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Pediatric Sepsis Curriculum

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Title: Pediatric Sepsis Curriculum


1
Pediatric Sepsis Curriculum
2
Dear Medical Student, Resident, or Pediatric
Subspecialty Fellow,You are being invited to
participate in a voluntary research survey and
curriculum. Your participation is voluntary, but
greatly appreciated. The goal of the study is to
improve knowledge and confidence in diagnosing
and treating Pediatric Sepsis.The risks of
participating in the study are minimal and are
consistent with every day educational practices
of curriculum participation and assessment. We
will be using Survey Monkeys 128-bit encryption
to ensure that your IP address will remain
private and that your email address will not be
collected or stored. Survey Monkey complies with
the US Department of Commerces Safe Harbor
Frameworks ensuring privacy of collected personal
information. Participation in this study is also
anonymous and confidential. Because a remote
website is being used to complete the surveys,
and because IP addresses will be disabled by
Survey Monkey, no unique personal identifiers
will be used in data collection. Participation in
demographic questions is optional, and the
demographic categories are broad enough to ensure
that the investigator cannot deduce the identity
of any person participating in the survey.The
pre-curriculum survey should take approximately
20 minutes to complete, and the suggested study
time for the curriculum is one hour. In
September, you will be invited to take a
post-curriculum survey which is similar to the
pre-curriculum survey in nature and should also
take about 20 minutes to complete. Estimated
maximum length of time spent on this study is
less than 3 hours over the course of 6 months for
both surveys and the curriculum.The benefits of
participating in the study are increased
knowledge and confidence diagnosing and treating
Pediatric Sepsis.By taking the pre- or
post-curriculum survey, you consent to
participating in this research study. If you
have any questions regarding this study, or if
you need to clarify the risks and benefits or
confidentiality of this study, please feel free
to email SNamjoshi_at_mednet.ucla.edu or call the
page operator at 310-825-6301, pager 28224. If
you have questions about your rights while taking
part in this study, or you have concerns or
suggestions and you want to talk to someone other
than the researchers about the study, you may
reach the UCLA Office of the Human Research
Protection Program (OHRPP) at (310) 825-7122 or
write toUCLA Office of the Human Research
Protection Program,11000 Kinross Avenue, Suite
211, Box 951694, Los Angeles, CA
90095-1694Sincerely,Shweta Namjoshi, MD
MPHUCLA Pediatrics PGY-1310.825.6301pager 28224
3
The pre-Curriculum Survey Has been disabled. If
you need to take the pre-test, please click here
https//www.surveymonkey.com/s/Z7YLP7B Post-Curr
iculum Survey
4
Sepsis Fact Sheet
  • What Sepsis, Whats a Bundle, and What Should I
    Do?

5
What is Sepsis?
  • Sepsis is a life threatening response to
    infection. It represents a continuum through
    SIRS, sepsis, and septic shock.
  • SIRS systemic inflammatory response syndrome
    2 or more of the following high or low white
    count, tachycardia, tachypnea, high or low
    temperature
  • Sepsis SIRS a suspected source of infection
    (ex., skin ulcer, pneumonia, central line)
  • Septic Shock sepsis hypotension(or signs of
    poor perfusion)
  • Signs of poor perfusion altered mental status,
    delayed cap refill, poor pulses, mesenteric
    ischemia (emesis, diarrhea), urine output lt
    1cc/kg/hr, hypoxia

6
Whats A Bundle?
  • A bundle is a group of treatments that improve
    outcomes when given together rather than
    separately.
  • Sepsis Resuscitation Bundle how to treat early
    sepsis 20cc/kg IVF boluses, broad spectrum IV
    antibiotics, blood culture, lactate within 1 hour
    of presentation. You may use up to 60cc/kg in the
    early phase of sepsis and move to pressors if
    vitals do not normalize.
  • Sepsis Management Bundle how to direct fluids
    and pressors to markers of improved cardiac
    output
  • markers of improved cardiac output normal
    mental status, UOP gt 1cc/kg/hr, cap refill lt2
    sec, normal MAP and CVP gt8, ScVO2 gt 70. There
    are several monitoring devices that can help with
    hemodynamic monitoring, and the PA catheter is
    the gold standard (though use of a PA catheter
    has not been shown to decrease mortality from
    sepsis). Reduction in serum lactate does not
    accurately reflect improved cardiac output.

