RHCE*01.22 - RHCE*ce.22
(ISBT table: RHCE-15th_July_2019)
This entry is an hybrid RHCE allele.
DHAR, R0Har, RHCE*ce 667T,697G,712G,733G,744C,787G,800A, RHCE*ce667T,697G,712G,733G,744C,787G,800A (ceHAR, ce.22), RHCE*ceHAR, RHCE-RHD(5)-RHCE, RhCE-D(5)-CE,
Molecular data
Nucleotides:
667G>T; 697C>G; 712A>G; 733C>G; 744T>C; 787A>G; 800T>A;
Amino acids: V223F; Q233E; M238V; L245V; S248S; R263G; M267K;
Hybrid allele encompassing at least one RHD exon:
RHCE(1-4)-RHD(5)-RHCE(6-10)
Comments on the molecular basis:
- mRNA analysis; "Sequence analysis revealed that intron 4 of the RHCE gene and the hybrid (allele) were identical."
- Table 1; molecular characterization assumed
- PCR pattern, exons 3, 4, 5, 6, 7 and 9
- PCR pattern
Extracellular position of one or more amino acid substitutions:
Splicing:
Unconventional prediction methods:
Phenotype
Main D phenotype: variable/discrepant (last update: Nov. 16, 2020)Reports by D phenotype
- D positive (apparently normal D or undetailed positive D)
- "strongly D+ with some monoclonal anti-D"
- "Polyclonal anti-D sera usually fail to induce agglutination, sometimes even in the indirect antiglobulin test, although anti-D can be eluted from the cells after absorption."
- Discrepant D phenotype (negative or positive depending on anti-D reagents and techniques)
- "strongly D+ with some monoclonal anti-D"
- "Polyclonal anti-D sera usually fail to induce agglutination, sometimes even in the indirect antiglobulin test, although anti-D can be eluted from the cells after absorption."
- Weak D phenotype
- "strongly D+ with some monoclonal anti-D"
- "Polyclonal anti-D sera usually fail to induce agglutination, sometimes even in the indirect antiglobulin test, although anti-D can be eluted from the cells after absorption."
Other RH phenotypes: RH:-2, -3, 4, 5, -12, 33, 50,
- RH:-2 inferred from the reported RHCE phenotypes of the carriers
- RH:-3 inferred from the reported RHCE phenotypes of the carriers
- RH:4
- RH:5 see also "Additional comments" section on the RhesusBase http://www.rhesusbase.info/RHDDHAR.htm weak very weak; Table 3 weak
- RH:-12
- RH:33 Table 2 review no new sample
- RH:50 see also "Additional comments" section on the RhesusBase http://www.rhesusbase.info/RHDDHAR.htm Table 2 review no new sample
Serology with monoclonal anti-D
- 15 anti-D non-reactive with variant, out of 16 monoclonal IgG tested (Table 3)
- 18 anti-D non-reactive with variant, out of 22 monoclonal IgG tested; 13 IgM were also used; epitope pattern mapping only detected epitopes 5 and 6/7 (Table 1, Table 2)
- multiple anti-D tested (Table 2)
- reactivity with some FDA-licensed anti-D reagents (Table 1)
- Epitope pattern: only epitopes D5 and D6/7 were detectable; compatible with other other R0Har Rh:33 individuals.
Antigen Density (Ag/RBC)
More phenotype data
Rhesus Similarity Index
Haplotype
Main CcEe phenotype association: ce (last update: Nov. 16, 2020)| ce | Ce | cE | CE | |
|---|---|---|---|---|
| ce | 6 | 0 | 0 | 0 |
| Ce | 0 | 0 | 0 | |
| cE | 0 | 0 | ||
| CE | 0 |
Reports by CcEe phenotype
Reports by allele association
Alloimmunization
Antibodies in carriers
Antibody specificity: D (RH1)
Summary: allo-anti-D (last update: May 16, 2020)Detailed information
-
Beckers EA et al. Transfusion (1996)
- Ab specificity: D (RH1)
- Number (auto- or allo-):
- Number listed as allo-: 1
- Number listed as auto-: 0
- Number of carriers of the allele assessed: 3
- DAT: ND
- Autologuous control: ND
- Elution: ND
- Autoadsorption: adsorption-elution with patient's own RBCs and 2 other RHef00621 probands yielded no Ab (negative)
- Titer: ND
- Was anti-LW excluded?: ND
- Other antibodies detected: none
- Cross matches (with Ab and RBCs from different partial types): anti-D did not agglutinate RBCs of two samples with the same genotype; cross-testing was positive with samples of phenotypes: RHef00587, RHef00585, RHef00586, RHef00578, RHef00581, RHef00582, RHef00583 (Table 4)
- Transfusion history: none
- Pregnancy history:
- Anti-D Ig history: none
- Context: pregnancy
- Hemolytic consequences: "neonatal complications were not mentioned in any proposita"
- Comment: anti-D was detected only on bromelain and papain-treated cells
-
Daniels G et al. Br J Haematol (2013)
(review; Table I)
- Ab specificity: D (RH1)
- Number (auto- or allo-):
- Number listed as allo-: no new case detailed (listed as allo-anti-D)
- Number listed as auto-: NA
- Number of carriers of the allele assessed: NA
- DAT: NA
- Autologuous control: NA
- Elution: NA
- Autoadsorption: NA
- Titer: NA
- Was anti-LW excluded?: NA
- Other antibodies detected: NA
- Cross matches (with Ab and RBCs from different partial types): NA
- Transfusion history: NA
- Pregnancy history:
- Anti-D Ig history: NA
- Context: NA
- Hemolytic consequences: NA
- Comment: list of D variants associated with alloanti-D formation
-
Hazenberg CA et al. Transfusion (1996)
- Ab specificity: D (RH1)
- Number (auto- or allo-):
- Number listed as allo-: 1
- Number listed as auto-:
- Number of carriers of the allele assessed:
- DAT: ND
- Autologuous control: ND
- Elution: ND
- Autoadsorption: ND
- Titer: 8 (score 36)
- Was anti-LW excluded?:
- Other antibodies detected: anti-E reactivity (only in a two-step bromelin technique)
- Cross matches (with Ab and RBCs from different partial types): anti-D did not react with other other R0Har Rh:33 individuals.
