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Colton antigen Prevalence
- Coa: 99.5% all
- Cob: 80% European ancestry
- Co3: 100% all
Expressed on cord cells
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Colton is resistant to:
Proteolytic enzymes
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Colton disease association
- Monosomy 7 - A rare type of dyserythropoietic anemia
- Leukemia
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Colton association with HDN & HTR
May cause severe HDFN & HTR
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Landsteiner-Weiner Phenotype & prevalenc
LW(a+b-): >99%
LW(a+b+): <1%
LW(a-b+): Very rare
LW(a-b-) : Very rare
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Landsteiner-Weiner cord expression and additional facts
Strongly expressed on D+ adult cells and all cord cells
Weakly expressed on D- adult cells
Rhnull are: LW (a-b-)
anti-Lwa may look like anti-D
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Landsteiner-Weiner destroyed by
DTT, AET, & Pronase
(D antigen is not destroyed by DTT) * How to differentiate
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LW antigen expression
- Expressed stronger on D+ than D- cell
- Even Stronger on cord cells
- No expressed on Rhnull or LWnull phenotypes
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LW Landsteiner-Weiner reactions
- IAT phase
- Not clinically significant (No HDFN or HTR
- Sometimes associated with:
- pregnancy or hematologic malignancy
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Chido/Rodgers System important facts
- Found on the fourht component of complement 4
- Formerly known as HTLA
- They are NOT intrinsic to the red cell
- Are ABSORBED onto the red cell from plasma
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Chido/Rodgers antibody characteristics
formerly HTLA
- **Neutralization: Antigen positive serum or plasma - Use for serological problem solving
- OR
- Adsorption with red cells coated with C4
NO - HTR or HDFN
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Chido/Rodgers reactions with enzymes or chemicals
Ficin/papain/trypsin: Sensitive
DTT, Chloroquine (RT): Resisitant
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Gerbich System High prevalence antigens
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Gerbich low prevalence antigens
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Gerbich chemical and enzyme reactions
Ge2 & 4 Destroyed by: Trypsin & Papain
- Ge3 destroyed by: Trypsin
- Ge3 resistant to: Papain
Papain distinguishes 3 form 2 & 4
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Gerbich antibody characteristics
Ge3 may cause HDN (2-4wks post delivery)
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Cromer system; Location
Located on the complement regulatory glycoprotein, decay accelerating factero (DAF or CD55)
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Cromer high prevalence ag's
Tca & WEb
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Cromer low prevalence ag's
Tcb, Tcc, & WEa
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Cromer enzyme and chemical results
- Destroyed by: a-chymotrypsin
- Only Slightly reduced: AET & DTT
- Resistant: papain, ficin, trypsin
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Cromer Ab characteristics
- Not clinically significant
- IgG
- IAT
*** Are inhibited by serum or concentrated urine from antigen positive individuals and are removed from serum by platelet concentrates.
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Cromer can produce what in a Cromer null phenotype (Inab phenotype)
anti-IFC
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Cromer: KNOW THIS!
*****KNOW: Cromer located on red cell membrane complement regulatory protein called Decay Accelerating Factor (DAF) and that the Null phenotype Inab, lacks DAF and therefore lacks all CROM antigens and can produce anti-IFC, which can be clinically significant.******
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Knops System Antibody characteristics
- IgG
- IAT
- Neutralization: Soluble CR1
Are NOT clnicaly significant & can be ignored when selecting blood. *** Give least incompatible due to the likelihood of having a positive XM.
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Knops null aka Helgeson phenotype expression
Indicates very low levels of red cell CR1 and very weak expression of Knops antigens
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Knops chemical and enzyme effects
Resistant to: Papain & ficin
Destroyed by trypsin and a-chymotrypsin
Weakened or possibly destroyed by: AET & DTT
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Knops disease associations
CR1 appears to be involved in resetting of red cells that is associated with severe P. falciparum malaria
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Knops McCb is associated with possible protection from what?
Parasites
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The Indian System high & low prevalence
- Ina (Arg46) = Low
- Inb (Pro46) = High
- Wj = High
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Indian system: Ina & Inb antibody characteristics
Reduced expression in the presence of In(Lu) phenotype
Often direct agglutinate, but IAT usually enhances.
- Not considered clinically significant
- **** However, there is one report of Inb causing HTR
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Indian system: AnWj antibody characteristic
Causes severe HTR
In(Lu) red cells should be selected for transfusion.
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OK (Oka, OKGV, & OKVM) System in one slide:
Prevalence
Chemical/Enzyme response
Ab characteristics
High prevalence
Oka - Resistant to: AET & DTT
Reactive by IAT
Possibly clinically significant
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Indian system location
Located on CD44, they glycosaminoglycan hyaluronan, a component of the extracellular matrix
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RAPH (MER2) system
One slide
Only 3 Jews identified as RAPH null phenotype
React in IAT - not clinically significant
Resistant to: Papain
Destroyed by: Trypsin, a-chymotrypsin, pronase, AET, & DTT
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John Milton Hagen
- Typically produced by thos who acquire CD108
- In elderly, sometimes associated with weak DAT's
- Reactive in IAT
- **Not considered clinically significant, however 1 case has resulted in acute HTR
- Destroyed by: proteolytic enzymes (AET & DTT)
- Not detected on cord cells
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GILL System Characteristics
- High prevalence
- Located on aquaporin 3, a member of the aquaporin superfamily of water and glycerol channels.
- Enhances permeability of RBC membrane by glycerol and water
IAT
Resistant to AET & DTT
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RHAG System
One slide
- Ola is rare
- Associated with Rhmod phenotype
RHAG4 is low prevalence - one case associated wit HDFN
Duclos & DSLK high prevalence
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FORS System
One slide
New blood group
Found on two donors from different families with the Apae phenotype
Naturally occurring Ab.
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Jr System
One slide
High Prevalence
Jra associated with drug resistance in cancer and Xenobiotics
Might be important in porphyrin hemostasis
Seen mostly in Japanese ancestry
IAT - Can cause HTR and HDFN
Resistant to AET & DTT
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Lan System
High Prevalence
IAT
Yes to HTR & HDFN
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Vel System
High Prev
Antigen expression is very weak on crod cells and varies from one person to antoher
- Mixture of IgG & IgM
- Readily activates complement
- HTR yes
- HDFN (though rare)
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High Prevalence Sda
- Agglutination of Sda+ cells may produce a "mixed-field" appearance
- When viewed microscopically, the agglutinates are retractile
- Inhibited by urine for Sda+ individuals and guinea pig urine
- Carried on Tam Horsfall Glycoprotein
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HLA Antigens
- Class I
- Bga represents HLA-B7
- Bgb = HLA-B17 (57 or 58)
- Bgc = HLA-A28 (68 OR 69)
Many do not express Bg antigens despite having the corresponding HLA antigen on their lymphocytes.
Nuisance antibodes (sometimes contaminants in reagens)
Destroyed by papain, ficin, pronase, trypsin, a-chymotrypsin, AET, & DTT
Can be stripped form red cells with chloroquine (method 2-20) or EDTA/glycine-HCL (method 2-21)
Seen in mono, leukemias, polycythemia, & hemotlytic anemias
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List of High Prevalence
- Ge2 & 3
- Cra
- Vel - Weak on cord
- Ata - Negative only in blacks
- Oka
- AnWj - Not on cord
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