Your search keyword '"Stone, William S."' showing total 868 results

1. Excessive interstitial free-water in cortical gray matter preceding accelerated volume changes in individuals at clinical high risk for psychosis

Author

Cho, Kang Ik K., Zhang, Fan, Penzel, Nora, Seitz-Holland, Johanna, Tang, Yingying, Zhang, Tianhong, Xu, Lihua, Li, Huijun, Keshavan, Matcheri, Whitfield-Gabrieli, Susan, Niznikiewicz, Margaret, Stone, William S., Wang, Jijun, Shenton, Martha E., and Pasternak, Ofer

Published

2024

2. Emergence and dynamics of delusions and hallucinations across stages in early psychosis

Author

Mourgues-Codern, Catalina, Benrimoh, David, Gandhi, Jay, Farina, Emily A., Vin, Raina, Zamorano, Tihare, Parekh, Deven, Malla, Ashok, Joober, Ridha, Lepage, Martin, Iyer, Srividya N., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cornblatt, Barbara, Keshavan, Matcheri, Stone, William S., Mathalon, Daniel H., Perkins, Diana O., Walker, Elaine F., Cannon, Tyrone D., Woods, Scott W., Shah, Jai L., and Powers, Albert R.

Subjects

Quantitative Biology - Neurons and Cognition

Abstract

Hallucinations and delusions are often grouped together within the positive symptoms of psychosis. However, recent evidence suggests they may be driven by distinct computational and neural mechanisms. Examining the time course of their emergence may provide insights into the relationship between these underlying mechanisms. Participants from the second (N = 719) and third (N = 699) iterations of the North American Prodrome Longitudinal Study (NAPLS 2 and 3) were assessed for timing of CHR-P-level delusion and hallucination onset. Pre-onset symptom patterns in first-episode psychosis patients (FEP) from the Prevention and Early Intervention Program for Psychosis (PEPP-Montreal; N = 694) were also assessed. Symptom onset was determined at baseline assessment and the evolution of symptom patterns examined over 24 months. In all three samples, participants were more likely to report the onset of delusion-spectrum symptoms prior to hallucination-spectrum symptoms (odds ratios (OR): NAPLS 2 = 4.09; NAPLS 3 = 4.14; PEPP, Z = 7.01, P < 0.001) and to present with only delusions compared to only hallucinations (OR: NAPLS 2 = 5.6; NAPLS 3 = 11.11; PEPP = 42.75). Re-emergence of delusions after remission was also more common than re-emergence of hallucinations (Ps < 0.05), and hallucinations more often resolved first (Ps < 0.001). In both CHR-P samples, ratings of delusional ideation fell with the onset of hallucinations (P = 0.007). Delusions tend to emerge before hallucinations and may play a role in their development. Further work should examine the relationship between the mechanisms driving these symptoms and its utility for diagnosis and treatment.

Published

2024

3. Longitudinal change in neurocognitive functioning in children and adolescents at clinical high risk for psychosis: a systematic review

Author

Pedruzo, Borja, Aymerich, Claudia, Pacho, Malein, Herrero, Jon, Laborda, María, Bordenave, Marta, Giuliano, Anthony J., McCutcheon, Robert A., Gutiérrez-Rojas, Luis, McGuire, Philip, Stone, William S., Fusar-Poli, Paolo, González-Torres, Miguel Ángel, and Catalan, Ana

Published

2024

4. The magnitude and variability of neurocognitive performance in first-episode psychosis: a systematic review and meta-analysis of longitudinal studies

Author

Catalan, Ana, McCutcheon, Robert A., Aymerich, Claudia, Pedruzo, Borja, Radua, Joaquim, Rodríguez, Victoria, Salazar de Pablo, Gonzalo, Pacho, Malein, Pérez, Jose Luis, Solmi, Marco, McGuire, Philip, Giuliano, Anthony J., Stone, William S., Murray, Robin M., Gonzalez-Torres, Miguel Angel, and Fusar-Poli, Paolo

Published

2024

5. Correction: Longitudinal change in neurocognitive functioning in children and adolescents at clinical high risk for psychosis: a systematic review

Author

Pedruzo, Borja, Aymerich, Claudia, Pacho, Malein, Herrero, Jon, Laborda, María, Bordenave, Marta, Giuliano, Anthony J., McCutcheon, Robert A., Gutiérrez-Rojas, Luis, McGuire, Philip, Stone, William S., Fusar-Poli, Paolo, González-Torres, Miguel Ángel, and Catalan, Ana

Published

2024

6. Unique Functional Neuroimaging Signatures of Genetic Versus Clinical High Risk for Psychosis

Author

Schleifer, Charles H., Chang, Sarah E., Amir, Carolyn M., O’Hora, Kathleen P., Fung, Hoki, Kang, Jee Won D., Kushan-Wells, Leila, Daly, Eileen, Di Fabio, Fabio, Frascarelli, Marianna, Gudbrandsen, Maria, Kates, Wendy R., Murphy, Declan, Addington, Jean, Anticevic, Alan, Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Walker, Elaine, Woods, Scott W., Uddin, Lucina Q., Kumar, Kuldeep, Hoftman, Gil D., and Bearden, Carrie E.

Published

2025

7. Robust Brain Correlates of Cognitive Performance in Psychosis and Its Prodrome

Author

Ward, Heather Burrell, Beermann, Adam, Xie, Jing, Yildiz, Gulcan, Felix, Karlos Manzanarez, Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin, Cannon, Tyrone D., Cornblatt, Barbara, Keshavan, Matcheri, Mathalon, Daniel, Perkins, Diana O., Seidman, Larry, Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott, Coleman, Michael J., Bouix, Sylvain, Holt, Daphne J., Öngür, Dost, Breier, Alan, Shenton, Martha E., Heckers, Stephan, Halko, Mark A., Lewandowski, Kathryn E., and Brady, Roscoe O., Jr.

Published

2025

8. Negative Symptom Trajectories in Individuals at Clinical High Risk for Psychosis: Differences Based on Deficit Syndrome, Persistence, and Transition Status.

Author

Tran, Tanya, Spilka, Michael J, Raugh, Ian M, Strauss, Gregory P, Bearden, Carrie E, Cadenhead, Kristin S, Cannon, Tyrone D, Cornblatt, Barbara A, Keshavan, Matcheri, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Seidman, Larry J, Stone, William S, Tsuang, Ming T, Walker, Elaine F, Woods, Scott W, and Addington, Jean M

Subjects

cognition, functioning, growth curve analysis, symptom course, Clinical Research, Pediatric, Mental Health, Brain Disorders, Serious Mental Illness

Abstract

Background and hypothesisNegative symptom trajectory in clinical high risk (CHR) for psychosis is ill defined. This study aimed to better characterize longitudinal patterns of change in negative symptoms, moderators of change, and differences in trajectories according to clinical subgroups. We hypothesized that negative symptom course will be nonlinear in CHR. Clinical subgroups known to be more severe variants of psychotic illness-deficit syndrome (DS), persistent negative syndrome (PNS), and acute psychosis onset-were expected to show more severe baseline symptoms, slower rates of change, and less stable rates of symptom resolution.Study designLinear, curvilinear, and stepwise growth curve models, with and without moderators, were fitted to negative symptom ratings from the NAPLS-3 CHR dataset (N = 699) and within clinical subgroups.Study resultsNegative symptoms followed a downward curvilinear trend, with marked improvement 0-6 months that subsequently stabilized (6-24 months), particularly among those with lower IQ and functioning. Clinical subgroups had higher baseline ratings, but distinct symptom courses; DS vs non-DS: more rapid initial improvement, similar stability of improvements; PNS vs non-PNS: similar rates of initial improvement and stability; transition vs no transition: slower rate of initial improvement, with greater stability of this rate.ConclusionsContinuous, frequent monitoring of negative symptoms in CHR is justified by 2 important study implications: (1) The initial 6 months of CHR program enrollment may be a key window for improving negative symptoms as less improvement is likely afterwards, (2) Early identification of clinical subgroups may inform distinct negative symptom trajectories and treatment needs.

Published

2023

9. The impact of early factors on persistent negative symptoms in youth at clinical high risk for psychosis

Author

Devoe, Daniel J, Lui, Lu, Cannon, Tyrone D, Cadenhead, Kristin Suzanne, Cornblatt, Barbara A, Keshavan, Matcheri, McGlashan, Tom H, Perkins, Diana O, Seidman, Larry J, Stone, William S, Tsuang, Ming T, Woods, Scott W, Walker, Elaine F, Mathalon, Daniel H, Bearden, Carrie E, and Addington, Jean

Subjects

Mental Health, Brain Disorders, Clinical Research, Pediatric, Pediatric Research Initiative, Physical Injury - Accidents and Adverse Effects, Schizophrenia, Mental health, persistent negative symptoms, clinical high risk, premorbid functioning, psychosis, trauma, life events, cannabis, early factors, Clinical Sciences, Public Health and Health Services, Psychology

Abstract

IntroductionPersistent negative symptoms (PNS) are described as continuing moderate negative symptoms. More severe negative symptoms have been associated with poor premorbid functioning in both chronic schizophrenia and first episode psychosis patients. Furthermore, youth at clinical high risk (CHR) for developing psychosis may also present with negative symptoms and poor premorbid functioning. The aim of this current study was to: (1) define the relationship between PNS and premorbid functioning, life events, trauma and bullying, previous cannabis use, and resource utilization, and (2) to examine what explanatory variables best predicted PNS.MethodCHR participants (N = 709) were recruited from the North American Prodrome Longitudinal Study (NAPLS 2). Participants were divided into two groups: those with PNS (n = 67) versus those without PNS (n = 673). A K-means cluster analysis was conducted to distinguish patterns of premorbid functioning across the different developmental stages. The relationships between premorbid adjustment and other variables were examined using independent samples t-tests or chi square for categorical variables.ResultsThere was significantly more males in the PNS group. Participants with PNS had significantly lower levels of premorbid adjustment in childhood, early adolescence, and late adolescence, compared to CHR participants without PNS. There were no differences between the groups in terms of trauma, bullying, and resource utilization. The non-PNS group had more cannabis use and more desirable and non-desirable life events.ConclusionIn terms of better understanding relationships between early factors and PNS, a prominent factor associated with PNS was premorbid functioning, in particular poor premorbid functioning in later adolescence.

