Pediatric Fever - Global Emergency Health Medicine
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Transcript Pediatric Fever - Global Emergency Health Medicine
An Approach to Fever without a
Source in Infants and Children
Authors:
Dr. April Kam MD, DTMH, MScPH, FRCPC
Parnian Arjmand MSc, MD Candidate
Dr. David Goldfarb MD, FRCPC
Date Created: December 2012
Global Health Emergency Medicine Teaching Modules by GHEM is licensed under
a Creative Commons Attribution-NonCommercial-ShareAlike 3.0 Unported License.
Learning Objectives
Be able to define Fever Without a Source
(FWS)
Develop an approach to categorizing and
managing a child presenting with fever
Learn about some of the key red flags and
special circumstances for children
presenting with fever
Caveats…
Need to be aware of local epidemiology
Prevalence of infections can vary dramatically
based on geography, season, context of epidemic
Fever Differential Diagnosis can be quite
broad– we will only cover most commonly
seen entities
Broaden your differential, particularly in
immunocompromised children (e.g. HIV, severely
malnourished, etc.)
Caveats…(cont’d)
In many countries the epidemiology is
changing dramatically due to newly
introduced vaccines (e.g. Hib, PCV) and
the spread of HIV
Can often see co-infections
e.g. Among < 5 yr olds in Nigeria with confirmed
malaria, 9% also had UTI (Okunola PO et al., 2012)
Caveats… (cont’d)
Very little published data on the
management of fever without localizing
signs in children in the developing world
Drug resistance rates climbing dramatically
in the developing world…
Target Audience
Health care providers working at first level
referral centre – primary care hospital
Basic laboratory facilities (e.g. microscopy)
and medications available
Need to adapt to your facility based on
epidemiology, testing, and antimicrobials
available – know the local guidelines!
Main reference
Integrated Management of Childhood
Illnesses – Management of a Child with
Serious Infection or Severe Malnutrition
https://apps.who.int/chd/publications/referral_c
are/contents.htm
Definitions
Fever without a Source (FWS) or Fever
without Localizing Signs (FWLS) or Fever
without a Focus (FWF):
Rectal temperature > 38°C (> 101ºF) in an
infant or child w/ a physical exam that does not
suggest a focus of infection
Fever
An intrinsic adaptive response that
activates the immune system
Is controlled by the hypothalamus
Shortens the length of disease
Etiologies
Infection
Infection
Infection
Other causes much less likely
Inflammation – e.g. Kawasaki disease
CNS disorder – e.g. Hypothalamic dysfunction
Metabolic
Iatrogenic: drugs, immunizations
4 Major Categories for child
presenting with fever
Fever due to infection without localized
signs – i.e. FWLS (no rash) in > 2 mo
Fever due to infection with localized signs
(no rash) in > 2 mo
Fever with rash in > 2 mo
Special Situations/Red Flags
Young infant (7 days - 2 months) – high risk
serious bacterial infection
HIV infection
Severe Malnutrition
Differential Dx of FWLS (no rash)
Diagnosis of fever
In favour
Malaria (only in children
exposed to malaria
transmission)
•
•
•
•
Septicemia
• Seriously and obviously ill with no apparent cause
• Purpura, petechiae
• Shock or hypothermia in young infant
Typhoid
•
•
•
•
Seriously and obviously ill with no apparent cause
Abdominal tenderness
Shock
Confusion
Urinary tract infection
•
•
•
•
Incontinence in previously continent child
Vomiting with no diarrhea
Crying on passing urine or increased frequency
White blood cells, bacteria or nitrites on micro/UA
Fever associated with HIV
infection
• Signs of HIV infection (see red flags)
