A high mean arterial pressure target is associated with improved microcirculation in septic shock patients with previous hypertension: a prospective open label study

This was a single-center, prospective, open-label study conducted in the intensive care unit of a tertiary care teaching hospital. The study protocol was approved by the Ethics Committee (Approval Number: 2011ZDllKY03.0) of Zhongda Hospital, School of Medicine, Southeast University, and informed consent was given by each patient or their next of kin.

Trial registration: Clinicaltrials.gov NCT01443494; registered 28 November 2011.

Patients admitted to the intensive care unit who met the following inclusion criteria were enrolled in the study: 1) patients with septic shock for less than 24 hours with a history of previous hypertension (septic shock was defined by the 2001 SCCM/ESICM/ACCP/ATS/SIS International Sepsis Definitions Conference [17]); 2) fluid resuscitation was performed according to the guidelines for treating septic shock to maintain the central venous pressure (CVP) at more than 8 mmHg and central venous oxygen saturation at more than 70%; 3) patients required norepinephrine (NE) to maintain a MAP of 65 mmHg. All patients were treated with mechanical ventilation, and received infusions of morphine and propofol. All patients had an arterial catheter and a central venous catheter in place.

Exclusion criteria were: pregnancy; age <18 years; inability to acquire the usual level of MAP; refusal of consent by the patient or relative; participation in other trials during the last 3 months; and hypertensive patients without antihypertensive therapy.

As chronic hypertensive patients are supposed to have undergone more blood pressure measurements in daily life than normotensive patients, the average MAP acquired from a patient’s physical examination records over the last 2 years was taken to be the target MAP. If the medical records were incomplete, a detailed enquiry about the target MAP to their next of kin was performed. In addition, age, gender, duration of shock prior to inclusion, Acute Physiology And Chronic Health Evaluation II score, intensive care unit length of stay, in-hospital mortality, source of infection and comorbidities were also recorded.

After stabilization for 30 minutes, basal measurements including hemodynamic and microcirculatory measurements were taken 20 minutes apart, and the NE doses were increased to titrate MAP to the target level. Patients were allowed to stabilize for 30 minutes before new measurements were taken. Thus, there was 50 minutes between the baseline and the second measurement. During the process, no other changes in treatment were allowed. The decision to stop the research was made by the treating intensivist according to predetermined safety limits for each patient. The detailed safety limits are reported in Additional file 1.

Serial measurements of NE dose, MAP, heart rate and CVP were performed. Noninvasive bioreactance cardiac output and stroke volume monitoring were obtained using the NICOM system (Cheetah Medical, Portland, OR, USA). Arterial and central venous gases were obtained to determine arterial pH, hemoglobin, lactate, arterial partial pressure of oxygen, arterial partial pressure of carbon dioxide, arterial hemoglobin saturation, arterial oxygen partial pressure to fractional inspired oxygen ratio and central venous hemoglobin saturation.

Measurements of the sublingual microcirculation were obtained using sidestream dark field (SDF; Microscan, Microvision Medical, Amsterdam, The Netherlands). The SDF probe was placed under the sublingual area without pressure after removal of secretions. Video sequences of 20 seconds each were recorded from three different sublingual sites. These images were stored and later renumbered by an identifier blinded to the clinical course. Videos were converted to the AVI (audio video interleaved) file format with video processing software, and analysis for each image was performed by two different investigators. Finally, all the variables were averaged to yield a single value for statistical analysis. The microcirculatory flow index (MFI), based on determination of the predominant type of flow in four quadrants for small vessels and total vessels, was determined with a semi-quantitative methodology. Flow was characterized as no flow = 0, intermittent = 1, sluggish = 2, and continuous = 3, to reflect blood velocity, identical to that described in consensus conference recommendations [18]. MFI was calculated for all quadrants of the image and averaged for each sublingual site. Detailed methods are reported in Additional file 2.

Statistical analysis of the data was performed using SPSS 16.0 (IBM, Somers, NY, USA). Histograms and normal-quantile plots were examined and Kolmogorov-Smirnov test was performed to verify the normality of the distributions of the data. Data are presented as the mean ± SD if normally distributed or median (interquartile range) if not normally distributed. Categorical variables are presented as number and percentage. For continuous data, paired t test or Wilcoxon signed-rank test were used. Differences were considered significant at P < 0.05.