Published

2023

10. Impact of adverse childhood experiences on risk for internalizing psychiatric disorders in youth at clinical high-risk for psychosis

Author

Giampetruzzi, Eugenia, Walker, Elaine F., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Woods, Scott W., and LoPilato, Allison M.

Published

2024

11. Sleep disturbance, suicidal ideation and psychosis-risk symptoms in individuals at clinical high risk for psychosis

Author

Cohen, Simon, Goldsmith, David R., Ning, Courtney S., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Seidman, Larry J., Stone, William S., Tsuang, Ming T., Woods, Scott W., Walker, Elaine F., and Miller, Brian J.

Published

2024

12. Associations between childhood ethnoracial minority density, cortical thickness, and social engagement among minority youth at clinical high-risk for psychosis

Author

Ku, Benson S., Collins, Meghan, Anglin, Deidre M., Diomino, Anthony M., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Druss, Benjamin G., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Tsuang, Ming T., Woods, Scott W., and Walker, Elaine F.

Published

2023

13. PsyCog: A computerised mini battery for assessing cognition in psychosis

Author

Gifford, George, Cullen, Alexis E., Vieira, Sandra, Searle, Anja, McCutcheon, Robert A., Modinos, Gemma, Stone, William S., Hird, Emily, Barnett, Jennifer, van Hell, Hendrika H., Catalan, Ana, Millgate, Edward, Taptiklis, Nick, Cormack, Francesca, Slot, Margot E., Dazzan, Paola, Maat, Arija, de Haan, Lieuwe, Facorro, Benedicto Crespo, Glenthøj, Birte, Lawrie, Stephen M., McDonald, Colm, Gruber, Oliver, van Amelsvoort, Thérèse, Arango, Celso, Kircher, Tilo, Nelson, Barnaby, Galderisi, Silvana, Bressan, Rodrigo A., Kwon, Jun Soo, Weiser, Mark, Mizrahi, Romina, Sachs, Gabriele, Kirschner, Matthias, Reichenberg, Abraham, Kahn, René, and McGuire, Philip

Published

2024

14. Neurocognition in adolescents and young adults at clinical high risk for psychosis: Predictive stability for social and role functioning

Author

Carrión, Ricardo E., Ku, Benson S., Dorvil, Sarah, Auther, Andrea M., McLaughlin, Danielle, Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott W., and Cornblatt, Barbara A.

Published

2024

15. Relations of Lifetime Perceived Stress and Basal Cortisol With Hippocampal Volume Among Healthy Adolescents and Those at Clinical High Risk for Psychosis: A Structural Equation Modeling Approach

Author

Aberizk, Katrina, Addington, Jean M., Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Tsuang, Ming T., Woods, Scott W., Walker, Elaine F., and Ku, Benson S.

Published

2024

16. Family-focused therapy for individuals at high clinical risk for psychosis: A confirmatory efficacy trial.

Author

Miklowitz, David J, Addington, Jean M, O'Brien, Mary P, Denenny, Danielle M, Weintraub, Marc J, Zinberg, Jamie L, Mathalon, Daniel H, Cornblatt, Barbara A, Friedman-Yakoobian, Michelle S, Stone, William S, Cadenhead, Kristin S, Woods, Scott W, Sugar, Catherine A, Cannon, Tyrone D, and Bearden, Carrie E

Subjects

Humans, Communication, Social Adjustment, Psychotic Disorders, Family Therapy, Adolescent, Adult, Young Adult, expressed emotion, family therapy, prodromal symptoms, psychotic disorders, social adjustment, Clinical Research, Serious Mental Illness, Mental Health, Pediatric, Prevention, Clinical Trials and Supportive Activities, Comparative Effectiveness Research, Behavioral and Social Science, 6.6 Psychological and behavioural, Evaluation of treatments and therapeutic interventions, Mental health, Good Health and Well Being, Clinical Sciences, Psychology, Psychiatry

Abstract

AimsYoung people with attenuated psychotic symptoms (APS), brief intermittent psychosis, and/or genetic risk and functional deterioration are at high risk for developing psychotic disorders. In a prior trial, family-focused therapy for clinical high risk youth (FFT-CHR) was more effective than brief psychoeducation in reducing APS severity over 6 months. This 7-site trial will compare the efficacy of FFT-CHR to a psychoeducational and supportive intervention (enhanced care) on APS and social functioning in CHR individuals over 18 months.MethodsParticipants (N = 220, ages 13-25 years) with a CHR syndrome will be randomly assigned to FFT-CHR (18 1-h sessions of family psychoeducation and communication/problem-solving skills training) or enhanced care (3 1-h family psychoeducational sessions followed by 5 individual support sessions), both given over 6 months. Participants will rate their weekly progress during treatment using a mobile-enhanced online platform. Family communication will be assessed in a laboratory interactional task at baseline and post-treatment. Independent evaluators will assess APS (primary outcome) and psychosocial functioning (secondary outcome) every 6 months over 18 months.ResultsWe hypothesize that, compared to enhanced care, FFT-CHR will be associated with greater improvements in APS and psychosocial functioning over 18 months. Secondarily, improvements in family communication over 6 months will mediate the relationship between treatment condition and primary and secondary outcomes over 18 months. The effects of FFT-CHR are predicted to be greater in individuals with higher baseline risk for psychosis conversion.ConclusionsResults of the trial will inform treatment guidelines for individuals at high risk for psychosis.

Published

2022

17. Plasma complement and coagulation proteins as prognostic factors of negative symptoms: An analysis of the NAPLS 2 and 3 studies

Author

Byrne, Jonah F., Healy, Colm, Föcking, Melanie, Heurich, Meike, Susai, Subash Raj, Mongan, David, Wynne, Kieran, Kodosaki, Eleftheria, Woods, Scott W., Cornblatt, Barbara A., Stone, William S., Mathalon, Daniel H., Bearden, Carrie E., Cadenhead, Kristin S., Addington, Jean, Walker, Elaine F., Cannon, Tyrone D., Cannon, Mary, Jeffries, Clark, Perkins, Diana, and Cotter, David R.

Published

2024

18. The associations between area-level residential instability and gray matter volumes from the North American Prodrome Longitudinal Study (NAPLS) consortium

Author

Ku, Benson S, Addington, Jean, Bearden, Carrie E, Cadenhead, Kristin S, Cannon, Tyrone D, Compton, Michael T, Cornblatt, Barbara A, Druss, Benjamin G, Keshavan, Matcheri, Mathalon, Daniel H, Perkins, Diana O, Stone, William S, Tsuang, Ming T, Woods, Scott W, and Walker, Elaine F

Subjects

Mental Health, Behavioral and Social Science, Brain Disorders, Neurosciences, Serious Mental Illness, Prevention, Good Health and Well Being, Adolescent, Adult, Cerebral Cortex, Child, Gray Matter, Humans, Longitudinal Studies, Magnetic Resonance Imaging, North America, Psychotic Disorders, Young Adult, Clinical high risk for psychosis, Caudal middle frontal gyms, Rostral anterior cingulate cortex, Residential instability, Schizophrenia, Caudal middle frontal gyrus, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

IntroductionArea-level residential instability (ARI), an index of social fragmentation, has been shown to explain the association between urbanicity and psychosis. Urban upbringing has been shown to be associated with reduced gray matter volumes (GMV)s of brain regions corresponding to the right caudal middle frontal gyrus (CMFG) and rostral anterior cingulate cortex (rACC). We hypothesize that greater ARI will be associated with reduced right CMFG and rACC GMVs.MethodsData were collected at baseline as part of the North American Prodrome Longitudinal Study Phase 2. Counties where participants resided during childhood were geographically coded using the US Census to area-level factors. ARI was defined as the percentage of residents living in a different house 5 years ago. Generalized linear mixed models tested associations between ARI and GMVs.ResultsThis study included 29 healthy controls (HC)s and 64 clinical high risk for psychosis (CHR-P) individuals who were aged 12 to 24 years, had remained in their baseline residential area, and had magnetic resonance imaging scans. ARI was associated with reduced right CMFG (adjusted β = -0.258; 95% CI = -0.502 to -0.015) and right rACC volumes (adjusted β = -0.318; 95% CI = -0.612 to -0.023). The interaction term (ARI-by-diagnostic group) in the prediction of both brain regions was not significant, indicating that the relationships between ARI and regional brain volumes held for both CHR-P and HCs.ConclusionsARI may adversely impact similar brain regions as urban upbringing. Further investigation into the potential mechanisms of the relationship between ARI and neurobiology, including social stress, is needed.

Published

2022

19. Individualized Prediction of Prodromal Symptom Remission for Youth at Clinical High Risk for Psychosis.

Author

Worthington, Michelle A, Addington, Jean, Bearden, Carrie E, Cadenhead, Kristin S, Cornblatt, Barbara A, Keshavan, Matcheri, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Stone, William S, Tsuang, Ming T, Walker, Elaine F, Woods, Scott W, and Cannon, Tyrone D

Subjects

Serious Mental Illness, Mental Health, Clinical Research, Pediatric, Brain Disorders, Prevention, Good Health and Well Being, Adolescent, Adult, Child, Disease Progression, Female, Humans, Longitudinal Studies, Machine Learning, Male, Prodromal Symptoms, Psychotic Disorders, Remission Induction, Risk Assessment, remission, clinical high risk, schizophrenia, psychosis, risk prediction, machine learning, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

The clinical high-risk period before a first episode of psychosis (CHR-P) has been widely studied with the goal of understanding the development of psychosis; however, less attention has been paid to the 75%-80% of CHR-P individuals who do not transition to psychosis. It is an open question whether multivariable models could be developed to predict remission outcomes at the same level of performance and generalizability as those that predict conversion to psychosis. Participants were drawn from the North American Prodrome Longitudinal Study (NAPLS3). An empirically derived set of clinical and demographic predictor variables were selected with elastic net regularization and were included in a gradient boosting machine algorithm to predict prodromal symptom remission. The predictive model was tested in a comparably sized independent sample (NAPLS2). The classification algorithm developed in NAPLS3 achieved an area under the curve of 0.66 (0.60-0.72) with a sensitivity of 0.68 and specificity of 0.53 when tested in an independent external sample (NAPLS2). Overall, future remitters had lower baseline prodromal symptoms than nonremitters. This study is the first to use a data-driven machine-learning approach to assess clinical and demographic predictors of symptomatic remission in individuals who do not convert to psychosis. The predictive power of the models in this study suggest that remission represents a unique clinical phenomenon. Further study is warranted to best understand factors contributing to resilience and recovery from the CHR-P state.