Blood film or rapid test positive
Severe anemia
Enlarged spleen
Jaundice
Differential Dx of Fever with
localizing signs (no rash)
Diagnosis of fever
In favour
Meningitis
•
•
•
•
Otitis media
• Red immobile ear-drum on otoscopy
• Pus draining from ear
• Ear pain
Mastoiditis
• Tender swelling above or behind ear
Osteomyelitis
• Local tenderness
• Refusal to move the affected limb
• Refusal to bear weight on leg
Skin and soft tissue
infection
•
•
•
•
LP positive
Stiff neck
Bulging fontanelle
Meningococcal rash (petechial or purpuric)
Cellulitis
Boils
Skin pustules
Pyomyositis (purulent infection of muscle)
Differential Dx of Fever with
localizing signs (no rash) – cont’d
Diagnosis of fever
In favour
Pneumonia
•
•
•
•
•
•
Viral upper respiratory
tract infection
• Symptoms of cough/cold (e.g. rhinorrhea)
• No systemic upset
Throat abscess
• Sore throat in older child
• Difficulty in swallowing/drooling of saliva
• Tender cervical nodes
Sinusitis
• Facial tenderness on percussion over affected sinus
• Foul nasal discharge
Cough with fast breathing
Lower chest wall indrawing
Fever
Coarse crackles
Nasal flaring
Grunting
Differential Dx of Fever with rash
Diagnosis of fever
In favour
Measles
•
•
•
•
•
•
Typical rash
Cough, runny nose, red eyes
Mouth ulcers
Corneal clouding
Recent exposure to a measles case
No documented measles immunization
Viral infection
•
•
Mild systemic upset
Transient non-specific rash
Meningococcal infection
•
•
•
•
Petechial or purpuric rash
Bruising
Shock
Stiff neck (if meningitis)
Relapsing fever
(borreliosis)
•
•
•
•
•
Petechial rash/skin haemorrhages
Jaundice
Tender enlarged liver and spleen
History of relapsing fever
Positive blood smear for Borrelia
Typhus
•
•
Epidemic of typhus in region
Characteristic macular rash
Dengue Hemorrhagic
Fever (or other HFs)
•
•
•
•
•
•
Bleeding from nose or gums, or in vomitus
Bleeding in stools or black stools
Skin petechiae
Enlarged liver and spleen
Shock
Abdominal tenderness
Special Situations/Red Flags
Young infant – 7 days to 2 months
HIV infected child
Severely malnourished child
Young infant 7 days – 2 months
Presume Serious Bacterial Infection
e.g. Pneumonia, sepsis, meningitis
Show less specific signs
Can present with Fever or Hypothermia
Irregular breathing, jaundice, apnea, grunting, seizure,
vomiting, abdominal distension, lethargy, anorexia
HIV infected or potentially infected
HIV infected children have higher risk of sepsis and
opportunistic infections
Signs common to HIV infected infants:
Recurrent infections, oral thrush, chronic parotitis,
generalized lymphadenopathy, hepatosplenomegaly,
persistent/ recurrent fever lasting >7 days, neurological
dysfunction, Herpes Zoster, HIV dermatitis
More specific signs: pneumocystic pneumonia, esophageal
candidiasis, lymphoid interstitial pneumonia, shingles or
Kapsosi sarcoma
Signs common to both HIV infected and non-infected infants:
chronic otitis media, persistent diarrhea, failure to thrive
Severe Malnutrition
Definition - edema in both feet or severe wasting
and weight for height < -3 SD or <70%
Assume that all severely malnourished children
have an infection (regardless of presence of
fever) and treat with antibiotics
On exam look for: dehydration, pallor, signs of
HIV infection/ local infection, fever, ulcers, skin
changes of kwashiorkor
HISTORY AND PHYSICAL
History
Duration of fever
Residence in or recent travel to an area with Plasmodium
falciparum (malaria) transmission
Skin rash
Stiff neck or neck pain
Headache
Pain on passing urine (generally child ≥ 3yr)
Ear pain – e.g. pulling on pinna
Immunizations
History (cont’d)
What was the temperature and how was it measured?
