Harrison's Hour - Sepsis Bundle 2016
Harrison's Hour - Sepsis Bundle 2016
Harrison's Hour - Sepsis Bundle 2016
THE THIRD INTERNATIONAL CONSENSUS DEFINITIONS FOR SEPSIS AND SEPTIC SHOCK (SEPSIS-3)
Sepsis life-threatening organ dysfunction caused by a dysregulated host response to infection
(For clinical operationalization, organ dysfunction can be represented by an increase in the Sequential [Sepsis-related] Organ
Failure Assessment / SOFA score of 2 points or more, which is associated with an in-hospital mortality greater than 10%.)
Septic shock a subset of sepsis with circulatory and cellular/metabolic dysfunction associated with a higher risk of
mortality
(Patients with septic shock can be clinically identified by a vasopressor requirement to maintain a mean arterial pressure of 65
mm Hg or greater and serum lactate level greater than 2 mmol/L (>18 mg/dL) in the absence of hypovolemia.)
In out-of-hospital, emergency department, or general hospital ward settings, adult patients with suspected infection can be rapidly
identified as being more likely to have poor outcomes typical of sepsis if they have at least 2 of the following clinical criteria that
together constitute a new bedside clinical score termed quickSOFA (qSOFA): respiratory rate of 22/min or greater, altered
mentation, or systolic blood pressure of 100 mm Hg or less.
C. DIAGNOSIS
1. We recommend that appropriate routine microbiologic cultures (including blood) be obtained before starting
antimicrobial therapy in patients with suspected sepsis or septic shock if doing so results in no substantial delay in
the start of antimicrobials (BPS).
Remarks: Appropriate routine microbiologic cultures always include at least two sets of blood cultures (aerobic
and anaerobic).
D. ANTIMICROBIAL THERAPY
1. We recommend that administration of IV antimicrobials should be initiated as soon as possible after recognition and
within one hour for both sepsis and septic shock (strong recommendation, moderate quality of evidence).
2. We recommend empiric broad-spectrum therapy with one or more antimicrobials for patients presenting with
sepsis or septic shock to cover all likely pathogens (including bacterial and potentially fungal or viral coverage)
(strong recommendation, moderate quality of evidence).
3. We recommend that empiric antimicrobial therapy be narrowed once pathogen identification and sensitivities are
established and/or adequate clinical improvement is noted (BPS).
4. We recommend AGAINST sustained systemic antimicrobial prophylaxis in patients with severe inflammatory states
of noninfectious origin (e.g., severe pancreas, burn injury) (BPS).
5. We recommend that dosing strategies of antimicrobials be optimized based on accepted pharmacokinetic/
pharmacodynamic principles and specific drug properties in patients with sepsis or septic shock (BPS).
6. We suggest empiric combination therapy (using at least two antibiotics of different antimicrobial classes) aimed
at the most likely bacterial pathogen(s) for the initial management of septic shock (weak recommendation, low
quality of evidence).
Remarks: Readers should review the table below for definitions of empiric, targeted/definitive, broad-spectrum,
combination, and multidrug therapy before reading this section.
Empiric therapy Initial therapy started in the absence of definitive microbiologic pathogen identification. Empiric therapy
maybe mono-, combination, or broad-spectrum, and/or multidrug in nature.
Targeted/definitive Therapy targeted to a specific pathogen (usually after microbiologic identification). Targeted/definitive
therapy therapy may be mono- or combination, but is not intended to be broad-spectrum.
Broad-spectrum The use of one or more antimicrobial agents with the specific intent of broadening the range of potential
therapy pathogens covered, usually during empiric therapy (e.g., piperacillin/tazobactam, vancomycin, and
anidulafungin; each is used to cover a different group of pathogens). Broad-spectrum therapy is
typically empiric since the usual purpose is to ensure antimicrobial coverage with at least one drug
when there is uncertainty about the possible pathogen. On occasion, broad-spectrum therapy may be
continued into the targeted/definitive therapy phase if multiple pathogens are isolated.
Multidrug therapy Therapy with multiple antimicrobials to deliver broad-spectrum therapy (i.e., to broaden coverage) for
empiric therapy (i.e., where pathogen is unknown) or to potentially accelerate pathogen clearance
(combination therapy) with respect to a specific pathogen(s) where the pathogen(s) is known or
suspected (i.e., for both targeted or empiric therapy). This term therefore includes combination therapy.
