Fever in children

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Fever in children

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Title: Fever in children

1
Fever in children

Dr. Osama Kentab, MD, FAAP, FACEP
Assistant Professor of Paediatrics and emergency
Medicine
King Saud Bin Abdulaziz university for Health
sciences
Riyadh

2
Epidemiology

Very common sign and symptom of illness in
childhood
May be indicative of an infection that is local
or systemic benign or invasive life
threatening
Normal body physiological reaction to pyrogen
( infective, inflammatory)

3
Thermoregulation

Central thermostat
Thermoregulatory center in hypothalamus
Receive input from
-Peripheral receptors
-Temp of blood around hypothalamus
Acts on autonomic,endocrine behavioral
mechanisms

4
Physiologic changes controlling body temp

Set point decreases to normal
Heat loss
-obligate heat loss
-vasodilatation
-sweating
-cold preference behavior
(65 Radiation,30 evap)

Set point increases
Heat generation
-? cell metabolism
-muscle activity
-involuntary shivering
Heat conservation
-vasoconstriction
-heat preference behavior

5
Body temperature variations

Age
Time of the day (Less in small infants).
Sex MgtF
Race? Black gt white
Environmental (false fevers)
-Ambient air temp -Excess
bundling
-Feeding (within 1 hour) -Exercise
-Teething (50 will have a new temp on day of
eruption

6
Implications of ?body temperature

Is it beneficial?
Rate of bacteraemia is 2-3 in all febrile
infants lt 2months (Baker 1999 Kadesh et al 1998)
Infants lt 2 months differ are less
immunocompetent unique group of bacteria (GBS,
Gram. Neg bacteria listeria)
Young infants show relative inability to
demonstrate clinical evidence of illness

7
What is the normal temperature?

Rectal 36.6 to 38 C
Ear 35.8 to 38
C
Oral 35.5 to 37.5
C
Axillary 34.7 to 37.3 C
Canadian pediatric society statement,Pediatric
Child Health 2000

8
Measurement sites

Core body temperature
Rectal / Oral /Axillary /TM
-indirect
-artifact
-lag time

9
Rectal Temperature

Slow to change in relation to changing core
temperature
Affected by the depth, local blood flow and
presence of stool
Rectal perforation has been described
?Gold standard
Robinson,J Pediatr,1998

10
Recommended Sites

lt 2 yrs 1.Rectal
(definitive)
2.Axillary
(screening)
2-5 yrs 1.Rectal
2.Tympanic
3.Axillary
gt 5 yrs 1.Oral
2.Tympanic
3.Axillary
Canadian pediatric society statement,Pediatric
Child Health 2000

11
Assessment Relevant history

Duration of fever
Pattern of fever intermittent or continuous
Hx of contact family members, friends, school
mates
Hx travel abroad country visited
Malaria endemic regions, enteric fever (Africa,
Asia) Travel immunization, malaria prophylaxis
Travel to mountainous region, camping in forest
(Rickettsial infection, Lyme disease)
Hx of Immunization

12
Relevant symptoms

Systemic symptoms Resp, ENT, Renal, GI
Rash Pattern/type (macular, papular, ulcerative,
erythematous, blanching)
Distribution (mucosal involvement-conjuctivitis,
mucositis, buttocks and extremities(HSP) Oral
ulcers (aphthous, herpes gingivostomatitis)

13
Relevant clinical signs

Unwell Toxic
Haemodynamic instability
Rash
Lower Respiratory signs
Joint involvement Arthritis/ Athralgia Reactive
viral arthritis, Septic arthritis, HSP, Rheumatic
fever, Chronic arthritis of childhood
Organomegaly Hepatomegaly, Splenomegaly, /-
Anaemia Systemic illness, Septicaemia,
Lymphoproliferative disorders

14
Causes of febrile illnesses in childhood

Common causes
URTI (viral or bact.)
LRTI
Gastroenteritis
UTI
Oral (dental abscess, hyperangina, herpetic
gingivitis, mumps)
MSS (septic arthritis, osteomyelitis, cellulitis

Serious causes
URTI (epiglottitis, croup, retropharyngeal
abscess)
LRTI
GI (appendicitis)
CNS (Meningitis, encephalitis)
Systemic (meningococcaemia, toxic shock syndrome

