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Approach to
a child with dysmorphism
Dr. Syeda Ismat Bukhari
Introduction
 The term dysmorphic is derived from the Greek words “dys”
(disordered, abnormal, painful) and “morph” (shape, form).
 Dysmorphology is a discipline of clinical genetics that studies and
attempts to interpret the patterns of human growth and structural
defects.
Dysmorphism Vs Syndrome
 The child with dysmorphic signs often does not have a major
malformation, and he or she may simply have an appearance that is
unusual compared with the general population and out of keeping
with that of unaffected close relatives.
 A syndrome is simply a recognizable pattern of dysmorphic signs that
have a common cause.
Understand the difference
 Major malformation
with medical +/- social implications
often require surgical repair
 Minor malformation
are of cosmetic significance sometimes
 Normal variants
Incidence
 Major congenital anomalies
At birth  2 – 3 %
At 5 yrs  4 – 6 %
 Minor congenital anomalies
At birth  15 %
The importance of recognizing minor anomalies
 Minor anomalies are often
indicators for relevant major
anomalies.
Causes of malformations
Cause Percent incidence
Genetic
Chromosome
Single gene
15 – 25
10 – 15
2 – 10
Multifactorial 20 – 25
Environmental
Maternal diseases
Uterine / Plazental
Drug / Chemicals
8 – 12
6 – 8
2 – 3
0.5 – 1
Twinning 0.5 – 1
Unknown 40 – 60
History of intrauterine development
Periods of malformation
Clinical approach
History
 Antenatal history
 Problems with infertility (medications [clomid]
 techniques [IVF - invitro fertilization, PGD - preimplantation genetic
diagnosis, ICSI - intracytoplasmic sperm injection])
 Fetal Movement (active, decreased)
 Exposures (medications, tobacco, alcohol, drugs, chemicals)
 Illnesses (fevers, exposures to infections)
 Problems (bleeding, pre-term labor, abnormal prenatal testing or
ultrasound)
 Birth history
 Presentation: breech/cephalic/oblique
 Delivery: vaginal, c-section (why?)
 Neonatal course (complications/problems and days hospitalized)
History
 Neonatal status
 APGAR
 Anthopometric measurements
 Resuscitation
 Newborn course
 Feeding
 Activity
 Obvious deformities
 Complications / issues
History
 Past Medical History
 Illnesses, hospitalizations, surgeries, immunizations, medications,
allergies
 A detailed review of systems.
 Developmental History
 Address parental concerns.
 Determine ages for milestones (gross motor, fine motor,
personal/social, language).
 Determine current milestones (appropriate for age?).
Family history
 Take a detailed, three-generation family history
Family history
Ask for:
 Birth defects
 Other genetic diseases
 Multiple miscarriages
 Parental ages and health status
 Consanguinity and geographic origin
Physical examination
 Growth monitoring
 Measurements of the child's weight, length, and head
circumference should be plotted on the standardized
growth charts.
 General appearance
 Body shape and size etc.
Physical examination
Investigations
 Cytogenetics is a mainstay of diagnosis in dysmorphology.
 However, chromosome studies are labour intensive and relatively
expensive.
 To be visible, a chromosome deletion or duplication probably
involves at least 3–4 kilobases of DNA10 (perhaps 15–30 genes,
depending upon the location and the chromosome).
Fluorescence in situ hybridization (FISH)
 Prader-Willi syndrome
 Angelman syndrome
 Smith-Magenis syndrome
 Miller-Dieker syndrome
 Velo-cardio-facial syndrome
 DiGeorge syndrome
Whole chromosome painting (WCP)
 WCP is very useful for identifying the origin of additional
chromosome material that is microscopically visible but not
distinctive enough to be assigned to a specific chromosome.
 It can also be used to search for light microscopically invisible
(cryptic) translocations where suspicion of a chromosome
abnormality remains, despite a normal standard karyotype.
 The exchange of similarly sized and banded material between 2
chromosomes, which is not visible in a standard study, becomes
visible because of the exchange of different colours.
