Neonatal Sepsis Alicia Pacala, RN BSN Prepared for MSN 621 Advanced Pathophysiology (Spring 2006)...
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Transcript of Neonatal Sepsis Alicia Pacala, RN BSN Prepared for MSN 621 Advanced Pathophysiology (Spring 2006)...
Neonatal Sepsis
Alicia Pacala, RN BSN
Prepared for MSN 621 Advanced Pathophysiology (Spring 2006)
Alverno College
Welcome !!Instructions on use
of Tutorial:
To start Tutorial:
tutorial
InstructionsInstructions Causes
Symptoms
Diagnosis
Treatments
Summary
What is Neonatal Sepsis?
Objectives
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Tutorial Objectives
Completing this tutorial will provide the learner with a better
understanding of Neonatal Sepsis:
* Pathology
* Causes
* Symptoms
* Diagnosis
* Treatments
What will I learn?
What is Neonatal Sepsis?
Neonatal Sepsis is a term
used for a severe infection
in newly born infants.
It can cause death if not recognized and treated properly.
Image used with permission and provided by www.steliz.org/newborn_center.htm
More facts about Neonatal Sepsis
Neonatal Sepsis affects approximately 2 infants per 1000 births with a higher incidence in premature & low birth weight infants [2].
There are two types of Neonatal Sepsis:
Early Onset
Late Onset
* This tutorial will focus primarily on Early Onset Sepsis
Causes of Neonatal Sepsis
The primary causes of Neonatal Sepsis are bacteria, such
as Staphylococcus and Group Beta Strep (GBS).
Bacteria may be the cause of neonatal sepsis, but neonates are more susceptible to these bacteria for two reasons [3&6]:
Immature immune response
Genetic predisposition
What makes a neonate’s immune system immature?
Normally an immune system responds to a pathogen in a specific manner, but if there are problems with any element
the immune system is unable to function properly [3&6].
Pathogen enters body
Neutrophils move in
Chemotaxis occurs
Opsonization causes phagocytosis
Monocytes kill pathogen
pathogens can enter a neonate’s body in many ways !
Pathogens can enter through the prenatal, perinatal, and postnatal periods [6].
Prenatal Maternal Substance Abuse
Premature Rupture of Membranes (>18 Hours)
Maternal Infection
Perinatal Microbial Colonization at Birth
Maternal Infection
Vaginal Exam of Mother
Postnatal Invasive Catheters
Endotracheal Intubation
Exposure to Nosocomial Microorganisms
Neutrophils: An important cell in immunity against pathogens
Neonatal neutrophils are deficient in
their ability to adhere to vessel walls at site of infection [2&6].
Further release of neutrophils
depletes a neonatal storage
pool because the bone marrow
storage of a neonate is only 20-30%
of the pool in an adult [2&6].
Neonatal neutrophils have a
decreased ability to “deform” &
migrate into tissues [2&6]. Neutrophils
Red Blood Cells
Image provided with permission from http://en.wikipedia.org/wiki/Image:Segmented_neutrophils.jpg
Chemotaxis
Imagine: Being in a dark tunnel without any direction or a way out. Finally you see light. You move towards the light and get out of the tunnel. Well this is like chemotaxis. The sun is the chemoattractant attracting you out to the world!!
Neonatal neutrophils have
decreased chemotaxis due to
decreased chemoattractant
Production [2&6].
Chemoattractants attract
neutrophils to the site of infection
[2&6].
Neonatal neutrophils therefore
cannot reach the site of infection
because of the chemotaxis
deficiency caused by decreased chemoattractant production.
OpsonizationOpsonization is the coating of a
pathogen with antibodies that makes it susceptible to phagocytosis [2&6].
Phagocytosis is the process of cells (phagocytes) engulfing, ingesting, &
destroying pathogens [2&6].
Neonates have a decreased amount of opsonins (antibodies that promote
opsonization) [2&6].
Opsonization
Pathogen
Monocytes: Another important cell in the fight against pathogens
Monocytes are a type of White Blood Cell that ingests pathogens.
