Does neuropsychological intraindividual variability index cognitive dysfunction, an invalid presentation, or both? Preliminary findings from a mixed clinical older adult veteran sample.

IF 1.8 4区心理学 Q3 CLINICAL NEUROLOGY

Journal of clinical and experimental neuropsychology Pub Date : 2024-08-01 Epub Date: 2024-08-09 DOI:10.1080/13803395.2024.2388096

Troy A Webber, Sara Lorkiewicz, Steven Paul Woods, Brian Miller, Jason R Soble

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引用次数: 0

Abstract

Introduction: Intraindividual variability across a battery of neuropsychological tests (IIV-dispersion) can reflect normal variation in scores or arise from cognitive impairment. An alternate interpretation is IIV-dispersion reflects reduced engagement/invalid test data, although extant research addressing this interpretation is significantly limited.

Method: We used a sample of 97 older adult (mean age: 69.92), predominantly White (57%) or Black/African American (34%), and predominantly cis-gender male (87%) veterans. Examinees completed a comprehensive neuropsychological battery, including measures of reduced engagement/invalid test data (a symptom validity test [SVT], multiple performance validity tests [PVTs]), as part of a clinical evaluation. IIV-dispersion was indexed using the coefficient of variance (CoV). We tested 1) the relationships of raw scores and "failures" on SVT/PVTs with IIV-dispersion, 2) the relationship between IIV-dispersion and validity/neurocognitive disorder status, and 3) whether IIV-dispersion discriminated the validity/neurocognitive disorder groups using receiver operating characteristic (ROC) curves.

Results: IIV-dispersion was significantly and independently associated with a selection of PVTs, with small to very large effect sizes. Participants with invalid profiles and cognitively impaired participants with valid profiles exhibited medium to large (d = .55-1.09) elevations in IIV-dispersion compared to cognitively unimpaired participants with valid profiles. A non-significant but small to medium (d = .35-.60) elevation in IIV-dispersion was observed for participants with invalid profiles compared to those with a neurocognitive disorder. IIV-dispersion was largely accurate at differentiating participants without a neurocognitive disorder from invalid participants and those with a neurocognitive disorder (areas under the Curve [AUCs]=.69-.83), while accuracy was low for differentiating invalid participants from those with a neurocognitive disorder (AUCs=.58-.65).

Conclusions: These preliminary data suggest IIV-dispersion may be sensitive to both neurocognitive disorders and compromised engagement. Clinicians and researchers should exercise due diligence and consider test validity (e.g. PVTs, behavioral signs of engagement) as an alternate explanation prior to interpretation of intraindividual variability as an indicator of cognitive impairment.

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神经心理学的个体内变异是认知功能障碍的指标，还是无效表现的指标，抑或两者兼而有之？来自临床老年退伍军人混合样本的初步研究结果。

简介神经心理测试中的个体内变异（IIV-离散性）可能反映了分数的正常变化，也可能源于认知障碍。另一种解释是，IIV-离散反映了参与度降低/测试数据无效，尽管针对这种解释的现有研究非常有限：我们使用了 97 名老年退伍军人样本（平均年龄：69.92 岁），他们主要是白人（57%）或黑人/非洲裔美国人（34%），主要是顺性别男性（87%）。作为临床评估的一部分，受试者完成了全面的神经心理测试，包括参与度降低/无效测试数据测量（一项症状有效性测试 [SVT]、多项表现有效性测试 [PVT]）。IIV 离散度使用方差系数（CoV）来表示。我们测试了：1）SVT/PVT 原始分数和 "失败 "与 IIV-离散度之间的关系；2）IIV-离散度与有效性/神经认知障碍状况之间的关系；3）IIV-离散度是否能利用接收器操作特征曲线区分有效性/神经认知障碍组：IIV-离散度与所选择的 PVTs 有明显的独立相关性，效应大小从很小到很大不等。与具有有效特征的认知功能未受损的参与者相比，具有无效特征的参与者和具有有效特征的认知功能受损的参与者的 IIV 分散性表现出中等到较大（d = .55-1.09）的升高。与有神经认知障碍的参与者相比，有无效特征的参与者的 IIV 分散性出现了小到中等程度（d = .35-.60）的升高，但并不显著。IIV-离散度在区分无神经认知障碍的参与者与无效参与者和有神经认知障碍的参与者方面基本准确（曲线下面积[AUCs]=.69-.83），而在区分无效参与者与有神经认知障碍的参与者方面准确性较低（AUCs=.58-.65）：这些初步数据表明，IIV-离散度可能对神经认知障碍和参与度降低都很敏感。临床医生和研究人员应恪尽职守，在将个体内变异性解释为认知障碍指标之前，应考虑测试的有效性（如PVTs、参与的行为迹象）作为替代解释。

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来源期刊

Journal of clinical and experimental neuropsychology 医学-临床神经学

CiteScore

3.20

自引率

4.50%

发文量

审稿时长

6-12 weeks

期刊介绍： Journal of Clinical and Experimental Neuropsychology ( JCEN) publishes research on the neuropsychological consequences of brain disease, disorders, and dysfunction, and aims to promote the integration of theories, methods, and research findings in clinical and experimental neuropsychology. The primary emphasis of JCEN is to publish original empirical research pertaining to brain-behavior relationships and neuropsychological manifestations of brain disease. Theoretical and methodological papers, critical reviews of content areas, and theoretically-relevant case studies are also welcome.