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Faheem Guirgis MD, FACEP
ED andTrauma Symposium – February 16th, 2017
Co-Chair Sepsis Committee
Assistant Professor of Emergency Medicine
Division of Research
Department of Emergency Medicine
UF Health Jacksonville
 K23GM115690 – National Institute of General
Medical Sciences
 Society of Critical Care MedicineWeil Grant
for Sepsis
 Dean’s Grants from UF
 Briefly discuss updated sepsis definitions
 Discuss principles of early severe sepsis
management
 Review pearls and tips for sepsis management
 Outline common pitfalls to avoid in sepsis
 Discuss the implications of recent literature
and potential future changes in sepsis care
 A. Under-recognized
 B. Under-treated
 C. Misunderstood (pathophysiology)
 D. All of the above
Sepsis 3?
OLD
NEW
Local Infection
Systemic signs?
Organ Dysfunction
(dysregulated response)
Shock
+
SOFA
1. Figure it out EARLY Sepsis Screening
2. Fill theTank = Fluids IVC US, Dynamic
measures, PLR
3. Fight the Bugs Antibiotics
Source Control
4. Fix perfusion MAP Organ fx
Lactate Inotropes
The 4 F’s
Institution-Wide Multidisciplinary Approach
 Sepsis Screening/Early recognition protocol
(Automated)
 Early Management Bundle/Order set
 Continued Care Bundle
 Education + Re-education = Culture of change
 Chart dives
 Be Data-driven
 Echo/IVC Ultrasound
 Passive Leg Raise
 Pulse PressureVariation
 StrokeVolumeVariation
QUICK ESTIMATION OF EF – GOOD SQUEEZE OR POOR SQUEEZE
1. Use Cardiac
Probe
2. Place probe in
the long axis,
SubX, just right
of midline
3. Find IVC and
measure 3 cm
distal to RA (at
or distal to HV)
4. Can use M-
mode
5. Have patient
sniff if
spontaneously
breathing
 IVC < 1 cm = give fluids
 IVC 1-2 cm w/ 50% collapse w/ inspiration=
give fluids
 IVC > 2 cm or w/o collapse = not fluid
responsive
 Pulmonary Hypertension/RHF may confound
your IVC US
 Patients on mechanical ventilation – look for
a 15-18% change in IVC diameter
3 cm
 ICU population
 Vasopressor dependent septic shock
 All on mechanical ventilation
 Limited Echo (LE) performed w/in 24 hours of
ICU admission
1. Systolic function:
normal, moderate, or
severely impaired
2. Assess for pericardial
effusion
3. IVC diameter
fluctuation < or > 15%
dIVC=[(dI−dE)/dE]×100
<15% dIVC with normal LV fx = stop
fluids
>15% dIVC w/ normal LV fx = 20 to 40
mL/kg fluids
>15% dIVC w/ mod to severe LV
dysfx = 10 to 20 mL/kg fluids and
dobutamine 5 mcg/kg
<15% dIVC w/ mod to severe LV
dysfx = dobutamine and no fluids
Passive leg raise.To perform a passive leg raise, a patient is
placed in a semi-recumbent position at 45°.The patient’s legs
are then elevated to 45° and the hemodynamic variable of
interest evaluated after 30−60 seconds.
1. Is fluid resuscitation adequate?
- Heart, IVC collapse, PPV, SVV
2. Is MAP adequate?
- MAP > 65
3. Is Oxygen Delivery adequate?
- Lactate normalization vs Lactate clearance?
Now Go Back and Ask 3 Questions…
What about individual measures of organ function?
