Diseases of Infancy

About This Presentation

Title:

Diseases of Infancy

Description:

Diseases of Infancy & Childhood * Figure 10-25 Congenital capillary hemangioma at birth (A) and at age 2 years (B) after spontaneous regression. – PowerPoint PPT presentation

Number of Views:433

Avg rating:3.0/5.0

Slides: 106

Provided by: medicalsch

Category:

more less

Transcript and Presenter's Notes

Title: Diseases of Infancy

1
Diseases of Infancy Childhood
2
Diseases of Infancyand Childhood

Congenital Anomalies
Birth Weight and Gestational Age
Birth Injuries
Perinatal Infections
Respiratory Distress Syndrome (RDS)
Necrotizing Enterocolitis
Intraventricular Hemorrhage
Hydrops
Inborn Metabolic/Genetic Errors
Sudden Infant Death Syndrome (SIDS)
Tumors

3
INFANT MORTALITY

USA 1970 20
USA 2000 7
USA WHITE X
USA BLACK 2X
SWEDEN 3
INDIA 82

4
Major Time Spans

Neonatal period
first four weeks of life
Infancy
the first year of life
Age 1 4 years (preschool)
Age 5 14 years (school age)

5
MORTALITY by TIME SPAN

NEONATE (0-4 WEEKS) CONGENITAL, PREMATURITY
UNDER ONE YEAR CONGENITAL, PREMATURITY/WEIGHT,
SIDS
1-4 YEARS ACCIDENTS, CONGENITAL, TUMORS
5-14 YEARS ACCIDENTS, TUMORS, HOMICIDES
15-24 YEARS ACCIDENTS, HOMICIDE, SUICIDE (NONE
ARE NATURAL CAUSES)

6
1Rates are expressed per 100,000 population
2Excludes congenital heart disease
7
Congenital Anomalies

Definitions
Causes
Pathogenesis

Malformations
primary errors of morphogenesis, usually
multifactorial
e.g. congenital heart defect
Disruptions
secondary disruptions of previously normal organ
or body region
e.g. amniotic bands
Deformations
extrinsic disturbance of development by
biomechanical forces
e.g. uterine constraint
Sequence
a pattern of cascade anomalies explained by a
single localized initiating event with secondary
defects in other organs
e.g. Oligohydramnios (Or Potter) Sequence
Syndrome
a constellation of developmental abnormalities
believed to be pathologically related
e.g Turner syndrome

9
Malformations
Polydactyly syndactyly
Cleft Lip
Severe Lethal Malformation
10
Disruption by an amniotic band
11
Oligohydramnios (Or Potter) Sequence

Oligohydramnios (decreased amniotic fluid)
Renal agenesis
Amniotic leak
Fetal Compression
flattened facies
club foot (talipes equinovarus)
Pulmonary hypoplasia
fetal respiratory motions important for lung
development
Breech Presentation

12
The Oligohydramnios Sequence
13
Infant with oligohydramnios sequence
14
Organ Specific Anomalies

Agenesis complete absence of an organ
Atresia absence of an opening
Hypoplasia incomplete development or under-
development of an organ with decreased numbers of
cells
Hyperplasia overdevelopment of an organ
associated with increased numbers of cells
Hypertrophy increase in size with no change in
number of cells
Dysplasia in the context of malformations
(versus neoplasia) describes an abnormal
organization of cells

15
Implantation and the Survival of Early Pregnancy

Only 50-60 of all conceptions advance beyond 20
weeks
Implantation occurs at day 6-7
75 of loses are implantation failures and are
not recognized
Pregnancy loss after implantation is 25-40

NEJM 2001 3451400-1408
16
(No Transcript)
17
1
2
3
18
CAUSES OF ANOMALIES

Genetic
karyotypic aberrations
single gene mutations
Environmental
infection
maternal disease
drugs and chemicals
irradiation
Multifactorial
Unknown

19
(No Transcript)
20
Embryonic Development

Embryonic period
weeks 1- 8 of pregnancy
organogenesis occurs in this period
Fetal period
weeks 9 to 38
marked by further growth and maturation

21
Critical Periods Of Development
22
Genetic Causes

Karyotypic abnormalities
80-90 of fetuses with aneuploidy die in utero
trisomy 21 (Down syndrome) most common karyotypic
abnormality (21,18,13)
sex chromosome abnormalities next most common
(Turner and Klinefelter)
autosomal chromosomal deletion usually lethal
karyotyping frequently done with aborted fetuses
with repeated abortions
Single gene mutations
covered in separate chapters

