<i><scp>RHD</scp></i> variants in <scp>F</scp>landers, <scp>B</scp>elgium

Sandt, Vicky Van; Gassner, Christoph; Emonds, Marie‐Paule; Legler, Tobias J.; Mahieu, Sarah; Körmöczi, Günther F.

doi:10.1111/trf.12947

Cited by 21 publications

(26 citation statements)

References 37 publications

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“…The distribution of RHD variants associated with the weak D phenotype is population dependent. Weak D types 1, 2 and 3 are most frequent in European and Canadian populations [6,8,10,[18][19][20]. Weak D types 4Á0 and 4Á1 have been reported as frequently occurring alleles in African populations from Egypt, Tunisia, Ethiopia and South Africa [7,21,22].…”

Section: Introductionmentioning

confidence: 99%

Diverse and novel RHD variants in Australian blood donors with a weak D phenotype: implication for transfusion management

et al. 2017

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Section: Introductionmentioning

confidence: 99%

Diverse and novel RHD variants in Australian blood donors with a weak D phenotype: implication for transfusion management

et al. 2017

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“…Interestingly, the RHD*721A>C allele was detected in seven cases whereas all other novel alleles, except the RHD*1074‐1G>A allele, were detected in single cases. This allele was not detected in previous studies performed in Germany, Austria, Poland and Belgium, respectively (Flegel et al , ; Polin et al , ; Orzinska et al , ; Van Sandt et al , , respectively, indicating that this allele is specific for the Dutch population. All women positive for the RHD*721A>C allele had Dutch surnames but we have no indication that these women are related.…”

Section: Discussionmentioning

confidence: 66%

Frequency and characterization of known and novel RHD variant alleles in 37 782 Dutch D‐negative pregnant women

et al. 2016

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To guide anti-D prophylaxis, Dutch D- pregnant women are offered a quantitative fetal-RHD-genotyping assay to determine the RHD status of their fetus. This allowed us to determine the frequency of different maternal RHD variants in 37 782 serologically D- pregnant women. A variant allele is present in at least 0·96% of Dutch D- pregnant women The D- serology could be confirmed after further serological testing in only 54% of these women, which emphasizes the potential relevance of genotyping of blood donors. 43 different RHD variant alleles were detected, including 15 novel alleles (11 null-, 2 partial D- and 2 DEL-alleles). Of those novel null alleles, one allele contained a single missense mutation (RHD*443C>G) and one allele had a single amino acid deletion (RHD*424_426del). The D- phenotype was confirmed by transduction of human D- erythroblasts, consolidating that, for the first time, a single amino acid change or deletion causes the D- phenotype. Transduction also confirmed the phenotypes for the two new variant DEL-alleles (RHD*721A>C and RHD*884T>C) and the novel partial RHD*492C>A allele. Notably, in three additional cases the DEL phenotype was observed but sequencing of the coding sequence, flanking introns and promoter region revealed an apparently wild-type RHD allele without mutations.

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“…3 Use of two different serologic methods or anti-D reagents have been shown to be an effective practice for identifying those patients who will benefit from RHD genotyping. 28,29,39,40,[44][45][46][47][48] Our interpretations of RHD genotype results are summarized in a crosswalk table of RHD allele assignments (Table 1) to standardize reporting and guidance to manage as D+, D−, or uncommonly as indeterminate risk. Indeed, AABBaccredited immunohematology reference laboratories are already required to provide recommendations for RhIG administration and selection of the most compatible RBCs for transfusion.…”

Section: Snv = Single-nucleotide Variationmentioning

confidence: 99%

It's time to phase out “serologic weak D phenotype” and resolve D types with RHD genotyping including weak D type 4

et al. 2020

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RHD variants in Flanders, Belgium

Abstract: Despite the enormous diversity of RHD alleles, first-line weak D genotyping was remarkably informative, allowing for rapid classification of most samples with conspicuous RhD phenotype in Flanders. The clinical implications are discussed.

Cited by 21 publications

References 37 publications

Diverse and novel RHD variants in Australian blood donors with a weak D phenotype: implication for transfusion management

Diverse and novel RHD variants in Australian blood donors with a weak D phenotype: implication for transfusion management

Frequency and characterization of known and novel RHD variant alleles in 37 782 Dutch D‐negative pregnant women

It's time to phase out “serologic weak D phenotype” and resolve D types with RHD genotyping including weak D type 4

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