15
Protocols for Identification of Low Risk Infants Protocols for Identification of Low Risk Infants Protocols for Identification of Low Risk Infants Protocols for Identification of Low Risk Infants Protocols for Identification of Low Risk Infants
Rochester 1985-1988 Boston 1992 Philadelphia 1993-1999 Pittsburgh 1999-2000
Age(days) 0-60 28-89 29-56 0-60
Past health gt37 wk,home with or before mom,no susequent hosp,no prenatal, post,or current ATB,no treatment for unexplained hyperbole,no chronic diseases - No known immundef. Rochester
Temp C ?38.0 ?38.0 ?38.0 ?38.0
Infant Obs.score no Yes Yes no
WBC 5-15,000 lt20,000 lt15,000 lt5gt15
Bands/BNR - lt1.5x10?/L lt0.2 BNR no
LP No Yes Yes lt8 wbc Yes ? 5
urine 10WBC/hpf - 10WBC/hpf EUA ? 9
Stool(if diarrhea) 5 wbc/hpf - - lt 5
CXR - - Yes Neg if sx
ATB(Ceftrx) No Yes No 34.7??
SBI in low risk Pts () 1.1 5.4 0 0
NPV() 98.9 94.6 100 100
Sens () 92.4 Not stated 100 100
16
Age lt 29 days

CBCD, glucose,BUN,Creat,lytes, /- cap.gasses
Blood culture
Urine cath (microscopy and culture)
LP (if infant unstable defer)
CXR (suspected respiratory disease)
NPW (suspected viral respiratory disease)
Stool for WBC, culture and heme test (suspected
eneteric infection)

17
Age lt 29 days

Contd
Supportive care
Antibiotics
Ampicillin AND
Gentamycin OR Ceftriaxone/Cefotaxime
Consider Acyclovir
Admit

18
29 to 60 days

CBCD, BNR
Blood culture
LP (if infant unstable defer)
Urine cath (microscopy and culture)
CXR (suspected respiratory disease)
Stool for WBC, heme test and culture (suspected
enteric infection)

19
29-60 days Low risk

Past history
Born gt37 wks
Home with or before the mother
No subsequent admission
No prenatal,postnatal,or current antibiotics
No treatment for unexplained hyperbilirubinemia
No known immune deficiency

20
29-60 days Low risk

P/E
Appears generally well (non-toxic)
No evidence of skin,soft tissue,bone,
joint,or ear infection

21
29-60 days Low risk

Laboratory
WBC gt5k lt15k
ANC lt10K or band/neutrophil ratio lt 0.2
Urine lt10 WBC/hpf, spun and negative Gram stain
CSF Non-bloody ,lt 8 WBC , normal glucose,
protein, negative Gram stain and latex agg.test
Normal CXR (if it was done)
Stool (if diarrhea) lt5 wbc/hpf

22
29-60 days Low Risk

Option II
Ceftriaxone 50 mg/kg IV or IM
Re-evaluate in 24 hours and 48 hours
Optional second dose of ceftriaxone at second
visit

Option I
No antibiotics
Admit for observation OR
Re-evaluate in 24 48 hours

Discharge only if Reliable caregiver Has nearby
telephone Adequate transportation
23
61-90 days Low Risk

Option I
No LP
No antibiotics
Admit for observation OR
Re-evaluate in 24 hours

Option II
LP if normal
Ceftriaxone 50 mg/kg (IV or IM) OR
NO antibiotics
Admit for observation.
OR
Re-evaluate in 24 hours

Discharge only if Reliable caregiver Has nearby
telephone Adequate transportation
24
29-90 days High risk

Toxic
Positive labs
Concerning history /social factors

Admit
Supportive care
Meningitis
Ceftriaxone and Vancomycin
Non-meningitis
Ampicillin and
Ceftriaxone OR Gentamycin

25
3-36 months

Toxic looking
Fever, meningeal signs, lethargic, limb,
mottled
Admit, septic work-up, parenteral antibiotics
Focal bacterial infection
OM, pharyngitis, sinusitis, etc (excluding SBI).
Oral/parenteral antibiotics, outpatient care
Well looking
Risk for occult bacteremia and serious
bacterial infection
Previous decision analysis( Pre-H. flu
immunization)
Current decision analysis

26
3-36 months

High risk/toxic
Admit
Supportive care
Septic work-up
IV antibiotics
Meningitis----gtVanco Ceftriaxone
Non-meningitis ----gt Ceftriaxone