Neonates have a sufficient amount of monocytes and full capability to kill
organisms [2], but because of a neonates deficiencies previously
discussed very few monocytes get to the site of infection.
Image provided with permission and copyrighted by amaxa GmbH at www.amaxa.com/mission3.html
What makes a neonate’s immune system susceptible to sepsis?
OR
Maturity
Immaturity
You’re Right!!!!
The immaturity of a neonate’s immune system makes them MORE SUSCEPTIBLE to sepsis.
Not Quite! Try Again
Genetic Predisposition to Sepsis
Multiple factors play into a neonate’s response to infection and the possible development of sepsis. One of these factors is genetics. As science has moved into recognizing the human genome there have also been advances with finding genetic contributions to sepsis.
The body’s first response to infection requires recognition of the presence of a pathogen. After recognition has occurred the body responds appropriately to resolve the problem [3&14]. Many polymorphisms have been recognized within both of these phases and they have been implicated in influencing the susceptibility to and/or outcome from sepsis [3&14].
Let’s look further into these two phases to see the
effect polymorphisms have on neonatal sepsis:
Recognition Phase Response Phase
Recognition Phase
The body’s initial response to infection requires recognition of the presence of a pathogen [3].
Polymorphisms in genes coding for proteins involved in the recognition
of pathogens can influence the susceptibility to and/or outcome of neonatal sepsis [3].
Let’s look into two of these:Mannose-Binding Lectine (MBL)
Lipopolysaccharide (LPS)
Response PhaseAfter the initial recognition of a pathogen occurs the body responds by releasing elevated levels of proinflammatory cytokines followed by a release of anti-inflammatory cytokines [3]. This dual release of opposite cytokines helps the cytokines return to a baseline level and that enables the start of tissue repair to start [3].
It is generally accepted that an imbalance between proinflammatory and anti-inflammatory cytokines result in clinical manifestations of sepsis [3]. This Imbalance is due to polymorphisms in various proteins involved in the response to pathogens.
Let’s look into two of these :
Tumor Necrosis Factor (TNF) Interleukin 10 (IL-10)
LPS, a major component of bacteria, is a powerful stimulator of the innate immune response [3].
LPS elicits it’s response by binding to a cell surface receptor that is compromised of 3 proteins [3].
One of these proteins is TLR4.
TLR4 is required for LPS to respond.
When there are polymorphisms in TLR4 there is a reduced response to LPS and that enhances the
susceptibility to infection!
Lipopolysaccharide (LPS)
Mannose-Binding Lectin (MBL)
MBL has two primary immunodefensive roles [3]: – involved with opsonization– leads to activation of complement system, independent
of antibodies.
Polymorphisms cause deficiencies in MBL level [3].
This results in decreased levels of MBL. This deficiency
is associated with increased susceptibility to infections!
Tumor Necrosis Factor (TNF)
TNF is a proinflammatory cytokine that is responsible
for the initial activation of the inflammatory response [3&14].
There are several polymorphisms associated with an
increased secretion of TNF resulting in the susceptibility
to sepsis[3].
Interleukin 10 (IL-10)
IL-10 is an anti-inflammatory cytokine produced by primarily monocytes [3]. IL-10 helps regulate the
over expression of proinflammatory cytokines.
There are three polymorphisms noted that result in an
over expression of IL-10. This over expression is proposed to induce immunosuppression in bacterial
sepsis and therefore increasing mortality by inhibiting
bacterial clearance [3].
What effect do polymorphisms have in Neonatal Sepsis?
They make a neonate more susceptible to sepsis.
They have no apparent effect.
They make a neonate less susceptible to sepsis.
Not quite! Try again.
Great answer! You’re correct!
Polymorphisms cause either an over expression or under expression of
proteins and/or genes that have significant roles in the immune
response to infection. This alters their ability to properly function which
makes a neonate more susceptible to sepsis.
This is not correct! Try again!
Symptoms of Neonatal SepsisThe symptoms of neonatal sepsis are not concrete and vary
widely [9].
