Your search keyword '"Martin, Charles-Olivier"' showing total 14 results

1. Neurocognitive profiles of 22q11.2 and 16p11.2 deletions and duplications

Author

Gur, Ruben C., Bearden, Carrie E., Jacquemont, Sebastien, Swillen, Ann, van Amelsvoort, Therese, van den Bree, Marianne, Vorstman, Jacob, Sebat, Jonathan, Ruparel, Kosha, Gallagher, Robert Sean, McClellan, Emily, White, Lauren, Crowley, Terrence Blaine, Giunta, Victoria, Kushan, Leila, O’Hora, Kathleen, Verbesselt, Jente, Vandensande, Ans, Vingerhoets, Claudia, van Haelst, Mieke, Hall, Jessica, Harwood, Janet, Chawner, Samuel J.R.A., Patel, Nishi, Palad, Katrina, Hong, Oanh, Guevara, James, Martin, Charles Olivier, Jizi, Khadije, Bélanger, Anne-Marie, Scherer, Stephen W., Bassett, Anne S., McDonald-McGinn, Donna M., and Gur, Raquel E.

Published

2025

2. Specific EEG resting state biomarkers in FXS and ASD

Author

Proteau-Lemieux, Mélodie, Knoth, Inga Sophia, Davoudi, Saeideh, Martin, Charles-Olivier, Bélanger, Anne-Marie, Fontaine, Valérie, Côté, Valérie, Agbogba, Kristian, Vachon, Keely, Whitlock, Kerri, Biag, Hazel Maridith Barlahan, Thurman, Angela John, Rosenfelt, Cory, Tassone, Flora, Frei, Julia, Capano, Lucia, Abbeduto, Leonard, Jacquemont, Sébastien, Hessl, David, Hagerman, Randi Jenssen, Schneider, Andrea, Bolduc, Francois, Anagnostou, Evdokia, and Lippe, Sarah

Published

2024

3. Using rare genetic mutations to revisit structural brain asymmetry

Author

Kopal, Jakub, Kumar, Kuldeep, Shafighi, Kimia, Saltoun, Karin, Modenato, Claudia, Moreau, Clara A., Huguet, Guillaume, Jean-Louis, Martineau, Martin, Charles-Olivier, Saci, Zohra, Younis, Nadine, Douard, Elise, Jizi, Khadije, Beauchamp-Chatel, Alexis, Kushan, Leila, Silva, Ana I., van den Bree, Marianne B. M., Linden, David E. J., Owen, Michael J., Hall, Jeremy, Lippé, Sarah, Draganski, Bogdan, Sønderby, Ida E., Andreassen, Ole A., Glahn, David C., Thompson, Paul M., Bearden, Carrie E., Zatorre, Robert, Jacquemont, Sébastien, and Bzdok, Danilo

Published

2024

4. Rare CNVs and phenome-wide profiling highlight brain structural divergence and phenotypical convergence

Author

Kopal, Jakub, Kumar, Kuldeep, Saltoun, Karin, Modenato, Claudia, Moreau, Clara A., Martin-Brevet, Sandra, Huguet, Guillaume, Jean-Louis, Martineau, Martin, Charles-Olivier, Saci, Zohra, Younis, Nadine, Tamer, Petra, Douard, Elise, Maillard, Anne M., Rodriguez-Herreros, Borja, Pain, Aurèlie, Richetin, Sonia, Kushan, Leila, Silva, Ana I., van den Bree, Marianne B. M., Linden, David E. J., Owen, Michael J., Hall, Jeremy, Lippé, Sarah, Draganski, Bogdan, Sønderby, Ida E., Andreassen, Ole A., Glahn, David C., Thompson, Paul M., Bearden, Carrie E., Jacquemont, Sébastien, and Bzdok, Danilo

Published

2023

5. Conditional canonical correlation estimation based on covariates with random forests

Author

Alakus, Cansu, Larocque, Denis, Jacquemont, Sebastien, Barlaam, Fanny, Martin, Charles-Olivier, Agbogba, Kristian, Lippe, Sarah, and Labbe, Aurelie

Subjects

Statistics - Methodology, Statistics - Applications, Statistics - Machine Learning

Abstract

Investigating the relationships between two sets of variables helps to understand their interactions and can be done with canonical correlation analysis (CCA). However, the correlation between the two sets can sometimes depend on a third set of covariates, often subject-related ones such as age, gender, or other clinical measures. In this case, applying CCA to the whole population is not optimal and methods to estimate conditional CCA, given the covariates, can be useful. We propose a new method called Random Forest with Canonical Correlation Analysis (RFCCA) to estimate the conditional canonical correlations between two sets of variables given subject-related covariates. The individual trees in the forest are built with a splitting rule specifically designed to partition the data to maximize the canonical correlation heterogeneity between child nodes. We also propose a significance test to detect the global effect of the covariates on the relationship between two sets of variables. The performance of the proposed method and the global significance test is evaluated through simulation studies that show it provides accurate canonical correlation estimations and well-controlled Type-1 error. We also show an application of the proposed method with EEG data., Comment: 27 pages, 8 figures, 1 table

