It is important to appreciate that many of the IV fluids in clinical use today were introduced into practice at a time when clinical trials were not standard and, thus, not subjected to the same rigorous evaluation as current drug therapies. It was not until the twenty-first century that a systematic evaluation of IV fluids in clinical practice began. Landmark clinical trials have investigated the comparative effectiveness and safety of albumin (1, 2) and synthetic colloid fluids (3). More recently attention has turned to investigating the safety of “balanced” crystalloid solutions relative to 0.9% saline (4–6). Another aspect of the use of IV fluids which has recently come under investigation is the question of dose, both volume and rate of administration, particularly in the setting of sepsis and septic shock. Current international guidelines recommend at least 30 mL/kg of fluid within 3 h as first-line therapy for sepsis-induced hypoperfusion or septic shock (7). Following “adequate” fluid resuscitation, vasopressors, preferably noradrenaline, are recommended to correct persistent hypotension/hypoperfusion with initial infusion via the peripheral route to prevent delays in vasopressor administration. Nonetheless, the evidence underpinning guidelines for early hemodynamic resuscitation is of low quality and the recommendations are graded as weak, leading to clinical uncertainty. The question of fluid dose and the relationship with early vasopressor administration as initial resuscitation in patients with sepsis and septic shock is the focus of this review.

Sepsis is a clinical syndrome characterized by life-threatening organ dysfunction caused by a dysregulated host response to infection (8). Septic shock is a subset of sepsis where the underlying cellular and metabolic abnormalities are profound enough to substantially increase mortality. According to the Sepsis 3 definition, septic shock is identified clinically as sepsis with persistent hypotension requiring vasopressors to maintain a mean arterial blood pressure of ≥ 65 mm Hg and a serum lactate level > 2 mmol/L despite adequate volume resuscitation (8).

The role of fluids and vasopressors came to prominence following the publication of a landmark, small, single-center, randomized trial of a protocolized resuscitation strategy termed early goal-directed therapy (43). The trial reported a 16% absolute risk reduction in mortality associated with the use of a resuscitation protocol that emphasized the administration of large volumes of fluid targeted at achieving a specified central venous pressure goal, followed by the use of vasoactive medication to achieve blood pressure and a central venous oxygen saturation (ScvO₂) target. This resuscitation algorithm was subsequently adopted into international guidelines for the management of patients with septic shock (44). The results of this trial have not been replicated in multi-center studies. Three large trials conducted in the United States (45), Australia and New Zealand (46) and the United Kingdom (47), and an individual patient data meta-analysis that included a total of 3,723 trial participants in 138 centers did not confirm a reduction in morality with the use of early goal-directed therapy compared to usual care (48). There are a number of possible reasons for this. For example, the initial ScvO₂ was higher in the validation trials, however, direct comparison is problematic since this was measured at baseline in Rivers trial whereas the initial measurement in the validation studies occurred post-randomization, when initial fluid resuscitation and antimicrobials had already been delivered. What is demonstrated is that IV fluid resuscitation had been adopted into standard practice, and that mortality rates in all arms of the validation studies were lower than in the intervention arm of the Rivers trial (Table 1).

Importantly, there was significant variation in resuscitation practices across these three large trials. While the baseline characteristics of the included populations in the trials were similar with respect to age and markers of severity of illness such as APACHE II score and lactate levels (48), there were differences in fluid and vasopressor therapy. For example, approximately 21% of participants enrolled in the ARISE trial (46) were receiving vasopressors at baseline, compared to 3% in the PROMISE trial (47). Trial participants randomized to usual care in the PROCESS trial (45) received on average 500 mL more IV fluid compared to those randomized to usual care in the ARISE trial (46). This variation in processes of care highlights the possibility that therapeutic strategies with a different emphasis on fluid administration compared to vasopressors may be a target to improve mortality for patients with septic shock.

