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Rh disease

March 07, 2023

Rh disease (also known as rhesus isoimmunization, Rh (D) disease, and blue baby disease) is a type of hemolytic disease of the fetus and newborn (HDFN). HDFN due to anti-D antibodies is the proper and currently used name for this disease as the Rh blood group system actually has more than 50 antigens and not only the D-antigen. The term "Rh Disease" is commonly used to refer to HDFN due to anti-D antibodies, and prior to the discovery of anti-Rho(D) immune globulin, it was the most common type of HDFN. The disease ranges from mild to severe, and occurs in the second or subsequent pregnancies of Rh-D negative women when the biologic father is Rh-D positive.

Rh disease
Other namesRhesus isoimmunization
SpecialtyPaediatrics, haematology, transfusion medicine

Due to several advances in modern medicine, HDFN due to anti-D is preventable by treating the mother during pregnancy and soon after delivery with an injection of anti-Rho(D) (RhoGam) immune globulin. With successful mitigation of this disease by prevention through the use of anti-Rho(D) immune globulin, other antibodies are more commonly the cause of HDFN today.

Signs and symptoms

Symptoms of Rh disease include yellowish amniotic fluid and enlarged spleen, liver or heart or buildup of fluid in the abdomen of the fetus.[1]

Pathophysiology

During the first pregnancy, the Rh- mother's initial exposure to fetal Rh+ red blood cells (RBCs) is usually not sufficient to activate her Rh-recognizing B cells. However, during delivery, the placenta separates from the uterine wall, causing umbilical cord blood to enter the maternal circulation, which results in the mother's proliferation of IgM-secreting plasma B cells to eliminate the fetal Rh+ cells from her blood stream. IgM antibodies do not cross the placental barrier, which is why no effects to the fetus are seen in first pregnancies for Rh-D mediated disease. However, in subsequent pregnancies with Rh+ fetuses, the IgG memory B cells mount an immune response when re-exposed, and these IgG anti-Rh(D) antibodies do cross the placenta and enter fetal circulation. These antibodies are directed against the Rhesus (Rh) factor, a protein found on the surface of the fetal RBCs. The antibody-coated RBCs are destroyed by IgG antibodies binding and activating complement pathways.[2]

The resulting anemia has multiple sequelae:[3][4][5]

  1. The immature hematopoietic system of the fetus is taxed as the liver and spleen attempt to put immature RBCs into circulation (erythroblasts, thus the previous name for this disease erythroblastosis fetalis).
  2. As the liver and spleen enlarge under this unexpected demand for RBCs, a condition called portal hypertension develops, and this taxes the immature heart and circulatory system.
  3. Liver enlargement and the prolonged need for RBC production results in decreased ability to make other proteins, such as albumin, and this decreases the plasma colloid oncotic pressure leading to leakage of fluid into tissues and body cavities, termed hydrops fetalis.
  4. The severe anemia taxes the heart to compensate by increasing output in an effort to deliver oxygen to the tissues and results in a condition called high output cardiac failure.
  5. If left untreated, the result may be fetal death.

The destruction of RBCs leads to elevated bilirubin levels (hyperbilirubinemia) as a byproduct. This is not generally a problem during pregnancy, as the maternal circulation can compensate. However, once the infant is delivered, the immature system is not able to handle this amount of bilirubin alone and jaundice or kernicterus (bilirubin deposition in the brain) can develop which may lead to brain damage or death. Sensitizing events during pregnancy include c-section, miscarriage, therapeutic abortion, amniocentesis, ectopic pregnancy, abdominal trauma and external cephalic version. However, in many cases there was no apparent sensitizing event. Approximately 50% of Rh-D positive infants with circulating anti-D are either unaffected or only mildly affected requiring no treatment at all and only monitoring. An additional 20% are severely affected and require transfusions while still in the uterus. This pattern is similar to other types of HDFN due to other commonly encountered antibodies (anti-c, anti-K, and Fy(a)).[citation needed]

Diagnosis

Maternal blood

In the United States, it is a standard of care to test all expecting mothers for the presence or absence of the RhD protein on their RBCs. However, when medical care is unavailable or prenatal care not given for any other reason, the window to prevent the disease may be missed. In addition, there is more widespread use of molecular techniques to avoid missing women who appear to be Rh-D positive but are actually missing portions of the protein or have hybrid genes creating altered expression of the protein and still at risk of HDFN due to Anti-D.[6][7]

  • At the first prenatal visit, the mother is typed for ABO blood type and the presence or absence of RhD using a method sensitive enough to detect weaker versions of this antigen (known as weak-D) and a screen for antibodies is performed.
    • If she is negative for RhD protein expression and has not formed anti-D already, she is a candidate for RhoGam prophylaxis to prevent alloimmunization.
    • If she is positive for anti-D antibodies, the pregnancy will be followed with monthly titers (levels) of the antibody to determine if any further intervention is needed.
  • A screening test to detect for the presence or absence of fetal cells can help determine if a quantitative test (Kleihauer-Betke or flow cytometry) is needed. This is done when exposure is suspected due to a potential sensitizing event (such as a car accident or miscarriage).
  • If the screening test is positive or the appropriate dose of RhoGam needs to be determined, a quantitative test is performed to determine a more precise amount of fetal blood to which the mother has been exposed.
    • The Kleihauer–Betke test or Flow Cytometry on a maternal blood sample are the most common ways to determine this, and the appropriate dose of RhoGam is calculated based on this information.
  • There are also emerging tests using Cell-free DNA. Blood is taken from the mother, and using PCR, can detect fetal DNA.[7] This blood test is non-invasive to the fetus and can help determine the risk of HDFN. Testing has proven very accurate and is routinely done in the UK at the International Blood Group Reference Laboratory in Bristol.[8]

