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TRISOMY 21- DOWN SYNDROME 
AND 
KLINEFELTER’S SYNDROME 
By : SEJWAL MADHUR KUMAR
CONTENTS 
1.DOWN SYNDROME 2.KLINEFELTER 
SYNDROME 
 INCIDENCE 
 GENETICS 
 CLINICAL FEATURES 
 HEMATOLOGICAL 
DISORDERS 
 DIAGNOSIS 
 MORTALITY 
• CAUSES 
• CLINICAL FEATURES 
• COMPLICATIONS 
• INVESTIGATIONS
DOWN SYNDROME 
Most common 
chromosomal disorder 
INCIDENCE 
If maternal age is <20 yrs 
,Approximately 1 in 1550 
live births, 
But if maternal age is >45 
yrs ,incidence is 1 in 25 live 
births
Genetics 
 Trisomy 21 (47,XX, +21), - 94 %, The 
frequency of trisomy increases with 
increasing maternal age. 
 Robertsonian translocation involving 
chromosome 21- Approx. 3-4 %, not related 
to maternal age. 
 Trisomy 21 mosaicism – 1-2% cases
Clinical Features 
 Head and neck 
 Flat facial profile 
 Up-slanting palpebral fissures 
 Epicanthal folds 
 Brushfield spots 
 Flat nasal bridge 
 Folded or dysplastic ears 
 Open mouth 
 Protruding tongue 
 Short neck 
 Excessive skin at the nape of 
neck 
 Extremities 
 Short broad hands 
 Short fifth finger 
 Incurved fifth finger 
 Transverse palmer crease 
 Space between first and 
second toe 
 Hyper flexibility of joints
Mental Retardation 
 Almost all DS babies have MR. 
 Mildly to moderately retarded . 
 Starts in the first year of life. 
 Average age of sitting(11 mon), and walking (26 
mon) is twice the typical age. 
 First words at 18 months. 
 IQ declines through the first 10 years of age, 
reaching a plateau in adolescence that continues 
into adulthood.
Heart Disease 
GI Abnormalities 
 50 % of Down Syndrome pts have heart disease 
 Atrioventricular septal defect 
 VSD 
 Secundum ASD 
 Mitral valve prolapse 
 Valvular malformation 
 GI abnormalities –in 5% cases of DS 
 Duodenal atresia or stenosis 
 Oesophageal atresia and intestinal stenosis
Hematologic disorders 
 The risk of leukemia is 1 to 1.5 percent. 
 65% of newborn have polycythemia resulting in 
hypoglycemia. 
 Risk of AML ( ACUTE MEGAKARYOBLASTIC 
LUEKEMIA )is also much higher than the general 
population. 
 Transient leukemia.
Diagnosis 
 Prenatal screening 
 If no screening – It is recognized from the 
characteristic phenotypic features. 
 Confirmed by Karyotype.
Mortality 
Median age of death has increased from 25 yrs 
to 49 yrs , an average of 1.7 yrs increase per 
year. 
Most likely cause of death is CHD, Dementia, 
Hypothyroidism and Leukemia. 
Improved survival is because of increased 
placements of infants in homes and 
changes in treatment for common causes of 
death. 
Survival is better for males and blacks.
KLINEFELTER’S 
SYNDROME
KLINEFELTER SYNDROME 
 It is the state of male hypogonadism 
due to 2 or more X chromosome with 
1 or more y chromosome. 
 INCIDENCE : 1 in 2000 live male 
births 
 KARYOTYPE: 82% have classical 
47,XXY 
15% mosaics , 46XY/47,XXY 
Remaining polysomic individuals
cause 
MEIOSIS 1 
(GAMETOGENESIS) 
NON DISJUNCTION 
occurs when 
homologous 
chromosomes ( X and Y) 
fails to separate and 
producing a sperm with 
extra X and Y 
chromosome
Clinical features 
 Abnormally 
increased distance 
between pubic ramus 
and sole of feet. 
 Lower body appears 
abnormally 
elongated also called 
as EUNUCHOID 
BODY HABITUS
CLINICAL FEATURES 
 Atrophied testes - testicular biopsy shows 
atrophied hyalinised seminiferous tubules 
with no spermatogenesis. 