Published

2022

20. Sleep Disturbance in Individuals at Clinical High Risk for Psychosis.

Author

Zaks, Nina, Velikonja, Tjasa, Parvaz, Muhammad A, Zinberg, Jamie, Done, Monica, Mathalon, Daniel H, Addington, Jean, Cadenhead, Kristin, Cannon, Tyrone, Cornblatt, Barbara, McGlashan, Thomas, Perkins, Diana, Stone, William S, Tsuang, Ming, Walker, Elaine, Woods, Scott W, Keshavan, Matcheri S, Buysse, Daniel J, Velthorst, Eva, and Bearden, Carrie E

Subjects

Humans, Disease Progression, Prognosis, Risk, Longitudinal Studies, Psychotic Disorders, Schizophrenia, Adolescent, Adult, North America, Female, Male, Young Adult, Prodromal Symptoms, Sleep Wake Disorders, prodrome, psychotic disorders, schizophrenia, ultra-high risk, Brain Disorders, Sleep Research, Mental Health, Serious Mental Illness, Clinical Research, Behavioral and Social Science, Aetiology, 2.3 Psychological, social and economic factors, Mental health, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

IntroductionDisturbed sleep is a common feature of psychotic disorders that is also present in the clinical high risk (CHR) state. Evidence suggests a potential role of sleep disturbance in symptom progression, yet the interrelationship between sleep and CHR symptoms remains to be determined. To address this knowledge gap, we examined the association between disturbed sleep and CHR symptoms over time.MethodsData were obtained from the North American Prodrome Longitudinal Study (NAPLS)-3 consortium, including 688 CHR individuals and 94 controls (mean age 18.25, 46% female) for whom sleep was tracked prospectively for 8 months. We used Cox regression analyses to investigate whether sleep disturbances predicted conversion to psychosis up to >2 years later. With regressions and cross-lagged panel models, we analyzed longitudinal and bidirectional associations between sleep (the Pittsburgh Sleep Quality Index in conjunction with additional sleep items) and CHR symptoms. We also investigated the independent contribution of individual sleep characteristics on CHR symptom domains separately and explored whether cognitive impairments, stress, depression, and psychotropic medication affected the associations.ResultsDisturbed sleep at baseline did not predict conversion to psychosis. However, sleep disturbance was strongly correlated with heightened CHR symptoms over time. Depression accounted for half of the association between sleep and symptoms. Importantly, sleep was a significant predictor of CHR symptoms but not vice versa, although bidirectional effect sizes were similar.DiscussionThe critical role of sleep disturbance in CHR symptom changes suggests that sleep may be a promising intervention target to moderate outcome in the CHR state.

Published

2022

21. White matter changes in psychosis risk relate to development and are not impacted by the transition to psychosis.

Author

Di Biase, Maria A, Cetin-Karayumak, Suheyla, Lyall, Amanda E, Zalesky, Andrew, Cho, Kang Ik Kevin, Zhang, Fan, Kubicki, Marek, Rathi, Yogesh, Lyons, Monica G, Bouix, Sylvain, Billah, Tashrif, Anticevic, Alan, Schleifer, Charlie, Adkinson, Brendan D, Ji, Jie Lisa, Tamayo, Zailyn, Addington, Jean, Bearden, Carrie E, Cornblatt, Barbara A, Keshavan, Matcheri S, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Cadenhead, Kristen S, Tsuang, Ming T, Woods, Scott W, Stone, William S, Shenton, Martha E, Cannon, Tyrone D, and Pasternak, Ofer

Subjects

Corpus Callosum, Humans, Longitudinal Studies, Psychotic Disorders, Adolescent, Adult, Child, Child, Preschool, Young Adult, Prodromal Symptoms, White Matter, Mental Health, Serious Mental Illness, Pediatric, Prevention, Neurosciences, Biomedical Imaging, Clinical Research, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Subtle alterations in white matter microstructure are observed in youth at clinical high risk (CHR) for psychosis. However, the timing of these changes and their relationships to the emergence of psychosis remain unclear. Here, we track the evolution of white matter abnormalities in a large, longitudinal cohort of CHR individuals comprising the North American Prodrome Longitudinal Study (NAPLS-3). Multi-shell diffusion magnetic resonance imaging data were collected across multiple timepoints (1-5 over 1 year) in 286 subjects (aged 12-32 years): 25 CHR individuals who transitioned to psychosis (CHR-P; 61 scans), 205 CHR subjects with unknown transition outcome after the 1-year follow-up period (CHR-U; 596 scans), and 56 healthy controls (195 scans). Linear mixed effects models were fitted to infer the impact of age and illness-onset on variation in the fractional anisotropy of cellular tissue (FAT) and the volume fraction of extracellular free water (FW). Baseline measures of white matter microstructure did not differentiate between HC, CHR-U and CHR-P individuals. However, age trajectories differed between the three groups in line with a developmental effect: CHR-P and CHR-U groups displayed higher FAT in adolescence, and 4% lower FAT by 30 years of age compared to controls. Furthermore, older CHR-P subjects (20+ years) displayed 4% higher FW in the forceps major (p

Published

2021

22. Use of the Chinese version of the MATRICS Consensus Cognitive Battery to assess cognitive functioning in individuals with high risk for psychosis, first-episode schizophrenia and chronic schizophrenia: a systematic review and meta-analysis

Author

Cai, Bing, Zhu, Yikang, Liu, Dongyang, Li, Yaxi, Bueber, Marlys, Yang, Xuezhi, Luo, Guoshuai, Su, Ying, Grivel, Margaux M., Yang, Lawrence H., Qian, Min, Stone, William S., and Phillips, Michael R.

Published

2024

23. Anticholinergic Medication Burden–Associated Cognitive Impairment in Schizophrenia

Author

Joshi, Yash B, Thomas, Michael L, Braff, David L, Green, Michael F, Gur, Ruben C, Gur, Raquel E, Nuechterlein, Keith H, Stone, William S, Greenwood, Tiffany A, Lazzeroni, Laura C, MacDonald, Laura R, Molina, Juan L, Nungaray, John A, Radant, Allen D, Silverman, Jeremy M, Sprock, Joyce, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, Swerdlow, Neal R, and Light, Gregory A

Subjects

Biological Psychology, Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Psychology, Clinical Research, Behavioral and Social Science, Schizophrenia, Serious Mental Illness, Neurosciences, Brain Disorders, Mental Health, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Mental health, Adolescent, Adult, Aged, Cholinergic Antagonists, Cognition, Cognitive Dysfunction, Cohort Studies, Cross-Sectional Studies, Humans, Middle Aged, Neuropsychological Tests, Young Adult, Anticholinergics, Cognition/Learning/Memory, Psychopharmacology, Schizophrenia Spectrum and Other Psychotic Disorders, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Clinical sciences, Clinical and health psychology

Abstract

ObjectiveMany psychotropic medications used to treat schizophrenia have significant anticholinergic properties, which are linked to cognitive impairment and dementia risk in healthy subjects. Clarifying the impact of cognitive impairment attributable to anticholinergic medication burden may help optimize cognitive outcomes in schizophrenia. The aim of this study was to comprehensively characterize how this burden affects functioning across multiple cognitive domains in schizophrenia outpatients.MethodsCross-sectional data were analyzed using inferential statistics and exploratory structural equation modeling to determine the relationship between anticholinergic medication burden and cognition. Patients with a diagnosis of schizophrenia or schizoaffective disorder (N=1,120) were recruited from the community at five U.S. universities as part of the Consortium on the Genetics of Schizophrenia-2. For each participant, prescribed medications were rated and summed according to a modified Anticholinergic Cognitive Burden (ACB) scale. Cognitive functioning was assessed by performance on domains of the Penn Computerized Neurocognitive Battery (PCNB).ResultsACB score was significantly associated with cognitive performance, with higher ACB groups scoring worse than lower ACB groups on all domains tested on the PCNB. Similar effects were seen on other cognitive tests. Effects remained significant after controlling for demographic characteristics and potential proxies of illness severity, including clinical symptoms and chlorpromazine-equivalent antipsychotic dosage.ConclusionsAnticholinergic medication burden in schizophrenia is substantial, common, conferred by multiple medication classes, and associated with cognitive impairments across all cognitive domains. Anticholinergic medication burden from all medication classes-including psychotropics used in usual care-should be considered in treatment decisions and accounted for in studies of cognitive functioning in schizophrenia.

Published

2021

24. Genetic and clinical analyses of psychosis spectrum symptoms in a large multiethnic youth cohort reveal significant link with ADHD.

Author

Olde Loohuis, Loes M, Mennigen, Eva, Ori, Anil PS, Perkins, Diana, Robinson, Elise, Addington, Jean, Cadenhead, Kristin S, Cornblatt, Barbara A, Mathalon, Daniel H, McGlashan, Thomas H, Seidman, Larry J, Keshavan, Matcheri S, Stone, William S, Tsuang, Ming T, Walker, Elaine F, Woods, Scott W, Cannon, Tyrone D, Gur, Ruben C, Gur, Raquel E, Bearden, Carrie E, and Ophoff, Roel A

Subjects

Brain, Humans, Cohort Studies, Attention Deficit Disorder with Hyperactivity, Psychotic Disorders, Multifactorial Inheritance, Adolescent, Adult, Child, Mental Health, Behavioral and Social Science, Genetics, Neurosciences, Brain Disorders, Pediatric Research Initiative, Clinical Research, Attention Deficit Disorder (ADD), Pediatric, 2.1 Biological and endogenous factors, 2.3 Psychological, social and economic factors, Mental health, Clinical Sciences, Public Health and Health Services, Psychology

Abstract

Psychotic symptoms are not only an important feature of severe neuropsychiatric disorders, but are also common in the general population, especially in youth. The genetic etiology of psychosis symptoms in youth remains poorly understood. To characterize genetic risk for psychosis spectrum symptoms (PS), we leverage a community-based multiethnic sample of children and adolescents aged 8-22 years, the Philadelphia Neurodevelopmental Cohort (n = 7225, 20% PS). Using an elastic net regression model, we aim to classify PS status using polygenic scores (PGS) based on a range of heritable psychiatric and brain-related traits in a multi-PGS model. We also perform univariate PGS associations and evaluate age-specific effects. The multi-PGS analyses do not improve prediction of PS status over univariate models, but reveal that the attention deficit hyperactivity disorder (ADHD) PGS is robustly and uniquely associated with PS (OR 1.12 (1.05, 1.18) P = 0.0003). This association is driven by subjects of European ancestry (OR = 1.23 (1.14, 1.34), P = 4.15 × 10-7) but is not observed in African American subjects (P = 0.65). We find a significant interaction of ADHD PGS with age (P = 0.01), with a stronger association in younger children. The association is independent of phenotypic overlap between ADHD and PS, not indirectly driven by substance use or childhood trauma, and appears to be specific to PS rather than reflecting general psychopathology in youth. In an independent sample, we replicate an increased ADHD PGS in 328 youth at clinical high risk for psychosis, compared to 216 unaffected controls (OR 1.06, CI(1.01, 1.11), P = 0.02). Our findings suggest that PS in youth may reflect a different genetic etiology than psychotic symptoms in adulthood, one more akin to ADHD, and shed light on how genetic risk can be investigated across early disease trajectories.

