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Haema 
is Greek for blood. 
Thalassa 
is Greek for the sea.
2ᶑ& 2 βchain 
97% Adult haemoglobin 
After birth Hb F is replaced by Hb A By six months of age 
HbF: 2ᶑ& 2 ϒchain 
At birth HbFis 70-90%, That fall to 25% by one month & <2% by one year of age 
HbA2 : 2ᶑ& 2δchain 
1.5 to <3.5% in normal adult 
Types of Haemoglobin
The Gene of Alpha chain is 
located on Chromosome 16. 
Molecular aspect of Thalassaemia 
The Gene of Beta chain is 
located on Chromosome 11.
SEQUENCE OF BASES - “GENE” 
Molecular aspect of Thalassaemia 
T C G A T G 
A G C T A C 
Substitution, Deletion , Insertion of base pair of a gene results in another sequence of GENE called “ GENE MUTATION”.
Mutation causes either decrease or absent synthesis of globin protein . 
•Decrease synthesis of Beta globin chain – 
•Beta Thalassaemia 
•Decrease synthesis of 
•Alpha globin chain - 
•Alpha Thalassaemia
•Approximately>200mutationsareknown 
tocauseThalassemiaallovertheworld. 
OfthemFivecommonThalassemia 
mutationsin“INDIA”are– 
•(IVS)1-S (G ->C) 
•IVS 1 -1 (G->T) 
•619 bp DELETION 
•+1 Codon 8/9(+G) 
•-Codon 41/42(-CTTT) 
Beta -Thalassaemia Major
Beta -Thalassaemia Pathophysiology
Repeated BT causes iron load. 
Desferoxamine is Given S.C. for 8 hours 
every day for 5-6 days a week so as to chelate 
iron load.
In 15 years of life span
Preventing the Birth of a “Thalassaemia” child is the only answer to this world wide problem
How does the birth of a thalassemia child occur ?
When both partners are carrier ,there is 25% chance of child to be affectectdwith Thalessaemiain each pregnancy 
CARRIER 
50 % CARRIER 
25% NORMAL 
25% T .MAJOR 
CARRIER
But when only one partner is carrier then no child will be affected with Thaessemia 
CARRIER 
50 % CARRIER 
NORMAL 
50% NORMAL
-Carriers are Asymptomatic -They are silent culprit
Hb11.5 gm% 
MCV60.6 MCH 18.6 
MENTZER INDEX -MCV/TRBC 60.6/6.12 = 9.8
GeneticCounseling 
If marriage is unavoidable due to cultural 
& social reasons or diagnosed as carriers after 
marriage or after conception
P 
Then what is the option ? 
PRENATAL DIAGNOSIS
G1P0A0 
Dx 
Haemogram 
MCV 53.2 
MCH 15.8 
TRBC5.6 
MCV/TRBC = 9. 
Couple came for consultation at 18 weeks
G1P0A0 
MCV 60.6 
MCH 18.8 
TRBC6.12 
MCV/TRBC = 9.9 
MCV 53.2 
MCH 15.8 
TRBC5.6 
MCV/TRBC = 9. 
Couple came for consultation at 18 weeks
G1P0A0 
Thalassemia carrier 
HbA2 4.6 
HbA2 5.5 
Couple came for consultation at 18 weeks 
Thalassemia carrier
G1P0A0 
Thalassemia carrier 
Couple came for consultation at 18 weeks 
Thalassemia carrier 
Amniocentesis 
Couple’s blood in EDTA along with amniotic fluid was 
sent for Gene mutation analysis
Invasive 
C.V.S. 