Other investigations
 Molecular (DNA) diagnostics
 Biochemical lab testing (to rule out any inborn error of metabolism,
storage diseases etc.)
The major problems of morphogenesis
Disruptions
 Morphological alterations of structures after formation
 Has low recurrence risk
Causes of disruption
 Ionization (x-ray, radioactive substance exposure)
 Hyperthermia
 Infections
 Teratogenic
 Metabolic
 Vascular disruption
 Amnion rupture sequence
Deformations
 Due to mechanical forces that mold a
part of fetus over a prolonged time
period
 The musculoskeletal system may be
involved, but may also be reversible
post-natally
Breech presentation
Risks for fetal constraint
 Maternal risk factors
 Primigravida
 Small uterus
 Uterine malformation
 Uterine fibromata
 Small maternal pelvis
 Fetal risk factors
 Oligohydroamnios
 Large fetus
 Multiple gestation
Deformations related to breech presentation
Malformations
Disorders of lymphatic drainage
Cleft palate
Telecantus, hyper-/hypo-telorsim
Ear defects
Chin
Digit anomalies
Non-disjunction syndromes
Down syndrome (trisomy 21)
 Low set ears
 Hypotonia
 Simian crease
 Wide space between first and
second toe
 Flat face
Patau syndrome (trisomy 13)
 Holoprosencephaly
 Cutis aplasia
 Microcephaly
 Microphthalmia
 Cleft lip +/- palate
 Polydactyly
 Congenital heart defect
Edwards syndrome (trisomy 18)
 Weak cry
 Polyhydroamnios
 Growth deficiency
 Low-set, malformed
auricles
 Clenched hand with
overlapping fingers
 Rocker bottom feet
 Congenital heart defect
Klinefelter syndrome (47xxy)
 Tall stature
 Behavioral issues
 Post-pubertal
hypogonadism
Turner syndrome (45x)
Not diagnosed until 5-6
yrs
 Webbed neck
 Shield chest
 Cubitus vulgaris
 Low hairline
 Short stature
 Renal anomalies
 Cardiac anomalies
(bicuspid aortic valve
and coarctation of
aorta)
Microdeleteions
Wolf hirshorn (4p)
 Hypertelorism
 Broad nasal bridge
 Cleft lip +/- palate
 Down turned mouth
 Severe mental retardation
Cri-du-chat (5p)
 Microcephaly
 Growth retardation
 High-pitched cat-like cry
 Congenital heart disease
 Hypotonia
Contiguous gene
syndrome
Prader-willi syndrome (15q11)
 Obesity
 Hypotonia
 Small hands and feet
 Upward slanting
palpebral fissures
 IQ : 60 – 70
 Micro-penis /
cryptorchidism
Angelman syndrome (15q11)
 Mental retardation
 Puppet like gait
 Paroxysms of inappropriate laughter
 Absent / limited speech
 Seizures
22q11 deletion syndromes
(Di-George, Velocardial-facial, Sprintzen)
 Micrognathia
 Low set ears
 Short palpebral fissures
 Blunted nose
 High-arched palate
 Cleft palate +/- bifid uvula
Autosomal dominant syndromes
Achondroplasia (FGFR3)
 Rhizomelic shortening of
limbs
 Short fingers held in trident
configuration
 Elarged head with depressed
nasal bridge
Neurofibromatosis
 > 6 café-au-lait spots
 >2 neurofibromas
 Lisch nodules (iris hematoma)
 Optic gliomas
 Angiofibromas
 Axillary or inguinal freckling
Osteogenesis imperfecta
 Fractures
 Osteopenia
 Blue sclera
 Hearing loss
 Short stature
 Four types
Autosomal recessive
Cystic fibrosis
Tay-Sacs disease
Sickle cell anemia
Teratogens
Fetal alcohol syndrome
Quiz
What are the most appropriate genetic condition
associated with the following physical findings?
 Webbed neck
 Macrosomia
 Rhizometric shortening
 Small hands
 Café-au-lait spots
What are the most appropriate genetic condition
associated with the following physical findings?
