The Non-Coding Regulatory Variant rs2863002 at chr11p11.2 Increases Neuroblastoma Risk by Affecting HSD17B12 Expression and Lipid Metabolism.

位于 chr11p11.2 的非编码调控变异 rs2863002 通过影响 HSD17B12 表达和脂质代谢来增加神经母细胞瘤的风险

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作者:Maiorino Teresa, Avitabile Marianna, Aievola Vincenzo, Montella Annalaura, Lasorsa Vito A, Bonfiglio Ferdinando, Cantalupo Mariagrazia, Cantalupo Sueva, Estinto Gilda, Tirelli Matilde, Morini Martina, Ardito Martina, Eva Alessandra, Cerbone Vincenza, Mauriello Lucia, Caterino Marianna, Ruoppolo Margherita, Maris John M, Diskin Sharon J, Iolascon Achille, Capasso Mario
期刊:Advanced Science影响因子:14.100
时间:2025起止号:2025 Sep;12(33):e15181
doi:10.1002/advs.202415181研究方向: 代谢、神经科学、细胞生物学
A Genome-wide association study (GWAS) on a European-American cohort identified chr11p11.2 as a neuroblastoma predisposition locus. Combining in-house and public genomic data from neuroblastoma cell lines, this work implicates rs2863002 as the candidate causal variant at the 11p11.2 locus, confirming its cis-regulatory activity through a luciferase reporter assay. The genetic association of rs2863002 with neuroblastoma risk is validated in an Italian case-control cohort. Using ChIP-qPCR, Hi-C, and CRISPR genome editing, this work deciphers the regulatory mechanisms at the risk locus, demonstrating that the rs2863002-C risk allele regulates HSD17B12 expression and reduces GATA3 binding affinity. In vitro functional assays and targeted lipidomic analyses reveal the involvement of the rs2863002-C risk allele in tumorigenicity and modulation of lipid metabolism in neuroblastoma cells through HSD17B12 regulation. This study provides new insights into the genetic basis of neuroblastoma and underscores the importance of post-GWAS functional characterization of risk loci in uncovering relevant biological findings for understanding complex diseases.

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