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Neonatal Septicemia Neonatal Septicemia Li Yijuan First Affiliated Hospital SUMS
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Neonatal septicemia

May 07, 2015

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Sumit Prajapati
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Page 1: Neonatal septicemia

Neonatal SepticemiaNeonatal Septicemia

Li Yijuan

First Affiliated Hospital

SUMS

Page 2: Neonatal septicemia

Will They Have Good Future ???

Page 3: Neonatal septicemia

Objectives

What will I learn?

Etiologies and risk factors

Symptoms

Diagnosis

Treatment

Page 4: Neonatal septicemia

Introduction

Common -20% of VLBW has sepsis

-In term 0.1%-Inter-institution difference 11-32% (NICHD net work)

Serious-mortality is 3-5 times more for infant with sepsis in NICU

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Page 6: Neonatal septicemia

What is Neonatal Sepsis?

Neonatal Septicemia is a generalized

infection characterized by the proliferation

of organisms in the blood circulation during

the first month of life.

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Some basic definitions

• SIRS(systemic inflammatory response syndrome ) - fever, tachypnoea, tachycardia, abnormal WBC

• Sepsis- systemic response to infection

• Severe sepsis- sepsis with organ dysfunction, hypotension

• Septic shock- severe sepsis with multiorgan

dysfunction

difficult to apply these definitions and a staging

system to the newborn

Page 8: Neonatal septicemia

Pathogen

• Staphylococcus • Escherichia coli• Conditional pathogen • Group B streptococcus

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Staphylococcus

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E. Coli

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• Staphylococcus epidermidis

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• Pseudomonas aeruginosa

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Klebsiella

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• Clostridium perfringens

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Group B -hemolytic streptococcus

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Route of Infection

• Prenatal infection

• infection during delivery

• postnatal infection

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Sepsis Risk Factors

• Prematurity

• Birth weight

– Term 0.1%

– 1,000 -1,500 g 10%

– <1,000 g 35%

– <750 g. 50%

• Delay enteral feeding and Prolonged TPN

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I.Risk Factors (maternal and neonatal)A.Major

1.Maternal prolonged Rupture of Membranes >24 hours 2.Intrapartum maternal fever >38 C (>100.4 F) 3.Chorioamnionitis 4.Sustained Fetal Tachycardia >160 beats per minute

B.Minor 1.Intrapartum maternal fever >37.5 C (>99.5 F) 2.Twin Gestation 3.Premature infant (<37 weeks) 4.Maternal Leukocytosis (White Blood Cell count >15000) 5.Rupture of Membranes > 12 hours 6.Tachypnea (<1 hour) 7.Maternal Group B Streptococcus Colonization 8.Low APGAR (<5 at 1 minute) 9.Low birth weight (<1500 grams) 10.Foul lochia

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What makes a neonate’s immune system susceptible to sepsis?

Maturity

Immaturity

or

Page 20: Neonatal septicemia

You’re Right!!!!

The immaturity of a neonate’s immune system makes them MORE SUSCEPTIBLE to sepsis.

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Why are newborns so vulnerable to infection?

Non-specific immunity

Specific immunity

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IMMUNE SYSTEM

Neutrophils –Qualitative

and quantitative

Complement andimmunoglobulinlevels decreased

T cells- antigenically naïve

limited cytokineproduction

Why are newborns so vulnerable to infection?

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• Poor skin barrier

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• Umbilical stump

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• Poor blood-brain barrier

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Classification

• Early onset sepsis (EOS):– bacteria acquired before and during delivery– 5-7/1000 live birth– 1.5% of VLBW infants had EOS (intrapartum

antibiotics)

• Late onset sepsis (LOS): – bacteria acquired after delivery (Nosocomial

or community)– 20% of VLBW infants

Page 27: Neonatal septicemia

Clinical menifestationsClinical menifestationsClinical menifestationsClinical menifestations

EOS LOS

Onset Within 7 days >7 days

Source Prenatal

During delivery

During delivery

Postnatal(nosocomial )

Pathogens G-bacili Staphylococcus;

Opportunitic

Presentation

Mortality

Pneumonia

High

Bacteremia and / or meningitis

Low

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Symptoms of Neonatal Sepsis

The symptoms are not concrete and vary widely

Tachypnea Heart Rate Changes

Feeding difficulties

Difficulty Breathing Temperature Instability

Jaundice Irritability

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Omphalitis

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Bleeding tendencyPoor perfusion

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Enlargement of liver and spleen

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toxical paralytic ileus

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NEC

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NEC

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dyspnea

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Clinical presentation

Early warning signs are often non-specific and subtle

easily confused with non-infective causes (e.g. apnea of prematurity, variation in environmental temperature or

acute exacerbation of chronic lung disease)

clinical course alarmingly fulminant

septic shock + DIC

death

Non-specific, multi- systems/organs involved

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Clinical manifestationClinical manifestation

The symptoms are so broad , non-specific,

and acute deterioration,

How to make a diagnosis as early as possible ?

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Laboratory studies

• Evidence for inflammation

• Evidence for infection

• Evidence for multiorgan system disease

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Laboratory Examination: CBC

• WBC<5×109/L or WBC>20× 109/L

• I/T≥0.2 , toxic granules

• thrombocytopenia <100×109/L

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Reference values for neutrophilic cells

Manroe BL, J Pediatr 1979;95:89-98.

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Total neutrophils

Immature neutrophil

I/T ratio

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Lab examination:CRP

• CRP

• α1-AG

• α1-AT

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Lab Exam: Organism detection

blood culture

culture of body fluid and secretion

plasma brown layer smear

--Detection of antigen: usually for antibody

of GBS or E coli in CSF, blood and urine

--Molecular biochemical method PCR

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Summary

Is there a diagnostic marker

for neonatal sepsis?

Page 46: Neonatal septicemia

Great answer! You’re correct!

• There is NOT a specific diagnostic marker, only determinants of infection

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Summary

The best approach for diagnosis of systemic bacterial infection:

• use of multiple markers (e.g. CRP, IL-6, TNF, CD64), and

• serial measurements

Page 48: Neonatal septicemia

Diagnosis • history

–high risk factors• clinical manifestation

--nonspecific S/S• lab results

- abnormal blood routine,

CRP, positive culture

or detection of organisms

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Therapy

• Infection should be the first thought

when an infant has symptoms

• Aggressive treatment should begin before

the diagnosis is confirmed.

• Therapy can be discontinued if sepsis is

excluded

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Treatment

Antibiotics therapy

management of complications

supporting therapy

Clearance of infectious focus

Immunotherapy

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Antibiotic therapy

• using antibiotics as early as possible

• choose antibiotics according to drug sensitivity

• giving drugs intravenously

• combine effective drugs to make synergism

• enough therapeutic course

• consider the possible side effects

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Dosages of antibiotics for newborns

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Supporting therapy

• Nursing care

--warm environment

--oxygen supply

• correction of acidosis and electrolyte

disturbance

• fluid , glucose and nutrition balance

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Management of complications

• Shock

• DIC

• Cerebral edema

• Pulmonary hemorrhage

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Immunotherapy

• IVIG

• Exchange transfusion

• Granulocyte transfusion , G-CSF

• Platelet transfusion

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Questions

• Could prophylatic IVIG reduce the

morbidity and mortality of neonatal

sepsis?

• Might prophylatic IVIG interfere the

development of the neonatal IM

system?

Page 57: Neonatal septicemia

Thank you for your attentionThank you for your attention