36 results on '"Booij, Linda"'
Search Results
2. Childhood exposure to pyrethroids and neurodevelopment in Canadian preschoolers
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Ntantu Nkinsa, Patrick, Fisher, Mandy, Muckle, Gina, Guay, Mireille, Arbuckle, Tye E., Fraser, William D., Boylan, Khrista, Booij, Linda, Walker, Mark, and Bouchard, Maryse F.
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- 2023
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3. Descriptive analysis of organophosphate ester metabolites in a pan-Canadian pregnancy cohort
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Ashley-Martin, Jillian, MacPherson, Susan, Zhao, Zhao, Gaudreau, Éric, Provencher, Gilles, Fisher, Mandy, Borghese, Michael M., Bouchard, Maryse F., Booij, Linda, and Arbuckle, Tye E.
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- 2023
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4. Emotional facial expression recognition and depression in adolescent girls: Associations with clinical features
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Porter-Vignola, Elyse, Booij, Linda, Bossé-Chartier, Gabrielle, Garel, Patricia, and Herba, Catherine M.
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- 2021
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5. DNA methylation differences in stress-related genes, functional connectivity and gray matter volume in depressed and healthy adolescents
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Chiarella, Julian, Schumann, Lyndall, Pomares, Florence B, Frodl, Thomas, Tozzi, Leonardo, Nemoda, Zsofia, Yu, Patricia, Szyf, Moshe, Khalid-Khan, Sarosh, and Booij, Linda
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- 2020
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6. Functional connectivity across social inclusion and exclusion is related to peer victimization and depressive symptoms in young adults
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McIver, Theresa A., Bosma, Rachael L., Goegan, Sarah, Sandre, Aislinn, Klassen, Janell, Chiarella, Julian, Booij, Linda, and Craig, Wendy
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- 2019
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7. DNA methylation differences at the glucocorticoid receptor gene in depression are related to functional alterations in hypothalamic–pituitary–adrenal axis activity and to early life emotional abuse
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Farrell, Chloё, Doolin, Kelly, O’ Leary, Niamh, Jairaj, Chaitra, Roddy, Darren, Tozzi, Leonardo, Morris, Derek, Harkin, Andrew, Frodl, Thomas, Nemoda, Zsófia, Szyf, Moshe, Booij, Linda, and O'Keane, Veronica
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- 2018
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8. Serotonin transporter gene promoter methylation in peripheral cells in healthy adults: Neural correlates and tissue specificity
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Ismaylova, Elmira, Di Sante, Jessica, Szyf, Moshe, Nemoda, Zsofia, Yu, Wei-Jo, Pomares, Florence B., Turecki, Gustavo, Gobbi, Gabriella, Vitaro, Frank, Tremblay, Richard E., and Booij, Linda
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- 2017
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9. DNA methylation as a mediator in the association between prenatal maternal stress and child mental health outcomes: Current state of knowledge.
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Azar, Naomi and Booij, Linda
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DNA methylation , *PSYCHOLOGICAL stress , *CHILDREN'S health , *MENTAL health , *DATA libraries , *PRENATAL influences , *BEGOMOVIRUSES , *VITAMINS , *PSYCHOLOGY of mothers , *PRENATAL exposure delayed effects , *QUESTIONNAIRES - Abstract
Background: Prenatal maternal stress is increasingly recognized as a risk factor for offspring mental health challenges. DNA methylation may be a mechanism, but few studies directly tested mediation. These few integrative studies are reviewed along with studies from three research areas: prenatal maternal stress and child mental health, prenatal maternal stress and child DNA methylation, and child mental health and DNA methylation.Methods: We conducted a narrative review of articles in each research area and the few published integrative studies to evaluate the state of knowledge.Results: Prenatal maternal stress was related to greater offspring internalizing and externalizing symptoms and to greater offspring peripheral DNA methylation of the NR3C1 gene. Youth mental health problems were also related to NR3C1 hypermethylation while epigenome-wide studies identified genes involved in nervous system development. Integrative studies focused on infant outcomes and did not detect significant mediation by DNA methylation though methodological considerations may partially explain these null results.Limitations: Operationalization of prenatal maternal stress and child mental health varied greatly. The few published integrative studies did not report conclusive evidence of mediation by DNA methylation.Conclusions: DNA methylation likely mediates the association between prenatal maternal stress and child mental health. This conclusion still needs to be tested in a larger number of integrative studies. Key empirical and statistical considerations for future research are discussed. Understanding the consequences of prenatal maternal stress and its pathways of influence will help prevention and intervention efforts and ultimately promote well-being for both mothers and children. [ABSTRACT FROM AUTHOR]- Published
- 2022
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10. Maternal pregnancy diet, postnatal home environment and executive function and behavior in 3- to 4-y-olds.