Amniocentesis 
Non Invasive 
Free fetal DNA in maternal blood 
PRENATAL DIAGNOSIS
Paternal mutant gene 
Absent 
Fetus is normal or 
carrier 
Continue the pregnancy 
Paternal mutant gene 
present 
Fetus has 50% 
chance being 
Thalassaemia Major 
Massively parallel DNA 
Sequencing done 
Maternal blood is collected for Isolation of Fetal DNA 
fetal DNA is then tested for Paternal mutant gene 
NONINVASIVE
PRENATAL DIAGNOSIS 
INVASIVE PROCEDURE 
under USG Guidance by 18 gauge needle 
Trans abdominal Trans vaginal 
- 
Chorionic villous sampling (CVS) 
11-14 weeks; Preferably at 11 weeks( 73 Days)
PRENATAL DIAGNOSIS 
Trans abdominal -Ultrasound guided after 16 weeks 
22 g needle 
Initial -2-3 ml is discarded 
Usually 20cc amniotic fluid 
Results –2 to 3 weeks 
AMNIOCENTESIS 
INVASIVE PROCEDURE
Gene mutation in DNA obtained from FETUS is matched with family gene mutation 
If fetus is normal 
or carrier for thalassaemia 
If fetus is thalassaemia Major 
After genetic counseling couple should be given option for termination of pregnancy 
Continue pregnancy 
Gene mutation study Should be done among all carrier for Future family planning after birth
G3P1A2 
Thalassemia carrier 
Thalassemia carrier 
Thalassemia Major
Pre-implantation Genetic diagnosis 
PGDisastateoftheARTprocedureusedininconjunctionwithIVF.InwhichtheembryoistestedforGeneticdisorderspriortobeingplacedinthewombofthewoman-
Pre-implantation Genetic 
diagnosis IVFBiopsy on Day 3Genetic AnalysisTransfer of Unaffected EmbryoNormal Baby-
Benefits of Pre-implantation Genetic diagnosis 
Forcoupleswhohavealreadyanaffectedchild,PGDallowsHLAmatchingforpre- selectionofpotentialdonorprogenyfortheaffectedsiblingwhorequirebonemarrowtransplantation. 
Psychologicalstressofterminationofpregnancycanbeavoided
World wide 240 million people are 
carriers of β-thalassemia i.e. 
1.5% of total world population. 
Approximately 15 million people are estimated to suffer from 
“Thalassemia Major”. 
Every year One lac children are 
born with thalassemia major
On an average 1 person in every 25 Indians is a thalassemia carrier i.e. approximately 30 million people are thalassaemia carrier . 
Every hour “One” Thalassaemia major child is born i.e. every year approximately10,000 new Thalassaemia patients are born in India.
beta-thalassemia trait in India 
Panjab 6.5% 
Delhi 2.2 -9.2% 
LarkanSindhi 17% 
DaduSindhi 8% 
Bhanishali15% 
Lohana13.6% 
Kerala 0.6% 
Assam 5 % 
Gujarat 10-15%
TO REDUCE TO PREVENT TO SET UP TO DIAGNOSE
Lack of 
Education 
Lack of 
experts 
Social factors 
Lack of 
National 
policy 
lack of 
Fetal medicine 
Centre 
Lack Genetic entre 
lack of 
Funds 
lack of 
Screening
Lack of Education 
Illiteracy is a big challenge for prevention of ThalassaemiaIn India
Lack of Education 
lack of Pre marital screening 
Detection of Carrier state 
seems to be is a “stigma” to 
their life and may 
Affect their marriages 
hence deprived of it. 
Lack of Pre-conception counseling– 
Even When family is having 
affected Child, Couple have 
unplanned pregnancy due 
lack of knowledge & fund for 
Screening methods.
Lack of Education 
They do not have early 
antenatal Booking 
Hence deprived of 
prenatal screening 
And 
prenatal diagnostic 
care for 
Thalassaemia
Lack of knowledge & attitude 
Of pregnant woman & her family
Challenges of Social factors 
Consanguineous Marriage 
Marriage among Close blood relative is a big hurdle for prevention of Thalassaemia. 
Feticide is “SIN”Hence they avoid termination of even when fetus is affected.