 Effective Abx within 1st hour for sepsis and
septic shock (2016)
 Every hour of delay in giving Abx is associated
with a measurable increase in mortality
(Kumar et al; Ferrer et al)
 Mortality significantly increased in patients
who received initial antibiotics after shock
recognition (n = 172 [59%]) compared with
before shock recognition (OR, 2.4; 1.1-4.5) –
Puskarich et al
 Gram + > Gram - > polymicrobial as the cause
of most septic shock
 Bolus drugs before infusion drugs
 Broad coverage guided by local prevalence
patterns
 All patients should receive a full loading dose
of antibiotics
 EmpiricTherapy – best guess, no bugs yet
 Broad SpectrumTherapy – broad spec abx to
cover multiple potential bugs
 CombinationTherapy – Using more than one
drug to cover the same bug (largely
unproven)
 Empiric combo therapy for initial
management of septic shock
 No Empiric combo therapy for regular sepsis
or bacteremia
 No combo therapy for neutropenic
sepsis/bacteremia
 If combo therapy is used – de-escalate in the
first few days if clinical improvement
 “Trauma is a compulsive search for injuries” –
Billy Mallon
 “Sepsis is a compulsive search for a source of
infection” – Me
 Treat the patient like a trauma – fully expose, etc
 The less the patient can tell you the more
compulsive the search
 And…the severity of the source should be
proportional to the severity of illness
 Source control as soon as possible (Rec 6-12
hrs from time of diagnosis)
 If intravascular device is a possible source, it
should be promptly removed after other
vascular access established
 Consider IR or Surgery
 Cultures of blood and other sites (urine, CSF,
wounds, respiratory secretions, etc) before
abx if possible
 Cultures from vascular access and peripheral
blood – 10 cc each
 If culture from vascular access is positive
earlier than peripheral blood then vascular
access = infectious source
DO NOT DELAY ANTIBIOTICS > 45 MIN
FOR BLOOD CULTURES
 Published in CCM in 2015
 Dopamine still a bad choice for SSh
 Greater hospital mortality – propensity-
matched scoring, n = 38,788; 25% vs 23.7%;
OR 1.08; 95% CI, 1.02-1.14)
 Most commonly used in the South!
 Norepinephrine 1st agent
 Vaso or Epi as 2nd agent
 Epi - especially if inotropy required
 Vaso – need alpha
 Phenylephrine if inotropy not needed
 Norepi causing arrhythmias
 CO is high and BP is low
 Salvage therapy
 Dobutamine – first choice inotrope
 Vaso +/- HC vs Norepi +/- HC for vasopressor
dependent septic shock
 Primary outcome – renal failure free days
 No difference
 Demonstrated thatVaso could be titrated up
to a dose of .06units/min
 Guide resuscitation to normalize lactate
 Lactate normalization (< 2)
 Clearance?
 Hydrocortisone 200 mg/day
 When starting your second pressor
 Management so far:
 Fluids
 Abx
 Source identified and controlled
 Pressors
 Lactate level
Prevalence Mortality
Lactate > 4
alone
5.4% 30% but
Perhaps 20%
Hypotension
alone
49.5% 36.7%
Lactate > 4 +
Hypotension
16.6% 46.1%
 1316 pts w/ sepsis w/in 4 hrs of ED arrival
 111 progressed to shock w/in 48 hrs (8.4%)
 Females (OR 1.59), nonpersistent hypotension
(OR 6.24), bandemia ≥ 10% (OR 2.6), lactate ≥ 4
(OR 5.3), PMH CAD (OR 2.01)
SEPSIS RECIDIVISM
 110 ED patients w/ SS/SSh
 28-90 days: 17% rate of
sepsis readmission
LONG-TERM MORTALITY
 Initial mortality 18% (90
survivors)
 3 year mortality 48% (only
53 survivors)
Chronic Critical Illness
Disease of the elderly who survive initial sepsis  dc LTAC, functionally dependent,
die outside of the hospital months to years later (Sepsis P50 – UF)
 Fiscal impact of 30 day sepsis readmission
Sepsis CHF Acute MI
Initial
Hospitalization
(2009-11)
240,198 193,153 105,684
Readmission rate 20.4% 23.6% 17.7%
Annual costs
(California)
$500
million/yr
$229
million/yr
$142
million/yr
 Improved sepsis diagnostics (biomarkers)
 Dys-HDL?
 Better understanding of pathophysiology
 CCI/PICS/CARS (thanks to UF G’ville – Moore, Moldawer,
Leeuwenburgh)
 Persistent/long-term organ dysfunction – who/why?
 Sepsis recidivism – why?
 Mitochondrial medicine?
 RACETrial - L-carnitine (increases cardiac mechanical
efficiency and facilitates mitochondria)
 Metabolic cocktails?
 Hypothermia?!
 ECMO?
