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Chromosomal aberrations
Definition :-
       ―Any deviation either in number or structure of the
 chromosomes is referred as chromosomal aberrations‖

Types :-
1) Structural aberrations.
2) Numerical aberrations.
Terminologies:
 Diploid


 Hapliod


 Polyploidy : in multiple of ‗n‘


 Aneuploidy : any number which is not exactly a multiple
 of ‗n‘
       2n - 1 ------ > Turners syndrome (45X)
Or     2n + 1 ------ > Down‘s syndrome (47, trisomy 21)
Genesis of anuploidy
Non-disjunction in meiosis. Or after formation of zygote.
Structural aberrations
 Stable:–
               - Deletions
               - Translocation
               - Insertion
               - Inversions
               - Isochromosomes
 Unstable:-
             - Dicentric
             - Ring chromosomes
May occur due to
a) Ionizing radiations
b) Chemical agents
c) viruses
Deletion
      This Involves loss of a part of chromosome.
1. Terminal deletion.
2. Interstitial deletion.


1. Terminal deletion.
    It involves a single break and the terminal part of the
    chromosome is lost.
e.g. cri-du-chat syndrome
- Deletion of 5p arm
- Cry of baby
- Typical facial appearance
- Microcephaly, hypertelorism,
- Antimongoloid slant of
  palpebral fissure.
- Low set ears, microganthia.
2) Interstitial deletion.
       It involves two breaks and the intervening portion of
  the chromosome is lost.
 Wilm‘s tumor with anirida. (11q13)


 Prader- will syndrome. (15q11-13)
 Angelman syndrome. (15q11-13)
Microdeletion syndrome - Deletion of 3 – 4 Mb
Prader- will syndrome. (15q11-13)
- Inherited from father
- Short stature, hypotonia
- Obesity
- Small hands & feet
- Mild to moderate mental retardation
- Hypogonadism


Angelman syndrome. (15q11-13)
- Inherited from mother
- Severe mental retardation
- Seizures & ataxic gait
Difference is due to genomic imprinting.
Translocation

1) Robertsonian translocation
- Involves two acrocentric
    chromosomes
-   D/G Translocation
-   Also called centric fusion
-   In 4% of down‘s cases
-   [50% from parents(balanced),
     50% de novo in baby]
2) Reciprocal Translocation
- Exchange of material distal to
  breaks
- In non homologus chromosomes
- No chromosome material is lost
- Abnormal production of gamets
- Spontaneous abortions/ baby with
  congenital malformations
- Carrier couple- repeated abortions.
Insertion
- Rare non-reciprocal type of translocation
- Involves 3 breaks
- 2 breaks to release fragment
- 1 break to admit fragment.
Inversions
 Pericentric – involves
  both arms p & q
 Paracentric – either p or q
 Do not give abnormal
  phenotype
 Abnormal gamets may
  give abnormal progeny.
Isochromosomes

- Abnormal split along
  the centromere
- Seperation of arms
- E.g. isochromosome X
  (Xq)
- In some cases of
  Turners syndrome
Ring chromosomes
- Two breaks at terminal ends
- Fusion of the cut ends
- 1/5th cases of turners syndrome
Factors playing role in chromosomal
aberrations
   Maternal age > 35 yrs
    non-disjunction during meiosis 1
   Radiation
    correlation between radiation and non-disjunction
   Chromosomal abnormalities
    balnced translocation in parents may produce
    aberrations in offsprings
   Autoimmune disorders - not clear
    High titer of thyroid autoantibodies in mother
    associated with Down‘s syndrome in their childrens
Numerical aberrations
 Autosomal :-
           Trisomy 21 / Down‘s syndrome
           Trisomy 18 / Edwards syndrome
           Trisomy 13 / Patau syndrome

 Sex chromosome related :-
           Turners syndrome / 45X
           Polysomy X syndrome / e.g. XXX, XXXX
           Klinfelters syndrome / 47 XXY
Autosomal
 Monosomies are fetal – Abortion.
 Trisomies are common.
Down’s syndrome / Trisomy 21
 1866 – first identified by Langdon
  Down.
 1959- Lejeune & associates
  demonstrated extra chromosome
  no.21
 Mongolism