Published

2021

25. Counterpoint. Early intervention for psychosis risk syndromes: Minimizing risk and maximizing benefit.

Author

Woods, Scott W, Bearden, Carrie E, Sabb, Fred W, Stone, William S, Torous, John, Cornblatt, Barbara A, Perkins, Diana O, Cadenhead, Kristin S, Addington, Jean, Powers, Albert R, Mathalon, Daniel H, Calkins, Monica E, Wolf, Daniel H, Corcoran, Cheryl M, Horton, Leslie E, Mittal, Vijay A, Schiffman, Jason, Ellman, Lauren M, Strauss, Gregory P, Mamah, Daniel, Choi, Jimmy, Pearlson, Godfrey D, Shah, Jai L, Fusar-Poli, Paolo, Arango, Celso, Perez, Jesus, Koutsouleris, Nikolaos, Wang, Jijun, Kwon, Jun Soo, Walsh, Barbara C, McGlashan, Thomas H, Hyman, Steven E, Gur, Raquel E, Cannon, Tyrone D, Kane, John M, and Anticevic, Alan

Subjects

Humans, Syndrome, Psychotic Disorders, Social Stigma, Autonomy, Beneficence, Biomarkers, Clinical high risk, Psychosis, Stigma, Clinical Research, Mental Health, Serious Mental Illness, Pediatric Research Initiative, Prevention, Good Health and Well Being, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

BackgroundMalhi et al. in this issue critique the clinical high risk (CHR) syndrome for psychosis.MethodResponse to points of critique.ResultsWe agree that inconsistency in CHR nomenclature should be minimized. We respectfully disagree on other points. In our view: a) individuals with CHR and their families need help, using existing interventions, even though we do not yet fully understand disease mechanisms; b) substantial progress has been made in identification of biomarkers; c) symptoms used to identify CHR are specific to psychotic illnesses; d) CHR diagnosis is not "extremely difficult"; e) the pattern of progression, although heterogenous, is discernible; f) "psychosis-like symptoms" are common but are not used to identify CHR; and g) on the point described as 'the real risk,' CHR diagnosis does not frequently cause harmful stigma.DiscussionMalhi et al.'s arguments do not fairly characterize progress in the CHR field nor efforts to minimize stigma. That said, much work remains in areas of consistent nomenclature, mechanisms of disease, dissecting heterogeneity, and biomarkers. With regard to what the authors term the "real risk" of stigma associated with a CHR "label," however, our view is that avoiding words like "risk" and "psychosis" reinforces the stigma that both they and we mean to oppose. Moreover, patients and their families benefit from being given a term that describes what is happening to them.

Published

2021

26. Depression: An actionable outcome for those at clinical high-risk

Author

Addington, Jean, Farris, Megan S, Liu, Lu, Cadenhead, Kristin S, Cannon, Tyrone D, Cornblatt, Barbara A, McGlashan, Thomas H, Perkins, Diana O, Seidman, Larry J, Tsuang, Ming T, Walker, Elaine F, Bearden, Carrie E, Mathalon, Daniel H, Stone, William S, Keshevan, Matcheri, and Woods, Scott W

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Depression, Pediatric Research Initiative, Behavioral and Social Science, Pediatric, Prevention, Mental Health, Clinical Research, Brain Disorders, Serious Mental Illness, Mental health, Good Health and Well Being, Adolescent, Depressive Disorder, Major, Diagnostic and Statistical Manual of Mental Disorders, Humans, Psychotic Disorders, Young Adult, Clinical high-risk, Psychosis, Prognosis, Symptoms, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Clinical sciences

Abstract

Comorbid diagnoses are common in youth who are at clinical high-risk (CHR) for developing psychosis, with depression being the most common. The aim of this paper is to examine depression over two years in a large sample of CHR youth who do not make the transition to psychosis, considering both categorical and dimensional ratings of depression severity. The sample consisted of 267 CHR youth who were followed for two years. Based on DSM-IV diagnoses over this time period, 100 CHR individuals never received a diagnosis of depression, 64 individuals continuously met criteria for depression, 92 individuals received a diagnosis of depression at one or more timepoints, and 11 participants had a diagnosis of depression only at 24-months. These groupings were supported by six-monthly ratings on the Calgary Depression Scale. The majority of this sample experienced a major depressive episode on more than one occasion, suggesting that depression and depressive symptoms identify a domain of substantial unmet clinical need. Recommendations are that depression in CHR youth and young adults should be monitored more frequently and that there is a need for clinical trials to address depression systematically in this vulnerable population.

Published

2021

27. Abnormally Large Baseline P300 Amplitude Is Associated With Conversion to Psychosis in Clinical High Risk Individuals With a History of Autism: A Pilot Study.

Author

Foss-Feig, Jennifer H, Guillory, Sylvia B, Roach, Brian J, Velthorst, Eva, Hamilton, Holly, Bachman, Peter, Belger, Aysenil, Carrion, Ricardo, Duncan, Erica, Johannesen, Jason, Light, Gregory A, Niznikiewicz, Margaret, Addington, Jean M, Cadenhead, Kristin S, Cannon, Tyrone D, Cornblatt, Barbara, McGlashan, Thomas, Perkins, Diana, Seidman, Larry J, Stone, William S, Tsuang, Ming, Walker, Elaine F, Woods, Scott, Bearden, Carrie E, and Mathalon, Daniel H

Subjects

EEG, P300, autism spectrum disorder, conversion, prodrome, psychosis, Autism, Intellectual and Developmental Disabilities (IDD), Pediatric, Mental Health, Neurosciences, Serious Mental Illness, Brain Disorders, Prevention, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, 2.3 Psychological, social and economic factors, Mental health, Clinical Sciences, Public Health and Health Services, Psychology

Abstract

Psychosis rates in autism spectrum disorder (ASD) are 5-35% higher than in the general population. The overlap in sensory and attentional processing abnormalities highlights the possibility of related neurobiological substrates. Previous research has shown that several electroencephalography (EEG)-derived event-related potential (ERP) components that are abnormal in schizophrenia, including P300, are also abnormal in individuals at Clinical High Risk (CHR) for psychosis and predict conversion to psychosis. Yet, it is unclear whether P300 is similarly sensitive to psychosis risk in help-seeking CHR individuals with ASD history. In this exploratory study, we leveraged data from the North American Prodrome Longitudinal Study (NAPLS2) to probe for the first time EEG markers of longitudinal psychosis profiles in ASD. Specifically, we investigated the P300 ERP component and its sensitivity to psychosis conversion across CHR groups with (ASD+) and without (ASD-) comorbid ASD. Baseline EEG data were analyzed from 304 CHR patients (14 ASD+; 290 ASD-) from the NAPLS2 cohort who were followed longitudinally over two years. We examined P300 amplitude to infrequent Target (10%; P3b) and Novel distractor (10%; P3a) stimuli from visual and auditory oddball tasks. Whereas P300 amplitude attenuation is typically characteristic of CHR and predictive of conversion to psychosis in non-ASD sample, in our sample, history of ASD moderated this relationship such that, in CHR/ASD+ individuals, enhanced - rather than attenuated - visual P300 (regardless of stimulus type) was associated with psychosis conversion. This pattern was also seen for auditory P3b amplitude to Target stimuli. Though drawn from a small sample of CHR individuals with ASD, these preliminary results point to a paradoxical effect, wherein those with both CHR and ASD history who go on to develop psychosis have a unique pattern of enhanced neural response during attention orienting to both visual and target stimuli. Such a pattern stands out from the usual finding of P300 amplitude reductions predicting psychosis in non-ASD CHR populations and warrants follow up in larger scale, targeted, longitudinal studies of those with ASD at clinical high risk for psychosis.

Published

2021

28. Heritability of acoustic startle magnitude and latency from the consortium on the genetics of schizophrenia

Author

Greenwood, Tiffany A, Swerdlow, Neal R, Sprock, Joyce, Calkins, Monica E, Freedman, Robert, Green, Michael F, Gur, Raquel E, Gur, Ruben C, Lazzeroni, Laura C, Light, Gregory A, Nuechterlein, Keith H, Radant, Allen D, Silverman, Jeremy M, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, Braff, David L, and Duncan, Erica

Subjects

Neurosciences, Clinical Research, Schizophrenia, Brain Disorders, Genetics, Mental Health, Acoustic Stimulation, Acoustics, Humans, Prepulse Inhibition, Reflex, Startle, Latency, Heritability, Acoustic startle, Endophenotype, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

BackgroundLatency of the acoustic startle reflex is the time from presentation of the startling stimulus until the response, and provides an index of neural processing speed. Schizophrenia subjects exhibit slowed latency compared to healthy controls. One prior publication reported significant heritability of latency. The current study was undertaken to replicate and extend this solitary finding in a larger cohort.MethodsSchizophrenia probands, their relatives, and control subjects from the Consortium on the Genetics of Schizophrenia (COGS-1) were tested in a paradigm to ascertain magnitude, latency, and prepulse inhibition of startle. Trial types in the paradigm were: pulse-alone, and trials with 30, 60, or 120 ms between the prepulse and pulse. Comparisons of subject groups were conducted with ANCOVAs to assess startle latency and magnitude. Heritability of startle magnitude and latency was analyzed with a variance component method implemented in SOLAR v.4.3.1.Results980 subjects had analyzable startle results: 199 schizophrenia probands, 456 of their relatives, and 325 controls. A mixed-design ANCOVA on startle latency in the four trial types was significant for subject group (F(2,973) = 4.45, p = 0.012) such that probands were slowest, relatives were intermediate and controls were fastest. Magnitude to pulse-alone trials differed significantly between groups by ANCOVA (F(2,974) = 3.92, p = 0.020) such that controls were lowest, probands highest, and relatives intermediate. Heritability was significant (p