 Lack of secondary sexual characteristics 
 Gynecomastia is seen 
 Mental intelligence is near normal 
 Greater the number of X chromosome 
,lower is the level of intelligence
COMPLICATIONS 
 Infertility 
 20x increased risk of ca breast 
 Increased risk of germ cell tumor 
 Increased risk of autoimmune 
diseases like SLE (SYSTEMIC 
LUPUS ERYTHEMATOSUS)
INVESTIGATION 
 Plasma gonadotropin level 
 Testicular biopsy 
 Total sperm count 
 karyotyping
THANK YOU 

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down syndrome and klinefelters syndrome

  • 1. TRISOMY 21- DOWN SYNDROME AND KLINEFELTER’S SYNDROME By : SEJWAL MADHUR KUMAR
  • 2. CONTENTS 1.DOWN SYNDROME 2.KLINEFELTER SYNDROME  INCIDENCE  GENETICS  CLINICAL FEATURES  HEMATOLOGICAL DISORDERS  DIAGNOSIS  MORTALITY • CAUSES • CLINICAL FEATURES • COMPLICATIONS • INVESTIGATIONS
  • 3. DOWN SYNDROME Most common chromosomal disorder INCIDENCE If maternal age is <20 yrs ,Approximately 1 in 1550 live births, But if maternal age is >45 yrs ,incidence is 1 in 25 live births
  • 4. Genetics  Trisomy 21 (47,XX, +21), - 94 %, The frequency of trisomy increases with increasing maternal age.  Robertsonian translocation involving chromosome 21- Approx. 3-4 %, not related to maternal age.  Trisomy 21 mosaicism – 1-2% cases
  • 5.
  • 6.
  • 7.
  • 8. Clinical Features  Head and neck  Flat facial profile  Up-slanting palpebral fissures  Epicanthal folds  Brushfield spots  Flat nasal bridge  Folded or dysplastic ears  Open mouth  Protruding tongue  Short neck  Excessive skin at the nape of neck  Extremities  Short broad hands  Short fifth finger  Incurved fifth finger  Transverse palmer crease  Space between first and second toe  Hyper flexibility of joints
  • 9.
  • 10.
  • 11. Mental Retardation  Almost all DS babies have MR.  Mildly to moderately retarded .  Starts in the first year of life.  Average age of sitting(11 mon), and walking (26 mon) is twice the typical age.  First words at 18 months.  IQ declines through the first 10 years of age, reaching a plateau in adolescence that continues into adulthood.
  • 12. Heart Disease GI Abnormalities  50 % of Down Syndrome pts have heart disease  Atrioventricular septal defect  VSD  Secundum ASD  Mitral valve prolapse  Valvular malformation  GI abnormalities –in 5% cases of DS  Duodenal atresia or stenosis  Oesophageal atresia and intestinal stenosis
  • 13. Hematologic disorders  The risk of leukemia is 1 to 1.5 percent.  65% of newborn have polycythemia resulting in hypoglycemia.  Risk of AML ( ACUTE MEGAKARYOBLASTIC LUEKEMIA )is also much higher than the general population.  Transient leukemia.
  • 14. Diagnosis  Prenatal screening  If no screening – It is recognized from the characteristic phenotypic features.  Confirmed by Karyotype.
  • 15. Mortality Median age of death has increased from 25 yrs to 49 yrs , an average of 1.7 yrs increase per year. Most likely cause of death is CHD, Dementia, Hypothyroidism and Leukemia. Improved survival is because of increased placements of infants in homes and changes in treatment for common causes of death. Survival is better for males and blacks.
  • 17. KLINEFELTER SYNDROME  It is the state of male hypogonadism due to 2 or more X chromosome with 1 or more y chromosome.  INCIDENCE : 1 in 2000 live male births  KARYOTYPE: 82% have classical 47,XXY 15% mosaics , 46XY/47,XXY Remaining polysomic individuals
  • 18. cause MEIOSIS 1 (GAMETOGENESIS) NON DISJUNCTION occurs when homologous chromosomes ( X and Y) fails to separate and producing a sperm with extra X and Y chromosome
  • 19. Clinical features  Abnormally increased distance between pubic ramus and sole of feet.  Lower body appears abnormally elongated also called as EUNUCHOID BODY HABITUS
  • 20. CLINICAL FEATURES  Atrophied testes - testicular biopsy shows atrophied hyalinised seminiferous tubules with no spermatogenesis.  Lack of secondary sexual characteristics  Gynecomastia is seen  Mental intelligence is near normal  Greater the number of X chromosome ,lower is the level of intelligence
  • 21. COMPLICATIONS  Infertility  20x increased risk of ca breast  Increased risk of germ cell tumor  Increased risk of autoimmune diseases like SLE (SYSTEMIC LUPUS ERYTHEMATOSUS)
  • 22. INVESTIGATION  Plasma gonadotropin level  Testicular biopsy  Total sperm count  karyotyping
  • 23.