The ACTH Response to Dexamethasone in PTSD

Twenty-nine men and nine women age 23 to 79 years (mean=54.47 years, SD=17.27) participated in the study. Recruitment was through advertisements placed in local newspapers or on bulletin boards around the Mount Sinai Hospital and the Bronx Veterans Affairs (VA) Medical Center requesting volunteers (including comparison subjects) for one of several research projects examining hormonal responses following extremely stressful life events. All procedures were approved by the institutional review boards at the Mount Sinai School of Medicine and the Bronx VA Medical Center, and all subjects provided written informed consent before their participation. Data on cortisol and glucocorticoid receptors from 16 of the current subjects (10 with PTSD, six without PTSD) have been previously reported (13).

Subjects were included in the study if they had an axis I diagnosis of PTSD or if they were free from a current or past history of PTSD or any other axis I disorder. Subjects with PTSD were excluded if they had comorbid substance abuse or dependence, bipolar disorder, psychosis, or obsessive-compulsive disorder but not if they were suffering from a unipolar mood disorder or other anxiety disorder (i.e., major depressive disorder, dysthymia, generalized anxiety disorder, panic disorder, social phobia, or agoraphobia). Gulf War veterans and adult children of Holocaust survivors were recruited for study, but their data were not included in the current analyses, as they will be presented elsewhere. Thirty subjects were excluded because of having had a major medical, endocrinological, or neurological illness and/or receiving standing doses of psychotropic agents or other medications likely to affect the HPA axis. Of the 38 subjects included, 21 subjects were not taking any medications. None of the remaining 17 subjects was receiving standing doses of psychotropic medications, but three were taking as-needed sedatives for sleep (i.e., zolpidem or trazodone). Examples of the other common medications that were not exclusionary were lipid-lowering agents, histamine-2 blockers, and nonsteroidal anti-inflammatory agents. Subjects were not withdrawn from medications for the purpose of study participation. As the study was conducted primarily at a VA medical center, the study group was predominantly male and does not reflect the typical predominance of women in epidemiologic samples of PTSD patients.

Information about lifetime traumatic life events and the ages at which these events occurred was obtained by using the Trauma History Questionnaire (14). The most disturbing experience reported by an individual was defined as the “focal” event and formed the basis of an interview for PTSD using the Clinician-Administered PTSD Scale (15). At this time, events were reviewed to determine whether they met the DSM-IV criterion A involving both 1) potential life threat or threat to physical integrity and 2) subjective distress (e.g., fear, helplessness, horror). In the group with PTSD, the focal events were combat-related events involving witnessing death and mutilation or experiencing mortal danger (N=10), traumatic separation from parents in early childhood (N=2), witnessing mass execution (N=1), torture (N=1), gunshot wound (N=1), rape in adulthood (N=1), attempted strangulation (N=1), domestic violence (N=1), and childhood physical abuse (N=1). Fifteen of the 19 subjects without PTSD reported experiencing potentially traumatic events, as evidenced by positive responses on one or more items of the Trauma History Questionnaire (e.g., mugging, assault, motor vehicle accident), and six of these reported events qualified as criterion A traumatic experiences (i.e., serious motor vehicle accident, combat, intruder with weapon in home, boat accident, near drowning in friend’s pool, and losing a friend in the World Trade Center bombing on 9/11). However, no subject endorsed current or lifetime symptoms sufficient or severe enough to qualify for any psychiatric diagnosis, including adjustment disorder or acute stress disorder. Thus, even with the inclusion of the subjects exposed to traumatic events, this comparison group constituted a homogenous group of symptom-free individuals.

Other axis I diagnoses were made by using the Structured Clinical Interview for DSM-IV (16). The diagnostic interviews were conducted by a trained psychologist (S.L.H.) or psychiatrist (J.A.G., L.M.B.) with established interrater reliability, and the diagnoses were reviewed at a consensus conference by clinicians blind to the biological data.

Baseline blood samples were obtained at 8:00 a.m. before dexamethasone administration for the determination of cortisol and ACTH levels. The participants ingested an oral dose of 0.5 mg of dexamethasone at 11:00 p.m., and blood samples for determination of cortisol, ACTH, and dexamethasone levels were obtained at 8:00 a.m. on the day following dexamethasone ingestion.

Plasma cortisol levels were determined by radioimmunoassay, as previously described (17). The intra-assay and interassay coefficients of variation were 4.0% and 6.8%, respectively. ACTH levels were assayed by using a commercially available kit (IncStar, Stillwater, Minn.). The intra-assay and interassay coefficients of variation were 4.7% and 7.1%, respectively. Dexamethasone levels were measured by using commercially available antibodies (IgG Corp., Nashville, Tenn.) according to a previously published method (18). The intra- and interassay coefficients of variation for dexamethasone were 8.0% and 9.0%, respectively.