Level of activity prior and after onset of fever
Infection(s) during pregnancy or at birth
Ill contacts or recent travel history
Oral intake
Presence of lethargy/ irritability
Presence of cough/ vomiting
Urination frequency/ abdominal pain/ back pain/ new onset of
incontinence (e.g. UTI)
Protection of the affected area in deep soft tissue/ bone infection
Underlying medical conditions (e.g. sickle cell disease, urinary tract
reflux, etc.)
History (cont’d) - Immunizations
It is particularly important to know if Hib, pneumococcal, meningococcal
and/or yellow fever vaccines have been given and are up to date
Nearly all low income countries have now rolled out Hib vaccine
> 18 countries in developing world have also recently introduced
PCV
6 countries in sub-Saharan “meningitis belt” have just introduced
new meningococcal A conjugate vaccine
Rapid increase in number of children vaccinated against yellow
fever with assistance GAVI
Vaccination with the above conjugate vaccines (i.e. Hib, PCV)
dramatically reduces the risk of occult bacterial infection in
children presenting with fever without localizing signs
Physical Examination
Always fully undress child
General appearance (alert, playful, irritable, consolable,
lethargic)
Oxygen saturations (if available)
Stiff neck
Hemorrhagic skin rash - purpura, petechiae
Skin infections - cellulitis or skin pustules
Discharge from ear/red immobile ear-drum on otoscopy
Severe palmar/conjunctival pallor
Refusal to move joint or limb
Local tenderness
Fast breathing
Physical Examination
Toxic-appearing:
Lethargic: decreased level of consciousness/ poor eye contact, failure
to interact with environment or parents
Poor perfusion and cyanosis
Hypo/ hyperventilation
Woods, CR.
Purpura may be present
Epiglottitis
(supraglottitis):
Clinical features
and diagnosis.
In: UpToDate,
Basow, DS
(Ed),
UpToDate, Walt
ham, MA, 2012.
Physical Examination
Watch for signs of raised intracranial
pressure:
Bulging fontanelle
Poor feeding, Vomiting
Headache, Irritability
Papilledema
Lethargy, Seizures
Cushing’s triad: hypertension, widened pulse
pressure, bradycardia
Management: Fever in 2 month
– 3 year GROUP
Fever 2 months – 3 years
The first step is to determine if the child is
toxic looking i.e. septic
If the patient is septic, do septic work up and
start antibiotics, fluids, and provide oxygen
Fever 2 months – 3 years
In the non-septic child, the second step is
to determine if the fever is due to an
infection with or without localized signs by
doing a detailed history and physical
If a focus is found, treat accordingly
If no focus is found, investigate as FWLS or
Fever without a source
Fever 2 months – 3 years
Example of an institutional algorithm for
FWLS in the 2 m – 3 year age group
developed for Botswana referral hospital
(where there is very low/no malaria, no
typhoid, no dengue) is provided on the next
page
Algorithm: Fever without a Source – Ages 2 months to 3 years
Definition: Child between 2 months and 3 years with an axillary temperature > 37.5 and
no obvious source of infection after a thorough History and Physical
*Normal Rates
Child Appears Toxic
• Lethargic (not interacting with
caregivers/environment)
•Poorly perfused (cap refill > 2sec)
•Hypoventilating or tachypneic for age
Yes
No
Child is HIV positive, CD4 <25% or unknown or
child is HIV Exposed and HIV status unknown
No
Yes
T > 38.5 axillary
Yes
No
Tests: Blood Cx or FBC and then
Blood Cultures only if WBC > 15,000
UA and Cx: if Male < 6 mo, Female <
2 yr or T > 40
CXR: if dyspnea, cough/rales
LP: if < 15 mo, or associated with
seizure and does not meet criteria for
simple febrile seizure
•No diagnostic test
•Paracetemol 15mg/kg/dose
•Discharge home
•Return if fever > 48 hrs or seems
more sick
•NO Antibiotics
Age
Respiratory
2-12 months
<50/min
Heart
<160/min
1-2 years
<40/min
<120/min
2-5 years
<40/min
<110/min
6-8 years
<30/min
<110/min
Sepsis evaluation
•Blood Culture
•Urinalysis and Culture
•CBC
•LP if indicated by symptoms
•Consider malaria smear if indicated
Admit to Ward
Start empiric antibiotics- Cefotaxime
50mg/kg/dose 6 hourly
Treatment:- If any diagnostic tests are suggestive of a source for infection treat according to protocol for that diagnosis .