Paternal blood

Blood is generally drawn from the father to help determine fetal antigen status.[9] If he is homozygous for the antigen, there is a 100% chance of all offspring in the pairing to be positive for the antigen and at risk for HDFN. If he is heterozygous, there is a 50% chance of offspring to be positive for the antigen.[10]

Prevention

In an RhD negative mother, Rho(D) immune globulin can prevent temporary sensitization of the maternal immune system to RhD antigens, which can cause rhesus disease in the current or in subsequent pregnancies. With the widespread use of RhIG, Rh disease of the fetus and newborn has almost disappeared in the developed world. The risk that an RhD negative mother can be alloimmunized by a RhD positive fetus can be reduced from approximately 16% to less than 0.1% by the appropriate administration of RhIG.[citation needed]

Management

As medical management advances in this field, it is important that these patients be followed by high risk obstetricians/maternal-fetal medicine, and skilled neonatologists postpartum to ensure the most up to date and appropriate standard of care[citation needed]

Antenatal

  • Routine prenatal labs drawn at the beginning of every pregnancy include a blood type and an antibody screen. Mothers who are Rh negative (A−, B−, AB−, or O− blood types) and have anti-D antibodies (found on the antibody screen) need to determine the fetus's Rh antigen. If the fetus is also Rh negative (A−, B−, AB−, or O− blood types) then the pregnancy can be managed like any other pregnancy. The anti-D antibodies are only dangerous to Rh positive fetuses (A+, B+, AB+, or O+ blood types).
    • The fetal Rh can be screened using non-invasive prenatal testing (NIPT). In the United States, BillionToOne, Inc. offers the Unity test. This test can screen for the fetus's Rh antigen (positive or negative) at the 10th week of gestation using a blood sample drawn from the mother. The Unity test uses NGS technology to look for Rh alleles (genes) in the cell free fetal DNA in the maternal bloodstream. In healthy pregnancies, at least 5% (fetal fraction) of the cell free DNA in the maternal bloodstream comes from the fetus (placenta cells shed DNA into the maternal bloodstream). This small fraction of cell free DNA from the fetus is enough to determine the fetus's Rh antigen.
  • Once a woman has been found to have made anti-D (or any clinically significant antibody against fetal red cells), she is followed as a high risk pregnancy with serial blood draws to determine the next steps
  • Once the titer of anti-D reaches a certain threshold (normally 8 to 16), serial Ultrasound and Doppler examinations are performed to detect signs of fetal anemia
    • Detection of increased blood flow velocities in the fetus are a surrogate marker for fetal anemia that may require more invasive intervention
  • If the flow velocity is found to be elevated a determination of the severity of anemia needs to ensue to determine if an intrauterine transfusion is necessary
    • This is normally done with a procedure called percutaneous umbilical cord blood sampling (PUBS or cordocentesis) [11]
  • Intrauterine blood transfusion[citation needed]
    • Intraperitoneal transfusion—blood transfused into fetal abdomen
    • Intravascular transfusion—blood transfused into fetal umbilical vein—This is the method of choice since the late 1980s, and more effective than intraperitoneal transfusion. A sample of fetal blood can be taken from the umbilical vein prior to the transfusion.
    • Often, this is all done at the same PUBS procedure to avoid the needs for multiple invasive procedures with each transfusion

Postnatal

  • Phototherapy for neonatal jaundice in mild disease
  • Exchange transfusion if the neonate has moderate or severe disease
  • Intravenous Immunoglobulin (IVIG) can be used to reduce the need for exchange transfusion and to shorten the length of phototherapy.[12][13]

History

In 1939 Drs. Philip Levine and Rufus E. Stetson published their findings about a 25-year-old mother who had a stillborn baby that died of hemolytic disease of the newborn.[14] Both parents were blood group O, so the husband's blood was used to give his wife a blood transfusion due to blood loss during delivery. However, she had a severe transfusion reaction. Since both parents were blood group O, which was believed to be compatible for transfusion, they concluded that there must be a previously undiscovered blood group antigen that was present on the husband's red blood cells (RBCs) but not present on his wife's. This suggested for the first time that a mother could make blood group antibodies because of immune sensitization to her fetus's RBCs as her only previous exposure would be the earlier pregnancy. They did not name this blood group antigen at the time, which is why the discovery of the rhesus blood type is credited to Drs. Karl Landsteiner and Alexander S. Wiener[15] with their first publication of their tables for blood-typing and cross-matching in 1940, which was the culmination of years of work. However, there were multiple participants in this scientific race and almost simultaneous publications on this topic. Levine published his theory that the disease known as erythroblastosis fetalis was due to Rh alloimmunization in 1941 while Landsteiner and Wiener published their method to type patients for an antibody causing transfusion reactions, known as “Rh".[16][17][18]

