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A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13

INTRODUCTION: Leishmaniasis continues to pose a substantial health burden in 97 countries worldwide. The progression and outcome of Leishmania infection are influenced by various factors, including the cytokine milieu, the skin microbiota at the infection site, the specific Leishmania species involv...

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Autores principales: Junior, José do Espírito Santo, de Souza, Josué Lacerda, da Silva, Lener Santos, da Silva, Cilana Chagas, do Nascimento, Tuanny Arruda, de Souza, Mara Lúcia Gomes, da Cunha, Alyne Farias, Batista, Jacqueline da Silva, Neto, José Pereira de Moura, Guerra, Marcus Vinitius de Farias, Ramasawmy, Rajendranath
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10613733/
https://www.ncbi.nlm.nih.gov/pubmed/37908348
http://dx.doi.org/10.3389/fimmu.2023.1232488
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author Junior, José do Espírito Santo
de Souza, Josué Lacerda
da Silva, Lener Santos
da Silva, Cilana Chagas
do Nascimento, Tuanny Arruda
de Souza, Mara Lúcia Gomes
da Cunha, Alyne Farias
Batista, Jacqueline da Silva
Neto, José Pereira de Moura
Guerra, Marcus Vinitius de Farias
Ramasawmy, Rajendranath
author_facet Junior, José do Espírito Santo
de Souza, Josué Lacerda
da Silva, Lener Santos
da Silva, Cilana Chagas
do Nascimento, Tuanny Arruda
de Souza, Mara Lúcia Gomes
da Cunha, Alyne Farias
Batista, Jacqueline da Silva
Neto, José Pereira de Moura
Guerra, Marcus Vinitius de Farias
Ramasawmy, Rajendranath
author_sort Junior, José do Espírito Santo
collection PubMed
description INTRODUCTION: Leishmaniasis continues to pose a substantial health burden in 97 countries worldwide. The progression and outcome of Leishmania infection are influenced by various factors, including the cytokine milieu, the skin microbiota at the infection site, the specific Leishmania species involved, the genetic background of the host, and the parasite load. In endemic regions to leishmaniasis, only a fraction of individuals infected actually develops the disease. Overexpression of IL-13 in naturally resistant C57BL/6 mice renders them susceptible to L. major infection. Haplotypes constructed from several single nucleotide variant (SNV) along a chromosome fragment may provide insight into any SNV near the fragment that may be genuinely associated with a phenotype in genetic association studies. METHODS: We investigated nine SNVs (SNV1rs1881457A>C, SNV2rs1295687C>G, SNV3rs2069744C>T, SNV4rs2069747C>T, SNV5rs20541A>G, SNV6rs1295685A>G, SNV7rs848A>C, SNV8rs2069750G >C, and SNV9rs847T>C) spanning the entire IL13 gene in patients with L. guyanensis cutaneous leishmaniasis (Lg-CL). RESULTS: Our analysis did not reveal any significant association between the SNVs and susceptibility/protection against Lg-CL development. However, haplotype analysis, excluding SNV4rs2069747 and SNV8rs2069750 due to low minor allele frequency, revealed that carriers of the haplotype CCCTAAC had a 93% reduced likelihood developing Lg-CL. Similarly, the haplotypes ACCCGCT (ORadj=0.02 [95% CI 0.00–0.07]; p-value, 6.0×10(−19)) and AGCTAAC (ORadj=0.00[95% CI 0.00–0.00]; p-value 2.7×10(−12)) appeared to provide protection against the development of Lg-CL. Conversely, carriers of haplotype ACCTGCC have 190% increased likelihood of developing Lg-CL (ORadj=2.9 [95%CI 1.68–5.2]; p-value, 2.5×10(−6)). Similarly, haplotype ACCCAAT (ORadj=2.7 [95%CI 1.5–4.7]; p-value, 3.2×10(−5)) and haplotype AGCCGCC are associated with susceptibility to the development of Lg-CL (ORadj=1.7[95%CI 1.04–2.8]; p-value, 0.01). In our investigation, we also found a correlation between the genotypes of rs2069744, rs20541, rs1295685, rs847, and rs848 and plasma IL-5 levels among Lg-Cl patients. Furthermore, rs20541 showed a correlation with plasma IL-13 levels among Lg-Cl patients, while rs2069744 and rs848 showed a correlation with plasma IL-4 levels among the same group. CONCLUSIONS: Overall, our study identifies three haplotypes of IL13 associated with resistance to disease development and three haplotypes linked to susceptibility. These findings suggest the possibility of a variant outside the gene region that may contribute, in conjunction with other genes, to differences in susceptibility and partially to the pathology.