7
What Should I Do?
  • If blood pressure doesnt increase with fluids
    and pressors, consider CIRCI (Critical Illness
    Related Corticosteroid Insufficiency). A random
    cortisol level lt 15 is diagnostic and IV
    hydrocortisone can help. A ACTH stim test is not
    needed. CIRCI is especially relevant to those who
    have previously been on steroids.
  • Do not wait to start pressors till central access
    is obtained. Dopamine can be started at low doses
    via peripheral IV.
  • Mortality form sepsis almost doubles with delays
    in bundled therapy and increases by 8 per hour
    with delays in IV antibiotics. Source removal is
    the ultimate treatment for sepsis. Advocate for
    your patients! Push fluids and antibiotics early!

8
Case 1
  • Outpatient Clinic

9
Case 1 History
  • CC Fever
  • Time 1050
  • HPI Two year-old female presents to clinic with
    a two-day history of irritability, subjective
    fevers, and chills. She has been less active
    than usual, complaining of leg and joint pain.
    Her mother notes she is developing a rash and
    that she had two episodes of emesis on the way to
    clinic.
  • PMH ex-full term infant with normal development,
    no allergies, no current medications, no
    surgeries, no hospitalizations. Delayed
    immunization schedule (missing one Inactivated
    polio and one Pneumococcal vaccine)
  • SH Lives in apartment with mom, dad, sister,
    three cousins, and grandmother. No smokers, no
    pets. No recent travel. One cousin is a marine.

10
Case 1 Physical Exam
  • Time 1100
  • Vitals T 39.2, HR 156, RR 50, BP 95/68
  • Physical Exam
  • General ill-appearing
  • Neuro rousable but intermittently lethargic, CN
    2-12 intact, 5/5 strength and sensation, antalgic
    gait, normal reflexes
  • HEENT mucous membranes dry, TM clear, OP clear,
    nasal flaring
  • CVS S1, S2, hyperdynamic precordium, 1/6
    systolic murmur LUSB, pedal pulses 1
  • Resp CTA b/l, subcostal retractions
  • Abdomen s/nt/nd, no hsm
  • Extremities cool feet and hands, joints are
    free of warmth or effusion
  • Skin small, diffuse, petechiae on arms, legs,
    and trunk, cap refill 2 sec,

11
Case 1 Assessment and Plan
  • Time 1110
  • Click on the next most appropriate step in
    management
  • perform lumbar puncture
  • disCharge home with return precautions and
    rheumatology referral
  • place peripheral IV
  • observe in clinic for 2 hours

12
Plan Lumbar Puncture
  • Time 1125
  • While setting up to perform your lumbar puncture,
    you notice that your patient becomes increasingly
    tachypneic. Her skin appears mottled and
    capillary refill is now 4 sec.
  • Repeat vitals are as follows
  • T 39, HR 160, RR 50, BP 70/48
  • The most appropriate next step in management is
  • place peripheral IV
  • proceed with lumbar puncture

13
Plan Observe
  • Time 1330
  • After two hours of close observation, your
    patients condition continues to deteriorate.
    Her skin is mottled, she is increasingly
    lethargic, and capillary refill is now 4
    seconds.
  • Repeat vitals are as follows
  • T 39, HR 160, RR 50, BP 60/45
  • You decide to transfer her to the UCLA emergency
    room for suspected septic shock. Upon arrival At
    UCLA, she is noted to have purpura and adrenal
    insufficiency, and she expires by early evening.
    Blood cultures are positive for neisseria
    meningitidis.
  • click here to redo the case