Combination therapy The use of multiple antibiotics (usually of different mechanistic classes) with the specific intent of
covering the known or suspected pathogen(s) with more than one antibiotic (e.g.,
piperacillin/tazobactam and an aminoglycoside or fluoroquinolone for gram-negative pathogens) to
accelerate pathogen clearance rather than to broaden antimicrobial coverage. Other proposed
applications of combination therapy include inhibition of bacterial toxin production (e.g., clindamycin
with beta-lactams for streptococcal toxic shock) or potential immune-modulatory effects (macrolides
with a beta-lactam for pneumococcal pneumonia).
7. We suggest that combination therapy not be routinely used for ongoing treatment of most other serious infections,
including bacteremia and sepsis without shock (weak recommendation, low quality of evidence).
Remarks: This does not preclude the use of multidrug therapy to broaden antimicrobial activity.
8. We recommend AGAINST combination therapy for the routine treatment of neutropenic sepsis/bacteremia (strong
recommendation, moderate quality of evidence).
Remarks: This does not preclude the use of multidrug therapy to broaden antimicrobial activity.
9. If combination therapy is used for septic shock, we recommend de-escalation with discontinuation of combination
therapy within the first few days in response to clinical improvement and/or evidence of infection resolution. This
applies to both targeted (for culture-positive infections) and empiric (for culture-negative infections) combination
therapy (BPS).
10. We suggest that an antimicrobial treatment duration of 7 to 10 days is adequate for most serious infections
associated with sepsis and septic shock (weak recommendation, low quality of evidence).
11. We suggest that longer courses are appropriate in patients who have a slow clinical response, undrainable foci
of infection, bacteremia with Staphylococcus aureus, some fungal and viral infections, or immunologic
deficiencies, including neutropenia (weak recommendation, low quality of evidence).
12. We suggest that shorter courses are appropriate in some patients, particularly those with rapid clinical
resolution following effective source control of intra-abdominal or urinary sepsis and those with
anatomically uncomplicated pyelonephritis (weak recommendation, low quality of evidence).
13. We recommend daily assessment for de-escalation of antimicrobial therapy in patients with sepsis and septic shock
(BPS).
E. SOURCE CONTROL
1. We recommend that a specific anatomic diagnosis of infection requiring emergent source control should be
identified or excluded as rapidly as possible in patients with sepsis or septic shock, and that any required source
control intervention should be implemented as soon as medically and logistically practical after the diagnosis is
made (BPS).
2. We recommend prompt removal of intravascular access devices that are a possible source of sepsis or septic
shock after other vascular access has been established (BPS).
F. FLUID THERAPY
1. We recommend that a fluid challenge technique be applied where fluid administration is continued as long as
hemodynamic factors continue to improve (BPS).
2. We recommend crystalloids as the fluid of choice for initial resuscitation and subsequent intravascular
volume replacement in patients with sepsis and septic shock (strong recommendation, moderate quality of
evidence).
3. We suggest using either balanced crystalloids or saline for fluid resuscitation of patients with sepsis or septic shock
(weak recommendation, low quality of evidence).
4. We suggest using albumin in addition to crystalloids for initial resuscitation and subsequent intravascular
volume replacement in patients with sepsis and septic shock, when patients require substantial amounts of
crystalloids (weak recommendation, low quality of evidence).
5. We recommend AGAINST using hydroxyethyl starches for intravascular volume replacement in patients with sepsis
or septic shock (strong recommendation, high quality of evidence).
6. We suggest using crystalloids over gelatins when resuscitating patients with sepsis or septic shock (weak
recommendation, low quality of evidence).
G. VASOACTIVE MEDICATIONS
1. We recommend norepinephrine as the first-choice vasopressor (strong recommendation, moderate quality of
evidence).
2. We suggest adding either vasopressin (up to 0.03 U/min) (weak recommendation, moderate quality of evidence) or
epinephrine (weak recommendation, low quality of evidence) to norepinephrine with the intent of raising mean
arterial pressure to target, or adding vasopressin (up to 0.03 U/min) (weak recommendation, moderate quality of
evidence) to decrease norepinephrine dosage.
3. We suggest using dopamine as an alternative vasopressor agent to norepinephrine ONLY in highly selected
patients (e.g., patients with low risk of tachyarrhythmias and absolute or relative bradycardia) (weak
recommendation, low quality of evidence).
