Your search keyword '"D variant"' showing total 3 results

1. Serologic strategy in detecting RHD altered alleles in Brazilian blood donors

Author

Afonso José Pereira Cortez, Flavia Roche Moreira Latini, Tatiane Aparecida de Paula Vendrame, Jordão Pellegrino, Carine Prisco Arnoni, Rosangela de Medeiros Person, Lilian Castilho, and Janaína Guilhem Muniz

Subjects

RHD alleles, Hemagglutination, D variant, medicine.drug_class, business.industry, lcsh:RC633-647.5, Hematology, lcsh:Diseases of the blood and blood-forming organs, Review Article, Partial D, Monoclonal antibody, Weak D, Molecular biology, Peripheral blood, Serology, Red blood cell, medicine.anatomical_structure, Antigen, medicine, Immunology and Allergy, Allele, Indirect Antiglobulin Test, business, RHD genotyping

Abstract

Background We evaluated different technological approaches and anti-D clones to propose the most appropriate serologic strategy in detecting the largest numbers of D variants in blood donors. Methods We selected 101 samples from Brazilian blood donors with different expressions of D in our donor routine. The tests were performed in immediate spin (IS) with eleven commercially available anti-D reagents in a tube and microplate. The D confirmatory tests for the presence of weak D included the indirect antiglobulin test (IAT) in a tube, gel and solid-phase red blood cell adherence (SPRCA). All DNA samples were extracted from peripheral blood and the D variants were classified using different molecular assays. Results The RHD variants identified by molecular analysis included weak D types (1, 2, 3, 11 and 38) and partial Ds (DAR1.2, DAR1, DAR3.1, DAU0, DAU2, DAU4, DAU5, DAU6, DMH and DVII). The monoclonal-monoclonal blend RUM-1/MS26 was the best anti-D reagent used in detecting the D antigen in the IS phase in a tube, reacting with 83.2% of the D variants, while the anti-D blend D175 + 415 was the best monoclonal antibody (MoAb) used in a microplate to minimize the need for an IAT, reacting with 83.2% of the D variants. The D confirmatory tests using SPRCA showed a reactivity (3 - 4+) with 100% of the D variant samples tested. Conclusion Our results show that, even using sensitive methods and MoAbs to ensure the accurate assignment of the D antigen, at least 17% of our donor samples need a confirmatory D test in order to avoid alloimmunization in D-negative patients.

Published

2019

2. RHD Genotyping of Rh-Negative and Weak D Phenotype among Blood Donors in Southeast Iran

Author

Younes Sadeghi-Bojd, Arezoo Oodi, and Naser Amirizadeh

Subjects

Transplantation, Oncology, business.industry, Weak D phenotype, Medicine, Hybrid Rhesus box, D variant, RHD gene deletion, RhD-negative phenotype, Weak D, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Hematology, business, Genotyping, Virology, Rh blood group system, RC254-282

Abstract

Background: The D antigen is a subset of Rh blood group antigens involved in the hemolytic disease of the newborn [HDFN] and hemolytic transfusion reaction [HTR]. The hybrid Rhesus box that was created after RH gene deletion, was known as a mechanism of the Rh-negative phenotype. Hybrid marker identification is used to confirm the deletion of the RHD gene and to determine zygosity. This study aims to detect this marker in Rh-negative and weak D phenotype blood donors of the southeast of Iran. Materials and Methods: The molecular analysis of the hybrid Rhesus box was performed on the 200 Rh-negative blood donors in Sistan and Baluchestan province, southeast Iran. The presence of alleles responsible for the D variants was assessed by DNA sequencing in 26 weak D phenotype donors. Results: Of the 200 Rh-negative blood samples, 198 samples were homozygous (99%), and two samples were heterozygous (1%). Heterozygous samples had RHD*01N.73 allele and the RHD*01N.18 allele. Of the 26 samples with weak D phenotype, 16 partial DLO (61%), 4 partial DBT1 (15.3%), 2 partial DV type 2 (7.7%), 1 weak D type 1, 1 weak D type 4.2.3, 1weak D type 105 and 1 RHD (S103P) (4%) were determined. Conclusion: Since RHD gene deletion is the main mechanism of the Rh-negativity in Sistan and Baluchestan provinces, a hybrid Rhesus box marker can be used in resolving RhD typing discrepancies by RHD genotyping methods.

Published

2020

3. D variants in the population of D‐negative blood donors in the north‐eastern region of Croatia

Author

Ante Ćorušić, Ivana Babić, Sandra Jagnjić, Vesna Dogic, Jasna Bingulac-Popović, Hana Safic Stanic, Ivona Herceg, and Irena Jukić

Subjects

Adult, Male, Adolescent, Genotype, Genotyping Techniques, Croatia, Population, Blood Donors, 030204 cardiovascular system & hematology, Biology, Real-Time Polymerase Chain Reaction, law.invention, 03 medical and health sciences, Exon, 0302 clinical medicine, Antigen, law, Humans, D antigen, D variant, RHD genotyping, partial D, weak D, Allele, education, Genotyping, Gene, Polymerase chain reaction, Polymorphism, Single-Stranded Conformational, Aged, education.field_of_study, Rh-Hr Blood-Group System, Hematology, Exons, Middle Aged, Molecular biology, genomic DNA, Female, 030215 immunology

Abstract

Objectives The aim of this study was to determine RHESUS D GENE (RHD) allelic variants among Croatian D-negative blood donors and compare our results with respective data from other European countries. Background Altered or reduced D antigen expression can result in D variants, which can be mistyped and can lead to the alloimmunisation of the blood recipient. RHD genotyping can distinguish D variants: weak D, partial D and DEL, thus preventing alloimmunisation. Material/methods A total of 6523 samples obtained from D-negative Croatian donors were screened for the presence of RHD using the real-time polymerase chain reaction (PCR) method. PCR-SSP was performed for D variant genotyping by using commercial genotyping kits (Inno-Train, Kronberg, Germany). Genomic DNA sequencing for all 10 exons of the RHD was performed when the genotyping kits failed to assign a D variant. Results RHD molecular screening revealed 23 (0.35%) RHD-PCR positive samples, all C/E positive, in decreasing frequency: 11 hybrid RHD-CE (2-9) D-CE variants, 4 weak partial D type 11 and 2 weak D type 2. Six samples remained unresolved and were sequenced. For 12 of 23 samples (excluding large hybrids), an adsorption/elution of anti-D serum was performed, confirming that all 12 were RhD+. The calculated frequency of clinically significant D alleles in RhD-negative blood donors was 1:543 (0.18%) or 1:53 (1.89%) in C/E blood donors. Conclusion Data on the significant frequency of D variants among serologically D-negative blood donors in the north-eastern region of Croatia could help in introducing RHD molecular screening of blood donors in a routine workflow.

Published

2020