14
Plan IV
  • Time 1223
  • Two- 20 gauge peripheral IVs are placed in each
    antecubital fossa.
  • Select the next most appropriate step in
    management
  • give 20cc/kg bolus normal saline
  • observe the child in clinic for 2 hours.
  • prescribe oral antibiotic discharge home with
    follow up appointment in 2-3 days

15
Plan Bolus
  • Time 1230
  • After placing a peripheral IV and giving a single
    20 cc/kg bolus, which is the most appropriate
    step in management
  • repeat 20cc/kg normal saline bolus, draw blood
    cultures and lactate, and give broad spectrum IV
    antibiotics
  • proceed with lumbar puncture
  • close observation in clinic for 2 hours

16
Plan Lumbar Puncture
  • Time 1300
  • You decide to proceed with lumbar puncture.
    However, your patients blood pressure continues
    to drop, her skin becomes increasingly cool and
    mottled, and she loses consciousness.
  • You call 911 and she is transferred to the UCLA
    emergency room in septic shock.
  • She decompensates within hours. At UCLA, she is
    noted to have purpura and adrenal insufficiency,
    and she expires by early evening. Blood cultures
    are positive for neisseria meningitidis.
  • click here to redo the case

17
Plan Lumbar Puncture
  • Time 1300
  • You decide to proceed with lumbar puncture after
    giving a single bolus of 20 cc/kg normal saline.
    However, your patients blood pressure continues
    to drop, her skin becomes increasingly cool and
    mottled, and she loses consciousness.
  • You call 911 and she is transferred to the UCLA
    emergency room in septic shock.
  • She decompensates within hours. At UCLA, she is
    noted to have purpura and adrenal insufficiency,
    and she is intubated and transferred to the PICU
    by early evening. Blood cultures grow neisseria
    meningitidis.
  • click here to redo the case

18
Plan Rheumatology Referral
  • Time 1930
  • Your patient has an appointment to see
    rheumatology for the rash and joint pain in 5
    days, and she returns home with strong return
    precautions. Your patients mother follows your
    counseling regarding persistent emesis and fever,
    and brings her to the nearest Emergency
    Department in the early evening. Her childs
    condition is rapidly deteriorating.
  • By 2125, the childs rash becomes purpuric, and
    she develops fulminant DIC. A random cortisol
    level is 5. She is diagnosed with adrenal
    insufficiency, and she expires from septic shock.
    Blood cultures drawn prior to death indicate that
    the source of sepsis was neiserria meningitidis.
  • click here to redo the case

19
Plan Discharge
  • Time 1930
  • Your patient returns home with oral antibiotics
    and strong return precautions. By 1830, Your
    patients mother follows your counseling
    regarding persistent emesis and fever, and brings
    her to the nearest Emergency Department. Her
    childs condition is rapidly deteriorating.
  • By 2125, she is diagnosed with DIC and adrenal
    insufficiency. She expires from septic shock,
    and blood cultures are positive for neiserria
    meningitidis.
  • click here to redo the case

20
Plan IV
  • Time 1123
  • Two- 20 gauge peripheral IVs are placed in each
    antecubital fossa.
  • Select the next most appropriate step in
    management
  • give a 20cc/kg bolus of normal saline
  • observe hemodynamics in clinic for 2 hours.
  • prescribe oral antibiotic discharge home with
    follow up appointment in 2-3 days

21
Plan Bolus
  • Time 1134
  • After placing a peripheral IV and giving a single
    20 cc/kg bolus, which is the most appropriate
    step in management
  • repeat 20cc/kg normal saline bolus, draw blood
    cultures and lactate to clinic lab, and start
    broad spectrum IV antibiotics
  • proceed with lumbar puncture once hemodynamics
    have improved
  • observe hemodynamics in clinic for 2 hours