However, if no tests are indicated or all test are normal AND If FBC or WBC > 15,000 THEN -> Amox/Clav for 48 hours
If FBC or WBC < 15,000 then do not give antibiotics
ALL children regardless of whether they are given abx NEED: F/U in 48 hours if still febrile or at any time if they appear
more sick & Paracetemol 15 mg/kg/dose
Management – Presumed
Septicemia
Treatment
Give benzylpenicillin IV (50 000 units/kg every 6 hrs)
or ampicillin 50 mg/kg IM every 6 hrs) plus
chloramphenicol (25 mg/kg every 8 hrs) for 7 days
If significant drug resistance to these antibiotics among
Gram-negative bacteria, follow the local guidelines for
management of septicaemia may be a thirdgeneration cephalosporin such as ceftriaxone (80
mg/kg IV, once daily over 30-60 minutes) for 7 days
Management – Presumed
Septicemia (cont’d)
Supportive care
If a high fever of ≥ 39°C (≥ 102.2°F) is
causing the child distress or discomfort, give
paracetamol (15mg/kg/dose every 4 hours,
maximum 5 doses/day )
Fluid intake and nutritional management
Manage complications including seizures,
hypoglycemia, electrolyte abnormalities
Investigations for FWLS –
Depending on availability
Blood smear or rapid diagnostic test (RDT) for
malaria (if endemic)
LP if signs suggest meningitis (with no signs of
raised intracranial pressure, in stable patient)
Blood culture in suspected sepsis
Full Blood Count
Urinalysis/Microscopy
CXR – if pneumonia is suspected
Management: FEVER in
7 day – 2 month old GROUP
Management 7 day to 2 month old
Investigations:
Check glucose
Do Cultures – Urine and Blood
Do an LP
CXR if available
Management: Oxygen, Fluids, Antibiotics
Management 7 day to 2 month old
Ampicillin (50 mg/kg IM/IV every 6 hrs for 2
days) then oral amoxicillin (15 mg/kg every 8
hrs for 5 days) OR oral ampicillin (50mg/kg
PO every 6 hrs on an empty stomach for 5
days)
plus IM gentamicin (7.5 mg/kg once daily) for
a total of 7 days of therapy
You may continue IV Ampicillin beyond 2 days
if child continues to appear unwell
Management 7 day to 2 month old
(cont’d)
If S. aureus is known to be an important
cause of neonatal sepsis locally, or signs
suggestive of severe staphylococcal
infection (e.g. skin pustules), give IM
cloxacillin (50 mg/kg every 6-8 hrs
depending on age) plus IM gentamicin (7.5
mg/kg once daily)
Management 7 day to 2 month old Suspected or Confirmed Meningitis
Give IM ampicillin (50 mg/kg every 6-8 hrs
depending on age) plus IM gentamicin (7.5
mg/kg once daily). An alternative regimen
is IM ampicillin plus IM chloramphenicol (25
mg/kg every 6 hours).
Chloramphenicol should not be used in
premature infants and should be avoided in
infants in the first week of life
Some centres use third generation
cephalosporins
MANAGEMENT: SEVERE
MALNUTRITION
Investigations may include
Glucose (mandatory)
Labs: Hb/ Htc if severe pallor
Electrolytes (generally hypokalemic)
Blood culture
TB investigations
HIV testing, etc.
