, Lionel, Anath C., Sato, Daisuke, Pinto, Dalila, Drmic, Irene, Noakes, Carolyn, Senman, Lili, Zhang, Xiaoyun, Mo, Rong, Gauthier, Julie, Crosbie, Jennifer, Pagnamenta, Alistair T., Munson, Jeffrey, Estes, Annette M., Fiebig, Andreas, Franke, Andre, Schreiber, Stefan, Stewart, Alexandre F. R., Roberts, Robert, McPherson, Ruth, Guter, Stephen J., Cook, Edwin H., Dawson, Geraldine, Schellenberg, Gerard D., Battaglia, Agatino, Maestrini, Elena, Jeng, Linda, Hutchison, Terry, Rajcan-Separovic, Evica, Chudley, Albert E., Lewis, Suzanne M. E., Liu, Xudong, Holden, Jeanette J., Fernandez, Bridget, Zwaigenbaum, Lonnie, Bryson, Susan E., Roberts, Wendy, Szatmari, Peter, Gallagher, Louise, Stratton, Michael R., Gecz, Jozef, Brady, Angela F., Schwartz, Charles E., Schachar, Russell J., Monaco, Anthony P., Rouleau, Guy A., Hui, Chi-chung, Lucy Raymond, F., Scherer, Stephen W., and Vincent, John B.

Abstract

Mutations of the X-linked gene PTCHD1are associated with autism spectrum disorders and intellectual disability.

Published
2010
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27. Pathogenic variants in KMT2C result in a neurodevelopmental disorder distinct from Kleefstra and Kabuki syndromes.

Author

Rots D, Choufani S, Faundes V, Dingemans AJM, Joss S, Foulds N, Jones EA, Stewart S, Vasudevan P, Dabir T, Park SM, Jewell R, Brown N, Pais L, Jacquemont S, Jizi K, Ravenswaaij-Arts CMAV, Kroes HY, Stumpel CTRM, Ockeloen CW, Diets IJ, Nizon M, Vincent M, Cogné B, Besnard T, Kambouris M, Anderson E, Zackai EH, McDougall C, Donoghue S, O'Donnell-Luria A, Valivullah Z, O'Leary M, Srivastava S, Byers H, Leslie N, Mazzola S, Tiller GE, Vera M, Shen JJ, Boles R, Jain V, Brischoux-Boucher E, Kinning E, Simpson BN, Giltay JC, Harris J, Keren B, Guimier A, Marijon P, Vries BBA, Motter CS, Mendelsohn BA, Coffino S, Gerkes EH, Afenjar A, Visconti P, Bacchelli E, Maestrini E, Delahaye-Duriez A, Gooch C, Hendriks Y, Adams H, Thauvin-Robinet C, Josephi-Taylor S, Bertoli M, Parker MJ, Rutten JW, Caluseriu O, Vernon HJ, Kaziyev J, Zhu J, Kremen J, Frazier Z, Osika H, Breault D, Nair S, Lewis SME, Ceroni F, Viggiano M, Posar A, Brittain H, Giovanna T, Giulia G, Quteineh L, Ha-Vinh Leuchter R, Zonneveld-Huijssoon E, Mellado C, Marey I, Coudert A, Aracena Alvarez MI, Kennis MGP, Bouman A, Roifman M, Amorós Rodríguez MI, Ortigoza-Escobar JD, Vernimmen V, Sinnema M, Pfundt R, Brunner HG, Vissers LELM, Kleefstra T, Weksberg R, and Banka S

Subjects
Humans, Male, Female, Child, Child, Preschool, Neoplasm Proteins genetics, Adolescent, Hypertrichosis genetics, Mutation, Failure to Thrive genetics, Histone-Lysine N-Methyltransferase genetics, Heart Defects, Congenital, Abnormalities, Multiple genetics, Vestibular Diseases genetics, Intellectual Disability genetics, Face abnormalities, Face pathology, DNA-Binding Proteins genetics, Hematologic Diseases genetics, Neurodevelopmental Disorders genetics, Craniofacial Abnormalities genetics, Chromosome Deletion, Chromosomes, Human, Pair 9 genetics, DNA Methylation genetics
Abstract

