Risk Factors for RhD Immunisation Despite Antenatal and Postnatal Anti-D Prophylaxis

Koelewijn, Joke M.; Haas, Masja de; Vrijkotte, Tanja G. M.; Schoot, C. Ellen van der; Bonsel, Gouke J.

doi:10.1097/01.ogx.0000367502.86137.2c

Cited by 7 publications

(9 citation statements)

References 24 publications

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“…Despite the increased volume of distribution of administered anti‐D in heavier women and the consequently lower circulating levels achieved with equivalent doses, protection against sensitisation depends on the total amount of anti‐D, not its blood concentration; heavier women should not be at greater risk of sensitisation, as the concentration of fetal red blood cells in maternal blood will also be reduced. This interpretation is supported by the results of a case–control study (42 cases, 339 controls) that found no association between weight and sensitisation …”

Section: Discussionmentioning

confidence: 73%

Single dose v two‐dose antenatal anti‐D prophylaxis: a randomised controlled trial

White

Cheng

Penova-Veselinovic

et al. 2019

Medical Journal of Australia

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Objective To compare rates of detectability of circulating Rh(D)‐immunoglobulin (anti‐D) at delivery with single and two‐dose antenatal anti‐D prophylaxis (RAADP) regimens; to compare compliance with the two regimens. Design Open label, randomised controlled trial between May 2013 and November 2015. Setting, participants 277 women who attended a tertiary obstetric referral hospital in Perth for antenatal care and were at least 18 years of age, less than 30 weeks pregnant and yet to receive RAADP, Rh(D)‐negative (negative antibody screen), and who intended to deliver their baby at the hospital. Exclusion criteria were prior anti‐D sensitisation, any contraindication of anti‐D administration, and a history of isolated IgA deficiency. Interventions One 1500 IU anti‐D dose at 28 weeks of pregnancy (single dose regimen); two doses of 625 IU each at 28 and 34 weeks of pregnancy (two‐dose regimen). Main outcome measures The primary outcome was the proportion of women with detectable anti‐D levels at delivery; the secondary outcome was compliance with the allocated RAADP regimen. Results Circulating anti‐D was detectable at delivery in a greater proportion of women in the two‐dose group (111 of 129, 86%) than in the single dose group (70 of 125, 56%; P < 0.001). Compliance was not significantly different between the single dose (86 of 138, 61%) and two‐dose groups (70 of 139, 50%; P = 0.06). Conclusions The two‐dose RAADP schedule currently recommended in Australia provides better protection against Rh(D) sensitisation than a one‐dose regimen. Trial registration Australian and New Zealand Clinical Trials Registry (ACTRN12613000661774).

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Section: Discussionmentioning

confidence: 73%

Single dose v two‐dose antenatal anti‐D prophylaxis: a randomised controlled trial

White

Cheng

Penova-Veselinovic

et al. 2019

Medical Journal of Australia

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“…Patient samples and clinical data from the prospective OPZI study (Detection and Prevention of Pregnancy Immunisation) were included after informed consent (Koelewijn et al , , ). The OPZI study included all Dutch pregnant women with clinically relevant non‐D RBC antibodies, detected at first trimester screening, from 1 Sept 2002–1 June 2003 and from 1 Oct 2003–1 July 2004 ( n = 230) and 964 controls and antigen‐negative children (Koelewijn et al , , ). None of the affected cases received intravenous immunoglobulin therapy.…”

Section: Methodsmentioning

confidence: 99%

Antigen specificity determines anti‐red blood cell IgG‐Fc alloantibody glycosylation and thereby severity of haemolytic disease of the fetus and newborn

et al. 2016

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Haemolytic disease of the fetus and newborn (HDFN) is a severe disease in which fetal red blood cells (RBC) are destroyed by maternal anti-RBC IgG alloantibodies. HDFN is most often caused by anti-D but may also occur due to anti-K, -c- or -E. We recently found N-linked glycosylation of anti-D to be skewed towards low fucosylation, thereby increasing the affinity to IgG-Fc receptor IIIa and IIIb, which correlated with HDFN disease severity. Here, we analysed 230 pregnant women with anti-c, -E or -K alloantibodies from a prospective screening cohort and investigated the type of Fc-tail glycosylation of these antibodies in relation to the trigger of immunisation and pregnancy outcome. Anti-c, -E and -K show - independent of the event that had led to immunisation - a different kind of Fc-glycosylation compared to that of the total IgG fraction, but with less pronounced differences compared to anti-D. High Fc-galactosylation and sialylation of anti-c correlated with HDFN disease severity, while low anti-K Fc-fucosylation correlated with severe fetal anaemia. IgG-Fc glycosylation of anti-RBC antibodies is shaped depending on the antigen. These features influence their clinical potency and may therefore be used to predict severity and identify those needing treatment.

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“…By not including women who developed D antibodies, part of the D– population (of which a considerable proportion might be “high‐responders,” very prone to develop additional antibodies) was excluded. This exclusion did not affect the found preventive effect of RhIG on the development of non‐Rh antibodies, as we previously found that in primiparous women with newly detected D antibodies and without a previous blood transfusion, non‐Rh antibodies in addition to D antibodies are rarely developed …”

Section: Discussionmentioning

confidence: 99%

ABO incompatibility and RhIG immunoprophylaxis protect against non‐D alloimmunization by pregnancy

et al. 2018

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Risk Factors for RhD Immunisation Despite Antenatal and Postnatal Anti-D Prophylaxis

Cited by 7 publications

References 24 publications

Single dose v two‐dose antenatal anti‐D prophylaxis: a randomised controlled trial

Single dose v two‐dose antenatal anti‐D prophylaxis: a randomised controlled trial

Antigen specificity determines anti‐red blood cell IgG‐Fc alloantibody glycosylation and thereby severity of haemolytic disease of the fetus and newborn

ABO incompatibility and RhIG immunoprophylaxis protect against non‐D alloimmunization by pregnancy

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