Al-Howasi Manual of Clinical Pediatrics PDF

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This is a manual of clinical pediatrics for medical students and postgraduate doctors, covering topics like neonatology, immunizations, infectious diseases, and more. It's an 8th edition of a well-established text.

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Manual of Clinical

PAEDIATRICS
For Medical Students & Postgraduate Doctors

Mansour N. Al Howasi
/ 8th
-:.. Edition
 MANUAL OF CLINICAL PAEDIATRICS
(For Medical Student & Postgraduate Doctors)

MANSOUR NASER ALHOWASI
M.B.B.ch, DCH, MRCP (UK), FRCP (E)

Consultant Paediatrician

Former
(Consultant Paediatrician, King Fahad medical city,
Paediatrric Hospital
Clinical Assistant Professor of Paediatrics
King Saud University
Teaching Professor at the Department of child life and
Health University of Edinburgh [part time]
Vice Minister of Health for Health Affairs)
Riyadh,KSA
 Distributed by

www.jarir.com

For More Details
[email protected]

© Mansour Naser Affiowasi, 1996

King Fahad National Library Cataloging-In-Publication Data

Manual of Clinical Paediatrics for Medical Student & Postgraduate Doctors/
Edited by Mansour Naser AlHowasi-Riyadh.. p.,.. cm

ISBN: 9960-31-345-X

1- Paediatrics 2- Children - Diseases - Diagnosis
I - AlHowasi, Mansour N. (ed.)
618.92 de 3619/16

First Edition 1996
Reprinted 1997
Second Edition 2000
Third Edition 2004
Reprinted 2005
Fourth Edition 2006
Fifth Edition 2008
Reprinted 2009
Sixth edition 2011
Reprinted 2012
Reprinted 2013
Seventh edition 2015
Eighth Edition 2019

All rights reserved. No part of this publication may be reproduced in any form or by
any means electronic or mechanical including photocopying without written
permission from the editor.
 Ill

TABLE OF CONTENTS
Chaoter Subiect Pa!!e No.
IDSTORY AND CLINICAL EXAMINATION I
Hjstory 1
Clinical exantlnation 6
Golden rules 9
NEONATOWGY 11
Delivery Room Management 11
Care of the normal newborn 13
Physical examination 14
The premature neonate 18
Neonatal problems of interest 21
Evaluation of neonatal jaundice 23
Infants of diabetic mother 25
Metabolic disorders in newborn 25
Newborn metabolic screening 26
NUTRITION 29
Nutritional reqmrements 30
Estimating energy needs 31
Enteral nutrition 33
Parenteral nutrition 34
Nutritional support 36
Infant Feeding 37
Infant formulas 39
Weaning 40
Common nutritional disorders 41
IMMUNIZATON IDSTORY 43
Basic Vaccination schedule 44
Vaccination in special circumstances 45
Active irnmuni:zation after exposure 46
BCG vaccine 46
DTP, DTaP vaccine 47
(HIB) vaccine 49
Hepatitis A Vaccine 49
Hepatitis B Vaccine so
Influen:za virus vaccine SI
MMR Vaccine 52
Meningococcal Vaccine 53
Pneumococcal Vaccine 54
Poliomyelitis Vaccines 55
Rota Virus Vaccine 56
Varicella Vaccine 57
Typhoid Vaccine 58
Summary Of Commonly Used Vaccines 59
INFECTIOUS DISEASES 60
Meningitis 60
Brucellosis 62
Enteric Fever 63
Tuberculosis 64
Malaria 65
Pertussis (whoopinh cough) 66
Septic Shock Algorithm 67
 IV

Approach To Pediatric Septic Shock 68
Measles 69
Rubella 70
Mumps 70
Infectious Mononucleosis 71
Chicken Pox 72
Viral Hepatitis 73
PEADIATRIC EMERGENCIES & INTENSfVE CARE 75
Norma l Vital Signs in infants and Children 75
Basic Life Support 75
Advanced Life Support 79
Respiratory Failure 80
Acute Respiratory Distress Syndrome 83
Diabetic Ketoacidosis 85
Status Epilepticus 87
Causes of Status Epilepticus 88
Traumatic Brain Injury and Increased lntracranial Pressure 89
Causes of Brain injury and increased ICP 90
Shock 92
Differential Diagnosis of septic shock 96
Acute Upper Airway Obstruction 98
Comatose Child 99
CARDIOVASCULAR SYSTEM 102
History 102
Examination l02
Innocent Murmur 104
Finger Clubbing l08
Chest Scar 108
Cyanosis 109
Presentation and Management of Heart Disease in the Neonatal Period 111
Ductus Dependent Lesion 112
Electrocardiogram (ECG) 113
Congenital Malformation syndromes associated with congenital heart disease 117
Acyanotic lesion with left to right shunt 118
Cyanotic Heart Disease 119
Obstructive Lesion 120
Valvular Lesions 121
Hypertentioa 122
RESPIRATORY SYSTEM 124
History 124
Clinical Examination 125
Examination Of The Young And Uncooperative Patients 130
Respiratory Failure 132
Clinical Anatomy of The Lungs 133
Causes of Some Important Respiratory Signs 134
Apnea 137
Bronchial Asthma 138
GASTROINTESTINAL SYSTEM 144
History 144
Examination 144
Causes of Ascitis ISO
Abnomial abdominal masses 151
 V

Causes of hepatomegal y 152
Causes of Splenomegaly 153
Portal Hypertension 154
Causes of Hepatosplenomega ly 154
Causes of Bleeding Per Rectu m 154
Di ffi rential Dianosis Of The Recurrent Abdominal Pain In Children 155
Etiology of Chronic Dian-hea In Children 156
The Major Causes OfCholestasis In Infa ncy 157
Dehydration 158
Oral Reydration solution (ORS) 159
RENAL SYSTEM 160
History 160
Examination 162
Urine Analysis 164
Urinary Tract Infection (UTI) 164
Hematuria 166
Proteinuria 169
Renal Tubular Acidosis (RTA) 170
Acute Renal Failure (ARF) 173
Chronic Renal Failure 176
ENDOCRINOLOGY & DIABETES 178
Growth 178
Short Stature 178
Obesity 180
Tall Stature 181
Calcium Disorders 181
Thyroid Disorders 184
Ambigious Genitalia 185
Hypoglycemia 188
Puberty 189
Precocious Puberty 190
Diabetes Mellitus 191
Di abetes lnsipidus (DI) 194
Adrenal ~1sufficiency 195
Cushing Disease / Syndrome 195
NERVOUS SYSTEM & DEVELOPMENT 198
Genera l Examination 199
Mental status examination 201
Cranial Nerves 203
Golden Rule 213
Refl exes 215
Golden Rule 222
Abnormal Head Shape 224
Abnormal Head Size 224
Clinical approach to abnormal head size 225
Sudden Onset of Unsteady Gait (ATAX IA) 226
Causes of Ataxia 227
Acute Paralysis 227
Acute Hemi plegia 229
Floppy In fa nt Syndrome 231
Cerebral Palsy (CP) 234
Neurodegenerati ve Disorders (N OD) 237
 VI

Developmental Examination 243
Essential Milestones 245
MUSCUOSKETLETAL SYSTEM 251
History 251
Examination 252
Knee joint examination 253
Genu Varum (Bow Legs) 255
Genu Valgum (Knock Knees) 255
HIP Joint Examination 256
Congenital Hip Dislocation (CDH) 257
Ankle Joint and Foot Examination 258
Flat foot (PES PLANUS) 259
PesCavus 259
II;permobility of the Joints 260
Talipes Equinovarus 260
Torti coll is 260
Toe Walking 261
Examination of the Spine for Scoliosis 261
Pain Amplification Syndromes in Children 262
Assessment of child with juvenile chronic arthritis 264
DEVELOPMENTAL AND BEHAVJORAL PEDIATRICS 267
Autism Spectrum Disorder (ASD) 267
Attention deficit Hyperactivity Disorder (ADHD) 269
Conduct disorder 274
BREAKING BAD NEWS 277
 VII

PREFACE

Previous edition of Manual of Clinical Pediatrics proved to be very successful as a
practical manual, both here and overseas; providing the opportunity for this eighth
edition.

Many chapters in the eighth edition of this manual have been extensively updated and
revised. The new chapters on Emergency and Intensive Care and Breaking Bad
News have been added. The format of the manual has remained essentially the same.

The management principles and protocols in the update of this manual are not based
on practices at only one institution. Contributors are from different institutions in the
Kingdom of Saudi Arabia. I feel this has enabled us to produce a manual that is not
institution-specific but reflects a cross section of contemporary approaches to
pediatric management.

My sincerest thanks to the contributors of the first, second, third, fourth, fifth, sixth
and seventh edition, and my family for their continued support, which has been
indispensable to the completion of this edition.