Published

2020

29. O5.6. ADVANCED DIFFUSION IMAGING IN PSYCHOSIS RISK: A CROSS-SECTIONAL AND LONGITUDINAL STUDY OF WHITE MATTER DEVELOPMENT

Author

Di Biase, Maria, Cetin Karayumak, Suheyla, Zalesky, Andrew, Kubicki, Marek, Rathi, Yogesh, Lyons, Monica G, Bouix, Sylvain, Billah, Tashrif, Higger, Matt, Anticevic, Alan, Addington, Jean, Bearden, Carrie E, Cornblatt, Barbara A, Keshavan, Matcheri S, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Cadenhead, Kristin S, Tsuang, Ming T, Woods, Scott W, Seidman, Larry J, Stone, William S, Shenton, Martha E, Cannon, Tyrone D, and Pasternak, Ofer

Subjects

Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Abstract Background Studies in individuals at clinical high risk (CHR) for psychosis provide a powerful means to predict outcomes and inform putative mechanisms underlying conversion to psychosis. In previous work, we applied advanced diffusion imaging methods to reveal that white matter pathology in a CHR population is characterized by cellular-specific changes in white matter, suggesting a preexisting neurodevelopmental anomaly. However, it remains unknown whether these deficits relate to clinical symptoms and/or conversion to frank psychosis. To address this gap, we examined cross-sectional and longitudinal white matter maturation in the largest imaging population of CHR individuals to date, obtained from the North American Prodrome Longitudinal Study (NAPLS-3). Methods Multi-shell diffusion magnetic resonance imaging (MRI) data were collected across multiple timepoints (1–6 at ~2 month intervals) in 286 subjects (age range=12–32 years). These were 230 unmedicated CHR subjects, including 11% (n=25) who transitioned to psychosis (CHR-converters), as well as 56 age and sex-matched healthy controls. Raw diffusion signals were harmonized to remove scanner/site-induced effects, yielding a unified imaging dataset. Fractional anisotropy of cellular tissue (FAt) and the volume fraction of extracellular free-water (FW) were assessed in 12 major tracts from the IIT Human Brain Atlas (v.5.0). Linear mixed effects (LME) models were fitted to infer developmental trajectories of FAt and FW across age for CHR-converters, CHR-nonconverters and control groups, while accounting for the repeated measurements on each individual. Results The rate at which FAt changed with age significantly differed between the three groups across commissural and association tracts (5 in total; p

Published

2020

30. Stressor-Cortisol Concordance Among Individuals at Clinical High-Risk for Psychosis: Novel Findings from the NAPLS Cohort.

Author

Cullen, Alexis E, Addington, Jean, Bearden, Carrie E, Stone, William S, Seidman, Larry J, Cadenhead, Kristin S, Cannon, Tyrone D, Cornblatt, Barbara A, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Tsuang, Ming T, Woods, Scott W, and Walker, Elaine F

Subjects

Hypothalamo-Hypophyseal System, Saliva, Humans, Disease Progression, Disease Susceptibility, Hydrocortisone, Longitudinal Studies, Stress, Psychological, Psychotic Disorders, Schizophrenia, Adolescent, Adult, Female, Male, Young Adult, Prodromal Symptoms, HPA axis responsivity, psychosis, schizophrenia, stress adversity, stressor-cortisol correspondence, Mental Health, Clinical Research, Serious Mental Illness, Behavioral and Social Science, Pediatric, Brain Disorders, 2.3 Psychological, social and economic factors, Aetiology, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Whilst elevations in basal cortisol levels have been reported among individuals at-risk for psychosis, the extent to which this represents hyperresponsivity of the hypothalamic-pituitary-adrenal (HPA) axis to psychosocial stressors encountered in the natural environment is currently unclear. We aimed to examine stressor-cortisol concordance among youth at clinical high-risk (CHR) for psychosis in the North American Prodrome Longitudinal Study 2 (NAPLS 2) and the relationship with clinical outcome. At baseline, CHR (N = 457) and healthy (N = 205) individuals provided salivary cortisol samples and completed daily stressor, life event, and childhood trauma measures. CHR youth were categorised as remitted, symptomatic, progression of positive symptoms, or psychosis conversion at the two-year follow-up. Within-group regression models tested associations between psychosocial stressors and cortisol; standardised beta coefficients (Stβ) were subsequently derived to enable within-group pooling of effect sizes across stressor types. After adjustment for potential confounders, all CHR subgroups reported greater exposure to life events and daily stressors, and more distress in relation to these events, relative to controls. All CHR groups were also more likely to experience childhood trauma; only CHR converters, however, were characterised by elevated basal cortisol. Daily stressor distress was significantly associated with cortisol in controls (β = 0.60, 95% CI: 0.12-1.08) and CHR youth who converted to psychosis (β = 0.91, 95% CI: 0.05-1.78). In controls only, life event exposure was associated with cortisol (β = 0.45, 95% CI: 0.08-0.83). When pooled across stressors, stressor-cortisol concordance was substantially higher among CHR converters (Stβ = 0.26, 95% CI: 0.07 to 0.44) relative to CHR progressed (Stβ = 0.02, 95% CI: -0.11 to 0.15), symptomatic (Stβ = 0.01, 95% CI: -0.11 to 0.12), and remitted groups (Stβ = 0.00, 95% CI: -0.13 to 0.13); however, unexpectedly, healthy controls showed intermediate levels of concordance (Stβ = 0.15, 95% CI: 0.05 to 0.26). In conclusion, whilst all CHR subgroups showed increased psychosocial stress exposure and distress relative to controls, only those who later converted to psychosis were characterised by significantly elevated basal cortisol levels. Moreover, only CHR converters showed a higher magnitude of stressor-cortisol concordance compared to controls, although confidence intervals overlapped considerably between these two groups. These findings do not support the notion that all individuals at CHR for psychosis show HPA hyperresponsiveness to psychosocial stressors. Instead, CHR individuals vary in their response to stressor exposure/distress, perhaps driven by genetic or other vulnerability factors.

Published

2020

31. Ethnoracial discrimination and the development of suspiciousness symptoms in individuals at clinical high-risk for psychosis

Author

Michaels, Timothy I., Carrión, Ricardo E., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Keshavan, Matcheri, Mathalon, Daniel H., McGlashan, Thomas H., Perkins, Diana O., Seidman, Larry J., Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott W., and Cornblatt, Barbara A.

Published

2023

32. The effects of age and sex on cognitive impairment in schizophrenia: Findings from the Consortium on the Genetics of Schizophrenia (COGS) study

Author

Lee, Junghee, Green, Michael F, Nuechterlein, Keith H, Swerdlow, Neal R, Greenwood, Tiffany A, Hellemann, Gerhard S, Lazzeroni, Laura C, Light, Gregory A, Radant, Allen D, Seidman, Larry J, Siever, Larry J, Silverman, Jeremy M, Sprock, Joyce, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, Gur, Ruben C, Gur, Raquel E, and Braff, David L

Subjects

Biomedical and Clinical Sciences, Applied and Developmental Psychology, Biological Psychology, Psychology, Pharmacology and Pharmaceutical Sciences, Schizophrenia, Behavioral and Social Science, Mental Health, Neurosciences, Basic Behavioral and Social Science, Brain Disorders, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Mental health, Adult, Age Factors, Aged, Case-Control Studies, Cognitive Dysfunction, Female, Humans, Linear Models, Male, Memory, Short-Term, Middle Aged, Neuropsychological Tests, Schizophrenic Psychology, Sex Factors, Young Adult, General Science & Technology

Abstract

Recently emerging evidence indicates accelerated age-related changes in the structure and function of the brain in schizophrenia, raising a question about its potential consequences on cognitive function. Using a large sample of schizophrenia patients and controls and a battery of tasks across multiple cognitive domains, we examined whether patients show accelerated age-related decline in cognition and whether an age-related effect differ between females and males. We utilized data of 1,415 schizophrenia patients and 1,062 healthy community collected by the second phase of the Consortium on the Genetics of Schizophrenia (COGS-2). A battery of cognitive tasks included the Letter-Number Span Task, two forms of the Continuous Performance Test, the California Verbal Learning Test, Second Edition, the Penn Emotion Identification Test and the Penn Facial Memory Test. The effect of age and gender on cognitive performance was examined with a general linear model. We observed age-related changes on most cognitive measures, which was similar between males and females. Compared to controls, patients showed greater deterioration in performance on attention/vigilance and greater slowness of processing social information with increasing age. However, controls showed greater age-related changes in working memory and verbal memory compared to patients. Age-related changes (η2p of 0.001 to .008) were much smaller than between-group differences (η2p of 0.005 to .037). This study found that patients showed continued decline of cognition on some domains but stable impairment or even less decline on other domains with increasing age. These findings indicate that age-related changes in cognition in schizophrenia are subtle and not uniform across multiple cognitive domains.