23
Maternal Viral Infection

Rubella (German measles) 1st TRIMESTER
at risk period first 16 weeks gestation
defects in lens (cataracts), heart, and CNS
(deafness and mental retardation)
rubella immune status important part of prenatal
workup
Cytomegalovirus 2nd TRIMESTER
most common fetal infection
highest at risk period is second trimester
central nervous system infection predominates

24
Drugs and Chemicals

Drugs
13 cis-retinoic acid (acne agent)
warfarin
angiotensin converting enzyme inhibitors (ACEI)
anticonvulsants
oral diabetic agents
thalidomide
Alcohol
Tobacco

25
Teratogen Actions

Proper cell migration to predetermined
locations that influence the development of other
structures
Cell proliferation, which determines the size
and form of embryonic organs
Cellular interactions among tissues derived
from different structures (e.g., ectoderm,
mesoderm), which affect the differentiation of
one or both of these tissues
Cell-matrix associations, which affect growth
and differentiation
Programmed cell death (apoptosis), which, as we
have seen, allows orderly organization of tissues
and organs during embryogenesis
Hormonal influences and mechanical forces,
which affect morphogenesis at many levels

26
Diabetes Mellitus

Fetal Macrosomy (gt10 pounds)
maternal hyperglycemia increases insulin
secretion by fetal pancreas, insulin acts with
growth hormone effects
Diabetic Embryopathy
most crucial period is immediately post
fertilization
malformations increased 4-10 fold with
uncontrolled diabetes, involving heart and CNS
Oral agents not approved in pregnancy
Diabetics attempting to conceive should be placed
on insulin

27
Birth Weight and Gestational Age

Appropriate for gestational age (AGA)
between 10 and 90th percentile for gestational
age
Small for gestational age (SGA) , lt10
Large for gestational age (LGA) , gt90
Preterm
born before 37 weeks (lt2500 grams)
Post-Term
delivered after 42 weeks

28
Prematurity

Defined as gestational age lt 37 weeks
Second most common cause of neonatal mortality
(after congenital anomalies)
Risk factors for prematurity
Preterm Premature Rupture Of fetal Membranes
(PROM)
Intrauterine infection
Uterine, cervical, and placental abnormalities
Multiple gestation

29
Fetal Growth Restriction

At least 1/3 of infants born at term are lt 2.5kg
Undergrown rather than immature
Commonly underlies SGA (small for gestational
age)
Prenatal diagnosis ultrasound measurements
Classification
Fetal
Placental
Maternal

30
Fetal FGR

Chromosomal abnormalities
17 of FGR overall
up to 66 of fetuses with ultrasound
malformations
Fetal Infection
Infection TORCH (Toxoplasmosis, Other, Rubella,
Cytomegalovirus, Herpes)
Characterized by symmetric growth restriction
head and trunk proportionally involved

31
Placental FGR

Vascular
umbilical cord anomalies (single artery,
constrictions, etc)
thrombosis and infarction
multiple gestation
Confined placental mosaicism
mutation in trophoblast
trisomy is common
Placental FGR tends to cause asymmetric growth
with relative sparing of the head

32
Maternal FGR

Most common cause of FGR by far
Vascular diseases
preeclampsia (toxemia of pregnancy)
hypertension
Toxins
ethanol
narcotics and cocaine
heavy smoking

33
Organ Immaturity

Lungs
alveoli differentiate in 7th month
surfactant deficiency
Kidneys
glomerular differentiation is incomplete
Brain
impaired homeostasis of temperature
vasomotor control unstable
Liver
inability to conjugate and excrete bilirubin

34
APGAR (Appearance, Pulse, Grimace, Activity,
Respiration)
35
Apgar Score and 28 Day Mortality

Score may be evaluated at 1 and 5 minutes
5 minute scores
0-1, 50 mortality
4, 20 mortality
7, nearly 0 mortality

36
Perinatal Infection

Transcervical (ascending)
inhalation of infected amniotic fluid
pneumonia, sepsis, meningitis
commonly occurs with PROM
passage through infected birth canal
herpes virus caesarian section for active herpes
Transplacental (hematogenous)
mostly viral and parasitic
HIVat delivery with maternal to fetal
transfusion
TORCH-Toxo, Other, Rubella, Cmv, Herpes
parvovirus B19 (Fifth), erythema infectiosum
bacterial
Listeria monocytogenes

37
Fetal Lung Maturation
38
Neonatal Respiratory Distress Syndrome (RDS)

60,000 cases / year in USA with 5000 deaths
Incidence is inversely proportional to
gestational age
The cause is lung immaturity with decreased
alveolar surfactant
surfactant decreases surface tension
first breath is the hardest since lungs must be
expanded
without surfactant, lungs collapse with each
breath