Tachypnea Heart Rate Changes
Feeding difficulties
Difficulty Breathing Temperature Instability
Jaundice Irritability
Why are symptoms so broad?
Symptoms
Symptom variability occurs because of the metabolic and inflammatory processes that occur in neonatal sepsis.
A neonate’s symptoms are rooted in
these two processes.
Let’s look more into these areas: Metabolism
Inflammation
Metabolism in Neonatal Sepsis
Sepsis can alter a neonate’s metabolism [11].
The Ebb & Flow Metabolic Response [11] best describes how a neonate’s metabolism is affected by sepsis.
Flow Phase
Ebb Phase
Ebb FlowThis is the initial phase and last only 1-3 days. This is how a neonate’s body
initially tries to compensate for losses that occur during sepsis. The body slows things down in order to let the body recover.
The Ebb Phase consists of several clinical manifestations [11]: – Hypometabolism – Decreased energy expenditure– Decreased cardiac output– Lowered oxygen consumption– Vasoconstriction
Flow PhaseThis is the phase that occurs after the initial Ebb Phase. If the body
doesn’t recover it goes into hyperdrive. This is partly due to the exaggerated inflammatory response (further discussion in inflammatory
process section). This phase leads to much of the mortality and morbidity related to neonatal sepsis [11].
The Flow Phase consists of several clinical manifestations [11]:– Hypermetabolism– Increased energy expenditure– Increased cardiac output– High oxygen consumption
What metabolic phase causes a neonate’s body into “hyperdrive”?
Hyper Phase
Flow Phase
Ebb Phase
This is not right!!
Wow! You’re so smart!!
The flow phase DOES put the neonate’s body into hyperdrive. This
phase leads to much of the mortality and morbidity in neonatal sepsis.
Not quite. Try again.
Inflammation in Neonatal Sepsis
It is widely known that sepsis occurs
because of an exaggerated
systemic inflammatory response (SIR) [12].
Let’s find out how this is true Inflammatory Process
Inflammatory Process
[12]
Pathogen enters body
Inflammatory mediators released (cytokines)
Injury to endothelium
Tissue factors released
Production of thrombin
Coagulation promotes clot formation
Increased activity of fibrinolysis inhibitors
Decreased fibrinolysis
Inflammation
Overall, the imbalance among inflammation, over coagulation, and decreased fibrinolysis are the cause for the majority of deaths in
sepsis [12].
How is Neonatal Sepsis Diagnosed?
There is no definite marker in neonatal sepsis, but there are determinants of infection.
When a neonate presents with sepsis symptoms a septic work-up
is completed [2]. What is included in a septic work up?
* Complete Blood Count (CBC)
* Blood & Urine cultures
* Lumbar Puncture (LP)
* Chest X-Ray
* Line cultures
Is there a diagnostic marker for neonatal sepsis?
True
False
Yeah!!! You are correct!
There is NOT a specific diagnostic marker, only determinants of infection (labs, x-rays).
Are you sure? Try again!
Treatments for Neonatal Sepsis
It is of vital importance that treatment is initiated as soon as sepsis is suspected, especially for those infants at risk.
Broad Spectrum Antibiotics (Ampicillin & Gentamycin) are the first line of defense against neonatal sepsis [2].
Why????
What are other recommendations/options?
Why is it so important to start antibiotic treatment?
If not treated as soon as sepsis is suspected a neonate is more likely to die from sepsis and it’s complications.
For this reason it is of vital importance that healthcare workers (nurses and physicians) notice and act upon even the most subtle changes in a neonates assessment, particularly those infants at risk (GBS+).
Treatment Recommendations
Antibiotics should be initiated after all cultures and lab work is completed to ensure proper diagnosis.
All neonates will remain on IV antibiotics until blood/urine culture results
come back in approximately 2-3 days. Further therapy will depend on
lab work results and the neonate’s response to treatment.* Every hospital/organization has an antibiotic protocol specific to their site.
Although antibiotic therapy is vital, it is just as important to continue the overall support of the neonate (i.e. respiratory & cardiac).