The first treatment for Rh disease was an exchange transfusion invented by Wiener[19] and later refined by Dr. Harry Wallerstein.[20] Approximately 50,000 infants received this treatment. However, this could only treat the disease after it took root and did not do anything to prevent the disease. In 1960, Ronald Finn, in Liverpool, England proposed that the disease might be prevented by injecting the at-risk mother with an antibody against fetal red blood cells (anti-RhD).[21] Nearly simultaneously, Dr. William Pollack,[22] an immunologist and protein chemist at Ortho Pharmaceutical Corporation, and Dr. John Gorman (blood bank director at Columbia-Presbyterian) with Dr. Vincent Freda (an obstetrician at Columbia-Presbyterian Medical Center), came to the same realization in New York City. The three of them set out to prove it by injecting a group of male prisoners at Sing Sing Correctional Facility with antibody provided by Ortho, obtained by a fractionation technique developed by Pollack.[23]

Animal studies had previously been conducted by Dr. Pollack using a rabbit model of Rh.[24] This model, named the rabbit HgA-F system, was an animal model of human Rh, and enabled Pollack's team to gain experience in preventing hemolytic disease in rabbits by giving specific HgA antibody, as was later done with Rh-negative mothers. One of the needs was a dosing experiment that could be used to determine the level of circulating Rh-positive cells in an Rh-negative pregnant female derived from her Rh-positive fetus. This was first done in the rabbit system, but subsequent human tests at the University of Manitoba conducted under Dr. Pollack's direction confirmed that anti-Rho(D) immune globulin could prevent alloimmunization during pregnancy.[citation needed]

Ms. Marianne Cummins was the first at risk woman to receive a prophylactic injection of anti-Rho(D) immune globulin (RHIG) after its regulatory approval.[25] Clinical trials were set up in 42 centers in the US, Great Britain, Germany, Sweden, Italy, and Australia. RHIG was finally approved in England and the United States in 1968.[26] The FDA approved the drug under the brand name RhoGAM, with a fixed dose of 300 µG, to be given within three days (72 hours) postpartum. Subsequently, a broader peripartum period was approved for dosing which included prophylaxis during pregnancy. Within a year, the antibody had been injected with great success into more than 500,000 women. Time magazine picked it as one of the top ten medical achievements of the 1960s. By 1973, it was estimated that in the US alone, over 50,000 babies' lives had been saved. The use of Rh immune globulin to prevent the disease in babies of Rh negative mothers has become standard practice, and the disease, which used to claim the lives of 10,000 babies each year in the US alone, has been virtually eradicated in the developed world. In 1980, Cyril Clarke, Ronald Finn, John G.Gorman, Vincent Freda, and William Pollack each received an Albert Lasker Award for Clinical Medical Research for their work on rhesus blood types and the prevention of Rh disease.[citation needed]

