Nielsen Kaspar René, Rodrigo-Domingo Maria, Steffensen Rudi, Baech John, Bergkvist Kim S, Oosterhof Liesbeth, Schmitz Alexander, Bødker Julie Støve, Johansen Preben, Vogel Ulla, Vangsted Anette, Dybkær Karen, Bøgsted Martin, Johnsen Hans Erik
a Department of Clinical Immunology , Aalborg University Hospital , Aalborg , Denmark.
b Department of Haematology , Aalborg University Hospital , Aalborg , Denmark.
Leuk Lymphoma. 2017 Nov;58(11):2695-2704. doi: 10.1080/10428194.2017.1306643. Epub 2017 Apr 9.
The origin of multiple myeloma depends on interactions with stromal cells in the course of normal B-cell differentiation and evolution of immunity. The concept of the present study is that genes involved in MM pathogenesis, such as immune response genes, can be identified by screening for single-nucleotide polymorphisms (SNPs) involved in the immune response and a subsequent statistical analysis that focusses on the association of SNPs, certain haplotypes or SNP-SNP interactions with MM risk and prognosis. We genotyped 348 Danish patients and 355 controls for 13 SNPs located in the TNFA, IL-4, IL-6, IL-10 and CHI3L1 gene promoters. The occurrence of single polymorphisms, haplotypes and SNP-SNP interactions were statistically analyzed for association with disease risk and outcome following high-dose therapy. Identified genes that carried SNPs or haplotypes that were identified as risk or prognostic factors were studied for expression in normal B-cell subsets and myeloma plasma cells. We observed a significantly reduced risk when harboring the TNFA-238A allele (OR = 0.51 (0.29-0.86)) and interactions between the TNFA-1031T/C * and IL-10 -3575T/A (p = .007) as well as the TNFA-308G/A * and IL-10-1082G/A (p = .008) allels. By statistical approaches, we observed association between prognosis and the TNFA-857CC genotype (HR = 2.80 (1.29-6.10)) and IL-10-1082GG + GA genotypes (HR = 1.93 (1.07-3.49)) and interactions between IL-6-174G/C and IL-10-3575T/A (p = .001) and between TNFA-308G/A and IL-4-1098T/G (p= .005). The 'risk genes' were analyzed for expression in normal B-cell subsets (N = 6) from seven healthy donors and we found TNFA and IL-6 expressed both in naïve and in memory B cells when compared to preBI, II, immature and plasma cells. The 'prognosis genes' CHI3L1, IL-6 and IL-10 were differential expressed in malignant plasma cells when comparing poor and good prognosis groups based on to the TC classification. In summary, these findings suggest that TNFA, IL-4, IL-6, IL-10 and CHI3L1 might be important players in MM pathogenesis during disease initiation and drug resistance in multiple myeloma.
多发性骨髓瘤的起源取决于其在正常B细胞分化及免疫演化过程中与基质细胞的相互作用。本研究的理念是,通过筛选参与免疫反应的单核苷酸多态性(SNP),并随后进行聚焦于SNP、特定单倍型或SNP-SNP相互作用与多发性骨髓瘤风险及预后关联的统计分析,来识别参与多发性骨髓瘤发病机制的基因,如免疫反应基因。我们对348例丹麦患者和355例对照进行了位于TNFA、IL-4、IL-6、IL-10和CHI3L1基因启动子区的13个SNP的基因分型。对单核苷酸多态性、单倍型和SNP-SNP相互作用的发生情况进行了统计分析,以确定其与高剂量治疗后疾病风险及转归的关联。对鉴定出携带被确定为风险或预后因素的SNP或单倍型的基因,研究其在正常B细胞亚群和骨髓瘤浆细胞中的表达。我们观察到,携带TNFA -238A等位基因时风险显著降低(OR = 0.
Zotero 插件