The results of the DST for ACTH and cortisol are expressed as both postdexamethasone hormonal levels and percentage suppression, i.e., 100 × [(predexamethasone hormone – postdexamethasone hormone) / predexamethasone hormone].

Group differences in cortisol and ACTH levels and in ACTH-to-cortisol ratios were examined by using analysis of variance (ANOVA) or covariance (ANCOVA). For the primary analyses comparing the hormonal responses to dexamethasone of the two groups, repeated-measures ANCOVA was used with the within-subjects factor being day (i.e., pre- or postdexamethasone). The hormone values were substantially kurtotic for predexamethasone cortisol (kurtosis=4.90) and for postdexamethasone ACTH (kurtosis=6.27); the former kurtosis likely reflects an extremely low predexamethasone cortisol level in the non-PTSD group, and the latter reflects a floor effect in response to dexamethasone administration. Therefore, the natural logarithms of both the pre- and postdexamethasone hormone values were used in all analyses, with the exception of calculations of percent suppression of ACTH and cortisol following dexamethasone administration. The raw data, however, will also be reported so that they can be compared to other observations in the literature.

The difference of two logarithms is equivalent to the logarithm of their ratio. Therefore, testing the effect of day (pre- versus postdexamethasone) in the repeated-measures analysis is equivalent to examining whether the log-transformed ratio of pre- to postdexamethasone ACTH or cortisol levels is significantly different from zero and, accordingly, provides the relative change in ACTH and cortisol values, respectively, from pre- to postdexamethasone. Analyses of the interactions of day with between-subjects variables are equivalent to tests of group differences in the respective log-transformed pre- to postdexamethasone ratios (i.e., they represent group differences in the relative change, respectively, in ACTH and cortisol following dexamethasone). Tests of the interactions of day with covariates in the analyses are equivalent to regression analyses of the logarithms of ratios.

Before analyses for the purpose of hypothesis testing were performed, initial analyses to identify potential confounds in the data were undertaken. Age, ethnicity, gender, medication status, weight, height, body mass index, diagnosis of major depression, and plasma dexamethasone level were tested individually for association with both the raw and log-transformed biological outcome measures. This screening process revealed a significant gender effect for the predexamethasone ACTH level (F=10.28, df=1, 36, p=0.003) and for both the raw (F=4.41, df=1, 36, p=0.05) and log-transformed (F=14.62, df=1, 36, p=0.001) postdexamethasone ACTH levels, justifying the use of gender as a covariate in analyses of ACTH and of the ACTH-to-cortisol ratio. None of the other variables assessed showed a significant association with the biological variables. For medication status in particular, receiving any medication at all was not significantly associated with the raw or log-transformed cortisol or ACTH level or with the ACTH-to-cortisol ratio, either at baseline or after dexamethasone administration (for all analyses, F≤1.69, df=1, 36, p≥0.20). The use of sedatives was similarly not significantly associated with any of the aforementioned hormonal values (in all cases, F≤0.68, df=1, 36, p≥0.41). A diagnosis of major depression was not significantly associated with any of the preceding variables for the group as a whole (in all cases, F≤2.30, df=1, 36, p≥0.14) or for the subgroup with PTSD (in all cases, F≤2.86, df=1, 17, p>0.10). Thus, neither major depressive disorder nor medication status was used as a covariate.

Lastly, the plasma dexamethasone level was not found to correlate significantly with either the raw or log-transformed value of ACTH (respectively, r=–0.16, p=0.34, and r=–0.22, p=0.19, covaried for gender, df=35) or cortisol (r=–0.01, p=0.98, and r=–0.07, p=0.69, N=38). However, the plasma concentration of dexamethasone differed significantly between the subjects with and without PTSD (F=4.87, df=1, 36, p=0.04) (Table 1); therefore, dexamethasone level was used as a covariate in all analyses involving postdexamethasone hormone values. Pearson’s correlations and partial correlations controlling for gender and, where appropriate, for dexamethasone level were performed to assess relationships among the biological measures and between these measures and symptom severity assessments.

Demographic characteristics of the subjects are reported in Table 1. Nineteen participants met the diagnostic criteria for PTSD. Eleven of those meeting criteria for PTSD also had a comorbid diagnosis of major depressive disorder (N=9), dysthymia (N=2), or another anxiety disorder (N=5). The ethnic groups included Caucasian (N=23), African American (N=10), Hispanic (N=3), and Asian (N=2). The participants in the groups with and without PTSD were comparable in age (F=0.01, df=1, 36, n.s.), gender (χ²=0.15, df=1, n.s.), ethnic distribution (Caucasian versus other, χ²=2.75, df=1, n.s.), and medication status (χ²=0.11, df=1, n.s.) (Table 1). Not surprisingly, there were significant group differences in PTSD symptom severity as measured by the intrusive (F=87.92, df=1, 36, p<0.0005), avoidance (F=162.92, df=1, 36, p<0.0005), and hyperarousal (F=126.36, df=1, 36, p<0.0005) subscales of the Clinician-Administered PTSD Scale as well as the total scale (F=202.73, df=1, 36, p<0.0005) and the Mississippi PTSD Scale (F=69.52, df=1, 33, p<0.0005).

