| Literature DB >> 25472859 |
Robyn Langdon1, Michael H Connors2, Megan Still3, Philip B Ward4, Stanley Catts5.
Abstract
BACKGROUND: People with chronic psychosis often display theory of mind impairments that are not fully accounted for by other, more general neurocognitive deficits. In these patients, both theory of mind and neurocognitive deficits contribute to poor functioning, independently of psychotic symptoms. In young people with recent-onset psychosis, however, it is unclear the extent to which theory of mind impairment is independent of neurocognitive deficits. The primary aim of this study was to examine the evidence for specific theory of mind impairments in early psychosis. A secondary aim was to explore the relations between theory of mind, neurocognition, symptom severity, and functional outcomes.Entities:
Mesh:
Year: 2014 PMID: 25472859 PMCID: PMC4263012 DOI: 10.1186/s12888-014-0316-6
Source DB: PubMed Journal: BMC Psychiatry ISSN: 1471-244X Impact factor: 3.630
Demographics of patients and controls
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|---|---|---|---|
| Males:females | 22:1 | 17:2 | χ2(1) = .599 |
| Age (years) | 20.91 ± 1.83 (18-25) | 20.79 ± 1.81 (17-24) |
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| Education (years) | 11.43 ± 2.02 (8-18) | 12.82 ± 1.94 (9-16) |
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| IQ | 96.65 ± 8.41 | 103.42 ± 9.32 |
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| Age of illness onset (years) | 19.91 ± 1.95 (16-24) | ||
| Duration of illness (weeks) | 50.74 ± 29.50 (12-104) | ||
| SAPS Positive Symptoms | 1.25 ± .94 (0.00-3.75) | ||
| SANS Negative Symptoms | 2.18 ± .72 (0.60-3.80) | ||
| Social Functioning | 50.87 ± 12.12 (30-80) | ||
| Quality of Life | 58.22 ± 22.78 (20-120) | ||
Note. Data expressed as means ± SD (range in parentheses). *p < .05. Positive and negative symptoms assessed using the Scales for the Assessment of Positive and Negative Symptoms of Schizophrenia (SAPS and SANS: Andreasen, 1983, 1984). The overall Positive and Negative rating is the average of global ratings on the SAPS and SANS respectively (‘0’ = absent; ‘1’ = questionable; ‘2’ = mild; ‘3’ = moderate; ‘4’ = marked; ‘5’ = severe).
Differences between patients and controls in ToM and neurocognition
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|---|---|---|---|
| ToM | −1.60 ± 2.16 | 1.94 ± 1.04 | 6.55** |
| Picture sequencing | 4.80 ± 1.19 | 5.87 ± .28 | 3.81** |
| Joke appreciation | 1.26 ± .47 | 1.90 ± .27 | 5.23** |
| Story comprehension | .72 ± .31 | 1.19 ± .27 | 5.17** |
| Neurocognition | −3.66 ± 3.77 | 4.21 ± 3.89 | 6.57** |
| IQ | 96.65 ± 8.41 | 103.42 ± 9.32 | 2.47* |
| Visual memory | 16.78 ± 3.26 | 19.84 ± 2.73 | 3.25** |
| Verbal memory | 26.39 ± 15.76 | 54.21 ± 13.44 | 6.08** |
| Verbal fluency | 28.00 ± 9.29 | 44.58 ± 13.47 | 4.71** |
| Semantic fluency | 32.43 ± 9.45 | 56.95 ± 12.94 | 7.09** |
| Inhibition | 32.30 ± 9.88 | 23.24 ± 5.92 | 3.49** |
| Set-Shifting | -.17 ± .93 | .20 ± .50 | 1.54 |
| Planning | 60.26 ± 7.84 | 55.63 ± 6.79 | 2.02 |
Note. Data expressed as means ± SD. *p < .05, **p < .01.
Figure 1Patients’ deficits in ToM and different neurocognitive domains relative to controls.
Zero-order correlations between ToM, neurocognition, symptom severity, and social functioning in patients
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|---|---|---|---|---|---|---|
| ToM |
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| -.01 | .26 | .16 | |
| Neurocognition |
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| −.06 |
| .30 | |
| Negative symptoms |
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| .18 |
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| Positive symptoms | -.01 | -.06 | .18 | .02 | -.09 | |
| Quality of Life | .26 |
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| .02 |
| |
| Social Functioning | .16 | .30 |
| -.09 |
|
Note. *p < .05, **p < .01.
Summary of hierarchical regression analyses predicting social functioning and quality of life in early psychosis patients
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|---|---|---|---|---|
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| .09 | |||
| Neurocognition | .30 | 1.39 | .18 | |
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| .09 | |||
| Neurocognition | .34 | 1.12 | .28 | |
| ToM | -.07 | .21 | .83 | |
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| .30 | |||
| Neurocognition | .20 | .70 | .49 | |
| ToM | -.22 | .76 | .46 | |
| Negative symptoms | -.53 | 2.30 | .03* | |
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| .29 | |||
| Neurocognition | .53 | 2.83 | .01 | |
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| .29 | |||
| Neurocognition | .60 | 2.22 | .04 | |
| ToM | -.09 | .33 | .74 | |
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| .42 | |||
| Neurocognition | .48 | 1.89 | .08 | |
| ToM | -.21 | .81 | .43 | |
| Negative symptoms | -.42 | 2.00 | .06! | |
*p < .05; ! p < .10.