Lack of well equipped laboratory
Lack of genetic laboratory
Challenges of Economic burden 
Fund for 
Education, Training and awareness programmes 
Fetal medicine Centre 50 -70 lacs 
Lab -Cell counter 08-10 lacs 
-HPLC 70-80 lacs 
Genetic lab 25-75 lacs
Economic burden on patients
Mass screening : 
Means screening of each individuals for thalassemia in reproductive age group (15 to 45 years)
P 
Report should be high lighted with logo of ‘Thalassemia free India”. 
Should calculate the Mentzer index and include it in haemogramreport 
Should highlight the MCV, MCH, TRBC indices in haemogramreport
3.Casscade screening : 
Screening of relatives of index Thalassemia major
Government should formulate a policy for implementation of universal Thalassaemia screening programme“FREE OF COST” for infants, school and college going children, And those attending preconceptional and antenatal clinics. “Registration of marriage by the court should be done only when Blood report of Thalassemia screening is produced”
Like “Janani surksha yojana” the government should formulate the policy Of “ SWASTH SHISHU YOJANA” to prevent the birth of child with “THALASSEMIA” by providing prenatal diagnostic facility “FREE OF COST” at each and every corner of our country. 
Psychological and financial support should be given to the pregnant women for safe termination of pregnancy if the fetus is affected with Thalassemia major.
Join hands
I AM A SMALL AND PRETTY CREATURE 
WILL SOON COME TO THIS WORLD IN FUTURE. 
BUT WOULD LIKE TO SEE SMILING DAD AND MOM 
WHEN I COME OUT OF THE WOMB 
THIS IS POSSIBLE ONLY WHEN 
I BORN HEALTHY ONLY THEN 
SO I APPEAL TO MY DOCTOR FRIENDS 
DO INVESTIGATE ON ME BEOFRE JOURNEY ENDS 
START WITH GENETIC COUNSELLING WITH MOM 
BEFORE I ARRIVE IN THE WOMB 
DO MOM’S HAEMOGRAM BLOOD TEST 
TAKE MCV &MCH CRITERIA IN SET 
IF MCV LESS THAN 75 & MCH LESS THAN 25 INDICE 
THEN GO FOR ESTIMATION OF HbA2 IN PRECISE 
IF VALUE COMES TO BE MORE THAN 3.5 PERCENT 
LABLE MY MOM AS THALASSAEMIA CARRIER INSTANT 
ADVISE FOR MY DAD’S CARRIER SCREEN TEST 
IF COMES POSITIVE , GO FOR MY PRENATAL TEST 
DO CVS AT 12 WEEKS OF MY GESTATIONAL LIFE 
TAKE OUT VILLOUS TISSUE BY SMALL NEEDLE PIPE 
SENT CVS TO GENETIC LAB FOR GENE MUTATION ANALYSIS 
ALONG WITH REPORT OF MY PARENT’S BLOOD ANALYSIS 
IF I STOOD THALASSAEMIA CARRIER OR NORMAL 
CONTINUE MY JOURNEY IN THE WOMB AS USUAL 
IF MY REPORT SHOW MUTATION FOR THALASSAEMIA DISORDER 
TAKE ME OUT OF WOMB TO PREVENT THIS GENETIC DISOREDR 
THIS WILL BE VERY PAINFUL TO MY MOM & DAD 
FOR ME ALSO, NOT TO GET ENTERY IN THIS WORLD 
HENCE I APPEAL TO YOU ALL MY DEAR 
GO FOR PREMARITAL SCREENING WITHOUT FEAR 
SO THAT MY LIFE NEVER COMES IN DANGER ZONE 
AND I COMLPETE MY JOURNEY HAPPILY IN THE WOMB 
I WOULD LIKE TO SEE ALL PARENTS WITH HAPPY & SMILLING FACE 
AND MY NATION WILL SHINE AS THALASSAEMIA FREE IN WORLD RACE 
.
“INVITATION” 
13THBIENNIAL CONFERENCE OF 
“ISPAT” 
JODHPUR 
SUN CITY OF INDIA 
13THBIENNIAL CONFERENCE OF 
JODHPUR 
SUN CITY OF INDIA

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Thalassemia free india 2014

  • 1.