39
RDS Risk Factors

1) Prematurity
by far the greatest risk factor
affected infants are nearly always premature
2) Maternal diabetes mellitus
insulin suppresses surfactant secretion
3) Cesarean delivery
normal delivery process stimulates surfactant
secretion

40
RDS Pathology

Gross
solid and airless (no crepitance)
sink in water
appearance is similar to liver tissue
Microscopic
atelectasis and dilation of alveoli
hyaline membranes composed of fibrin and cell
debris line alveoli (HMD former name)
minimal inflammation

41
(No Transcript)
42
(No Transcript)
43
V/Q Mismatch
44
RDS Prevention and Treatment

Delay labor until fetal lung is mature
amniotic fluid phospholipid levels are useful in
assessing fetal lung maturity
Induce fetal lung maturation with antenatal
corticosteriods
Postnatal surfactant replacement therapy with
oxygen and ventilator support

45
Treatment Complications

Oxygen toxicity
oxygen derived free radicals damage tissue
Retrolental fibroplasia
hypoxia causes ? Vascular Endothelial Growth
Factor (VEGF) and angiogenesis
Oxygen Rx suppresses VEGF and causes endothelial
apoptosis
Bronchopulmonary dysplasia
oxygen suppresses lung septation at the saccular
stage
mechanical ventilation
epithelial hyperplasia, squamous metaplasia, and
peribronchial and interstitial fibrosis were seen
with old regimens of ventilator usage and no
surfactant use, but are now uncommon
lung septation is still impaired

46
Necrotizing Enterocolitis

Incidence is directly proportional to
prematurity, like RDS
approaches 10 with severe prematurity
2000 cases yearly in USA
Pathogenesis
not fully understood
intestinal ischemia
inflammatory mediators
breakdown of mucosal barrier

47
Necrotizing Enterocolitis
48
Hydrops Fetalis

Chromosomal abnormalities
Turner syndrome with cystic hygromas
other
Cardiovascular with heart failure
anemia with high output failure
immune hemolytic anemia
hereditary hemolytic anemia (a-thalassemia)
parvovirus B19 infection
twin to twin in utero transfusion
congenital heart defects

49
Hydrops Fetalis
50
Immune Hydrops

Fetus inherits red cell antigens from the father
that are foreign to the mother
Mother forms IgG antibodies which cross the
placenta and destroy fetal RBCs
Fetus develops severe anemia with CHF and
compensatory ? hematopoiesis (frequently
extramedullary)
Most cases involve Rh D antigen
mother is Rh Neg and fetus is Rh Pos
ABO and other antigens involved less often

51
Pathogenesis of Sensitization

Fetal RBCs gain access to maternal circulation
largely at delivery or upon abortion
Since IgM antibodies are involved in primary
response and prior sensitization is necessary,
the first pregnancy is not usually affected
Maternal sensitization can be prevented in most
cases with Rh immune globulin (Rhogam) given at
time of delivery or abortion (spontaneous or
induced)

52
Treatment of Immune Hydrops

In utero
identification of at risk infants via blood
typing by amniocentesis, (Chorionic Villi
Sampling) CVS, or fetal blood sampling
fetal transfusions via umbilical cord
early delivery
Live born infant
monitoring of hemoglobin and bilirubin
exchange transfusions

53
(No Transcript)
54
Kernicterus
55
Pathogenesis of Immune Hydrops
56
Inborn Errors of Metabolism(Genetic)

PhenylKetonUria (PKU)
Galactosemia
Cystic Fibrosis (CF) (Mucoviscidosis)

57
PHENYLKETONURIA (PKU)

Ethnic distribution
common in persons of Scandinavian descent
uncommon in persons of African-American and
Jewish descent
Autosomal recessive
Phenylalanine hydroxylase deficiency leads to
hyperphenylalaninemia, brain damage, and mental
retardation
Phenylananine metabolites are excreted in the
urine
Treatment is phenylalanine restriction
Variant forms exist

58
GALACTOSEMIA

Autosomal recessive
Lactose ? glucose galactose
Galactose-1-phosphate uridyl transferase (GALT)
GALT is involved in the first step in the
transformation of galactose to glucose
absence of GALT activity ? galactosemia
Symptoms appear with milk ingestion
liver (fatty change and fibrosis), lens of eye
(cataracts), and brain damage involved (mechanism
unknown)
Diagnosis suggested by reducing sugar in urine
and confirmed by GALT assay in tissue
Treatment is removal of galactose from diet for
at least the two first years of life

