Chen Y X, Peng J, Novaretti M, Reid M E, Huang C-H
Biochemistry and Molecular Genetics Laboratory and the Immunohematology Laboratory, New York Blood Center, 310 East 67th Street, New York, NY 10021, USA.
Transfusion. 2004 Mar;44(3):391-8. doi: 10.1111/j.1537-2995.2004.00650.x.
Rh CcEe antigens occur as ce, Ce, cE, or CE alleles in the RBC membrane. Their epitope structures and the location of their cis interacting products remain to be defined.
A rare blood sample from a white male whose parents are first cousins was identified. Hemagglutination was performed using standard methods. RH structure and genotype was assessed by Southern blots. Rh transcripts were obtained by gene-specific RT-PCR and sequenced. The mutation was verified by genomic PCR assays.
The donor's RBCs typed D+C-c+E-e-f(Rh6)- with a normal c dose, suggesting the Dc- phenotype. Further tests revealed a weak and qualitatively altered e expression. Southern blots indicated a genotype of Dce/dce without other gross changes. RT-PCR detected a triplet deletion (Delta685AGA687) in the Rhce gene that specifies codon 229 for arginine (Arg229). Sequencing of the region around the mutated exon 5 confirmed the donor to be homozygous for the AGA deletion.
Arg229 is invariant on external loop 4 and close to the Ala226Pro change specific for e/E polymorphism. The qualitative and quantitative alteration of e antigen defines Arg229 as a crucial component for e/E epitope presentation. Given a normal dose of c antigen, the disruption of f (Rh6) by Arg229 deletion suggests that external loop 4 is a major structural element contributing to the expression of RHCE cis interacting antigenic products.
Rh CcEe抗原以ce、Ce、cE或CE等位基因的形式存在于红细胞膜中。它们的表位结构及其顺式相互作用产物的位置仍有待确定。
鉴定出一份来自白人男性的罕见血样,其父母为近亲。采用标准方法进行血凝试验。通过Southern印迹法评估Rh结构和基因型。通过基因特异性逆转录聚合酶链反应(RT-PCR)获得Rh转录本并进行测序。通过基因组PCR分析验证突变。
供者的红细胞血型为D+C-c+E-e-f(Rh6)-,c剂量正常,提示为Dc-表型。进一步检测发现e表达微弱且性质改变。Southern印迹显示基因型为Dce/dce,无其他明显变化。RT-PCR检测到Rhce基因中有一个三联体缺失(Delta685AGA687),该缺失指定了精氨酸(Arg229)的密码子229。对突变的外显子5周围区域进行测序,证实供者为AGA缺失的纯合子。
Arg229在外部环4上是不变的,且靠近e/E多态性特有的Ala226Pro变化。e抗原的定性和定量改变将Arg229定义为e/E表位呈现的关键成分。鉴于c抗原剂量正常,Arg229缺失导致f(Rh6)破坏,提示外部环4是有助于RHCE顺式相互作用抗原产物表达的主要结构元件。