  • 2.
  • 3.
  • 4.
  • 5.
  • 6. Haema is Greek for blood. Thalassa is Greek for the sea.
  • 7.
  • 8. 2ᶑ& 2 βchain 97% Adult haemoglobin After birth Hb F is replaced by Hb A By six months of age HbF: 2ᶑ& 2 ϒchain At birth HbFis 70-90%, That fall to 25% by one month & <2% by one year of age HbA2 : 2ᶑ& 2δchain 1.5 to <3.5% in normal adult Types of Haemoglobin
  • 9. The Gene of Alpha chain is located on Chromosome 16. Molecular aspect of Thalassaemia The Gene of Beta chain is located on Chromosome 11.
  • 10. SEQUENCE OF BASES - “GENE” Molecular aspect of Thalassaemia T C G A T G A G C T A C Substitution, Deletion , Insertion of base pair of a gene results in another sequence of GENE called “ GENE MUTATION”.
  • 11. Mutation causes either decrease or absent synthesis of globin protein . •Decrease synthesis of Beta globin chain – •Beta Thalassaemia •Decrease synthesis of •Alpha globin chain - •Alpha Thalassaemia
  • 12. •Approximately>200mutationsareknown tocauseThalassemiaallovertheworld. OfthemFivecommonThalassemia mutationsin“INDIA”are– •(IVS)1-S (G ->C) •IVS 1 -1 (G->T) •619 bp DELETION •+1 Codon 8/9(+G) •-Codon 41/42(-CTTT) Beta -Thalassaemia Major
  • 14.
  • 15.
  • 16.
  • 17. Repeated BT causes iron load. Desferoxamine is Given S.C. for 8 hours every day for 5-6 days a week so as to chelate iron load.
  • 18. In 15 years of life span
  • 19.
  • 20.
  • 21.
  • 22.
  • 23.
  • 24. Preventing the Birth of a “Thalassaemia” child is the only answer to this world wide problem
  • 25. How does the birth of a thalassemia child occur ?
  • 26. When both partners are carrier ,there is 25% chance of child to be affectectdwith Thalessaemiain each pregnancy CARRIER 50 % CARRIER 25% NORMAL 25% T .MAJOR CARRIER
  • 27. But when only one partner is carrier then no child will be affected with Thaessemia CARRIER 50 % CARRIER NORMAL 50% NORMAL
  • 28. -Carriers are Asymptomatic -They are silent culprit
  • 29.
  • 30.
  • 31. Hb11.5 gm% MCV60.6 MCH 18.6 MENTZER INDEX -MCV/TRBC 60.6/6.12 = 9.8
  • 32.
  • 33.
  • 34.
  • 35. GeneticCounseling If marriage is unavoidable due to cultural & social reasons or diagnosed as carriers after marriage or after conception
  • 36. P Then what is the option ? PRENATAL DIAGNOSIS
  • 37. G1P0A0 Dx Haemogram MCV 53.2 MCH 15.8 TRBC5.6 MCV/TRBC = 9. Couple came for consultation at 18 weeks
  • 38. G1P0A0 MCV 60.6 MCH 18.8 TRBC6.12 MCV/TRBC = 9.9 MCV 53.2 MCH 15.8 TRBC5.6 MCV/TRBC = 9. Couple came for consultation at 18 weeks
  • 39. G1P0A0 Thalassemia carrier HbA2 4.6 HbA2 5.5 Couple came for consultation at 18 weeks Thalassemia carrier
  • 40. G1P0A0 Thalassemia carrier Couple came for consultation at 18 weeks Thalassemia carrier Amniocentesis Couple’s blood in EDTA along with amniotic fluid was sent for Gene mutation analysis
  • 41. Invasive C.V.S. Amniocentesis Non Invasive Free fetal DNA in maternal blood PRENATAL DIAGNOSIS
  • 42. Paternal mutant gene Absent Fetus is normal or carrier Continue the pregnancy Paternal mutant gene present Fetus has 50% chance being Thalassaemia Major Massively parallel DNA Sequencing done Maternal blood is collected for Isolation of Fetal DNA fetal DNA is then tested for Paternal mutant gene NONINVASIVE
  • 43. PRENATAL DIAGNOSIS INVASIVE PROCEDURE under USG Guidance by 18 gauge needle Trans abdominal Trans vaginal - Chorionic villous sampling (CVS) 11-14 weeks; Preferably at 11 weeks( 73 Days)