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spelling pubmed-106137332023-10-31 A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13 Junior, José do Espírito Santo de Souza, Josué Lacerda da Silva, Lener Santos da Silva, Cilana Chagas do Nascimento, Tuanny Arruda de Souza, Mara Lúcia Gomes da Cunha, Alyne Farias Batista, Jacqueline da Silva Neto, José Pereira de Moura Guerra, Marcus Vinitius de Farias Ramasawmy, Rajendranath Front Immunol Immunology INTRODUCTION: Leishmaniasis continues to pose a substantial health burden in 97 countries worldwide. The progression and outcome of Leishmania infection are influenced by various factors, including the cytokine milieu, the skin microbiota at the infection site, the specific Leishmania species involved, the genetic background of the host, and the parasite load. In endemic regions to leishmaniasis, only a fraction of individuals infected actually develops the disease. Overexpression of IL-13 in naturally resistant C57BL/6 mice renders them susceptible to L. major infection. Haplotypes constructed from several single nucleotide variant (SNV) along a chromosome fragment may provide insight into any SNV near the fragment that may be genuinely associated with a phenotype in genetic association studies. METHODS: We investigated nine SNVs (SNV1rs1881457A>C, SNV2rs1295687C>G, SNV3rs2069744C>T, SNV4rs2069747C>T, SNV5rs20541A>G, SNV6rs1295685A>G, SNV7rs848A>C, SNV8rs2069750G >C, and SNV9rs847T>C) spanning the entire IL13 gene in patients with L. guyanensis cutaneous leishmaniasis (Lg-CL). RESULTS: Our analysis did not reveal any significant association between the SNVs and susceptibility/protection against Lg-CL development. However, haplotype analysis, excluding SNV4rs2069747 and SNV8rs2069750 due to low minor allele frequency, revealed that carriers of the haplotype CCCTAAC had a 93% reduced likelihood developing Lg-CL. Similarly, the haplotypes ACCCGCT (ORadj=0.02 [95% CI 0.00–0.07]; p-value, 6.0×10(−19)) and AGCTAAC (ORadj=0.00[95% CI 0.00–0.00]; p-value 2.7×10(−12)) appeared to provide protection against the development of Lg-CL. Conversely, carriers of haplotype ACCTGCC have 190% increased likelihood of developing Lg-CL (ORadj=2.9 [95%CI 1.68–5.2]; p-value, 2.5×10(−6)). Similarly, haplotype ACCCAAT (ORadj=2.7 [95%CI 1.5–4.7]; p-value, 3.2×10(−5)) and haplotype AGCCGCC are associated with susceptibility to the development of Lg-CL (ORadj=1.7[95%CI 1.04–2.8]; p-value, 0.01). In our investigation, we also found a correlation between the genotypes of rs2069744, rs20541, rs1295685, rs847, and rs848 and plasma IL-5 levels among Lg-Cl patients. Furthermore, rs20541 showed a correlation with plasma IL-13 levels among Lg-Cl patients, while rs2069744 and rs848 showed a correlation with plasma IL-4 levels among the same group. CONCLUSIONS: Overall, our study identifies three haplotypes of IL13 associated with resistance to disease development and three haplotypes linked to susceptibility. These findings suggest the possibility of a variant outside the gene region that may contribute, in conjunction with other genes, to differences in susceptibility and partially to the pathology. Frontiers Media S.A. 2023-10-16 /pmc/articles/PMC10613733/ /pubmed/37908348 http://dx.doi.org/10.3389/fimmu.2023.1232488 Text en Copyright © 2023 Junior, Souza, Silva, Silva, Nascimento, Souza, Cunha, Batista, Neto, Guerra and Ramasawmy https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Junior, José do Espírito Santo
de Souza, Josué Lacerda
da Silva, Lener Santos
da Silva, Cilana Chagas
do Nascimento, Tuanny Arruda
de Souza, Mara Lúcia Gomes
da Cunha, Alyne Farias
Batista, Jacqueline da Silva
Neto, José Pereira de Moura
Guerra, Marcus Vinitius de Farias
Ramasawmy, Rajendranath
A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title_full A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title_fullStr A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title_full_unstemmed A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title_short A fine mapping of single nucleotide variants and haplotype analysis of IL13 gene in patients with Leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines IL-4, IL-5, and IL-13
title_sort fine mapping of single nucleotide variants and haplotype analysis of il13 gene in patients with leishmania guyanensis-cutaneous leishmaniasis and plasma cytokines il-4, il-5, and il-13
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10613733/
https://www.ncbi.nlm.nih.gov/pubmed/37908348
http://dx.doi.org/10.3389/fimmu.2023.1232488
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