I would like to extend my SPECIAL THANKS TO DR. SAMEEH GHAZAL who
had worked very hard, in spite of his tight schedule on reviewing all the manuscripts,
in addition to his contribution to the manual by two chapters, several drawing, and
figures.

Also I would like to thank Dr. MARAM SAMEER for her great effort to prepare
and design this edition.

I welcome any suggestions and comments regarding the manual; letters should be
addressed to:

Dr. Mansour AI-Howasi
P.O. Box 62300
Riyadh, 11585
KS.A.

[email protected]
 VIII

CONTRIBUTORS

(Alphabetic order)

PROFESSOR ABDULLAH AL HERBISH
MBBS, FRCPC, FAAP
Consultant, Professor of Pediatrics and Endocrinology
College of Medicine & King Saud University, Riyadh
(Endocrinology)

Dr. ALIA AL IBRAHIM
MBBS, DCH, CABP, Fellowship in Paediatric Nephrology
Consultant in Paediatrics & Paediatric Nephrologist
KKUH Hospital
Riyadh, KSA
(Renal System)

9 PROFESSOR ASAAD ABDULLAH ASSIRJ
MBBCh, MRCP (UK), FRCP
Consultant, Professor of Paediatrics and Gastroenterology
King Saud University, Riyadh, KSA
(Gastrointestinal System)

Dr. DHIMAN CHOW1JHURY
MBBS, DCH, MRCP (UK), FRCP (Edin.)
Consultant and Assistant Professor of Paediatrics
!WK Grave Health Center, Department of pediatrics, Dalhousie University. Canada
(Gastrointestinal System)

Dr. IBRAHIM S. ALHIFZI
MBBS, DCH, CABP, FRCPCH, FRCP
Consultant Neonatologist
Clinical Professor of Paediatrics
Armed Forces Hospital, Southern Region
(Examination of Neonate)

Dr. MAHER AHMED KHALIFA
MBBCh, DCH, MRCP (UK)
Consultant Paediatrician & Paediatric Neurologist
Insurance Hospital (Riyadh), Riyadh, KSA
(Neurology & Development)

Dr. MANSOUR M. ALQURASHI
MBBS, DCII, MRCP (UK), ABP, Fellowship in Cardiology
Consultant PaediatTician & Paediatric Cardiologist
AlYammamah hospital,
Clinical Assistant Professor of Paediatrics
King Saud University
Riyadh, KSA
(Cardiovascular System)
 IX

Dr. MANSOUR NASER ALHOWASI
MBBCh, DCH, MRCP (UK), FRCP (Edin.)
Consultant Paediatrician. KSA
Former, (consultant paediatrician King Fahad Medical City K.S.A
Clinical Assistant Professor of Pediatrics
King Saud University
Teaching Professor at the Department of child life and Health University of Edinburgh [part
time]
Deputy Minister for Executive Affairs, MOH) Riyadh, KSA
(History and Clinical Examination, Neonatology, Immunization, Nutrition and infant feeding,
Cardiovascular system, Gastrointestinal system, Urinary system, Neurology and development,
[nfectious Diseases)

Dr. MOHAMMED F. FAROUQ
MBB.ch, F AAP
Consultant in Paediatrics and Infectious Disease
Assistant Professor in Paediatrics and Haed of paeditrics department
King Abdu laziz University, Jeddah, K.S.A.
(Immunization)

PROFESSOR MOHAMMED MOHAMMED JAN
MBBCh, FRCPC
Consultant Paediatric neurology
Professor of Paediatrics & Neurology
King Abdu laziz University Hospital &
' King Faisal Specialist Hospital and Research Center, Jeddah, K.S.A.
(Neurology)

Dr. SALEH MOHAMMED ALSALEHI
MD, DBP
Consultant Developmental and Behavioral Pediatrics, KFMC
Assistant Professor KSU, Riyadh, K.S.A.
(Developmental and Behavioral Pediatrics)

Dr. SAMEEH S. GHAZAL
MBBCh, DCH, MRCP (UK), ABP, MRCPCH (UK), CIC (USA), Epidemiology fellowship
(USA)
Consultant Paediatrician, Infectious Diseases and infection Control
Prince Mohammad bin Abdulaziz Hospital (Medical Director)
Assistant Professor of Paediatrics
King Saud Bin AbdulAziz University- Health Science, Riyadh, KSA
(Infectious Diseases & Respiratory System and Bronchial asthma)

Dr. SMRJTI CHOWDHURY
MBBS, DCH, MRCP (UK)
Consultant Paediatrician
Department ofneonatology, Dalhousie University. Canada
(Gastrointestinal System)

Dr. WAFAA AL SUWAIRJ
MBBS, DCH, MRCP (UK), ABPP.
Consultant Paediatric Rheumatologist
King Abdulazez Medical City, National Guard, Riyadh, KS.A.
(Musculoskeletal System)
 X

Dr. WALEED HAMED ALBUALI
Consultant pediatric lntensivist, Assistant professor
Pediatric ICU director, Department of Pediatrics
King Fahd Hospital of the University
AI-khobar, Saudi Arabia
(Emergency & Intensive Care)

Dr. YOUSEF K. GHAZAL
MBBCh, MRCP (UK), CABP, SBP, MRCPCH (UK)
Consultant Paediatrician, lntensivist
King Fahad Medical City, Children 's Hospital, Riyadh, KSA
(Nutrition & Infectious Diseases)
1 History & Clinical Examination

History
Demographic data:

Name
Age (date of birth)
Sex
Nationality
Address
Source of history: (mother, father & others)

Presenting complaints:

Use their words. (The parents may actually tell you the diagnosis).
Symptoms with duration.

History of presenting complaints:

Obtain a complete chronological sequence of events. Deeper inquiry about important
symptoms must be made regarding:

Onset
Course
Duration
Site
Frequency
Severity
Relieving factors
Exacerbating factors
Diurnal or seasonal variation
Relation to food
Relation to exercise e.g. cough
School missing related to the complaint
Any associated symptoms

1
 System Inquiry:
System inquiry is important when there is complain not specific to one system. E.g.
fever or when there is there multisystem disease.
There are few questions, which provide useful "screening"

General e.g.:
Feeding and appetite ( very important)
Irritability
Weight loss

Cardiovascular e.g.:
Breathlessness
Sweaty on feeding
Cyanosis

Respiratory e.g.:
Breathlessness
Runny nose
Cough
Noisy breathing (wheeze or strider)
Sore throat or earache
Hemoptysis

Gastrointestinal e.g.:
Vomiting
Abdominal pain
Constipation or diarrhea (frequency and appearance of stool)
Jaundice

Genitourinary e.g.:
Frequency
Dysuria
Nocturia or enuresis
Hematuria
Incontinence
Age of menarche

2
 Neurological e.g.:
Irritability
Drowsiness
Fits or abnormal movements
Headache
Numbness or unpleasant sensation
Weakness

Hematological & oncological e.g.:
Pallor
Jaundice
Bone pain
Bruises
Bleeding from the nose

Infections e.g.:
Skin rash
Contact with infectious patients
Recent travel

Musculoskeletal& skin e.g.:
Joint swelling
Joint pain
Skin rash

N.B. If any symptom during the system review is positive, deeper inquiry must be
made
e.g.:
Cough-Nocturnal or related to exercise points towards bronchial asthma.
Purulent sputum points towards suppurative lung disease.

Past medical history:
This includes:
Previous diseases
Previous medications taken by patient:
-Frequency

3
 -Does
Previous hospitalization
Previous surgery
Previous transfusion
Any known drug or food allergies?

Pregnancy and neonatal history:
Follow up during pregnancy
Mother's illness during pregnancy (nature of the illness-which trimester) e.g.-flue like
illness or skin rash during early pregnancy may point towards congenital infections.
Mother's medication: e.g.- Valproate taken by the mother during pregnancy increase
risk of fetal neural tube defect.
Anabolic steroids taken by the mother during pregnancy may cause virilization of
female fetus.
Phenytoin taken by the mother during pregnancy may cause increase risk of fetal
congenital anomaly especially cardiac anomaly.
Exposure of mother to radiation during pregnancy.
Fetal movement: weak fetal movement may point towards intrauterine hypotonia. e.g.
dystrophia myotonica, spinal muscular atrophy.
Polyhydramnios- may point towards fetal GIT obstruction. e.g. esophageal atresia or
intrauterine hypotonia.
Oligohydramnios:- may point towards fetal urinary system abnormality. e.g. bilateral
renal agenesis.
Length of gestation.
Mode of delivery.
Birth weight, height and head circumference.
Apgar score.
Any neonatal disease or admission and why?

Nutritional history:

Breast-fed or bottle-fed and for how long?
If bottle-fed:

-Which formula did he receive?

-How is it prepared?

4
-What volume did he take at each feed?

-And how long did he take it?

-Frequency offeeds

-Total daily intake

Time of weaning- timing of introduction of solids and cereals.