  • 44. PRENATAL DIAGNOSIS Trans abdominal -Ultrasound guided after 16 weeks 22 g needle Initial -2-3 ml is discarded Usually 20cc amniotic fluid Results –2 to 3 weeks AMNIOCENTESIS INVASIVE PROCEDURE
  • 45. Gene mutation in DNA obtained from FETUS is matched with family gene mutation If fetus is normal or carrier for thalassaemia If fetus is thalassaemia Major After genetic counseling couple should be given option for termination of pregnancy Continue pregnancy Gene mutation study Should be done among all carrier for Future family planning after birth
  • 46. G3P1A2 Thalassemia carrier Thalassemia carrier Thalassemia Major
  • 47. Pre-implantation Genetic diagnosis PGDisastateoftheARTprocedureusedininconjunctionwithIVF.InwhichtheembryoistestedforGeneticdisorderspriortobeingplacedinthewombofthewoman-
  • 48. Pre-implantation Genetic diagnosis IVFBiopsy on Day 3Genetic AnalysisTransfer of Unaffected EmbryoNormal Baby-
  • 49. Benefits of Pre-implantation Genetic diagnosis Forcoupleswhohavealreadyanaffectedchild,PGDallowsHLAmatchingforpre- selectionofpotentialdonorprogenyfortheaffectedsiblingwhorequirebonemarrowtransplantation. Psychologicalstressofterminationofpregnancycanbeavoided
  • 50.
  • 51. World wide 240 million people are carriers of β-thalassemia i.e. 1.5% of total world population. Approximately 15 million people are estimated to suffer from “Thalassemia Major”. Every year One lac children are born with thalassemia major
  • 52. On an average 1 person in every 25 Indians is a thalassemia carrier i.e. approximately 30 million people are thalassaemia carrier . Every hour “One” Thalassaemia major child is born i.e. every year approximately10,000 new Thalassaemia patients are born in India.
  • 53. beta-thalassemia trait in India Panjab 6.5% Delhi 2.2 -9.2% LarkanSindhi 17% DaduSindhi 8% Bhanishali15% Lohana13.6% Kerala 0.6% Assam 5 % Gujarat 10-15%
  • 54. TO REDUCE TO PREVENT TO SET UP TO DIAGNOSE
  • 55.
  • 56. Lack of Education Lack of experts Social factors Lack of National policy lack of Fetal medicine Centre Lack Genetic entre lack of Funds lack of Screening
  • 57. Lack of Education Illiteracy is a big challenge for prevention of ThalassaemiaIn India
  • 58. Lack of Education lack of Pre marital screening Detection of Carrier state seems to be is a “stigma” to their life and may Affect their marriages hence deprived of it. Lack of Pre-conception counseling– Even When family is having affected Child, Couple have unplanned pregnancy due lack of knowledge & fund for Screening methods.
  • 59. Lack of Education They do not have early antenatal Booking Hence deprived of prenatal screening And prenatal diagnostic care for Thalassaemia
  • 60. Lack of knowledge & attitude Of pregnant woman & her family
  • 61. Challenges of Social factors Consanguineous Marriage Marriage among Close blood relative is a big hurdle for prevention of Thalassaemia. Feticide is “SIN”Hence they avoid termination of even when fetus is affected.
  • 62. Lack of well equipped laboratory
  • 63. Lack of genetic laboratory
  • 64. Challenges of Economic burden Fund for Education, Training and awareness programmes Fetal medicine Centre 50 -70 lacs Lab -Cell counter 08-10 lacs -HPLC 70-80 lacs Genetic lab 25-75 lacs
  • 65. Economic burden on patients
  • 66.
