Introduction: Dysregulation of the hypothalamus-pituitary-adrenal (HPA) axis is known to occur in bipolar disorder patients. Cortisol awakening response (CAR), a pronounced increase in cortisol level that peaks at approximately 30 to 40 minutes after waking in the morning, is an indicator of the function of HPA axis. Literature on the cortisol level in patients with bipolar disorder at different disease status (e.g. acute episode vs. remission) and controls are few and did not report consistent findings. Moreover, there are only one prior study examined the CAR level in bipolar disorder patients. The goal of the present study is to examine the level of CAR in bipolar disorder patients at different disease status (acute episode vs. partial remission) and severity while compared with controls. Additionally, we measured detailed variables that previous studies suggest to have influence on the CAR level. Methods: Data were collected from 27 hospitalized bipolar disorder patients (15 in manic and 12 in depressive episode) at different disease status (acute episode and partial remission). In addition, 25 healthy controls were recruited. Saliva samples were collected at the time of awakening (T0), 30, and 45 minutes after awakening to determine the CAR; the CAR indicators including delta and AUCi (area under the curve respect to cortisol increase) were calculated. Episodic symptom severity was measured using 17-item Hamilton Depression Rating Scale (HAMD) and Young Mania Rating Scale (YMRS). Covariates including demographic, sleep variables and clinical variables were measured. Student t-test was used to examine the differences in comparing patients to controls or different patient groups. The CAR differences between episodes and partial remission within the same patient was examined by Paired t-test. We calculated Pearson correlation for the relationship between CAR levels and symptom severity. Moreover, the associations between independent variables (i.e. CAR indexes), dependent variables (e.g. patient/control) and covariates were examined by tetrachroic correlation between categorical variables, biserial correlation between categorical variables and continuous variables and Pearson correlation between continuous variables. Results: We found a lower level of CAR in patients and the CAR distinguishes healthy controls from bipolar depressive patients despite of the disease status (either in acute or partial remission). Additionally, patients in depressive episode seem to exhibit a blunted CAR, and this phenomenon changes to be normal at partial remission. The CAR levels were no different between episode and partial remission in both bipolar-mania and bipolar-depression patients and no association were found between symptom severity and the CAR levels (r= -0.32 to -0.36, p>0.05). The variable, whether sleep lower than 6 hours at night, exhibited significant correlations with the CAR indexes either in acute or partial remission data points (r=0.31 to 0.39). Conclusion: The CAR can distinguish healthy controls from bipolar depressive patients. Depressive patients with acute episode exhibit a blunted CAR and a normal CAR while in recovery. These findings could assist to design further studies to investigate the regulation mechanisms of the HPA axis in bipolar disorder.