Abstract
Psychological distress persisting for weeks or more promotes pro-inflammatory immune dysregulation, a risk factor for a range of chronic diseases. We have recently shown that mindfulness training reduces distress among university students. Here we present an exploratory trial to study immune dysregulation in a cohort of students who were exposed to progressively greater stress as the exam period approached, and to explore whether mindfulness training mitigated this dysregulation. Healthy University of Cambridge students were randomised to join an 8-week mindfulness course (N = 27), or to mental health support as usual (N = 27). Psychological distress, immune cell proportions, cytokines, CRP and serum cortisol were measured at baseline and during the exam period. Increased distress was associated with statistically significant increases in the proportion of B cells, regardless of trial arm (*p = 0.027). There were no other associations between any of the measured parameters, distress or mindfulness. Our finding that the proportion of B cells increases with psychological distress supports the findings of other studies. However, we found no evidence that mindfulness training is able to buffer the effects of psychological distress on healthy participants’ immune system. In order to detect these effects, should they exist, larger randomised trials will be required.
Highlights
Psychological distress persisting for weeks or more promotes pro-inflammatory immune dysregulation, a risk factor for a range of chronic diseases
Regardless of whether the students underwent mindfulness training or not, several immune parameters were significantly increased across the whole cohort during the exam period when compared with the baseline measurements
A potential confounding factor lies in the season of sampling; all baseline measurements were collected in January whereas the exam period measurements were collected in June
Summary
Psychological distress persisting for weeks or more promotes pro-inflammatory immune dysregulation, a risk factor for a range of chronic diseases. Psychological distress, immune cell proportions, cytokines, CRP and serum cortisol were measured at baseline and during the exam period. Our finding that the proportion of B cells increases with psychological distress supports the findings of other studies. The effects of stress on immune function are thought to be mediated in part by the steroid hormone cortisol which may increase during psychological distress. Modulation of immune function by cortisol and other hormones could be mediated by direct interaction with immune cells or sympathetic nervous system fibres[7], or indirectly by dysregulating the production of cytokines[5,8,9]. Several studies have demonstrated shifts in favour of Th2 cytokine imbalance in response to stress[11,12]
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