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

2. Sex differences in clinical presentation in youth at high risk for psychosis who transition to psychosis.

3. Sampling from different populations: Sociodemographic, clinical, and functional differences between samples of first episode psychosis individuals and clinical high-risk individuals who progressed to psychosis.

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

5. Auditory N100 amplitude deficits predict conversion to psychosis in the North American Prodrome Longitudinal Study (NAPLS-2) cohort.

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

7. Perceptual pathways to hallucinogenesis.

8. Three prominent self-report risk measures show unique and overlapping utility in characterizing those at clinical high-risk for psychosis.

10. North American Prodrome Longitudinal Study (NAPLS 3): Methods and baseline description.

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

12. 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.

14. Visual cortical plasticity and the risk for psychosis: An interim analysis of the North American Prodrome Longitudinal Study.

15. Commentary. Toward a core outcomes assessment set for clinical high risk.

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

17. Persistent negative symptoms in youth at clinical high risk for psychosis: A longitudinal study.

18. Incorporating cortisol into the NAPLS2 individualized risk calculator for prediction of psychosis.

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

20. Social decline in the psychosis prodrome: Predictor potential and heterogeneity of outcome.

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

22. Progressive reconfiguration of resting-state brain networks as psychosis develops: Preliminary results from the North American Prodrome Longitudinal Study (NAPLS) consortium.

23. Modeling perception and behavior in individuals at clinical high risk for psychosis: Support for the predictive processing framework.

24. Predictive validity of conversion from the clinical high risk syndrome to frank psychosis.

25. Duration of the psychosis prodrome.

26. Impact of childhood adversity on corticolimbic volumes in youth at clinical high-risk for psychosis.

27. Adding a neuroanatomical biomarker to an individualized risk calculator for psychosis: A proof-of-concept study.

28. The Early Psychosis Screener for Internet (EPSI)-SR: Predicting 12 month psychotic conversion using machine learning.

29. Longitudinal changes in social cognition in individuals at clinical high risk for psychosis: An outcome based analysis.

30. Neurocognitive profiles in the prodrome to psychosis in NAPLS-1.

31. Metabolic abnormalities and low dietary Omega 3 are associated with symptom severity and worse functioning prior to the onset of psychosis: Findings from the North American Prodrome Longitudinal Studies Consortium.

32. Age-related trajectories of social cognition in youth at clinical high risk for psychosis: An exploratory study.

33. Latent class cluster analysis of symptom ratings identifies distinct subgroups within the clinical high risk for psychosis syndrome.

34. The Early Psychosis Screener (EPS): Item development and qualitative validation.

35. The Early Psychosis Screener (EPS): Quantitative validation against the SIPS using machine learning.

36. Exploration of clinical high-risk dropouts.

37. Depression and clinical high-risk states: Baseline presentation of depressed vs. non-depressed participants in the NAPLS-2 cohort.

38. Comorbid diagnoses for youth at clinical high risk of psychosis.

39. Ventricular enlargement and progressive reduction of cortical gray matter are linked in prodromal youth who develop psychosis.

40. Traumatic brain injury in individuals at clinical high risk for psychosis.

41. Healthy adolescent performance on the MATRICS Consensus Cognitive Battery (MCCB): Developmental data from two samples of volunteers.

42. The relations of age and pubertal development with cortisol and daily stress in youth at clinical risk for psychosis.

43. Social cognition over time in individuals at clinical high risk for psychosis: Findings from the NAPLS-2 cohort.

44. Severity of thought disorder predicts psychosis in persons at clinical high-risk.

45. Demographic correlates of attenuated positive psychotic symptoms.

46. Stress exposure and sensitivity in the clinical high-risk syndrome: initial findings from the North American Prodrome Longitudinal Study (NAPLS).

47. Movement abnormalities predict transitioning to psychosis in individuals at clinical high risk for psychosis.

48. Current status specifiers for patients at clinical high risk for psychosis.

49. Impact of substance use on conversion to psychosis in youth at clinical high risk of psychosis.

50. Social cognition as a mediator between neurocognition and functional outcome in individuals at clinical high risk for psychosis.

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