RomqvrstI.Grun N.Dalianis 1.Human papillomavirus and tonsillar andbase of tongue cancer.Viruses 2015;7:1332-1343.
Rea.P.Clinical anatomy of thecramal nerves.Academic Press.2014.
RosenTield RM.Schwartz SR. Pynnonen MA.et al.Clinical practice guideline:tympanostomy lubes inchildren.Otolaryngol Head Neck Surg 2013:49:S1-S33.
RosenfeldRM.Brown L.Cannon CR.etal.Clinical practice guideline:Acute otitis externa.Otolaryngol Head Neck Surg 2006:134(4):S4-S23.
Rosenfeld FM.ShinJJ,SchwartzSR.et aL Clinical practice guideline:Otitis media with effusion (update).Otolaryngol Head Neck Surg 2016;154:S1-S41.
Sander R.Otitis Externa:A practical Guide to Treatment andPrevention.Am Fam Physician2001:63(5):927-937.
Schaefer P.Baugh RF. Acute Otitis Externa:An Update. Am Fam Physician 2012;86(11):1055-1061.
Schularick.HM.Mowry SE. Soken H.et al.Is eleclroneumgraphy beneficial in the management of Bell's palsy? laryngoscope 2013:123:1066-1067.
Schwartz SR.Magil AE. Rosenfeld RM.clat. Clinical Practice Guideline (Update):Earwax (Cerumen Impaction). Otolaryngol Head Neck Surg 2017:156:51-529.
Scholes MA.Ramakiishnan VR (editors).EN1 secrets. 4th ed. Philadelphia:Elsevier. 2016.
Smalt P.KeithPK.Kim H. Allergic rhinitis.Allergy Asthma Clin Immunol 2018:14:51.
Smith SS.Terence EH.Evans CT.etal.Ihe prevalence of bacterial infection in acute rhlnosinusitis:a systematic review and mela analysis.Laryngoscope 2015;125:57- 69.
SraffordIID.Wilde A. Parotid cancer.Surg Oncol1997:6:209-213.
Sur DKC.Ptesa ML.Chronic nonallergic rhinitis.Am Fam Physician 2018:98(3):171-176.
TehraniAS,Kattah JC,Kerber KA.etal.Diagnosing stroke inacute dizziness and verbgo:pitfalls andpearls.Stroke 2018:49(3):788-795.
Tesster FN.Middleton WD. Grant EG.etal.ACR Thyroid Imaging.Reporting and Data System (TI-RADS):White Paper of Ihe ACR TI-RADS Committee.JACR 2017;14|5):587-95
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OT52 Otolaryngology Toronto Notes 2023
Valencucla CV.Newbill CP.Johnston C cl at. Proliferative laryngitis with airway obstruction Inan adult: consider herpes, laryngoscope 2016;126:945-948.
Vcnekamp HP.SandetsS,Glasclou PP.et at.Antibiotics lor acute otitis mediainchildren.Cochrane DB Syst Rev 2013:1:C0000219.
VenekampRP.Thompson MJ.Rovers MM.Systemic corticosteroid therapy lor acute sinusitis.JAMA 313:1258-1259.
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medullary thyroid carcinoma.Thyroid 2015;25:567-610.
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Wu V.Cooke B.Eilulis S.ctal.Approach to tinnitus management. Can Fam Physician 2018:64( 71 -191 -195.
Wurdermann N.Wagner S,Sharma SJ.elal.Prognostic impact of A JCC/UICC 8th edition new staging rulesIn oropharyngeal squamous cell carcinoma.Front Oncol 2017:7:129.
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Paediatrics
Onyinyechukwu Esenwa, Anna Jiang, Kahna Rasouli,Mary Xie, and Tingting Yan,chapter editors
Ming Li and Dorrin Zarrin Khat, associate editors
Vijithan Sugumar, EBM editor
Dr. Tanvi Agarwal, Dr.Jillian Baker, Dr. Tyler Groves, Dr. Joey Latino, Dr. Shazeen Suleman, and Dr.
Janaki Vallipuram,staff editors
Acronyms
Paediatric Quick Reference Values
Primary Care
Visit Overview
Routine Immunization
Growth and Development
Nutrition
Circumcision
Common Complaints
Breath Holding Spells
Crying/Fussing Child
Infantile Colic
Dentition and Caries
Enuresis
Encopresis
Toilet Training
Failure to Thrive
Obesity
Poison Prevention
Rashes
Sleep Disturbances
Sudden Infant Death Syndrome
Adolescent Medicine
Child Abuse and Neglect
Physical Abuse
Sexual Abuse
Neglect
Cardiology
Congenital Heart Disease
Acyanotic Congenital Heart Disease
Cyanotic Congenital Heart Disease
Congestive Heart Failure
Dysrhythmias
Heart Murmurs
Infective Endocarditis
Development
Global Developmental Delay
Intellectual Disability
Language Delay
Specific Learning Disorder
Fetal Alcohol Spectrum Disorder
Attention Deficit Hyperactivity Disorder
Autism Spectrum Disorder
Motor Delay
Endocrinology
Antidiuretic Hormone
Diabetes Mellitus
Growth
Hypercalcemia/Hypocalcemia/Rickets
Hyperthyroidism and Hypothyroidism
Disorders of Sexual Development
Fluids and Electrolytes
Approach to Infant/Child with Dehydration
Gastroenterology
Vomiting
Gastroesophageal Reflux
Tracheoesophageal Fistula
Pyloric Stenosis
Duodenal Atresia
Malrotation of the Intestine
Diarrhea
P3 Gastroenteritis
Toddler's Diarrhea
Lactase Deficiency (Lactose Intolerance)
Irritable Bowel Syndrome
Celiac Disease
Cow's Milk Allergy
Inflammatory Bowel Disease
Cystic Fibrosis
Constipation
Abdominal Pain
Chronic Abdominal Pain
Abdominal Mass
Upper Gastrointestinal 8leeding
Lower Gastrointestinal Bleeding
Genetics,Dysmorphisms,and Metabolism
Hematology
Approach to Anemia
Physiologic Anemia
Iron Deficiency Anemia
Vitamin K Deficiency
Anemia of Chronic Disease
Sickle Cell Disease
Thalassemia
Hereditary Spherocytosis
Glucose-6-Phosphate Dehydrogenase Deficiency
Bleeding Disorders
Immune Thrombocytopenic Purpura
Hemophilia
von Willebrand's Disease
Oncology
Lymphadenopathy
Leukemia
Lymphoma
Brain Tumours
Wilms' Tumour (Nephroblastoma)
Neuroblastoma
Bone Tumours
Cancer Predisposition Syndromes
Infectious Diseases
Fever
Acute Otitis Media
Otitis Media with Effusion
Gastroenteritis
HIV Infection
Infectious Paediatric Exanthems
Infectious Mononucleosis
Infectious Pharyngitis/Tonsillitis
Meningitis
Mumps
Pertussis
Pneumonia
Periorbital (Preseptal) and Orbital Cellulitis
Sexually Transmitted Infections
Sinusitis
Urinary Tract Infection
Neonatology.