N. B. Normally, breast-fed baby might pass up 6 motions daily.

Immunization history:

The recommended vaccination program in Saudi Arabia will be described later on:

Check immunization card.
If there is fai lure in taking any vaccine ask for the reasons in details.

Developmental history:

This includes:

Gross motor.
Fine motor.
Speech and hearing.
Social and play.
Schooling (level and performance).

N.B. -If the mother has other children, compare his or her development with his or her other
siblings.

-some important development milestones will be described later on.

Family and social history:

Ages of parents.
Consanguinity
Number of siblings and age range (any sibling from previous or another marriage)
Family history of similar condition.

5
 Which region the parents originally came from (e.g. sickle cell anemia common in
south- west and eastern region of Saudi Arabia)
Neonatal deaths (e.g. metabolic disease)
Previous abortions.
Housing - type of accommodation (rented or owned, house or flat, number of
bedrooms, washing and toilet facilities, air conditions and heaters)
Parents' occupation and income of the family.
Parents' education
Parents' smoking habit (especially in bronchial asthma cases)
Contact with animals
Recent travels (e.g. malaria in southwest of Saudi Arabia)

N.B.
Pay more attention to detailed family history, if hereditary, allergy or infectious
disease is involved e.g. sickle cell anemia, bronchial asthma, and tuberculosis.
Transportation: Make sure there is available transportation for the child and his or her
attendance to be able to attend any follow-up.
Try to make the appointment of any follow-up suitable for the condition of the
father's work.
If the patient came from poor family, contact the social worker to arrange for the
family financial support and airplane tickets between the regions if the family came
from far area... etc.
Golden role: at the end of your history, ask the historian if she or he likes to inform you
anything else or if she or he expects you to ask her or him any other question about her or
his child that was not asked yet.

Clinical examination
General advice on examining children:
I. Introduce yourself to the child and or his attendant.
2. Ask the child's name.
3. Wash your hands especially if the child is an infant.
4. Warm your hands and remove watch or ring, which might scratch the child.
5. Inform the child that you are going to examine him e.g. I am going to percuss
your chest.
6. Avoid standing over a small child by getting down to his level.

6
 7. Distract the child with a toy or any other thing if this will help you to continue
your examination.
8. Talk to the child as you examine and smile to him or her.
9. Remember to thank him at the end of the examination.
10. During examination some of the examiners like to hear running commentary
while you examine the child.

Never & Do not
Never handle the child roughly.
Never refer to a child as dysmorphic without first seeing the parents
(except the common known syndromes e.g. trisomy2 l)
Do not get the sex of the child wrong.
Do not use potentially worrying tenns in front of parents without
explaining them e.g. tumor or mental retardation.
Do not use abbreviations in your clinical notes except if it is
internationally known and accepted.
Do not discuss the case with your colleague in front of parents using
foreign language without explaining to the parents what you are doing
and reassuring them.

General examination:
General condition:
Looking sick
Looking well
Vital signs: (very important)
Temperature
Respiratory rate
Pulse
Blood pressure
Growth parameter: (plot them in standard centile chart) very important
Weight
Height
Head circumference
Color:
Pallor
Jaundice
Cyanosis

7
Dysmorphic features:
Upward slanting eyes
Depressed nasal bridge
Obvious abnormality:
Club foot
Legs censoring
Pectus deformities
Skin condition:
Hyperpigmentation
Skin rashes
Supportive measures:
Oxygen
Intravenous fluid
Splint
Wheelchair

Systemic examination:

Inspection:
A great deal of information can often be elicited without even touching the child. In
addition some children will cry as soon as you touch them. You should expose the
relevant area, (the whole chest, the whole abdomen or the legs).
If the parents are present ask them to undress the child, otherwise you will miss an
operation scar, hydrocele, muscle wasting or some other important signs.
Do comment in the general condition of the patient (well or ill), and on intravenous
drips, nasogastric tubes, urinary catheter, or obvious dysmorphic features if
present... etc.

Palpation:
If there is any possibility of the part you are palpating being painful, you should ask
the patient if it hurts and being particularly gentle.
e.g. abdomen, joints and lumps.

Percussion:
Do not forget the percussion is an important method to detect organomegaly
especially in young children.

8
 Technique of Percussion:

Auscultation:
Do not forget to auscultate the abdomen
, for intestinal sound and bruits.
Do not forget to auscultate the anterior fontanel for bruits when you examine a
newborn with heart failure. (A-V malformation)
N.B. - Try to start from the periphery then go central.
Sequence of examination might be difficult to apply in young children.

~Golden Rules:
✓ If there is one congenital anomalies, look for other congenital anomalies.

e.g. examine the heart and urinary system in any child with dysmorphic features.

✓ If there is one endocrine disease, look for other endocrine diseases.

e.g. look for signs of hypothyroidism in any diabetic patients.

✓ If there is one nutritional disease, look for other nutritional disease.

e.g. look for iron deficiency anemia in any patient with rickets.

9
✓ If there is one "atopic" disease look for other atopic diseases.

e.g. look for atopic eczema in any patient with bronchial asthma.

✓ If there is one autoimmune disease, look for other autoimmune diseases.

e.g. look for signs of Addison's disease in any patient who has alopecia area or vitiligo.

Do not forget in clinical examination the principles:

Growa paramt tr

10
2 Neonatology

The success of the health care system in countries is commonly judged by infant
mortality rate (death occurring from birth to 12 months / 1000 live births).

The neonatal period ( I s1 four weeks of life) is a highly vulnerable time for the infant
and neonatal mortality where it accounts for about 65% of infant mortality; hence
proper care of the neonate contributes significantly to reduction in infant mortality.

I. Delivery Room Management
1. Anticipation
Proper information obtained from the obstetrician or the midwife about
maternal condition should identify neonates at risk of developing problems in
the delivery room. This includes mothers with certain diseases or problems
such as premature labor, IUGR, prolonged rupture of membranes (18 hours
before delivery), oligohydramnios, polyhydramnios, diabetes, pregnancy
induced hypertension, infections, fetal distress, etc.

2. Preparation
Check the resuscitation equipment and the medications needed for
resuscitation.

1. Radiant warmer switched on, warm towels
2. Arnbu bag connected to air-oxygen blinder
3. Laryngoscope and blades (Size: 00, 0, 2)
4. Endotracheal tubes (size 2.5, 3, 3.5)
5. Stethoscope
6. Stop clock
7. Catheters, cannulas, syringes and needles
8. Medications

11
 3. Ressuscitation :

Place Wider" raiianl heater
(SUclion trachea if mecomm-siained Iliad)
Dry thorougHy
Remove wet Lenin :I Evauate response
Position
SUclion mouth then nose Non or gasping Spontaneous
Provide tactile stimulation respiration breathing

l
Provide positive I Evaluate heart rate
preSSure ventilation
for 30 Secs
~ < 100/min >100/min
Evaluate heart rate I
l J.
--..L
!
Below60 HR fi0-100 HR 60-100 Above 100 --l Evaluate. Continue not increasing Increasing Watch for
color
veritilatioo. Continue
spontaneous. Chest

~
ventilation. Continue respiration
compression. Chest
ventilation then DIC
compression
ventilation

I
Initiate medication if HR < 60
after 30 Secs.
I Pink or peripheral cyanosis Provide
,I, oxygen

PPV and chest compression I Observe and mocitor
- Resuscitation with room air is safe and effective
- lntrapartum suctioning of oro and nasopharynx is not recommended for infant born with
meconium stained liquor and suction of trachea is not recommended if baby is vigorous.
During this process Apgar score should be estimated as fo llows:

SCORE 0 2
A = Appearance Blue/ Pale Blue extremities Pink

P = Pulse (HR)/min. 0 < 100 > 100
G = Grimace None Grimace Cry
(Reflex Irritability)

A= Activity Flat Some limbflexion Active movements
(Muscle Tone)
R = Respiration Absent Slow, irregular Strong cry
Leuthner et al Ped Clinic of NA Vol 41 No 5 Oct 1994

12
Chest compressjon techniques Ccardjac massage}
a) Two Thumbs Method (Preferred}
Place both thumbs on the middle third of the sternum just below an imaginary line drawn
between the nipples, with the fingers encircling the chest and supporting the back. The xiphoid
or lower portion of sternum should not be compressed to avoid abdominal trauma.
:W Two Finger Method
The index and middle finger are placed over the middle third of the sternum.

Medications
The medications that are currently recommended during resuscitation of the newborn infant are:

Adrenaljne ffipjnephrine}:
0.01 - 0.03 mg / kg of 1: 10000 solution using high dose Epinephrine may lead to hypertension,
decreased myocardial function and poor neurological outcome. ET dose is 0.1 mg/kg/dose.

Naloxone:
Used to reverse respiratory depression caused by narcotic administration to the mother.
Dose: 0.1 mg I kg Route: IV only.

Volume Expander:
10 mls / kg as Normal Saline, or O-Negative blood if blood loss is suspected.