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Mortaji, Neda, Krzeczkowski, John E, Boylan, Khrista, Booij, Linda, Perreault, Maude, and Van Lieshout, Ryan J
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HOME environment ,EXECUTIVE function ,MOTHERS ,CONFIDENCE intervals ,CHILD development ,DIET ,NUTRITIONAL requirements ,COGNITION ,PUERPERIUM ,QUESTIONNAIRES ,PREGNANCY - Abstract
Background Optimal maternal nutrition during pregnancy has been linked to better cognitive and behavioral development in children. However, its influence on the effects of suboptimal postnatal exposures like reduced stimulation and support in the home is not known. Objectives To examine the effect of maternal pregnancy diet on executive function and/or behavioral development in children raised in suboptimal home environments. Methods Data were provided by 808 mother–infant dyads from the Canadian Maternal-Infant Research on Environmental Chemicals–Child Development study. Maternal pregnancy diet was self-reported using the Healthy Eating Index 2010 questionnaire. Stimulation and support in the home was assessed using the Home Observation for Measurement of the Environment (HOME) when children were 3–4 y old. Child executive function was reported by mothers at this age using the Behavior Rating Inventory of Executive Functioning–Preschool Edition, and child behavior was assessed using the Behavior Assessment System for Children–2nd Edition. We examined the interaction of maternal pregnancy diet and postnatal HOME scores on child executive function and behavior using linear regression adjusted for maternal education, postpartum depression, prepregnancy BMI, and smoking. Results Maternal pregnancy diet was associated with an increasingly positive association with child working memory (β: 0.21; 95% CI: 0.82, 3.41; P = 0.001), planning (β: 0.17; 95% CI: 0.38, 2.84; P = 0.007), and adaptability (β: –0.13; 95% CI: –1.72, –0.08; P = 0.032) as levels of postnatal stimulation decreased. Conclusions The positive association of maternal pregnancy diet quality and executive function and adaptability in 3- to 4-y-olds appeared to increase with decreasing levels of postnatal stimulation and support. These results suggest that overall maternal pregnancy diet could be linked to better child neurodevelopment in families experiencing barriers to providing stimulation and support to children in their home. [ABSTRACT FROM AUTHOR]
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- 2021
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11. M51 - DOES IT MATTER WHICH CELLS WE USE IN DNA METHYLATION ANALYSES OF GLUCOCORTICOID SIGNALING GENES?
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Nemoda, Zsofia, Yu, Wei-Jo, Di Sante, Jessica, Suderman, Matthew, Kruk, Emese, Fazekas, Kata, Unoka, Zsolt, Tremblay, Richard Ernest, Szyf, Moshe, and Booij, Linda
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- 2019
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12. Perinatal effects on in vivo measures of human brain serotonin synthesis in adulthood: A 27-year longitudinal study
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Booij, Linda, Benkelfat, Chawki, Leyton, Marco, Vitaro, Frank, Gravel, Paul, Lévesque, Mélissa L., Arseneault, Louise, Diksic, Mirko, and Tremblay, Richard E.
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- 2012
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13. Altered patterns of brain activity during transient sadness in children at familial risk for major depression
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Lévesque, Mélissa L., Beauregard, Mario, Ottenhof, Koen W., Fortier, Émilie, Tremblay, Richard E., Brendgen, Mara, Pérusse, Daniel, Dionne, Ginette, Robaey, Philippe, Vitaro, Frank, Boivin, Michel, and Booij, Linda
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- 2011
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14. Emotional processing as a predictor of symptom change: An acute tryptophan depletion study in depressed patients
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Booij, Linda and Van der Does, A.J. Willem
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- 2011
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15. Social cognition and depression in adolescent girls.
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Porter-Vignola, Elyse, Booij, Linda, Dansereau-Laberge, Ève Marie, Garel, Patricia, Bossé Chartier, Gabrielle, Seni, Anne G., Beauchamp, Miriam H., and Herba, Catherine M.
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Background and Objectives: Depression has been associated with alterations in social functioning. Decoding and understanding others' mental states and adaptive reasoning are important for social functioning. This study examined theory of mind (ToM) and socio-moral reasoning (SMR) in adolescent girls with and without depression. Within the depression group, we examined associations between relevant clinical features (depression severity, anxiety symptoms and borderline personality traits) and ToM and SMR.Methods: A cross-sectional study was conducted, whereby 43 adolescent girls (mean age = 16.19, SD = 1.24) meeting full or subthreshold criteria for depression and 40 adolescent girls (mean age = 15.44, SD = 1.24) with no psychiatric diagnosis were recruited. ToM was assessed using the Movie for the Assessment of Social Cognition; SMR was evaluated via the Socio-Moral Reasoning Aptitude Level task.Results: Analyses of covariance indicated that adolescents with depression did not differ from controls in ToM abilities but showed lower socio-maturity scores on the SMR task. This difference disappeared after controlling for the number of words used to justify responses. Amongst adolescents with depression, multiple linear regression analyses revealed that higher levels of borderline personality traits were associated with lower levels of mentalization (ToM task), and more severe depressive symptoms were associated with lower socio-moral maturity stages (SMR task) LIMITATIONS: Directional associations were not studied, and the sample included only girls.Conclusions: Findings may help to explain clinical heterogeneity in social cognitive functioning observed in individuals with depression. [ABSTRACT FROM AUTHOR]- Published
- 2022
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16. Genetic and environmental contributions to saliva testosterone levels in male and female infant twins
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Caramaschi, Doretta, Booij, Linda, Petitclerc, Amélie, Boivin, Michel, and Tremblay, Richard E.