Published

2020

6. Genetic Heterogeneity Shapes Brain Connectivity in Psychiatry

Author

Moreau, Clara A., Harvey, Annabelle, Kumar, Kuldeep, Huguet, Guillaume, Urchs, Sebastian G.W., Douard, Elise A., Schultz, Laura M., Sharmarke, Hanad, Jizi, Khadije, Martin, Charles-Olivier, Younis, Nadine, Tamer, Petra, Rolland, Thomas, Martineau, Jean-Louis, Orban, Pierre, Silva, Ana Isabel, Hall, Jeremy, van den Bree, Marianne B.M., Owen, Michael J., Linden, David E.J., Labbe, Aurelie, Lippé, Sarah, Bearden, Carrie E., Almasy, Laura, Glahn, David C., Thompson, Paul M., Bourgeron, Thomas, Bellec, Pierre, and Jacquemont, Sebastien

Published

2023

7. Genome-wide analysis of gene dosage in 24,092 individuals estimates that 10,000 genes modulate cognitive ability

Author

Huguet, Guillaume, Schramm, Catherine, Douard, Elise, Tamer, Petra, Main, Antoine, Monin, Pauline, England, Jade, Jizi, Khadije, Renne, Thomas, Poirier, Myriam, Nowak, Sabrina, Martin, Charles-Olivier, Younis, Nadine, Knoth, Inga Sophia, Jean-Louis, Martineau, Saci, Zohra, Auger, Maude, Tihy, Frédérique, Mathonnet, Géraldine, Maftei, Catalina, Léveillé, France, Porteous, David, Davies, Gail, Redmond, Paul, Harris, Sarah E., Hill, W. David, Lemyre, Emmanuelle, Schumann, Gunter, Bourgeron, Thomas, Pausova, Zdenka, Paus, Tomas, Karama, Sherif, Lippe, Sarah, Deary, Ian J., Almasy, Laura, Labbe, Aurélie, Glahn, David, Greenwood, Celia M. T., and Jacquemont, Sébastien

Published

2021

8. Effects of eight neuropsychiatric copy number variants on human brain structure

Author

Modenato, Claudia, Kumar, Kuldeep, Moreau, Clara, Martin-Brevet, Sandra, Huguet, Guillaume, Schramm, Catherine, Jean-Louis, Martineau, Martin, Charles-Olivier, Younis, Nadine, Tamer, Petra, Douard, Elise, Thébault-Dagher, Fanny, Côté, Valérie, Charlebois, Audrey-Rose, Deguire, Florence, Maillard, Anne M., Rodriguez-Herreros, Borja, Pain, Aurèlie, Richetin, Sonia, Melie-Garcia, Lester, Kushan, Leila, Silva, Ana I., van den Bree, Marianne B. M., Linden, David E. J., Owen, Michael J., Hall, Jeremy, Lippé, Sarah, Chakravarty, Mallar, Bzdok, Danilo, Bearden, Carrie E., Draganski, Bogdan, and Jacquemont, Sébastien

Published

2021

9. Subcortical Brain Alterations in Carriers of Genomic Copy Number Variants.

Author

Kumar, Kuldeep, Modenato, Claudia, Moreau, Clara, Ching, Christopher R.K., Harvey, Annabelle, Martin-Brevet, Sandra, Huguet, Guillaume, Jean-Louis, Martineau, Douard, Elise, Martin, Charles-Olivier, Younis, Nadine, Tamer, Petra, Maillard, Anne M., Rodriguez-Herreros, Borja, Pain, Aurélie, Kushan, Leila, Isaev, Dmitry, Alpert, Kathryn, Ragothaman, Anjani, and Turner, Jessica A.

Subjects

DNA copy number variations, ATTENTION-deficit hyperactivity disorder, DISEASE complications, MENTAL illness, BIPOLAR disorder