  • 67.
  • 68.
  • 69.
  • 70.
  • 71.
  • 72. Mass screening : Means screening of each individuals for thalassemia in reproductive age group (15 to 45 years)
  • 73.
  • 74.
  • 75.
  • 76. P Report should be high lighted with logo of ‘Thalassemia free India”. Should calculate the Mentzer index and include it in haemogramreport Should highlight the MCV, MCH, TRBC indices in haemogramreport
  • 77.
  • 78. 3.Casscade screening : Screening of relatives of index Thalassemia major
  • 79. Government should formulate a policy for implementation of universal Thalassaemia screening programme“FREE OF COST” for infants, school and college going children, And those attending preconceptional and antenatal clinics. “Registration of marriage by the court should be done only when Blood report of Thalassemia screening is produced”
  • 80. Like “Janani surksha yojana” the government should formulate the policy Of “ SWASTH SHISHU YOJANA” to prevent the birth of child with “THALASSEMIA” by providing prenatal diagnostic facility “FREE OF COST” at each and every corner of our country. Psychological and financial support should be given to the pregnant women for safe termination of pregnancy if the fetus is affected with Thalassemia major.
  • 81.
  • 82.
  • 84.
  • 85. I AM A SMALL AND PRETTY CREATURE WILL SOON COME TO THIS WORLD IN FUTURE. BUT WOULD LIKE TO SEE SMILING DAD AND MOM WHEN I COME OUT OF THE WOMB THIS IS POSSIBLE ONLY WHEN I BORN HEALTHY ONLY THEN SO I APPEAL TO MY DOCTOR FRIENDS DO INVESTIGATE ON ME BEOFRE JOURNEY ENDS START WITH GENETIC COUNSELLING WITH MOM BEFORE I ARRIVE IN THE WOMB DO MOM’S HAEMOGRAM BLOOD TEST TAKE MCV &MCH CRITERIA IN SET IF MCV LESS THAN 75 & MCH LESS THAN 25 INDICE THEN GO FOR ESTIMATION OF HbA2 IN PRECISE IF VALUE COMES TO BE MORE THAN 3.5 PERCENT LABLE MY MOM AS THALASSAEMIA CARRIER INSTANT ADVISE FOR MY DAD’S CARRIER SCREEN TEST IF COMES POSITIVE , GO FOR MY PRENATAL TEST DO CVS AT 12 WEEKS OF MY GESTATIONAL LIFE TAKE OUT VILLOUS TISSUE BY SMALL NEEDLE PIPE SENT CVS TO GENETIC LAB FOR GENE MUTATION ANALYSIS ALONG WITH REPORT OF MY PARENT’S BLOOD ANALYSIS IF I STOOD THALASSAEMIA CARRIER OR NORMAL CONTINUE MY JOURNEY IN THE WOMB AS USUAL IF MY REPORT SHOW MUTATION FOR THALASSAEMIA DISORDER TAKE ME OUT OF WOMB TO PREVENT THIS GENETIC DISOREDR THIS WILL BE VERY PAINFUL TO MY MOM & DAD FOR ME ALSO, NOT TO GET ENTERY IN THIS WORLD HENCE I APPEAL TO YOU ALL MY DEAR GO FOR PREMARITAL SCREENING WITHOUT FEAR SO THAT MY LIFE NEVER COMES IN DANGER ZONE AND I COMLPETE MY JOURNEY HAPPILY IN THE WOMB I WOULD LIKE TO SEE ALL PARENTS WITH HAPPY & SMILLING FACE AND MY NATION WILL SHINE AS THALASSAEMIA FREE IN WORLD RACE .
  • 86.
  • 87.
  • 88. “INVITATION” 13THBIENNIAL CONFERENCE OF “ISPAT” JODHPUR SUN CITY OF INDIA 13THBIENNIAL CONFERENCE OF JODHPUR SUN CITY OF INDIA