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TESTOSTERONE , *MALE reproductive organs , *SOCIAL dominance , *HERITABILITY , *TWINS , *HUMAN sexuality , *HEALTH - Abstract
Summary: Background: Testosterone is the key hormone for the development of male reproductive organs and secondary sexual characteristics. In addition, testosterone is associated with behavioural traits, including sexual behaviour and social dominance. The level of circulating testosterone in the human body is determined by genetic and environmental factors. Twin studies have shown moderate to high heritability in adolescence and adulthood, but heritability in early childhood has not been investigated. This study aimed at disentangling the genetic and environmental contributions to testosterone levels soon after birth. Methods: Using a sample of 314 twin pairs, saliva testosterone levels were measured at 5 months after birth. Quantitative genetic modelling was used to assess genetic and environmental contributions to the variation in testosterone levels. Results: Variation in testosterone levels was explained by common (56.6%) and unique (43.4%) environmental factors. Conclusions: Taken together, these data from the largest study of twin testosterone levels suggest that, in contrast to findings in adulthood, environmental factors determine the interindividual variability in testosterone levels in early infancy. This may have consequences for the development of sex-related behaviour during childhood and calls for studies designed to unravel specific genetic and environmental factors involved in this process. [ABSTRACT FROM AUTHOR]
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- 2012
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17. Poster #24 FROM LAB TO LIFE: PREFRONTAL DOPAMINERGIC HYPOREACTIVITY TO PSYCHOSOCIAL STRESS PREDICTS PSYCHOTIC EXPERIENCES IN RESPONSE TO DAILY LIFE STRESS IN INDIVIDUALS WITH A FAMILIAL RISK OF PSYCHOSIS
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Hernaus, Dennis, Lataster, lohan, Collip, Dina, Ceccarini, Jenny, Booij, Linda, van Os, Jim, Pruessner, Jens, van Laere, Koen, and Myin-Germeys, Inez
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- 2012
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18. Tryptophan Depletion Affects Heart Rate Variability and Impulsivity in Remitted Depressed Patients with a History of Suicidal Ideation
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Booij, Linda, Swenne, Cees A., Brosschot, Jos F., Haffmans, P.M. Judith, Thayer, Julian F., and Van der Does, A.J. Willem
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MENTAL depression , *CARDIOVASCULAR diseases , *DISEASE risk factors , *HEART beat , *TRYPTOPHAN - Abstract
Background: Depression is a major risk factor for cardiovascular disease. An important risk factor for cardiovascular disease, low heart rate variability, often has been found in depressed patients and has been associated with impulsivity. The present study investigated whether experimental lowering of serotonin would decrease heart rate variability and increase impulsivity in remitted depressed patients, in particular in those patients with disturbed impulse control. Methods: Nineteen patients in remission from depression received high-dose and low-dose acute tryptophan depletion in a randomized, counterbalanced, double-blind crossover design. Heart rate variability and impulsivity were assessed during each acute tryptophan depletion session and during a baseline session. Suicidal ideation during past depression was used as an index for individual differences in impulse control. Results: High-dose acute tryptophan depletion led to a larger increase in depressive symptoms than did low-dose acute tryptophan depletion. High-dose acute tryptophan depletion decreased heart rate variability and increased impulsivity and anxiety, but only in patients with a history of suicidal ideation. Symptom effects of high-dose acute tryptophan depletion correlated with low heart rate variability at baseline. Conclusions: Depressed patients who have problems with controlling impulsivity might be more at risk for developing cardiovascular disease, possibly related to increased vulnerability to impaired 5-hydroxytryptamine function. [Copyright &y& Elsevier]
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- 2006
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19. Acute tryptophan depletion in depressed patients treated with a selective serotonin–noradrenalin reuptake inhibitor: Augmentation of antidepressant response?
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Booij, Linda, Van der Does, A.J. Willem, Haffmans, P.M. Judith, and Riedel, Wim J.
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AMINO acids , *SEROTONIN , *NEUROTRANSMITTERS , *NEURAL transmission - Abstract
Abstract: Background: It has frequently been demonstrated that experimental lowering of serotonin (5-HT) neurotransmission by acute tryptophan depletion (ATD) induces a transient depressed mood in 50–60% of patients treated with a selective serotonin reuptake inhibitor (SSRI) who are in remission from depression. In unmedicated depressed patients, ATD has no immediate effect on symptoms. The effects in currently depressed medicated patients have not been investigated. Methods: Fourteen currently depressed patients (seven patients treated with a selective serotonin–noradrenalin reuptake inhibitor (SSNRI); seven other treatment, non-SSNRI) received ATD in a double-blind, crossover design. Different strengths of the ATD mixture (aimed at 50% and 90% reduction of tryptophan) were used on separate days. Psychiatric symptoms were assessed at both sessions prior to, at +6.5 h, and at +24 h after ATD. Results: The ATD mixtures induced the expected reductions of plasma tryptophan levels. Full but not partial depletion improved mood and other psychiatric symptoms at +24 h in patients who received SSNRI treatment, as indicated by clinical ratings and self-report. Subjective sleep quality also improved. Conclusions: The effects of ATD on psychiatric symptoms in currently depressed patients are remarkably different from the results in recently remitted SSRI-treated patients. ATD in currently depressed patients treated with serotonergic antidepressants possibly provides important information about the mechanism of action of SSRIs. [Copyright &y& Elsevier]
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- 2005
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20. Prenatal exposure to polybrominated diphenyl ethers (PBDEs) and cognitive ability in early childhood.
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Azar, Naomi, Booij, Linda, Muckle, Gina, Arbuckle, Tye E., Séguin, Jean R., Asztalos, Elizabeth, Fraser, William D., Lanphear, Bruce P., and Bouchard, Maryse F.