22
Sepsis Resuscitation Bundle
  • Time 1215
  • Within an hour of presentation, you have
    successfully given your patient all four aspects
    of the Sepsis Resuscitation Bundle. You quickly
    recognized symptoms of SIRS (Systemic
    inflammatory response syndrome) and suspected
    that meningococcemia could be a source of this
    childs infection. By implementing a bundle, or a
    collection of plans given together to improve
    patient outcomes, you have changed this childs
    course with meningococcemia.
  • The components of the Sepsis Resuscitation Bundle
    are listed below
  • up to three- 20 cc/kg boluses of normal saline,
    directed to hemodynamics
  • broad spectrum IV antibiotics within 1 hour of
    presentation
  • baseline serum lactate
  • serum blood culture
  • Vitals currently are as follows
  • Vitals T 38.7, HR 112, RR 23, BP 87/65
  • You transfer her via ambulance to the UCLA
    Emergency Department for source control. Two
    additional IV fluid boluses are given in the
    ambulance, and vitals improve by time of arrival
    in the ED. She remains febrile with poor PO
    intake and is admitted to the ICU with
    meningococcemia and dehydration. She heals well,
    is transferred to the floor, discharged home
    after three days of IV antibiotics and
    hemodynamic monitoring.

23
Sepsis Resuscitation Bundle (Delayed)
  • Time 1400
  • Your patient successfully receives all four
    aspects of the sepsis resuscitation bundle, but
    due to late recognition of symptoms of SIRS
    (Systemic inflammatory response syndrome) and
    suspected sepsis, IV antibiotics and early fluids
    are delayed by 3 hours. The relative risk of
    mortality increases approximately 10 for every
    hour that bundle implementation is delayed.
  • The 4 parts of the Sepsis Resuscitation Bundle
    are
  • up to three- 20 cc/kg boluses normal saline,
    directed to hemodynamics
  • broad spectrum IV antibiotics within 1 hour of
    presentation
  • baseline serum lactate
  • blood culture prior to antibiotic administration
  • Vitals currently are as follows
  • Vitals T 39, HR 130, RR 34, BP 90/65
  • You transfer her via ambulance to the UCLA
    Emergency Department for higher level care and
    source control. Two additional IV fluid boluses
    are given in the ambulance, and vitals are
    improved by time of arrival in the ED. Due to
    delay in antibiotics, she remains in the ICU on
    IV antibiotics and is transferred to the floor
    after one week of supportive care.