Gestational Age and Size
Routine Neonatal Care
Neonatal Resuscitation
Common Conditions of Neonates
Apnea
Bleeding Disorders in Neonates
Bronchopulmonary Dysplasia
Cyanosis
P3
P4
P10
P50
P50
P17
P18
P20 P54
P26
P58
P30
P38
P70 P40 r->
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Paediatrics
Diaphragmatic Hernia
Hypoglycemia
Neonatal Hyperbilirubinemia
Necrotizing Enterocolitis
Persistent Pulmonary Hypertension of the Newborn
Respiratory Distress in the Newborn
Retinopathy of Prematurity
Sepsis in the Neonate
Skin Conditions of the Neonate
Nephrology
Common Paediatric Renal Diseases
Hemolytic Uremic Syndrome
Nephritic Syndrome
Nephrotic Syndrome
Hypertension in Childhood
Neurology
Cerebral Palsy
Febrile Seizures
Hypotonia
Neurocutaneous Syndromes
Recurrent Headache
Seizure Disorders
Respirology
Asthma
Bronchiolitis
Cystic Fibrosis
Pneumonia
Respiratory Distress
Rheumatology
Growing Pains
Juvenile Idiopathic Arthritis
Limb Pain
Lyme Arthritis
Reactive Arthritis
Septic Arthritis and Osteomyelitis
Systemic Lupus Erythematosus
Transient Synovitis of the Hip
Vasculitides
Common Medications
Landmark Paediatric Trials
References
P82
P87
P91
P95
P99
P100
P100
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Acronyms
AAP American Academy o( Pediatrics 01
ABG arterial blood gas
ACE angiotensin converting enzyme
ACEI angiotensin converting enzyme OKA
inhibitor
ADH antidiuretic hormone
AGA appropriate for gestational age OS
ALL acute lymphoblastic leukemia OSD
ALPS autoimmune lymphoprolilerativc EBV
syndrome
AML acute myelogenousleukemia
ANA antinuclear antibody
AOM acute otitis media
ARB angiotensin receptor blocker
ARBO alcohol-related birth defects FIT
ARNO alcohol-related
ncurodevclopmcntal disorder
ASD atrial septal delect
ASOT antistreptolysin-o titre
AIN acute tubular necrosis
AVM arteriovenous malformation GN
BRUE
CAH congenital adrenal hyperplasia
CAS Children's Aid Society
COGP constitutional delay of growth
and puberty
CF cystic fibrosis
CFIR cystic fibrosis transmembrane
conductance regulator
CHO congenital heart defect
CML chronic myelogenous leukemia
CMV cytomegalovirus
CP cerebral palsy
CPAP continuous positive airway
pressure
CPS Canadian Paediatric Society
DAT direct antiglobulin test
DDAVP 1-desamino-8-Darginine
vasopressin
diabetes insipidus
QIC disseminated intravascular
coagulation
diabetic ketoacidosis
DMARD disease modifying antirheumatic
drug
Down syndrome
disorder of sexual differentiation IVIg
Epstcin-Barr virus
Echo echocardiogram
FAS fetal alcohol syndrome
FASD fetal alcohol spectrum disorder LGA
FISH fluorescent insitu hybridization LLSB
FSS familial short stature
inflammatory bowel disease
ideal body weight
intracranial hemorrhage
immune thrombocytopenic
I6D
IBW PPHN persistent pulmonary
hypertension of newborn
PPV positive pressure ventilation
PUVA psoralen *
UVA
RAD right axis deviation
RAS renal artery stenosis
RBB8 right bundle branch block
RDS respiratory distress syndrome
RF rheumatoid factor
Rhesus factor
RL Ringer’s lactate
RSV respiratory syncytial virus
RUS8 right upper sternal border
RVH right ventricular hypertrophy
RVOTO right ventricular outflow tract
obstruction
ICH
IIP
purpura
intrauterine growth restriction
intraventricular hemorrhage
intravenous immunoglobulin
juvenile idiopathic arthritis
left atrial hypertrophy
low birth weight
large for gestational age
lower left sternal border
lower motor neuron
level of consciousness
IUGR
IVH
JIA
LAH
LBW Rh
LMN
failure to thrive LOC
gestational age
GAS group A Streptococcus
G8M glomerular basement membrane LV
GBS group B Streptococcus
GERD gastroesophageal reflux disease MAS
glomerulonephritis
brief resolved unexplained events GSO glycogen storage disease
GTPAL Gravidity Term Preterm Abortion MOD
Living
HBsAg hepatitis B surface antigen
HDN8 hemorrhagic disease of the
newborn
GA LP lumbar puncture
lower respiratory tract infection
left ventricle
left ventricular hypertrophy
LRII
SEM systolic ejection murmur
SGA small for gestational age
meconium aspiration syndrome SIAOH syndrome of inappropriate
MCAD medium-chain acyl-CoA
dehydrogenase
minimal change disease
metered dose inhaler
MEE middle ear effusion
MSUO maple syrup urine disease
NCS nerve conduction study
necrotizing enterocolitis
neurofibromatosis
NICU neonatal intensive care unit
normal saline
LVH
antidiuretic hormone
SIDS sudden infant death syndrome
STEC Shiga toxin-producing E. coli
SVT supraventricular tachycardia
TEF tracheoesophageal fistula
tympanic membrane
total parenteral nutrition
transient tachypnea of the
newborn
UMN upper motor neuron
URTI upper respiratory tract infection
UVA ultraviolet A
VCUG voiding cystourethrogram
VKDB vitamin K deficiency bleeding
VSD ventricular septal defect
VUR vesicoureteralreflux
WPW Wolff-Parkinson-White
r.
’
Li
1M
TPN
HEEADSSSHome Education/Employment NEC
Eating Activities Drugs Sexuality NF
Suicide/depression Safety/
violence
Haemophilus influenzae type b OOP
HIDA hepatobiliary iminodiacetic acid OME
HIE hypoxic ischemic encephalopathy ORT
HPA human platelet antigen
HRV human rotavirus
HSP Henoch-Schonlein purpura
HSV herpes simplex virus
HUS hemolytic uremic syndrome
TIN
NS
oral contraceptive pill
otitis media with effusion
oral rehydration therapy
obstructive sleep apnea
premature atrial contraction
polycystic ovarian syndrome
patent ductus arteriosus
phenylketonuria
Hib
OSA
PAC
PCOS
PDA
PKU
Paediatric Quick Reference Values
Table 1. Normal HR and RR at Various Ages
Age (yr) Pulse (bpm) Respiratory Rate (br/min)
Canadian Immunization Guide
National Advisory Committee on
Immunization. Canadian Immunization
Guide (CIG). Last Modified 2021.Public
Health Agency of Canada, 2006.
Available at https://www.canada.ca/
en/public-health/services/canadianimmunization-guide.html
Neonale (- 28 d)
Infant (1-12 mo)
Toddler (1-2 yr)
Preschool (3-5 yr)
School-age (6-11yr)
Adolescent (12-15 yr)
100-205
100-190
98-140
80-120
30-53
22-37
20-28
75-118 18-25
60100 12-20
Table 2. Normal sBP at Various Ages
Age sBP (mmHg)
Birth<1kg (12h)
Birth 3 kg (12h)
Neonate (96 h)
Infant (1-12 mo)
Toddler (1-2 yr)
Preschool (3-5 yr)
School-age (6-9 yr)
Preadolescent (10-11yr)
Adolescent (12-15 yr)
39-59
60-76
67-84
72-104
86-106
89-112
97-115
102-120
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Table 3. Normal Temperature Ranges
Method Normal Temperature Range Fever
36.6°Cto 38°C
35.8”C to 38"C
35.5”C 10 37.5’C
36.5"C to 37.5"C
Rectal >38“C +
Ear >38“C
>37.5“C
>37.5VC
Oral
Axillary
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P I Paediatrics Toronto Notes 2023
Table 4. Temperature Measurement Technique Recommendations
Age Suggested Technique
Birth to 2 yr 1.Rectal (definitive)
2. Axillary (screening low risk children)
Over 2yr to 1.Rectal (delinltive)
2.Axillary.Tympanic (or Temporal Artery if inhospital) (screening)
Older than 1.Oral (definitive)
2.Axillary,Tympanic (or Temporal Artery if in hospital) (screening)
5 yr
5yr
Primary Care
Visit Overview
•schedule of well-child visits
• newborn (within <18-72 h post-discharge), 2, <1, 6, 9, 12, and 18 mo
annually between ages 2-5; every 1-2 yr between ages 6-18
•content
history and physical exam including growth, development, and nutrition
routine immunizations
counselling and anticipatory guidance
see evidence based clinical tools such as Rourke Baby Record and Greig Health Record for more
information
According to the Centers for Disease
Control and Prevention (CDC).the weight
of currently available scientific evidence
does not support the hypothesis that
the Measles, Mumps and Rubella (MMR)
vaccine causes either autism or IBD. The
landmark paper linking autism to the
MMR vaccine (Lancet1998:351:637-641)
was retracted due to false claims in the Standard Paediatric History article (Lancet 2010:375:445)
• BINDS: Birth, Immunization, Nutritional, Developmental, Social
• ID: name, age, major chronic medical concerns
•chief complaint (GC)/reason for referral (RI-
'
R)
• HPI: child and caregiver
• OPQRSTU
• recent travel,sick contacts
•obstetrical history
• prenatal/pregnancy history
conception
GTPAL
screening:blood group, Rh, DAT, HBsAg, rubella,syphilis, HIV, GBS
genetic screening:maternal serum screening (MSS), first trimesterscreening (ITS),
integrated prenatal screening (IPS), amniocentesis,special tests
ultrasounds
complications: illnesses, infections, bleeding, gestational diabetes(GDM), gestational
hypertension (GHTN)
medications, vitamins, iron,smoking, drinking, drug use
• labour and delivery or birth history, and why
gestational age at birth, birth weight
labour complications: prolonged rupture of membranes, maternal fever, fetal tachycardia,
meconium
Adverse Reactions Associated with
Any Vaccine
• Local:induration,tenderness,
redness, swelling
• Systemic:fever,rash, irritability
• Allergic:urticaria,rhinitis,
anaphylaxis
Contraindication:
• Moderate/severe illness ± fever
• Allergy to vaccine component
• No need to delay vaccination for
mild URTI
Vaccination in Caseiol Asplenia or Hyposplenia
(such as SickleCell Disease)
• Should receive all routine lmiitaaiHUoat,ia(Mia|
the yearly inltuerna vaccine
• No vaccines are contraindicated, though
live vaccines can be contraindicated a
immunodeficienciessuch as DiGeorge syndrome
(22q11.2 deletion)
• Susceptible tu infection by encapsulated bactena
(*SHiNE KISS'
-S. poemotim.H.mftierae.I.