The routine use of Sodium Bicarbonate is discouraged, except in prolonged arrest. Atropine and
calcium is not recommended in resuscitation of the newborn.
A brief examination should be done in delivery room to look for major congenital
malformations. The baby will then be sent to Nursery or Neonatal ICU according to his/her
condition.

II. CARE OF THE NORMAL NEWBORN
Normal newborns should be given to mothers as soon as they are stable enough to be breast-fed
and should always be nursed with their mothers. A detailed examination must be performed
within 24 hours of birth.
It should be done in the presence of the mother or both parents to answer their questions and to
give advice about feeding and care of their baby. Vaccinations should be given, routinely BCG
and hepatitis B vaccine, but hepatitis B irnmunoglobulin is added to babies of mothers with
hepatitis B positive screening.

13
1,..............---. -: : -.'I -·.. _ _._ _... -----:-~- - - -~~

Physical examination of the newborn infant

This requires patience, gentleness, & flexibility, so auscultation of the heart and palpation of
the abdomen can be done while the infant is quiet and relaxed. Adequate light, warm hands
and environment are prerequisite. Proper hand washing before examination is essential.

Vital signs should be recorded: Pulse (normal 120 - 160 / minute), Respiratory Rate (30 - 60 I
minute), and temperature.
Weight, length, and head circumference should be plotted on centile
GENERAL APPERANCE
Alertness
Movements
Color (cyanosis of cold periphery is normal)
Dysmorphism
SKIN
Pallor (circulatory failure or anemia)
Mottling
Plethora (polycythemia)
Jaundice
Birth marks, hemangiomas, mongolian blue spots
Rash (erythema toxicum, septic spots, herpes, transient pustular melanosis)
Edema (generalized: hydrops) (localized: hands and feet in Turner's syndrome)
HEAD
Size
- Microcephaly: familial, congenital infection
- Macrocephaly: hydrocephalus, familial, achondroplasia,hydranencephaly, etc.
Shape
Fontanelles & sutures
Masses - cephalohematoma (collection of blood w1der the periosteum which does
not cross sutures) - Caput succedaneum (edematous scalp of the presenting part)
FACE
Dysmorphic features
EYES
Microphthalmia as in congenital rubella syndrome
Buphthalmos (corneal diameter > I cm)
Slant of palpebral fissures (upward or downward)
Conjunctiva! hemorrhage
Coloboma of the lids or the iris (syndromes)
Aniridia (association with Wilms tumor and other urogenital anomalies)
Red reflex suggests absence of cataract and major intraocular pathologies
Leukokoria (white pupillary reflex) seen with cataract, ROP, and retinoblastoma

14
 Hypertelorism (widely spread eyes), or hypotelorism

EARS
Low set ears (classically seen in Down' s Syndrome)
Malformations and periauricular tags
Ear drums appear normally dull gray

MOUTH
Natal teeth (remove only if loose or interfere with feeding)
Large tongue is seen in congenital hypothyroidism, Beckwith-Wiedemann syndrome and others
but glossoptosis is seen with Pierre Robin syndrome
Cleft lip and palate
High arched palate
Lingual thyroid

NECK
Normally short
Swellings: goiter, cystic hygroma, thyroglossal cyst, sternomastoid mass.
Redundant skin at the back of the neck is seen with Down's Syndrome and is assoc iated with
webbing in Turner's Syndrome

RESPIRATORY
Chest Shape: pectus, nipples, space
Sounds: (grunting, stridor, crying), air entry, breath sounds, added sounds
Movements

CARDIOVASCULAR
Pulse: rate, rhythm, volume, etc.
Weak femoral pulse and higher BP in upper limbs than lower limbs (Coarctation of the Aorta)
Dextrocardia
Heart sounds
Murmur

ABDOMEN
Distended or scaphoid
Organomegaly
Hernias
Bowel sounds

GENITALIA
Sex
Ambiguity
Testis

15
-- - - - -- -- - -- --~ -~.~- --=--~ -

'.

Labial fusion
Hypospadias
Check anal patency

NEUROLOGY
Alertness
Movement and posture
Tone
Reflexes
Primitive reflexes: (Leave them to the end of examination)

Reflex Stimulus Response Appearance Disappearance
(Gestational (Corrected age)
age)
Moro Lift the head slightly Rapid extension & 28 - 32 weeks 3 - 5 months
and then drop it gently abduction of arms with
on your palm hand opening followed
by slow return to mid
line
Sucking Nipple or teat Strong & synchronized 32 weeks 4- 7 months
sucking
Rooting Gently stroke the cheek Baby searches with his 32 weeks 4 - 7months
with finger tip mouth
Palmar Touch the baby's open Baby grasps the finger 32 weeks 3-4 months
palm with your finger
Plantar Firmly press the ball of Toes flex 32 weeks 8 months
infant's sole with your
thumb
Stepping Hold the infant Alternating stepping 34 weeks 2 months
upright with the sole movement
touching a flat surface
Placing Touch the dorsum of a Baby climbs over the 34 weeks 5 months
foot with the edge of the edge of the table
table

EXTREMITIES
Size and shape (e.g. hernihypertrophy)
Digits (count, syndactyly, etc.)
Club feet

BACK
Mongo lian blue spots
Hair tuft

16
 Dimples
Sinus
Scoliosis

HIPS
Asymmetry of groin creases
Barlow's & Ortolani's Test - (to assess hip dislocation)
Lay the infant supine on a flat hard surface and remove the nappy. Stand in the mid line at the
foot end of the infant, flex infant's knees fully and hips to 90°. Hold the lower limbs with your
thumbs on the medial condyles and tips of the middle finger on the greater trochanters of each
femur. Bring the knees together and attempt to push the hips posteriorly. If you feel a 'click ', it
means the head of the femur has dislocated (Barlow's sign). Keeping the grip unchanged, now
abduct the infant's thighs with the thumbs and lift the femoral heads forward with the middle
fingers. If you feel a definite 'clunk', it means the previously dislocated head of the femur has
slipped back into the acetabu lum (Orto lani's sign).

e.rtowtt ~
t>ac art111 to vy to
P.i., -,.~
--- diskx:sie hlo

Ort.olanl Utt
Ali,iil,cting ther-,, tc U}' to
n:locak hlr
F~..-'1i pu!,I, mur forw rd
rtca~l,ui.;rr.

Examine newborn requires:

Patience, gentleness

& flexibility

17
 THE PREMATURE NEONATE

The New Ballard Score
New Ballard Score Sheet
Use this score sheet to assess the gestational maturity of your baby. At the end of the
examination the total score determines the gestational maturity in weeks.
NEUROMUSCULAR MATURITY
-
SIGN SCORE SIGN
SCORE
-1 0 1 2 3 4 5
Posture
a:i=: ~ « ~ ~
Square
Window
r~. [ r,~ ~ 45 ~w r~
~, ~ tr~
Arm
Recoil
1 1 ~.1w 110- 140" ttllO"

CD''°" c6 cb d) ~
Popliteal
Angle CI:)
,w
a:) ,t 8 ears ol
1st drug:
Doxycycline/Tetracycline 1st drug :
(6 weeks) Bactrim 6 weeks
Simple infections
2nd drug 2nd drug:
Bactrim (3 weeks) or Rifampicin 6 weeks
Rifampicin (6 weeks)

-Use Streptomycin (2 weeks) or Gentamicin (1-2 weeks) in
place of the 2nd drug.
*Serious infection or -N.B. Rifampicin can be used as well as adjunctive therapy to
complications: reduce the rate of relapse.
- Endocarditis -For life threatening complication such as meningitis or
- Osteomyelitis endocarditis, the duration of therapy is often extended for
- Meningitis several months.
-For osteomyelitis, earty surgical intervention should be
considered.

DRUG DOSE/DAY Divided to
--=-~--___;;==;;;;;:;;=;;;;
Bactrim Trim. 10mg/kg/day + Sulph.-50mg/kg/day 2 doses

Rifampicin 20 mg/kg/day 1 or 2 doses
~--~--- ~------====;;;;
Doxycycline 2-4 mg/kg/day 2 doses
------------
Tetracycline 30-40 mg/kg/day
-----====="'"".
4 doses

-------
Streptomycine
Gentamicin
20
5 mg/kg/day
{IM) --=2_...dc,018S
3 doses
_---====:::::

NB. Ist drug should be given to all patients
Inform infection control department in all positive cases

ENTERIC FEVER
Clinical manifestation:
Fever
Constitutional symptoms: e.g. Headache, malaise, anorexia and lethargy
Abdominal pain, tenderness, splenomegaly and hepatomegaly

63
 Rose spot (maculopapular rash)
Change in mental status

Diagnosis:
1) Cultures: Blood culture
Urine and stool culture after the first week
Bone marrow culture (the most sensitive method)
2) Serology: Wida! test

Treatment:
Empirical therapy with Ceftriaxone or Cefotaxirne until antibiotic susceptibility is available
In case ofresistance to Ceftriaxone, Ciprofloxacillin can be used as alternative.