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POLYBROMINATED diphenyl ethers , *COGNITIVE ability , *NEURAL development - Abstract
• Prenatal PBDE exposure can interfere with children's neurodevelopment. • PBDE blood concentrations in Canada are less than half those in the U.S.A. • We measured PBDEs in maternal blood and assessed IQ for 592 3-year-old children. • Prenatal PBDE exposure was related to lower IQ scores, but only among boys. • It suggests sex-specific neurotoxicity at the low PDBE levels in Canada. Prenatal exposure to polybrominated diphenyl ethers (PBDEs) has been associated with adverse neurodevelopmental outcomes in children, but evidence remains mixed regarding sex differences in this association. To examine the prospective association between prenatal PBDE exposure and cognitive ability in young children, as well as potential sex differences. The study was conducted in a multi-site Canadian pregnancy cohort recruited in 2008–11. PBDEs were measured in maternal plasma samples collected early in pregnancy. Cognitive ability was assessed using the Wechsler Preschool and Primary Scale of Intelligence (WPPSI-III) in children at age 3 years (mean = 3.4). Multiple linear regression was used to analyze the association between maternal PBDE plasma concentrations (lipid-standardized and log10-transformed) and Verbal, Performance, and Full Scale IQ scores on the whole sample and stratified by sex, adjusting for confounders. The sample was composed of 592 children (291 boys and 301 girls). A tenfold increase in maternal blood PBDE concentration (sum of BDE-47, −99, −100, and −153) was associated with lower Full Scale scores in boys (−3.4 points; 95% CI: −7.0, 0.1), after adjusting for confounders. BDE-47 was the congener with the highest concentrations in maternal blood and a tenfold increase in exposure was associated with significantly lower Full Scale IQ scores in boys (−4.4 points; 95% CI: −7.9, −0.9), after adjusting for confounders. Verbal and Performance IQ scores were similarly associated with PBDE exposure. Maternal blood PBDE concentrations were not associated with IQ scores in girls. Prenatal exposure to background levels of PBDEs, especially BDE-47, was associated with lower IQ scores in boys, but not in girls. Our results support that exposure to PBDEs during early development may be sex-dependent and detrimental to a child's neurodevelopmental trajectory. [ABSTRACT FROM AUTHOR]
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- 2021
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21. Cognitive Therapy Does Not Prevent a Response to Tryptophan Depletion in Patients also Treated with Antidepressants
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Van der Does, A.J. Willem and Booij, Linda
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TRYPTOPHAN , *PATIENTS , *SEROTONINERGIC mechanisms , *DEPRESSED persons , *NORADRENERGIC mechanisms - Abstract
Background: Acute tryptophan depletion (ATD) induces depressive symptoms in remitted depressed patients treated with serotonergic medications, but not in patients treated with noradrenergic medications or electroconvulsive therapy. A recent study suggests that cognitive therapy (CT) protects against the effects of ATD, but the evidence is questionable. The present study compared the effect of ATD in patients who were treated with antidepressant medication and CT (n = 17) versus antidepressant medication alone (n = 23) during their latest episode. Methods: Forty remitted depressed patients underwent high-dose and low-dose ATD in a randomized double-blind crossover design. Results: There were no differences in response to ATD between treatment groups. This applied to groups defined by lifetime and by recent CT experience. Conclusions: Cognitive therapy does not protect against the effects of rapidly lowered plasma tryptophan levels in remitted depressed patients who are also treated with antidepressant medication. [Copyright &y& Elsevier]
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- 2005
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22. Peripheral DNA methylation of HPA axis-related genes in humans: Cross-tissue convergence, two-year stability and behavioural and neural correlates.
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Di Sante, Jessica, Ismaylova, Elmira, Booij, Linda, Yu, Wei-Jo, Vitaro, Frank, Tremblay, Richard E., Gouin, Jean-Philippe, Caldwell, Warren, Szyf, Moshe, and Nemoda, Zsofia
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BRAIN imaging , *DNA methylation , *HYPOTHALAMIC-pituitary-adrenal axis , *GLUCOCORTICOID receptors , *CARRIER proteins , *PHYSIOLOGICAL stress - Abstract
Highlights • Daily life stress is associated with HPA-axis related gene methylation. • DNA methylation in HPA-axis genes is stable over time in healthy volunteers. • DNA methylation-brain associations are gene and tissue specific. • Measuring methylation in different tissues in the same persons can be recommended. Abstract Environmental factors can influence gene expression via epigenetic modifications such as DNA methylation. DNA methylation levels of regulatory regions in Hypothalamo-Pituitary-Adrenal (HPA) axis-related genes assessed from brain tissues as well as from surrogate, peripheral tissues have been associated with vulnerability to stress-related psychopathologies. Commonly used peripheral samples to assess DNA methylation in living humans are derived from blood, saliva or buccal cells. Although psychiatric epigenetic studies are increasingly relying on peripheral measures of DNA methylation, it is still unknown to what extent methylation patterns across peripheral tissues are associated with each other and with measures of brain processes and behavioural stress. In the present study, with a sample of 51 healthy adults, we assessed cross-tissue correlations of DNA methylation patterns in the glucocorticoid receptor (NR3C1) 1 F promoter and the FK506 Binding Protein 5 (FKBP5) gene intron 7 region using saliva and buccal cell samples, and assessed two-year stability in both tissues in a male subsample (N = 14). We also investigated associations between peripherally-derived DNA methylation and measures of neural function and perceived daily stress, and compared the extent of these associations across tissue samples. DNA methylation cross-tissue correlations were highly significant for FKBP5 , but not significant for NR3C1. DNA methylation in both genes remained stable for two years. Tissue- and gene-specific associations were found for brain resting state connectivity and neural responses to sadness, thereby suggesting that saliva- and buccal cell-derived DNA methylation levels of NR3C1 -1 F and FKBP5 gene regions might differently capture different measures of putatively related brain processes. It was also found that greater buccal cell- (but not saliva-) derived NR3C1 -1 F methylation was associated with lower perceived daily life demands. Results of the present study may inform the design of future epigenetic studies on FKBP5 -intron-7 and NR3C1 -1 F-promoter methylation in relation to neuro-imaging and behavioural measures, and provide insight for the development of peripheral DNA methylation correlates of stress sensitivity and resilience. [ABSTRACT FROM AUTHOR]
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- 2018
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23. Major depressive disorder and anxiety disorders from the glial perspective: Etiological mechanisms, intervention and monitoring.
