Plasmodium vivax GPI-anchored micronemal antigen (PvGAMA) binds human erythrocytes independent of Duffy antigen status

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作者
Yang Cheng
Feng Lu
Bo Wang
Jian Li
Jin-Hee Han
Daisuke Ito
Deok-Hoon Kong
Lubin Jiang
Jian Wu
Kwon-Soo Ha
Eizo Takashima
Jetsumon Sattabongkot
Jun Cao
Myat Htut Nyunt
Myat Phone Kyaw
Sanjay A. Desai
Louis H. Miller
Takafumi Tsuboi
Eun-Taek Han
机构
[1] School of Medicine,Department of Medical Environmental Biology and Tropical Medicine
[2] Kangwon National University,Department of Parasitology
[3] Wuxi Medical School,Department of Clinical Laboratory
[4] Jiangnan University,Department of Parasitology
[5] Laboratory of Malaria and Vector Research (LMVR),Division of Malaria Research
[6] National Institute of Allergy and Infectious Diseases (NIAID),Department of Molecular and Cellular Biochemistry
[7] National Institutes of Health (NIH),undefined
[8] Jiangsu Institute of Parasitic Diseases,undefined
[9] The First Affiliated Hospital of Anhui Medical University,undefined
[10] College of Basic Medicine,undefined
[11] Hubei University of Medicine,undefined
[12] Proteo-Science Center,undefined
[13] Ehime University,undefined
[14] School of Medicine,undefined
[15] Kangwon National University,undefined
[16] Key Laboratory of Molecular Virology and Immunology,undefined
[17] Unit of Human Parasite Molecular and Cell Biology,undefined
[18] Institut Pasteur of Shanghai,undefined
[19] Mahidol Vivax Research Unit,undefined
[20] Faculty of Tropical Medicine,undefined
[21] Mahidol University,undefined
[22] Department of Medical Research,undefined
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摘要
Plasmodium vivax, a major agent of malaria in both temperate and tropical climates, has been thought to be unable to infect humans lacking the Duffy (Fy) blood group antigen because this receptor is critical for erythrocyte invasion. Recent surveys in various endemic regions, however, have reported P. vivax infections in Duffy-negative individuals, suggesting that the parasite may utilize alternative receptor-ligand pairs to complete the erythrocyte invasion. Here, we identified and characterized a novel parasite ligand, Plasmodium vivax GPI-anchored micronemal antigen (PvGAMA), that bound human erythrocytes regardless of Duffy antigen status. PvGAMA was localized at the microneme in the mature schizont-stage parasites. The antibodies against PvGAMA fragments inhibited PvGAMA binding to erythrocytes in a dose-dependent manner. The erythrocyte-specific binding activities of PvGAMA were significantly reduced by chymotrypsin treatment. Thus, PvGAMA may be an adhesion molecule for the invasion of Duffy-positive and -negative human erythrocytes.
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