 Incidence- Approximately one in
  1000 live births.
Clinical features
 Mental retardation –
  predominant feature
 IQ – 25-50
 Small stature
 Hypotonia of muscles
 Brachycephaly with flat
  occiput
 Epicanthal fold—mongoloid
  slant
 Flat nose, low nasal bridge
 Mouth is open with
  protruded tongue
 Highly arched palate
  with delayed dentition
 Hands are short and
  broad
 Cardiovascular defect in
  1/10th cases.
 Ears are low set and malformed
Dermatoglyphics
 Simian crease- classical feature
 Wide gap between first and second toe.
Cytogenetics
 Trisomy 21 (47, +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 – 2 to 3 % cases
Karyotype of Down’s syndrome
Risk of Down’s syndrome
 Maternal age
 Does the couple already have baby with down’s
  syndrome?
 What is karyotype of baby?(typical / translocation)
 Parent carrier of translocation?
Diagnosis
 Prenatal screening
 If no screening – It is recognized from the
  characteristic phenotypic features.
 Confirmed by Karyotype.( chorionic villous biopsy ,
  amniocentesis)
Management
Counseling
 May begin when a prenatal diagnosis is made.
 Discuss the wide range of variability in manifestation and
  prognosis.
 Medical and educational treatments and interventions
  should be discussed.
 Initial referrals for early intervention, informative
  publications, parent groups, and advocacy groups.
Management cont..
1. Growth – Measurements should be plotted on the
  appropriate growth chart for children with DS.
 This will help in prevention of obesity and early diagnosis
  of celiac disease and hypothyroidism.

2. Cardiac disease – All newborns should be evaluated by
  cardiac ECHO for CHD in consultation with pediatric
  cardiologist.

3. Hearing – Screening to be done in the newborn period,
  every 6 months until 3 yrs of age and then annually.
4. Eye disorders - An eye exam should be performed in the
  newborn period or at least before 6 months of age to detect
  strabismus, nystagmus, and cataracts.

5. Thyroid Function – Should be done in newborn period and
  should be repeated at six and 12 months , and then
  annually.

6. Celiac Disease – Screening should begin at 2 yrs. Repeat
  screening if signs/Sx develop.
7.   Hematology – CBC with differential at birth to evaluate for
     polycythemia as well as WBC.

8.   Atlanto-axial instability – X ray for evidence of AAI or sub-
     luxation at 3 to 5 years of age.

9.   Alzheimer‘s disease – Adult with a Down Syndrome has
     earlier onset of symptoms. When diagnosis is
     considered, thyroid disease and possible depression
     should be excluded.
Chromosomal aberrations,downs syndrome-Dr.Gourav

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Chromosomal aberrations,downs syndrome-Dr.Gourav