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Sild, Mari, Ruthazer, Edward S., and Booij, Linda
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MENTAL depression , *ANXIETY disorders , *BRAIN imaging , *NEUROGLIA , *CENTRAL nervous system diseases , *DISEASES , *DIAGNOSIS - Abstract
Despite intense ongoing research efforts, the etiology of psychiatric disorders remains incompletely understood. Among biological factors playing a role in Major Depressive Disorder (MDD) and Anxiety Disorders (ANX), emerging evidence points to the relevance of different types of glia cells and efficient neuron-glia interactions. Here, we review recent findings highlighting the involvement of central nervous system (CNS) glia in MDD and ANX etiology and treatment response. Additionally, several relatively underexplored topics will be discussed: (1) glial response to non-pharmacological therapies, (2) impact of early life adversity on glia, (3) influence of lifestyle factors on glia in the context of MDD and ANX, and (4) monitoring glial functions in patients. It can be concluded that despite the sequence of events is still unclear, alterations in glial cell types are common and somewhat overlapping in ANX, MDD and corresponding animal models. Furthermore, glia are responsive to a variety of treatment and lifestyle options. Looking forward, new research developments can lead to novel types of therapeutic or symptom-relieving approaches targeting glia. [ABSTRACT FROM AUTHOR]
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- 2017
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24. Adversity in early adolescence promotes an enduring anxious phenotype and increases serotonergic innervation of the infralimbic medial prefrontal cortex.
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Tao, Cindy S., Dhamija, Prateek, Booij, Linda, and Menard, Janet L.
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SEROTONINERGIC mechanisms , *INNERVATION , *PHENOTYPES , *ADOLESCENT psychology , *IMMUNOHISTOCHEMISTRY , *HIPPOCAMPUS (Brain) - Abstract
Stress during early development produces lasting effects on psychopathological outcomes. We analysed the impact of prior intermittent, physical stress (IPS) during early adolescence (PD 22–33) on anxiety-like behaviour of female rats in adulthood. After behavioural testing, we used immunohistochemistry for the 5-HT transporter (SERT) to evaluate 5-HT innervation profiles in the medial prefrontal cortex (mPFC) and ventral hippocampus (VH). Administration of IPS (i.e., water immersion, elevated platform, foot shock) in early adolescence increased rats’ anxiety-like behaviour in the elevated plus-maze but had no effects in the shock-probe burying test. In the social interaction test, IPS decreased social interaction, and this effect was driven by selective decreases in the frequency of playfighting with no evident changes in contact and investigative behaviours. Selective stress-induced increases in the density of SERT- ir positive fibres were found in the infralimbic (IL) subregion of the mPFC but not in the cingulate or prelimbic (PL) subregions. IPS in early adolescence did not affect 5-HT innervation profiles in any sub-fields of the VH. Our findings confirm and extend on earlier evidence that stress during early adolescence promotes the emergence of an anxious phenotype and provide novel evidence that these effects are associated with increased 5-HT innervation of the IL mPFC. [ABSTRACT FROM AUTHOR]
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- 2017
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25. Prazosin for treating sleep disturbances in adults with posttraumatic stress disorder: a systematic review and meta-analysis of randomized controlled trials.
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Khachatryan, Davit, Groll, Dianne, Booij, Linda, Sepehry, Amir A., and Schütz, Christian G.
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PREVENTION of post-traumatic stress disorder , *PRAZOSIN , *CONFIDENCE intervals , *DREAMS , *META-analysis , *PLACEBOS , *POST-traumatic stress disorder , *SLEEP disorders , *SYSTEMATIC reviews , *RANDOMIZED controlled trials , *BLIND experiment , *DESCRIPTIVE statistics , *THERAPEUTICS - Abstract
Objective Posttraumatic stress disorder (PTSD) is a disorder with significant sleep morbidity and limited treatment options. Prazosin may constitute a novel management approach and has been tested recently in a number of trials. We conducted a meta-analysis to examine the effectiveness of prazosin for nightmares and other sleep disturbances in adults with PTSD. Method A systematic review of databases for randomized, double-blind, placebo-controlled trials of adults diagnosed with PTSD and reporting sleep disturbances that were treated with prazosin was conducted in January 2015. No limitations were placed on language or year of publication. Results Six randomized controlled trials of prazosin for sleep disturbances in patients with PTSD were included (sample n = 240). We found that prazosin was statistically significantly more effective than placebo in improving sleep quality [ g = 0.987, 95% confidence interval (CI): 0.324–1.651] and in reducing overall PTSD symptoms ( g = 0.699, 95% CI: 0.139–1.260) and sleep disturbances in particular ( g = 0.799, 95% CI: 0.391–1.234). Conclusions Prazosin showed medium-to-large and statistically significant effects on PTSD symptoms in general and sleep disturbances in particular. While promising, results should be interpreted with caution given the limited total number of participants and the limitations induced by the majority of participants being male and noncivilian. [ABSTRACT FROM AUTHOR]
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- 2016
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26. Is subthreshold depression in adolescence clinically relevant?
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Noyes, Blake K., Munoz, Douglas P., Khalid-Khan, Sarosh, Brietzke, Elisa, and Booij, Linda
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DEPRESSION in adolescence , *MENTAL depression , *MEDICAL care use , *BRAIN anatomy , *DISEASE progression , *SUICIDE risk factors , *THRESHOLD (Perception) , *DIAGNOSIS of mental depression , *SYSTEMATIC reviews , *LITERATURE reviews , *COMORBIDITY - Abstract
Background: Subthreshold depression is highly prevalent in adolescence, but compared to major depressive disorder, the clinical impact is under-researched. The aim of this review was to compare subthreshold depression and major depressive disorder in adolescents by reviewing available literature on epidemiology, risk factors, illness trajectories, brain anatomy and function, genetics, and treatment response.Methods: We conducted a scoping review of papers on subthreshold depression and major depressive disorder in adolescence published in English. Studies in adults were included when research in adolescence was not available.Results: We found that individuals with subthreshold depression were similar to individuals with major depressive disorder in several regards, including female/male ratio, onset, functional impairment, comorbidity, health care utilization, suicidal ideation, genetic predisposition, brain alterations, and treatment response. Further, subthreshold depression was about two times more common than major depressive disorder.Limitations: The definition of subthreshold depression is highly variable across studies. Adolescent-specific data are limited in the areas of neurobiology and treatment.Conclusions: The findings of the current review support the idea that subthreshold depression is of clinical importance and provide evidence for a spectrum, versus categorical model, for depressive symptomatology. Given the frequency of subthreshold depression escalating to major depressive disorder, a greater recognition and awareness of the significance of subthreshold depression in research, clinical practice and policy-making may facilitate the development and application of early prevention and intervention. [ABSTRACT FROM AUTHOR]- Published
- 2022
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27. Inclusion of currently diagnosed or treated individuals in studies of depression screening tool accuracy: a meta-research review of studies published in 2018-2021.