 Old definitions
 SEVERE SEPSIS: SIRS + sepsis-induced organ dysfunction:
 SBP < 90 or MAP < 70 mm Hg
 Creatinine > 2.0 mg/dl or Urine Output < 0.5 ml/kg/hour for > 2
hours
 Bilirubin > 2 mg/dl (34.2 mmol/L)
 Platelet count < 100,000
 Coagulopathy (INR >1.5 or aPTT >60 secs)
 Lactate > 2 mmol/L
 SEPTIC SHOCK:
 Lactate > 4 mmol/L, OR
 SBP < 90 or MAP < 70 mm Hg, not responsive to fluids
 A. measure lactate level
 B. obtain blood cultures prior to antibiotics
 C. administer broad spectrum antibiotics
 D. administer 30 ml/kg crystalloid for hypotension or
lactate = 4 mmol/L
 E. apply vasopressors (for hypotension that does not
respond to initial fluid resuscitation to maintain a
mean arterial pressure = 65)
 F. in the event of persistent hypotension after initial
fluid administration (MAP < 65 mm Hg) or if initial
lactate was = 4 mmol/L, reassess volume status and
tissue perfusion and document findings.*
 2/4 of the following
 Measure CVP
 Measure ScvO2
 Bedside cardiovascular ultrasound
 Dynamic assessment of fluid responsiveness with
passive leg raise or fluid challenge
 OR Focused exam† including vital signs,
cardiopulmonary, capillary refill, pulse and skin
findings.
 Remeasure lactate if initial lactate is elevated
 But sadly, it’s the end of my lecture 
 Thank you!
 Fluids - 30 ml/kg in the first 3 hours, crystalloid first, then maybe
albumin, use dynamic markers and/or fluid challenges
 Goal MAP>65
 EGDT is no longer recommended
 Lactate - attempt to normalize lactate
 Blood Cultures - get them before antibiotics, if obtaining them will
not delay the provision of antibiotics
 Antibiotics -Within 1 hour of sepsis or septic shock
 Vasopressors - Norepi is the first choice, add in epi or vaso, Do not
use dopamine
 Steroids - 200 mg Hydrocortisone for patients who are still
unstable after fluids and vasopressors
 Blood - In most circumstances, use a trigger of <7.0 g/dL
 Glucose - goal is < 180 mg/dL
 Bicarb - Not recommended if pH is >7.15 (which in no way means it
is recommended for pHs less than that)

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Faheem Guirgis MD Sepsis Update

  • 1. Faheem Guirgis MD, FACEP ED andTrauma Symposium – February 16th, 2017 Co-Chair Sepsis Committee Assistant Professor of Emergency Medicine Division of Research Department of Emergency Medicine UF Health Jacksonville
  • 2.  K23GM115690 – National Institute of General Medical Sciences  Society of Critical Care MedicineWeil Grant for Sepsis  Dean’s Grants from UF
  • 3.  Briefly discuss updated sepsis definitions  Discuss principles of early severe sepsis management  Review pearls and tips for sepsis management  Outline common pitfalls to avoid in sepsis  Discuss the implications of recent literature and potential future changes in sepsis care
  • 4.
  • 5.  A. Under-recognized  B. Under-treated  C. Misunderstood (pathophysiology)  D. All of the above Sepsis 3?
  • 6.
  • 7.
  • 9. Local Infection Systemic signs? Organ Dysfunction (dysregulated response) Shock
  • 10. +
  • 11. SOFA
  • 12.
  • 13. 1. Figure it out EARLY Sepsis Screening 2. Fill theTank = Fluids IVC US, Dynamic measures, PLR 3. Fight the Bugs Antibiotics Source Control 4. Fix perfusion MAP Organ fx Lactate Inotropes The 4 F’s
  • 14. Institution-Wide Multidisciplinary Approach  Sepsis Screening/Early recognition protocol (Automated)  Early Management Bundle/Order set  Continued Care Bundle  Education + Re-education = Culture of change  Chart dives  Be Data-driven
  • 15.
  • 16.  Echo/IVC Ultrasound  Passive Leg Raise  Pulse PressureVariation  StrokeVolumeVariation
  • 17. QUICK ESTIMATION OF EF – GOOD SQUEEZE OR POOR SQUEEZE
  • 18. 1. Use Cardiac Probe 2. Place probe in the long axis, SubX, just right of midline 3. Find IVC and measure 3 cm distal to RA (at or distal to HV) 4. Can use M- mode 5. Have patient sniff if spontaneously breathing
  • 19.  IVC < 1 cm = give fluids  IVC 1-2 cm w/ 50% collapse w/ inspiration= give fluids  IVC > 2 cm or w/o collapse = not fluid responsive  Pulmonary Hypertension/RHF may confound your IVC US  Patients on mechanical ventilation – look for a 15-18% change in IVC diameter
  • 20. 3 cm
  • 21.