Summary
Neonatal Sepsis is a severe infection in neonates that has the ability to cause death if not
recognized and treated appropriately. The primary causes of sepsis are pathogens, such
as Staphylococcus and Group Beta Strep [2&6]. These pathogens can enter a neonate’s
body during the prenatal, perinatal, and postnatal period [6]. Although pathogens are the
culprit in sepsis, neonates have factors that make them more susceptible to sepsis. One
of these factors is the immaturity of the neonate’s immune system [6]. The second factor
is related to a possible genetic predisposition that is caused by polymorphisms [3&14]. A
Neonate’s symptoms in sepsis are broad and vary [9]. This is due in part to the
metabolic and inflammatory processes that occur in neonatal sepsis. Because symptoms
are broad and not very concrete, it is of vital importance that the healthcare professional
notice even the most subtle changes in a neonate’s assessment. When sepsis is
suspected a neonate will undergo a septic work up [2], which includes lab work and x-
rays. After lab work is completed intravenous antibiotics are initiated immediately and will
continue until lab work demonstrates no infection and the neonate shows no further
symptoms.
I hope you have enjoyed your experience and have learned some
new information about neonatal sepsis.
Contact Information: [email protected]
References1. Amaxa Biosystems. (n.d.). “Mission #3: Transfect human monocytes”. [Online image]. Retrieved March 22, 2006
from www.amaxa.com/mission3.html
2. Bellig, L.L. & Ohning, B.L. (2004). Neonatal Sepsis. Retrieved February 8, 2006, from emedicine:http://wwwemedicine.com/ped/topic2630.htm
3. Dahmer, M.K., Randolph, A., Vitali, S., & Quasney, M.W. (2005). Genetic polymorphisms in sepsis. Pediatric Critical Care Medicine, 6(3), 61-73. Retrieved February 23, 2006 from PubMed database.
4. Farlex Inc. (n.d.). The Free Dictionary. Retrieved March 30, 2006, from www.thefreedictionary.com
5. LaRosa, S.P. (2002). Sepsis. Retrieved February 14,2006, from The Cleveland ClinicWebsite: http://www.clevelandclinicmeded.com/diseasemanagement/infectiousdisease/sepsis.htm
6. McKenney, W.M. (2001). Neonatal nursing: Understanding the neonatal immune system: High risk for infection. Crtitical Care Nurse, 21(6), 35-58. Retrieved February 14, 2006, from ProQuest database.
7. Microsoft Corp. (2006). Microsoft Clip Art. Retrieved March 30, 2006, from www.microsoftclipart.com
8. Mrozek, J.D., Georgieff, M.K., Blazer, B.R., Mammel, M.C., & Schwarzenburg, S.J. (2000). Effect of sepsis syndrome on neonatal protein and energy metabolism. [Electronic version] Journal of Perinatology, 2, 96-100.
References9. Neonatal Handbook:Sepsis. (n.d.). Retrieved February 14, 2006, from
http://www.netsvic.org.au/nets/handbook/index.cfm?doc_id=898
10. Oostdyk, R. (2005). “Neutrophil”. [Online image]. Retrieved April 20, 2006, fromhttp://en.wikipedia.org/wiki/Image:Segmented_neutrophils.jpg
11. Orr, P.A., Case, K.O., & Stevenson, J.J. (2002). Metabolic response and parenteral nutrition in trauma sepsis and burns. Journal of Infusion Nursing, 25(1), 45-53. Retrieved March 7, 2006 from Ovid database.
12. Sharma, S. & Mink, S. (2004). Septic shock. Retrieved February 14, 2006, from emedicine: http://www.emedicine.com/MED/topic2101.htm
13. St. Elizabeth Hospital. (n.d.). “The newborn center at St. Elizabeth’s”. [Online image]. Retrieved March 22, 2006 from www.steliz.org/newborn_center.htm
14. Villar, J., Maca-Meyer, N., Perez-Mendez, L., & Flores, C. (2204). Bench to bedside review: Understanding genetic predisposition to sepsis. Critical Care, 8(3), 180-189. Retrieved February 23, 2006, from PubMed database.
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