AI Article Synopsis

  • - The study investigates how negative symptoms in individuals at clinical high risk (CHR) for psychosis change over time, hypothesizing that these changes are not linear and vary by clinical subgroups.
  • - Using data from 699 participants, the research found that negative symptoms improved significantly in the first six months but became more stable afterwards, with different clinical subgroups showing unique patterns of symptom change.
  • - The findings suggest the importance of closely monitoring negative symptoms in CHR, emphasizing that the first six months of treatment are crucial and that identifying clinical subgroups early can guide tailored treatment strategies.

Article Abstract

Background And Hypothesis: Negative 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 Design: Linear, curvilinear, and stepwise growth curve models, with and without moderators, were fitted to negative symptom ratings from the NAPLS-3 CHR dataset ( = 699) and within clinical subgroups.

Study Results: Negative 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.

Conclusions: Continuous, 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.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10287168PMC
http://dx.doi.org/10.1093/schizbullopen/sgad014DOI Listing

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