See also

References

  1. ^ "Rh Disease". The Children's Hospital of Philadelphia. 2014-08-23. Retrieved 2021-11-21.{{cite web}}: CS1 maint: url-status (link)
  2. ^ Punt, J., Stranford, S., Jones, P., & Owen, J. A. (2018). Chapter 15: Allergy, Hypersensitivities, and Chronic Inflammation. In Kuby immunology (8th ed., pp. 1086-1087). WH Freeman
  3. ^ Maitra, Anirban (2010). "Diseases of Infancy and Childhood". Robbins and Cotran Pathologic Basis of Disease. The Indian Medical Gazette. Vol. 43. Elsevier. pp. 447–483. doi:10.1016/b978-1-4377-0792-2.50015-8. ISBN 9781437707922. PMC 5182838.
  4. ^ Wong, EC, ed. (2015). Alloimmune cytopenias. In: Pediatric Transfusion: A physician's handbook. 4th ed. AABB. pp. 45–61.
  5. ^ Fung MK, Grossman BJ, Hillyer CD, Westhoff CM, eds (2014). Technical Manual. 18th ed. Bethesda, MD: AABB. {{cite book}}: |last= has generic name (help)CS1 maint: multiple names: authors list (link)
  6. ^ Kacker, Seema; Vassallo, Ralph; Keller, Margaret A.; Westhoff, Connie M.; Frick, Kevin D.; Sandler, S. Gerald; Tobian, Aaron A.R. (2015-03-21). "Financial implications ofRHDgenotyping of pregnant women with a serologic weak D phenotype". Transfusion. 55 (9): 2095–2103. doi:10.1111/trf.13074. ISSN 0041-1132. PMC 4739823. PMID 25808011.
  7. ^ a b Fasano, Ross M. (February 2016). "Hemolytic disease of the fetus and newborn in the molecular era". Seminars in Fetal and Neonatal Medicine. 21 (1): 28–34. doi:10.1016/j.siny.2015.10.006. ISSN 1744-165X. PMID 26589360.
  8. ^ Finning, Kirstin; Martin, Peter; Summers, Joanna; Daniels, Geoff (2007). "Fetal genotyping for the K (Kell) and Rh C, c, and E blood groups on cell-free fetal DNA in maternal plasma". Transfusion. 47 (11): 2126–33. doi:10.1111/j.1537-2995.2007.01437.x. PMID 17958542. S2CID 8292568.
  9. ^ Scheffer, PG; Van Der Schoot, CE; Page-Christiaens, Gcml; De Haas, M (2011). "Noninvasive fetal blood group genotyping of rhesus D, c, E and of K in alloimmunised pregnant women: Evaluation of a 7-year clinical experience". BJOG: An International Journal of Obstetrics & Gynaecology. 118 (11): 1340–8. doi:10.1111/j.1471-0528.2011.03028.x. PMID 21668766. S2CID 32946225.
  10. ^ Transfusion Medicine and Hemostasis: Clinical and Laboratory Aspects ISBN 978-0-12-397788-5[page needed]
  11. ^ "Percutaneous Umbilical Cord Blood Sampling". pennmedicine.adam.com. Retrieved 2019-09-11.
  12. ^ Gottstein, R (2003). "Systematic review of intravenous immunoglobulin in haemolytic disease of the newborn". Archives of Disease in Childhood: Fetal and Neonatal Edition. 88 (1): F6–10. doi:10.1136/fn.88.1.F6. PMC 1755998. PMID 12496219.
  13. ^ Webb, Jennifer; Delaney, Meghan (October 2018). "Red Blood Cell Alloimmunization in the Pregnant Patient". Transfusion Medicine Reviews. 32 (4): 213–219. doi:10.1016/j.tmrv.2018.07.002. ISSN 1532-9496. PMID 30097223. S2CID 51958636.
  14. ^ Levine, Philip; Stetson, Rufus E. (1939). "An Unusual Case of Intra-Group Agglutination". Journal of the American Medical Association. 113 (2): 126–7. doi:10.1001/jama.1939.72800270002007a.
  15. ^ Landsteiner, K.; Wiener, A. S. (1940). "An Agglutinable Factor in Human Blood Recognized by Immune Sera for Rhesus Blood". Experimental Biology and Medicine. 43: 223. doi:10.3181/00379727-43-11151. S2CID 58298368.
  16. ^ Landsteiner, K. (1941-10-01). "STUDIES ON AN AGGLUTINOGEN (Rh) IN HUMAN BLOOD REACTING WITH ANTI-RHESUS SERA AND WITH HUMAN ISOANTIBODIES". Journal of Experimental Medicine. 74 (4): 309–320. doi:10.1084/jem.74.4.309. ISSN 0022-1007. PMC 2135190. PMID 19871137.
  17. ^ LEVINE, P.; VOGEL, P.; KATZIN, E. M.; BURNHAM, L. (1941-10-17). "Pathogenesis of Erythroblastosis Fetalis: Statistical Evidence". Science. 94 (2442): 371–372. Bibcode:1941Sci....94..371L. doi:10.1126/science.94.2442.371. ISSN 0036-8075. PMID 17820878.
  18. ^ Zimmerman, DR (1973). Rh: The Intimate History of a Disease and Its Conquest. Macmillan Publishing Co.
  19. ^ Reid, Marion E. (October 2008). "Alexander S. Wiener: the man and his work". Transfusion Medicine Reviews. 22 (4): 300–316. doi:10.1016/j.tmrv.2008.05.007. ISSN 1532-9496. PMID 18848157.
  20. ^ Wallerstein, H. (1946). "Treatment of Severe Erythroblastosis by Simultaneous Removal and Replacement of the Blood of the Newborn Infant". Science. 103 (2680): 583–584. Bibcode:1946Sci...103..583W. doi:10.1126/science.103.2680.583. PMID 21026828.
  21. ^ Wright, Pearce (2004-06-26). "Ronald Finn". Lancet. 363 (9427): 2195. doi:10.1016/S0140-6736(04)16525-2. ISSN 1474-547X. PMID 15248345. S2CID 2243030.
  22. ^ "William Pollack dies at 87; helped conquer deadly Rh disease". Los Angeles Times. 2013-11-17. Retrieved 2019-09-11.
  23. ^ Freda, V. J.; Gorman, J. G.; Pollack, W. (January 1964). "Successful Prevention of Experimental Rh Sensitization in Man with an Anti-Rh Gamma2-Globulin Antibody Preparation: A Preliminary Report". Transfusion. 4: 26–32. doi:10.1111/j.1537-2995.1964.tb02824.x. ISSN 0041-1132. PMID 14105934. S2CID 35474015.
  24. ^ Pollack, W.; Gorman, J. G.; Hager, H. J.; Freda, V. J.; Tripodi, D. (1968-05-06). "Antibody-Mediated Immune Suppression to the Rh Factor: Animal Models Suggesting Mechanism of Action". Transfusion. 8 (3): 134–145. doi:10.1111/j.1537-2995.1968.tb04891.x. ISSN 0041-1132. PMID 4173360. S2CID 10535055.
  25. ^ Vossoughi, Sarah; Spitalnik, Steven L. (July 2019). "Conquering erythroblastosis fetalis: 50 years of RhIG". Transfusion. 59 (7): 2195–2196. doi:10.1111/trf.15307. ISSN 0041-1132. PMID 31268587. S2CID 195786606.
  26. ^ Pollack, W.; Gorman, J. G.; Ereda, V. J.; Ascari, W. Q.; Allen, A. E.; Baker, W. J. (1968-05-06). "Results of Clinical Trials of RhoGAM in Women". Transfusion. 8 (3): 151–153. doi:10.1111/j.1537-2995.1968.tb04895.x. ISSN 0041-1132. PMID 4173363. S2CID 42240813.
  • Friesen A.D., Bowman J.M., Price H.W. (1981). "Column Ion Exchange Preparation and Characterization of an Rh Immune Globulin (WinRho) for Intravenous Use". J. Appl. Biochem. 3: 164–175.{{cite journal}}: CS1 maint: multiple names: authors list (link)