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Nassar, Elsa-Lynn, Levis, Brooke, Rice, Danielle B., Booij, Linda, Benedetti, Andrea, and Thombs, Brett D.
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PREVENTION of mental depression , *DIAGNOSIS of mental depression , *CONFIDENCE intervals , *SYSTEMATIC reviews , *MEDICAL screening , *MENTAL depression - Abstract
Screening is done to improve health outcomes by identifying and effectively treating individuals with unrecognized conditions. Depression screening has been proposed to identify previously unrecognized depression cases. Including individuals already diagnosed or treated for depression in screening test accuracy studies could exaggerate accuracy and the yield of new cases from screening. The present study investigated (1) the proportion of depression screening tool accuracy primary studies published in 2018–2021 that excluded individuals with a confirmed depression diagnosis or who were already undergoing treatment; and (2) whether this has improved since the last review of studies published in 2013–2015, which found that five of 89 (5.6%) primary studies appropriately excluded such individuals. MEDLINE was searched from January 1, 2018 through May 21, 2021 for primary studies on depression screening tool accuracy. Eighteen of 106 (17.0%; 95% Confidence Interval [CI], 11.0% to 25.3%) primary studies excluded currently diagnosed or treated individuals. This was 11.4% (95% CI, 2.8% to 20.0%) greater than in similar studies published in 2013–2015. There has been an improvement since 2015, but the proportion of studies that exclude individuals already known to have depression remains low. This may bias research findings intended to inform clinical practice. [ABSTRACT FROM AUTHOR]
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- 2022
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28. Methodological and clinical challenges associated with biomarkers for psychiatric disease: A scoping review.
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Kirkpatrick, Ryan H., Munoz, Douglas P., Khalid-Khan, Sarosh, and Booij, Linda
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MENTAL illness , *BIOMARKERS , *PATHOLOGY , *MEDICAL specialties & specialists ,PSYCHIATRIC research - Abstract
Over the past decade, psychiatric research has been on an important hunt for biomarkers of psychiatric disease. In psychiatry, the term "biomarker" is a broad umbrella term used to identify any biological variable that can be objectively measured and applied to a diagnosis; this includes genetic and epigenetic assessments, hormone levels, measures of neuro-anatomy and many other scientific modalities. However, despite hundreds of studies on the topic being published yearly and other medical specialties having success in discovering biomarkers, clinical psychiatric practice has not had the same success. This paper aims to consolidate the many opinions on the search for psychiatric biomarkers to suggest key methodological and clinical challenges that psychiatric biomarker research faces. Psychiatry as a specialty has many fundamental differences compared to other medical specialties in methods of diagnosing, underlying etiology and disease pathologies that may be limiting the success of biomarker research in itself and puts strict requirements on the research being conducted. The academic and clinical environment in which the research is being conducted also heavily influences the translation of the findings. Finally, once biomarkers are identified, more often than not they are inapplicable to clinical settings, unable to integrate into clinical practice and fail to outperform current diagnostic practices and guidelines. We also make six recommendations for more promising future research in psychiatric biomarkers. • For biomarker research to be successful, multiple techniques must be combined. • There are intricacies unique to psychiatry that make successful biomarker identification difficult. • Improved research methodologies that are easily combined are needed. • Multidisciplinary teams should be involved at all stages of biomarker research. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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29. The neuroscience of sadness: A multidisciplinary synthesis and collaborative review.
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Arias, Juan A., Williams, Claire, Raghvani, Rashmi, Aghajani, Moji, Baez, Sandra, Belzung, Catherine, Booij, Linda, Busatto, Geraldo, Chiarella, Julian, Fu, Cynthia HY, Ibanez, Agustin, Liddell, Belinda J., Lowe, Leroy, Penninx, Brenda W.J.H., Rosa, Pedro, and Kemp, Andrew H.
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SADNESS , *WALKING speed , *PREFRONTAL cortex , *RESPONSE inhibition , *NEUROSCIENCES , *AFFECTIVE disorders - Abstract
• Sadness involves reduction of cortical control over evolutionarily ancient brain systems. • Basic emotion theorists have identified a SADNESS circuit, based on animal research. • Psychological constructionists have identified patterns of activity that dependent on context. • Competing models may relate to different levels on a phylogenetic hierarchy. • Dedicated funding to facilitate collaborative and transdisciplinary opportunities is needed. Sadness is typically characterized by raised inner eyebrows, lowered corners of the mouth, reduced walking speed, and slumped posture. Ancient subcortical circuitry provides a neuroanatomical foundation, extending from dorsal periaqueductal grey to subgenual anterior cingulate, the latter of which is now a treatment target in disorders of sadness. Electrophysiological studies further emphasize a role for reduced left relative to right frontal asymmetry in sadness, underpinning interest in the transcranial stimulation of left dorsolateral prefrontal cortex as an antidepressant target. Neuroimaging studies – including meta-analyses – indicate that sadness is associated with reduced cortical activation, which may contribute to reduced parasympathetic inhibitory control over medullary cardioacceleratory circuits. Reduced cardiac control may – in part – contribute to epidemiological reports of reduced life expectancy in affective disorders, effects equivalent to heavy smoking. We suggest that the field may be moving toward a theoretical consensus, in which different models relating to basic emotion theory and psychological constructionism may be considered as complementary, working at different levels of the phylogenetic hierarchy. [ABSTRACT FROM AUTHOR]
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- 2020
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30. TPH2 polymorphisms across the spectrum of psychiatric morbidity: A systematic review and meta-analysis.