  • 1.
  • 2. Chromosomal aberrations Definition :- ―Any deviation either in number or structure of the chromosomes is referred as chromosomal aberrations‖ Types :- 1) Structural aberrations. 2) Numerical aberrations.
  • 3. Terminologies:  Diploid  Hapliod  Polyploidy : in multiple of ‗n‘  Aneuploidy : any number which is not exactly a multiple of ‗n‘ 2n - 1 ------ > Turners syndrome (45X) Or 2n + 1 ------ > Down‘s syndrome (47, trisomy 21)
  • 4. Genesis of anuploidy Non-disjunction in meiosis. Or after formation of zygote.
  • 5. Structural aberrations  Stable:– - Deletions - Translocation - Insertion - Inversions - Isochromosomes  Unstable:- - Dicentric - Ring chromosomes May occur due to a) Ionizing radiations b) Chemical agents c) viruses
  • 6. Deletion This Involves loss of a part of chromosome. 1. Terminal deletion. 2. Interstitial deletion. 1. Terminal deletion. It involves a single break and the terminal part of the chromosome is lost. e.g. cri-du-chat syndrome
  • 7. - Deletion of 5p arm - Cry of baby - Typical facial appearance - Microcephaly, hypertelorism, - Antimongoloid slant of palpebral fissure. - Low set ears, microganthia.
  • 8.
  • 9. 2) Interstitial deletion. It involves two breaks and the intervening portion of the chromosome is lost.  Wilm‘s tumor with anirida. (11q13)  Prader- will syndrome. (15q11-13)  Angelman syndrome. (15q11-13) Microdeletion syndrome - Deletion of 3 – 4 Mb
  • 10. Prader- will syndrome. (15q11-13) - Inherited from father - Short stature, hypotonia - Obesity - Small hands & feet - Mild to moderate mental retardation - Hypogonadism Angelman syndrome. (15q11-13) - Inherited from mother - Severe mental retardation - Seizures & ataxic gait Difference is due to genomic imprinting.
  • 11.
  • 12. Translocation 1) Robertsonian translocation - Involves two acrocentric chromosomes - D/G Translocation - Also called centric fusion - In 4% of down‘s cases - [50% from parents(balanced), 50% de novo in baby]
  • 13. 2) Reciprocal Translocation - Exchange of material distal to breaks - In non homologus chromosomes - No chromosome material is lost - Abnormal production of gamets - Spontaneous abortions/ baby with congenital malformations - Carrier couple- repeated abortions.
  • 14. Insertion - Rare non-reciprocal type of translocation - Involves 3 breaks - 2 breaks to release fragment - 1 break to admit fragment.
  • 15. Inversions  Pericentric – involves both arms p & q  Paracentric – either p or q  Do not give abnormal phenotype  Abnormal gamets may give abnormal progeny.
  • 16. Isochromosomes - Abnormal split along the centromere - Seperation of arms - E.g. isochromosome X (Xq) - In some cases of Turners syndrome
  • 17. Ring chromosomes - Two breaks at terminal ends - Fusion of the cut ends - 1/5th cases of turners syndrome
  • 18. Factors playing role in chromosomal aberrations  Maternal age > 35 yrs non-disjunction during meiosis 1  Radiation correlation between radiation and non-disjunction  Chromosomal abnormalities balnced translocation in parents may produce aberrations in offsprings  Autoimmune disorders - not clear High titer of thyroid autoantibodies in mother associated with Down‘s syndrome in their childrens
  • 19. Numerical aberrations  Autosomal :- Trisomy 21 / Down‘s syndrome Trisomy 18 / Edwards syndrome Trisomy 13 / Patau syndrome  Sex chromosome related :- Turners syndrome / 45X Polysomy X syndrome / e.g. XXX, XXXX Klinfelters syndrome / 47 XXY
  • 20. Autosomal  Monosomies are fetal – Abortion.  Trisomies are common.
  • 21. Down’s syndrome / Trisomy 21  1866 – first identified by Langdon Down.  1959- Lejeune & associates demonstrated extra chromosome no.21  Mongolism  Incidence- Approximately one in 1000 live births.
  • 22. Clinical features  Mental retardation – predominant feature  IQ – 25-50  Small stature  Hypotonia of muscles  Brachycephaly with flat occiput  Epicanthal fold—mongoloid slant  Flat nose, low nasal bridge
  • 23.  Mouth is open with protruded tongue  Highly arched palate with delayed dentition  Hands are short and broad  Cardiovascular defect in 1/10th cases.
  • 24.  Ears are low set and malformed
  • 25. Dermatoglyphics  Simian crease- classical feature  Wide gap between first and second toe.
  • 26. Cytogenetics  Trisomy 21 (47, +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 – 2 to 3 % cases
  • 28. Risk of Down’s syndrome  Maternal age  Does the couple already have baby with down’s syndrome?  What is karyotype of baby?(typical / translocation)  Parent carrier of translocation?
  • 29. Diagnosis  Prenatal screening  If no screening – It is recognized from the characteristic phenotypic features.  Confirmed by Karyotype.( chorionic villous biopsy , amniocentesis)
  • 30. Management Counseling  May begin when a prenatal diagnosis is made.  Discuss the wide range of variability in manifestation and prognosis.  Medical and educational treatments and interventions should be discussed.  Initial referrals for early intervention, informative publications, parent groups, and advocacy groups.
  • 31. Management cont.. 1. Growth – Measurements should be plotted on the appropriate growth chart for children with DS.  This will help in prevention of obesity and early diagnosis of celiac disease and hypothyroidism. 2. Cardiac disease – All newborns should be evaluated by cardiac ECHO for CHD in consultation with pediatric cardiologist. 3. Hearing – Screening to be done in the newborn period, every 6 months until 3 yrs of age and then annually.
  • 32. 4. Eye disorders - An eye exam should be performed in the newborn period or at least before 6 months of age to detect strabismus, nystagmus, and cataracts. 5. Thyroid Function – Should be done in newborn period and should be repeated at six and 12 months , and then annually. 6. Celiac Disease – Screening should begin at 2 yrs. Repeat screening if signs/Sx develop.
  • 33. 7. Hematology – CBC with differential at birth to evaluate for polycythemia as well as WBC. 8. Atlanto-axial instability – X ray for evidence of AAI or sub- luxation at 3 to 5 years of age. 9. Alzheimer‘s disease – Adult with a Down Syndrome has earlier onset of symptoms. When diagnosis is considered, thyroid disease and possible depression should be excluded.