Liberal IV fluids with positive fluid balance in sepsis is associated with increased organ failure, intensive care length of stay and mortality (49, 50). Two randomized trials comparing liberal vs. conservative intravenous fluid resuscitation in children (51) and adults (52) with sepsis in Africa showed increased mortality in the treatment arms receiving higher IV fluid volumes, with the excess mortality being due to persistent shock (53). Potential mechanisms of harm relate to edema, hemodilution, exacerbation of endothelial glycocalyx shedding, reflex vasodilatation, release of natriuretic peptides and the flushing of inflammatory mediators from previously closed capillary beds. In line with this, recent experimental data suggests that fluid resuscitation preceding the start of vasopressors is associated with higher lactate levels and a paradoxical increase in vasopressor requirements when compared with an immediate start of vasopressor therapy without previous fluid administration (54). It is important to acknowledge important differences in population (high prevalence of malaria, anemia, HIV infection) and resources (limited healthcare infrastructure, lack of access to critical care) which prevent translation to high income countries. Nevertheless, several observational studies also suggest that increased volume of resuscitation fluids and net positive fluid balance is associated with mortality in sepsis (55–57).

Observational and pre-clinical data support the hypothesis that IV fluid restriction during the resuscitation phase for septic shock patients, and maintenance of organ perfusion with vasopressors, may improve outcomes via an altered host inflammatory response (54, 58–60). The reduction in the host inflammatory response may be mediated by several mechanisms, including; (1) increased cardiac output by vasoconstriction-mediated increased preload, moving fluid from unstressed to stressed circulation (61) and by improving myocardial contractility (62); (2) increased microcirculatory perfusion in septic shock (63–66), especially when the baseline microcirculatory blood flow is abnormal (67) and; (3) improved regional distribution of blood flow (54). It is important to consider that the optimal strategy for fluid restriction may differ between individuals, and rather than a fixed volume approach, this should be tailored to the individual requirements across the different phases of care including initial resuscitation, optimization, stabilization and ultimately fluid elimination (68).

The purported advantages of restrictive fluid practices, in combination with earlier vasopressors, include more rapid restoration of blood pressure and organ perfusion, reduced tissue edema and decreased endothelial injury and acute renal injury associated with rapid fluid bolus administration. As noted previously, initiation of noradrenaline improves cardiac output via increased preload from increasing the volume of the stressed circulation and increasing myocardial contractility, as well as its effect as a peripheral vasoconstrictor (61).

Laboratory models of sepsis have shown improved mortality associated with the early administration of norepinephrine in septic shock (54). In a propensity matched cohort of 186 ICU patients with septic shock, Ospina-Tascon et al. reported that early vasopressors (<1 h) vs. delayed initiation (>1 h) was associated with a separation in total IV fluids at 6 h (900 vs. 2,000 mL, P < 0.001) and net fluid balance at 24 h (3,905 vs. 5,400 mL, P < 0.001) (67). Decreased mortality was also reported with early initiation (hazard ratio 0.31, 95% confidence intervals 0.17–0.57, P < 0.001). Similarly, Bai et al. found increased mortality in patients with septic shock when norepinephrine was commenced more than 3 h after the onset of shock (odds ratio 2.16, 95%confidence intervals 1.23–3.81, P = 0.0007) (69). Conversely, in a large, observational study evaluating a state-wide sepsis protocol in patients presenting to the emergency department (ED), in-hospital mortality was not associated with time to completion of an initial fluid bolus (30 mL/kg) up to 12 h after presentation (50). It is important to note, however, that any conclusions drawn from observational and retrospective studies are limited by factors such as indicator bias and unknown/unmeasured confounders and high quality, large-scale randomized clinical trials are required.

Traditionally vasoactive drugs have required to be administered via a central venous line, generally in an intensive care setting. This poses a practical and logistical barrier to early initiation of vasopressors. The potential risks associated with peripheral administration need to be balanced against harms associated with delay to restoring adequate perfusion. Several observational studies point to the safety of peripheral administration of vasopressors, at least during the first few hours (70). In the ARISE EGDT trial, vasopressors were initiated via a peripheral cannula in 42% of cases which was associated with a shorter time to commencement (71).