27
3-36 months

Non-toxic
If lt3 yrs,temp gt39
Obtain CBC,Blood culture,Urinalysis culture
Stool culture,CXR as indicated
If WBCgt15k ---gtEmpiric antibiotics
(Ceftriaxone,Clavulin,Biaxin, omnicef or
Suprax )
If urine is positive treat as UTI
If WBC normal ,urine is negative no therapy
needed

28
3-36 months

Contd
IF Temp lt 39, Non-toxic, No focus of infection
NO INVESTIGATIONS ARE REQUIRED
Follow up all in 24 hours

29
Management of fever in children with underlying
illness
30
Oncology patients

At risk of overwhelming sepsis
CBC, CXR, blood culture, urine culture, and LP
when clinically indicated
Neutropenic patients at risk for Pseudomonas and
other gram negative
Broad spectrum antibiotics

31
Acquired Immunodeficiency Syndrome

Repeated risk of infection with common bacterial
pathogens, risk of Pneumocytsis carinii,
mycobacterial infections, cryptococcosis, CMV,
Ebstein-Barr virus.
Low CD4 septic work up and broad spectrum
antibiotic

32
Sickle Cell Anemia

Functional asplenia susceptible to overwhelming
infection esp. encapsulated organisms such as
pneumococci and H. flu
Parvovirus can cause aplastic crisis
Osteomyelitis should be suspected in fever and
bone pain
CBC, retics,blood culture, stool culture, and
urine culture recommended
Ceftriaxone
Hospitalization recommended

33
Congenital Heart Diseases

Children with valvular heart disease are at risk
for endocarditis
Fever without obvious source with a new or
changing murmur hospitalization, serial blood
cultures, echo, antibiotics against S.viridans,
S aureus, S. fecalis, S. pneumo,
enterococci, H. flu, and other gram neg rods
Suggested antibiotics include Vancomycin and
Gentamycin until cultures are known

34
Ventriculoperitoneal shunts

Must be evaluated for shunt infection esp if
patient displays headache, stiff neck, vomiting,
or irritability
Shunt reservoir should be aspirated and examined
for pleocytosis and bacteria
Most common pathogen is S. epidermidis
CT head also warranted

35
Febrile Seizures

455 children with simple febrile seizure
-1.3 with bacteremia
-5.9 UTI
- 12.5 with abnormal chest x-ray
-Normal CSF in all who had an LP (135)
Trainor J, et al Clin Pediatr Emerg Med 1999

36
Febrile Seizures

486 children with bacterial meningitis
-complex seizures present in 79
-93 of those with seizures were obtunded
-of the few with normal LOC, 78 had
nuchal rigidity
Green SM, et al Pediatrics 1993

37
Febrile Seizures

Synopsis of the American Academy of Pediatric
practices parameters on the evaluation and
treatment of children with febrile seizures
LP strongly considered in the first seizure in
infants less than 12 month because signs and
symptoms of meningitis may be absent in this age
group
12-18 months LP should be considered because sign
of meningitis may be subtle in this age group
18 months LP only if signs and symptoms of
meningitis
(Peditrics 1999)

38
Febrile Seizures

Routine lab (CBC, lytes, Ca, phos, Mg, or
glucose) should not be performed in simple
febrile seizure
Neuro-imaging should not be performed routinely
on simple febrile seizure
EEG is not performed in a neurologically healthy
child with simple febrile seizure
Anticonvulsant therapy is not recommended in
simple febrile seizure

39
DDx Fever with rash

Viral exanthems
Streptococcal infection
Staphylococcal scalded skin syndrome / Toxic
shock syndrome
Kawasaki disease
Meningococcal disease
Henoch Schonlein purpura (HSP)

40
Measles

paramyxo virus
Spread by respiratory droplets
Incubation period 7 12 days
CF prodromal period (fever, conjuctivitis,
coryza, dry cough, koplik spots /-
lymphadenopathy) florid maculopapular rash
appearing over head and neck spreading to cover
the whole body X 3-4 days
Infectious from the prodromal period until 4 days
after rash appeared
Dx Measles Antibodies in saliva or serum
Complications OM, pneumonia, encephalitis,
subacute sclerosing pan encephalitis

41
Chicken pox (Varicella)

varicella zoster DNA virus, IP 14 21 days
Fever malaise X 5-6 days followed by crops of
skin lesions that go through stages of macules,
papules, vesicles, and crusting
Infectious 2 days before rash until vesicles
dry/crust
Complications Secondary bact. Infection of
lesions, haemorrhagic varicella, pneumonia,
encephalitis, ataxia at 7-10 days after rash
Severe illness in immunocompromised adults, preg.
Women neonates