  • 22.  ICU population  Vasopressor dependent septic shock  All on mechanical ventilation  Limited Echo (LE) performed w/in 24 hours of ICU admission
  • 23. 1. Systolic function: normal, moderate, or severely impaired 2. Assess for pericardial effusion 3. IVC diameter fluctuation < or > 15% dIVC=[(dI−dE)/dE]×100 <15% dIVC with normal LV fx = stop fluids >15% dIVC w/ normal LV fx = 20 to 40 mL/kg fluids >15% dIVC w/ mod to severe LV dysfx = 10 to 20 mL/kg fluids and dobutamine 5 mcg/kg <15% dIVC w/ mod to severe LV dysfx = dobutamine and no fluids
  • 24. Passive leg raise.To perform a passive leg raise, a patient is placed in a semi-recumbent position at 45°.The patient’s legs are then elevated to 45° and the hemodynamic variable of interest evaluated after 30−60 seconds.
  • 25. 1. Is fluid resuscitation adequate? - Heart, IVC collapse, PPV, SVV 2. Is MAP adequate? - MAP > 65 3. Is Oxygen Delivery adequate? - Lactate normalization vs Lactate clearance? Now Go Back and Ask 3 Questions… What about individual measures of organ function?
  • 26.
  • 27.  Effective Abx within 1st hour for sepsis and septic shock (2016)  Every hour of delay in giving Abx is associated with a measurable increase in mortality (Kumar et al; Ferrer et al)  Mortality significantly increased in patients who received initial antibiotics after shock recognition (n = 172 [59%]) compared with before shock recognition (OR, 2.4; 1.1-4.5) – Puskarich et al
  • 28.  Gram + > Gram - > polymicrobial as the cause of most septic shock  Bolus drugs before infusion drugs  Broad coverage guided by local prevalence patterns  All patients should receive a full loading dose of antibiotics
  • 29.  EmpiricTherapy – best guess, no bugs yet  Broad SpectrumTherapy – broad spec abx to cover multiple potential bugs  CombinationTherapy – Using more than one drug to cover the same bug (largely unproven)
  • 30.  Empiric combo therapy for initial management of septic shock  No Empiric combo therapy for regular sepsis or bacteremia  No combo therapy for neutropenic sepsis/bacteremia  If combo therapy is used – de-escalate in the first few days if clinical improvement
  • 31.  “Trauma is a compulsive search for injuries” – Billy Mallon  “Sepsis is a compulsive search for a source of infection” – Me  Treat the patient like a trauma – fully expose, etc  The less the patient can tell you the more compulsive the search  And…the severity of the source should be proportional to the severity of illness
  • 32.  Source control as soon as possible (Rec 6-12 hrs from time of diagnosis)  If intravascular device is a possible source, it should be promptly removed after other vascular access established  Consider IR or Surgery
  • 33.  Cultures of blood and other sites (urine, CSF, wounds, respiratory secretions, etc) before abx if possible  Cultures from vascular access and peripheral blood – 10 cc each  If culture from vascular access is positive earlier than peripheral blood then vascular access = infectious source
  • 34. DO NOT DELAY ANTIBIOTICS > 45 MIN FOR BLOOD CULTURES
  • 35.
  • 36.
  • 37.
  • 38.  Published in CCM in 2015  Dopamine still a bad choice for SSh  Greater hospital mortality – propensity- matched scoring, n = 38,788; 25% vs 23.7%; OR 1.08; 95% CI, 1.02-1.14)  Most commonly used in the South!
  • 39.  Norepinephrine 1st agent  Vaso or Epi as 2nd agent  Epi - especially if inotropy required  Vaso – need alpha  Phenylephrine if inotropy not needed  Norepi causing arrhythmias  CO is high and BP is low  Salvage therapy  Dobutamine – first choice inotrope
  • 40.  Vaso +/- HC vs Norepi +/- HC for vasopressor dependent septic shock  Primary outcome – renal failure free days  No difference  Demonstrated thatVaso could be titrated up to a dose of .06units/min
  • 41.  Guide resuscitation to normalize lactate  Lactate normalization (< 2)  Clearance?
  • 42.
  • 43.  Hydrocortisone 200 mg/day  When starting your second pressor
  • 44.
