Abstract

The Kell blood group is composed of two proteins, Kell and XK, linked by a single disulfide bond. Kell is a 93 kDa type II membrane glycoprotein and XK a 50.9 kDa protein that traverse the membrane ten times. Kell protein exists in many polymorphic forms and some of its antigens are highly immunogenic and can cause severe reactions if mismatched blood is transfused. Maternal alloimmunization to Kell antigens can also cause fetal and neonatal anemia. Recent studies from our laboratory demonstrated that Kell is an enzyme that activates the endothelins and has marked preference for endothelin-3. The endothelins are potent vasoconstrictors and are also involved in developmental processes. The function of XK is not known but its absence, the McLeod phenotype, is associated with red cell acenthocytosis and late onset forms of muscular and neurological abnormalities. Our objectives are to define the define the physiological functions of the Kell/XK complex and to determine the cellular mechanisms by which antibodies to kell elicit fetal and neonatal anemia. Recent studies from our laboratory demonstrated that Kell is an enzyme that activates the endothelins and has marked preference for endothelin-3. The endothelins are potent vasoconstrictors and are also involved in developmental processes. The function of XK is not known but its absence, the McLeod phenotype, is associated with red cell acanthocytosis and late onset forms of muscular and neurological abnormalities. Our objectives are to define the physiological functions of the Kell/XK complex and to determine the cellular mechanisms by which antibodies to Kell elicit fetal and neonatal anemia. To achieve our objectives we have three specific aims. 1. To identify the domains of Kell that are necessary for substrate and enzymatic specificity and to compare the enzymatic properties of wild-type Kell to those of KEL1 and KEL6. The KEL1 and KEL6 polymorphisms have distinctive distributions in persons of African heritage, as compared to Caucasians, and may have developed due to selective pressures. 2. To determine the complementary roles of Kell and XK proteins, by studying targeted disruption of the Kell and XK loci and mice. 3. To determine the mechanisms by which antibodies to Kell suppress erythropoiesis, with emphasis on the interactions of Kell antibodies with nascent Kell antigens that occur on erythroid progenitor cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Specialized Center (P50)
Project #
5P50HL054459-07
Application #
6564982
Study Section
Project Start
2002-01-01
Project End
2002-12-31
Budget Start
Budget End
Support Year
7
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
New York Blood Center
Department
Type
DUNS #
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Migliaccio, Anna Rita (2018) A vicious interplay between genetic and environmental insults in the etiology of blood cancers. Exp Hematol 59:9-13
Ciaffoni, Fiorella; Cassella, Elena; Varricchio, Lilian et al. (2015) Activation of non-canonical TGF-?1 signaling indicates an autoimmune mechanism for bone marrow fibrosis in primary myelofibrosis. Blood Cells Mol Dis 54:234-41
Hricik, Todd; Federici, Giulia; Zeuner, Ann et al. (2013) Transcriptomic and phospho-proteomic analyzes of erythroblasts expanded in vitro from normal donors and from patients with polycythemia vera. Am J Hematol 88:723-9
Poletto, Valentina; Rosti, Vittorio; Villani, Laura et al. (2012) A3669G polymorphism of glucocorticoid receptor is a susceptibility allele for primary myelofibrosis and contributes to phenotypic diversity and blast transformation. Blood 120:3112-7
Huang, Cheng-Han; Ye, Mao (2010) The Rh protein family: gene evolution, membrane biology, and disease association. Cell Mol Life Sci 67:1203-18
Zhu, Xiang; Rivera, Alicia; Golub, Mari S et al. (2009) Changes in red cell ion transport, reduced intratumoral neovascularization, and some mild motor function abnormalities accompany targeted disruption of the Mouse Kell gene (Kel). Am J Hematol 84:492-8
Mutschler, Manuel; Magin, Angela S; Buerge, Martina et al. (2009) NF-E2 overexpression delays erythroid maturation and increases erythrocyte production. Br J Haematol 146:203-17
Walker, Ruth H; Danek, Adrian; Uttner, Ingo et al. (2007) McLeod phenotype without the McLeod syndrome. Transfusion 47:299-305
Ford, Louise; Lobo, Cheryl A; Rodriguez, Marilis et al. (2007) Differential antibody responses to Plasmodium falciparum invasion ligand proteins in individuals living in malaria-endemic areas in Brazil and Cameroon. Am J Trop Med Hyg 77:977-83
Peng, Jianbin; Redman, Colvin M; Wu, Xu et al. (2007) Insights into extensive deletions around the XK locus associated with McLeod phenotype and characterization of two novel cases. Gene 392:142-50

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