Published

2020

33. Genome-wide Association of Endophenotypes for Schizophrenia From the Consortium on the Genetics of Schizophrenia (COGS) Study

Author

Greenwood, Tiffany A, Lazzeroni, Laura C, Maihofer, Adam X, Swerdlow, Neal R, Calkins, Monica E, Freedman, Robert, Green, Michael F, Light, Gregory A, Nievergelt, Caroline M, Nuechterlein, Keith H, Radant, Allen D, Siever, Larry J, Silverman, Jeremy M, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, Gur, Ruben C, Gur, Raquel E, and Braff, David L

Subjects

Schizophrenia, Neurosciences, Human Genome, Genetics, Mental Health, Clinical Research, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Mental health, Good Health and Well Being, Adult, Cognitive Dysfunction, Endophenotypes, Female, Genome-Wide Association Study, Humans, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Male, Middle Aged, Neuregulins, Potassium Channels, Other Medical and Health Sciences, Psychology, Cognitive Sciences

Abstract

ImportanceThe Consortium on the Genetics of Schizophrenia (COGS) uses quantitative neurophysiological and neurocognitive endophenotypes with demonstrated deficits in schizophrenia as a platform from which to explore the underlying neural circuitry and genetic architecture. Many of these endophenotypes are associated with poor functional outcome in schizophrenia. Some are also endorsed as potential treatment targets by the US Food and Drug Administration.ObjectiveTo build on prior assessments of heritability, association, and linkage in the COGS phase 1 (COGS-1) families by reporting a genome-wide association study (GWAS) of 11 schizophrenia-related endophenotypes in the independent phase 2 (COGS-2) cohort of patients with schizophrenia and healthy comparison participants (HCPs).Design, setting, and participantsA total of 1789 patients with schizophrenia and HCPs of self-reported European or Latino ancestry were recruited through a collaborative effort across the COGS sites and genotyped using the PsychChip. Standard quality control filters were applied, and more than 6.2 million variants with a genotyping call rate of greater than 0.99 were available after imputation. Association was performed for data sets stratified by diagnosis and ancestry using linear regression and adjusting for age, sex, and 5 principal components, with results combined through weighted meta-analysis. Data for COGS-1 were collected from January 6, 2003, to August 6, 2008; data for COGS-2, from June 30, 2010, to February 14, 2014. Data were analyzed from October 28, 2016, to May 4, 2018.Main outcomes and measuresA genome-wide association study was performed to evaluate association for 11 neurophysiological and neurocognitive endophenotypes targeting key domains of schizophrenia related to inhibition, attention, vigilance, learning, working memory, executive function, episodic memory, and social cognition.ResultsThe final sample of 1533 participants included 861 male participants (56.2%), and the mean (SD) age was 41.8 (13.6) years. In total, 7 genome-wide significant regions (P

Published

2019

34. Clinical Profiles and Conversion Rates Among Young Individuals With Autism Spectrum Disorder Who Present to Clinical High Risk for Psychosis Services.

Author

Foss-Feig, Jennifer H, Velthorst, Eva, Smith, Lauren, Reichenberg, Abraham, Addington, Jean, Cadenhead, Kristin S, Cornblatt, Barbara A, Mathalon, Daniel H, McGlashan, Thomas H, Perkins, Diana O, Seidman, Larry J, Stone, William S, Keshavan, Matcheri, Tsuang, Ming T, Walker, Elaine F, Woods, Scott W, Cannon, Tyrone D, and Bearden, Carrie E

Subjects

Humans, Disease Progression, Linear Models, Risk, Case-Control Studies, Longitudinal Studies, Predictive Value of Tests, Psychotic Disorders, Adolescent, North America, Female, Male, Young Adult, Prodromal Symptoms, Autism Spectrum Disorder, comorbidity, development, prodrome, schizophrenia, symptoms, Clinical Research, Serious Mental Illness, Mental Health, Autism, Brain Disorders, Intellectual and Developmental Disabilities (IDD), Prevention, Schizophrenia, Pediatric, Behavioral and Social Science, Aetiology, 2.3 Psychological, social and economic factors, Mental health, Medical and Health Sciences, Psychology and Cognitive Sciences, Developmental & Child Psychology

Abstract

ObjectiveThe overlap versus independence of autism spectrum disorder (ASD) and schizophrenia is a topic that has garnered the attention of generations of clinicians and scientists. Although high rates of psychotic symptoms have been identified in individuals with ASD, the nature, prevalence, and prognostic significance of subclinical psychotic experiences in ASD remain poorly understood.MethodThis study sought to compare baseline characteristics, clinical profiles, and conversion outcomes between young individuals at clinical high risk for psychosis (CHR) who presented with or without a prior ASD diagnosis during the second phase of the North American Prodrome Longitudinal Study (NAPLS, N = 764).ResultsPatients with CHR and ASD (CHR/ASD+, n = 26) tended to exhibit greater social and social cognitive difficulties, but expressed relatively levels of core psychosis symptoms similar to those of to patients with CHR but no ASD (CHR/ASD-). Risk for conversion to co-occurring psychosis (18.2% CHR/ASD+ versus 16.8% CHR/ASD-) was equivalent between CHR/ASD+ and CHR/ASD- groups, and the NAPLS2 Psychosis Risk Calculator predicted conversion to psychosis equally well across groups.ConclusionThese results suggest that baseline psychosis symptoms, predictors of risk for conversion, and ultimate conversion rates are similar in patients with CHR with and without ASD. They further suggest that ASD must not be considered a mutually exclusive diagnosis when such youth present in CHR settings. Future research is needed to better track trajectories in larger cohorts of individuals with CHR and comorbid ASD and to understand whether treatment recommendations effective in the broader CHR population are useful for this particular population as well.

Published

2019

35. Nonlinear dynamics underlying sensory processing dysfunction in schizophrenia

Author

Lainscsek, Claudia, Sampson, Aaron L, Kim, Robert, Thomas, Michael L, Man, Karen, Lainscsek, Xenia, Swerdlow, Neal R, Braff, David L, Sejnowski, Terrence J, Light, Gregory A, Green, Michael F, Greenwood, Tiffany A, Gur, Raquel E, Gur, Ruben C, Lazzeroni, Laura C, Nuechterlein, Keith H, Radant, Allen D, Seidman, Larry J, Sharp, Richard F, Siever, Larry J, Silverman, Jeremy M, Sprock, Joyce, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, and Turetsky, Bruce I

Subjects

Serious Mental Illness, Mental Health, Schizophrenia, Brain Disorders, Neurosciences, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Mental health, Good Health and Well Being, Acoustic Stimulation, Adult, Attention, Brain, Cognition, Electroencephalography, Evoked Potentials, Auditory, Female, Humans, Male, Middle Aged, Nonlinear Dynamics, Sensation, nonlinear dynamics, delay differential analysis, mismatch negativity, schizophrenia, EEG, COGS Investigators

Abstract

Natural systems, including the brain, often seem chaotic, since they are typically driven by complex nonlinear dynamical processes. Disruption in the fluid coordination of multiple brain regions contributes to impairments in information processing and the constellation of symptoms observed in neuropsychiatric disorders. Schizophrenia (SZ), one of the most debilitating mental illnesses, is thought to arise, in part, from such a network dysfunction, leading to impaired auditory information processing as well as cognitive and psychosocial deficits. Current approaches to neurophysiologic biomarker analyses predominantly rely on linear methods and may, therefore, fail to capture the wealth of information contained in whole EEG signals, including nonlinear dynamics. In this study, delay differential analysis (DDA), a nonlinear method based on embedding theory from theoretical physics, was applied to EEG recordings from 877 SZ patients and 753 nonpsychiatric comparison subjects (NCSs) who underwent mismatch negativity (MMN) testing via their participation in the Consortium on the Genetics of Schizophrenia (COGS-2) study. DDA revealed significant nonlinear dynamical architecture related to auditory information processing in both groups. Importantly, significant DDA changes preceded those observed with traditional linear methods. Marked abnormalities in both linear and nonlinear features were detected in SZ patients. These results illustrate the benefits of nonlinear analysis of brain signals and underscore the need for future studies to investigate the relationship between DDA features and pathophysiology of information processing.

Published

2019

36. Brain structural abnormalities of the associative striatum in adolescents and young adults at genetic high-risk of schizophrenia: Implications for illness endophenotypes

Author

Nestor, Paul G., Levin, Laura K., Stone, William S., Giuliano, Anthony J., Seidman, Larry J., and Levitt, James J.

Published

2022

37. Cannabis use and attenuated positive and negative symptoms in youth at clinical high risk for psychosis

Author

Santesteban-Echarri, Olga, Liu, Lu, Miller, Madeline, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., McGlashan, Thomas H., Perkins, Diana O., Seidman, Larry J., Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott W., and Addington, Jean

Published

2022

38. Neurodegenerative model of schizophrenia: Growing evidence to support a revisit

Author

Stone, William S., Phillips, Michael R., Yang, Lawrence H., Kegeles, Lawrence S., Susser, Ezra S., and Lieberman, Jeffrey A.

Published

2022

39. Family history of psychosis in youth at clinical high risk: A replication study

Author

Santesteban-Echarri, Olga, Sandel, Danah, Liu, Lu, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., McGlashan, Thomas H., Perkins, Diana O., Seidman, Larry J., Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott W., and Addington, Jean

Published

2022

40. The associations between area-level residential instability and gray matter volumes from the North American Prodrome Longitudinal Study (NAPLS) consortium

Author

Ku, Benson S., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Compton, Michael T., Cornblatt, Barbara A., Druss, Benjamin G., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Tsuang, Ming T., Woods, Scott W., and Walker, Elaine F.