Several small, randomized, pilot studies evaluating a conservative fluid approach have demonstrated the feasibility and safety of a restrictive fluid resuscitation strategy combined with earlier vasopressors in septic shock. An association with improved clinical outcomes compared with usual care has also been reported (72–74). The REFRESH trial evaluated restricted fluids and early vasopressors vs. usual care for initial resuscitation in 99 patients with sepsis-induced hypotension within 8 Australian ED. Fluid separation at 6 h was achieved (30 vs. 43 mL/kg, P < 0.001). The restricted fluid strategy was also associated with a shorter time to vasopressor initiation [34 (interquartile range 15–88) min vs. 150 (interquartile range 63–224) min] and an increased proportion of patients receiving a vasopressor within the ED (72 vs. 47%, P = 0.011) (72). Similarly, a small, single-center randomized trial of restricted fluids for 72 h after ED presentation with septic shock demonstrated decreased IV fluid resuscitation volumes compared to usual care (73); albeit no mortality differences were observed in either the REFRESH or RIFTS trial. Of note, the double-blind, randomized CENSER trial reported decreased cardiovascular complications (new-onset arrhythmia and cardiogenic pulmonary edema) and a trend to decreased 28-day mortality with an early fixed dose of norepinephrine for 24 h (0.05μg/kg/min) vs. standard care after presentation to the ED with sepsis-induced hypotension (75).

A large, multicentre, randomized trial of fluid restriction vs. standard fluid therapy in 1,554 patients admitted to ICU with septic shock (within 12 h of onset) has recently been conducted (Conservative vs. liberal fluid therapy in septic shock; CLASSIC) (76). Fluid separation after 1 day was minus 813 mL (median) in the restrictive vs. standard care group and minus 1,627 mL after 5 days. Ninety-day mortality was not different between treatment groups (42.3 vs. 42.1%); in the pre-specified sub-group stratified according to pre-randomized fluid volume, no heterogenous treatment effect was observed between the group receiving ≥ 30 mL/kg and those patients receiving < 30 mL/kg.

Notably, patients in CLASSIC required receipt of a vasopressor or inotropic agent to meet study eligibility and the intervention was not confined to the first 6–24 h after presentation; rather, the resuscitation strategy was delivered for the duration of the ICU stay. In contrast, there are 2 large multicentre, randomized trials currently evaluating a restricted fluids strategy compared to usual care wherein the intervention period is limited to the early resuscitation period (24 h) in patients presenting to the ED with sepsis-induced hypotension; CLOVERS (United States NCT03434028) and ARISE-FLUIDS (Australia and New Zealand, NCT04569942). The planned sample size for CLOVERS was 2,320 patients with the primary outcome being hospital mortality censored at 90-days. Enrolment was recently closed for futility following the second interim analysis. The ARISE FLUIDS is actively recruiting with a planned sample size of 1,000 patients and a primary outcome of days alive out-of- hospital to 90 days. A third, large, randomized trial, EVIS (United Kingdom NCT05179499) in 3,286 patients with septic shock is evaluating whether an early peripheral vasopressor infusion targeted to a mean arterial pressure > 65 mm Hg for 48 h improves survival to 30-days compared to usual care. The results of all three trials is eagerly awaited and will undoubtedly inform the early hemodynamic resuscitation of patients presenting to the ED with septic shock, particularly the initial fluid volume and the timing of vasopressors.

The Surviving Sepsis Campaign guidelines recommend at least 30 mL/kg of fluid within 3 h as first-line therapy for sepsis-induced hypoperfusion or septic shock with the subsequent introduction of vasopressors. The evidence underpinning these guidelines is low quality and the recommendations are, accordingly, graded as weak. A growing body of evidence suggests that initial hemodynamic resuscitation with a restrictive fluid approach, combined with earlier vasopressors, may improve clinical outcomes, including mortality. Several large-scale, multicentre trials are currently evaluating such a strategy. High quality evidence from these trials will inform both bedside clinicians and future international guidelines. Until then, the optimal fluid dose and the timing of vasopressors remains uncertain.

All authors listed have made a substantial, direct, and intellectual contribution to the work, and approved it for publication.