4. We recommend AGAINST using low-dose dopamine for renal protection (strong recommendation, high quality of
evidence).
5. We suggest using dobutamine in patients who show evidence of persistent hypoperfusion despite adequate
fluid loading and the use of vasopressor agents (weak recommendation, low quality of evidence).
Remarks: If initiated, dosing should be titrated to an end point reflecting perfusion, and the agent reduced or
discontinued in the face of worsening hypotension or arrhythmias.
6. We suggest that all patients requiring vasopressors have an arterial catheter placed as soon as practical if
resources are available (weak recommendation, very low quality of evidence).
H. CORTICOSTEROIDS
1. We suggest AGAINST using IV hydrocortisone to treat septic shock patients if adequate fluid resuscitation and
vasopressor therapy are able to restore hemodynamic stability. If this is not achievable, we suggest IV
hydrocortisone at a dose of 200 mg per day (weak recommendation, low quality of evidence).
I. BLOOD PRODUCTS
1. We recommend that RBC transfusion occur only when hemoglobin concentration decreases to < 7.0 g/dL in
adults in the absence of extenuating circumstances, such as myocardial ischemia, severe hypoxemia, or acute
hemorrhage (strong recommendation, high quality of evidence).
2. We recommend AGAINST the use of erythropoietin for treatment of anemia associated with sepsis (strong
recommendation, moderate quality of evidence).
3. We suggest AGAINST the use of fresh frozen plasma to correct clotting abnormalities in the absence of bleeding
or planned invasive procedures (weak recommendation, very low quality of evidence).
4. We suggest prophylactic platelet transfusion when counts are:
• < 10,000/mm3 (10 x 109/L) in the absence of apparent bleeding
• < 20,000/mm3 (20 x 109/L) if the patient has a significant risk of bleeding.
Higher platelet counts (50,000/mm3 [50 x 109/L]) are advised for active bleeding, surgery, or invasive procedures
(weak recommendation, very low quality of evidence).
K. BLOOD PURIFICATION
1. We make no recommendation regarding the use of blood purification techniques.
L. ANTICOAGULANTS
1. We recommend AGAINST the use of antithrombin for the treatment of sepsis and septic shock (strong
recommendation, moderate quality of evidence).
2. We make no recommendation regarding the use of thrombomodulin or heparin for the treatment of sepsis or septic
shock.
M. MECHANICAL VENTILATION
1. We recommend using a target tidal volume of 6 mL/kg predicted body weight compared with 12 mL/kg in
adult patients with sepsis-induced acute respiratory distress syndrome (ARDS) (strong recommendation, high
quality of evidence).
2. We recommend using an upper limit goal for plateau pressures of 30 cm H2O over higher plateau pressures in
adult patients with sepsis-induced severe ARDS (strong recommendation, moderate quality of evidence).
3. We suggest using higher positive end-expiratory pressure (PEEP) over lower PEEP in adult patients with
sepsis-induced moderate to severe ARDS (weak recommendation, moderate quality of evidence).
4. We suggest using recruitment maneuvers in adult patients with sepsis-induced, severe ARDS (weak
recommendation, moderate quality of evidence).
5. We recommend using prone position over supine position in adult patients with sepsis-induced ARDS and a
PaO2/FIO2 ratio <150 (strong recommendation, moderate quality of evidence).
6. We recommend AGAINST using high-frequency oscillatory ventilation in adult patients with sepsis-induced
ARDS (strong recommendation, moderate quality of evidence).
7. We make no recommendation regarding the use of noninvasive ventilation for patients with sepsis-induced ARDS.
8. We suggest using neuromuscular blocking agents for 48 hours in adult patients with sepsis-induced ARDS and
a PaO2/FIO2 ratio < 150 mm Hg (weak recommendation, moderate quality of evidence).
9. We recommend a conservative fluid strategy for patients with established sepsis-induced ARDS who do not have
evidence of tissue hypoperfusion (strong recommendation, moderate quality of evidence).
10. We recommend AGAINST the use of ß-2 agonists for the treatment of patients with sepsis-induced ARDS without
bronchospasm (strong recommendation, moderate quality of evidence).
11. We recommend AGAINST the routine use of the pulmonary artery catheter for patients with sepsis-induced ARDS
(strong recommendation, high quality of evidence).
