School of Medicine, University of California San Diego, 9500 Gilman Drive, La Jolla, CA 92093, United States.
Department of Psychiatry, University of California San Diego, 9500 Gilman Drive, La Jolla, CA 92093, United States.
Schizophr Res. 2024 Sep;271:186-193. doi: 10.1016/j.schres.2024.07.019. Epub 2024 Jul 19.
Individuals at Clinical High Risk (CHR) for psychosis or in their First Episode (FE) of psychosis are in a pivotal time in adolescence or young adulthood when illness can greatly impact their functioning. Finding relevant biomarkers for psychosis in the early stages of illness can contribute to early diagnosis, therapeutic management and prediction of outcome. One such biomarker that has been studied in schizophrenia (SZ) is visual contrast sensitivity (VCS). VCS can be used to differentiate visual information processing function in the magnocellular versus parvocellular visual pathways. Few studies have assessed VCS in early psychosis.
Participants included CHR (n = 68), FE psychosis (n = 34) and Healthy Comparison (HC) (n = 63). All were clinically assessed and completed a VCS paradigm that involved near threshold luminance and chromatic stimuli.
CHR and FE participants had lower VCS in the luminance condition (F[2166] = 3.42, p < 0.05) compared to HC. There was also a significant sex X group interaction (F[5163] = 4.3, p < 0.001) in the luminance condition (F[5163] = 4.3, p < 0.001) as FE males (p < 0.01) and CHR females (p < 0.01) had the greatest deficits compared to male and female HC participants respectively. VCS deficits in the luminance condition were associated with more thought disorder, slower processing speed, worse executive functioning and poor global functioning (r's 0.25-0.50, p < 0.05).
This study supports the hypothesis that there are deficits in visual information processing, particularly in tasks that emphasize the magnocellular pathway, in patients experiencing early psychosis. VCS therefore has the potential to be used as a biomarker in this population.
处于精神病临床高风险(CHR)或精神病首发期(FE)的个体正处于青春期或成年早期的关键时期,此时疾病可能极大地影响他们的功能。在疾病的早期阶段寻找精神病的相关生物标志物可以促进早期诊断、治疗管理和预后预测。在精神分裂症(SZ)中研究过的一种生物标志物是视觉对比敏感度(VCS)。VCS 可用于区分大细胞与小细胞视觉通路中的视觉信息处理功能。很少有研究评估早期精神病中的 VCS。
参与者包括 CHR(n=68)、FE 精神病(n=34)和健康对照组(HC)(n=63)。所有人都经过临床评估,并完成了一项涉及近阈值亮度和色度刺激的 VCS 范式。
CHR 和 FE 参与者的亮度条件下的 VCS 较低(F[2166]=3.42,p<0.05),与 HC 相比。在亮度条件下,还存在显著的性别 x 组交互作用(F[5163]=4.3,p<0.001)(F[5163]=4.3,p<0.001),因为 FE 男性(p<0.01)和 CHR 女性(p<0.01)与男性和女性 HC 参与者相比,VCS 缺陷最大。亮度条件下的 VCS 缺陷与更多的思维障碍、较慢的加工速度、较差的执行功能和较差的整体功能相关(r 值为 0.25-0.50,p<0.05)。
本研究支持这样一种假设,即处于早期精神病的患者存在视觉信息处理缺陷,特别是在强调大细胞通路的任务中。因此,VCS 有可能成为该人群的生物标志物。