TUBERCULOSIS

Clinical manifestation:
General: Fever, night sweat, anorexia, decreased activity, weight loss...
Local: According to site involved

Diagnosis:
High index of suspicion
High ESR
Positive PPD test (Mantoux test)
Quantiferone golden test
Chest x ray
Positive smear for acid-fast bacilli and/or culture for mycobacterium tuberculosis fromsputum,
gastric aspirate, lymph node or other involved site.
Mantoux test: is intradermal injection of 0.1 ml containing 2 tuberculin units (TU) of purified
protein derivative (PPD)
Interpretation of PPD skin test: PPD considered positive if the amount of indurations after 48-72
hours is either:

History of contact with open Personal risk factors No personal or
case or. < 4 years environmental risk
Suspected tuberculosis. Lymphoma factors
(symptoms, signs or chest. D.M.
radiograph) or. Renal failure
lmmunocompromised patient. Malnutrition
or
- Environmental risk factors
(environmental exposure to TB)

64
 Treatment:
Short course of treatment gives better compliance and drugs combination decreases the risk of
resistance, so the following protocol is recommended:
A- Positive PPD in otherwise normal child (clinically and after investigation)
Start INH alone for 3 months (as prophylaxis) then re-evaluate the patient:
I. No disease continue INH for 6 months
2. Sign of disease: treat as in B

8- Diseased patient: Full treatment:
1. INH: 6 months and
2. Rifampicin: 6 months and
3. Pyrazinamide: 2 months
4. In severe infections: (meningitis, rniliary) give in addition Streptomycin (in patients < 8
years of age) or Ethambutol in patients> 8 years of age for 2-3 weeks

N.B. In Renal, Bone and CNS infection, treatment should continue for up to 12-18 months.
Before starting therapy and during follow up CBCs, liver functions tests should be
monitored.
Tuberculosis is a reportable disease, report to the health authority.

MALARIA

Clinical manifestation:
- History of travel to endemic area
- Fever, chills, rigors, sweat, headache, pallor, jaundice, hepatosplenomegaly.

Diagnostic test:
Stained blood film:
- Thick blood film: for parasite identification
- Thin blood film: for species identification
Parasitic index: % of infected RBCs
< 1%: mild Parasitemia
1-5%: moderate Parasiternia
> 5%: severe Parasiternia

Treatment:
I. Supportive therapy: for fever, fluid and electrolytes
2. Specific therapy:
A. Oral therapy: all types of malaria provided that P. Falciparum is susceptible.

65
 - Chloroquine phosphate: l Omg/kg stat, then 5 mg/kg 6 hours later, then 5 mg/kg/day for
2 consecutive days.
- lf no response (no decrease in the parasitemic index in 24 hours) after consultation of
infectious disease department give Fansidar (Pyrimethamine and sulphadoxine) as
single dose. If no response - Mefloquine hydrochloride as single dose (not in children
< 15 kg weight).
B. Parenteral therapy: For those who have persistent vomiting or who are in coma.
- Quinine dihydrochloride, if not available
- Quinidine gluconate, if not available
- Chloroquine hydrochloride
- Parenteral therapy should be replaced by oral therapy as soon as possible.

C. Prevention of relapses (plasmodium vivax or p. ovale): - Primaquine phosphate for 14 days
starting in the 3rd day of chloroquine phosphate.

Chemoprophylaxis:
Starting day: 1 week before traveling to endemic area
End day: 8 weeks after leaving the endemic area
Drugs: Chloroquine is generally preferred: 5 mg/kg/once per week
For chloroquine resistant area other drugs can be used like: proguanil or fansidar.

PERTUSSIS (WHOOPING COUGH)
Etiology: Bordetella pertussis (Gram-negative bacilli).

[ncubation period: 6 - 21 days

Clinical features:
Catarrhal phase ( 1-2 wk): rhinorrhea.
Paroxysmal phase (2-4 weeks or longer): Bouts of coughing in runs of IO or more followed by
whoop and ends by vomiting.
Convalescent phase (1-2 weeks): coughing slowly subsides over period which can last up to 3
months (hundred days cough as used to be said).

Complications:
Respiratory: Pneumonia (more commonly by secondary bacterial infection), apnea, atelectasis,
otitis media, sinusitis, pneumomediastinum, pneumothorax, interstitial or subcutaneous
emphysema. Later on: Bronchiectasis.
Hemorrhage: Epistaxis, retinal, subconjunctival, intraventricular.
Hernia: Inguinal, umbilical, rectal prolapse, rupture of diaphragm.

66
 Cerebral anoxia: following apnea manifests as fits - 2.5%, encephalopathy 0.5%, apnea and
sudden death may occur during very severe paroxysm.

Treatment:
Erythromycin, when given within 14 days ofonset of the disease, may eliminate the organism
from nasopharynx, improve symptoms and reduce communicability.
In severe paroxysmal attacks salbutamol nebulization and steroid might be helpful.
Treat complications.

Isolation & infectivity:
The patient should be placed in droplets precautions for at least 5 days
Treat with erythromycin for a total of 14 days.
Close contacts of less than 7 year of age who are unimmunized or who have received fewer than
4 doses of DTP should have pertussis vaccine according to the recommended DTP schedule and
erythromycin for 14 days.

SEPTIC SHOCK ALGORITHM
Definitions
Systemic inflammatory response syndrome - SIRS is the presence of two or more of the
following criteria (one of which must be abnormal temperature or leukocyte count):
o Core temperature of >38.5°C or 2 standard deviations above normal for age
o Mean respiratory rate >2 standard deviations above normal for age
o Leukocyte count elevated or depressed for age, or > 10 percent immature
neutrophils

Infection - Infection is defined as a suspected or proven infection caused by any pathogen.
Sepsis - SIRS in the presence of or as a result of suspected or proven infection.
Severe sepsis - Sepsis associated with cardiovascular organ dysfunction, or acute respiratory
distress syndrome, or with two or more other organ dysfunctions.
Septic shock - Sepsis with cardiovascular dysfunction despite the administration of 2:40 mL/kg
of isotonic fluid in one hour.

Do not discuss the case with your colleague in front
of parents using foreign language without explaining
to the parents what you are doing and reassuring
them.

67
 Approach to Pediatric Septic Shock
0 min
' Recognize decreased mental status and perfusion.
5 min Maintain airway and establish access according to PALS
guidelines.

Push 20cc/kg isotonic saline or colloid boluses up and over
60cc/kg.
Correct hypoglycemia and hypocalcemia.
Administer antibiotics.
J
15
Fluid refractory shock
min
+ i---
Fluid responsive 1 Establish central venous access, begin dopamine or
dobutamine therapy and establish arterial monitoring.

Fluid refractory - dopamine/dobutamine resistant

L Obs~rve in]
PICU
Titrate epmephrine for cold shock, norepinephrine for warm
shock to normal clinical endpoints and ScvO2 saturation ~70%
7

Catecholamine - resistant shock t
l
60 min
r
L__
Begin hydrocortisone if at r'.sk for absolute adrenai
msuffic1ency __J
7
__ i=
Normal Blood Low Blood Pressure
Pressure Pressure
Cold Shock Cold Shock Warm Shock
ScvO2t at 1 year
- Start chest compression at lower half sternum or one finger below nipple line in infants.
a) < 1 year give 100 compressions/min: depth 2 cm
b) 1 year give 100 compressions/min: depth 3 cm
c) Old child: depth 4-5 cm or 1h- ½ depth of chest.
d) Give I breath/ 5 compressions in general
e) For neonate give 120 compressions/min & l breathe for every 3 compressions. Old child (>8yrs)
may also be given 2 breaths/IS compressions as adult.
f) For compression use 2 fingers (index and middle finger) or both thumbs encircling the chest for
neonates & small babies, and use heel of one hand for younger children, and heel of 2 hands for
older children. Continue BLS until advanced life support can be offered or ifno response after 30
minutes. Activate advanced life supp01t team after 1 minute & continue resuscitation.

8: For breathing:
- Open airway: Head tilt and chin lift or jaw- thrust (in case of suspected neck trauma)
- Check breathing: Look to respiratory movement, Listen breathing sound, and feel flow of air by
your -- - - + I Aclivale emergency l8SpOllS9
and monitor until Is pulse definitely felt syslem [If not ahady dona)
emargancy withi, 10 seconds? after 2 mirutas.
l9SJlOll(lels a'l'MI. Conln,e 1811Q18braalhing;
check pulse about_,
No breathing 2 mi-ua If no pulse, begin
or only gasping, IOGll itll Mlllllle.

