Shock Syndromes I
ii.
A systematic review and fixed-effect meta-analysis of albumin compared with alternative fluids
for resuscitation in patients with sepsis found an association between albumin use and lower
mortality (OR 0.82; 95% CI, 0.67–1.0; p=0.047). The benefit of albumin was retained when the
analysis was restricted to crystalloids as the comparator (OR 0.78; 95% CI, 0.62–0.99; p=0.04).
These data should be interpreted with caution, however, because many of the included studies
had poor methodological quality, and when a random-effects model was used, the results for
the overall analysis were not statistically significant (OR 0.84; 95% CI, 0.69–1.02, p=0.08).
iii.
These data have renewed interest in 4%–5% albumin as a resuscitation fluid for patients with
sepsis and septic shock. As such, the 2021 SSC guidelines suggest albumin as a component
of the fluid resuscitation regimen when patients require a substantial amount of crystalloids.
Hydroxyethyl starch solutions should not be used for fluid resuscitation.
Compared with patients with sepsis allocated to lactated Ringer’s solution, those allocated to
pentastarch (a hydroxyethyl starch formulation) had a significantly higher incidence of acute
renal failure (34.9% vs. 22.8%, p=0.002) and need for renal replacement therapy (31.0% vs.
18.8%, p=0.001), with no difference in 28-day mortality (26.7% vs. 24.1%, p=0.48).
ii.
Compared with patients with sepsis randomized to receive Ringer’s acetate solution, patients
with sepsis randomized to receive hydroxyethyl starch had a significantly higher 90-day
mortality (51% vs. 43%, p=0.03) and need for renal replacement therapy (22% vs. 16%, p=0.04).
iii.
The increased need for renal replacement therapy and lack of mortality benefit in these studies
led to the strong recommendation against the use of hydroxyethyl starch for fluid resuscitation
in patients with sepsis and septic shock in the 2021 SSC guidelines.
Hyperoncotic (20%–25%) albumin replacement may be beneficial in patients with septic shock.
An open-label study compared the replacement of albumin (with 20% albumin) to a goal serum
albumin concentration of 3 g/dL plus crystalloid solution administration with the administration
of crystalloid solution alone in patients with sepsis or septic shock. The albumin and crystalloid
groups did not differ in the incidence of 28-day mortality (31.8% vs. 32.0%, p=0.94), but patients
allocated to albumin had a shorter time to cessation of vasoactive agents (median 3 vs. 4 days,
p=0.007). A post hoc subgroup analysis of patients with septic shock at enrollment showed that
those randomized to albumin had a lower 90-day mortality rate (RR 0.87; 95% CI, 0.77–0.99); 90-
day mortality did not differ in patients without septic shock (RR 1.13; 95% CI, 0.92–1.39; p=0.03
for heterogeneity). Of note, this post hoc subgroup analysis was performed on the secondary end
point of 90-day mortality, and an analysis of the primary outcome of 28-day mortality was not
reported. These data suggest that albumin replacement does not improve outcomes in patients with
sepsis but that it has hemodynamic (and potentially mortality) advantages in patients with septic
shock. Hence, the role of albumin replacement in patients with septic shock warrants further study.
Norepinephrine is the recommended first-line vasoactive medication. A meta-analysis of
randomized trials that compared norepinephrine with dopamine for the treatment of septic shock
found a higher risk of short-term mortality (RR 1.12; 95% CI, 1.01–1.20; p=0.035) and arrhythmias
(RR 2.34; 95% CI, 1.46–3.77; p=0.001) in patients allocated to dopamine.
The optimal approach to using vasoactive agents and inotropes beyond the choice of initial
vasopressor is unclear, but the choice should be based on patient-specific clinical factors.
Potential interventions could include using norepinephrine monotherapy (with appropriate
dose escalation) or initiating an additional therapy (i.e., a second catecholamine vasopressor,
arginine vasopressin (AVP), corticosteroids, an inotrope, or a combination of these therapies).
ii.
The optimal time or norepinephrine dose at which to consider additional therapies is unknown.
A dose that constitutes the failure of norepinephrine is not well defined in the literature, and
the maximal doses used by clinicians (or institutions) are variable and often subjective.