 Upward slanting palpebral fissures
 Downward slanting palpebral fissures
 Lich nodules
 Kayser-fleischer ring
Thank you

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Approach to a child with dysmorphism

  • 1. Approach to a child with dysmorphism Dr. Syeda Ismat Bukhari
  • 2. Introduction  The term dysmorphic is derived from the Greek words “dys” (disordered, abnormal, painful) and “morph” (shape, form).  Dysmorphology is a discipline of clinical genetics that studies and attempts to interpret the patterns of human growth and structural defects.
  • 3. Dysmorphism Vs Syndrome  The child with dysmorphic signs often does not have a major malformation, and he or she may simply have an appearance that is unusual compared with the general population and out of keeping with that of unaffected close relatives.  A syndrome is simply a recognizable pattern of dysmorphic signs that have a common cause.
  • 4. Understand the difference  Major malformation with medical +/- social implications often require surgical repair  Minor malformation are of cosmetic significance sometimes  Normal variants
  • 5. Incidence  Major congenital anomalies At birth  2 – 3 % At 5 yrs  4 – 6 %  Minor congenital anomalies At birth  15 %
  • 6. The importance of recognizing minor anomalies  Minor anomalies are often indicators for relevant major anomalies.
  • 7.
  • 8. Causes of malformations Cause Percent incidence Genetic Chromosome Single gene 15 – 25 10 – 15 2 – 10 Multifactorial 20 – 25 Environmental Maternal diseases Uterine / Plazental Drug / Chemicals 8 – 12 6 – 8 2 – 3 0.5 – 1 Twinning 0.5 – 1 Unknown 40 – 60
  • 11.
  • 13. History  Antenatal history  Problems with infertility (medications [clomid]  techniques [IVF - invitro fertilization, PGD - preimplantation genetic diagnosis, ICSI - intracytoplasmic sperm injection])  Fetal Movement (active, decreased)  Exposures (medications, tobacco, alcohol, drugs, chemicals)  Illnesses (fevers, exposures to infections)  Problems (bleeding, pre-term labor, abnormal prenatal testing or ultrasound)  Birth history  Presentation: breech/cephalic/oblique  Delivery: vaginal, c-section (why?)  Neonatal course (complications/problems and days hospitalized)
  • 14. History  Neonatal status  APGAR  Anthopometric measurements  Resuscitation  Newborn course  Feeding  Activity  Obvious deformities  Complications / issues
  • 15. History  Past Medical History  Illnesses, hospitalizations, surgeries, immunizations, medications, allergies  A detailed review of systems.  Developmental History  Address parental concerns.  Determine ages for milestones (gross motor, fine motor, personal/social, language).  Determine current milestones (appropriate for age?).
  • 16. Family history  Take a detailed, three-generation family history
  • 17. Family history Ask for:  Birth defects  Other genetic diseases  Multiple miscarriages  Parental ages and health status  Consanguinity and geographic origin
  • 18. Physical examination  Growth monitoring  Measurements of the child's weight, length, and head circumference should be plotted on the standardized growth charts.  General appearance  Body shape and size etc.
  • 20. Investigations  Cytogenetics is a mainstay of diagnosis in dysmorphology.  However, chromosome studies are labour intensive and relatively expensive.  To be visible, a chromosome deletion or duplication probably involves at least 3–4 kilobases of DNA10 (perhaps 15–30 genes, depending upon the location and the chromosome).
  • 21. Fluorescence in situ hybridization (FISH)  Prader-Willi syndrome  Angelman syndrome  Smith-Magenis syndrome  Miller-Dieker syndrome  Velo-cardio-facial syndrome  DiGeorge syndrome
  • 22. Whole chromosome painting (WCP)  WCP is very useful for identifying the origin of additional chromosome material that is microscopically visible but not distinctive enough to be assigned to a specific chromosome.  It can also be used to search for light microscopically invisible (cryptic) translocations where suspicion of a chromosome abnormality remains, despite a normal standard karyotype.  The exchange of similarly sized and banded material between 2 chromosomes, which is not visible in a standard study, becomes visible because of the exchange of different colours.
