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Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil

BACKGROUND: The atypical chemokine receptor 1 (ACKR1) gene encodes the Duffy blood group antigens in two allelic forms: FY*A (FY*01) and FY*B (FY*02), which define the Fy(a+b-), Fy(a-b+), and Fy(a+b+) phenotypes. FY*BES (FY*02N.01) is a single T to C substitution at nucleotide -67 that prevents the...

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Autores principales: Langhi, Dante, Albuquerque, Sérgio, Serafim, Rui, Duarte, Gustavo de Carvalho, Covas, Dimas Tadeu, Bordin, José O.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Sociedade Brasileira de Medicina Tropical - SBMT 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9344938/
https://www.ncbi.nlm.nih.gov/pubmed/35946633
http://dx.doi.org/10.1590/0037-8682-0490-2021
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author Langhi, Dante
Albuquerque, Sérgio
Serafim, Rui
Duarte, Gustavo de Carvalho
Covas, Dimas Tadeu
Bordin, José O.
author_facet Langhi, Dante
Albuquerque, Sérgio
Serafim, Rui
Duarte, Gustavo de Carvalho
Covas, Dimas Tadeu
Bordin, José O.
author_sort Langhi, Dante
collection PubMed
description BACKGROUND: The atypical chemokine receptor 1 (ACKR1) gene encodes the Duffy blood group antigens in two allelic forms: FY*A (FY*01) and FY*B (FY*02), which define the Fy(a+b-), Fy(a-b+), and Fy(a+b+) phenotypes. FY*BES (FY*02N.01) is a single T to C substitution at nucleotide -67 that prevents the FY*B from being expressed in red blood cells (RBCs). METHODS: We evaluated 250 residents from a Brazilian malarial endemic region (RsMR). All individuals were phenotyped for Fy(a) and Fy(b) antigens and genotyped for FY*A, FY*B, FY*B ( SE ) , and FY*B ( weak ) alleles. RESULTS: Among the 250 individuals, 209 (83.6%) reported previous malaria infection, and 41 (16.4%) did not. The Fy(a+b+) phenotype was present in 97/250 (38.8%), while the Fy(a-b-) was present in 7/250 (2.8%). The FY*A/FY*B was found in 130/250 (52%) and the FY*A/FY*A in 45/250 (18%). The c.1-67>TC was present, in homozygosity, in 11/250 (4.4%). Among 34 individuals with the Fy(a+b-) and FYA*/FYB* mutations, 4/34 (11.8%) had homozygosity for the c.1-67T>C. One individual presented the Fy(a+b-), FY*A/FY*B, and c.1-67T>C in homozygosis, whereas the other presented the Fy(a+b-), FY*A/FY*A, and c.1-67T>C in heterozygosis. CONCLUSIONS: We reported a low prevalence of the Fy(a-b-) in persons who had previously been infected with Plasmodium vivax (67.5%). We observed that 102/141 (72.3%) individuals expressing the Fy(b) antigen had a P. vivax infection, indicating the importance of the Fy(b) antigen, silenced by a c.1-67T>C mutation in homozygosis, in preventing the P. vivax infection. We showed that the c.1-67T>C mutation in the FY*A did not silence the FY*A expression on RBCs.
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spelling pubmed-93449382022-08-18 Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil Langhi, Dante Albuquerque, Sérgio Serafim, Rui Duarte, Gustavo de Carvalho Covas, Dimas Tadeu Bordin, José O. Rev Soc Bras Med Trop Major Article BACKGROUND: The atypical chemokine receptor 1 (ACKR1) gene encodes the Duffy blood group antigens in two allelic forms: FY*A (FY*01) and FY*B (FY*02), which define the Fy(a+b-), Fy(a-b+), and Fy(a+b+) phenotypes. FY*BES (FY*02N.01) is a single T to C substitution at nucleotide -67 that prevents the FY*B from being expressed in red blood cells (RBCs). METHODS: We evaluated 250 residents from a Brazilian malarial endemic region (RsMR). All individuals were phenotyped for Fy(a) and Fy(b) antigens and genotyped for FY*A, FY*B, FY*B ( SE ) , and FY*B ( weak ) alleles. RESULTS: Among the 250 individuals, 209 (83.6%) reported previous malaria infection, and 41 (16.4%) did not. The Fy(a+b+) phenotype was present in 97/250 (38.8%), while the Fy(a-b-) was present in 7/250 (2.8%). The FY*A/FY*B was found in 130/250 (52%) and the FY*A/FY*A in 45/250 (18%). The c.1-67>TC was present, in homozygosity, in 11/250 (4.4%). Among 34 individuals with the Fy(a+b-) and FYA*/FYB* mutations, 4/34 (11.8%) had homozygosity for the c.1-67T>C. One individual presented the Fy(a+b-), FY*A/FY*B, and c.1-67T>C in homozygosis, whereas the other presented the Fy(a+b-), FY*A/FY*A, and c.1-67T>C in heterozygosis. CONCLUSIONS: We reported a low prevalence of the Fy(a-b-) in persons who had previously been infected with Plasmodium vivax (67.5%). We observed that 102/141 (72.3%) individuals expressing the Fy(b) antigen had a P. vivax infection, indicating the importance of the Fy(b) antigen, silenced by a c.1-67T>C mutation in homozygosis, in preventing the P. vivax infection. We showed that the c.1-67T>C mutation in the FY*A did not silence the FY*A expression on RBCs. Sociedade Brasileira de Medicina Tropical - SBMT 2022-08-05 /pmc/articles/PMC9344938/ /pubmed/35946633 http://dx.doi.org/10.1590/0037-8682-0490-2021 Text en https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License
spellingShingle Major Article
Langhi, Dante
Albuquerque, Sérgio
Serafim, Rui
Duarte, Gustavo de Carvalho
Covas, Dimas Tadeu
Bordin, José O.
Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title_full Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title_fullStr Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title_full_unstemmed Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title_short Serological and Molecular Study of the Duffy Blood Group among Malarial Endemic Region Residents in Brazil
title_sort serological and molecular study of the duffy blood group among malarial endemic region residents in brazil
topic Major Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9344938/
https://www.ncbi.nlm.nih.gov/pubmed/35946633
http://dx.doi.org/10.1590/0037-8682-0490-2021
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