  • 45.  Management so far:  Fluids  Abx  Source identified and controlled  Pressors  Lactate level
  • 46. Prevalence Mortality Lactate > 4 alone 5.4% 30% but Perhaps 20% Hypotension alone 49.5% 36.7% Lactate > 4 + Hypotension 16.6% 46.1%
  • 47.  1316 pts w/ sepsis w/in 4 hrs of ED arrival  111 progressed to shock w/in 48 hrs (8.4%)  Females (OR 1.59), nonpersistent hypotension (OR 6.24), bandemia ≥ 10% (OR 2.6), lactate ≥ 4 (OR 5.3), PMH CAD (OR 2.01)
  • 48. SEPSIS RECIDIVISM  110 ED patients w/ SS/SSh  28-90 days: 17% rate of sepsis readmission LONG-TERM MORTALITY  Initial mortality 18% (90 survivors)  3 year mortality 48% (only 53 survivors) Chronic Critical Illness Disease of the elderly who survive initial sepsis  dc LTAC, functionally dependent, die outside of the hospital months to years later (Sepsis P50 – UF)
  • 49.  Fiscal impact of 30 day sepsis readmission Sepsis CHF Acute MI Initial Hospitalization (2009-11) 240,198 193,153 105,684 Readmission rate 20.4% 23.6% 17.7% Annual costs (California) $500 million/yr $229 million/yr $142 million/yr
  • 50.
  • 51.  Improved sepsis diagnostics (biomarkers)  Dys-HDL?  Better understanding of pathophysiology  CCI/PICS/CARS (thanks to UF G’ville – Moore, Moldawer, Leeuwenburgh)  Persistent/long-term organ dysfunction – who/why?  Sepsis recidivism – why?  Mitochondrial medicine?  RACETrial - L-carnitine (increases cardiac mechanical efficiency and facilitates mitochondria)  Metabolic cocktails?  Hypothermia?!  ECMO?
  • 52.  Old definitions  SEVERE SEPSIS: SIRS + sepsis-induced organ dysfunction:  SBP < 90 or MAP < 70 mm Hg  Creatinine > 2.0 mg/dl or Urine Output < 0.5 ml/kg/hour for > 2 hours  Bilirubin > 2 mg/dl (34.2 mmol/L)  Platelet count < 100,000  Coagulopathy (INR >1.5 or aPTT >60 secs)  Lactate > 2 mmol/L  SEPTIC SHOCK:  Lactate > 4 mmol/L, OR  SBP < 90 or MAP < 70 mm Hg, not responsive to fluids
  • 53.  A. measure lactate level  B. obtain blood cultures prior to antibiotics  C. administer broad spectrum antibiotics  D. administer 30 ml/kg crystalloid for hypotension or lactate = 4 mmol/L  E. apply vasopressors (for hypotension that does not respond to initial fluid resuscitation to maintain a mean arterial pressure = 65)  F. in the event of persistent hypotension after initial fluid administration (MAP < 65 mm Hg) or if initial lactate was = 4 mmol/L, reassess volume status and tissue perfusion and document findings.*
  • 54.  2/4 of the following  Measure CVP  Measure ScvO2  Bedside cardiovascular ultrasound  Dynamic assessment of fluid responsiveness with passive leg raise or fluid challenge  OR Focused exam† including vital signs, cardiopulmonary, capillary refill, pulse and skin findings.  Remeasure lactate if initial lactate is elevated
  • 55.  But sadly, it’s the end of my lecture   Thank you!
  • 56.
  • 57.
  • 58.