Abstract

Copy number variants (CNVs) are well-known genetic pleiotropic risk factors for multiple neurodevelopmental and psychiatric disorders (NPDs), including autism (ASD) and schizophrenia. Little is known about how different CNVs conferring risk for the same condition may affect subcortical brain structures and how these alterations relate to the level of disease risk conferred by CNVs. To fill this gap, the authors investigated gross volume, vertex-level thickness, and surface maps of subcortical structures in 11 CNVs and six NPDs. Subcortical structures were characterized using harmonized ENIGMA protocols in 675 CNV carriers (CNVs at 1q21.1, TAR, 13q12.12, 15q11.2, 16p11.2, 16p13.11, and 22q11.2; age range, 6–80 years; 340 males) and 782 control subjects (age range, 6–80 years; 387 males) as well as ENIGMA summary statistics for ASD, schizophrenia, attention deficit hyperactivity disorder, obsessive-compulsive disorder, bipolar disorder, and major depression. All CNVs showed alterations in at least one subcortical measure. Each structure was affected by at least two CNVs, and the hippocampus and amygdala were affected by five. Shape analyses detected subregional alterations that were averaged out in volume analyses. A common latent dimension was identified, characterized by opposing effects on the hippocampus/amygdala and putamen/pallidum, across CNVs and across NPDs. Effect sizes of CNVs on subcortical volume, thickness, and local surface area were correlated with their previously reported effect sizes on cognition and risk for ASD and schizophrenia. The findings demonstrate that subcortical alterations associated with CNVs show varying levels of similarities with those associated with neuropsychiatric conditions, as well distinct effects, with some CNVs clustering with adult-onset conditions and others with ASD. These findings provide insight into the long-standing questions of why CNVs at different genomic loci increase the risk for the same NPD and why a single CNV increases the risk for a diverse set of NPDs. [ABSTRACT FROM AUTHOR]

Published

2023

10. Brain functional connectivity mirrors genetic pleiotropy in psychiatric conditions.

Author

Moreau, Clara A, Kumar, Kuldeep, Harvey, Annabelle, Huguet, Guillaume, Urchs, Sebastian G W, Schultz, Laura M, Sharmarke, Hanad, Jizi, Khadije, Martin, Charles-Olivier, Younis, Nadine, Tamer, Petra, Martineau, Jean-Louis, Orban, Pierre, Silva, Ana Isabel, Hall, Jeremy, Bree, Marianne B M van den, Owen, Michael J, Linden, David E J, Lippé, Sarah, and Bearden, Carrie E

Subjects

GENETIC pleiotropy, LARGE-scale brain networks, FUNCTIONAL connectivity, FLUID intelligence, FUNCTIONAL magnetic resonance imaging, GENETIC variation

Abstract

Pleiotropy occurs when a genetic variant influences more than one trait. This is a key property of the genomic architecture of psychiatric disorders and has been observed for rare and common genomic variants. It is reasonable to hypothesize that the microscale genetic overlap (pleiotropy) across psychiatric conditions and cognitive traits may lead to similar overlaps at the macroscale brain level such as large-scale brain functional networks. We took advantage of brain connectivity, measured by resting-state functional MRI to measure the effects of pleiotropy on large-scale brain networks, a putative step from genes to behaviour. We processed nine resting-state functional MRI datasets including 32 726 individuals and computed connectome-wide profiles of seven neuropsychiatric copy-number-variants, five polygenic scores, neuroticism and fluid intelligence as well as four idiopathic psychiatric conditions. Nine out of 19 pairs of conditions and traits showed significant functional connectivity correlations (r Functional connectivity), which could be explained by previously published levels of genomic (r Genetic) and transcriptomic (r Transcriptomic) correlations with moderate to high concordance: r Genetic— r Functional connectivity = 0.71 [0.40–0.87] and r Transcriptomic— r Functional connectivity = 0.83 [0.52; 0.94]. Extending this analysis to functional connectivity profiles associated with rare and common genetic risk showed that 30 out of 136 pairs of connectivity profiles were correlated above chance. These similarities between genetic risks and psychiatric disorders at the connectivity level were mainly driven by the overconnectivity of the thalamus and the somatomotor networks. Our findings suggest a substantial genetic component for shared connectivity profiles across conditions and traits, opening avenues to delineate general mechanisms—amenable to intervention—across psychiatric conditions and genetic risks. [ABSTRACT FROM AUTHOR]

Published

2023

11. EEG Signal Complexity Is Reduced During Resting-State in Fragile X Syndrome.

Author

Proteau-Lemieux, Mélodie, Knoth, Inga Sophia, Agbogba, Kristian, Côté, Valérie, Barlahan Biag, Hazel Maridith, Thurman, Angela John, Martin, Charles-Olivier, Bélanger, Anne-Marie, Rosenfelt, Cory, Tassone, Flora, Abbeduto, Leonard J., Jacquemont, Sébastien, Hagerman, Randi, Bolduc, François, Hessl, David, Schneider, Andrea, and Lippé, Sarah

Subjects

FRAGILE X syndrome, INTELLECTUAL disabilities, ELECTROENCEPHALOGRAPHY, STAGNATION point, AGE distribution, NEURAL development