External links

  • National institute of Clinical Excellence (NICE) Guidelines for anti-D prophylaxis
  • Summary of transfusion reactions in the US

March 07, 2023
disease, also, known, rhesus, isoimmunization, disease, blue, baby, disease, type, hemolytic, disease, fetus, newborn, hdfn, hdfn, anti, antibodies, proper, currently, used, name, this, disease, blood, group, system, actually, more, than, antigens, only, antig. Rh disease also known as rhesus isoimmunization Rh D disease and blue baby disease is a type of hemolytic disease of the fetus and newborn HDFN HDFN due to anti D antibodies is the proper and currently used name for this disease as the Rh blood group system actually has more than 50 antigens and not only the D antigen The term Rh Disease is commonly used to refer to HDFN due to anti D antibodies and prior to the discovery of anti Rho D immune globulin it was the most common type of HDFN The disease ranges from mild to severe and occurs in the second or subsequent pregnancies of Rh D negative women when the biologic father is Rh D positive Rh diseaseOther namesRhesus isoimmunizationSpecialtyPaediatrics haematology transfusion medicineDue to several advances in modern medicine HDFN due to anti D is preventable by treating the mother during pregnancy and soon after delivery with an injection of anti Rho D RhoGam immune globulin With successful mitigation of this disease by prevention through the use of anti Rho D immune globulin other antibodies are more commonly the cause of HDFN today Contents 1 Signs and symptoms 2 Pathophysiology 3 Diagnosis 3 1 Maternal blood 3 2 Paternal blood 4 Prevention 5 Management 5 1 Antenatal 5 2 Postnatal 6 History 7 See also 8 References 9 External linksSigns and symptoms EditSymptoms of Rh disease include yellowish amniotic fluid and enlarged spleen liver or heart or buildup of fluid in the abdomen of the fetus 1 Pathophysiology EditDuring the first pregnancy the Rh mother s initial exposure to fetal Rh red blood cells RBCs is usually not sufficient to activate her Rh recognizing B cells However during delivery the placenta separates from the uterine wall causing umbilical cord blood to enter the maternal circulation which results in the mother s proliferation of IgM secreting plasma B cells to eliminate the fetal Rh cells from her blood stream IgM antibodies do not cross the placental barrier which is why no effects to the fetus are seen in first pregnancies for Rh D mediated disease However in subsequent pregnancies with Rh fetuses the IgG memory B cells mount an immune response when re exposed and these IgG anti Rh D antibodies do cross the placenta and enter fetal circulation These antibodies are directed against the Rhesus Rh factor a protein found on the surface of the fetal RBCs The antibody coated RBCs are destroyed by IgG antibodies binding and activating complement pathways 2 The resulting anemia has multiple sequelae 3 4 5 The immature hematopoietic system of the fetus is taxed as the liver and spleen attempt to put immature RBCs into circulation erythroblasts thus the previous name for this disease erythroblastosis fetalis As the liver and spleen enlarge under this unexpected demand for RBCs a condition called portal hypertension develops and this taxes the immature heart and circulatory system Liver enlargement and the prolonged need for RBC production results in decreased ability to make other proteins such as albumin and this decreases the plasma colloid oncotic pressure leading to leakage of fluid into tissues and body cavities termed hydrops fetalis The severe anemia taxes the heart to compensate by increasing output in an effort to deliver oxygen to the tissues and results in a condition called high output cardiac failure If left untreated the result may be fetal death The destruction of RBCs leads to elevated bilirubin levels hyperbilirubinemia as a byproduct This is not generally a problem during pregnancy as the maternal circulation can compensate However once the infant is delivered the immature system is not able to handle this amount of bilirubin alone and jaundice or kernicterus bilirubin deposition in the brain can develop which may lead to brain damage or death Sensitizing events during pregnancy include c section miscarriage therapeutic abortion amniocentesis ectopic pregnancy abdominal trauma and external cephalic version However in many cases there was no apparent sensitizing event Approximately 50 of Rh D positive infants with circulating anti D are either unaffected or only mildly affected requiring no treatment at all and only monitoring An additional 20 are severely affected and require transfusions while still in the uterus This pattern is similar to other types of HDFN due to other commonly encountered antibodies anti c anti K and Fy a citation needed Diagnosis EditMaternal blood Edit In the United States it is a standard of care to test all expecting mothers for the presence or absence of the RhD protein on their RBCs However when medical care is unavailable or prenatal care not given for any other reason the window to prevent the disease may be missed In addition there is more widespread use of molecular techniques to avoid missing women who appear to be Rh D positive but are actually missing portions of the