24
BILBIOLOGRAPHY Bochud PY, Bonten M, Marchetti O,
et al. Antimicrobial therapy for patients with
severe sepsis and septic shock An evidence-based
review. Crit Care Med. 200432(Suppl.)S495S512.
  Booy R, Habibi P, Nadel S, et al. Meningococcal
research group reduction in case fatality from
meningococcal disease associated with improved
healthcare delivery. Arch Dis Child 2001
85386-390. Bone M, Diver M, Selby A, Sharples
A, Addison M, Clayton P. Assessment of adrenal
function in the initial phase of meningococcal
disease. Pediatrics. 2002 Sep110(3)563-9.   Bone
RC. Immunologic dissonance a continuation
evolution in our understanding of the systemic
inflammatory response syndrome (SIRS) and the
multiple organ dysfunction syndrome (MODS). Ann
Int Med 1996 125680-7.   Brierly J, Carcillo
JA, Choong K, et al. Clinical practice parameters
for hemodynamic support of pediatric and neonatal
patients in septic shock 2007 update from the
American College of Critical Care Medicine. Crit
Care Med. 200937(2)666-668.   Briegel J,
Vogeser M, Annane D, et al. Measurement of
cortisol in septic shock Interlaboratory
harmonization. Am Rev Respir Crit Care Med. 2007
175A436   Carcillo JA, Davis AL, Zaritsky A.
Role of early fluid resuscitation in pediatric
septic shock. JAMA. 1991 2601242-1245.   Casarte
lli CH, Garcia PCR, Piva JP, Branco RG.  Adrenal
insufficiency in children with septic shock. J
Pediatr (Rio J) 200379(Suppl 2)S169-S76 Delling
er, RP, Levy, MM, Carlet, JM, et al. Surviving
Sepsis Campaign International guidelines for
management of severe sepsis and septic shock
2008. Crit Care Med. 2008 published correction
appears in Crit Care Med. 2008 361394-1396
36296-327   Han YY, Carcillo JA, Dragotta MA,
et al. Early reversal of pediatric-neonatal
septic shock by community physicians is
associated with improved outcomes. Pediatrics.
112793-799. Herbert PC, Wells G, Blajchman MA,
Marshall J, Martin C, Pagliarello G, Tweeddale M,
Schweitzer I, Yetisir E. A multicenter,
randomized, controlled clinical trial of
transfusion requirements in critical care.
Transfusion Requirements in Critical Care
Investigators, Canadian Critical Care Trials
Group. N Engl J Med. 1999 Feb 11340(6)409-17. K
umar A, Roberts D, Wood KE, et al. Duration of
hypotension prior to initiation of effective
antimicrobial therapy is the critical determinant
of survival in human septic shock. Crit Care Med.
2006 341589-1596   Lemson J, Nusmeier A, Van
Der Hoeven JG. Advanced hemodynamic monitoring in
critically ill children. Pediatrics 2011 1283
560-571 Rivers E, Nguyen B, Havstad S, Ressler
J, Muzzin A, Knoblich B, Peterson E, Tomlanovich
M. Early goal directed therapy in the treatment
of severe sepsis and septic shock. N Engl J Med
2001 3451368-1377 Watson RS, Carcillo JA,
Linde-Zwirble WT et al The epidemiology of
severe sepsis in the United States. Am J Respir
Crit Care Med 2003 167695-701. Wiedemann HP,
Wheeler AP, Bernarnd GR et al. Comparison of two
fluid management strategies in acute lung injury
2006 3542564-2575.
25
Reminders...
  • WHAT IS SEPSIS?
  • Systemic Inflammatory Response Syndrome SIRS
    2 or more of the following high or low white
    count, tachycardia, tachypnea, high or low
    temperature
  • Sepsis SIRS a suspected source of infection
    (ex., gangrenous toe, pneumonia, central line,
    mucositis)
  • Septic Shock sepsis hypotension (or signs of
    poor perfusion).
  • Signs of poor perfusion altered mental status,
    delayed cap refill, poor pulses, mesenteric
    ischemia (emesis, diarrhea), urine output lt
    1cc/kg/hr, hypoxia
  • WHAT IS A BUNDLE a group of treatments that
    improve outcomes when given together
  • Sepsis Resuscitation Bundle how to treat early
    sepsis
  • 20cc/kg IVF boluses, broad spectrum IV
    antibiotics, blood culture, lactate within 1 hour
    of presentation. You may use up to 60cc/kg in the
    early phase of sepsis and move to pressors if
    vitals do not normalize.
  • Sepsis Management Bundle how to direct fluids
    and pressors to markers of improved cardiac
    output
  • normal mental status, UOP gt 1cc/kg/hr, cap
    refill lt2 sec, normal MAP and CVP gt8, ScVO2 gt
    70. There are several monitoring devices that
    can help with hemodynamic monitoring, and the PA
    catheter is the gold standard (though use of a PA
    catheter has not been shown to decrease mortality
    from sepsis). Reduction in serum lactate does not
    accurately reflect improved cardiac output.
  • WHAT SHOULD I DO?
  • If blood pressure doesnt increase with fluids
    and pressors, consider CIRCI (Critical Illness
    Related Corticosteroid Insufficiency). A random
    cortisol level lt 15 is diagnostic and IV
    hydrocortisone can help. A ACTH stim test is not
    needed. CIRCI is especially relevant to those who
    have previously been on steroids.
  • Do not wait to start pressors till central access
    is obtained. Dopamine can be started at low doses
    via peripheral IV.
  • Mortality form sepsis almost doubles with every
    hour delay in resuscitation bundle and increases
    by 8 per hour with delays in IV antibiotics.
    Source removal is the ultimate treatment for
    sepsis. Advocate for your patients! Push fluids
    and antibiotics early!

