Literature DB >> 8329720

Immunochemical characterization of rhesus proteins with antibodies raised against synthetic peptides.

P Hermand1, I Mouro, M Huet, C Bloy, K Suyama, J Goldstein, J P Cartron, P Bailly.   

Abstract

Rabbit polyclonal antibodies were raised against synthetic peptides corresponding to hydrophilic regions of the human Rhesus (Rh) IX cDNA-encoded polypeptide predicted to be extracellularly or intracellularly exposed in the topologic model of the Rh blood group protein. Four antibodies encompassing residues 33-45 (MPC1), 224-233 (MPC4), 390-404 (MPC6), and 408-416 (MPC8) were characterized and compared with a polyclonal anti-Rh protein obtained by immunization with purified Rh proteins. All antibodies had specificity for authentic Rh polypeptides and reacted on Western blot with Rh proteins immunoprecipitated with human monoclonal anti-RhD, -c, and -E. MPC1, but not the other antibodies, agglutinated all human erythrocytes except Rhnull and Rhmod cells, which either lack totally or are severely deficient in Rh proteins, respectively. Immunoblotting analysis with membrane proteins from common and rare variants showed that MPC1 and MPC8 reacted in Western blot with 32-Kd Rh polypeptides from all common red blood cells except those from Rhnull and Rhmod, indicating that peptide regions 33-45 and 408-416 may be common to several if not all Rh proteins, whatever the Rh blood group specificity. MPC4 reacted only with membrane preparations from cells carrying the E antigen, whereas MPC6 recognized preferentially the Rh proteins from E and Ee preparations, suggesting that the protein encoded by the RhIXb cDNA carries the E and/or e antigen(s). Immunoadsorption experiments using inside-out or right-side-out sealed vesicules from DccEE red blood cells as competing antigen showed that the MPC6 and MPC8 antibodies bound only to the cytoplasmic side of the erythrocyte membrane, thus providing evidence for the intracellular orientation of the C-terminal 27 residues of the Rh polypeptides. Attempts to transiently or stably express the Rh polypeptides. Attempts to transiently or stably express the Rh cDNA in eukaryotic cells were largely unsuccessful, suggesting that Rh antigen expression at the cell surface requires correct transport and/or folding of the Rh proteins, possibly as a complex with one-membrane proteins of the Rh cluster that are lacking in Rhnull cells.

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Year:  1993        PMID: 8329720

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  9 in total

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Authors:  I Salvignol; P Calvas; W W Socha; Y Colin; C Le Van Kim; P Bailly; J Ruffié; J P Cartron; A Blancher
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2.  The RHD gene is highly detectable in RhD-negative Japanese donors.

Authors:  H Okuda; M Kawano; S Iwamoto; M Tanaka; T Seno; Y Okubo; E Kajii
Journal:  J Clin Invest       Date:  1997-07-15       Impact factor: 14.808

3.  Present situation of the analysis of Rh genes.

Authors:  S Ikemoto; F Umenishi; S Iwamoto; S Tsuchida; T Oyamada; E Kajii
Journal:  Biochem J       Date:  1995-07-15       Impact factor: 3.857

4.  The LW blood group glycoprotein is homologous to intercellular adhesion molecules.

Authors:  P Bailly; P Hermand; I Callebaut; H H Sonneborn; S Khamlichi; J P Mornon; J P Cartron
Journal:  Proc Natl Acad Sci U S A       Date:  1994-06-07       Impact factor: 11.205

5.  The two-gene model of the RH blood-group locus.

Authors:  J P Cartron; C Le Van Kim; B Cherif-Zahar; I Mouro; C Rouillac; Y Colin
Journal:  Biochem J       Date:  1995-03-15       Impact factor: 3.857

6.  The human Kell blood group binds the erythroid 4.1R protein: new insights into the 4.1R-dependent red cell membrane complex.

Authors:  Slim Azouzi; Emmanuel Collec; Narla Mohandas; Xiuli An; Yves Colin; Caroline Le Van Kim
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7.  Molecular characterization of the Rh-like locus and gene transcripts from the rhesus monkey (Macaca mulatta).

Authors:  I Mouro; C Le Van Kim; B Cherif-Zahar; I Salvignol; A Blancher; J P Cartron; Y Colin
Journal:  J Mol Evol       Date:  1994-02       Impact factor: 2.395

8.  Intricate combinatorial patterns of exon splicing generate multiple Rh-related isoforms in human erythroid cells.

Authors:  E Kajii; F Umenishi; T Omi; S Ikemoto
Journal:  Hum Genet       Date:  1995-06       Impact factor: 4.132

9.  Mice expressing RHAG and RHD human blood group genes.

Authors:  Dominique Goossens; Nelly da Silva; Sylvain Metral; Ulrich Cortes; Isabelle Callebaut; Julien Picot; Isabelle Mouro-Chanteloup; Jean-Pierre Cartron
Journal:  PLoS One       Date:  2013-11-18       Impact factor: 3.240

  9 in total

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