- Transfusion history:
- Pregnancy history:
- Anti-D Ig history:
- Context: pregnancy
- Hemolytic consequences: HDFN: neonate readmitted on day 6, required intensive phototherapy, recovery was uneventful
- Comment:
Antibodies in D negative recipients
Alloimmunization in recipients: expected to be possible, see phenotype data
Reports
Summary: few descriptions, in individuals of Caucasian descent, or compatible with such descent (last update: April 28, 2020)Detailed reports
- 3.0 unrelated donors Caucasian
- 2 related samples Dutch
- 1 sample White, in German or Austrian population
- 1/163 selected variants included for the development of a genotyping assay mainly in the Dutch population (samples may have been included in other studies)
- 1 alleles in 226 patients SCD children systematically genotyped in an alloimmunization study in the USA population (Philadelphia)
- 8/627 weak D typing (95% from patients, 5% from donors; 21,2% were identified as RHef00442 or RHef00446 by authors, "mostly (…) inconclusive serology consequent to recent transfusion") in the Belgian (Flanders) population
Allele or phenotype frequency
Structure mapping
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References
- International Society of Blood Transfusion et al. International Society of Blood Transfusion (ISBT) allele table Online ressource, 1935. — Online ressource — [RHeference]
- Hazenberg CA et al. Hemolytic disease of the newborn caused by alloanti-D from an R0Har r Rh:33 mother. Transfusion, 1996. [Citation] [RHeference]
- Beckers EA et al. The R0Har RH:33 phenotype results from substitution of exon 5 of the RHCE gene by the corresponding exon of the RHD gene. Br J Haematol, 1996. [Citation] [RHeference]
- Beckers EA et al. The RoHar antigenic complex is associated with a limited number of D epitopes and alloanti-D production: a study of three unrelated persons and their families. Transfusion, 1996. [Citation] [RHeference]
- Gassner C et al. RHD/CE typing by polymerase chain reaction using sequence-specific primers. Transfusion, 1997. [Citation] [RHeference]
- Maaskant-van Wijk PA et al. Genotyping of RHD by multiplex polymerase chain reaction analysis of six RHD-specific exons. Transfusion, 1998. [Citation] [RHeference]
- Avent ND et al. The rhesus blood group system: insights from recent advances in molecular biology. Transfus Med Rev, 1999. [Citation] [RHeference]
- Flegel WA et al. The RHCE allele ceCF: the molecular basis of Crawford (RH43). Transfusion, 2006. [Citation] [RHeference]
- Westhoff CM et al. Rh complexities: serology and DNA genotyping. Transfusion, 2007. [Citation] [RHeference]
- Flegel WA et al. DCS-1, DCS-2, and DFV share amino acid substitutions at the extracellular RhD protein vestibule. Transfusion, 2008. [Citation] [RHeference]
- Schmid P et al. Specific amino acid substitutions cause distinct expression of JAL (RH48) and JAHK (RH53) antigens in RhCE and not in RhD. Transfusion, 2010. [Citation] [RHeference]
- Wagner FF and Flegel WA et al. The Human RhesusBase Online ressource, 2011. — Online ressource — [RHeference]
- Chou ST et al. High prevalence of red blood cell alloimmunization in sickle cell disease despite transfusion from Rh-matched minority donors. Blood, 2013. [Citation] [RHeference]
- Daniels G et al. Variants of RhD--current testing and clinical consequences. Br J Haematol, 2013. [Citation] [RHeference]
- Haer-Wigman L et al. RHD and RHCE variant and zygosity genotyping via multiplex ligation-dependent probe amplification. Transfusion, 2013. [Citation] [RHeference]
- Van Sandt VS et al. RHD variants in Flanders, Belgium. Transfusion, 2015. [Citation] [RHeference]
- Floch A et al. Comment from Rheference Online ressource, 2020. — Online ressource — [RHeference]
Last update: Nov. 26, 2020