Trithorax-related H3K4 methyltransferases, KMT2C and KMT2D, are critical epigenetic modifiers. Haploinsufficiency of KMT2C was only recently recognized as a cause of neurodevelopmental disorder (NDD), so the clinical and molecular spectrums of the KMT2C-related NDD (now designated as Kleefstra syndrome 2) are largely unknown. We ascertained 98 individuals with rare KMT2C variants, including 75 with protein-truncating variants (PTVs). Notably, ∼15% of KMT2C PTVs were inherited. Although the most highly expressed KMT2C transcript consists of only the last four exons, pathogenic PTVs were found in almost all the exons of this large gene. KMT2C variant interpretation can be challenging due to segmental duplications and clonal hematopoesis-induced artifacts. Using samples from 27 affected individuals, divided into discovery and validation cohorts, we generated a moderate strength disorder-specific KMT2C DNA methylation (DNAm) signature and demonstrate its utility in classifying non-truncating variants. Based on 81 individuals with pathogenic/likely pathogenic variants, we demonstrate that the KMT2C-related NDD is characterized by developmental delay, intellectual disability, behavioral and psychiatric problems, hypotonia, seizures, short stature, and other comorbidities. The facial module of PhenoScore, applied to photographs of 34 affected individuals, reveals that the KMT2C-related facial gestalt is significantly different from the general NDD population. Finally, using PhenoScore and DNAm signatures, we demonstrate that the KMT2C-related NDD is clinically and epigenetically distinct from Kleefstra and Kabuki syndromes. Overall, we define the clinical features, molecular spectrum, and DNAm signature of the KMT2C-related NDD and demonstrate they are distinct from Kleefstra and Kabuki syndromes highlighting the need to rename this condition., Competing Interests: Declaration of interests R.W. is a consultant (equity) for Alamya Health., (Copyright © 2024 American Society of Human Genetics. All rights reserved.)

Published
2024
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28. The spiking output of the mouse olfactory bulb encodes large-scale temporal features of natural odor environments.

Author

Lewis SM, Suarez LM, Rigolli N, Franks KM, Steinmetz NA, and Gire DH

Abstract

In natural odor environments, odor travels in plumes. Odor concentration dynamics change in characteristic ways across the width and length of a plume. Thus, spatiotemporal dynamics of plumes have informative features for animals navigating to an odor source. Population activity in the olfactory bulb (OB) has been shown to follow odor concentration across plumes to a moderate degree (Lewis et al., 2021). However, it is unknown whether the ability to follow plume dynamics is driven by individual cells or whether it emerges at the population level. Previous research has explored the responses of individual OB cells to isolated features of plumes, but it is difficult to adequately sample the full feature space of plumes as it is still undetermined which features navigating mice employ during olfactory guided search. Here we released odor from an upwind odor source and simultaneously recorded both odor concentration dynamics and cellular response dynamics in awake, head-fixed mice. We found that longer timescale features of odor concentration dynamics were encoded at both the cellular and population level. At the cellular level, responses were elicited at the beginning of the plume for each trial, signaling plume onset. Plumes with high odor concentration elicited responses at the end of the plume, signaling plume offset. Although cellular level tracking of plume dynamics was observed to be weak, we found that at the population level, OB activity distinguished whiffs and blanks (accurately detected odor presence versus absence) throughout the duration of a plume. Even ~20 OB cells were enough to accurately discern odor presence throughout a plume. Our findings indicate that the full range of odor concentration dynamics and high frequency fluctuations are not encoded by OB spiking activity. Instead, relatively lower-frequency temporal features of plumes, such as plume onset, plume offset, whiffs, and blanks, are represented in the OB., Competing Interests: Competing interest statement The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published
2024
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29. Exome sequencing identified a de novo mutation of PURA gene in a patient with familial Xp22.31 microduplication.

Author

Qiao Y, Bagheri H, Tang F, Badduke C, Martell S, Lewis SME, Robinson W, Connolly MB, Arbour L, and Rajcan-Separovic E

Subjects
Child, Craniofacial Abnormalities pathology, Developmental Disabilities pathology, Genetic Diseases, X-Linked pathology, Heterozygote, Humans, Male, Mutation, Missense, Syndrome, Chromosome Duplication, Chromosomes, Human, X genetics, Craniofacial Abnormalities genetics, DNA-Binding Proteins genetics, Developmental Disabilities genetics, Genetic Diseases, X-Linked genetics, Phenotype, Transcription Factors genetics
Abstract

The clinical significance of Xp22.31 microduplication is controversial as it is reported in subjects with developmental delay (DD), their unaffected relatives and unrelated controls. We performed multifaceted studies in a family of a boy with hypotonia, dysmorphic features and DD who carried a 600 Kb Xp22.31 microduplication (7515787-8123310bp, hg19) containing two genes, VCX and PNPLA4. The duplication was transmitted from his cognitively normal maternal grandfather. We found no evidence of the duplication causing the proband's DD and congenital anomalies based on unaltered expression of PNPLA4 in the proband and his mother in comparison to controls and preferential activation of the paternal chromosome X with Xp22.31 duplication in proband's mother. However, a de novo, previously reported deleterious, missense mutation in Pur-alpha gene (PURA) (5q31.2), with a role in neuronal differentiation was detected in the proband by exome sequencing. We propose that the variability in the phenotype in carriers of Xp22.31 microduplication can be due to a second and more deleterious genetic mutation in more severely affected carriers. Widespread use of whole genome next generation sequencing in families with Xp22.31 CNV could help identify such cases., (Copyright © 2018. Published by Elsevier Masson SAS.)