  • 23. Other investigations  Molecular (DNA) diagnostics  Biochemical lab testing (to rule out any inborn error of metabolism, storage diseases etc.)
  • 24. The major problems of morphogenesis
  • 25. Disruptions  Morphological alterations of structures after formation  Has low recurrence risk
  • 26. Causes of disruption  Ionization (x-ray, radioactive substance exposure)  Hyperthermia  Infections  Teratogenic  Metabolic  Vascular disruption  Amnion rupture sequence
  • 27.
  • 28. Deformations  Due to mechanical forces that mold a part of fetus over a prolonged time period  The musculoskeletal system may be involved, but may also be reversible post-natally
  • 30. Risks for fetal constraint  Maternal risk factors  Primigravida  Small uterus  Uterine malformation  Uterine fibromata  Small maternal pelvis  Fetal risk factors  Oligohydroamnios  Large fetus  Multiple gestation
  • 31. Deformations related to breech presentation
  • 34.
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  • 39.
  • 40.
  • 41. Chin
  • 43.
  • 44.
  • 45.
  • 46.
  • 47.
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  • 49.
  • 51. Down syndrome (trisomy 21)  Low set ears  Hypotonia  Simian crease  Wide space between first and second toe  Flat face
  • 52. Patau syndrome (trisomy 13)  Holoprosencephaly  Cutis aplasia  Microcephaly  Microphthalmia  Cleft lip +/- palate  Polydactyly  Congenital heart defect
  • 53. Edwards syndrome (trisomy 18)  Weak cry  Polyhydroamnios  Growth deficiency  Low-set, malformed auricles  Clenched hand with overlapping fingers  Rocker bottom feet  Congenital heart defect
  • 54. Klinefelter syndrome (47xxy)  Tall stature  Behavioral issues  Post-pubertal hypogonadism
  • 55. Turner syndrome (45x) Not diagnosed until 5-6 yrs  Webbed neck  Shield chest  Cubitus vulgaris  Low hairline  Short stature  Renal anomalies  Cardiac anomalies (bicuspid aortic valve and coarctation of aorta)
  • 57. Wolf hirshorn (4p)  Hypertelorism  Broad nasal bridge  Cleft lip +/- palate  Down turned mouth  Severe mental retardation
  • 58. Cri-du-chat (5p)  Microcephaly  Growth retardation  High-pitched cat-like cry  Congenital heart disease  Hypotonia
  • 60. Prader-willi syndrome (15q11)  Obesity  Hypotonia  Small hands and feet  Upward slanting palpebral fissures  IQ : 60 – 70  Micro-penis / cryptorchidism
  • 61. Angelman syndrome (15q11)  Mental retardation  Puppet like gait  Paroxysms of inappropriate laughter  Absent / limited speech  Seizures
  • 62. 22q11 deletion syndromes (Di-George, Velocardial-facial, Sprintzen)  Micrognathia  Low set ears  Short palpebral fissures  Blunted nose  High-arched palate  Cleft palate +/- bifid uvula
  • 64. Achondroplasia (FGFR3)  Rhizomelic shortening of limbs  Short fingers held in trident configuration  Elarged head with depressed nasal bridge
  • 65. Neurofibromatosis  > 6 café-au-lait spots  >2 neurofibromas  Lisch nodules (iris hematoma)  Optic gliomas  Angiofibromas  Axillary or inguinal freckling
  • 66. Osteogenesis imperfecta  Fractures  Osteopenia  Blue sclera  Hearing loss  Short stature  Four types
  • 67. Autosomal recessive Cystic fibrosis Tay-Sacs disease Sickle cell anemia
  • 70. Quiz
  • 71. What are the most appropriate genetic condition associated with the following physical findings?  Webbed neck  Macrosomia  Rhizometric shortening  Small hands  Café-au-lait spots
  • 72. What are the most appropriate genetic condition associated with the following physical findings?  Upward slanting palpebral fissures  Downward slanting palpebral fissures  Lich nodules  Kayser-fleischer ring