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Ottenhof, Koen Willem, Sild, Mari, Lévesque, Mélissa Luce, Ruhé, Henricus Gerardus, and Booij, Linda
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TRYPTOPHAN hydroxylase , *SEROTONIN , *PATHOLOGICAL psychology , *AFFECTIVE disorders , *META-analysis , *SYSTEMATIC reviews - Abstract
Tryptophan hydroxylase 2 (TPH2) is the rate-limiting enzyme in brain serotonin synthesis. The TPH2 gene has frequently been investigated in relation to psychiatric morbidity. The aim of the present review is to integrate results from association studies between TPH2 single nucleotide polymorphisms (SNPs) and various psychiatric disorders, which we furthermore quantified with meta-analysis. We reviewed 166 studies investigating 69 TPH2 SNPs in a broad range of psychiatric disorders, including over 30,000 patients. According to our meta-analysis, TPH2 polymorphisms show strongest associations with mood disorders, suicide (attempt) and schizophrenia. Despite small effect sizes, we conclude that TPH2 SNPs in the coding and non-coding areas (rs4570625, rs11178997, rs11178998, rs10748185, rs1843809, rs4290270, rs17110747) are each associated with one or more psychopathological conditions. Our findings highlight the possible common serotonergic mechanisms of the investigated psychiatric disorders. Yet, the functional relevance of most TPH2 polymorphisms is unclear. Characterizing how exactly the different TPH2 variants influence the serotonergic neurotransmission is a next necessary step in understanding the psychiatric disorders where serotonin is implicated. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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31. Dehydroepiandrosterone impacts working memory by shaping cortico-hippocampal structural covariance during development.
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Nguyen, Tuong-Vi, Wu, Mia, Lew, Jimin, Albaugh, Matthew D, Botteron, Kelly N, Hudziak, James J, Fonov, Vladimir S, Collins, D. Louis, Campbell, Benjamin C, Booij, Linda, Herba, Catherine, Monnier, Patricia, Ducharme, Simon, and McCracken, James T
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DEHYDROEPIANDROSTERONE , *ADRENOCORTICAL hormones , *SHORT-term memory , *NEURAL development , *DEVELOPMENTAL neurobiology - Abstract
Existing studies suggest that dehydroepiandrosterone (DHEA) may be important for human brain development and cognition. For example, molecular studies have hinted at the critical role of DHEA in enhancing brain plasticity. Studies of human brain development also support the notion that DHEA is involved in preserving cortical plasticity. Further, some, though not all, studies show that DHEA administration may lead to improvements in working memory in adults. Yet these findings remain limited by an incomplete understanding of the specific neuroanatomical mechanisms through which DHEA may impact the CNS during development. Here we examined associations between DHEA, cortico-hippocampal structural covariance, and working memory (216 participants [female=123], age range 6–22 years old, mean age: 13.6 +/−3.6 years, each followed for a maximum of 3 visits over the course of 4 years). In addition to administering performance-based, spatial working memory tests to these children, we also collected ecological, parent ratings of working memory in everyday situations. We found that increasingly higher DHEA levels were associated with a shift toward positive insular-hippocampal and occipito-hippocampal structural covariance. In turn, DHEA-related insular-hippocampal covariance was associated with lower spatial working memory but higher overall working memory as measured by the ecological parent ratings. Taken together with previous research, these results support the hypothesis that DHEA may optimize cortical functions related to general attentional and working memory processes, but impair the development of bottom-up, hippocampal-to-cortical connections, resulting in impaired encoding of spatial cues. [ABSTRACT FROM AUTHOR]
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- 2017
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32. Prenatal exposure to legacy PFAS and neurodevelopment in preschool-aged Canadian children: The MIREC cohort.
