Abstract
Objectives: Developmentally specified measures that identify clinically salient irritability are needed for early school-age youth to meaningfully capture this transdiagnostic risk factor for psychopathology. Thus, the current study modeled the normal:abnormal irritability spectrum and generated a clinically optimized screening tool for this population. Methods: The irritability spectrum was modeled via the youth version of the Multidimensional Assessment Profile Scales—Temper Loss Scale (MAPS-TL-Youth) in children (n = 474; 6.0–8.9 years) using item response theory (IRT). Both cross-cutting core irritability items from the early childhood version and new developmentally specific items were included. Items uniquely associated with impairment were identified and used to derive a brief, clinically optimized irritability screener. Longitudinal data were then utilized to test the predictive utility of this clinically optimized screener in preadolescence (n = 348; 8.0–12.9 years). Results: Most children exhibit irritability regularly, but daily occurrence was rare. Of the top 10 most severe items from the IRT analyses, 9 were from the developmentally specific items added for the MAPS-TL Youth version. Two items associated with concurrent impairment were identified for the clinically optimized irritability screener (“Become frustrated easily” and “Act irritable”). The MAPS-TL-Youth clinically optimized screener demonstrated good sensitivity (69%) and specificity (84%) in relation to concurrent DSM 5 irritability-related diagnoses. Youth with elevated scores on the screener at early school age (ESA) had more than 7x greater odds of irritability-related psychopathology at pre-adolescence. Conclusions: The MAPS-TL-Youth characterized the developmental spectrum of irritability at ESA and a clinically optimized screener showed promise at predicting psychopathology risk. Rigorous testing of clinical applications is a critical next step.
Original language | English (US) |
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Article number | e1985 |
Journal | International Journal of Methods in Psychiatric Research |
Volume | 32 |
DOIs | |
State | Published - Nov 2023 |
Funding
The authors gratefully acknowledge the contribution of Erica Anderson (Northwestern University) for outstanding oversight of clinical measurements. The MAPS study was supported by NIMH grants: R01MH082830, 2U01MH082830 to Lauren Wakschlag and U01MH090301 to Margaret Briggs-Gowan. The other authors received no additional funding that contributed to this work. The funder (NIH) had no role in the design or conduct of the study. The authors gratefully acknowledge the contribution of Erica Anderson (Northwestern University) for outstanding oversight of clinical measurements. The MAPS study was supported by NIMH grants: R01MH082830, 2U01MH082830 to Lauren Wakschlag and U01MH090301 to Margaret Briggs‐Gowan. The other authors received no additional funding that contributed to this work. The funder (NIH) had no role in the design or conduct of the study.
Keywords
- assessment
- developmental psychopathology
- pediatric irritability
ASJC Scopus subject areas
- Psychiatry and Mental health