59
Cystic Fibrosis

Normal Gene
Mutational Spectra
Genetic/Environmental Modifiers
Morphology
Clinical Course

60
Cystic Fibrosis (Mucoviscidosis)

Autosomal recessive
Most common lethal genetic disease affecting
Caucasians (1 in 3,200 live births in the USA)
2-4 of population are carriers
Uncommon in Asians and African-Americans
Widespread disorder in epithelial chloride
transport CFTR affecting fluid secretion in
exocrine glands, (SWEAT)
epithelial lining of the respiratory,
gastrointestinal, and reproductive tracts
Abnormally viscid mucus secretions

61
Cellular Metabolism Of The Cystic Fibrosis
Transmembrane Regulator (CFTR)
Harrisons Internal Med, 16th Ed
62
CFTR Gene Normal

Cystic Fibrosis Transmembrane Conductance
Regulator (CFTR)
CTFR ? epithelial chloride channel protein
agonist induced regulation of the chloride
channel
interacts with epithelial sodium channels (ENaC)
Sweat gland
CTFR activation increases luminal Cl- resorption
ENaC increases Na resorption
sweat is hypotonic
Respiratory and Intestinal epithelium
CTFR activation increases active luminal
secretion of chloride
ENaC is inhibited

63
CFTR Gene Cystic Fibrosis

Sweat gland
CTFR absence decreases luminal Cl- resorption
ENaC decreases Na resorption
sweat is hypertonic
Respiratory and Intestinal epithelium
CTFR absence decreases active luminal secretion
of chloride
lack of inhibition of ENaC is opens sodium
channel with active resorption of luminal sodium
secretions are decreased but isotonic

64
Chloride Channel Defect and Effects
65
CFTR Gene Mutational Spectra

More than 800 mutations are known
These are grouped into six classes
mild to severe
Phenotype is correlated with the combination of
these alleles
correlation is best for pancreatic disease
genotype-phenotype correlations are less
consistent with pulmonary disease
Other genes and environment further modify
expression of CFTR

66
Clinical Manifestations Of Mutations In The
Cystic Fibrosis Gene
67
Organ Pathology

Plugging of ducts with viscous mucus and loss of
ciliary function of respiratory mucosa
Pancreas
atrophy of exocrine pancreas with fibrosis
islets are not affected
Liver
plugging of bile canaliculi with portal
inflamation
biliary cirrhosis may develop
Genitalia
Absence of vas deferens and azoospermia
Sweat glands
normal histology

68
(No Transcript)
69
(No Transcript)
70
Lung Pathology in CF

More than 95 of CF patients die of complications
resulting from lung infection
Viscous bronchial mucus with obstruction and
secondary infection
S. aureus
Pseudomonas
Hemophilus
Bronchiectasis
dilatation of bronchial lumina
scarring of bronchial wall

71
(No Transcript)
72
Cystic Fibrosis Clinical Manifestations
73
CF Diagnosis

Clinical criteria
sinopulmonary
gastrointestinal
pancreatic
intestinal
salt loss
male genital tract
Sweat chloride analysis
Nasal transepithelial potential difference
DNA Analysis
gene sequencing

74
Clinical Course and Treatment

Highly variable median life expectance is 30
years
7 of patients in the United States are diagnosed
as adults
Clearing of pulmonary secretions and treatment of
pulmonary infection
Transplantation
lung
liver-pancreas

75
Sudden Infant Death Syndrome (SIDS)

Epidemiology
Morphology
Pathogenesis

76
Sudden Infant Death Syndrome

NIH Definition
sudden death of an infant under 1 year of age
which remains unexplained after a thorough case
investigation, including performance of a
complete autopsy, examination of the death scene,
and review of the clinical history
Crib death
another name based on the fact that most die in
their sleep

77
Epidemology of SIDS

Leading cause of death in USA of infants between
1 month and 1 year of age
90 of deaths occur 6 months age, mostly
between 2 and 4 months
In USA 2,600 deaths in 1999 (down from 5,000 in
1990)

78
Risk Factors for SIDS

Parental
Young maternal age (age lt20 years)
Maternal smoking during pregnancy
Drug abuse in either parent, specifically
paternal marijuana and maternal opiate, cocaine
use
Short intergestational intervals
Late or no prenatal care
Low socioeconomic group
African American and American Indian ethnicity (?
socioeconomic factors)
Infant
Brain stem abnormalities, associated defective
arousal, and cardiorespiratory control
Prematurity and/or low birth weight
Male sex
Product of a multiple birth
SIDS in a prior sibling
Antecedent respiratory infections
Environment
Prone sleep position
Sleeping on a soft surface
Hyperthermia