AED analyzes rhythm.
Shodcable rhythm?
Yes, No,
shockable nonshockable

Give 1 shock. R8Slm8 CPR Resume CPR inmediately for
immediately for about 2 mrutes about 2 minutes (until prompted
('-"llil prompted by AED to allow by AED to allow rhythm check).
rhythm check). Conlnle w1lil Al.S pnwiclers take
ConlnJe until AI..S p,oviders take av« or victim ats to move.
IMl'Of vic:llm.... loimN.

0 2015 American Heart - l i o n

78
 2.ADV ANCED LIFE SUPPORT(ALS):Remember by letters A & B, C, D, E, F.
: Invasive procedures aimed at restoration of ventilation and circulation. These include bag-
valve-mask venti lation, endotracheal intubation, intravenous, introsseous and /or endotracheal
drug administration

A & B: Airway & Breathing:
- Intubate and ventilate with 100% 02, alternatively use Ambubag and mask for ventilation.

C: Circulation:
- Continue cardiac massage same as in BLS.

D: Drugs:
- Intravenous or Intraosseous line for drugs
Drugs used most commonly for ALS.
a) Adrenaline: (0.1 ml/kg of I in 10,000) IV or via ET tube (10 times of IV dose via ET
tube). Dose of adrenaline may be increased ifthere are recurrent subsequent arrests.
b) Bicarbonate 1 mmol/kg of 8.4% IV (dilute in 5% dextrose 1: 1), Should not be given
until ventilation is established.
c) Atropine 0.02 mg/kg (maximum 0.6 mg) IV or via ET tube (used mainly for vagal
induced bradycardia)
d) Other ionotropic agents, antiarrhythmic drugs, DC shock, colloids and crystalloids are
used in special circumstances subsequently.
E: Evaluation:
- Evaluate the success of CPR by clinical examination: When there is spontaneous cardiac output
feel for pulse if pulse& BP good, stop cardiac massage & monitor ECG. Evaluate the success of
CPR further by some essential laboratory investigations.
- Investigations:
- Arterial blood gas, complete blood count, urea, creatinine, glucose,
- Electrolytes, liver functions, chest x-ray, ECG.
F: Further steps & follow up:
Inform family about cardiac arrest & resuscitation.
Proceed for further history, examination and management. Decide about fluid therapy. Look for
urine output. Consider ionotropic support by dopamine and/ or dobutamine 2-20 µgm/ kg/min.
Consider need for further ventilatory management. Maintain body temperature. Find and treat
underlying cause of cardiac arrest. Follow up for neurological impairment.

79
 RESPIRATORY FAILURE
Definition:
Respiratory failure is said to occur when the respiratory system is unable to deliver oxygen to
and/or remove carbon dioxide from pulmonary circulation, there by leading to hypoxemia and/or
hypercapnia.

Classifications:
a) Acute & chronic
b) Type l & type II
Type I: Low arterial PaO2 (hypoxemia) & normal or low PaCO2
Type II: Low arterial PaO2 (hypoxemia) & elevated PaCO2 (hypercapnia)

Clinical Features:
Features due to hypoxemia:
Cyanosis, pallor, restlessness, irritability, tachycardia, increased respiratory efforts evident by:
active alae-nasi; intercostals; subcostal; suprasternal retractions; grunting, etc.
Features due to hypercapnia:
Sweating, tremor, warm extremities, bounding pulses, hypertension, bradycardia, headache,
mental confusion, seizure, coma etc.
Other features: may be related to the underlying cause of respiratory failure.
Diagnosis of respiratory failure is to be confirmed by arterial blood gas estimation.
Etiology of Respiratory Failure: Respiratory failure may result from-
a) Obstructive respiratory diseases:
- Neonates and young infants: Choanal atresia, meconium aspiration, bronchiolitis etc.
- Older infants & children: bronchial asthma, adenotonsillar hypertrophy
Bronchopneumonia, foreign body inhalation, epiglottitis etc.
b) Restrictive respiratory diseases:
- Neonates & young infants: hyaline membrane disease, Pulmonary hypoplasia,
diaphragmatic hernia, congenital lobar emphysema etc.
- Older infants & children:
o Pulmonary: pneumonia, pneumothorax, plural effusion etc.
o Neurological: Depression of respiratory centre from poisoning, injury or raised
intracranial pressure, or weakness of respiratory muscles (poliomyelitis, Guillain-
Barre syndrome, myasthenia gravis, myopathies etc.).
o Mechanical: severe obesity, kyphoscoliosis, chest wall injury etc.
c) Inefficient gas transfer:
- Pulmonary edema, carbon monoxide poisoning, embolism, severe anemia, Right to left
shunt..

80
Approach to Management:
Severest from of respiratory failure may present with cardiopulmonary arrest.
Management in such cases should be according to the guidelines of cardiopulmonary
resuscitation. Most of the respiratory illnesses which presents with respiratory failure come to
the hospital before arrested. Following is a general guideline for their management.
l. Oxygen therapy:
Oxygen may be given by; nasal cannulas, nasal prongs, face mask, or by head box. Many
patient's with Type I respiratory failure will improve with oxygen therapy while proper
treatment for the underlying cause is provided. Oxygen therapy may be guided by pulse
oxyrnetric monitoring. Give enough oxygen to keep SpO2 (02 saturation) around 95%. SpO2 of
less than 90% while patient on high inspired oxygen may indicate the need for more aggressive
steps.

2. Further respiratory support:
If despite of oxygen therapy and adequate treatment of underlying cause the patient continues to
deteriorate, following respiratory supports should be considered:
a) Continuous positive airway pressure (CP AP)
b) Artificiel ventilatory support (traditional artificiel ventilation)
c) High frequency ventilation
d) Extra corporeal membrane oxygenation (ECMO)

3. Investigational therapy: Liquid ventilation, Nitric oxide inhalation.

Artificial ventilatory support:
Present day most of the artificial ventilators deliver air and oxygen to the patients by positive
pressure. Institution of intermittent positive pressure ventilation (IPPV) requires endotracheal
intubation. Size of the endotracheal (ET) tube varies with age of the child.
At birth: 1 kg. birth weight 3.0 mm.
1 - 6 months 3.5 mm.
6 - 12 months 4.0 mm.
12 - 18 months 4.5 mm.

After 2 years use the following formula or select a size comparing the little finger of the patient.

Age in years
ETT Size=-------------------+ 4mm (3mm for cuffed tube)± 0.5mm.
4

Changes ofventilator settings Suggested in Hypoxemia and Hypercapnea:
If the patient is hypoxemic:
I. Increase FiO2 ( Fractional Inspiratory Oxygen or 02%
2. Increase PEEP (Positive End Expiratory Pressure)

81
3. Increase PIP (Peak Inspiratory Pressure), MAP(Mean Airway Pressure), I:E (Inspiratory
Expiratory ratio )
4. Increase Rate of Respiration or Frequency
If patient is hypercapnic:
I. Increase Rate
2. Increase PIP
3. Reduce PEEP and I:E
Every change in ventilator settings is to be followed by blood gases to see the desired effect. One
or two changes should be made at a time. Consider the possible complications of changes of
ventilator setting to the patient.

Complications of artificial ventilation:
A) Respiratory:
- Complications related to intubation: Cardiac arrest during the procedure from vagal
stimulation, injury to nose and mouth, sinusitis, otitis media, subglottic stenosis.
- Barotrauma - pneumothorax, pulmonary interstitial emphysema,
pneumomediastinum
- Complications of oxygen therapy: Retinopathy of prematurity, adult respiratory
distress syndrome, bronchopulmonary dysplasia etc.
8) Circulatory:
- Reduced venous return, reduced cardiac output, systemic hypotension.
- Impaired venous return from high PEEP and high mean airway pressure may increase
venous congestion in the brain causing raise of intracranial pressure and chance of
intracranial hemorrhage.
C) Complications from medications which are used for assisted ventilation

Checklists for a patient who suddenly deteriorates on artificial ventilation:
Remember by the abbreviation DOPED:
I. The tube may be displaced from trachea to the pharynx and esophagus. During bagging air
will go to the stomach which may be heard over epigastrium by the stethoscope, abdomen
will be distended. Remove and replace the tube to the trachea.
2. The tube may be obstructed by thick mucous secretions. You will feel high resistance during
Ambu bagging. Chest wall will not move. Absent breathe sounds on both sides. The
endotracheal tube is to be removed and replaced by another new tube. You can see the mucus
plug in the previous ET tube.
3. Patient may have developed pneumothorax. Breath sounds will be absent or reduced on the
side ofpneumothorax. Percussion note will be hyper-resonant. Bed side transillumination
will be positive in neonates. Patient needs intercostal drainage.
4. l'..quipment failure: Check the ventilatory circuit, a tube might have been accidentally
disconnected. Disconnect the patient from ventilator and ventilate by Ambu-bag and oxygen,
patient will improve. Connect again the disconnected tube
5. The pathological process might have been seriously deteriorated.