26
Case 2
  • Inpatient Wards

27
History
  • Time 1330
  • HPI While on weekend call, you are asked to
    evaluate a a 12-year-old girl who is complaining
    of dizziness and shortness of breath. Your
    signout shows that she is day 45 from a bone
    marrow transplant. She has been afebrile for two
    weeks, and her WBC counts recovered enough
    earlier in the week to discontinue prophylactic
    antibiotics. Before they left, the primary team
    told you that they drained a 2-cm blood blister
    on the patients foot earlier in the day.

28
Physical Exam
  • Time 1330
  • Vitals T 37.8, HR 125, BP 105/75, RR 30, SpO2
    97RA
  • Physical Exam
  • General Thin girl lying in her hospital bed,
    mild distress
  • Neuro Appears anxious, expresses concern she is
    going to faint, somewhat confused when answering
    your questions.
  • HEENT Alopecia. MMM.
  • CVS Tachycardic. Normal S1/S2. No M/R/G present.
    Very brisk capillary refill x4 extremities.
  • Resp Good air movement. Mild tachypnea. Few
    scattered crackles heard in the lung bases.
  • Abd Soft, NT/ND.
  • Ext/Skin Warm throughout. Drained lesion on
    right foot is covered by a C/D/I dressing. There
    is some mild erythema surrounding that area and
    in the distal calf. She complains of tenderness
    to palpation of the calf of the affected side.

29
Initial Plan
  • Time 1345
  • Click on the next most appropriate step in
    management
  • Tell the RN that you will check back on the
    patient soon and plan to send blood and urine
    cultures if she becomes febrile gt38C
  • Place an additional IV, order an IVF bolus, and
    place on supplemental O2
  • Order an EKG, ultrasound of the bilateral lower
    extremities, and CTA of the chest
  • Using her portacath, send a CBC, BMP and coag
    panel and review her last CXR

30
Plan Rapid Response
  • Time 1430
  • You hear an overhead page for a rapid response to
    the patients room. Upon entering her primary
    nurse tells you that the patient fainted when
    trying to walk to the restroom. The fall was
    witnessed and she did not appear to have any head
    trauma, but since being placed back into her bed
    she appears to be very sleepy.
  • Repeat vitals T 38.5, HR 140, BP 100/70, RR 38,
    SpO2 95RA
  • The most appropriate next step in management is
    to
  • Place an additional IV, order an IVF bolus, and
    place on supplemental O2
  • Using her portacath, send a CBC and blood culture
  • Order a STAT head CT and review her medication
    administration record for any possible medication
    reactions that could be causing her symptoms

31
Plan Refractory Shock
  • Time 1530
  • The lab calls you and tells you that her platelet
    count is 15. When you go to tell the patient that
    she will require a transfusion, you are not able
    to arouse her. Repeat vitals demonstrate T 40, HR
    150, BP 85/60. You note skin erythema that has
    spread from her foot up her left leg. You start
    to initiate treatment for septic shock but the
    patient remains hypotensive and within a few
    hours the patient is requiring mechanical
    ventilation in the PICU. She dies later that
    night and you learn that her blood cultures were
    positive for Pseudomonas.
  • Restart the case

32
Plan Refractory Shock
  • Time 1445
  • Once arriving in the radiology suite the patient
    is found to be unresponsive. When the code team
    arrives she is found to be hypotensive. Sepsis is
    suspected and although appropriate treatments are
    initiated in the PICU, the patient dies within
    the next few hours. A blood culture obtained
    prior to death is found to be positive for
    Pseudomonas.
  • Restart the case

33
Plan Awaiting Studies
  • Time 1410
  • You review the EKG and note only sinus
    tachycardia. The laboratory technician has not
    yet arrived for the ultrasound and you are told
    that it will be at least a few hours before the
    CTA can be arranged. The nurse tells you that the
    patient becomes febrile.
  • The most appropriate next step in management is
    to
  • Place an additional IV, order an IVF bolus, and
    place on supplemental O2
  • Using her portacath, send a CBC and blood culture

