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Alloimmune Hemolytic Disease Of The Fetus / Newborn: Rh Isoimmunization

Alloimmune Hemolytic Disease Of The Fetus / Newborn: Rh Isoimmunization. Professor Hassan A Nasrat Department of Obstetrics and Gynecology Faculty of Medicine King Abdul-Aziz University. Alloimmune Hemolytic Disease Of The Fetus / Newborn:. Definition:

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Alloimmune Hemolytic Disease Of The Fetus / Newborn: Rh Isoimmunization

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  1. Alloimmune Hemolytic Disease Of The Fetus / Newborn: Rh Isoimmunization Professor Hassan A Nasrat Department of Obstetrics and Gynecology Faculty of Medicine King Abdul-Aziz University

  2. Alloimmune Hemolytic Disease Of The Fetus / Newborn: Definition: A condition in which the Red Cells Of The Fetus Or Newborn Are Destroyed By Maternally Derived Alloantibodies • The Antibodies Arise In The Mother As The Direct Result Of A Blood Group Incompatibility Between The Mother And Fetus. • The mother become Isoimmunized. • In The Fetus: Erythroblastosis Fetalis • In The Newborn: HDN.

  3. Antibodies That May Be Detected During Pregnancy: • Innocuous Antibodies: • Most Of These Antibody Are IgM Therefore Cannot Cross The Placental Barrier • Antibodies Capable Of Causing Significant Hemolytic Transfusion Reactions: • IgG antibodies, Their Corresponding Antigens Are Not Well Developed At Birth E.g. Lu (b), Yt (a), And VEL — • Antibodies That Are Responsible For HDN : • Anti-c, Anti-d, Anti-e, And Anti-k (Kell)

  4. ISO: is a prefix means similar, equal or uniform. Isoimmunization: is the process of immunizing a species with antigen derived from the same subject.

  5. Distribution of Rh negative Blood Group • RhD D negativity primarily occurs among Caucasians; the average incidence is 15 percent in this group. • Examples of the blood group distribution in various populations are illustrated below: •    Basques — 30 to 35 percent   Finland — 10 to 12 percent   American blacks — 8 percent   Indo-Eurasians — 2 percent   Native Americans and Inuit Eskimos — 1 to 2 percent. • Local Studies (population) + 8%

  6. The RH Antigen – Biochemical and Genetic Aspects • Mechanism of Development of Maternal Rh Isoimmunization • Natural History of Maternal isoimmunization /HD of the Newborn • Pathogenesis of Fetal Erythroblastosis Fetalis • Diagnosis of Rh isoimmunization

  7. The RH Antigen – Biochemical and Genetic Aspects

  8. The Rh Antigen- Biochemical Aspects: • The Rh Antigen Is A Complex Lipoprotein. Distributed Throughout The Erythrocyte Membrane In A Nonrandom Fashion • It Can Not Be Seen By Routine Microscopy, But Can Be Identified By Specific Antisera Function of the Rh antigen: Its Precise Function Is Unknown. Rh Null Erythrocytes Have Increased Osmotic Fragility And Abnormal Shapes.

  9. The RH Antigen- Genetic Aspect • The Rh gene complex is located on the distal end of the short arm of chromosome one. • A given Rh antigen complex is determined by a specific gene sequence inherited in a Mendelian fashion from the parents. one haploid from the mother and one from the father. • Three genetic loci, determine the Rh antigen (i.e. Rh blood group). • Each chromosome will be either D positive or D negative (there is no "d" antigen), C or c positive, and E or e positive.

  10. Genetic Expression (Rh Surface ProteinAntigenicity): Grades Of “Positively” Due To Variation In The Degree Genetic Expression Of The D Antigen. Incomplete Expression May Result In A Weakly Positive Patient e.g. Du Variant Of Weakly Rh Positive Patient (They May Even Be Determined As Rh Negative). A Mother With Du Rh Blood Group (Although Genetically Positive) May Become Sensitized From A D-positive Fetus Or The Other Way Around May Take Place.

  11. Genetic Expression (Rh Surface ProteinAntigenicity): Du Variant Frank D Positive Incomplete Expression Of The D Antigen Result In A Weakly Positive Patient e.g. Du Variant Of Weakly Rh Positive Patient.

  12. Factors Affect The Expression Of The Rh Antigen • The Number Of Specific Rh-antigen Sites: • - The Gene Dose, • - The Relative Position Of The Alleles, • - The Presence Or Absence Of Regulator Genes. • Interaction Of Other Components Of The Rh Blood Group. Erythrocytes Of Individuals Of Genotype Cde/cde Express Less D Antigen Than Do The Erythrocytes Of Individuals Of Genotype cDE/cde. • The Exposure Of The D Antigen On The Surface Of The Red Cell Membrane.