meomyifidrs,£ coll Klebsiella.SolmseHo.Croup
SSfreyx),so must add:
• Quadrivalent conjugated Meningococcal C
vaccine (Men-C -ACYW) and Meningococcal S
vaccine (4CMenB|at time of d agnosrsif >2
mo (2-4 doses given at least 8 vrk apart) vrith
booster every 5 yr thereafter
• Canonirtroutine Men - goccccal C Co - .gate
at 11 mo if received Men C -ACVWacd expected
to receive a second dose wittier 8 «k
• Pneumococcal polysaccharide vaccme
(Pneu P -23|at >2 yr and single booster >5yr
alter first dose
• Pneumococcal conjugate vaccine (Pneu-C-tt)1-2
doses8wk a pa rl if >12 mo at time of diagnosis
• Consider single booster Nib at >5yr
« spontaneous vaginal delivery, interventions required: forceps, vacuum, caesarean delivery
(CD)
medications used during labour
resuscitation: APGARs
length of hospital stay, N1CU stay
•past medical history
• hospitalizations, ED visits, past surgeries, chronic illnesses, accidents or injuries, community
resources/services involved or referrals in place, otherspecialistsinvolved in care
medications
•allergies
•immunizations (including contraindications,such as previous anaphylaxis, or immunosuppression)
•developmental history
• meeting major milestones
• behavioural concerns
• nutritional history
• breast vs. formula feeding
• milk intake
• solids, variety, etc.
•family history
consanguinity, recurrent pregnancy losses, early childhood deaths
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P5 Paediatrics Toronto Notes 2023
• social history
• who lives at home? Siblings?
does the child attend daycare or school? Primary care givers?
• school adjustment, friends, activities,safety,stability,stressors
• HEhADSSS history for adolescents
ITHELPS -income, transportation, home, education, legal status, personal safety,support
Routine Immunization
Table 5.Publicly Funded Immunization Schedule for Ontario
DTaP- TdaP- Pneu- Rot
-5
IPV-Hib IPV C-13
MMR Var MMRV Men-C- HepB HPV-9 Tdap Inf
ACYW
Men'
Injection site
Infants (<12 mo):anterolateral thigh
C-C
2 mo
4 mo
AO -MM ^IM
-MM -4|M m
AO
6 mo
12 mo
15 mo
18 mo
4-6 yr’
Grade 7
^
IM AO A Systematic Review of the Effect of Rotavirus
Vaccination onDiarrhea OotcomesAmong
Oiildren Younger Than 5 Years
Pediatr Infect Dis J 2016:35(9)592-998
Purpose: To review evidence of rotavirus vaccine
efficacy and effectiveness by tMenm.m Development
Goal Region.
Method: RCIs and observaf studies on rotavirus
vaccine In children < 5 yfo were included m this review.
Primary oulcomes included rotavirus diarrhea or
diarrhea olunspecified ehofogy.Secondary outcomes
included diarrhea episodes of any severity,and
seveie diarihea episodes,hospitalization,and death.
Results: 48 studies were eligible for orelusion
in this review.Rotavirus vaccine was found to he
effective and efficacious.Across all millennium
development regions rotavirus vaccine prevented
rotaviiusdiarihea.seveie rotavirus diarrhea, and
rotavirus hospitalization, the vaccine also reduced
seveie diarihea and diarrhea related hospitalization
in general.
v'lM ^IM -
/SC
AC
^IM
•AM AC
^IM VIM 3
doses
(0.1.6
VIM 2
doses
(0.6
mo) mo)
14-16 yr VIM
Every autumn
(beginning at
age 6 mo)
VIM
IM - intramuscutar:PO = per oral:SC = subcutaneous
•Preferably given at 4 yt of age
DTaP'IPV-Hib *
diphtheria,tetanus,acellular pertussis,inoctivated polio,Haemophilus inlluenxue type b vaccine(ie.Pcdiacc! ) TdaP-IPV
diphtheria,tetanus,acellular pertussis. Inactivated polio vaccine (l.c. Adacel Polio):HepB •hepatitis B vaccine:HPV-4 •human papillomavirus
vaccine:Ini•Intluenza vaccine:MMR - measles,mumps, tubellu vaccine:Mun-C-C •meningococcal c conjugate vaccine:Mon
-C-ACYW •
meningococcal vaccine;MMRV - measles,mumps,rubella,vailcella vaccine;Pneu- C -13 « pneumococcal13-valent conjugate vaccine;Rul
-5 •
rotavirus oral vaccine:Var
- varicella vaccine
Table 6. Adverse Reactions and Contraindications of Routine Immunizations
Vaccine Adverse Reaction Contraindication
Prolonged crying
Hypotonic unresponsive state (rare)
Seizure on day ol vaccine (race)
Cough
Diarrhea,vomiting
fever
Intussusception
Measles-like cash (7-14 d)
Lymphadenopathy,arthralgia,arthritis
Parotitis (care)
Especially painful injection
transient thrombocytopenia (1430000)
Mild varicella-like papules or vesicles:
2 wk may gel local or generalized rash
Evolving unstable neurologic disease
Hypoiesponsivelhypotonic following previous vaccine
Anaphylactic reaction to neomycin or streptomycin
History ol intussusception
Immunocompromised
Abdominal disorder (e.g. Meckel'
s diverticulum)
TdaP-IPV
RolS
MMR Pregnancy
Immunocompromised infants (except healthy HIV positive children)
Anaphylactic ceaction to gelatin
Pregnant or planning lo gelpregnant within 3 mo
Anaphylactic leadion to gelatin
Anaphylactic reaction to Baker's yeast
Same as MMR and Var vaccines
1st trimester pregnancy
<6 mo of age
Immunocompromised
Egg-allergic individuals - Live attenuated influenza vaccine is not
recommended lor those wilh an egg allergy.In these individuals.
Irivalenl or quadrivalent vaccine can be givenin an environment
where anaphylaxis can be managed
Var
HepB
MMRV Same as MMR and Var vaccines
DTaP
Ini Malaise,myalgia
febrile seizure when given withPneu-C-13 or DTaP
Hypersensitivity reaction
HPV-9
Men-B'
Prerilus
Anaphylactic reaction to Men-B vaccine or its components in the past
Anaphylactic reaction to Men-8 vaccine or its components in the past
ri
Men-C-ACYW Syncope (rare) L J
* Currently onlypublicly funded lor select groups(asplenia. antibodyVcomplement deficiencies, cochlear implant recipients.HIV,close contacts
with infected individuals)
DTaP 3diphtheria,tetanus,acellular pertussis vaccine: TdaP-IPV 3 diphtheria,tetanus,acellular pertussis,inactivated polio vaccine (i.e.Adacel -
Polio);HepB 3 hepatitis B vaccine:HPV-4 3
humanpapillomavirus vaccine;Ini 3
intluenza vaccine:MMR 3measles,mumps,rubella vaccine:
Mun-B 3 multicomponent meningococcalB vaccine: Men-C-C > meningococcal c conjugate vaccine:Men-C-ACYW 3 meningococcal vaccine.
MMRV - measles,mumps,lubella,vailcella vaccine:Rot
-5 3 iotavirus oral vaccine:Var •varicella vaccine +
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P6 Paediatrics Toronto Notes 2023
• adverse effects following immunization:must be reported to the local or regional health unit when
the event: has a temporal association with a vaccine, has no other clear cause at the time of reporting,
meets one or more of the seriousness criteria, is unexpected
• temperature regulation in vaccine storage: cold chain generally + 2 to +8
#
C
Modifications to the Routine Vaccination Schedule
• catch-up immunization schedules for children not previously immunized
• additional immunizationsfor children at-risk due to underlying medical conditions
• update Dec 2020: current Ontario catch-up program for HPV vaccine - 2-3 dosesfor Grades 8-11
(males) and Grades8-12 (females)
Immunization of Immunocompromised Patients
• susceptibility to infection and vaccine response varies
• individualized vaccine schedule based on patient’s immune status
• inactivated vaccines: may be administered if indicated; responses may be reduced or absent and
duration of immunity may be reduced (compared to healthy individuals);dose increase or extra
booster doses may be indicated
• live attenuated vaccines:
avoid ifseverely immunocompromised or if uncertain of immune status
can be given to those with isolated IgA,IgG subclass or complement deficiency,or asplenia
live viral vaccines are okay for most children with phagocyte or neutrophil disorders, but live
bacterial vaccines are contraindicated
• additional vaccines: may need vaccines that are not usually recommended for otherwise healthy
children or not usually administered beyond a certain age
• timing: vaccinesshould be administered when maximum immune response is expected (i.e. when not
immunosuppressed medically, pharmacologically, or immediately post transplant)
• response:asimmune response may be inadequate, consider post-immunization antibody titresif
appropriate; positive serologic test may be due to immunoglobulin therapy or maternal antibody
(infants <18 mo)
Vaccine-Hesitant Parents
• healthcare professional vaccine advice plays a key role in parental decision-making
do not dismiss vaccine-hesitant familiesfrom your practice
• use a presumptive approach (for giving the vaccine) and motivational interviewing
use open-ended questions and listen to parent concerns and opinions - do not assume the health
concerns of the parent
• address concerns non-judgmentally and non-confrontationally; validate why parents may hold
their belief
use compelling stories of vaccine-preventable disease
• communicate clearly to discuss disease risks and vaccine benefits and risks
• address immunization pain
• community protection (herd immunity)
• “wait and see" approach to vaccinate in an outbreak scenario is not advisable
promote altruism - not receiving immunization can have consequences for others
• parents who refuse to immunize their children need to be informed of associated risks of diseases and
responsibilities- considerations include:
protection of child from acquiring illnesses (e.g. vaccine, avoid sick contacts)
not vaccinating risksthe health of others(weakened immune system, chronic conditions,
newborns, elderly)
inform healthcare professionals of lack of vaccination when child issick
if a vaccine-preventable disease is in your community: get vaccine, may be required to stay away
front school, consider disease-specific risks, learn whatsymptoms to look out for
tetanus(>10% mortality) does not have community protection
travel - vaccinesspecific to geographical regions, refused permission to travel
Growth and Development
Growth'
• growth is not linear
most rapid growth during first 2 yr and at puberty
• measurement of growth
• WHO Growth Charts used to monitor growth in infants and children
premature infants(<37 wk) use lenton Curve to assess for small for gestational age (SGA) vs.