ACTH responses to dexamethasone are illustrated in Figure 1, grouped by presence or absence of PTSD diagnosis; group means are presented in Table 1. Repeated-measures ANCOVA of pre- and postdexamethasone ACTH levels revealed a significant group-by-day interaction (F=13.17, df=1, 34, p=0.001), demonstrating a greater reduction of ACTH following dexamethasone ingestion in individuals with than without PTSD. In this within-subject analysis, neither gender nor plasma dexamethasone level was a significant covariate. When the results were expressed as the percentage of suppression of ACTH, one-way ANCOVA demonstrated a significant main effect of group (F=12.59, df=1, 34, p=0.001), reflecting significantly greater dexamethasone-induced suppression of ACTH in the PTSD group. Again, neither gender nor dexamethasone level was a significant covariate.

With respect to cortisol, repeated-measures ANCOVA similarly demonstrated a significant group-by-day interaction (F=7.29, df=1, 35, p=0.02), indicating a greater reduction in cortisol following dexamethasone ingestion in individuals with than without PTSD. Plasma dexamethasone level was not a significant covariate in the interaction with day. When these relationships were expressed as the percentage of cortisol suppression, one-way ANCOVA demonstrated a significant main effect of group (F=5.08, df=1, 35, p=0.04), without a significant effect of plasma dexamethasone level.

In order to estimate adrenal responsiveness in PTSD, we examined the ACTH-to-cortisol ratios before and after dexamethasone administration. Repeated-measures ANCOVA revealed no significant main effect of day (F=0.00, df=1, 34, n.s.) or of group (F=0.44, df=1, 34, n.s.) and no significant group-by-day (F=0.04, df=1, 34, n.s.) or gender-by-day (F=0.22, df=1, 34, n.s.) interaction. However, the between-subjects analysis showed gender to be a significant covariate (F=13.90, df=1, 34, p=0.001) because of the lower predexamethasone ACTH-to-cortisol ratio in women (mean=1.05, SD=1.03; N=9) than in men (mean=2.87, SD=1.88; N=29). Dexamethasone level was not a significant covariate.

To further explore this gender effect, we performed a two-way ANOVA and ANCOVA, with both PTSD and gender as main effects, on the pre- and postdexamethasone ACTH-to-cortisol ratios, respectively. Results for both the basal ACTH-to-cortisol ratio (F=16.42, df=1, 34, p<0.0005) and the postdexamethasone ACTH-to-cortisol ratio (F=8.31, df=1, 33, p=0.007) showed significant main effects for gender, but neither demonstrated a significant group effect, and dexamethasone level was not a significant covariate in the postdexamethasone analysis. Finally, we examined the possibility of a gender-by-group interaction in a two-way repeated-measures analysis of pre- and postdexamethasone ACTH-to-cortisol ratios, which demonstrated only a between-subjects main effect of gender (F=13.34, df=1, 33, p=0.001) (i.e., for the average of the pre-and postdexamethasone ratios) without evidence of a significant PTSD effect, PTSD-by-gender interaction, or association with dexamethasone level as a covariate. There was no significant between-subjects effect of day or interaction with day.

Correlations were used to examine associations among log-transformed biological measures, between these biological variables and the severity of PTSD symptoms, and between percentage suppression of ACTH or cortisol and symptom severity. There were significant associations between pre- and postdexamethasone cortisol levels (r=0.49, df=35, p=0.002), with dexamethasone concentration controlled for, and between pre- and postdexamethasone ACTH levels (r=0.59, df=34, p<0.0005), with gender and dexamethasone level controlled for. Additionally, postdexamethasone ACTH and cortisol levels were significantly correlated (r=0.42, df=34, p=0.02), with gender and dexamethasone level controlled for. In contrast, the predexamethasone ACTH and cortisol levels were not significantly correlated (r=0.10, df=35, n.s.), with gender effects controlled for. Percentage of ACTH suppression was significantly correlated with percentage of cortisol suppression (r=0.42, df=34, p=0.01), with gender and dexamethasone level controlled for.

Table 2 shows correlations between the biological variables and severity of PTSD symptoms for the 34 subjects who had been exposed to at least one potentially traumatic event and were interviewed with the Clinician-Administered PTSD Scale. Postdexamethasone ACTH and cortisol levels, but not predexamethasone values, were significantly correlated with PTSD symptoms. Both percentage of ACTH suppression and percentage of cortisol suppression were significantly correlated with severity of PTSD as represented by scores on the Mississippi PTSD Scale and the Clinician-Administered PTSD Scale. Neither the pre- nor postdexamethasone ACTH-to-cortisol ratio was significantly correlated with symptom severity (data not shown).