  13. Phenotype Genotype eCd/EcD D positive • Antigenicity of the Rh surface protein: • genetic expression of the D allele. • Number of specific Rh antigen sites. • Interaction of components of the Rh gene complex. • Exposure of the D antigen on the surface of the red cell e C d E c D

  14. Mechanism of Development of Maternal Rh Isoimmunization

  15. The Mechanism of Development of the Rh Immune Response: Fetal RBC with Rh +ve antigen Maternal circulation of an Rh –ve mother The Rh +ve antigen will be cleared by macrophages; processed and transferred to plasma stem cell precursors (Develop an almost permanent immunologic memory) (Primary immune response) With subsequent exposure the plasma cell line proliferate to produce humeral antibodies (Secondary immune response).

  16. The Primary Response: • Is a slow response (6 weeks to 6 months). • IgM antibodies • a molecular weight of 900,000 that does not cross the placenta. • The Secondary Response: • Is a Rapid response • IgG antibodies • a molecular weight of 160,000 that cross the placenta.

  17. Exposure to maternal antigen in utero “the grandmother theory”: Explains the development of fetal isoimmunization in a primigravida, who has no history of exposure to incompatible Rh blood. Rh negative Fetus and the mother is Rh positive The Fetus is exposed to the maternal Rh antigen through maternal-fetal transplacental bleed. The fetus immune system develop a permanent template (memory) for the Rh-positive antigen. When the fetus becomes a mother herself and exposed to a new load of D antigen from her fetus (hence the grandmother connection) the immune memory is recalled and a secondary immune response occur.

  18. Mother 1. Cleared by Macrophage Primary Response 2. Plasma stem cells • 6 wks to 6 M. • IGM. IGM antibodies Placental The First Pregnancy is not Affected

  19. Mother Macroph. antigen Presenting cell T- helper cell Secondary Response • Small amount • Rapid • IgG B cell IgG Anti - D Placental Fetal Anemia

  20. Mother Macroph. Antigen Presenting Cell Group “O” Rh Negative T-Hellper Anti - A Anti - B B-cell Anti-D Placenta B Rh positive A Rh Positive Infant “O” Rh positive

  21. Natural History of Maternal isoimmunization /HD of the Newborn

  22. Natural History of Rh Isoimmunization And HD Fetus and Newborn • Without treatment: • less than 20% of Rh D incompatible pregnancies actually lead to maternal isoimmunization • 25-30% of the offspring will have some degree of hemolytic anemia and hyperbilirubinemia. • 20-25% will be hydropic and often will die either in utero or in the neonatal period. • Cases of hemolysis in the newborn that do not result in fetal hydrops still can lead to kernicterus.

  23. The Risk of development of Fetal Rh-disease is affected by: Less than 20% of Rh D incompatible pregnancies actually lead to maternal alloimmunization • The Husband Phenotype And Genotype (40 % Of Rh Positive Men Are Homozygous And 60% Are Heterozygous). • The Antigen Load And Frequency Of Exposure. • ABO Incompatibility

  24. Why Not All the Fetuses of Isoimmunized Women Develop the Same Degree of Disease? • Expression Of The Rh Antigen: • Classes Of IgG Family • The Non-responders: • ABO Incompatibility:

  25. Pathogenesis of Fetal Erythroblastosis Fetalis

  26. Rh Antibodies Antibodies Coated Red Cells Destruction of Fetal Cells by Fetal RES Fetal Anemia Fetal Hypoxia and Stimulate of Erythropoietin Extra Medullary Red Cells Synthesis Hepatomegaly Hepatic Cell Failure Hypoproteinemia, Increased Intrahepatic Pressure, Portal hypertension Ascites, Edema, hypoxia, Placental Thickness, Polyhydramnios, Pericardial effusion

  27. Complications of Fetal-Neonatal Anemia: • Fetal Hydrops And IUFD • Hepatosplenomegaly • Neonatal Jaundice • Compilations Of Neonatal Kernicterus (Lethargy, Hypertonicity, Hearing Loss, Cerebral Palsy And Learning Disability) • Neonatal Anemia

  28. Management - Prevention: • Treatment:

  29. Prevention of Rh Isoimmunization • Screening all women for D Factor and antibodies • Prophylaxis (Anti D Immunoglobulin) only for those who are negative for antibodies • Anti D Is given 72 hours after delivery, 28-32 weeks, and any other time when there is risk of Fetomaternal Bleeding The dose of Immunoglobulin depends the volume of Blood

  30. Dose of prophylactic Anti-D Ig: 10 mcg of anti-D Ig should be administered for every mL of fetal blood in the maternal circulation. Thus, the 300-mcg dose covers hemorrhage volumes up to 30 mL of whole fetal blood. In the less than 1% of cases where the volume of fetomaternal hemorrhage exceeds 30 mL, utilizing the Kleihauer-Betke test to quantitate the volume of fetal blood in the maternal circulation and administer the appropriate amount of anti-D.

  31. MONOCLONAL ANTI-D • Most polyclonal RhiG comes from male volunteers who are intentionally exposed to RhD-positive red blood cells. • Potential Problems: • infectious risk • solve supply problems. • ethical issues • anti-D monoclonal antibody: • Although monoclonal anti-D is promising, it cannot be recommended at this time as a replacement for polyclonal RhIg.