large for gestational age (LGA);corrected GA until 2 yr
body proportion = upper/lower segment ratio (use symphysis pubis as midpoint)
newborn = 1.7,adult male = 0.9, adult female = 1.0
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P7 Paediatrics Toronto Notes 2023
Average Growth Parameters
Table 7. Parameters of Average Growth at Birth
Normal Growth Comments
3.25 kg|7 lbs)* Gain 20-30 g/d [term neonate)
2 x birth wt by 4- S mo
3
*
birth wl by 1yr
4 x birth wt by 2 yr
25 cm in 1st yr
12 cm in 2nd yr
8 cm in 3rd yr. then 4-7 tm/yr until
puberty
8-12 cm/yt in adolescence
1/2 adult height at 2 yr
2 cm/mo for 1st 3 mo
1cm/mo at 3-6 mo
0.5 cm/mo at 6-12 mo
Weight loss (up to 10% of birth
weight)in first 7 d ol life is normal
Neonate should regain birlh
weight by -10-14 d
Measure supine length until 2 yr,
then measure standing height
Birth Weight
Length/Height 50 cm (20 in)*
Head Circumference 35 cm(14 in)* Measure around occipital,
parietal,and Irontal prominences
to obtain the greatest
circumference
* note these ate averages,and may differ based on ethnicity and gestationalage
Reflexes
Table 8. Developmental or Primitive Reflexes
Reflex Maneuver to Elicit Reflex Appropriate Reflex
Response
Age of Disappearance
Abnormal Reflex Response (primitive
reflex response present in infancy;
tendon reflex response always present)
• Primitive reflex responses are
abnormal if: absent during neonatal
period; asymmetric;or persistent
after 4-6 mo (e.g. cerebral palsy)
• Tendon reflex responses:asymmetry
suggests focal motor lesions (e.g.
brachial plexus injury) and absence
or hyper-reflexia may suggest CNS
abnormality
• Upgoing plantar reflex (Babinski's
sign) normal in infants up to 2 yr
Abduction and extension of the 3-6 mo
arms,opening of Ihe hands,
followed by flexion and adduction
olarms
Infant placed semi-upright, head
supported by examiner's hand,
sudden withdrawal olsupportcd
head with immediate returnol
support
Infant held in ventral suspension
and one side ol back is stroked
along paravertebral line
Placement of examiner's finger in
infant's palm
(urn infant's head to one side
More
Galant Pelvis will move in Ihe direction of 2-3mo
stimulated side
Grasp Flexion of infant's ftngers 3- 4 mo
'Fencing" posture (extension of 4-61110
ipsilateral arm and leg. flexion of
contralateral arm andleg)
Flexion followed by extension
of ipsilateral limb up onto table
(resembles primitive walking)
Infant turns head and opens 2-3mo
mouth to suck on same side that
cheek was stroked
Ipsilateral arm extension, present Does not disappear
by 6- 8 mo
ATNR
Stepping Dorsal surface of infant's fool 2-3mo
placed touching edge of table
Rooting Stroke infant’s cheek
lateral Propping lilt infant to side white in sitting
position
ATNR = asymmetric tonic neck reflex
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PH Paediatrics Toronto Notes 2023
Developmental Milestones
Table 9. Developmental Milestones Developmental Red Flags
• Gross motor:not walking at 18 mo;
rolling too early at <3 mo
• Fine motor:hand preference at
<18 mo
• Speech:<6 words at 18 mo
• Social:not smiling at 4 mo:not
pointing at15-18 mo
• See the Nipissing District
Developmental Screen for a checklist
of important 18 mo milestones:www.
ndds.ca
• Regression (i.o.loss of a previously
acquired skill)is a red flag at any age
Fine Motor Speech and
Language
Cognitive/
Problem Solving
Age" Gross Motor Social/Emotional
Primitive reflexes:
step,place.Moro.
Babinski,ATNR;Hexed
posture
Primitive reflex:grasp Primitive reflexes:
root,suck:orients to
Fixes and follows slow Bonding between
horizontal arc;prefers parent and child
Newborn
sound:variable cries contrast,colours,
faces,high-pitched
voices:visual focal
length
-10"
2 mo Raises head 45'
when Hands open hall the
time,balsa!objects
Rolls prone to supine. Palmar grasp,reaches Squeals,laughs
sits with support. and obtains items,
raises head up 90'
brings objects to
and lifts chest when midline
prone
Tripod sit,rolls
both ways,postural
reflexes
Turns lo voice,cooing Prefers familiar
caregiver
Social smile
prone
Purposeful sensory Explores parent's face
exploration olobjects
(eyes,hands,mouth),
anticipates routines
4 mo
6 mo Transfers objects
from hand tohand,
raking grasp
Babbles (nonspecific) Stranger anxiety.
looks for dropped
object
Expresses emotions:
happy,sad.mad:
memory for ~24hr
Sils well without
support,crawls (not pokes objects
all),pulls lo stand
Walks a few steps,
wide gait
9 mo Inferior pincer grasp, " Mama,dada" Plays games (e.g. Separation anxiety
Gestures "bye bye”, peek - a-boo)
“up”,gesture games Object permanence
1word with meaning Uses objects
firesides mama, functionally,cause
dada).responds to and effect,trial and memory
own name,follows error,imitates
1-step command with
gesture
4-5 words,follows Looks for moved Shared attention:
1-step command hidden object if saw it points at interesting
without gesture.1 being moved
body part
15-25 words
3 body parts
12 mo Fine pincer
(fingertips),fingerfeeds cheerios.
voluntary release
Points at wanted
items,narrative
Slacks 2 blocks,uses
spoon
15 mo Walks without
support,crawls up
stairsfsteps items to show to
parent
18 mo Runs.stoops and
recovers
Tower of 4 blocks,
scribbling, fisted
pencil grasp,removes
clothing
Tower of 6 blocks,
handedness
established,uses
utensil
Symbolic play with Parallel play
doll or bear
24 mo 2-3 word phrases. New problem-solving testing limits,
uses "I.me.you." strategies without
50% intelligible. rehearsal
understands 2-step
commands.50*
words
3-step commands. Identifies shapes.
3- 4 word phrases. counts to3.simple
"W”questions time concepts
(“why?").200 words.
75% intelligible
Hops on Hoot, climbs Uses scissors,buttons Speech 100%
down stairs1fool clothes
per step
Skips,rides bicycle Prints name,ties
shoelaces,tripod tense
pencil grasp
Jumps on two feet,
up and down slalrs
'marking time'
tantrums,negativism
(“no!"), possessive
(••mine!")
3 yr Rides tricycle,climbs Toilet trained,
up stairs alternating undresses,draws
circle andcrossf*
)
Cooperative play,role
play (pretend play),
separates easily,
sharing
feet
Identifies 4 colours,
intelligible,uses past counts to 4
tense,tells a story
Fluent speech,future Counts to 10
accurately,recites
ABCs
Has a preferred
friend,elaborate
fantasy play
Has groupol friends
4 yr
Syr
'llpremature,use corrected GA until 2 yr
Nutrition
See Landmark Paediatric Inals table for more
information on LEAP trial,which details the benefits
of early introduction of peanuts in decreasing
prevalence of peanut a lergies inchildren deemed
at risk.
