Shock Syndromes I
ii.
Participants treated had more arrhythmias with dopamine than with norepinephrine. The
authors concluded that major changes to clinical practice are not needed but that selection of
vasopressors could be better individualized and could be based on clinical variables reflecting
hypoperfusion. This systematic review is limited by the small number of patients enrolled in
randomized studies of some agents (e.g., phenylephrine) and few studies with combination
therapy.
| d. | Angiotensin II is a novel vasopressor agent being evaluated for patients with vasodilatory shock. |
|---|
In a phase III study of patients with shock (the Angiotensin II for the Treatment of High-Output
Shock [ATHOS-3] study) (n=321) without evidence of a low CO (about 90% with sepsis), use
of angiotensin II, compared with placebo, more often led to a MAP response (MAP of 75 mm
Hg or greater or MAP increase of 10 mm Hg or greater, without an increase in open-label
vasopressor dose) at hour 3 (69.9% vs. 23.4%, p<0.001). Angiotensin II significantly reduced
the cardiovascular Sequential Organ Failure Assessment (SOFA) subscore at hour 48, but not
the total SOFA score. Patients in the angiotensin II group more often developed a thrombotic
event (12.9% vs. 5.1%, p=0.02), a new infection (30.1% vs. 19.0%, p=0.029), and delirium
(5.5% vs. 0.6%, p=0.036).
ii.
A post hoc analysis of patients from the ATHOS-3 study with acute kidney injury requiring
renal replacement therapy found that patients treated with angiotensin II had longer survival
(adjusted hazard ratio [HR] 0.44; 95% CI, 0.24–0.80) and were more likely to discontinue
renal replacement therapy within 7 days (adjusted HR 2.90; 95% CI, 1.29–6.52) than those
who received placebo.
iii.
One retrospective study evaluating angiotensin II use found that of the 270 included patients,
67% had a positive hemodynamic response 3 hours after its initiation. Of note, 92% of patients
were also receiving vasopressin at the time of angiotensin II initiation.
iv.
These evaluations suggest that angiotensin II is an effective vasopressor for patients with
vasodilatory shock, particularly in those with acute kidney injury, but outcomes-based studies
are needed before this agent is implemented into routine clinical practice.
Because of the increased risk of thrombosis associated with angiotensin II, concurrent venous
thromboembolism prophylaxis is recommended.
Levosimendan
In a study of patients with sepsis, adding blinded levosimendan for 24 hours compared with
placebo did not lead to a significant difference in the mean SOFA score (6.68 ± 3.89 vs. 6.06 ±
3.89, respectively, p=0.053). Mortality at 28 days also did not differ between the levosimendan
and placebo groups (34.5% vs. 30.9%, p=0.43). Patients in the levosimendan group more often
developed a supraventricular tachyarrhythmia (3.1% vs. 0.4%, p=0.04).
ii.
A study of levosimendan compared with placebo for 48 hours in patients with circulatory
shock after cardiac surgery was terminated early for futility. Thirty-day mortality did not
differ between the levosimendan and placebo groups (12.9% vs. 12.8%, p=0.97), nor did the
groups differ in duration of mechanical ventilation or incidence of cardiac arrhythmias.
iii.
These data suggest that levosimendan does not improve outcomes in patients with sepsis or
circulatory shock after cardiac surgery and should not be used in these patients.