  32. The amount of fetal cells in maternal blood: The Kleihauer-Braun-Betke Test

  33. Management of cases of Rh isoimmunization • Diagnosis Of RH Isoimmunization • Evaluation of Fetal Condition

  34. Diagnosis of Rh isoimmunization The diagnose is Based on the presence of anti-Rh (D) antibody in maternal serum. • Methods of Detecting Anti D Antibodies in Maternal Serum: • The Enzymatic Method • The Antibody Titer In Saline, In Albumin • The Indirect Coombs Tests.

  35. Diagnosis Maternal Isoimmunization Antibody Titre in Saline: RhD-positive cells suspended in saline solution are agglutinated by IgM anti-RhD antibody, but not IgG anti-RhD antibody. Thus, this test measure IgM, or recent antibody production. Antibody Titre in Albumin: Reflects the presence of any anti-RhD IgM or IgG antibody in the maternal serum. • The Indirect Coombs Test: • First Step: • RhD-positive RBCs are incubated with maternal serum • Any anti-RhD antibody present will adhere to the RBCs. • Second Step: • The RBCs are then washed and suspended in serum containing antihuman globulin (Coombs serum). • Red cells coated with maternal anti-RhD will be agglutinated by the antihuman globulin (positive indirect Coombs test).

  36. The Direct Coombs Test Is Done After Birth To Detect The Presence Of Maternal Antibody On The Neonate's RBCs. The Infant's RBCs Are Placed In Coombs Serum. If The Cells Are Agglutinated This Indicate The Presence Of Maternal Antibody

  37. Fetal Rhesus Determination • RHD Type And Zygosity (If RHD-positive) Of The Father • Amniocentesis To Determine The Fetal Blood Type Using The Polymerase Chain Reaction (PCR) • Detection Of Free Fetal RHD DNA (FDNA) Sequences In Maternal Plasma Or Serum Using PCR • Flow Cytometry Of Maternal Blood For Fetal Cells

  38. Management of cases of Rh isoimmunization • Diagnosis Of RH Isoimmunization • Evaluation of Fetal Condition

  39. Goals of managing Fetal Alloimmunization: • Initially detecting fetal anemia prior to the occurrence of fetal compromise. • Minimize fetal morbidity and mortality by correcting this anemia until fetal lung maturity and delivery can be achieved.

  40. Evaluation of Fetal Condition • Past Obstetric History • Measurements Of Antibodies in Maternal Serum • Determination of Fetal Rh Blood Group • Ultrasonography • Amniocentesis • Fetal Blood Sampling

  41. Past Obstetric History: Although not reliably accurate in predicting severity of fetal disease, past obstetrical history can be somewhat prognostic

  42. Maternal Anti-D Titer • Antibody Titer Is A Screening Test. • A Positive Anti-d Titer Means That The Fetus Is At Risk For Hemolytic Disease, Not That It Has Occurred Or Will Develop. • Variation In Titer Results Between Laboratories And Intra Laboratory Is Common. • A Truly Stable Titer Should Not Vary By More Than One Dilution When Repeated In A Given Laboratory.

  43. Ultrasound Image of Transabdominal Chorion Villus Sampling

  44. Ultrasonography: • To Establish The Correct Gestational Age. • In Guiding Invasive Procedures And Monitoring Fetal Growth And Well-being. • Ultrasonographic Parameters To Determine Fetal Anemia: • Placental Thickness. • Umbilical Vein Diameter • Hepatic Size. • Splenic Size. • Polyhydramnios. • Fetal Hydrops (e.g. Ascites, Pleural Effusions, Skin Edema).

  45. Doppler Velocimetry Of The Fetal Middle Cerebral Artery (MCA) Anemic Fetus Preserves Oxygen Delivery To The Brain By Increasing Cerebral Flow Of Its Already Low Viscosity Blood. • For Predicting Fetal Anemia • To Predict The Timing Of A Second Intrauterine Fetal Transfusion.

  46. Invasive Techniques ( Amniocentesis and Fetal Blood Sampling): Indications: • A Critical Anti-D Titer: • I.E. A Titer Associated With A Significant Risk For Fetal Hydrops. Anti-D Titer Value Between 8 And 32 • Previous Seriously Affected Fetus Or Infant (e.g. Intrauterine Fetal Transfusion, Early Delivery, Fetal Hydrops, Neonatal Exchange Transfusion).

  47. Amniocentesis • Normally Bilirubin In Amniotic Fluid Decreases With Advanced Gestation. • It Derives From Fetal Pulmonary And Tracheal Effluents. • Its Level Rises in Correlation With Fetal Hemolysis. Determination Of Amniotic Fluid Bilirubin: By The Analysis Of The Change In Optical Density Of Amniotic Fluid At 450 nm On The Spectral Absorption Curve (delta OD450) Procedures Are Undertaken At 10-15 Days Intervals Until Delivery Data Are Plotted On A Normative Curve Based Upon Gestational Age.

  48. Ultrasound image of amniocentesis at 16 weeks of gestation

  49. Extended Liley graph.

  50. Queenan curve (Deviation in amniotic fluid optical density at a wavelength of 450 nm in Rh-immunized pregnancies from 14 to 40 weeks' gestation)

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