Dietary Requirements
<10 kg 10 -20 kg
1000 cal
*
SO kcaifkg/d for each
kg >10
>20 kg
1500 cal *
20 keal/kg/d for each
kg -20
Weight
Heeds 100 keal/kg/d
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Dietary Recommendations
• 0-6 mo: breast milk or formula
exclusive breastfeeding during first 6 mo is recommended unless contraindicated; breastfeeding
can continue beyond 2 yr as long as mother and child want
breastfed infants require supplements: vitamin D (400 lU/d or 800 lU/d if infant or maternal risk
factors present)
• if not consuming iron-fortified cereals, meats, meat alternatives after 6 mo, at risk of iron
deficiency: give iron (after at least 4 mo and before 6 mo)
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Dietary Exposures audAllergy Preventionin
High-Risk Infants
Paedratr Child Health 2013:I8|10|:545-549
thereis no evdence thatrestriction of highly
a ergenic foods is benefibal in thehist yr of life.
Later introduction of peanut,fish,or egg does not
prevent, and may increase the risk of developing
food allergy.There is also no evidence that dietary
restrictions during pregnancy or breastfeeding are
protective to the child.
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• >6 mo:solid food introduction - do not delay beyond 9 mo
• 2-3 new foods per wk, wait at least 2 d in between each food to allow time for adverse reaction
identification
common allergens:eggs, milk, mustard, peanuts,seafood,sesame,soy, tree nut, wheat
• early introduction of highly allergenic foods is recommended
offer lumpy,soft-cooked, pureed, mashed textured foods
• encourage self-feeding and introduce open cup (should be done by 18 mo)
• 9-24 mo:switch to homogenized (3.25%) cow’s milk, offer 16 oz/d if non-breastfeeding
• offer vegetables, fruit, grains, and full-fat milk in any order after iron-rich foods are given
provide up to 3 large feedings (meals) with 1-2 smaller feedings (snacks),depending on child's
hunger/satiety cues
• foods to avoid
honey until past 12 mo (risk of botulism)
added sugar,salt
excessive milk (i.e. maximum 500 mL or 16 oz/d after 1 yr) - associated with iron deficiency
anemia
limit juice intake (not nutritious, too much sugar), maximum 4-6 oz (1/2 cup) daily
anything that is a choking hazard (chunks, round foods like grapes)
• 2-6 yr:switch to 2% milk (500 mL/d)
• can maintain breastfeeding during this time complementary to solids
Breastfeeding
• content of breast milk
colostrum (first few days postpartum): clear, rich in nutrients(i.e. high protein, low fat),
immunoglobulin
mature milk:70:30 whey:casein ratio,fat from dietary butterfat, carbohydrate from lactose
• advantages
easily digested, low renal solute load
• immunologic
reduction of acute illnesses(i.e. diarrhea, respiratory tract illnesses, acute otitis media) and
may have longer term benefits
contains IgA, macrophages, active lymphocytes, lysozymes, lactoferrin (which inhibits E. coli
growth in intestine)
lower pH promotes growth of Lactobacillus in (il tract
• parent-child bonding
economical, convenient
• maternal contraindications
absolute contraindications: HIV, HT'LV type 1 and II, infant galactosemia
relative contraindications: chemotherapy, radioactive compounds, or certain medications known
to cross to breast milk with neonatal effects
active untreated TB (2 wk), active HSV-2 lesions on breast (can still feed expressed breast milk
from unaffected breast)
OCPs are not a contraindication to breastfeeding (estrogen may decrease lactation, but is not
dangerous to infant)
• if poor weight gain: consider dehydration or 1 1 1 and may consider formula supplementation if
insufficient milk production or intake
• oral candidiasis(thrush): treat baby with antifungal such as nystatin and ensure all nipples, bottles,
pacifiers are sanitized to avoid re-infection;can occur in breast or bottle-fed infants
Medications that Cross into Breast Milk
Antimetabolites
Chloramphenicol
Diazepam
Ergots
Gold
Metronidazole
Tetracycline
Lithium
Cyclophosphamide
Signs of Inadequate Intake
• <6 wet diapers/d after first wk
• <7 feedsfd
• Sleepy or lethargic,sleeping
throughout the night <6 wk
• Weight loss >10% of birth weight
(past10-14 d of life)
• Jaundice
Signs of Adequate Intake
• 1wet diaper/d of age for first wk
. 1-2 black or dark green stools
(meconium)/don Day1and 2
• 3
- brown/grectVyellow stools/d on
Day 3 and 4
. 3+ yellow,seedy stools/d onDay 5+
Table 10. Common Formulas Compared to Breast Milk
Type of Nutrition Indications Content (as compared to breast milk)
Prematurity
Transition to breastfeeding
Contraindication to breastfeeding
tow birth weight
Prematurity
Lower whey:casein ratio
Plant fatsinstead of dietary butterfat
Cow’s Milk-Based
(Enfamil
*
Similar )
Fortified Formula Higher calotiesand vitamins A. C. D. K
May only be used in hospital due to risk ol
fat-soluble vitamin toxicity
Galactosemia Corn syrup solids orsucrose in place of lactose
Desire for vegetarianfvegan diet*
Delayed gastric emptying
Risk of cow's milk protein allergy
Malabsorption
Food allergy including cow's milk protein
allergy
SoyProtein
(Isomil •
; Prosobee •
)
Partially Hydrolyzed Proteins
(Good Starr )
Protein Hydrolysate
(llutramigen '
, Alimentum '
,
Pregestimil »,Portagen '
)
Protein is100% whey with no casein
Protein is100% casein with no whey
Corn syrup solids,sucrose,or tapioca starch
instead of lactose
Expensive
Free amino acids (no protein)
Corn syrup solids Instead of lactose
Very expensive
Various different compositions for children
with galactosemia, propionic acidemia,etc.
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Food allergy
Short gut
Amino Acid
(lleocate . PurAmino ')
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Metabolic Inborn errors of metabolism
’10- 35% of children with cow's milk protein allerg/ also have reactions to soy-based formula
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P10 Paediatrics Toronto Notes 2023
Injury Prevention Counselling
• injuries are the leading cause of death in children >1 yr
• main causes:motor vehicle crashes,burns, drowning, falls, choking, infanticide
Table 11. Injury Prevention Counselling
0-6 mo 6-12 mo 1-2 yr 25 yr
Do not leave atone on bed.on Installstair barriers
changing table,or in tub
Keep crib rails up
Check water temperature before
Hever leave unattended
Discourage use of walkers Keep pot handlesturned to back
Avoid play areaswith sharp- edged of stove
tables and corners
Bicycle helmet
Never leave unsupervised at
home, driveway,or pool
Caution with whole grapes, nuts, teach bike safety,strangersafely,
raw carrots, holdogs, etc. due to and street safety
Swimming lessons(>4 yr),
sunscreen (from 6 mo),fences
around pools
Appropriate carseats
Ensure large devices (such as TVs)
secured to walls
bathing Cover electrical outlets
Do not hold hot liquid and infant at Unplug appliances when not in use choking hatard
No running whileeating
Appropriate carseats
the same time Keep small objects, plastic
bags, cleaning products, and
medications out of reach
Check milk temperature before
feeding
Appropriate carseats are required Supervise during feeding
before leaving hospital Appropriate car scats
Avoid co-slecping with Infant
Note:Thislist is not exhaustive. For more details,see Rourke Baby Record (http://www.rourkebabyrecord.ca/downloads)
Circumcision
• elective procedure
CPS affirms that circumcision is not medically indicated, and does not recommend routine
circumcision for every newborn male
often done for religious or cultural reasons
• benefits: prevention of phimosis and slightly reduced incidence of UTI,S'
l
'
l, balanitis, cancer of the
penis
• complications (<1%):local infection,bleeding, urethral injury,meatal stenosis
• complication rate increased in children compared with infants
• contraindications: presence of genital abnormalities (e.g. hypospadias) or known bleeding disorder
Paediatr Child Health 2015;20(6):311-320
The Canadian Paediatric Society and American
A udemy of Pediatrics have both petviousty indicated
that cltcumelslon of newborn males Is not a med itally
indicated procedure.Some evidence hassubsequently
suggested decreased urinary tract infectiousand
incidence ofsome sexually transmitted infections,
including HIV,with circumcision.While such a
benefit may be present in some boys and high -risk
populationswhere the procedure may be considered
n the context of reduction or treatment,theCanadian
Paediatric Society continues to not recommend Common Complaints routine circumcision for every newborn male.
