Molecular basis of the D variant phenotypes DNU and DII allows localization of critical amino acids required for expression of Rh D epitopes epD3, 4 and 9 to the sixth external domain of the Rh D protein

Avent, Neil D.; Jones, Jeffrey W.; Liu, Wendy; Scott, Marion L.; Voak, D.; Flegel, Willy A.; Wagner, Franz F.; Green, Charles

doi:10.1046/j.1365-2141.1997.632710.x

Cited by 40 publications

(29 citation statements)

References 22 publications

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“…Initial contributions were the frequency of the D category VI (today known as DVI) in the German population [14]; characterization of the partial D DNU [15]; and of a third molecular basis for DVI [16], which proved that the low antigen density of many DVI could not be explained by the loss of D epitopes. Based on these contributions, the German Guidelines for Blood Group Determination and Blood Transfusion were changed in 1996 [17]: the use of monoclonal anti-D with distinct characteristics was implemented for determination of the D antigen; the concept of ‘D u ' carriers considered as D-positive blood donors and D-negative transfusion recipients was replaced by distinct recommendations for weak D (D-positive transfusion strategy) and partial D carriers (D-negative transfusion strategy, especially for DVI).…”

Section: Introductionmentioning

confidence: 99%

The Rhesus Site

Wagner¹,

Flegel²

2014

Transfus Med Hemother

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100

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The Rhesus Site is a resource for information of the ‘Rhesus' blood group. It is intended for specialists and non-specialists. The website details research in the field relevant for transfusion medicine, immunohematology, and molecular research. Link areas guide to important publications and to methodological resources for Rhesus. Many data originally presented at The Rhesus Site have been formally published later. The ‘RhesusBase' section represents the largest database for RHD alleles; the ‘RhesusSurveillance' section details the results of the largest prospective observational study on anti-D immunization events in D-positive patients. Visitors to the website are encouraged to explore the intricacies of the most complex blood group gene locus.

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Section: Introductionmentioning

confidence: 99%

The Rhesus Site

Wagner¹,

Flegel²

2014

Transfus Med Hemother

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100

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“…Some D variants have a specific part of the RHD polypeptide fragment replaced by the equivalent RHCE polypeptide, and are designated D–CE–D [6, 7, 8, 9, 10, 11, 12, 13]. Others have a point mutation causing an amino acid change in an extracellular domain of the RHD polypeptide [4, 5, 14]. …”

Section: Introductionmentioning

confidence: 99%

“…D variants lack some of the D epitopes and a lack of specific epitopes defines D category phenotypes (D II–VII , DFR, DBT, DHMi, DHMii, DNU, and DHR) [2, 3, 4, 5]. Some D variants have a specific part of the RHD polypeptide fragment replaced by the equivalent RHCE polypeptide, and are designated D–CE–D [6, 7, 8, 9, 10, 11, 12, 13].…”

Section: Introductionmentioning

confidence: 99%

Polymorphisms of RhDVa and a New RhDVa–Like Variant Found in Japanese Individuals

et al. 2000

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Background and Objectives: Red cell type RhD^Va lacks epD1 and 5 and is encoded by hybrid RHD–CE(5)–D alleles. We analyzed RhD^Va and RhD^Va–like samples in Japanese blood donors. Materials and Methods: Ten RhD^Va samples lacked epD1 and 5 and 3 RhD^Va–like variants also lacked, epD2 and a part of 6/7. We identified the full–length nucleotide sequences of the complementary DNA (cDNA) synthesized from 4 samples: 3 of type D^Va and the 4th a D^Va–like variant. Results: Although their sequences differed from each other, all the substitutions were exclusively in exon 5. Three D^Va samples had hybrid RHD–CE(5)–D alleles, but the D^Va–like variant had a unique nucleotide substitution with a single amino acid change, E233K. Exon 5 of the genomic DNA from all 13 samples was analyzed by sequencing. No other sequences were identified. Conclusion: All RhD^Va and RhD^Va–like variants had the substitution for E233. E233 seems to be a determinant of epD1 and 5. A new category of RhD variant, DYO, was identified.

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“…The rediscovery of the original Category II propositus led to the subdivision of epD3 [209] . DNU (Gly353Arg) [159] and DNB (Gly355Ser) [168] are D variants with similar epitope profi les to DII. DNU (Gly353Arg) [159] and DNB (Gly355Ser) [168] are D variants with similar epitope profi les to DII.…”

Section: DII Dnu Dnbmentioning

confidence: 99%

Rh and RHAG Blood Group Systems

Daniels

2013

Human Blood Groups

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Molecular basis of the D variant phenotypes DNU and D^II allows localization of critical amino acids required for expression of Rh D epitopes epD3, 4 and 9 to the sixth external domain of the Rh D protein

Cited by 40 publications

References 22 publications

The Rhesus Site

The Rhesus Site

Polymorphisms of RhD<sup>Va</sup> and a New RhD<sup>Va</sup>–Like Variant Found in Japanese Individuals

Rh and RHAG Blood Group Systems

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Molecular basis of the D variant phenotypes DNU and DII allows localization of critical amino acids required for expression of Rh D epitopes epD3, 4 and 9 to the sixth external domain of the Rh D protein

Cited by 40 publications

References 22 publications

The Rhesus Site

The Rhesus Site

Polymorphisms of RhD<sup>Va</sup> and a New RhD<sup>Va</sup>&ndash;Like Variant Found in Japanese Individuals

Rh and RHAG Blood Group Systems

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Product

Resources

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Molecular basis of the D variant phenotypes DNU and D^II allows localization of critical amino acids required for expression of Rh D epitopes epD3, 4 and 9 to the sixth external domain of the Rh D protein

Polymorphisms of RhD<sup>Va</sup> and a New RhD<sup>Va</sup>–Like Variant Found in Japanese Individuals