Published

2022

41. Mapping genomic loci implicates genes and synaptic biology in schizophrenia

Author

Trubetskoy, Vassily, Pardiñas, Antonio F., Qi, Ting, Panagiotaropoulou, Georgia, Awasthi, Swapnil, Bigdeli, Tim B., Bryois, Julien, Chen, Chia-Yen, Dennison, Charlotte A., Hall, Lynsey S., Lam, Max, Watanabe, Kyoko, Frei, Oleksandr, Ge, Tian, Harwood, Janet C., Koopmans, Frank, Magnusson, Sigurdur, Richards, Alexander L., Sidorenko, Julia, Wu, Yang, Zeng, Jian, Grove, Jakob, Kim, Minsoo, Li, Zhiqiang, Voloudakis, Georgios, Zhang, Wen, Adams, Mark, Agartz, Ingrid, Atkinson, Elizabeth G., Agerbo, Esben, Al Eissa, Mariam, Albus, Margot, Alexander, Madeline, Alizadeh, Behrooz Z., Alptekin, Köksal, Als, Thomas D., Amin, Farooq, Arolt, Volker, Arrojo, Manuel, Athanasiu, Lavinia, Azevedo, Maria Helena, Bacanu, Silviu A., Bass, Nicholas J., Begemann, Martin, Belliveau, Richard A., Bene, Judit, Benyamin, Beben, Bergen, Sarah E., Blasi, Giuseppe, Bobes, Julio, Bonassi, Stefano, Braun, Alice, Bressan, Rodrigo Affonseca, Bromet, Evelyn J., Bruggeman, Richard, Buckley, Peter F., Buckner, Randy L., Bybjerg-Grauholm, Jonas, Cahn, Wiepke, Cairns, Murray J., Calkins, Monica E., Carr, Vaughan J., Castle, David, Catts, Stanley V., Chambert, Kimberley D., Chan, Raymond C. K., Chaumette, Boris, Cheng, Wei, Cheung, Eric F. C., Chong, Siow Ann, Cohen, David, Consoli, Angèle, Cordeiro, Quirino, Costas, Javier, Curtis, Charles, Davidson, Michael, Davis, Kenneth L., de Haan, Lieuwe, Degenhardt, Franziska, DeLisi, Lynn E., Demontis, Ditte, Dickerson, Faith, Dikeos, Dimitris, Dinan, Timothy, Djurovic, Srdjan, Duan, Jubao, Ducci, Giuseppe, Dudbridge, Frank, Eriksson, Johan G., Fañanás, Lourdes, Faraone, Stephen V., Fiorentino, Alessia, Forstner, Andreas, Frank, Josef, Freimer, Nelson B., Fromer, Menachem, Frustaci, Alessandra, Gadelha, Ary, Genovese, Giulio, Gershon, Elliot S., Giannitelli, Marianna, Giegling, Ina, Giusti-Rodríguez, Paola, Godard, Stephanie, Goldstein, Jacqueline I., González Peñas, Javier, González-Pinto, Ana, Gopal, Srihari, Gratten, Jacob, Green, Michael F., Greenwood, Tiffany A., Guillin, Olivier, Gülöksüz, Sinan, Gur, Raquel E., Gur, Ruben C., Gutiérrez, Blanca, Hahn, Eric, Hakonarson, Hakon, Haroutunian, Vahram, Hartmann, Annette M., Harvey, Carol, Hayward, Caroline, Henskens, Frans A., Herms, Stefan, Hoffmann, Per, Howrigan, Daniel P., Ikeda, Masashi, Iyegbe, Conrad, Joa, Inge, Julià, Antonio, Kähler, Anna K., Kam-Thong, Tony, Kamatani, Yoichiro, Karachanak-Yankova, Sena, Kebir, Oussama, Keller, Matthew C., Kelly, Brian J., Khrunin, Andrey, Kim, Sung-Wan, Klovins, Janis, Kondratiev, Nikolay, Konte, Bettina, Kraft, Julia, Kubo, Michiaki, Kučinskas, Vaidutis, Kučinskiene, Zita Ausrele, Kusumawardhani, Agung, Kuzelova-Ptackova, Hana, Landi, Stefano, Lazzeroni, Laura C., Lee, Phil H., Legge, Sophie E., Lehrer, Douglas S., Lencer, Rebecca, Lerer, Bernard, Li, Miaoxin, Lieberman, Jeffrey, Light, Gregory A., Limborska, Svetlana, Liu, Chih-Min, Lönnqvist, Jouko, Loughland, Carmel M., Lubinski, Jan, Luykx, Jurjen J., Lynham, Amy, Macek, Jr, Milan, Mackinnon, Andrew, Magnusson, Patrik K. E., Maher, Brion S., Maier, Wolfgang, Malaspina, Dolores, Mallet, Jacques, Marder, Stephen R., Marsal, Sara, Martin, Alicia R., Martorell, Lourdes, Mattheisen, Manuel, McCarley, Robert W., McDonald, Colm, McGrath, John J., Medeiros, Helena, Meier, Sandra, Melegh, Bela, Melle, Ingrid, Mesholam-Gately, Raquelle I., Metspalu, Andres, Michie, Patricia T., Milani, Lili, Milanova, Vihra, Mitjans, Marina, Molden, Espen, Molina, Esther, Molto, María Dolores, Mondelli, Valeria, Moreno, Carmen, Morley, Christopher P., Muntané, Gerard, Murphy, Kieran C., Myin-Germeys, Inez, Nenadić, Igor, Nestadt, Gerald, Nikitina-Zake, Liene, Noto, Cristiano, Nuechterlein, Keith H., O’Brien, Niamh Louise, O’Neill, F. Anthony, Oh, Sang-Yun, Olincy, Ann, Ota, Vanessa Kiyomi, Pantelis, Christos, Papadimitriou, George N., Parellada, Mara, Paunio, Tiina, Pellegrino, Renata, Periyasamy, Sathish, Perkins, Diana O., Pfuhlmann, Bruno, Pietiläinen, Olli, Pimm, Jonathan, Porteous, David, Powell, John, Quattrone, Diego, Quested, Digby, Radant, Allen D., Rampino, Antonio, Rapaport, Mark H., Rautanen, Anna, Reichenberg, Abraham, Roe, Cheryl, Roffman, Joshua L., Roth, Julian, Rothermundt, Matthias, Rutten, Bart P. F., Saker-Delye, Safaa, Salomaa, Veikko, Sanjuan, Julio, Santoro, Marcos Leite, Savitz, Adam, Schall, Ulrich, Scott, Rodney J., Seidman, Larry J., Sharp, Sally Isabel, Shi, Jianxin, Siever, Larry J., Sigurdsson, Engilbert, Sim, Kang, Skarabis, Nora, Slominsky, Petr, So, Hon-Cheong, Sobell, Janet L., Söderman, Erik, Stain, Helen J., Steen, Nils Eiel, Steixner-Kumar, Agnes A., Stögmann, Elisabeth, Stone, William S., Straub, Richard E., Streit, Fabian, Strengman, Eric, Stroup, T. Scott, Subramaniam, Mythily, Sugar, Catherine A., Suvisaari, Jaana, Svrakic, Dragan M., Swerdlow, Neal R., Szatkiewicz, Jin P., Ta, Thi Minh Tam, Takahashi, Atsushi, Terao, Chikashi, Thibaut, Florence, Toncheva, Draga, Tooney, Paul A., Torretta, Silvia, Tosato, Sarah, Tura, Gian Battista, Turetsky, Bruce I., Üçok, Alp, Vaaler, Arne, van Amelsvoort, Therese, van Winkel, Ruud, Veijola, Juha, Waddington, John, Walter, Henrik, Waterreus, Anna, Webb, Bradley T., Weiser, Mark, Williams, Nigel M., Witt, Stephanie H., Wormley, Brandon K., Wu, Jing Qin, Xu, Zhida, Yolken, Robert, Zai, Clement C., Zhou, Wei, Zhu, Feng, Zimprich, Fritz, Atbaşoğlu, Eşref Cem, Ayub, Muhammad, Benner, Christian, Bertolino, Alessandro, Black, Donald W., Bray, Nicholas J., Breen, Gerome, Buccola, Nancy G., Byerley, William F., Chen, Wei J., Cloninger, C. Robert, Crespo-Facorro, Benedicto, Donohoe, Gary, Freedman, Robert, Galletly, Cherrie, Gandal, Michael J., Gennarelli, Massimo, Hougaard, David M., Hwu, Hai-Gwo, Jablensky, Assen V., McCarroll, Steven A., Moran, Jennifer L., Mors, Ole, Mortensen, Preben B., Müller-Myhsok, Bertram, Neil, Amanda L., Nordentoft, Merete, Pato, Michele T., Petryshen, Tracey L., Pirinen, Matti, Pulver, Ann E., Schulze, Thomas G., Silverman, Jeremy M., Smoller, Jordan W., Stahl, Eli A., Tsuang, Debby W., Vilella, Elisabet, Wang, Shi-Heng, Xu, Shuhua, Adolfsson, Rolf, Arango, Celso, Baune, Bernhard T., Belangero, Sintia Iole, Børglum, Anders D., Braff, David, Bramon, Elvira, Buxbaum, Joseph D., Campion, Dominique, Cervilla, Jorge A., Cichon, Sven, Collier, David A., Corvin, Aiden, Curtis, David, Forti, Marta Di, Domenici, Enrico, Ehrenreich, Hannelore, Escott-Price, Valentina, Esko, Tõnu, Fanous, Ayman H., Gareeva, Anna, Gawlik, Micha, Gejman, Pablo V., Gill, Michael, Glatt, Stephen J., Golimbet, Vera, Hong, Kyung Sue, Hultman, Christina M., Hyman, Steven E., Iwata, Nakao, Jönsson, Erik G., Kahn, René S., Kennedy, James L., Khusnutdinova, Elza, Kirov, George, Knowles, James A., Krebs, Marie-Odile, Laurent-Levinson, Claudine, Lee, Jimmy, Lencz, Todd, Levinson, Douglas F., Li, Qingqin S., Liu, Jianjun, Malhotra, Anil K., Malhotra, Dheeraj, McIntosh, Andrew, McQuillin, Andrew, Menezes, Paulo R., Morgan, Vera A., Morris, Derek W., Mowry, Bryan J., Murray, Robin M., Nimgaonkar, Vishwajit, Nöthen, Markus M., Ophoff, Roel A., Paciga, Sara A., Palotie, Aarno, Pato, Carlos N., Qin, Shengying, Rietschel, Marcella, Riley, Brien P., Rivera, Margarita, Rujescu, Dan, Saka, Meram C., Sanders, Alan R., Schwab, Sibylle G., Serretti, Alessandro, Sham, Pak C., Shi, Yongyong, St Clair, David, Stefánsson, Hreinn, Stefansson, Kari, Tsuang, Ming T., van Os, Jim, Vawter, Marquis P., Weinberger, Daniel R., Werge, Thomas, Wildenauer, Dieter B., Yu, Xin, Yue, Weihua, Holmans, Peter A., Pocklington, Andrew J., Roussos, Panos, Vassos, Evangelos, Verhage, Matthijs, Visscher, Peter M., Yang, Jian, Posthuma, Danielle, Andreassen, Ole A., Kendler, Kenneth S., Owen, Michael J., Wray, Naomi R., Daly, Mark J., Huang, Hailiang, Neale, Benjamin M., Sullivan, Patrick F., Ripke, Stephan, Walters, James T. R., and O’Donovan, Michael C.

