<scp>SCAR</scp>: The high‐prevalence antigen 013.008 in the <scp>Scianna</scp> blood group system

Srivastava, Kshitij; Albasri, Jasem; Alsuhaibani, Omar; Aljasem, Hassan; Bueno, Marina; Antonacci, Tania; Branch, Donald R.; Denomme, Gregory A.; Flegel, Willy A.

doi:10.1111/trf.16152

Cited by 5 publications

(12 citation statements)

References 49 publications

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“…70 The ERMAP protein inhibited the antibody in our study, which allowed us to define the antibody as being directed against a hitherto unknown high-prevalence Scianna antigen, dubbed SCAR (SC8). 70 The standard approach was using red cells with rare null phenotypes (null cells) [102][103][104] to define new blood group systems and new high-prevalence antigens. Unless alternatives are available, null cells are needed because ISBT guidelines 1 for establishment of new blood group systems or new antigens in an established system require demonstration of antigen expression specifically in erythroid cells.…”

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 72%

“…The ISBT Working Party on Red Cell Immunogenetics and Blood Group Terminology has begun accepting evidence from rBGPs alone, 65,66,70,81,84 without testing against red cells lacking the protein or antigen, to satisfy the requirements 1 for defining novel blood group antigens. The first example was the YTEG antigen of the YT blood group system in 2017, 65 followed by the YT antigens YTLI and YTOT 66 and the Indian antigen INSL 84 in 2018.…”

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

“…Since 1996, multiple studies have exploited soluble or cell membrane‐bound recombinant proteins to screen human sera for blood‐group‐specific antibodies (Table 1). 27,29,32,44–95 There are 190 red cell antigens classified as high‐prevalence by the ISBT (see web resources) 96 . To identify antibody specificities against all high‐prevalence antigens, up to 190 distinct red cells lacking high‐prevalence antigens or lacking the whole carrier protein would be needed.…”

Section: Rbgps and Antibody Characterizationmentioning

confidence: 99%

“…To confirm a new high‐prevalence antigen actually belonged to the Scianna blood group system, we recently applied a soluble recombinant ERMAP protein 70 . The ERMAP protein inhibited the antibody in our study, which allowed us to define the antibody as being directed against a hitherto unknown high‐prevalence Scianna antigen, dubbed SCAR (SC8) 70 . The standard approach was using red cells with rare null phenotypes (null cells) 102–104 to define new blood group systems and new high‐prevalence antigens.…”

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

“…The first example was the YTEG antigen of the YT blood group system in 2017, 65 followed by the YT antigens YTLI and YTOT 66 and the Indian antigen INSL 84 in 2018. SCAR 70 in the Scianna blood group system 105 and DACY and YCAD 81 in the Knops blood group system 106 were accepted in 2020 based on rBGP evidence without testing against red cells lacking the relevant blood group protein.…”

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

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When recombinant proteins can replace rare red cells in immunohematology workups

Flegel

Srivastava

2021

Transfusion

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Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 72%

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

Section: Rbgps and Antibody Characterizationmentioning

confidence: 99%

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

Section: Rbgps and Novel Antigens In Known Blood Group Systemsmentioning

confidence: 99%

See 3 more Smart Citations

When recombinant proteins can replace rare red cells in immunohematology workups

Flegel

Srivastava

2021

Transfusion

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Two new Scianna variants causing loss of high prevalence antigens: ERMAP model and 3D analysis of the antigens

et al. 2022

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Background Scianna (Sc) antigens, seven high and two of low prevalence, are expressed on erythrocyte membrane‐associated protein (ERMAP). We investigated SC (ERMAP) in individuals who made antibodies to high prevalence Scianna antigens, and propose a 3D model for ERMAP to precisely localize the residues associated with the known antigens. Methods Serological testing and DNA sequencing was performed by standard methods. A 3D structural model was built using a multi‐template homology approach. Protein structures representing missense variants associated with the loss or gain of an antigen were generated. Residue accessibility and intraprotein interactions were compared with the wild‐type protein. Results Two new SC alleles, one with c.349C > T (p.Arg117Cys) in a woman from South India with anti‐Sc3 in her plasma, and a c.217_219delinsTGT (p.Arg73Cys) in an African‐American woman with an antibody to a new high prevalence antigen, termed SCAC, were identified. Six structural templates were used to model ERMAP. 3D analysis showed that residues key for Scianna antigen expression were all exposed at the surface of the extracellular domain. The p.Arg117Cys change was predicted to abolish interactions between residues 93 and 117, with no compensating interactions. Conclusion We confirm the extracellular location of Scianna residues responsible for antigen expression which predicts direct accessibility to antibodies. Loss of intraprotein interactions appear to be responsible for a Sc null and production of anti‐Sc3 with p.117Cys, SC*01 N.03, and for loss of a high prevalence antigen with p.73Cys, termed SCAC for Sc Arg to Cys. Comparative modeling aids our understanding of new alleles and Scianna antigen expression.

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International Society of Blood Transfusion Working Party on Red Cell Immunogenetics and Blood Group Terminology Report of Basel and three virtual business meetings: Update on blood group systems

et al. 2022

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Background and Objectives Under the ISBT, the Working Party (WP) for Red Cell Immunogenetics and Blood Group Terminology is charged with ratifying blood group systems, antigens and alleles. This report presents the outcomes from four WP business meetings, one located in Basel in 2019 and three held as virtual meetings during the COVID‐19 pandemic in 2020 and 2021. Materials and Methods As in previous meetings, matters pertaining to blood group antigen nomenclature were discussed. New blood group systems and antigens were approved and named according to the serologic, genetic, biochemical and cell biological evidence presented. Results Seven new blood group systems, KANNO (defined numerically as ISBT 037), SID (038), CTL2 (039), PEL (040), MAM (041), EMM (042) and ABCC1 (043) were ratified. Two (039 and 043) were de novo discoveries, and the remainder comprised reported antigens where the causal genes were previously unknown. A further 15 blood group antigens were added to the existing blood group systems: MNS (002), RH (004), LU (005), DI (010), SC (013), GE (020), KN (022), JMH (026) and RHAG (030). Conclusion The ISBT now recognizes 378 antigens, of which 345 are clustered within 43 blood group systems while 33 still have an unknown genetic basis. The ongoing discovery of new blood group systems and antigens underscores the diverse and complex biology of the red cell membrane. The WP continues to update the blood group antigen tables and the allele nomenclature tables. These can be found on the ISBT website (http://www.isbtweb.org/working-parties/red-cell-immunogenetics-and-blood-group-terminology/).

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SCAR: The high‐prevalence antigen 013.008 in the Scianna blood group system

Cited by 5 publications

References 49 publications

When recombinant proteins can replace rare red cells in immunohematology workups

When recombinant proteins can replace rare red cells in immunohematology workups

Two new Scianna variants causing loss of high prevalence antigens: ERMAP model and 3D analysis of the antigens

International Society of Blood Transfusion Working Party on Red Cell Immunogenetics and Blood Group Terminology Report of Basel and three virtual business meetings: Update on blood group systems

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