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1. Proteomic Biomarkers for the Prediction of Transition to Psychosis in Individuals at Clinical High Risk: A Multi-cohort Model Development Study.

2. Machine learning based prediction and the influence of complement – Coagulation pathway proteins on clinical outcome: Results from the NEURAPRO trial

3. Evidence that complement and coagulation proteins are mediating the clinical response to omega-3 fatty acids: A mass spectrometry-based investigation in subjects at clinical high-risk for psychosis

4. The association of plasma inflammatory markers with omega-3 fatty acids and their mediating role in psychotic symptoms and functioning: An analysis of the NEURAPRO clinical trial

5. The association between migrant status and transition in an ultra-high risk for psychosis population

6. Supplementation with the omega-3 long chain polyunsaturated fatty acids: Changes in the concentrations of omega-3 index, fatty acids and molecular phospholipids of people at ultra high risk of developing psychosis

7. Comparison of erythrocyte omega-3 index, fatty acids and molecular phospholipid species in people at ultra-high risk of developing psychosis and healthy people

9. Cognitive functioning in ultra-high risk for psychosis individuals with and without depression: Secondary analysis of findings from the NEURAPRO randomized clinical trial

10. The NEURAPRO Biomarker Analysis: Long-Chain Omega-3 Fatty Acids Improve 6-Month and 12-Month Outcomes in Youths at Ultra-High Risk for Psychosis

11. Trajectories of symptom severity and functioning over a three-year period in a psychosis high-risk sample: A secondary analysis of the Neurapro trial

13. Neurocognition as a predictor of transition to psychotic disorder and functional outcomes in ultra-high risk participants: Findings from the NEURAPRO randomized clinical trial

14. Clinical trajectories in the ultra-high risk for psychosis population

17. Opening the Black Box of Cognitive-Behavioural Case Management in Clients with Ultra-High Risk for Psychosis

18. Urgent call for research into imagery rescripting to reduce suicidal mental imagery: clinical research considerations.

21. Effects of omega-3 polyunsaturated fatty acid supplementation on cognitive functioning in youth at ultra-high risk for psychosis: secondary analysis of the NEURAPRO randomised controlled trial

22. Evidence that complement and coagulation proteins are mediating the clinical response to omega-3 fatty acids:A mass spectrometry-based investigation in subjects at clinical high-risk for psychosis

23. Distress Related to Attenuated Psychotic Symptoms:Static and Dynamic Association With Transition to Psychosis, Nonremission, and Transdiagnostic Symptomatology in Clinical High-Risk Patients in an International Intervention Trial

24. Twelve-Month Cognitive Trajectories in Individuals at Ultra-High Risk for Psychosis:A Latent Class Analysis

25. Machine learning based prediction and the influence of complement – Coagulation pathway proteins on clinical outcome:Results from the NEURAPRO trial

26. NEURAPRO‐E study protocol: a multicentre randomized controlled trial of omega‐3 fatty acids and cognitive‐behavioural case management for patients at ultra high risk of schizophrenia and other psychotic disorders

27. Effect of ω-3 Polyunsaturated Fatty Acids in Young People at Ultrahigh Risk for Psychotic Disorders: The NEURAPRO Randomized Clinical Trial

28. Machine learning based prediction and the influence of complement - coagulation pathway proteins on clinical outcome: results from the NEURAPRO trial

30. Twelve-Month Cognitive Trajectories in Individuals at Ultra-High Risk for Psychosis: A Latent Class Analysis

32. Characterization and prediction of clinical pathways of vulnerability to psychosis through graph signal processing

34. Author response: Characterization and prediction of clinical pathways of vulnerability to psychosis through graph signal processing

35. Characterization and prediction of clinical pathways of vulnerability to psychosis through graph signal processing

36. Prediction of clinical outcomes beyond psychosis in the ultra-high risk for psychosis population

37. Omega‐3 fatty acids and neurocognitive ability in young people at ultra‐high risk for psychosis

38. Corrigendum: Relationship Between Polyunsaturated Fatty Acids and Psychopathology in the NEURAPRO Clinical Trial (Frontiers in Psychiatry, (2019), 10, 10.3389/fpsyt.2019.00393)

39. Supplementation with the omega-3 long chain polyunsaturated fatty acids:Changes in the concentrations of omega-3 index, fatty acids and molecular phospholipids of people at ultra high risk of developing psychosis

40. Cognitive functioning in ultra-high risk for psychosis individuals with and without depression:Secondary analysis of findings from the NEURAPRO randomized clinical trial

41. The NEURAPRO Biomarker Analysis:Long-Chain Omega-3 Fatty Acids Improve 6-Month and 12-Month Outcomes in Youths at Ultra-High Risk for Psychosis

42. Trajectories of symptom severity and functioning over a three-year period in a psychosis high-risk sample:A secondary analysis of the Neurapro trial

43. Corrigendum: Relationship between polyunsaturated fatty acids and psychopathology in the NEURAPRO clinical trial

44. Greater preference for eveningness is associated with negative symptoms in an ultra‐high risk for psychosis sample

45. Omega‐3 fatty acids and neurocognitive ability in young people at ultra‐high risk for psychosis

46. Prediction of clinical outcomes beyond psychosis in the ultra‐high risk for psychosis population

47. Characterization and Prediction of Clinical Pathways of Vulnerability to Psychosis through Graph Signal Processing

48. T34. THE IMPACT OF ANTIDEPRESSANT USE ON THE TRANSITION TO PSYCHOSIS RATE IN THE NEURAPRO TRIAL

49. Distress Related to Attenuated Psychotic Symptoms: Static and Dynamic Association With Transition to Psychosis, Nonremission, and Transdiagnostic Symptomatology in Clinical High-Risk Patients in an International Intervention Trial.

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