Published

2022

42. Deficient prepulse inhibition in schizophrenia in a multi-site cohort: Internal replication and extension.

Author

Swerdlow, Neal R, Light, Gregory A, Thomas, Michael L, Sprock, Joyce, Calkins, Monica E, Green, Michael F, Greenwood, Tiffany A, Gur, Raquel E, Gur, Ruben C, Lazzeroni, Laura C, Nuechterlein, Keith H, Radant, Allen D, Seidman, Larry J, Siever, Larry J, Silverman, Jeremy M, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, and Braff, David L

Subjects

Humans, Gait Disorders, Neurologic, Antipsychotic Agents, Acoustic Stimulation, Analysis of Variance, Cohort Studies, Schizophrenia, Psychiatric Status Rating Scales, Neural Inhibition, Adolescent, Adult, Middle Aged, Female, Male, Young Adult, Endophenotypes, Prepulse Inhibition, Endophenotype, Prepulse inhibition, Replication, Startle, Clinical Research, Mental Health, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

BackgroundThe Consortium on the Genetics of Schizophrenia (COGS) collected case-control endophenotype and genetic information from 2457 patients and healthy subjects (HS) across 5 test sites over 3.5 years. Analysis of the first "wave" (W1) of 1400 subjects identified prepulse inhibition (PPI) deficits in patients vs. HS. Data from the second COGS "wave" (W2), and the combined W(1+2), were used to assess: 1) the replicability of PPI deficits in this design; 2) the impact of response criteria on PPI deficits; and 3) PPI in a large cohort of antipsychotic-free patients.MethodsPPI in W2 HS (n=315) and schizophrenia patients (n=326) was compared to findings from W1; planned analyses assessed the impact of diagnosis, "wave" (1 vs. 2), and startle magnitude criteria. Combining waves allowed us to assess PPI in 120 antipsychotic-free patients, including many in the early course of illness.ResultsANOVA of all W(1+2) subjects revealed robust PPI deficits in patients across "waves" (p

Published

2018

43. O2.8. TRAJECTORIES OF NEUROCOGNITIVE FUNCTIONING OVER TIME IN YOUTH AT CLINICAL HIGH RISK WHO DO AND DO NOT TRANSITION TO PSYCHOSIS

Author

Woodberry, Kristen, Stone, William S, Shapiro, Daniel I, Chokran, Cole M, Addington, Jean, Bearden, Carrie, Cadenhead, Kristin, Cannon, Tyrone D, Cornblatt, Barbara A, McGlashan, Thomas H, Mathalon, Daniel H, Perkins, Diana O, Tsuang, Ming T, Walker, Elaine F, Woods, Scott W, and Seidman, Larry J

Subjects

Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Abstract Background In spite of evidence for the premorbid and prodromal onset of cognitive deficits in schizophrenia and related psychotic disorders, there is some limited evidence to suggest that deficits may progress with psychosis onset. Cognitive remediation in youth at risk for psychosis is being touted as an opportunity not only to remediate deficits but to potentially prevent this progression. Yet trajectories of cognitive functioning over time remain poorly understood in youth at risk, including the degree to which age at assessment or illness onset, sociodemographic factors, or symptom progression influence these trajectories. Methods The North American Prodrome Longitudinal Study (NAPLS) -2 collected data on an extensive battery of neuropsychological (NP) tests at baseline, one year, two years, and post-conversion in a sample of clinical high risk (CHR) youth and healthy comparison (HC) subjects ages 12–35 (N= 960, 92% of the full sample) followed clinically for up to 2 years. NP data were available for 694 at CHR and 265 HC. Linear mixed effects analyses were used to test the effects of group, age, gender, age of onset, maternal education, and clinical outcome on cognitive trajectories. Results Those who transitioned to a psychotic disorder over the course of follow-up performed significantly below those who did not and well below healthy comparisons. Tasks reliant on attention, visual and auditory working memory, visuospatial and verbal memory, and processing speed best differentiated those who transitioned from those who did not at one year (Cohen’s d from -0.33 to -0.54). Discrepancies from normal functioning on these tests were generally large (Cohen’s d from -0.67 to -1.02) consistent with findings for first episode samples. Although clinical outcome was not associated with a significantly different trajectory over time on any cognitive domain, these are likely due to high rates of conversion in this sample within the first year. Predictors of different trajectories will be presented. Discussion These data from one of the largest CHR studies to date suggest that much of the neuropsychological dysfunction in major psychotic disorders is present early in the course of illness and prior to its full expression. However, trajectories are highly heterogeneous. More frequent assessment prior to and during the onset of illness are needed to fully understand the cognitive correlates of psychosis onset and the implications for early intervention.

Published

2018

44. O9.8. STRESS AND COGNITIVE FUNCTION AMONG INDIVIDUALS AT CLINICAL HIGH-RISK FOR PSYCHOSIS: FINDINGS FROM THE NAPLS COHORT

Author

Cullen, Alexis, Cadenhead, Kristin S, Addington, Jean, Bearden, Carrie E, Cannon, Tyrone, Cornblatt, Barbara A, Mathalon, Daniel, McGlashan, Thomas H, Perkins, Diana O, Seidman, Larry, Stone, William S, Tsuang, Ming, Woods, Scott W, and Walker, Elaine F

Subjects

Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Abstract Background Accumulated evidence from non-human animal studies suggests that the prominent deficits in memory and executive function that characterise individuals with psychosis may, at least in part, be due to the effects of stress on the brain regions that support these functions. However, studies of patients with established psychosis have yielded inconsistent findings with regards to the relationship between stress and cognition, and research in high-risk populations is notably lacking. Utilising data from the North American Prodrome Longitudinal Study 2 (NAPLS 2), we aimed to further elucidate the relationship between stress (daily stressors, life events, and childhood trauma) and cognitive function in clinical high-risk (CHR) individuals and healthy controls (HC). We additionally explored the role of potential mediators [hypothalamic-pituitary-adrenal (HPA) axis function] and moderators (group status, sex, family history of illness). Methods The sample comprised 885 participants (CHR=646; HC=239) who completed measures of stress and cognitive function at the NAPLS 2 baseline assessment. Stress measures included the Daily Stress Inventory and a modified version of the Psychiatric Epidemiology Research Interview Life Events Scale, both of which provided continuous measures of stress exposure (number of events) and distress (subjective feelings of distress). Participants were also interviewed using the Childhood Trauma and Abuse Scale to determine any exposure to childhood trauma (abuse, neglect, and bullying occurring prior to age 16 years). Basal HPA axis activity was determined via salivary cortisol samples obtained at the baseline assessment and standardised scores from selected subtests from the Measurement and Treatment Research to Improve Cognition in Schizophrenia (MATRICS) were used to derive two cognitive domain scores (memory and executive function). To examine relationships between stress and cognitive domain scores, linear regression analyses were performed on standardised variables. Results Daily stressor exposure, daily stressor distress, and life event exposure exhibited negative quadratic (i.e., inverted U-shaped) associations with both memory and executive function (P < 0.01 for all). In contrast, the reverse pattern (i.e., a negative linear relationship and a positive quadratic relationship) was shown in the model for life event distress and memory domain scores (P < 0.01) whilst trauma history showed only a trend-level association with poorer memory performance (P = 0.084). These relationships, which did not differ across CHR and healthy control groups, were largely unchanged after adjusting for demographic factors and salivary cortisol. Exploratory analyses suggested that trauma exposure and a family history of psychosis may moderate the relationship between daily stressors/life events and cognitive function. Discussion In this large sample of predominately CHR individuals, we observed that the association between stress and cognition is complex and differs across stressor types. The negative quadratic associations that we observed for daily stressor exposure, daily stressor distress, and life event exposure imply that whist lower levels of stress may facilitate memory and executive function, there may be a negative impact on cognition when these stressors become more frequent and distressing. Interventions aiming to minimise stress exposure and promote effective coping strategies might feasibly improve cognition in CHR individuals.

Published

2018

45. Examining the variability of neurocognitive functioning in individuals at clinical high risk for psychosis: a meta-analysis

Author

Catalan, Ana, Radua, Joaquim, McCutcheon, Robert, Aymerich, Claudia, Pedruzo, Borja, González-Torres, Miguel Ángel, Baldwin, Helen, Stone, William S., Giuliano, Anthony J., McGuire, Philip, and Fusar-Poli, Paolo

Published

2022

46. 451. Group Iterative Multiple Model Estimation Reveals Individuals at Clinical High-Risk for Psychosis and Healthy Comparisons Self-Organize by Premorbid Adjustment According to Patterns of Temporoparietal Brain Connectivity

Author

Aberizk, Katrina, primary, Ku, Benson S., additional, Addington, Jean M., additional, Bearden, Carrie E., additional, Cadenhead, Kristin S., additional, Cannon, Tyrone D., additional, Cornblatt, Barbara A., additional, Keshavan, Matcheri, additional, Mathalon, Daniel H., additional, Perkins, Diana O., additional, Stone, William S., additional, Tsuang, Ming T., additional, Woods, Scott W., additional, and Walker, Elaine F., additional

Published

2024

47. Association between residential instability at individual and area levels and future psychosis in adolescents at clinical high risk from the North American Prodrome Longitudinal Study (NAPLS) consortium

Author

Ku, Benson S., Addington, Jean, Bearden, Carrie E., Cadenhead, Kristin S., Cannon, Tyrone D., Compton, Michael T., Cornblatt, Barbara A., Keshavan, Matcheri, Mathalon, Daniel H., Perkins, Diana O., Stone, William S., Tsuang, Ming T., Walker, Elaine F., Woods, Scott W., and Druss, Benjamin G.

Published

2021

48. Enhancing attention and memory of individuals at clinical high risk for psychosis with mHealth technology

Author

Li, Huijun, Yang, Shuwen, Chi, Hongmei, Xu, Lihua, Zhang, Tianghong, Singleton, Gwendolyn, Tang, Yingying, Stone, William S., and Wang, Jijun

Published

2021

49. MK-Curve improves sensitivity to identify white matter alterations in clinical high risk for psychosis

Author

Zhang, Fan, Cho, Kang Ik Kevin, Tang, Yingying, Zhang, Tianhong, Kelly, Sinead, Biase, Maria Di, Xu, Lihua, Li, Huijun, Matcheri, Keshevan, Whitfield-Gabrieli, Susan, Niznikiewicz, Margaret, Stone, William S., Wang, Jijun, Shenton, Martha E., and Pasternak, Ofer

Published

2021

50. Concordance and factor structure of subthreshold positive symptoms in youth at clinical high risk for psychosis

Author

Calkins, Monica E., Woods, Scott W., Bearden, Carrie E., Liu, Lu, Moore, Tyler M., Cadenhead, Kristin S., Cannon, Tyrone D., Cornblatt, Barbara A., McGlashan, Thomas H., Perkins, Diana O., Seidman, Larry J., Tsuang, Ming T., Walker, Elaine F., Mathalon, Daniel H., Keshavan, Matcheri, Stone, William S., and Addington, Jean

Published

2021