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Goodman, Carly V., Till, Christine, Green, Rivka, El-Sabbagh, Jana, Arbuckle, Tye E., Hornung, Richard, Lanphear, Bruce, Seguin, Jean R., Booij, Linda, Fisher, Mandy, Muckle, Gina, Bouchard, Maryse F., and Ashley-Martin, Jillian
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PRENATAL exposure , *EXECUTIVE function , *FLUOROALKYL compounds , *PERFLUOROOCTANOIC acid , *PERFLUOROOCTANE sulfonate , *NEURAL development , *CHILD development , *PERFORMANCE in children - Abstract
Exposure to perfluoroalkyl substances (PFAS) has been shown to be neurotoxic in experimental studies, but epidemiological evidence linking prenatal PFAS exposure to child neurodevelopment is equivocal and scarce. To quantify associations between prenatal exposure to legacy PFAS and children's intelligence (IQ) and executive functioning (EF) in a Canadian pregnancy and birth cohort and to determine if these associations differ by child sex. We measured first-trimester plasma concentrations of perfluorooctanoic acid (PFOA), perfluorooctanesulfonic acid (PFOS), and perfluorohexanesulfonic acid (PFHxS) in the Maternal-Infant Research on Environmental Chemicals (MIREC) study and assessed children's full-scale (n = 522), performance (n = 517), and verbal (n = 519) IQ using the Wechsler Preschool and Primary Scale of Intelligence (WPPSI-III). Children's working memory (n = 513) and ability to plan and organize (n = 514) were assessed using a parent-reported questionnaire, the Behavior Rating Inventory of Executive Function - Preschool Version (BRIEF-P). We quantified associations between individual log2-transformed PFAS exposure and children's IQ and EF using multiple linear regression analyses and evaluated effect modification by child sex. We also used Repeated Holdout Weighted Quantile Sum (WQS) regression models with effect modification by child sex to quantify the effect of combined exposure to all three PFAS chemicals on IQ and EF. All models were adjusted for key sociodemographic characteristics. Geometric mean plasma concentrations (IQR) for PFOA, PFOS and PFHxS were 1.68 (1.10–2.50), 4.97 (3.20–6.20) and 1.09 (0.67–1.60) μg/L respectively. We found evidence of effect modification by child sex in all models examining performance IQ (p <.01). Specifically, every doubling of PFOA, PFOS, and or PFHxS was inversely associated with performance IQ, but only in males (PFOA: B = −2.80, 95% CI: −4.92, −0.68; PFOS: B = −2.64, 95% CI: −4.77, −0.52; PFHxS: B = −2.92, 95% CI: −4.72, −1.12). Similarly, every quartile increase in the WQS index was associated with poorer performance IQ in males (B = −3.16, 95% CI: −4.90, −1.43), with PFHxS contributing the largest weight to the index. In contrast, no significant association was found for females (B = 0.63, 95% CI: −0.99, 2.26). No significant associations were found for EF in either males or females. Higher prenatal PFAS exposure was associated with lower performance IQ in males, suggesting that this association may be sex- and domain-specific. • We assessed associations between PFAS and child neurodevelopment. • PFOS, PFOS and PFHxS were inversely associated with nonverbal IQ in males. • In mixture models, PFHxS was identified as a chemical of concern. • We observed no associations between PFAS and executive functioning. • The association between PFAS and IQ may be sex and domain-specific. [ABSTRACT FROM AUTHOR]
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- 2023
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33. Maturational changes of neonatal electroencephalogram: A comparison between intra uterine and extra uterine development.
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Nunes, Magda Lahorgue, Khan, Richard Lester, Gomes Filho, Irênio, Booij, Linda, and da Costa, Jaderson Costa
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ELECTROENCEPHALOGRAPHY , *NEWBORN infants , *PREMATURE infants , *CEREBRAL palsy , *DEVELOPMENTAL biology , *NEUROPHYSIOLOGY - Abstract
Highlights: [•] Preterm neonates when matched for conceptional age to term controls have less mature EEG patterns. [•] Sleep organization of preterm neonates is influenced by extra uterine development. [•] Background abnormalities recorded in neonatal EEG might predict cerebral palsy. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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34. Decreased [18F]MPPF Binding Potential in the Dorsal Raphe Nucleus After a Single Oral Dose of Fluoxetine: A Positron-Emission Tomography Study in Healthy Volunteers
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Sibon, Igor, Benkelfat, Chawki, Gravel, Paul, Aznavour, Nicolas, Costes, Nicolas, Mzengeza, Shadrek, Booij, Linda, Baker, Glen, Soucy, Jean-Paul, Zimmer, Luc, and Descarries, Laurent
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SEROTONIN , *LIGANDS (Biochemistry) , *AUTORECEPTORS , *NEUROTRANSMITTERS - Abstract
Background: Brain serotonin-1A (5-HT1A) autoreceptors internalize when activated by agonist or by their endogenous ligand, serotonin. This positron-emission tomography (PET) study tested the hypothesis that 5-HT1A autoreceptor internalization might be indexed in vivo by a decrease in the specific binding of the 5-HT1A radioligand, 4-[18F]fluoro-N-[2-[1-(2-methoxyphenyl)-1 piperazinyl]ethyl-N-2-pyridinyl-benzamide ([18F]MPPF), in the dorsal raphe nucleus (DRN) of healthy adult men administered a single oral dose of the selective serotonin reuptake inhibitor, fluoxetine. Methods: [18F]MPPF binding potential was measured in the DRN and other brain regions endowed with 5-HT1A receptors in eight healthy volunteers, 5 hours after the randomized, double-blind administration of fluoxetine (20 mg) or placebo. Results: In every subject, [18F]MPPF binding potential was decreased in the DRN only (44% ± 22 SD), in response to fluoxetine. Conclusions: Imaging the functional state of 5-HT1A autoreceptors (i.e., internalization) in the human brain, using [18F]MPPF/PET, may represent a promising avenue for investigating the neurobiology of serotonin-related disorders and notably of major depression. [Copyright &y& Elsevier]
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- 2008
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35. The association between childhood stressors and histone deacetylase density in the brain of adults followed since childhood: A positron emission tomography study.
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Chiarella, Julian, Sild, Mari, Casey, Kevin F., Massarweh, Gassan, Soucy, Jean-Paul, Leyton, Marco, Azar, Naomi, Tremblay, Richard E., Hooker, Jacob, Benkelfat, Chawki, and Booij, Linda
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POSITRON emission tomography , *HISTONE deacetylase , *CHILDREN , *BRAIN , *ADULTS - Published
- 2019
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36. F135. FKBP5 Methylation is Associated With Frontal-Limbic Brain Structure and Function in Depressed Adolescents and Healthy Controls.
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Chiarella, Julian, Pomares, Florence, Tozzi, Leonardo, Frodl, Thomas, Khalid-Khan, Sarosh, Schumann, Lyndall, Nguyen, Tuong-Vi, Yu, Wei-Jo, Szyf, Moshe, Nemoda, Zsofia, and Booij, Linda
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DEPRESSION in adolescence , *METHYLATION , *DNA methylation - Published
- 2018
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- View/download PDF
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