Management of child admitted with
severe malnutrition
Multidimensional management in two
phases of stabilization and rehabilitation
[see chapter 7 in the WHO manual]
Management of child admitted with
severe malnutrition
All severely malnourished children
receive
A broad-spectrum antibiotic
Ampicillin (50 mg/ kg IM/IV 6-hourly for 2 days) then oral
amoxicillin (15 mg/ kg 8-hourly for 5 days) OR oral ampicillin (50
mg/kg IM/IV for 5 days) over a total of 7 days
Gentamicin (7.5 mg/kg IM/IV) once daily for 7 days
If child fails to improve within 48 hours: add chloramphenicol
(25 mg/kg IM/IV 8-hourly) for 5 days
Local antibiotic regimen may be different
due to different resistance rates
Management of child admitted with
severe malnutrition
Measles vaccine if child > 6 mo (not
immunized) or > 9 month
Delay vaccination if in shock
MANAGEMENT: COMMON
INFECTIONS
Diagnostic Criteria for Urinary Tract
Infections
Clinical signs:
Malodorous urine/ hematuria
Abdominal tenderness/ suprapubic pain
Vomiting, irritability, diarrhea
Fever > 38 °C for over 24 hrs
Dysuria, vaginitis/ vulvalitis
Labs:
Urinalysis from suprapubic aspirate or transurethral catheter
Leukocyte esterase
Nitrite
WBC
Culture
Treatment of Urinary Tract
Infections
For Oral agents, be aware of local
susceptibilities – treatment include:
Amoxicillin/Clavulanate, First generation
cephalosporins, Quinolones
If <6months, or septic, require admission
and IV Ampicillin & Gentamicin
Other Common Infections
Malaria (seehttp://apps.who.int/medicinedocs/documents/s19105en/s19105en.pdf for
details)
Varies by severity, endemic species, and resistance patterns
Antimalarial treatment:
IM/IV Artesunate first line for severe malaria due to P. falciparum in
most regions (pre-referral rectal artesunate an option)
Measles
Two doses of Vitamin A to all children; immediately on diagnosis
and within 24 hours
Other Common Infections
Typhoid
Chloramphenicol (25 mg/ kg every 8 hours) for 14 days
If systemic signs/ upset: benzylpenicillin (50 000 units/ kg every 6
hours) for 14 days in addition to chloramphenicol (dosed as above)
Ear infections
Acute otitis media - Amoxicillin (50 mg/kg PO TID) X 7 days
Chronic suppurative otitis media – wicking and topical antibiotic such as
chloramphenicol drops if available
Summary
FWS: fever without a specific source in an acutely ill, temp
(rectal) > 38ºC (100.4ºF)
Infection is the most common etiology of FWS
There are four categories of infants presenting with fever: young
infant with serious risk of bacterial infection, infectious fever
without rash, fever due to infection with localized signs, and fever
with rash
Management strategies vary depending on geographical area,
access to resources, presentation, and infant age
Red flags to watch out for: severely malnourished infant, infant
with signs of HIV and young infant (7 days to 2 months)
General References
MANAGEMENT OF THE CHILD WITH A SERIOUS
INFECTION OR SEVERE MALNUTRITION
Guidelines for care at the first-referral level in
developing countries. WHO. 2000
IMCI UTI guidelines: Urinary Tract Infections in Infants
and Children in Developing Countries in the Context
of IMCI
http://whqlibdoc.who.int/hq/2005/WHO_FCH_CAH_05
.11.pdf
Credits
Dr. April Kam MD DTMH MScPH FRCPC
Assistant Professor, Pediatric Emergency Medicine
Department of Pediatrics, McMaster Children’s Hospital
Parnian Arjmand MSc MD Candidate
McMaster University
Dr. David Goldfarb MD FRCPC
Assistant Professor, Infectious Diseases
Department of Pediatrics, McMaster Children’s Hospital
Adjunct Senior Lecturer, University of Botswana