Published
2019
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30. Disruption at the PTCHD1 Locus on Xp22.11 in Autism spectrum disorder and intellectual disability.

Author

Noor A, Whibley A, Marshall CR, Gianakopoulos PJ, Piton A, Carson AR, Orlic-Milacic M, Lionel AC, Sato D, Pinto D, Drmic I, Noakes C, Senman L, Zhang X, Mo R, Gauthier J, Crosbie J, Pagnamenta AT, Munson J, Estes AM, Fiebig A, Franke A, Schreiber S, Stewart AF, Roberts R, McPherson R, Guter SJ, Cook EH Jr, Dawson G, Schellenberg GD, Battaglia A, Maestrini E, Jeng L, Hutchison T, Rajcan-Separovic E, Chudley AE, Lewis SM, Liu X, Holden JJ, Fernandez B, Zwaigenbaum L, Bryson SE, Roberts W, Szatmari P, Gallagher L, Stratton MR, Gecz J, Brady AF, Schwartz CE, Schachar RJ, Monaco AP, Rouleau GA, Hui CC, Lucy Raymond F, Scherer SW, and Vincent JB

Subjects
Animals, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases genetics, Female, Humans, In Situ Hybridization, Male, Mice, Mutation, Nerve Tissue Proteins genetics, Oligonucleotide Array Sequence Analysis, Potassium Channels genetics, Reverse Transcriptase Polymerase Chain Reaction, Autistic Disorder genetics, Genes, X-Linked genetics, Intellectual Disability genetics, Membrane Proteins genetics
Abstract

Autism is a common neurodevelopmental disorder with a complex mode of inheritance. It is one of the most highly heritable of the complex disorders, although the underlying genetic factors remain largely unknown. Here, we report mutations in the X-chromosome PTCHD1 (patched-related) gene in seven families with autism spectrum disorder (ASD) and in three families with intellectual disability. A 167-kilobase microdeletion spanning exon 1 was found in two brothers, one with ASD and the other with a learning disability and ASD features; a 90-kilobase microdeletion spanning the entire gene was found in three males with intellectual disability in a second family. In 900 probands with ASD and 208 male probands with intellectual disability, we identified seven different missense changes (in eight male probands) that were inherited from unaffected mothers and not found in controls. Two of the ASD individuals with missense changes also carried a de novo deletion at another ASD susceptibility locus (DPYD and DPP6), suggesting complex genetic contributions. In additional males with ASD, we identified deletions in the 5' flanking region of PTCHD1 that disrupted a complex noncoding RNA and potential regulatory elements; equivalent changes were not found in male control individuals. Thus, our systematic screen of PTCHD1 and its 5' flanking regions suggests that this locus is involved in ~1% of individuals with ASD and intellectual disability.

Published
2010
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31. The DLX1and DLX2 genes and susceptibility to autism spectrum disorders.

Author

Liu X, Novosedlik N, Wang A, Hudson ML, Cohen IL, Chudley AE, Forster-Gibson CJ, Lewis SM, and Holden JJ

Subjects
Cohort Studies, Family, Humans, Polymorphism, Single Nucleotide, Autistic Disorder genetics, Genetic Predisposition to Disease, Homeodomain Proteins genetics, Transcription Factors genetics
Abstract

An imbalance between excitation and inhibition in the cerebral cortex has been suggested as a possible etiology of autism. The DLX genes encode homeodomain-containing transcription factors controlling the generation of GABAergic cortical interneurons. The DLX1 and DLX2 genes lie head-to-head in 2q32, a region associated with autism susceptibility. We investigated 6 Tag SNPs within the DLX1/2 genes in two cohorts of multiplex (MPX) and one of simplex (SPX) families for association with autism. Family-based association tests showed strong association with five of the SNPs. The common alleles of rs743605 and rs4519482 were significantly associated with autism (P<0.012) in the first sample of 138 MPX families, with the latter remaining significant after correction for multiple testing (P(cor)=0.0046). Findings in a second sample of 169 MPX families not only confirmed the association at rs4519482 (P=0.034) but also showed strong allelic association of the common alleles at rs788172, rs788173 and rs813720 (P(cor)=0.0003-0.04). In the combined MPX families, the common alleles were all significantly associated with autism (P(cor)=0.0005-0.016). The GGGTG haplotype was over transmitted in the two MPX cohorts and the combined samples [P(cor)<0.05: P(cor)=0.00007 for the combined MPX families, Odds Ratio: 1.75 (95% CI: 1.33-2.30)]. Further testing in 306 SPX families replicated the association at rs4519482 (P=0.033) and the over transmission of the haplotype GGGTG (P=0.012) although P-values were not significant after correction for multiple testing. The findings support the presence of two functional polymorphisms, one in or near each of the DLX genes that increase susceptibility to, or cause, autism in MPX families where there is a greater genetic component for these conditions.