protein or have hybrid genes creating altered expression of the protein and still at risk of HDFN due to Anti D 6 7 At the first prenatal visit the mother is typed for ABO blood type and the presence or absence of RhD using a method sensitive enough to detect weaker versions of this antigen known as weak D and a screen for antibodies is performed If she is negative for RhD protein expression and has not formed anti D already she is a candidate for RhoGam prophylaxis to prevent alloimmunization If she is positive for anti D antibodies the pregnancy will be followed with monthly titers levels of the antibody to determine if any further intervention is needed A screening test to detect for the presence or absence of fetal cells can help determine if a quantitative test Kleihauer Betke or flow cytometry is needed This is done when exposure is suspected due to a potential sensitizing event such as a car accident or miscarriage If the screening test is positive or the appropriate dose of RhoGam needs to be determined a quantitative test is performed to determine a more precise amount of fetal blood to which the mother has been exposed The Kleihauer Betke test or Flow Cytometry on a maternal blood sample are the most common ways to determine this and the appropriate dose of RhoGam is calculated based on this information There are also emerging tests using Cell free DNA Blood is taken from the mother and using PCR can detect fetal DNA 7 This blood test is non invasive to the fetus and can help determine the risk of HDFN Testing has proven very accurate and is routinely done in the UK at the International Blood Group Reference Laboratory in Bristol 8 Paternal blood Edit Blood is generally drawn from the father to help determine fetal antigen status 9 If he is homozygous for the antigen there is a 100 chance of all offspring in the pairing to be positive for the antigen and at risk for HDFN If he is heterozygous there is a 50 chance of offspring to be positive for the antigen 10 Prevention EditIn an RhD negative mother Rho D immune globulin can prevent temporary sensitization of the maternal immune system to RhD antigens which can cause rhesus disease in the current or in subsequent pregnancies With the widespread use of RhIG Rh disease of the fetus and newborn has almost disappeared in the developed world The risk that an RhD negative mother can be alloimmunized by a RhD positive fetus can be reduced from approximately 16 to less than 0 1 by the appropriate administration of RhIG citation needed Management EditAs medical management advances in this field it is important that these patients be followed by high risk obstetricians maternal fetal medicine and skilled neonatologists postpartum to ensure the most up to date and appropriate standard of care citation needed Antenatal Edit Routine prenatal labs drawn at the beginning of every pregnancy include a blood type and an antibody screen Mothers who are Rh negative A B AB or O blood types and have anti D antibodies found on the antibody screen need to determine the fetus s Rh antigen If the fetus is also Rh negative A B AB or O blood types then the pregnancy can be managed like any other pregnancy The anti D antibodies are only dangerous to Rh positive fetuses A B AB or O blood types The fetal Rh can be screened using non invasive prenatal testing NIPT In the United States BillionToOne Inc offers the Unity test This test can screen for the fetus s Rh antigen positive or negative at the 10th week of gestation using a blood sample drawn from the mother The Unity test uses NGS technology to look for Rh alleles genes in the cell free fetal DNA in the maternal bloodstream In healthy pregnancies at least 5 fetal fraction of the cell free DNA in the maternal bloodstream comes from the fetus placenta cells shed DNA into the maternal bloodstream This small fraction of cell free DNA from the fetus is enough to determine the fetus s Rh antigen Once a woman has been found to have made anti D or any clinically significant antibody against fetal red cells she is followed as a high risk pregnancy with serial blood draws to determine the next steps Once the titer of anti D reaches a certain threshold normally 8 to 16 serial Ultrasound and Doppler examinations are performed to detect signs of fetal anemia Detection of increased blood flow velocities in the fetus are a surrogate marker for fetal anemia that may require more invasive intervention If the flow velocity is found to be elevated a determination of the severity of anemia needs to ensue to determine if an intrauterine transfusion is necessary This is normally done with a procedure called percutaneous umbilical cord blood sampling PUBS or cordocentesis 11 Intrauterine blood transfusion citation needed Intraperitoneal transfusion blood transfused into fetal abdomen Intravascular transfusion blood transfused into fetal umbilical vein This is the method of choice since the late 1980s and more effective than intraperitoneal transfusion A sample of fetal blood can be taken from the umbilical vein prior to the transfusion Often this is all done at the same PUBS procedure to avoid the needs for multiple invasive procedures with each transfusionPostnatal Edit Phototherapy for neonatal jaundice in mild disease Exchange