Forssman J.Die Herstellunhochwertiger spezifisher Schafhämolysine ohne Verwendunvon Schafblut:Ein BeitraZur Lehre von heterologer Antikörperbildung[J]. Biochemische Zeitung,2010:78-115.

Hult AK, Yazer MH, Jrgensen R, et al. WeaA phenotypes associated with novel alleles carryinthe A2-related 1061C deletion and various missense substitutions[J]. Transfusion,2010,50:1471-1486.

Seltsam A, Wagner FF, Gruger D, et al. Weablood group B phenotypes may be caused by variations in the CCAAT-bindinfactor/NF-Y enhancer region of the ABO gene[J].Transfusion, 2007,47:2330-2335.

YuL-C, ChanC-Y, Twu Y-C, Lin M. Human histo-blood group ABO glycosyltransferase genes:different enhancer structures with different transcriptional activities[J]. Biochem Biophys Res Comm, 2000,273:459-466.

Thuresson B, Chester MA, Storry JR,et al. ABO transcript levels in peripheral blood and erythropoietic culture show different allele-related patterns independent of the CBF/NF-Y enhancer motif and multiple novel allele-specifi c variations in the 5'-and 3'-noncodinregions[J].Transfusion,2008,48:493-504.

Marion E Reid. PDh, Academic Press is an imprint of elesvier fasts boothe blood group antigen[M]. 3rd ed. 2012:31-51.

Ferraro M. The rare red cell phenotype, FOR (-), in an African-American[abstract][J].Transfusion,2000,40:121-129.

Lowe JB, Marth JD. A genetic approach to mammalian glycan function[J]. Annu Rev Biochem,2003,72:643-691.

Tormey CA, StacG. Immunogenicity of blood group antigens:a mathematical model corrected for antibody evanescence with exclusion of naturally occurrinand pregnancy-related antibodies[J]. Blood,2009,114:4279-4282.

Daniels G. Human blood groups:Introduction[M]. 3rd ed. Oxford, UK:Wiley-Blackwell, 2013:44-49.

Denomme GA. Molecular basis of blood group expression[J]. Transfus Apher Sci,2011,44:53-63.

Denomme GA. Prospects for the provision of genotyped blood for transfusion[J]. Br J Haematol,2013,163:3-9.

Mielke JH, KonigsberLW, Relethford JH. Human biological variation[M]. New York:Oxford University Press,2006:112-115.

Anstee DJ. The relationship between blood groups and disease[J]. Blood,2010,115:635-636.

Lomas-Francis C, Reid ME. The Dombrocblood group system:a review[J]. Immunohematology,2010,26:71-78.

Oliver C, Blake D, Henry S. Modelintransfusion reactions and predictinin vivo cell survival with kodecytes[J]. Transfusion,2011,51:1723-1730.

Henry SM. Modification of red blood cells for laboratory quality control use[J]. Curr Opin Hematol,2009,16:467-472.

Svensson L, Hult AK, Stamps R, et al. Forssman expression on human erythrocytes:biochemical and genetic evidence of a new histo-blood group system[J]. Blood,2013,121:1459-1468.

PatnaiSK, HelmberW, Blumenfeld OO. BGMUT:NCBI dbRBC database of allelic variations of genes encodinantigens of blood group systems[J]. Nucleic Acids Res, 2012,40:D1023-1024.

Castilho L, Baleotti WJ, Tossas E, et al. Molecular studies of DO alleles reveal that JO is more prevalent than HY in Brazil, whereas HY is more prevalent in New York[J]. Immunohematology. 2008,24:135-137.

Baleotti W Jr, Suzuki RB, Polotto M,et al. A PCR-based strategy for Dombrocscreeninin Brazilian blood donors reveals a novel allele:the DO*A-WL[J]. J Clin Lab Anal,2011,25:79-82.

Piassi FC, Santos SM, Castilho LM, et al. Dombrocgenotypinin Brazilian blood donors reveals different regional frequencies of the HY allele[J]. Rev Bras Hematol Hemoter,2013,35:400-403.

Hirvonen T, Suila H, Kotovuori A, et al. The blood group antigen as a marker for umbilical cord blood-derived mesenchymal stem cells[J]. Stem Cells Develop,2012,21:455-464.