  • 59.  Fluids - 30 ml/kg in the first 3 hours, crystalloid first, then maybe albumin, use dynamic markers and/or fluid challenges  Goal MAP>65  EGDT is no longer recommended  Lactate - attempt to normalize lactate  Blood Cultures - get them before antibiotics, if obtaining them will not delay the provision of antibiotics  Antibiotics -Within 1 hour of sepsis or septic shock  Vasopressors - Norepi is the first choice, add in epi or vaso, Do not use dopamine  Steroids - 200 mg Hydrocortisone for patients who are still unstable after fluids and vasopressors  Blood - In most circumstances, use a trigger of <7.0 g/dL  Glucose - goal is < 180 mg/dL  Bicarb - Not recommended if pH is >7.15 (which in no way means it is recommended for pHs less than that)

Editor's Notes

  1. THE PERFECT STORM THAT TORE THROUGH GEORGIA ON MY FLIGHT TO LOS ANGELES Wall of storms that spun off tornadoes
  2. Complicated disease – sepsis for which there are no biomarkers or gold standard tests biological concepts that are currently incompletely understood, such as genetic influences and cellular abnormalities, comorbidities - No troponin like a heart attack - can’t be diagnosed with a CT scan - Lactate can’t tell you whether or not to think someone is septic, only how sick they are after you recognize the sepsis Involve CMS regulations – word for word interpretation of the definitions, mandate how patients with suspected sepsis are to be cared for Change the definitions for this complicated disease
  3. Conceptual Framework for sepsis Infection + Organ dysfunction
  4. OLD – Sepsis and infection were almost one and the same NEW – Sepsis is very distinct from most infections MY OPINION -
  5. Cellulitis – could be localized, no systemic signs Pneumonia – may have systemic signs, fever, tachycardia, etc Sepsis – confusion, oliguria, mottling, thrombocytopenia, hypoxia Shock - – MAP < 65 (not responsive to fluids), vasopressors, lactate > 2
  6. Dangerous as a screening tool - Rule in for high risk sepsis 38% sensitive, 85% specific for death Use it – but understand the limitations Positive = move to resus bay, jump on this patient Neg = keep looking
  7. Robust scoring system – very well –studied Look for new changes in SOFA components Accurate prognosis for death associated with need for intensive care Associated with long-term organ dysfunction and poor outcomes as well as sepsis recidivism NOT USER FRIENDLY – EPIC AUTO CALCULATOR?
  8. First 10 decisions you make in a critically ill, un-resuscitated patient are critical determinants of life or death Intubate Give blood in a trauma (OR when to go to the OR) Manage a head injury – avoid hypoxia or hypotension When to start antibiotics in sepsis, how much fluids you give and how quickly What tests to order – lytes on a blood gas in a patient with bradycardia for HyperK US-Guided Decision making – FAST, Echo, RUSH exam, Lung US
  9. Basic Rules for managing sepsis
  10. Negative pressure created by the inspiration of the patient increases venous return to the heart, briefly collapsing the IVC.
  11. Improved 28 day survival Reduced rates of AKI
  12. Changed from 3 hrs for sepsis, 1 hr for shock in 2012 guidelines
  13. Modern abx are more effective – no benefit in neutropenic fever/sepsis without shock Balance risk benefit – for shock, benefit > risk For non-shock sepsis – Risk of AKI, etc prob > benefit
  14. Foci of infection readily amenable to source control - intra-abdominal abscesses, gastrointestinal perforation, ischemic bowel or volvulus, cholangitis, cholecystitis, pyelonephritis associated with obstruction or abscess, necrotizing soft tissue infection, other deep space infection (e.g., empyema or septic arthritis), and implanted device infections. Lines in for greater than 48 hours (if suspected source should be pulled as quickly as possible
  15. Septic patients treated with Dopamine had increased risk of death in observational studies (relative risk 1.23, p<0.01) and randomized trials (relative risk 1.12, p<0.035) Increased risk of arrhythmias with Dopamine (relative risk 2.34, p< 0.001) – Debacker et al
  16. Dobutamine is not a pressor! It’s an inotrope! But Epi is prob a better choice Arterial line as soon as possible Remember – Epi can be bad for splanchnic circulation and increases lactate and may preclude lactate normalization as a resuscitation endpoint (stimulates skeletal muscle B2 receptors) Vaso at higher doses cardiac, digital, and splanchnic ischemia
  17. Picking an arbitrary clearance target not as good though there is some evidence Increases in the serum lactate level may represent tissue hypoxia, accelerated aerobic glycolysis driven by excess beta-adrenergic stimulation, or other causes (e.g., liver failure). Regardless of the source, increased lactate levels are associated with worse outcomes [32].
  18. TRISS trial
  19. 1. Rushing to intubate the under-resuscitated patients or overdosing RSI meds 2. ignoring high lactates or not rechecking high lactates? Could talk about the controversy behind where lactate comes from 3. Not enough fluids, or too much? 4. Passing off AMS 5. Missing subtle signs of organ dysfunction 6. Post-shock vs pre-shock abx, same as hourly delay in abx 7. Not following resuscitative end points - 3 windows to the world, improvements in mental status, increased urine output, IVC US, echo
  20. This will become an issue!
  21. - sore throat/fever, 10 wks pregnant - workup negative except abnormal labs, admitted, decompensate to ARDS/shock - undiagnosed autoimmune disease resulting in diffuse alveolar hemorrhage, cause of miscar.