79
Morphology of SIDS

SIDS is a diagnosis of exclusion
Non-specific autopsy findings
Multiple petechiae
Pulmonary congestion pulmonary edema
These may simply be agonal changes as they are
found in non-SIDS deaths also
Subtle changes in brain stem neurons
Autopsy typically reveals no clear cause of death

80
Pathogenesis of SIDS

Generally accepted to be multifactorial
Triple risk model
Vulnerable infant
Critical development period in homeostatic
control
Exogenous stressors
Brain stem abnormalities, associated defective
arousal, and cardio-respiratory control

81
Prevention of SIDS

Maternal factors
attention to risk factors previously mentioned
redress problems in medical care for
underprivileged
Environmental
avoid prone sleeping
back to sleep program infant should sleep in
supine position
Avoid sleeping on soft surfaces
no pillows, comforters, quilts, sheepskins, and
stuffed toys
Sleeping clothing (such as a sleep sack) may be
used in place of blankets.
Avoid hyperthermia
no excessive blankets
set thermostat to appropriate temperature
avoid space heaters

82
Diagnosis of SIDS

SIDS is a diagnosis of exclusion
Complete autopsy
Examination of the death scene
Review of the clinical history
Differential diagnosis
child abuse
intentional suffocation

83
TUMORS

Benign
Malignant

84
BENIGN

Hemangiomas
Lymphatic Tumors
Fibrous Tumors
Teratomas (also can be malignant)

85
Hemangioma

Benign tumor of blood vessels
Are the most common tumor of infancy
Usually on skin, especially face and scalp
Regress spontaneously in many cases

86
Congenital Capillary Hemangioma
At 2 years After spontaneous regression
At birth
87
Teratomas

Composed of cells derived from more than one germ
layer, usually all three
Sacrococcygeal teratomas
most common childhood teratoma
frequency 120,000 to 140,000 live births
4 times more common in boys than girls
Aproximately 12 are malignant
often composed of immature tissue
occur in older children

88
Sacrococcygeal Teratoma
89
MALIGNANT

Neuroblastic Tumors
Wilms Tumor
Incidence and Types

90
(No Transcript)
91
Small Round Blue Cell Tumors

Frequent in pediatric tumors
Differential diagnosis
Lymphoma
Neuroblastoma
Wilms tumor
Rhabdomyosarcoma
Ewings tumor
Diagnostic procedures
immunoperoxidase stains
electron microscopy
chromosomal analysis and molecular markers

92
Neuroblastomas

Second most common malignancy of childhood (650
cases / year in USA)
Neural crest origin
adrenal gland, medulla, like a pheo 40
sympathetic ganglia 60
In contrast to retinoblastoma, most are sporadic
but familiar forms do occur
Median age at diagnosis is 22 months

93
Neuorblastoma Morphology

Small round blue cell tumor
neuorpil formation
rosette formation
immunochemistry neuron specific enolase
EM secretory granules (catecholamine)
Usual features of anaplasia
high mitotic rate is unfavorable
evidence of Schwann cell or ganglion
differentiation favorable
Other prognostic predictors are used by
pathologists and oncologists

94
Neuorblastoma

Neuropil Homer-Wright Rosettes
95
(No Transcript)
96
(No Transcript)
97
Clinical Course and Prognosis

Hematogenous and lymphatic metastases to liver,
lungs and bone
90 produce catecholamines, but hypertension is
uncommon
Age and stage are most important prognostically
lt 1 year age good prognosis regardless of stage
Amplification of N-myc oncogene
present in 25-30 of cases and is unfavorable
up to 300 copies on N-myc has been observed
Risk Stratification
low risk 90 cure rate
high risk 20 cure rate

98
Wilms Tumor

Most common primary renal tumor of childhood
Incidence 10 per million children lt 15 years
Usually diagnosed between age 2-5
5 10 are multi-focal, i.e., bilateral
synchronous
metachronous

99
Clinical Features

Most children present with a large abdominal mass
Treatment
nephrectomy and combination chemotherapy
two year survival up to 90 even with spread
beyond the kidney

100
Pathogenesis of Wilms Tumor

10 of Wilms tumors arise in one of three
congenital malformation syndromes with distinct
chromosomal loci
Familial disposition for Wilms is rare, and most
of these patients have de novo mutations
Nephrogenic rests of adjacent parenchyma
present in 40 of unilateral tumors, 100 of
bilateral tumors
if found in one kidney, these rests predict an
increased risk for tumor in the contralateral
kidney

101
Pathology of Wilms Tumor