transfusion if the neonate has moderate or severe disease Intravenous Immunoglobulin IVIG can be used to reduce the need for exchange transfusion and to shorten the length of phototherapy 12 13 History EditIn 1939 Drs Philip Levine and Rufus E Stetson published their findings about a 25 year old mother who had a stillborn baby that died of hemolytic disease of the newborn 14 Both parents were blood group O so the husband s blood was used to give his wife a blood transfusion due to blood loss during delivery However she had a severe transfusion reaction Since both parents were blood group O which was believed to be compatible for transfusion they concluded that there must be a previously undiscovered blood group antigen that was present on the husband s red blood cells RBCs but not present on his wife s This suggested for the first time that a mother could make blood group antibodies because of immune sensitization to her fetus s RBCs as her only previous exposure would be the earlier pregnancy They did not name this blood group antigen at the time which is why the discovery of the rhesus blood type is credited to Drs Karl Landsteiner and Alexander S Wiener 15 with their first publication of their tables for blood typing and cross matching in 1940 which was the culmination of years of work However there were multiple participants in this scientific race and almost simultaneous publications on this topic Levine published his theory that the disease known as erythroblastosis fetalis was due to Rh alloimmunization in 1941 while Landsteiner and Wiener published their method to type patients for an antibody causing transfusion reactions known as Rh 16 17 18 The first treatment for Rh disease was an exchange transfusion invented by Wiener 19 and later refined by Dr Harry Wallerstein 20 Approximately 50 000 infants received this treatment However this could only treat the disease after it took root and did not do anything to prevent the disease In 1960 Ronald Finn in Liverpool England proposed that the disease might be prevented by injecting the at risk mother with an antibody against fetal red blood cells anti RhD 21 Nearly simultaneously Dr William Pollack 22 an immunologist and protein chemist at Ortho Pharmaceutical Corporation and Dr John Gorman blood bank director at Columbia Presbyterian with Dr Vincent Freda an obstetrician at Columbia Presbyterian Medical Center came to the same realization in New York City The three of them set out to prove it by injecting a group of male prisoners at Sing Sing Correctional Facility with antibody provided by Ortho obtained by a fractionation technique developed by Pollack 23 Animal studies had previously been conducted by Dr Pollack using a rabbit model of Rh 24 This model named the rabbit HgA F system was an animal model of human Rh and enabled Pollack s team to gain experience in preventing hemolytic disease in rabbits by giving specific HgA antibody as was later done with Rh negative mothers One of the needs was a dosing experiment that could be used to determine the level of circulating Rh positive cells in an Rh negative pregnant female derived from her Rh positive fetus This was first done in the rabbit system but subsequent human tests at the University of Manitoba conducted under Dr Pollack s direction confirmed that anti Rho D immune globulin could prevent alloimmunization during pregnancy citation needed Ms Marianne Cummins was the first at risk woman to receive a prophylactic injection of anti Rho D immune globulin RHIG after its regulatory approval 25 Clinical trials were set up in 42 centers in the US Great Britain Germany Sweden Italy and Australia RHIG was finally approved in England and the United States in 1968 26 The FDA approved the drug under the brand name RhoGAM with a fixed dose of 300 µG to be given within three days 72 hours postpartum Subsequently a broader peripartum period was approved for dosing which included prophylaxis during pregnancy Within a year the antibody had been injected with great success into more than 500 000 women Time magazine picked it as one of the top ten medical achievements of the 1960s By 1973 it was estimated that in the US alone over 50 000 babies lives had been saved The use of Rh immune globulin to prevent the disease in babies of Rh negative mothers has become standard practice and the disease which used to claim the lives of 10 000 babies each year in the US alone has been virtually eradicated in the developed world In 1980 Cyril Clarke Ronald Finn John G Gorman Vincent Freda and William Pollack each received an Albert Lasker Award for Clinical Medical Research for their work on rhesus blood types and the prevention of Rh disease citation needed See also EditJames Harrison blood donor Australian who donated blood over 1150 times to save babies with Rh diseaseReferences Edit Rh Disease The Children s Hospital of Philadelphia 2014 08 23 Retrieved 2021 11 21 a href Template Cite web html title Template Cite web cite web a CS1 maint url status link Punt J Stranford S Jones P amp Owen J A 2018 Chapter 15 Allergy Hypersensitivities and Chronic Inflammation In Kuby immunology 8th ed pp 1086 1087 WH Freeman Maitra Anirban 2010 Diseases of Infancy and Childhood Robbins and Cotran Pathologic Basis of Disease The