Published
2009
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32. Complete rescue of lipoprotein lipase-deficient mice by somatic gene transfer of the naturally occurring LPLS447X beneficial mutation.

Author

Ross CJ, Liu G, Kuivenhoven JA, Twisk J, Rip J, van Dop W, Excoffon KJ, Lewis SM, Kastelein JJ, and Hayden MR

Subjects
Adenoviridae genetics, Animals, Animals, Newborn, CHO Cells, Cholesterol, HDL blood, Cricetinae, Fertility, Gene Transfer Techniques, Humans, Hypertriglyceridemia blood, Hypertriglyceridemia genetics, Lactation, Mice, Mice, Inbred C57BL, Mice, Mutant Strains, RNA, Messenger analysis, Triglycerides blood, Genetic Therapy methods, Hypertriglyceridemia therapy, Lipoprotein Lipase genetics, Lipoprotein Lipase metabolism, Point Mutation
Abstract

The naturally occurring human lipoprotein lipase S447X variant (LPLS447X) exemplifies a gain-of function mutation with significant benefits including decreased plasma triglycerides (TG), increased high-density lipoprotein (HDL) cholesterol, and reduced risk of coronary artery disease. The S447X variant may be associated with higher LPL catalytic activity; however, in vitro data supporting this hypothesis are contradictory. We wanted to investigate the in vivo mechanism by which the LPLS447X variant improves the lipid profile of S447X carriers. We conducted a functional assessment of human LPLS447X compared with LPLWT in mice. LPL variants were compared in the absence of endogenous mouse LPL in newborn LPL(-/-) mice by adenoviral-mediated gene transfer. LPL(-/-) mice normally exhibit severe hypertriglyceridemia and die within 48 hours of birth. LPLWT gene transfer prolonged the survival of mice up to 21 days. In contrast, LPLS447X completely rescued 95% of the mice to adulthood and increased LPL catalytic activity in postheparin plasma 2.1-fold compared with LPLWT at day 3 (P=0.003). LPLS447X also reduced plasma TG 99% from baseline (P<0.001), 2-fold more than LPLWT, (P<0.01) and increased plasma HDL cholesterol 2.9-fold higher than LPLWT (P<0.01). These data provide in vivo evidence that the increased catalytic activity of LPLS447X improves plasma TG clearance and increases the HDL cholesterol pool compared with LPLWT.

Published
2005
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33. Mutations in the human ortholog of Aristaless cause X-linked mental retardation and epilepsy.

Author

Strømme P, Mangelsdorf ME, Shaw MA, Lower KM, Lewis SM, Bruyere H, Lütcherath V, Gedeon AK, Wallace RH, Scheffer IE, Turner G, Partington M, Frints SG, Fryns JP, Sutherland GR, Mulley JC, and Gécz J

Subjects
Amino Acid Sequence, Animals, Family Health, Female, Haplotypes, Humans, Male, Mice, Models, Genetic, Molecular Sequence Data, Mutation, Missense, Nucleic Acid Hybridization, Pedigree, Poly A genetics, Sequence Homology, Amino Acid, Tissue Distribution, Transcription, Genetic, Drosophila Proteins genetics, Epilepsy genetics, Intellectual Disability genetics, Mutation, X Chromosome
Abstract

Mental retardation and epilepsy often occur together. They are both heterogeneous conditions with acquired and genetic causes. Where causes are primarily genetic, major advances have been made in unraveling their molecular basis. The human X chromosome alone is estimated to harbor more than 100 genes that, when mutated, cause mental retardation. At least eight autosomal genes involved in idiopathic epilepsy have been identified, and many more have been implicated in conditions where epilepsy is a feature. We have identified mutations in an X chromosome-linked, Aristaless-related, homeobox gene (ARX), in nine families with mental retardation (syndromic and nonspecific), various forms of epilepsy, including infantile spasms and myoclonic seizures, and dystonia. Two recurrent mutations, present in seven families, result in expansion of polyalanine tracts of the ARX protein. These probably cause protein aggregation, similar to other polyalanine and polyglutamine disorders. In addition, we have identified a missense mutation within the ARX homeodomain and a truncation mutation. Thus, it would seem that mutation of ARX is a major contributor to X-linked mental retardation and epilepsy.

Published
2002
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