Volume 55, Issue 12 pp. 2912-2919
IMMUNOHEMATOLOGY

Extended matched intrauterine transfusions reduce maternal Duffy, Kidd, and S antibody formation

Henk Schonewille

Corresponding Author

Henk Schonewille

Center for Clinical Transfusion Research, Sanquin Research

Jon J. van Rood Center for Clinical Transfusion Research, Sanquin-Leiden University Medical Center

Address correspondence to: Henk Schonewille, Center for Clinical Transfusion Research, Sanquin Research, Plesmanlaan 1a, 2333 BZ Leiden, the Netherlands; e-mail: [email protected].Search for more papers by this author
Karin J.M. Prinsen-Zander

Karin J.M. Prinsen-Zander

Department of Immuno-hematology and Blood Transfusion, Leiden University Medical Center, Leiden, the Netherlands

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Mila Reijnart

Mila Reijnart

Sanquin Blood Bank, Sanquin Blood Supply, Dordrecht, the Netherlands

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Leo van de Watering

Leo van de Watering

Center for Clinical Transfusion Research, Sanquin Research

Jon J. van Rood Center for Clinical Transfusion Research, Sanquin-Leiden University Medical Center

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Jaap-Jan Zwaginga

Jaap-Jan Zwaginga

Center for Clinical Transfusion Research, Sanquin Research

Department of Immuno-hematology and Blood Transfusion, Leiden University Medical Center, Leiden, the Netherlands

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Robertjan H. Meerman

Robertjan H. Meerman

Department of Obstetrics and Fetal Medicine, Leiden University Medical Center, Leiden, the Netherlands

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Inge L. van Kamp

Inge L. van Kamp

Department of Obstetrics and Fetal Medicine, Leiden University Medical Center, Leiden, the Netherlands

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Anneke Brand

Anneke Brand

Jon J. van Rood Center for Clinical Transfusion Research, Sanquin-Leiden University Medical Center

Department of Immuno-hematology and Blood Transfusion, Leiden University Medical Center, Leiden, the Netherlands

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First published: 14 July 2015
Citations: 23

Abstract

BACKGROUND

Severe alloimmune hemolytic disease of the fetus is treated with intrauterine transfusions (IUTs). Despite C, c, E, e, and K matching between mother and donor, IUT results in new antibodies in approximately 25% of women. Newly formed Fya, Fyb, Jka, Jkb, and S antibodies are in 83% presumably induced by the IUT donor. Therefore, we intentionally extended matching between mother and IUT donor for these additional antigens. The results, after almost 8 years of applying this protocol, are reported.

STUDY DESIGN AND METHODS

Data from February 2007 to August 2014 on IUT patients were retrieved from the Leiden University Medical Center database and from donors from the Sanquin National Donor Database. Maternal data included red blood cell (RBC) antigen profiles, RBC antibodies, and date and consecutive number of each IUT. From the fathers, children, and IUT donors the RBC antigen profiles were retrieved.

RESULTS

A total of 182 fetuses from 159 women were treated with 481 IUTs. Of these, 317 IUTs (66%) were matched for Duffy, Kidd, and S antigens. Only matched IUTs were received by 77 women (48%) and 82 (52%) received (partly) nonmatched IUTs. Evaluable for new antibodies were 142 women. Duffy, Kidd, or S antibodies were formed by three of 69 women (4.3%) after matched IUTs and by eight of 73 women (11.0%) after nonmatched IUTs.

CONCLUSION

Extended matching for all IUTs was not possible for approximately 50% of women. Strict adherence to Duffy, Kidd, and S antigens–matched IUTs decreased immunization against these antigens by 60% compared to nonmatched IUTs.

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