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 Parents of a 4 year old child were referred for
  genetic study.
 The child had “jaundice” with fluid in his tummy
  for over a year and died because of the same.
 Parents are planning second pregnancy and are
  worried that the second pregnancy might also be
  affected as they were told that their first child
  could have died because of some “inherited”
  disease.


                                                      2
 How come their child has “inherited disease
  when they are healthy?
 What could have gone “wrong” ?

 What tests will guarantee that their next child
  will be healthy?
 How and where the tests will be done?




                                                    3
 Patterns of inheritance will easily explain this...
 But there are spontaneous mutations and

 there is a role of environmental factors also,

   e.g. tobacco




                                                        4
   Malfunctioning of a gene/s




                                 5
 It is a functional area on a chromosome which is
  made up of various nucleotides, which will
  manufacture various proteins, that will carry out
  various bodily functions.
 If it works well, our body works well

 If it is not working well, a genetic defect, then
  our body may have some malfunction.




                                                      6
Gene




       7
8
 A car engine has several parts
 If one part is defective,
     the engine may not work,
     works defectively or
     it may breakdown half way through




    Same thing will happen, when a gene has some
      defective parts

                                                   9
10
   Chromosomal abnormalities or mutation or aberration
    are according to their structural and numerical changes
    they termed as

   Structural abnormalities
   Numerical abnormalities



                                                         11
   Gene mutations have varying effects on health, depending on where
    they occur and whether they alter the function of essential proteins.
    The types of mutations include:

 Missense mutation
 Nonsense mutation
 Insertion
 Deletion
 Duplication
 Repeat expansion

                                                                     12
 Normal function
 Partially normal function

 Totally non-functional
        Lethal
        Compatible with life in a limited or compromised way




                                                                13
   One which is frequently seen in a given disease
    due to genetic defect




                                                      14
If a Bajaj scooter is not working,
most commonly you have to tilt it !!




But there could be other reasons
also, the uncommon causes              15
Bajaj scooter and Honda may not start
for entirely different reasons




Indians may have different mutations
responsible for Wilson’s disease than
Caucasians                              16
   More mutations we test, more chances are that
    we will be more confident in your predictions

   So we have to know mutations in our population,
    otherwise we may keep making mistakes.




                                                      17
   We can’t proceed further without knowing what
    was the disease and what was the mutation
    responsible for their first child’s, “the proband’s”,
    death




                                                            18
   All we can offer them is the common mutation
    tests for commonly occurring genetically
    inherited liver diseases.

   As we may understand, this may lead to lots of
    problems.




                                                     19
On the other hand....
 Had we known the disease and the mutation in
  the proband, then certainly we can test the fetus
  for that particular mutation and reasonably
  certainly counsel the parents.




                                                      20
   If we don’t know what happened to the proband,
    we can’t do much in the next pregnancy




                                                     21
 Carrier testing before conception
 Best example is screening for DMD




                                      22
   Testing the fertilized embryo for genetic dosing.




                                                        23
 By amniotic fluid at 16 weeks; and
 Chorion Villous Biopsy at 12 weeks

 Triple marker test




                                       24
   By New Born Screening (NBS)




                                  25
26
 Some disorders that "run in families" can be traced to
  shared environmental exposures rather than any inherited
  susceptibility. In addition, some mutations detected by a
  positive test may never lead to disease.
 Furthermore, because existing tests look only for the
  more common mutations in a gene, but some disease-
  causing mutations may escape detection.




                                                              27
 Gene can go wrong in various ways. This is called
  mutation.
 Different races have different mutations, some
  common and some uncommon and what applies
  in Caucasians may not apply in India.
 Looking for mutation in sibling without knowing
  mutation in the proband is no..no..
 But a reliably diagnosed mutation could be the
  most accurate way of diagnosing a genetic
  diseases.
                                                      28
29
30

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Introduction to genetics final

  • 1.
  • 2.  Parents of a 4 year old child were referred for genetic study.  The child had “jaundice” with fluid in his tummy for over a year and died because of the same.  Parents are planning second pregnancy and are worried that the second pregnancy might also be affected as they were told that their first child could have died because of some “inherited” disease. 2
  • 3.  How come their child has “inherited disease when they are healthy?  What could have gone “wrong” ?  What tests will guarantee that their next child will be healthy?  How and where the tests will be done? 3
  • 4.  Patterns of inheritance will easily explain this...  But there are spontaneous mutations and  there is a role of environmental factors also, e.g. tobacco 4
  • 5. Malfunctioning of a gene/s 5
  • 6.  It is a functional area on a chromosome which is made up of various nucleotides, which will manufacture various proteins, that will carry out various bodily functions.  If it works well, our body works well  If it is not working well, a genetic defect, then our body may have some malfunction. 6
  • 7. Gene 7
  • 8. 8
  • 9.  A car engine has several parts  If one part is defective,  the engine may not work,  works defectively or  it may breakdown half way through Same thing will happen, when a gene has some defective parts 9
  • 10. 10
  • 11. Chromosomal abnormalities or mutation or aberration are according to their structural and numerical changes they termed as  Structural abnormalities  Numerical abnormalities 11
  • 12. Gene mutations have varying effects on health, depending on where they occur and whether they alter the function of essential proteins. The types of mutations include:  Missense mutation  Nonsense mutation  Insertion  Deletion  Duplication  Repeat expansion 12
  • 13.  Normal function  Partially normal function  Totally non-functional  Lethal  Compatible with life in a limited or compromised way 13
  • 14. One which is frequently seen in a given disease due to genetic defect 14
  • 15. If a Bajaj scooter is not working, most commonly you have to tilt it !! But there could be other reasons also, the uncommon causes 15
  • 16. Bajaj scooter and Honda may not start for entirely different reasons Indians may have different mutations responsible for Wilson’s disease than Caucasians 16
  • 17. More mutations we test, more chances are that we will be more confident in your predictions  So we have to know mutations in our population, otherwise we may keep making mistakes. 17
  • 18. We can’t proceed further without knowing what was the disease and what was the mutation responsible for their first child’s, “the proband’s”, death 18
  • 19. All we can offer them is the common mutation tests for commonly occurring genetically inherited liver diseases.  As we may understand, this may lead to lots of problems. 19
  • 20. On the other hand....  Had we known the disease and the mutation in the proband, then certainly we can test the fetus for that particular mutation and reasonably certainly counsel the parents. 20
  • 21. If we don’t know what happened to the proband, we can’t do much in the next pregnancy 21
  • 22.  Carrier testing before conception  Best example is screening for DMD 22
  • 23. Testing the fertilized embryo for genetic dosing. 23
  • 24.  By amniotic fluid at 16 weeks; and  Chorion Villous Biopsy at 12 weeks  Triple marker test 24
  • 25. By New Born Screening (NBS) 25
  • 26. 26
  • 27.  Some disorders that "run in families" can be traced to shared environmental exposures rather than any inherited susceptibility. In addition, some mutations detected by a positive test may never lead to disease.  Furthermore, because existing tests look only for the more common mutations in a gene, but some disease- causing mutations may escape detection. 27
  • 28.  Gene can go wrong in various ways. This is called mutation.  Different races have different mutations, some common and some uncommon and what applies in Caucasians may not apply in India.  Looking for mutation in sibling without knowing mutation in the proband is no..no..  But a reliably diagnosed mutation could be the most accurate way of diagnosing a genetic diseases. 28
  • 29. 29
  • 30. 30