Detecting acute distress and risk of future psychological morbidity in critically ill patients: validation of the intensive care psychological assessment tool

The IPAT was adapted from the 18-item intensive care stress scale (ICUSS), previously created as a research tool for a prospective cohort study of intensive care psychological outcomes [2]. The ICUSS was derived from a comprehensive literature review of stressors and stress reactions in intensive care, and had four sub-scales: physical stress, delirious symptoms, control and support. Previous work showed that the ICUSS has good reliability, and concurrent and predictive validity [2].

To develop the IPAT, we added four mood-items to the ICUSS (the cohort study demonstrated that mood disturbance in critical care was one of the strongest risk factors for future psychological morbidity) and then shortened the resulting IPAT to fourteen items - communication, difficulty breathing, pain, sleep, anxiety, panic, depression, disorientation, delusions, hallucinations, intrusive memories, amnesia and self-reported psychological history. Items from ICUSS were selected for IPAT if they had significant medium to large correlation with ICUSS or mood scales and with at least one outcome (self-reported PTSD, depression and anxiety) in the cohort study, and satisfied NICE CG83 requirements [13]. Correlations of items selected for IPAT and concurrent stress or mood scores in the previous cohort study [2] ranged from r =0.42, P <0.01 to r =0.75, P <0.01. Correlation of items selected for IPAT and psychological outcomes in the cohort study ranged from r =0.25, P <0.01 to r =0.47, P <0.01. There are three possible responses for each item (no; yes a bit; yes a lot). Patients are asked to respond about feelings `since you’ve been in intensive care’. Data from the cohort study were useful to guide development of the IPAT, but further data were needed to validate it.

There are no definitive criteria for the required sample size in a validation study of this kind, as the properties of the items and their scalability are not known in advance. However, assuming a median inter-item correlation of around 0.3, and that items are reasonably well separated, a sample size of 100 patients is sufficient for the proposed analysis. As 3-month data were collected to test for predictive validity, a sample size of 150 was proposed to allow for a one-third loss to follow up.

The sample size requirement for test-retest reliability was based on the assumption that reliability would be around 0.8. For a sample size of 50 patients, the 95% confidence intervals of 0.70 to 0.87 allowed the rejection of the hypothesis that reliability was 0.8 if the observed reliability fell below 0.7 [23].

Sensitivity and specificity were derived for concurrent anxiety, depression and general distress in the critical care unit, as well as future risk of self-reported PTSD, and general psychological morbidity using coordinates on the receiver operating characteristic (ROC) curve, and the best cut point on the IPAT scale identified.

A sample of 166 patients was recruited (see Figure 1). After giving informed consent, the 166 patients completed IPAT once (day 1). The median time from critical care admission to assessment on day 1 was 6 days (IQR 7). Later on day 1, 161 (97%) of the patients completed the validation questionnaire. On day 2, 56 (34%) patients completed the IPAT a second time (a sample size of 50 was deemed sufficient for this purpose). Between the assessment in critical care and 3-month follow up, 28 (17%) patients died: 106 (77% of surviving patients) returned the follow-up questionnaire sent at 3 months.

Table 1 shows there were no significant differences in any baseline characteristics or on IPAT scores between patients in day 1, day 2 and follow-up samples. Additional clinical data (not in Table 1) showed that more than half of the total sample was mechanically ventilated, and opiates and sedation were commonly administered. Regarding psychological outcomes, the mean score on the PDS was 10 (SD 9) and on the CES-D 17 (SD 13).

Non-parametric Mokken-scale analysis (see Table 2) selected 10 of the 14 IPAT items as the components of a scale with reliability >0.8 (good). The ten items were hopelessness, tension, panic, delusions, intrusive memories, sadness, sleeplessness, communication difficulties, hallucinations and disorientation. The four excluded items were pain, difficulty breathing, amnesia for intensive care stay, and self-reported psychological history. This scale structure was also seen with day-2 IPAT data (reliability =0.8). All further analyses were carried out using the 10-item version of IPAT.

The correlation of IPAT total day-1 and IPAT total day-2 scores showed that test-retest reliability was 0.8. For the internal reliability for IPAT day-1 scores, Cronbach alpha = 0.8, and for IPAT day-2 scores, Cronbach alpha = 0.8.

Three doctors, three nurses and three patients returned a face-validity questionnaire. The IPAT scored 89% for face validity (nine people rated 10 items each; 80 out of 90 ratings were positive). The other 10 ratings were mostly `not sureʼ or suggestions for slight alterations to wording, rather than answering no. One patient, one nurse and one doctor indicated that all items had clear face validity. One patient, one nurse and one doctor indicated that 9 out of 10 items had clear face validity. Two patients, one nurse and one doctor indicated 8 items had clear face validity.

Table 3 shows that there were large significant correlations between IPAT anxiety and STAI anxiety scores measured on the same day, between IPAT depression and PHQ-2 depression scores the same day, and between total IPAT, STAI and PHQ-2 scores on the same day. There was medium significant correlation between previous CAM-ICU status and both IPAT total and IPAT delirious-symptom scores. Correlation was slightly increased when `likely deliriumʼ (combining additional observations of delirium with CAM-ICU results) was used.

With a cut point ≥7, the IPAT (day-1 data) had a sensitivity of 82% (95% CI 70, 91) and specificity of 65% (95% CI 55, 75) to detect concurrent anxiety in critical care patients. With the same cut point, the IPAT had 80% sensitivity (95% CI 68, 89) and 66% specificity (95% CI 55, 75) to detect concurrent low mood in critical care patients; and 75% sensitivity (95% CI 65, 84) and 74% specificity (95% CI 62, 83) to detect acute distress in critical care patients. The area under the curve (AUC) was 0.8 in all three cases.

In Table 4 we can see that there were highly significant correlations between IPAT total scores and the psychological outcomes of PTSD, depression and anxiety symptoms at 3 months. By Fisher’s z-transformation, none of the correlations between IPAT and other measures differed significantly between day 1 and day 2 (P >0.05). No significant relationships were found between CAM-ICU delirium results and psychological outcomes.

With a cut point ≥7, the IPAT (day-1 data) had 71% sensitivity (95% CI 49, 87) and 48% specificity (95% CI 37, 59) for future diagnosis of PTSD (AUC =0.6). With a cut point ≥7, the IPAT had 69% specificity (95% CI 55, 82) and 57% sensitivity (95% CI 43, 70) to predict future psychological morbidity (AUC =0.7).