The purpose of this study was to conduct a two-stage case control association study including 654 acute myeloid leukaemia (AML) patients and 3477 controls ascertained through the NuCLEAR consortium to evaluate the effect of 27 immune-related single nucleotide polymorphisms (SNPs) on AML risk. In a pooled analysis of cohort studies, we found that carriers of the IL13rs1295686A/A genotype had an increased risk of AML (PCorr = 0.0144) whereas carriers of the VEGFArs25648T allele had a decreased risk of developing the disease (PCorr = 0.00086). In addition, we found an association of the IL8rs2227307 SNP with a decreased risk of developing AML that remained marginally significant after multiple testing (PCorr = 0.072). Functional experiments suggested that the effect of the IL13rs1295686 SNP on AML risk might be explained by its role in regulating IL1Ra secretion that modulates AML blast proliferation. Likewise, the protective effect of the IL8rs2227307 SNP might be mediated by TLR2-mediated immune responses that affect AML blast viability, proliferation and chemorresistance. Despite the potential interest of these results, additional functional studies are still warranted to unravel the mechanisms by which these variants modulate the risk of AML. These findings suggested that IL13, VEGFA and IL8 SNPs play a role in modulating AML risk.

Host immune genetic variations influence the risk of developing acute myeloid leukaemia: results from the NuCLEAR consortium / Sanchez-Maldonado, J. M.; Campa, D.; Springer, J.; Badiola, J.; Niazi, Y.; Moniz-Diez, A.; Hernandez-Mohedo, F.; Gonzalez-Sierra, P.; Ter Horst, R.; Macauda, A.; Brezina, S.; Cunha, C.; Lackner, M.; Lopez-Nevot, M. A.; Fianchi, L.; Pagano, L.; Lopez-Fernandez, E.; Potenza, L.; Luppi, M.; Moratalla, L.; Rodriguez-Sevilla, J. J.; Fonseca, J. E.; Tormo, M.; Solano, C.; Clavero, E.; Romero, A.; Li, Y.; Lass-Florl, C.; Einsele, H.; Vazquez, L.; Loeffler, J.; Hemminki, K.; Carvalho, A.; Netea, M. G.; Gsur, A.; Dumontet, C.; Canzian, F.; Forsti, A.; Jurado, M.; Sainz, J.. - In: BLOOD CANCER JOURNAL. - ISSN 2044-5385. - 10:7(2020), pp. 1-11. [10.1038/s41408-020-00341-y]

Host immune genetic variations influence the risk of developing acute myeloid leukaemia: results from the NuCLEAR consortium

Potenza L.;Luppi M.;
2020

Abstract

The purpose of this study was to conduct a two-stage case control association study including 654 acute myeloid leukaemia (AML) patients and 3477 controls ascertained through the NuCLEAR consortium to evaluate the effect of 27 immune-related single nucleotide polymorphisms (SNPs) on AML risk. In a pooled analysis of cohort studies, we found that carriers of the IL13rs1295686A/A genotype had an increased risk of AML (PCorr = 0.0144) whereas carriers of the VEGFArs25648T allele had a decreased risk of developing the disease (PCorr = 0.00086). In addition, we found an association of the IL8rs2227307 SNP with a decreased risk of developing AML that remained marginally significant after multiple testing (PCorr = 0.072). Functional experiments suggested that the effect of the IL13rs1295686 SNP on AML risk might be explained by its role in regulating IL1Ra secretion that modulates AML blast proliferation. Likewise, the protective effect of the IL8rs2227307 SNP might be mediated by TLR2-mediated immune responses that affect AML blast viability, proliferation and chemorresistance. Despite the potential interest of these results, additional functional studies are still warranted to unravel the mechanisms by which these variants modulate the risk of AML. These findings suggested that IL13, VEGFA and IL8 SNPs play a role in modulating AML risk.
2020
10
7
1
11
WOS:000549600400001
2-s2.0-85087929703
32678078
Host immune genetic variations influence the risk of developing acute myeloid leukaemia: results from the NuCLEAR consortium / Sanchez-Maldonado, J. M.; Campa, D.; Springer, J.; Badiola, J.; Niazi, Y.; Moniz-Diez, A.; Hernandez-Mohedo, F.; Gonzalez-Sierra, P.; Ter Horst, R.; Macauda, A.; Brezina, S.; Cunha, C.; Lackner, M.; Lopez-Nevot, M. A.; Fianchi, L.; Pagano, L.; Lopez-Fernandez, E.; Potenza, L.; Luppi, M.; Moratalla, L.; Rodriguez-Sevilla, J. J.; Fonseca, J. E.; Tormo, M.; Solano, C.; Clavero, E.; Romero, A.; Li, Y.; Lass-Florl, C.; Einsele, H.; Vazquez, L.; Loeffler, J.; Hemminki, K.; Carvalho, A.; Netea, M. G.; Gsur, A.; Dumontet, C.; Canzian, F.; Forsti, A.; Jurado, M.; Sainz, J.. - In: BLOOD CANCER JOURNAL. - ISSN 2044-5385. - 10:7(2020), pp. 1-11. [10.1038/s41408-020-00341-y]
Sanchez-Maldonado, J. M.; Campa, D.; Springer, J.; Badiola, J.; Niazi, Y.; Moniz-Diez, A.; Hernandez-Mohedo, F.; Gonzalez-Sierra, P.; Ter Horst, R.; M...espandi
File in questo prodotto:
File Dimensione Formato  
s41408-020-00341-y.pdf

Open access

Tipologia: Versione pubblicata dall'editore
Dimensione 656.8 kB
Formato Adobe PDF
Visualizza/Apri
656.8 kB Adobe PDF Visualizza/Apri
Pubblicazioni consigliate

Licenza Creative Commons
I metadati presenti in IRIS UNIMORE sono rilasciati con licenza Creative Commons CC0 1.0 Universal, mentre i file delle pubblicazioni sono rilasciati con licenza Attribuzione 4.0 Internazionale (CC BY 4.0), salvo diversa indicazione.
In caso di violazione di copyright, contattare Supporto Iris

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11380/1223078
Citazioni
  • ???jsp.display-item.citation.pmc??? 1
  • Scopus 2
  • ???jsp.display-item.citation.isi??? 2
social impact