Download presentation
Published byMeryl Nelson Modified over 9 years ago
1
In Vitro Fertilization and Preimplantation Genetic Diagnosis
Adrianna Vlachos, MD DBA Camp 2015
2
In Vitro Fertilization and Pre-Implantation Genetic Diagnosis
Goal: Child unaffected by a genetic (hereditary) illness defined by a known genetic mutation Secondary goal: “Creating” a child unaffected by the genetic illness who is a transplant donor for the affected child
3
In Vitro Fertilization and Pre-Implantation Genetic Diagnosis
IVF Hormonal therapy to the mother to get many eggs for ovulation Number of eggs depends on age of mother Side effects of these medications to mother Eggs harvested (under anesthesia) Eggs are fertilized with sperm outside of mother (“in the test tube”)
4
In Vitro Fertilization and Pre-Implantation Genetic Diagnosis
PGD Fertilized egg reaches 8-cell stage One cell taken for RP/HLA testing “RP neg, HLA matched” fertilized egg implanted in mother (1/8 chance) Hormonal therapy to continue pregnancy, usually until weeks CVS (10 wks) or Amnio (18 wks) for confirmation
5
Pre-natal vs Pre-implantation diagnosis
Dr. I. Souter, MGH Fertility Center
6
Pre-natal Diagnosis Amniocentesis Chorionic Villus Sampling (CVS)
7
Pre-implantation Diagnosis
Introduced initially in 1990 Biopsy of a single cell per embryo followed by its genetic diagnosis through different techniques the subsequent replacement to the patient of those embryos classified by genetic diagnosis as unaffected
8
PGD Indications Primary Goal Procedure is offered to couples:
With known single gene disorders that can be detected by PGD - DBA With known chromosomal abnormalities that can be detected by PGD requesting sex selection for X-linked disorders – DBA
9
PGD Indications Secondary Goal
Requesting PGD for HLA-typing (to allow selection of embryos that are histocompatible with live siblings)
10
Single Gene Disorders
11
PGD Process Ovulation Induction Retrieval Fertilization
Embryo Bx on Day-3 Genetic Analysis Embryo Transfer
12
Ovulation induction
13
Oocyte Retrieval
14
Fertilization Conventional Insemination
Intracytoplasmic Sperm Injection (ICSI)
15
Embryo Culture
16
Day 3/Cleavage Stage Embryo
17
Cleavage Stage Biopsy
18
Genetic Analysis/PCR DNA amplification Mutation Characterization
sequence harboring the mutation Mutation Characterization FISH PCR HLA Matching
19
Embryo Transfer
20
Early Pregnancy
21
Risks Embryo damage Oocyte and Embryo Biopsy are invasive procedures Misdiagnosis False negative result False positive result The chance for NO result The chance for mosaicism IVF Risks Not Achieving Pregnancy There may not be any normal embryos available for transfer. The embryos may not implant and develop even if they do not have the defect. The workup for PGD is expensive and labor intensive PGD can only detect a specific genetic disease in an embryo. It cannot detect many genetic disorders at a time and cannot guarantee that the fetus will not have an unrelated birth defect. . The Risk of Embryo Biopsy While PGD is a relatively new procedure in IVF, the micromanipulation or biopsy techniques required to perform the procedure have been in use for many years. The risk of accidental damage to an embryo during removal of the cell(s) is very low %. Concerns have been expressed regarding the development and viability of the embryo after biopsy Studies have shown that biopsy at the 8 cell stage has no detrimental effects on further growth The balance between potential biopsy damage and beneficial effects of PGD seems to be positive. The other risks include those common to all IVF treatments - and these include: OHSS ( ovarian hyperstimulation syndrome), ectopic pregnancy and multiple pregnancy Misdiagnosis Mosaicism is defined as the embryo having cells with different chromosome make up. Typically, all cells of the embryo have the same chromosomal make up as they originate from the same fertilized egg. However , it is possible for cells of the same embryo to have differing numbers of chromosomes. . If we analyze a cell that has normal chromosomal content, but another cell has an extra chromosome, we erroneously diagnosed that embryo as being chromosomally normal. Due to the chance of misdiagnosis as well as the presence of anueploidy for which we do not test, we recommend prenatal testing as stated earlier. What Is The Reliability of PGD? There is a small error rate with PGD due to the complexity of testing a single cell in the laboratory.. It must be stressed that this technology is still considered experimental. For this reason, prenatal testing by chorionic villus sampling or amniocentesis is required by the PGD laboratory to confirm their diagnosis. PGD can only detect a specific genetic disease in an embryo. It cannot detect many genetic disorders at a time and cannot guarantee that the fetus will not have an unrelated birth defect. Patients opting for PGD have to be aware of the limitations Conventional prenatal diagnosis still needs to be recommended to patients to confirm PGD results by amniocentesis or CVS. they have to go through IVF even though they may be fertile, the workup of new diagnosis for PGD is labour intensive, expensive and may take some time, Single cell PCR is a technically challenging procedure as it is at risk of contamination and allele dropout (ADO). Since only 1 cell is amplified, if another cell or piece of DNA enters the tube, it will also be amplified. Therefore ICSI is used to ensure that there are no excess sperm present (paternal contamination) and all of the cumulus cells have to be carefully removed (maternal contamination). Stringent conditions have to be employed to ensure that no other contamination results No part of the future fetus will be lacking because one or two cells are removed form the embryo approximately 2 days after fertilization. All the cells of the embryo remain totipotent until after the fourth day which means having all the potential into growing into a whole fetus. The accuracy of the PGD for translocation is 90%.
22
Summary Before PGD is performed, genetic counseling must be provided to ensure that patients fully understand the risk for having an affected child the impact of the disease the available options the multiple technical limitations including the possibility of an erroneous result Prenatal diagnostic testing is strongly encouraged to confirm the results of PGD
23
Conclusions It is a personal choice!!!
This requires identification of your family’s DBA gene. Obstacles Practical Religious Ethical Financial There are other options available Adoption Sperm/egg donation Just having a baby
Similar presentations
© 2024 SlidePlayer.com. Inc.
All rights reserved.