Abstract

Introduction: Fragile X syndrome (FXS) is a genetic disorder caused by a mutation of the fragile X mental retardation 1 gene (FMR1). FXS is associated with neurophysiological abnormalities, including cortical hyperexcitability. Alterations in electroencephalogram (EEG) resting-state power spectral density (PSD) are well-defined in FXS and were found to be linked to neurodevelopmental delays. Whether non-linear dynamics of the brain signal are also altered remains to be studied. Methods: In this study, resting-state EEG power, including alpha peak frequency (APF) and theta/beta ratio (TBR), as well as signal complexity using multi-scale entropy (MSE) were compared between 26 FXS participants (ages 5–28 years), and 7 neurotypical (NT) controls with a similar age distribution. Subsequently a replication study was carried out, comparing our cohort to 19 FXS participants independently recorded at a different site. Results: PSD results confirmed the increased gamma, decreased alpha power and APF in FXS participants compared to NT controls. No alterations in TBR were found. Importantly, results revealed reduced signal complexity in FXS participants, specifically in higher scales, suggesting that altered signal complexity is sensitive to brain alterations in this population. The replication study mostly confirmed these results and suggested critical points of stagnation in the neurodevelopmental curve of FXS. Conclusion: Signal complexity is a powerful feature that can be added to the electrophysiological biomarkers of brain maturation in FXS. [ABSTRACT FROM AUTHOR]

Published

2021

12. Conditional canonical correlation estimation based on covariates with random forests.

Author

Alakuş, Cansu, Larocque, Denis, Jacquemont, Sébastien, Barlaam, Fanny, Martin, Charles-Olivier, Agbogba, Kristian, Lippé, Sarah, and Labbe, Aurélie

Subjects

RANDOM forest algorithms, AIRBORNE lasers, STATISTICAL correlation, STATISTICAL hypothesis testing, GENDER, ELECTROENCEPHALOGRAPHY

Abstract

Motivation Investigating the relationships between two sets of variables helps to understand their interactions and can be done with canonical correlation analysis (CCA). However, the correlation between the two sets can sometimes depend on a third set of covariates, often subject-related ones such as age, gender or other clinical measures. In this case, applying CCA to the whole population is not optimal and methods to estimate conditional CCA, given the covariates, can be useful. Results We propose a new method called Random Forest with Canonical Correlation Analysis (RFCCA) to estimate the conditional canonical correlations between two sets of variables given subject-related covariates. The individual trees in the forest are built with a splitting rule specifically designed to partition the data to maximize the canonical correlation heterogeneity between child nodes. We also propose a significance test to detect the global effect of the covariates on the relationship between two sets of variables. The performance of the proposed method and the global significance test is evaluated through simulation studies that show it provides accurate canonical correlation estimations and well-controlled Type-1 error. We also show an application of the proposed method with EEG data. Availability and implementation RFCCA is implemented in a freely available R package on CRAN (https://CRAN.R-project.org/package=RFCCA). Supplementary information Supplementary data are available at Bioinformatics online. [ABSTRACT FROM AUTHOR]

Published

2021

13. Author Correction: Using rare genetic mutations to revisit structural brain asymmetry.

Author

Kopal, Jakub, Kumar, Kuldeep, Shafighi, Kimia, Saltoun, Karin, Modenato, Claudia, Moreau, Clara A., Huguet, Guillaume, Jean-Louis, Martineau, Martin, Charles-Olivier, Saci, Zohra, Younis, Nadine, Douard, Elise, Jizi, Khadije, Beauchamp-Chatel, Alexis, Kushan, Leila, Silva, Ana I., van den Bree, Marianne B. M., Linden, David E. J., Owen, Michael J., and Hall, Jeremy

Published

2024

14. INFLUENCE OF READING HABITS ON CEREBRAL PLASTICITY FOR DISCOURSE COMPREHENSION IN AGING.

Author

Martin, Charles-Olivier, Desrochers, Marianne, Demers, Catrine, Scherer, Lilian Cristine, and Ska, Bernadette

Subjects

PSYCHOLOGY of reading, BOOKS & reading, NEUROPLASTICITY, DISCOURSE, PSYCHOLOGICAL aspects of aging, PREFRONTAL cortex

Abstract

The goal of this study was to evaluate the influence of reading habits on cerebral plasticity in the performance of a discourse comprehension task in aging. he main hypothesis was that participants with higher frequency and quality of reading habits should exhibit reduced brain activity because the task should be easier for them. two groups of native French speakers, 16 young adults and 16 elderly adults, participated in a task using the NIRS (near-infrared spectroscopy) technique. hey read short stories and answered true or false probes after each one. hey also completed a questionnaire about their previous reading habits. he results show that the more experienced readers had higher activation in the superior let region of the prefrontal cortex while they were reading the stories but lower activation in the same region when they were retrieving the information to answer the probe. Thus, more effort is required to acquire and maintain the information needed to answer, and this effort makes it easier to give the answer. These results reinforce the hypothesis that brain plasticity is promoted by cognitive activities throughout the lifespan. [ABSTRACT FROM AUTHOR]

Published

2012