Breath Holding Spells
• clinical features
cyanotic type (more common), usually associated with anger/frustration
pallid type, usually associated with pain/surprise
• epidemiology: 0.1-5% of healthy children 6 mo-4 yr, usually start during first yr of life
• etiology
cyanotic type:child is provoked (usually by anger or upsetting event) -> holds breath and
becomessilent > spontaneously resolves or loses consciousness
pallid type: child falls or is frightened > heart rate is reduced by vagal stimulation -> cerebral
hypoperfusion -> loses consciousness
• management
usually resolvesspontaneously and rarely progresses to seizure;median age of remission is 4 yr,
and almost all children stop by 8 yr
• help child control response to frustration and avoid drawing attention to spell
may be associated with iron deficiency anemia, improves with supplemental iron
if episodes prolonged/frequent, triggered by non-traumatic stimuli, or if there is a family history
ofsyncope orsudden death -» in-depth cardiac evaluation indicated - check for prolonged QT
syndrome
Crying/Fussing Child
• common etiologies:functional (e.g. hungry'
, irritable), colic, trauma, illness
• history
description of baseline feeding,sleeping, crying patterns
« infectioussymptoms:fever, tachypnea, rhinorrhea, ill contacts
feeding intolerance:gastroesophageal reflux with esophagitis, N/V, diarrhea, constipation
• physical injury (unintentional or non-accidental)
recent immunizations (vaccine reaction) or medications (drug reactions), including maternal
drugs taken during pregnancy (neonatal withdrawal syndrome) and drugs that may be
transferred via breast milk
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inconsistent history, pattern of numerous emergency department visits,difficult social living
conditions(e.g. parental substance use, precariousliving circumstances) can raise concerns for
maltreatment
consider broad array of possible underlying causessuch as meningitis,sepsis, respiratory distress,
constipation, etc.
Infantile Colic
• clinical features: unexplained paroxysms of irritability and crying for >3 h/d, >3 d/wk for >3 wk in an
otherwise healthy, well-fed baby (rule of 3s- Wessel criteria)
• epidemiology:10% of infants; usual onset 10 d to 3mo of age with peak at 6-8 wk
• etiology: unknown,
'
theories: alterations in fecal microflora, cow'
s milk intolerance, Gl immaturity or
inflammation, poor feeding, maternalsmoking
• diagnosis: diagnosis of exclusion after thorough history and physical exam to rule out identifiable
causessuch as otitis media, cow’
s milk intolerance,Gl problem,fracture
• management
parental relief, rest, and reassurance
change breastfeeding or bottle-feeding technique
hold baby,soother, car ride,music, vacuum, check diaper
limited evidence for probiotics;further research required
» breast-fed infants: time-limited trial (typically 1-2 wk) ofa hypoallergenic maternal diet (i.e. no
cow’s milk, eggs, nuts, wheat) while monitoring baby’s behaviour
formula-fed infants:time-limited trial (typically 1-2 wk) of hydrolyzed formula
prognosis:all resolve, most in the first 3-6 mo of life, no long-term adverse effects
Dentition and Caries
Dentition
• primary dentition (20 teeth)
first tooth at 5-9 mo (lower incisor), then 1/mo
6-8 central teeth by 1 yr
assessment by dentist 6 mo after eruption of first tooth and certainly by 1 yr of age (Grade B
recommendation)
• secondary dentition (32 teeth)
first adult tooth is 1st molar at 6 yr,then lower incisors
Caries
• early childhood caries: presence of one or more decayed, missing (due to caries), or filled tooth
surfaces in any primary tooth in a preschool-aged child
• etiology:multifactoriai with biomedical factors (e.g. diet, bacteria, host) and social determinants of
health
inappropriate feeding practices (e.g. frequent, prolonged bottle feeding, putting to bed with
bottle, prolonged breastfeeding, and excessive juice consumption) are important factors
• prevention
no bottle at bedtime, clean teeth after last feed
minimize juice and sweetened pacifier
dean gums with damp washcloth or soft-bristle toothbrush (no toothpaste) when no teeth present
<3 yr:daily brushing with fluoridated toothpaste (size of a grain of rice) assoon as teeth are
present
3-6 yr: assisted to brush teeth using pea sized amount of fluoridated toothpaste
ensure every child visits dentist by I yr
1 yr and beyond:involve dental public health programs (e.g. Healthy Smiles) to support access for
children in low-income households
Enuresis
Definition
• involuntary urinary incontinence by day and/or night in child >5 yr
General Approach
• should be evaluated if:dysuria; change in colour, odour, or stream;secondary or diurnal;change in
gait;orstool incontinence are present
Primary Nocturnal Enuresis
• clinical features: enuresis when bladder control has never been attained
• epidemiology:10% of children age 6,3% of children age 12,1% of children age 18,family history
important
• etiology: developmental disorder or maturational lag in bladder control while asleep
Treatment for primary nocturnal enuresis
should not be considered until 7 yr due
to high rate of spontaneous cure
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•management
• time, reassurance (~20% resolve spontaneously each yr), and avoidance of punishment or
humiliation to maintain self-esteem
behaviour modification (limiting fluids and avoid caffeine-containing food before bedtime, void
prior to sleep, ensure access to toilet, take out of diapers)
conditioning: “wet"
alarm wakes child upon voiding (70% success rate)
• medications (for children >7 yr, considered second line,short
-term therapy, may be used for
sleepovers/camp):desmopressin (DDAVP) oral tablets (similar success rate as “wet"
alarm
therapy but higher relapse rate),imipramine (Tofranil") (rarely used;lethal if overdose;side
effects: cardiac toxicity, anticholinergic effects)
Management andtreatment of Nocturnal
Enuresis - An UpdatedStandardization Document
f rom theInternationalChildren'
s Continence
Society
J Pcdiati Urol 2020.10 19
Additional Investigationsere not warranted In
aneisuretic child crithoutcertain waningsigns.
Key comorbidities to considerinclude psychiatric
disorders, constipation, urinary tract infections, and
snoring nr sleep apneas, floating constipation and
daytime incontinence tan lead to symptom resolution.
Irealingconcomitant sleepdisorder may alsu lead
to symptom resolution and is indicated.If enuresn
is non-monosymptomatic. treatmentshould begin
with advice on eveningdrinklng and voiding habits.
In monosymptomatic enuresis,treatmentshould
begin with either desmopressin oi an enuresisalaim.
Second line treatment includes anticholinergic
medications.Antidepressants may be considered
in rehactoiy enuresis though eipert opinion should
besought.
Secondary Enuresis
•clinical features:enuresis develops after child hassustained period of bladder control (>6 mo)
•etiology: inorganic regression due to stress or anxiety (e.g. birth of sibling,significant loss,
family
discard,sexual abuse),secondary to organic disease (UTI, DM, Dl,sleep apnea, neurogenic bladder,
CP,seizures, pinworms)
•management; treat underlying cause,specialist referral as appropriate
Diurnal Enuresis
•clinical features:daytime wetting (60-80% also wet at night)
•etiology: micturition deferral (holding urine until last minute) due to psychosocial stressor (e.g.shy),
structural anomalies(e.g. ectopic ureteral site, neurogenic bladder). UT I. constipation,CNS disorders,
DM
•management:treat underlying cause, behavioural (scheduled toileting, double voiding,good bowel
program,sitting backwards on toilet, charting/incentive system,relaxation/biofeedback),good
constipation management, pharmacotherapy
Encopresis
•clinical features: fecal incontinence in a child >4 y r, at least once per mo for 3 mo
•prevalence: 1-1.5% ofschool-aged children (rare in adolescence); M:l-
'
=6:1 in school-aged children
•causes: chronic constipation (retentive encopresis), Hirschsprung disease, hypothyroidism,
hypercalcemia,spinal cord lesions,CP, hypotonia, anorectal malformations, bowel obstruction
Retentive Encopresis
•definition:child holds bowel movement, develops constipation,leading to fecal impaction and
seepage of soft or liquid stool (overflow incontinence)
•etiology
physical:painfulstooling often secondary to constipation
emotional:disturbed parent-child relationship, coercive toilet training,socialstressors
•clinical features
history
crosseslegs orstands on toesto resist urge to defecate
distressed by symptoms,soiling of clothes
toilet training coercive or lacking in motivation
may show oppositional behaviour
abdominal pain
physical exam
digital rectal exam or abdominal x-ray:large fecal mass in rectal vault
anal fissures (result from passage of hard stools)
palpable stool in LLQ abdomen (50% of children with fecal incontinence)
staining of underwear with stool
•management
complete clean-out of bowel:PEG 3350 given orally is most effective and first line; enemas and
suppositories may be second line therapies, but these are invasive, often less effective, and not
recommended as first line
maintenance of regular bowel movements (see Constipation, P46)
assessment and guidance regarding psychosocial stressors
behavioural modification
•complications: recurrence, toxic ntegacolon (requires >3-12 mo to treat), bowel perforation
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P13Paediatrics Toronto Notes 2023
Toilet Training
• 90% of children attain bowel control before bladder control
• generally, females train earlier than males
• 25% by 2 yr (in North America), 98% by 3 yr have daytime bladder control
• signs of toilet readiness(usually 18-24 mo)
ambulating independently,stable on potty,desire to be independent or to please caregivers(i.e.
