Family-Focused Treatment for Adolescents and Young Adults at High Risk for Psychosis: Results of a Randomized Trial

Miklowitz, David J.; O’Brien, Mary P.; Schlosser, Danielle; Addington, Jean; Candan, Kristin; Marshall, Catherine; Domingues, I.; Walsh, Barbara C.; Zinberg, Jamie; Silva, Sandra D. De; Friedman‐Yakoobian, Michelle; Cannon, Tyrone D.

doi:10.1016/j.jaac.2014.04.020

Cited by 153 publications

(147 citation statements)

References 34 publications

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“…For example, Miklowitz et al [11] reported a reduction in positive symptoms of psychosis as a result of family interventions in conjunction with skills-based training for adolescents at risk for psychosis. They noted that the combination of teaching strategies for stress reduction and problem solving with increased family support and improved communication proved to be beneficial.…”

Section: Need For Research On Early Intervention and Preventionmentioning

confidence: 99%

Limitations of Research on Psychosis in Childhood and Adolescence:Current Controversies and Future Directions

McCarthy¹,

Libby²

2016

J Ment Disord Treat

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Section: Need For Research On Early Intervention and Preventionmentioning

confidence: 99%

Limitations of Research on Psychosis in Childhood and Adolescence:Current Controversies and Future Directions

McCarthy¹,

Libby²

2016

J Ment Disord Treat

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“…This hope of early actionable concerns has led investigators to push prevention research toward earlier and earlier points of development. In schizophrenia research, children or adolescents are treated at the point when familial risk and early symptoms converge (Miklowitz et al, 2014). In ASD research, high-risk populations such as younger siblings are tracked during infancy to identify the first warning signs of atypical trajectory that may in turn be treated incrementally from low-to high-intensity approaches as the specific trajectory and response of the child becomes clearer (Green et al, 2013).…”

Section: Are Behavioral Disorders Similar To Cancers More Treatablementioning

confidence: 99%

“…Although this group is at much heightened risk, the majority do not go on to receive a diagnosis within 2 years. Some promising data have emerged for the use of cognitivebehavioral therapy, family therapy, atypical antipsychotic medications, and omega 3 fatty acids to prevent progression to schizophrenia, but these initial findings are quite mixed and await replication (Marshall and Rathbone, 2011;Miklowitz et al, 2014). One concerning finding is that while some could potentially be protected from progressing to a psychotic disorder, all of those who are treated are exposed to side effects of medications, most notably weight gain because of atypical antipsychotic medications including risperidone and olanzapine (Marshall and Rathbone, 2011).…”

Section: The Earlier the Better? Risk Vs Impairment When Contemplatinmentioning

confidence: 99%

“…Unfortunately, outcomes measured 6-8 years after MTA study completion were not predicted by treatment in the randomized trial but were instead predicted by initial symptom trajectory, regardless of treatment (Molina et al, 2009). Longitudinal follow-up of promising short-term treatment studies, such as the recent Prevention Trial of Family-Focused Treatment in Youth at Risk for Psychosis (Miklowitz et al, 2014), is critical to understand the relationship between initial symptomatic response and meaningful long-term outcomes.…”

Section: Measurement Challenges: Differentiating Treatment Effects Frmentioning

confidence: 99%

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Intervention in the Context of Development: Pathways Toward New Treatments

Veenstra‐VanderWeele

Warren

2014

Neuropsychopharmacol

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Neuropsychiatric disorders vary substantially in age of onset but are best understood within the context of neurodevelopment. Here, we review opportunities for intervention at critical points in developmental trajectories. We begin by discussing potential opportunities to prevent neuropsychiatric disorders. Once symptoms begin to emerge, a number of interventions have been studied either before a diagnosis can be made or shortly after diagnosis. Although some of these interventions are helpful, few are based upon an understanding of pathophysiology, and most ameliorate rather than resolve symptoms. As such, in the next portion of the review, we turn our discussion to genetic syndromes that are rare phenocopies of common diagnoses such as autism spectrum disorder or schizophrenia. Cellular or animal models of these syndromes point to specific regulatory or signaling pathways. As examples, findings from the mouse models of Fragile X and Rett syndromes point to potential treatments now being tested in randomized clinical trials. Paralleling oncology, we can hope that our treatments will move from nonspecific, like chemotherapies thrown at a wide range of tumor types, to specific, like the protein kinase inhibitors that target molecularly defined tumors. Some of these targeted treatments later show benefit for a broader, yet specific, array of cancers. We can hope that medications developed within rare neurodevelopmental syndromes will similarly help subgroups of patients with disruptions in overlapping signaling pathways. The insights gleaned from treatment development in rare phenocopy syndromes may also teach us how to test treatments based upon emerging common genetic or environmental risk factors.

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“…Indeed, one of the primary motivations behind these changes was to encourage intervention in the prodromal phase of psychiatric disorders, with the aim of preventing progression (4). Support for this paradigm came partly from encouraging studies of early intervention in youth at risk of schizophrenia and other neuropsychiatric disorders (5)(6)(7)(8)(9). To identify patients who might benefit from intervention, the NIMH called for research into physiological biomarkers for psychiatric disease, particularly into neuroimaging biomarkers.…”

mentioning

confidence: 99%

Overdiagnosis in the Era of Neuropsychiatric Imaging

Nucifora¹

2015

Academic Radiology

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Family-Focused Treatment for Adolescents and Young Adults at High Risk for Psychosis: Results of a Randomized Trial

Cited by 153 publications

References 34 publications

Limitations of Research on Psychosis in Childhood and Adolescence:Current Controversies and Future Directions

Limitations of Research on Psychosis in Childhood and Adolescence:Current Controversies and Future Directions

Intervention in the Context of Development: Pathways Toward New Treatments

Overdiagnosis in the Era of Neuropsychiatric Imaging

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