Validation and functional characterization of GWAS-identified variants for chronic lymphocytic leukemia: a CRuCIAL study
Metadata
Show full item recordAuthor
García Martín, Paloma; Moñiz Díez, Ana; Sánchez Maldonado, José Manuel; Cabrera Serrano, Antonio José; Hernández Mohedo, Francisca; González Sierra, Pedro Antonio; Cañadas Garre, Marisa; López Nevot, Miguel Ángel; Jurado Chacón, Manuel; Sáinz Pérez, JuanEditorial
Nature
Date
2022-05-17Referencia bibliográfica
García-Martín, P... [et al.]. Validation and functional characterization of GWAS-identified variants for chronic lymphocytic leukemia: a CRuCIAL study. Blood Cancer J. 12, 79 (2022). [https://doi.org/10.1038/s41408-022-00676-8]
Sponsorship
European Union's Horizon 2020 research and innovation program 856620; Instituto de Salud Carlos III PI17/02256 PI20/01845; Consejeria de Economia, Conocimiento, Empresas y Universidad (Granada, Spain) A-CTS-448-UGR18 Consejeria de Transformacion Economica, Industria, Conocimiento y Universidades (Sevilla, Spain) PY20/01282; Generalitat de Catalunya; General Electric 17SGR437; Gilead Sciences GLD17/00282; "Xarxa de Bancs de tumors" - Pla Director d'Oncologia de Catalunya (XBTC); Fondazione AIRC per la ricerca sul cancro Fondazione Cariplo TRIDEO 16923 AIRC IG21436; Spanish Association Against Cancer (AECC) Scientific Foundation grant GCTRA18022MORE; Consortium for Biomedical Research in Epidemiology and Public Health (CIBERESP), action GenriskAbstract
In conclusion, this study confirmed the association of 31 GWASidentified
SNPs with CLL risk and shed some light on the function
of some of these biomarkers in the modulation of TReg, B, and T
cell differentiation and proliferation, blood concentrations of B
cell-related proteins, cell survival, and the expression of immuneand
non-immune-related loci. Though outside the scope of the
current study, it is important to mention that additional functional
studies using blood samples from CLL patients are still required to
validate our findings and to decipher the exact biological
mechanisms behind the observed associations. A potential
limitation of this work was the relatively small population size of
the CRuCIAL cohort that hampered the validation of the SNPs
showing modest associations.