motivation),sufficient expressive and receptive language skills (2-step command level), can stay
dry for several hours(large enough bladder), can recognize need to go, able to remove clothing
• stepwise approach used to familiarize child with the potty chair and create a connection between
elimination and the potty chair;praise with use of potty chair
Failure to Thrive s • definition
• weight <3rd percentile, falls across two major percentile curves on growth chart,or <80% of
expected weight for height and age
inadequate caloric intake most common factor in poor weight gain
may have other nutritional deficiencies (e.g. protein, iron, vitamin D)
• factors affecting physical growth: genetics, intrauterine factors, nutrition, endocrine hormones,
chronic infections/diseases, psychosocial factors
• clinical features
• history
nutritional intake
currentsymptoms
past illnesses
family history:growth, puberty, parental height and weight (including mid-parental height)
psychosocial history
• physical exam
growth parameters, plotted
<2 yr:height, weight, head circumference
>2 yr:height, weight, BMI
vital signs
complete head to toe exam
dysmorphic features or evidence of chronic disease
upper to lower segment ratio
sexual maturity staging
signs of maltreatment or neglect
• investigations (asindicated by clinical features)
CBC, blood smear, electrolytes,Tt, TSH. urea, ferritin, Ca ,celiac screen, and vitamins A, D, H
bone age x-ray
chromosomes/karyotype
chronic illness: chest (CXR,sweat Cl -), cardiac (CXR, ECG, echo), Gl (celiac screen, inflammatory
markers, malabsorption), renal (urinalysis),liver (enzymes, albumin)
Mid-Parental Height
• Boys target height-(father height
mother height *13) /2
• Girls target height
-(father height*
mother height-13) /2
Note:heightshould be taken in cm
Clinical Signs of FTT
SMALL KID
Subcutaneousfat loss
Muscle atrophy
Alopecia
Lethargy
Lagging behind normal
Kwashiorkor
Infection (recurrent)
Dermatitis
Upper to Lower Segment Ratio
• Increased in achondroplasia,short
limb syndromes, hypothyroidism,
storage diseases
• Decreased In Marfan’s. Klinefelter’s,
Kallman’ssyndromes, and
testosterone deficiency
• Calculation:uppersegment/lower
segment
• Upper segment:top of head to pubic
symphysis
• Lower segment:pubic symphysis
to floor
Table 12. Failure to Thrive Patterns
Growth Parameters Suggestive Abnormality
Decreased Wt Normal Ht Normal HC Caloric insufficiency
Decreased intake
Structural dystrophies
Endocrine disorder
DecreasedWl Decreased HI Normal HC
DecreasedWt Decreased Ht DecreasedHC Intrauterine insult
BA - bene age:CA » chronological age: HC * head circumference:Ht * height:Wl *weight
Etiology
• an interplay between pathophysiology and psychosocial influences
• investigationsshould assess:
1.complex factors in the parent-child relationship
dietary intake, knowledge about feeding, improper mixing of formula
feeding environment
parent-child interaction, attachment
child behaviours, hunger/satiety cues
postpartum depression
social factors:stress, poverty, neglect, child/domestic abuse, parental substance misuse,
restricted diets
2.inadequate caloric intake:inadequate milk supply/latching, mechanical feeding difficulty (cleft
palate), oromotor dysfunction, toxin-induced anorexia
3.inadequate absorption: biliary atresia, celiac, 1BD,CP, inborn errors of metabolism, milk protein
allergy, pancreatic cholestatic conditions
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4.increased metabolism: chronic infection, CP,lung disease from prematurity, hyperthyroidism,
asthma,1BD,malignancy, renal failure
5.increased losses
6.increased utilization (e.g.chromosomal disorders)
7. prenatal factors:placental insufficiency, intrauterine infections,genetic,maternal
Management
•most as outpatient using multidisciplinary approach: primary care physician, occupational therapist,
dietitian, psychologist,social work, CAS
•medical:oromotor problems, iron deficiency anemia, gastroesophageal reflux
•nutritional:educate about age-appropriate foods, calorie boosting, mealtime schedules, and
environment;goal to reach 90-110% 1BW, correct nutritional deficiencies,and promote catch-up
growth/development
•behavioural:positive reinforcement, mealtime environment, no distractions(e.g.toys, books, or TV)
during mealtime
Energy Requirements
•see S
'
utrition, P8
Obesity Periaatal aid EartjCttdkood Factorsfor
Overweight aad Obesity iw Young Canadian
CCJ Public Heads 2013304(lteS9 H
Purpose: Id assess pcSutal eartj-lrfe factors and
their atenbtetiocsfcpjw ~ obesity among young
C a - ac:a t* :r
Methods Oatafromasa'jouDyreiitesentatne
sample of clddren ages6 Tt a the Canadian Health
MeasuresSurrey were anatyted.the associations
of permatal acd ea'y ctTdhood heterosis and
socioecooosic facarswitb oeecwtrgbt or obesity
were erabated sagsuA-enete logtsbc regression
models.
Jesuits:0*
'
55a term-bom ctidren.21% were
orerweigbt and another 13% were obese.Maternal
smoking faring pregsanq was posiStely associated
will obesity.Tbs assotiatba wasseriated by
bvth weight and onceoufroleithestrength of
the association between saoksg and ch ild obesity
increased by12%.Srtd weigti per 100 g (1.05;
1.005-1.09)wassjgn bcanyassociated with obesity.
Eidushe treastfeedwgfor Smo.adequate sleep
hon.and Seng ptyscaly actne were found to be
protect*
,fceasr'
eedtag.whether eidusnreor not,
sigmSundjredsced obesity risk among children
w:set:re s -tie- - . e; .•
Coodasm:ffesstndy rdeafied mgitp'
e perinatal
and chidhood factors associated wits obesity in
yoong Canadian children,ESectnre preientun
slraagestargeting fotr oodAaKe onatemal and
chid risk factors may rednee cbidhood obesity by op
to 54% la Canada.
• definition
Age Overweight Obese
0-2 yr eight for length >97th percentile
BMI >97Ui percentile
BUI >1511!percentile
Weight lor length >995th percentile
BMI >99.9th percentile
BMI >97th percentile
2-5yr
5-19 yr
• risk factors:genetic predisposition (e.g. both parents obese-80% chanceof obese child), psychosocial/
environmental contributors
• etiology
increased intake (dietary,social/behavioural, and iatrogenic such as drugs and hormones)
• decreased energy expenditure
• organic causes are rare (<5%):neuroendocrine (e.g. hypothyroidism,Cushing,PCOS), genetic
(e.g.Prader-Willi,Carpenter,Turner Syndromes)
plications:association with HTN, dyslipidemia,slipped capital femoral epiphysis, T2DM,
asthma,OSA,gynecomastia, polycystic ovarian disease, early menarche, irregular menses,
psychological trauma (e.g.bullying, decreased self-esteem, unhealthy coping mechanisms,
depression)
• childhood obesity often persistsinto adulthood
• investigations:BP, pulse,screen for:dyslipidemia,fatty liver disease (ALT),T2DM (based on risk
factors)
• com
• management
encouragement and reassurance; engagement of entire familv
• diet:qualitative changes (do not encourage weight loss, but allow for linear growth to catch up
with weight),special diets used by adults and very low calorie diets are not encouraged
• behaviour modification:increase activity, change eating habits/meal patterns,limit juice/sugary
drinks,ensure adequate sleep
• education:multidisciplinary approach, dietitian, counselling
• surgery and pharmacotherapy are rarely used in children
increase physical activity (1 h/d), reduce screen time (<2 h/d)
small changes in energy expenditure and intake (lose 1 lb/mo)
• long term goal:maintain BMI <85th percentile
Screen Time Guidelines (Canadian
Society foe Exerdse Physiology)
• Screen time is not recommended for
children under 2 yr
. <1 h/d screen time is appropriate for
children 2-5 yr
. <2 h/d screen time is appropriate for
children 5-17 yr
Poison Prevention
• keep all types of medicines, vitamins, and chemicals locked up in a secure container,out ofsight, and
out of reach
• potentially dangerous:medications, illicit drugs, drain cleaners,furniture polish, insecticides,
cosmetics, nail polish remover, automotive products
• do not store any chemicals in juice,soft drink, or water bottles
• keep alcoholic beverages out of reach:3oz hard liquor can kill a 2 y/o
• always read labels before administering medicine to ensure correct medication drug and dose and/or
speak with a pharmacist or healthcare provider
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Rashes
Table 13. Common Paediatric Rashes
Type of Rash Differential Appearance Management
Diaper Dermatitis Shiny, red macules/palches, no
skin fold involvement
Irritant contad deimatitis f llininale direct skin contact with urine
and feces, allow peiiods ol rest without
a diaper. Irequentdiaper changes,
topical barriers Ipelrolalum. zinc oxide
or pastel,short-term low potency topical
corlicostcroids(severe cases)
Short- term, mostuiiscrs. topical
antifungal (kctoconaiolc), low potency
topical corticosteroids
Seborrheic dermatitis Yellow,greasy macules/plaques
on erythema,scales
Candidal dermatitis frylhematous macerated papules! Antrlungal agents le g. dotrimarole.
