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1. Differential trajectories of tobacco smoking in people at ultra-high risk for psychosis: Associations with clinical outcomes

2. Generalized neurocognitive impairment in individuals at ultra‐high risk for psychosis: The possible key role of slowed processing speed

3. No Effects of Cognitive Remediation on Cerebral White Matter in Individuals at Ultra-High Risk for Psychosis—A Randomized Clinical Trial

4. Social cognition in patients at ultra-high risk for psychosis: What is the relation to social skills and functioning?

5. Changes in negative symptoms are linked to white matter changes in superior longitudinal fasciculus in individuals at ultra-high risk for psychosis

6. Global fractional anisotropy predicts transition to psychosis after 12 months in individuals at ultra‐high risk for psychosis

7. Cognitive remediation plus standard treatment versus standard treatment alone for individuals at ultra-high risk of developing psychosis: Results of the FOCUS randomised clinical trial

8. Widespread higher fractional anisotropy associates to better cognitive functions in individuals at ultra‐high risk for psychosis

9. Generalized neurocognitive impairment in individuals at ultra-high risk for psychosis: The possible key role of slowed processing speed

11. Are attenuated positive symptoms and cortisol levels associated?

12. Baseline measures of cerebral glutamate and GABA levels in individuals at ultrahigh risk for psychosis:Implications for clinical outcome after 12 months

13. Pre-training inter-rater reliability of clinical instruments in an international psychosis research project

14. Multiple measures of HPA axis function in ultra high risk and first-episode schizophrenia patients

15. Patterns of white matter microstructure in individuals at ultra-high-risk for psychosis: associations to level of functioning and clinical symptoms

16. T18. EFFECTS OF COGNITIVE REMEDIATION ON WHITE MATTER IN INDIVIDUALS AT ULTRA-HIGH RISK FOR PSYCHOSIS – A RANDOMIZED, CONTROLLED CLINICAL TRIAL

17. Negative symptoms mediate the relationship between neurocognition and function in individuals at ultrahigh risk for psychosis

18. Cerebral Glutamate and Gamma-Aminobutyric Acid Levels in Individuals at Ultra-high Risk for Psychosis and the Association With Clinical Symptoms and Cognition

19. Gender differences of patients at-risk for psychosis regarding symptomatology, drug use, comorbidity and functioning – Results from the EU-GEI study

20. Interview and questionnaire assessment of cognitive impairment in subjects at ultra-high risk for psychosis: Associations with cognitive test performance, psychosocial functioning, and positive symptoms

21. Premorbid adjustment in individuals at ultra-high risk for developing psychosis: a case-control study

22. Systemic oxidative DNA and RNA damage are not increased during early phases of psychosis: A case control study

23. EFFECTIVENESS OF DIALECTICAL BEHAVIOR THERAPY VERSUS COLLABORATIVE ASSESSMENT AND MANAGEMENT OF SUICIDALITY TREATMENT FOR REDUCTION OF SELF-HARM IN ADULTS WITH BORDERLINE PERSONALITY TRAITS AND DISORDER-A RANDOMIZED OBSERVER-BLINDED CLINICAL TRIAL

24. T46. THE EFFECT OF COMPREHENSIVE COGNITIVE REMEDIATION IN INDIVIDUALS AT ULTRA-HIGH RISK FOR PSYCHOSIS: A SINGLE-BLIND, RANDOMISED, CLINICAL TRIAL (FOCUS)

25. T97. PATTERNS OF COGNITIVE FUNCTION ARE UNIQUELY ASSOCIATED WITH WHITE MATTER-MICROSTRUCTURE IN INDIVIDUALS AT ULTRA-HIGH RISK FOR PSYCHOSIS

26. White matter maturation during 12 months in individuals at ultra-high-risk for psychosis

27. SA81. Glutamatergic and GABAergic Disturbances in Individuals at Ultra-High Risk of Psychosis: Implications for Clinical and Functional Outcome

28. Examining speed of processing of facial emotion recognition in individuals at ultra-high risk for psychosis: Associations with symptoms and cognition

29. Psychopathology and social functioning of 42 subjects from a Danish ultra high-risk cohort

30. Social cognition in patients at ultra-high risk for psychosis: What is the relation to social skills and functioning?

31. Premorbid adjustment in individuals at ultra-high risk for developing psychosis: a case-control study

32. The FOCUS trial: cognitive remediation plus standard treatment versus standard treatment for patients at ultra-high risk for psychosis: study protocol for a randomised controlled trial

33. Poster #S227 REMEMBERING DAILY COGNITIVE FUNCTIONING IN SUBJECTS AT ULTRA-HIGH RISK FOR PSYCHOSIS: A CROSS-SECTIONAL STUDY ON EVERYDAY MANIFESTATIONS OF COGNITIVE DEFICITS IN AN ULTRA-HIGH RISK COHORT

34. Poster #S174 STRESS, CORTISOL AND PITUITARY VOLUME DURING PSYCHOSIS

35. Poster #T124 CLINICAL AND BRAIN STRUCTURAL PREDICTORS OF ‘TRANSITION TO PSYCHOSIS’ OR ‘RISK REMISSION’ IN INDIVIDUALS AT ULTRA HIGH-RISK FOR SCHIZOPHRENIA

36. Poster #T106 PSYCHOPATHOLOGY, LEVEL OF FUNCTIONING AND SOCIOECONOMIC STATUS: A DESCRIPTIVE STUDY OF 42 SUBJECTS FROM AN ULTRA HIGH-RISK COHORT

39. Impact of Comorbid Affective Disorders on Longitudinal Clinical Outcomes in Individuals at Ultra-high Risk for Psychosis

40. Obsessive-Compulsive Symptoms and Other Symptoms of the At-risk Mental State for Psychosis

41. Clinical, cognitive and neuroanatomical associations of serum NMDAR autoantibodies in people at clinical high risk for psychosis The EUGEI High-Risk Study

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