Indian Medical Gazette Vol 43 Elsevier pp 447 483 doi 10 1016 b978 1 4377 0792 2 50015 8 ISBN 9781437707922 PMC 5182838 Wong EC ed 2015 Alloimmune cytopenias In Pediatric Transfusion A physician s handbook 4th ed AABB pp 45 61 Fung MK Grossman BJ Hillyer CD Westhoff CM eds 2014 Technical Manual 18th ed Bethesda MD AABB a href Template Cite book html title Template Cite book cite book a last has generic name help CS1 maint multiple names authors list link Kacker Seema Vassallo Ralph Keller Margaret A Westhoff Connie M Frick Kevin D Sandler S Gerald Tobian Aaron A R 2015 03 21 Financial implications ofRHDgenotyping of pregnant women with a serologic weak D phenotype Transfusion 55 9 2095 2103 doi 10 1111 trf 13074 ISSN 0041 1132 PMC 4739823 PMID 25808011 a b Fasano Ross M February 2016 Hemolytic disease of the fetus and newborn in the molecular era Seminars in Fetal and Neonatal Medicine 21 1 28 34 doi 10 1016 j siny 2015 10 006 ISSN 1744 165X PMID 26589360 Finning Kirstin Martin Peter Summers Joanna Daniels Geoff 2007 Fetal genotyping for the K Kell and Rh C c and E blood groups on cell free fetal DNA in maternal plasma Transfusion 47 11 2126 33 doi 10 1111 j 1537 2995 2007 01437 x PMID 17958542 S2CID 8292568 Scheffer PG Van Der Schoot CE Page Christiaens Gcml De Haas M 2011 Noninvasive fetal blood group genotyping of rhesus D c E and of K in alloimmunised pregnant women Evaluation of a 7 year clinical experience BJOG An International Journal of Obstetrics amp Gynaecology 118 11 1340 8 doi 10 1111 j 1471 0528 2011 03028 x PMID 21668766 S2CID 32946225 Transfusion Medicine and Hemostasis Clinical and Laboratory Aspects ISBN 978 0 12 397788 5 page needed Percutaneous Umbilical Cord Blood Sampling pennmedicine adam com Retrieved 2019 09 11 Gottstein R 2003 Systematic review of intravenous immunoglobulin in haemolytic disease of the newborn Archives of Disease in Childhood Fetal and Neonatal Edition 88 1 F6 10 doi 10 1136 fn 88 1 F6 PMC 1755998 PMID 12496219 Webb Jennifer Delaney Meghan October 2018 Red Blood Cell Alloimmunization in the Pregnant Patient Transfusion Medicine Reviews 32 4 213 219 doi 10 1016 j tmrv 2018 07 002 ISSN 1532 9496 PMID 30097223 S2CID 51958636 Levine Philip Stetson Rufus E 1939 An Unusual Case of Intra Group Agglutination Journal of the American Medical Association 113 2 126 7 doi 10 1001 jama 1939 72800270002007a Landsteiner K Wiener A S 1940 An Agglutinable Factor in Human Blood Recognized by Immune Sera for Rhesus Blood Experimental Biology and Medicine 43 223 doi 10 3181 00379727 43 11151 S2CID 58298368 Landsteiner K 1941 10 01 STUDIES ON AN AGGLUTINOGEN Rh IN HUMAN BLOOD REACTING WITH ANTI RHESUS SERA AND WITH HUMAN ISOANTIBODIES Journal of Experimental Medicine 74 4 309 320 doi 10 1084 jem 74 4 309 ISSN 0022 1007 PMC 2135190 PMID 19871137 LEVINE P VOGEL P KATZIN E M BURNHAM L 1941 10 17 Pathogenesis of Erythroblastosis Fetalis Statistical Evidence Science 94 2442 371 372 Bibcode 1941Sci 94 371L doi 10 1126 science 94 2442 371 ISSN 0036 8075 PMID 17820878 Zimmerman DR 1973 Rh The Intimate History of a Disease and Its Conquest Macmillan Publishing Co Reid Marion E October 2008 Alexander S Wiener the man and his work Transfusion Medicine Reviews 22 4 300 316 doi 10 1016 j tmrv 2008 05 007 ISSN 1532 9496 PMID 18848157 Wallerstein H 1946 Treatment of Severe Erythroblastosis by Simultaneous Removal and Replacement of the Blood of the Newborn Infant Science 103 2680 583 584 Bibcode 1946Sci 103 583W doi 10 1126 science 103 2680 583 PMID 21026828 Wright Pearce 2004 06 26 Ronald Finn Lancet 363 9427 2195 doi 10 1016 S0140 6736 04 16525 2 ISSN 1474 547X PMID 15248345 S2CID 2243030 William Pollack dies at 87 helped conquer deadly Rh disease Los Angeles Times 2013 11 17 Retrieved 2019 09 11 Freda V J Gorman J G Pollack W January 1964 Successful Prevention of Experimental Rh Sensitization in Man with an Anti Rh Gamma2 Globulin Antibody Preparation A Preliminary Report Transfusion 4 26 32 doi 10 1111 j 1537 2995 1964 tb02824 x ISSN 0041 1132 PMID 14105934 S2CID 35474015 Pollack W Gorman J G Hager H J Freda V J Tripodi D 1968 05 06 Antibody Mediated Immune Suppression to the Rh Factor Animal Models Suggesting Mechanism of Action Transfusion 8 3 134 145 doi 10 1111 j 1537 2995 1968 tb04891 x ISSN 0041 1132 PMID 4173360 S2CID 10535055 Vossoughi Sarah Spitalnik Steven L July 2019 Conquering erythroblastosis fetalis 50 years of RhIG Transfusion 59 7 2195 2196 doi 10 1111 trf 15307 ISSN 0041 1132 PMID 31268587 S2CID 195786606 Pollack W Gorman J G Ereda V J Ascari W Q Allen A E Baker W J 1968 05 06 Results of Clinical Trials of RhoGAM in Women Transfusion 8 3 151 153 doi 10 1111 j 1537 2995 1968 tb04895 x ISSN 0041 1132 PMID 4173363 S2CID 42240813 Friesen A D Bowman J M Price H W 1981 Column Ion Exchange Preparation and Characterization of an Rh Immune Globulin WinRho for Intravenous Use J Appl Biochem 3 164 175 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link External links EditNational institute of Clinical Excellence NICE Guidelines for anti D prophylaxis Summary of transfusion reactions in the US Retrieved from https en wikipedia org w index php title Rh disease amp oldid 1119387147, wikipedia, wiki, book, books, library,

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