plaques,satellite lesions,
involvement of skin folds
nystatin)
Other Dermatitis Atopx dermatitis Erythematous, papules/
plaques, oonng. excoriation,
lichenification. classic areas ol
involvement
Annular erythematous plaques,
oozing,crusting
Eliminatecxaccrbating factors,
maintain skin hydration (daily baths and
moisturisers), corticosteroids, topical
calcineurin inhibitor (2nd line)
Avoid irritant if identified, potent topical
steroid in emollient base,short-term
systemic steroids tantibiotics (severe)
Mild:soothing lotion (e.g.calamine lotion)
Moderate:low-to-intermediate potency
topical corticosteroids
Severe:systemic corticosteroids and
antihistamine
Avoid skin contact
Nummular dermatibs
Red papules/plaques/vesicles/
bullae,only in area ol allergen
Allergic contact dermatitis
Irritant contact dermatitis
Dyshidrotic dermatibs
Morphology depends on irritant
Papulovesicular, cracking/ Mild/moderate:medium/potent topical
Assuring, hands and feet (“tapioca corticosteroids
pudding") Severe:systemic corticosteroids,local
PUVA or UVA treatments
Infectious Scabies Polymorphic (red excoriated Permethrin (Nix5) 5% cream for patient
papules/nodules, burrows), in web and family (2 applications,1wk apart)
spaces/folds, very pruritic
Often affects multiple lamily
members
Honey-coloured crusts or
superficial bullae
Mild:topical anlibiolics (e.g.fucidic acid or
mupirocin cream)
Severe: oral antibiotics (e.g.cephalexin /
erythromycin )
Round erythematous plaques, topical antifungal for skin,systemic
central clearing and scaly border anlilungals for nalls/head
Impetigo
Tinea corporis
Paediatric Exanthcms (see fn/ec/rous Pocdiotiic Iwnthems,
Acne (see Oermaloloqy.014)
Neonatal skin conditions|see Skin Conditiom ollhe Heonolc. P82)
Sleep Disturbances
Types of Sleep Disturbances
• BEARS screening tool
• insufficient sleep quantity
• difficulty falling asleep (e.g. limit setting sleep disorder)
preschool and older children
bedtime resistance
due to caregiver’sinability to set consistent bedtime rules and routines
often exacerbated by child’s oppositional behaviours
• poor sleep quality
frequent arousals (e.g.sleep-onset association disorder)
infants and toddlers
child learns to fall asleep only under certain conditions or associations (e.g.with parent, held,
rocked or fed, with light on, in front of television), and loses ability to self-soothe
Daily Sleep Requirement
6 co 16 h
6 mo H.5 h
12 13.5 h
2p 13 h
< P 11.5 h
6 y> 9.5 h
12 yr 8.5 h
BP 8h
Nap n
Patterns
2'dat1yi
Vd at 2 yr(2-3 h long)
0.5 d at 5yr (1.7 h longl
. OSA
• definition:partial or intermittent complete airway obstruction during sleep causing disrupted
ventilation and sleep pattern
diagnostic criteria:clinical suspicion ( based on features like snoring, daytime sleepiness, and
witnessed apneas, and /or risk factors like neuromuscular disorders and Down syndrome); a
polysomnography is the gold standard for definite diagnosis
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epidemiology: 1-5% of preschool aged children, more common in Black children
• clinical features:snoring/gasping/noisy breathing during sleep and irritable/tired/hyperactive
during the day
complications:cardiovascular (HTN/LV remodelling due to sympathetic activation), growth,
cognitive, and behavioural problems
etiology: adenotonsillar hypertrophy, craniofacial abnormalities, obesity
investigations: polysomnography can be done, but is not required (expensive, inaccessible);
treatment can be initiated based on clinical judgement
• management: adcnotonsillectomy and weight management are first-line tx, follow-up for residual
OSA. Watchful waiting acceptable in mild-moderate cases
adcnotonsillectomy does not improve executive function/attention, but improves behaviour,
QOL, polysomnographic findings
use (.
'
PAP if adcnotonsillectomy is contraindicated (deft palate/bleeding disorder/acute
tonsillitis), OSA with minimal adenotonsillar tissue, residual OSA
avoid pollutants/tobacco smoke, allergens
avoid use of corticosteroids and antibiotics
•parasomnias
episodic nocturnal behaviours (c.g.sleepwalking,sleep terrors, nightmares)
often involves cognitive disorientation and autonomic/skeletal muscle disturbance
Management of Sleep Disturbances
•setstrict bedtimes and “wind-down" routines
•do not send child to bed hungry
•positive reinforcement for: limit setting sleep disorder
•alwayssleep in own bed, in a dark, quiet, and comfortable room
•avoid screens before bedtime and avoid caffeine-containing food
•do not use bedroom for timeouts
•systematic ignoring and gradual extinction for:sleep-onset association disorder
Nightmares
•epidemiology: common in boys, 4-7 yr
•associated with RKM sleep (generally last one third ofsleep)
•clinical features:upon awakening, child is alert and clearly recallsfrightening dream ± associated
with daytime stress/anxiety
•management:reassurance
Night Terrors
•epidemiology: 15% of children have occasional episodes
•usually in first one third of night;arousal from deep (slow wave) sleep
•clinical features:abruptsitting up, eyes open,screaming/vocalization, occurs in early hours of
sleep,stage 4 ofsleep;signs of autonomic arousal with no memory of event, disoriented if awakened,
inconsolable,stress/anxiety can aggravate them
•management: reassurance from parents,ensure child issafe (e.g. ifsleepwalks), parents can try to
identify pattern and wake up child 15 min before to disrupt pattern, often remitsspontaneously before
puberty
Brief Resolved Unexplained Events
(BRUE)
These arc sudden, brief (<1min) and
now resolved episodesin an infant
with one or more of the following:
cyanosis or pallor; absent, decreased or
irregular breathing:change in tone; and/
or altered level of consciousness. The
observer fears the child may be dying.
The child should be asymptomatic on
presentation and there is no c xplanation
after a history and physical for the
cause.There is no clear connection
between most BRUEs and SIDS.
Evaluating for a cause of the BRUE (e g.
infection, cardiac, neurologic, child
Diels abuse. metabolic disease, toxins, etc.)
KISK rciCIOrS quide<J by history, physical exam,
• prematurity (<37 wk), early bed sharing (<12 wk), alcohol use during pregnancy,soft bedding, low amJ o( observation. Etiology:
birthweight. Indigenous background, male, no prenatal care,smoking in household, prone sleep inherently unknown, but affected
position, poverty Wants ®PPe»to have (1) underlying
• risk of SIDS is increased 5-6x in siblings of infants who have died of SIDS genetic or anatomic (e.g. brainstem
• bed sharing:sleeping on a sofa, adult sleeping with an infant after consumption of alcohol/street drugs ujOTerevent (e g maternal smoking
or extreme fatigue,sleeping on a surface with a fixed wall (couch/sofa), infantsleeping with someone airflow obstruction).A BRUE appearsto
other than primary caregiver happen when (1) and (2) occur during a
vulnerable stage of development
Sudden Infant Death Syndrome
Definition
• sudden and unexpected death of an infant <12 mo in which the cause of death cannot be found by
history, examination, or a thorough postmortem and death scene investigation
Epidemiology
• 0.5 in 1000 (leading cause of death between 1 -12 mo); M:l
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*3:2
• more common in children placed in prone position
• in full term infants, peak incidence is 2-4 mo, 95% of cases occur by 6 mo
• increase in deaths during peak KSV season
• most deaths occur between midnight and 8 AM
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Prevention
• “Back to Sleep, Front to Play” (place infant on back when sleeping, daily supervised play/“tummy
time” in prone position)
• avoid sharing bed with infant
• avoid tobacco smoke exposure
• avoid overheating and overdressing
• appropriate infant bedding (firm mattress, avoid loose bedding, pillows,stuffed animals, and crib
bumper pads)
• exclusive breastfeeding in first mo and no smoking
• pacifiers appear to have a protective effect; do not reinsert if falls out during sleep
• infant monitors do not reduce incidence
Adolescent Medicine
Adolescent Psychosocial Assessment
Adolescent History (HEEADSSS)
• review confidentiality and its limits with adolescent prior to taking history
• tailor your history according to the clinical context
Home: W ho do you live with? What kind of place do you live in? Do you get along with your parents
and/or siblings? Is your home a safe place for you?
HEEADSSS
Home
Education/Employment
Eating
Activities
Drugs
Sexuality
Suicide and depression
Safcty/violcnce
Education/Kniploymcnt: What grade are you in? What are your favourite subjects? Tell me about your
grades. How often do you missscnool/dass? Do you work (ifso, how much)? Do you get along with
teachers/employers?
Eating:Tell me about your meals/snacks In a typical day. Have you ever gone on a diet? What are your
favourite and least favourite foods? (see Psychiatry. Hating Disorders, PS39)
Activities: What do you do after school? On the weekends? How much time do you spend on the
computer/watching TV every day? Do you use social media (i.e. I
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