82
 Acute Respiratory Distress Syndrome

Definition:
Acute respiratory distress characterized by acute lung injury, noncardiogenic pulmonary edema
and severe hypoxia.
Diagnostic Criteria
I. Identifiable associated condition
2. Acute onset
3. Pulmonary artery wedge pressure < or = to 18mm or absence of evidence of left atrial
hypertension
4. Bilateral infiltrates on chest radiography
5. Pao2/Fio2 ratio < or= to 200
*[Pao2/Fio2 ratio < or = to 300 is defined as Acute Lung Injury]
-American-European Consensus Connference Statement, 1994

Risk Factors~
Pulmonary Extra-pu !woo ao:
Bacterial pneumonia Sepsis
Viral pneumonia Trauma
Aspiration Multiple transfusion
Near Drowning Peritonitis
Inhalation injury Cardiopulmonary bypass

Pathophysiology:
1. Direct lung injury or systemic insult occurs
2. Release of pro-inflammatory agents i.e. TNFa, interleukins
3. Migration of neutrophils producing oxygen radicals and proteases
4. Endothelial and epithelial cell damage leads to increased permeability and the influx offluid into
the alveolar space. (pulmonary ARDS-epithelial damage, extra-pulmonary ARDS-endothelial
damage initially)
5. Surfactant is abnormal
6. Impaired fibrinolysis leads to capillary thrombosis/microinfarction.

To test for severity of Respiratory
Distress ask the patient to speak or
count.

83
 Pathology of ARDS
Exudative Phase Proliferative Phase Fibrotic Phase
(Day 1-7) (Day 7-21) (>Day v21)
Interstitial and intra- Interstitial Collageneous fibrosis
alveolar edema myofibroblast reaction
Hemorrhage Lumenal organizing Microcystic honeycombing
Fibrosis
Leukoagglutination Chronic inflammation Traction bronchiectasis
Necrosis-Type I Parenchymal necrosis Arterial tortuosity
Hyaline membranes Type TI pneumocyte Mural fibrosis
hyperplasia
Platelet-fibrin Obilterative endartitis Medial hypertrophy
thrombi
Macrothrombi
Tomoashefski, J. Acute Respiratory Distress Syndrome. Clinics in Chest medicine: 21 (3) Sept. 2000

Evaluation :
physical exam: tachypnea, tachycardia, altered mental status
blood gas montoring: initial respiratory alkalosis may precede infiltrates, later: alveolar edema ➔
VQ mismatch/shunt ➔ severe hypoxia
lma2io~: CXR progression from diffuse interstitial infiltrates to diffuse, fluffy alveolar spaces; later
reticular pattern suggests interstitial fibrosis. CT demonstrates dependent (posterior if supine)
infiltrates and atelectasis, with anterior hyperinflation.
*most patients with ARDS develop diffuse alveolar infiltrates and progress to respiratory failure
within 48 hours of the onset of symptoms

Treatment:
I. Treatment of underlying cause or associated condition
2. Yentilatory support- ensure "adequate" oxygenation/ventilation while minimizing ventilator
induced lung injury.
Avoid over or under-inflation: Usually this requires PEEP of 6-12, depending on severity.
Remember things tend to get worse before they get better-it is not unusual for patients to require
increasing PEEP as their disease worsens.
Use low tidal volumes, 5-7 cc/kg. Monitor peak pressure (PIP or plateau pressure). It should be
less than 30-35.
Use longer inspiratory times than usual for age.
Tolerate hypercapnia, monitor pH, try to keep >7.2
Tolerate hypoxemia if necessary to keep FiO2 21 mm under 1 year).
Sin V1 greater than 30 mm(> 20 mm under I year).
An increase in the R/S ratio in Vs, V6-
S in VI greater than twice R in Vs.
Left axis deviation for the patient's age (LAD).

Right Ventricular Hypertrophy:
R in Y1 greater than 20 mm (after 1 month).
S in V6 greater than 6 mm (after 1 month).
An increase in the R/S ratio in Y1, Y2.
Upright.T wave in V3R or Y1 after 3 days.
QR pattern in V1, V3 R.
Right axis deviation for the patient's age (RAD).

Combined ventricular hypertrophy:
Large equi phasic QRS complexes in mid - precordial leads V3- V4 greater than 70 mm.
RVH and S in VI or R in V6 greater than mean for age.
LVH and R in VI or S in V6 greater than mean for age.

RVH in Newborn:
I. Pure R wave in VI greater than IO mm.
2. R in VI greater than 25 mm or R in AYR greater than 8 mm
3. QR pattern in V1 (can occur in 10% of normal newborn).
4. Upright Tin V1 after 3 days ofage.
5. RAD greater than + 180 degree.

115
 OBSTRUCTIVE LESION

CARDIAC LESION HEART SOUND MURMURS

Ejection systolic murmur in
Wide splitting of second sound,
the pulmonary area, following
Pulmonary stenosis single second sound in severe
ejection systolic click.
stenosis.

Ejection systolic murmur in
1. Narrow splitting of second
aortic area. It radiates to the
sound (mild}.
neck, may be heard also at
2. Single second sound
Aortic stenosis apex and lower left sternal
(moderate).
edge. It may be preceded by
3. Paradoxical splitting of second
ejection systolic click.
sound (severe stenosis).

Short systolic murmur at left
sternal edge and between
Normal scapulae, occasionally
Coarctation of aorta
murmur of collaterals over the
scapula (continuous).

Occasionally systolic murmur
Hypoplastic left heart Normal or single second sound.
at left sternal edge.
syndrome

Ejection systolic murmur in
Loud second sound (pulmonary the pulmonary area. Early
Pulmonary
component). diastolic murmur in the
hypertension
pulmonary area.

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 VALVULAR LESIONS

CARDIAC LESION HEART SOUND MURMUR

Late systolic murmur at apex. It is
often preceded by a mid systolic
Normal
Mitral valve prolapse click, more prominent with standing
and the Valsalva maneuver.

Wide splitting of the second
Blowing pansystolic murmur at
heart sound occasionally 3rd
Mitral regurg itation apex radiates to left axilla.
heart sound.

Low-pitched mild diastolic rumbling
murmur at apex proceeded by
Mitral stenosis Loud 1st heart sound
opening snap.

High pitched early diastolic,
blowing murmur over left sternal
Aortic regurgitation Normal edge. It is best heard with
expiration.

Normal or wide splitting of the
second sound. Narrow splitting Pansystolic murmur at lower part
Tricuspid
in the presence of the of left sternal edge.
regurgitation
pulmonary hypertension.

Pulmonary Normal or narrowly splitting Early diastolic murmur in the
regurgitation second sound. pulmonary area.

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 HYPERTENSION
Hypertension is defined as an average diastolic or systolic blood pressure exceeding the 95th
percentile for age and sex measured on at least three occasions.

Classification of hypertension by age group
Significant Severe
Age Group
Hypertension (mmHg)
Newborn
IHypertension( mmH g)

7 Days SBPc:96 SBPc:106
8-30 Days SBPc:104 SBPc:110
Infant (< 2 yr) SBPc:112 SBPc:118
DBPc:74 DBPc:82
Children
3 - 5 yr SBPc:116 SBPc:124
DBPc:76 DBPc:84
6 - 9 yr SBPc:122 SBPc:130
DBPc:78 DBPc:86
10-12yr SBPc:126 SBPc:134
DBPc:82 DBPc:90
Adolescent
13-15yr SBPc:136 SBPc:144
--
DBPc:86 DBPc:92
16-18yr SBPc:142 SBPc:150
DBPc:92 DBPc:98
(SBP= Systolic blood pressure -DBP= Diastolic blood pressure)

Causes of hypertension in children and adolescents
Renal Disease
Renal artery stenosis
Cardiovascular
Coarctation of the aorta
Endocrine
Mineralocorticoid excess
Primary hyperaldosteronism
11 B - Hydroxy lase deficiency
17a - Hydroxylase deficiency
Dexamethasone - suppressible hyperaldosteronism
Apparent mineralocorticoid excess
Hyperthyroidism
Pheochromocytoma
Hypercalcemia

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 Tumors
Neurofibromatosis
Neurogenic tumors
Others
Immobilization - induced
Essential hypertension

REFERENCES:

AlbertW. Pruitt, M.D., Welton M. Gersony, MD.Nelson test book of Pediatrics 14th ed.
Philadelphia, W.B. Saunders Co, 1992.
Anderson RH , Macartney FJ , Shirebourne EA: Pediatric Cardiology. Vol.1 and 2 Edinburgh ,
Churchill Livingstone 1987.
John Vann Jones, Roger Black Wood: Outline of cardiology 2nd ed. 1992. Butterwonth
Heinemann Ltd.
Jordan SC, Scott 0 : Heart disease in Pediatric, London Butterworths 1989
Kathleen M. Finta, MD; Stuart Berger, M.D.: Pediatric clinics of North America.Vol. 46 No. 2,
Apr. 1999
Michael D. Freed , M.D.: Nada s Pediatric Cardiology Philadelphia. Hanley and Belfus INC 1992
M.L. Rigby: Current Paediatrics 1994 (4) Long Man Group Ltd. 1994
Mohamed Ali Khan , Saad Al Yousef: Saudi Medical Journal 1988 9 (3)
Mohamed Ali Khan : Saudi Medical Journal 1988, 9 (2)
Myung K. Park, Warren G. Gunthorath: How to Read Pediatric ECG. Second ed. Mosby year
Book Inc. 1987
N. Wilson : Current Paediatrics 1994, 4 Long man Group Ltd. 1994
Park MK: Pediatric Cardiology of practitioners 2nd Chicago, year book medical. Publishers,
1988
Pediatric Physical diagnosis: 1985 Appleton - Century - Crofts
S.C. Jordan : Current Paediatrics 1994, 4 Long Man Group Ltd. 1994
Moss and Adams; Heart Disease in infants, children and adolescents. 5th Edition, 1995
Neonatal Clinical Pharmacology and Therapeutics; Rylance, Harvey and Avanda
Freed MD. Heymann MA. Lewis AB. Roelh SL. Kensey RC. Prostaglandin El in infants with
ductus arteriosus-dependent congenital heart disease. Circulation 1981; 64:899-905
Silove ED. Medical manipulation of the ductus arteriosus. In : Macartney FJ ed. Congenital heart
disease. Current status of clinical cardiology Series. Lancaster, UK: MTP, 1986: 133 -143.

123
8 Respiratory System

HISTORY
Please refer to the chapter dealing with the history taking. In addition give particular
emphasis to the following points:

Cough :
Character: barking, croupy.
Duration: acute or chronic (more than 3 weeks)
Severity: interfers with sleeping, feeding, and speaking.
Painful cough: lesion related to the pleura or ribs (pleurisy, rib fracture)
Timing: more at night, seasonal (asthma)
Dry or productive: dry in pleurisy, productive in pneumonia.
Notice character of sputum:
- Nature: purulent, mucoid, frothy.
- Quantity: scanty or copious.
- Color: blood stained (pneumonia, mitral stenosis), greenish (cystic fibrosis),
yellowish (pneumonia).
- Smell: fetid (lung abscess, cystic fibrosis, bronchiectasis)

Difficulty in breathing
At rest or on exertion (during feeding in infant)

Choking during feed or inability to complete feeds.

Bluish discoloration of the lips (cyanosis)

Presence of abnormal sounds during breathing
Wheezing: may be heard without stethoscope.
Stridor: "Harsh high pitched sound, heard during or at the end of inspiration"
Snoring: "Stridor that occurs at sleep"
Grunting: ''Noise produced at the beginning of expiration by a forceful expiration
against a partially closed glottis"
Rattling: "Rapid succession of short, sharp sounds due to passage of air in pooled
saliva in the throat"

Other important symptoms:
Fever: mention character
Loss of weight: acute or chronic
Presence of loose foul smelling stools. Chronic diarrhea
Known chronic diseases: neuromuscular, cardiopulmonary, immunodeficiency.

124
 Gestational age
History of mechanical ventilation
Family history of atopic disorders.

CLINICAL EXAMINATION
General evaluation : Look for:
General appearance: well or ill looking.
State ofalertness
Color (pallor, cyanosis)
Speech ability (reading Qura'an, counting 1-10 in one breath)
Tachypnea (respiratory rate > expected for age)
Gnmting
Active ala-Nazi
Audible wheezes
Stridor
Snoring
Built and nutrition
Note the presence of: Oxygen supply and delivery systems (nebulizer apparatus, spacer devices,
and inhaler devices) sputum pot.

Examination of upper limbs: Check for:
Clubbing: increased rounded appearance of the nails with obliteration of the angle between the
nail and its soft tissue base, or a positive Scrarnroth's sign (obliteration of the diamond shaped
space when the nail beds of two corresponding fingers of both hands meet together).
Peripheral cyanosis.
Pulse: count and note the character (bounding pulse - CO2 retention) "count apex beat in children
below the age of 3 years".
Blood pressure: Pulsus paradoxus (> 10 mm Hg fall of systolic blood pressure during
inspiration) e.g. severe asthma, constrictive pericarditis.

Examination of the face: Check for:
Lips: peripheral cyanosis
Tongue: central cyanosis
Ala-Nazi: active or not

Examination of the Ear, Nose and Throat:
Keep it for the last, but remember to do it. Explain to the patient or use proper restrain as
indicated.

125
 Throat:
- Use a good source of light and a strong wooden spatula.
- Don't miss a spontaneous gag to have a clear view of the throat.
- Don't over-interpret tonsillar enlargement in a gagging child.

Ears:
- Use proper size speculum.
- Gently pull the auricle upward, backward and laterally to make the external
auditory canal straight to have a better view of the tympanic membrane. Note:
presence of wax or foreign body.
- Examine the tympanic membrane for: light reflex, color (remember the ear drum
may appear reddish in a crying child), bulging or retracted. perforation, discharge
and mobility (by a pneumatic device in the otoscope)

Nose:
- Use large size speculum and the usual otoscope (if indicated)
- Look for:
Foreign body
Foul smell
Bleed
Color of the nasal mucosa.
- Presence of discharge and its character
- Turbinate hypertrophy
- Polyps
- Edema of the nasal mucosa (allergy)

Examination of the chest:
Examine both front and back of the chest. Proceed to the back after completion of the
examination of the front.
Inspection:
- Respiratory rate (minimum 30 seconds)
- Expose the chest fully and look for:
Type of breathing:
o Abdominal in infants.
o Thoracic after 4 - 5 years of age
o Flat abdomen with reduced movements indicates diaphragmatic hernia
Use of accessory muscles: suprastemal, intercostal and subcostal retractions.
Apex pulsation
Scars, describe its type
Shape of the chest:
o Pectus Excavatum (funnel shaped chest)
o Pectus Carinatum (pigeon shaped)
o Barrel shaped (increased antero-posterior diameter)
126
o Harrison Sulcus (indrowing of the lower chest with rib flaring)
o Chest wall asymmetry and unequal chest movement (should be observed from the
foot end of the bed, with keeping your eye in the same level of chest wall)
o Shield-shaped chest: Turner's syndrome
o Flattening of the hemi-chest, absence ofpectoralis muscle i.e., Poland anomaly
o Others:
Rachitic rosary
Absent clavicle in cleidocranial dysplasia
Supernumerary nipple in renal anomaly
Palpation:
Proceed gently with warm hands.
Note:
o Obvious swelling and tenderness
o Position of trachea: by comparing the gap between the sternal head of the
stemomastoid and tracheal margin by your index finger. Normally trachea is
slightly deviated to the right. In young children this is not a reliable sign to
detect mediastinal shift
o Position of the apex beat. Remember dextrocardia
o Tactile vocal fremitus: (in older children) place the palm of the hand on either
side of the upper chest and ask the child to say ninety-nine. Feel the difference
between sides rather than absolute increase or decrease.
o Chest expansion: (in older children) hook little fingers of both hands in the
axillae with thumbs meeting in the mid-line. Ask the child to take a deep
breath and observe which thumb moves the least.
Percussion:
- Perform very gently
- Explain to the older patients and the attendants
- Use:
1. Pleximeter finger: placed in an intercostal space flush with the chest wall,
other fingers kept away from touching the chest wall.
ii. Percussing finger (plexor): middle finger of the dominant hand. Finger should
pivot at wrist and not at the elbow, with a gentle blow hitting perpendicularly
to pleximeter finger.
Percuss at: (corresponding points) from up to down.
Mid-clavicular lines, and
mid-axillary lines
Note:
o apices: percuss on the clavicle directly
o Area of the liver dullness
o Area of cardiac dullness
o Character of resonance: (normal, increased, reduced, absent, stony dullness)

127
 - - ·-..!I.

Auscultation.
Use a child size stethoscope
Be sure that the chest piece is adequately warm
Use either the bell or the diaphragm (practice the use of any one).
Apply the chest piece firmly to the chest wall to avoid rubbing noises and escape ofbreath
sounds
Auscultate the corresponding points in both sides:

Front

1. Character of air entry:
- Normal - Reduced
- Equality on both sides
2. Character of breath sounds:
I

Vesicular with prolonged expiration + rhonchi

Character of inspiratory and expiratory phase note whether:
- Inspiration prolonged.
- Expiration prolonged.
3. Presence of added sounds:
- Wheezes: continuous, uninterrupted, musical sound
Inspiratory: example: croup
Expiratory: example: asthma
- Crackle: discontinuous, interrupted sounds like popping of bubble which may
be:
Course: i.e., friction rub (rubbing leathery sound)
Medium
Fine crepitations may also be:
- Early inspiratory i.e., in obstructive airway disease
- Late inspiratory i.e., in restrictive airway disease
4. Vo