12. We suggest using lower tidal volumes over higher dal volumes in adult patients with sepsis-induced respiratory
failure without ARDS (weak recommendation, low quality of evidence).
13. We recommend that mechanically ventilated sepsis patients be maintained with the head of the bed elevated
between 30 and 45 degrees to limit aspiration risk and to prevent the development of ventilator-associated
pneumonia (strong recommendation, low quality of evidence).
14. We recommend using spontaneous breathing trials in mechanically ventilated patients with sepsis who are
ready for weaning (strong recommendation, high quality of evidence).
15. We recommend using a weaning protocol in mechanically ventilated patients with sepsis-induced respiratory failure
who can tolerate weaning (strong recommendation, moderate quality of evidence).
O. GLUCOSE CONTROL
1. We recommend a protocolized approach to blood glucose management in ICU patients with sepsis, commencing
insulin dosing when two consecutive blood glucose levels are > 180 mg/dL. This approach should target an
upper blood glucose level <180 mg/dL rather than an upper target blood glucose level <110 mg/dL (strong
recommendation, high quality of evidence).
2. We recommend that blood glucose values be monitored every 1 to 2 hours until glucose values and insulin
infusion rates are stable, then every 4 hours thereafter in patients receiving insulin infusions (BPS).
3. We recommend that glucose levels obtained with point-of-care testing of capillary blood be interpreted with caution
because such measurements may not accurately estimate arterial blood or plasma glucose values (BPS).
4. We suggest the use of arterial blood rather than capillary blood for point-of-care testing using glucose meters
if patients have arterial catheters (weak recommendation, low quality of evidence).
Q. BICARBONATE THERAPY
1. We suggest AGAINST the use of sodium bicarbonate therapy to improve hemodynamics or to reduce
vasopressor requirements in patients with hypoperfusion-induced lactic acidemia with pH > 7.15 (weak
recommendation, moderate quality of evidence).
T. NUTRITION
1. We recommend AGAINST the administration of early parenteral nutrition alone or parenteral nutrition in
combination with enteral feedings (but rather initiate early enteral nutrition) in critically ill patients with sepsis or
septic shock who can be fed enterally (strong recommendation, moderate quality of evidence).
2. We recommend AGAINST the administration of parenteral nutrition alone or in combination with enteral feeds (but
rather to initiate IV glucose and advance enteral feeds as tolerated) over the first 7 days in critically ill patients with
sepsis or septic shock for whom early enteral feeding is not feasible (strong recommendation, moderate quality of
evidence).
3. We suggest the early initiation of enteral feeding rather than a complete fast or only IV glucose in critically ill
patients with sepsis or septic shock who can be fed enterally (weak recommendation, low quality of evidence).
4. We suggest either early trophic/hypocaloric or early full enteral feeding in critically ill patients with sepsis or septic
shock; if trophic/hypocaloric feeding is the initial strategy, then feeds should be advanced according to patient
tolerance (weak recommendation, moderate quality of evidence).
5. We recommend AGAINST the use of omega-3 fatty acids as an immune supplement in critically ill patients with
sepsis or septic shock (strong recommendation, low quality of evidence).
6. We suggest AGAINST routinely monitoring gastric residual volumes in critically ill patients with sepsis or septic
shock (weak recommendation, low quality of evidence). However, we suggest measurement of gastric residuals in
patients with feeding intolerance or who are considered to be at high risk of aspiration (weak recommendation, very
low quality of evidence).
Remarks: This recommendation refers to nonsurgical critically ill patients with sepsis or septic shock.
7. We suggest the use of prokinetic agents in critically ill patients with sepsis or septic shock and feeding intolerance
(weak recommendation, low quality of evidence).
8. We suggest placement of post-pyloric feeding tubes in critically ill patients with sepsis or septic shock with
feeding intolerance or who are considered to be at high risk of aspiration (weak recommendation, low quality of
evidence).
9. We recommend AGAINST the use of IV selenium to treat sepsis and septic shock (strong recommendation,
moderate quality of evidence).
10. We suggest AGAINST the use of arginine to treat sepsis and septic shock (weak recommendation, low quality of
evidence).
11. We recommend AGAINST the use of glutamine to treat sepsis and septic shock (strong recommendation,
moderate quality of evidence).
12. We make no recommendation about the use of carnitine for sepsis and septic shock.
Prepared by:
ROBERT C. REÑA, MD
01/22/18