42
Rubella (german measles)

RNA rubella virus
Incubation period 14 21 days
Fever, rash, posterior cervical lymph node
Complications Deafness,encephalitus, Congenital
rubella syndrome
Rx Symptomatic

43
Roseola infantum (Human herpes virus type 6)
44
Roseola infantum

Caused by Human herpes DNA virus type 6 7
Many children already infected by 2 years
Incubation period 5- 15 days
CF short febrile illness x 3- 5 days and an
erythematous rash
Complication Meningoencephalitis Sz

45
Erythema infectiosum (Fifth dis/ Slapped cheek
dis)

Human parvo virus B19
Incubation period 7 17 days
Head ache malaise
rash on face ( slapped cheek app.) spreading to
the trunk and limbs with maculopapular lesion
evolving to a lace- like reticular pattern
Complications Aplastic crisis with underlying
chronic haemolytic anaemia, Aseptic meningitis,
Hydrops fetalis

46
Hand, Foot Mouth disease

Caused by coxsackie A16, A19 and Enterovirus 71
RNA viruses
Incubation period 4 7 days
CF fever, malaise , head ache, pharyngitis,
vesicular lesions on the hands and feet including
palms soles
May be complicated by chronic recurrent skin
lesions
Rx Symptomatic

47
Infectious mononucleosis (Glandular fever)

Ebstein Barr (DNA) virus
CF fever, lymphadenopathy, tonsillitis,
headache, malaise, myalgia, splenomegaly,
petechiae on soft palate, rash (macular,
maculopapular, urticarial or erythema multiforme)
DX EBV specific IgM Paul Bunnell test
Complication Splenic rupture, ataxia, facial
nerve palsy, aplastic anaemia, interstitial
pneumonia
Rx Symptomatic

48
UTI in childhood

UTI is common
VUR is assoc with renal scarring particularly in
the 1st year pf life
chronic renal failure
Neonates irritability, refusal of feeds,
vomiting, FTT, prolonged NNJ, toxic/extremely
unwell
Pre-school vomiting, poor wt. Gain, fever,
malaise, freq, dysuria, enuresis, haematuria,
loin pain

49
UTI

Inv Urine m/c/s x 2 (or 1 SPA urine sample)
mid stream, clean catch, bag, SPA urine sample
Pyuria, organism on microscopy
Significant bacteruria gt 10 5 org/ml or and
growth from SPA
Treatment Antibiotics PO or iv
Commence low dose prophylactic antibiotic
Refer to the Paediatrician for further
investigations

50
Meningococcal disease

Gram neg. diplococci
Nasopharyngeal carriage in 25
Invasive disease in 1 carriers
15 meningitis 60 Septicaemia endotoxaemia
fulminant septicaemic shock with circulatory
failure wide spread purpura
Rx Antibiotics management of shock, anticipate
ventilatory failure
Transfer to PICU and contact public health dept
Prognosis Poor if lt1 year, better if evolution
of ds slower overall mortality approx. 30

51
Kawasaki disease

Systemic vasculitis of early childhood
80 cases lt 4 years MF ratio 1.51
No single diagnostic test 5/6 clinical criteria
fever gt5 days
Changes in the mucous membrane of URT
Changes in the peripheral extremities (oedema,
desquamation
Polymorphous rash (urticarial, maculopapular,
multiforme)
Cervical lymph adenopathy
Exclusion of staphylococcal streptococcal
infection others (Measles, drug reaction, JCA)
Coronary aneurysm fever 3 / 4 criteria

52
Kawasaki disease

Other features irritability, arthritis, aseptic
meningitis, hepatitis, hydropic gall bladder
20-30 Myocarditis, pericarditis, arthymia,
cardiac failure, coronary aneurysm
Rx High dose IV Ig 2g/Kg over 12-18 hrs
High dose Aspirin 30mg/Kg/day until fever
resolves then 3-5mg/Kg/day
Cardiac echo for coronary aneurysm

53
Investigation

According to the differential diagnosis
Indicated if child is unwell and or no cause
identified
full infection screen
Urinalysis Urine m/c/s
where no focus of infection
All children lt2 years where SS of UTI is non
specific and diagnosis has implication for future
management
With urinary symptoms
Before starting antibiotics

54
Complete Infection Screen