| Literature DB >> 23375130 |
Jennifer R Murphy1, Caroline Rawdon, Ian Kelleher, Deirdre Twomey, Patrick S Markey, Mary Cannon, Richard Ap Roche.
Abstract
BACKGROUND: Deficits in the mismatch negativity (MMN) and P3a components are the most reliable and robust findings in schizophrenia. These abnormalities have also been recently documented in individuals clinically at risk for psychosis, indicating that the MMN may be a potential biomarker for psychosis. However, the at risk samples included in MMN studies are characterised by pre-existing clinical symptomatology and significant functional decline which are related to MMN amplitude. These factors may be potential confounds in determining whether deficient MMN is present prior to clinical manifestation of the disorder. Therefore, investigating the MMN in the extended psychosis phenotype comprising adolescents with psychotic symptoms from the general population may provide important information on whether abnormal MMN is apparent in the earliest stages of risk.Entities:
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Year: 2013 PMID: 23375130 PMCID: PMC3598448 DOI: 10.1186/1471-244X-13-45
Source DB: PubMed Journal: BMC Psychiatry ISSN: 1471-244X Impact factor: 3.630
Figure 1MMN and subsequent P3a activity across frontocentral scalp regions of the controls (blue) and the at risk (red) groups and reversed MMN/P3a polarity at the left and right temporal sites.
MMN/P3a mean amplitude (μV) and standard deviation values at frontal and temporal electrodes for each group
| ## | |||
|---|---|---|---|
| −1.24 μV (1.11) | −0.60 μV (1.07) | −0.59 (−0.28) | |
| −1.40 μV (1.17) | −0.38 μV (1.40) | −0.79 (−0.37) | |
| −1.24 μV (1.15) | −0.32 μV (1.90) | −0.59 (−0.28) | |
| −1.37 μV (0.87) | −0.79 μV (0.81) | −0.69 (−0.33) | |
| −1.09 μV (0.87) | −0.70 μV (1.20) | −0.37 (−0.19) | |
| −1.03 μV (1.05) | −0.80 μV (1.30) | −0.19 (−0.10) | |
| −0.91 μV (0.59) | −0.67 μV (0.72) | −0.36 (−0.18) | |
| −0.62 μV (0.73) | −0.52 μV (0.96) | −0.12 (−0.06) | |
| −0.60 μV (0.76) | −0.63 μV (1.09) | 0.03 (0.02) | |
| −1.56 μV (1.29) | −0.93 μV (0.98) | −0.55 (−0.27) | |
| −0.19 μV (0.66) | −0.22 μV (0.80) | 0.04 (0.02) | |
| −0.17 μV (0.74) | −0.42 μV (0.92) | 0.30 (0.15) | |
| 1.69 μV (1.08) | 0.93 μV (1.69) | 0.54 (0.26) | |
| 1.55 μV (1.14) | 0.71 μV (1.12) | 0.74 (0.35) | |
| 1.47 μV (1.00) | 1.25 μV (1.34) | 0.19 (0.09) | |
| 0.29 μV (0.84) | 0.81 μV (0.96) | −0.58 (−0.28) |
Note: Effect sizes are calculated as the standardised mean differences: ES = (Mean of at-risk group minus the mean of controls)/Pooled SD. ‘μV’ = microvolts.
The means and standard deviations of demographic variables overall and for each group
| 11.48 (.60) | 11.57 (.85) | 11.41 (.50) | ||
| 16 M; 20 F | 8 M; 6 F | 8 M; 14 F | ||
| 35 R; 5 L | 13 R; 1 L | 19 R; 3 L | ||
| N=34; 6 Other | N=11; 3 Other | N=19; 2 Other |
Note: SES=Socio-economic Status; Number of participant’s parents occupations in Professional/Managerial or Other roles.