34
Plan Awaiting Lab Results
  • Time 1405
  • Upon review of her CXR from yesterday, there is
    no evidence of infiltrates. While awaiting the
    lab results you hear an overhead page for a rapid
    response to the patients room. Upon entering her
    primary nurse tells you that the patient fainted
    when trying to walk to the restroom. The fall was
    witnessed and she did not appear to have any head
    trauma, but since being placed back into her bed
    she appears to be very sleepy.
  • Repeat vitals T 38.5, HR 140, BP 100/70, RR 38,
    SpO2 95RA
  • The most appropriate next step in management is
    to
  • Place an additional IV, order an IVF bolus, and
    place on supplemental O2
  • Order a STAT head CT and review her medication
    administration record for any possible medication
    reactions that could be causing her symptoms

35
Plan Bolus Infusing
  • Time 1420
  • The IV access is placed and the bolus starts
    infusing. The high flow nasal cannula is
    initiated and the patient appears slightly more
    comfortable, but is also starting to complain
    that she is very sleepy. Her repeat vital signs
    demonstrate T 38.5, HR 130, BP 100/70, RR 38,
    SpO2 98 10L HFNC. Her exam is significant for
    decreased responsiveness, brisk capillary refill,
    bounding pulses, and an unchanged respiratory
    exam. You check a point-of-care blood glucose
    level which is normal. STAT electrolytes and a
    CBC are pending.
  • The most appropriate next step in management is
    to
  • Order a STAT CXR, STAT head CT, and review her
    medication administration record for any possible
    medication reactions that could be causing her
    symptoms
  • Repeat the fluid bolus

36
Plan Repeat Bolus
  • Time 1440
  • You repeat the fluid bolus two more times but her
    vital signs have not improved. She remains
    confused and difficult to arouse. The crackles
    you had heard on her initial exam are now more
    diffuse and her work of breathing has increased.
    Her laboratory results are still pending.
  • The most appropriate next step in management is
    to
  • Start broad spectrum antibiotics and begin an IV
    inotrope
  • Order a STAT echocardiogram and consult cardiology

37
Plan Inotropes Initiated
  • Time 1500
  • Dopamine is started and the first doses of
    antibiotics are given. The patient is transferred
    to the PICU where she requires intubation. Her
    status remains critical for the next 24 hours,
    but she eventually fully recovers from what is
    discovered to be Pseudomonal sepsis.

38
Plan Awaiting Studies
  • Time 1500
  • While awaiting the echocardiogram and cardiology
    consult the patient becomes unresponsive. When
    the code team arrives she is found to be
    hypotensive. Sepsis is suspected and although
    appropriate treatments are initiated in the PICU,
    the patient dies within the next few hours. A
    blood culture obtained prior to death is found to
    be positive for Pseudomonas.
  • Restart the case

39
BILBIOLOGRAPHY Bochud PY, Bonten M, Marchetti O,
et al. Antimicrobial therapy for patients with
severe sepsis and septic shock An evidence-based
review. Crit Care Med. 200432(Suppl.)S495S512.
  Booy R, Habibi P, Nadel S, et al. Meningococcal
research group reduction in case fatality from
meningococcal disease associated with improved
healthcare delivery. Arch Dis Child 2001
85386-390. Bone M, Diver M, Selby A, Sharples
A, Addison M, Clayton P. Assessment of adrenal
function in the initial phase of meningococcal
disease. Pediatrics. 2002 Sep110(3)563-9.   Bone
RC. Immunologic dissonance a continuation
evolution in our understanding of the systemic
inflammatory response syndrome (SIRS) and the
multiple organ dysfunction syndrome (MODS). Ann
Int Med 1996 125680-7.   Brierly J, Carcillo
JA, Choong K, et al. Clinical practice parameters
for hemodynamic support of pediatric and neonatal
patients in septic shock 2007 update from the
American College of Critical Care Medicine. Crit
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