Institute of Applied Biosciences, Centre for Research and Technology Hellas, Thessaloniki, Greece.
Department of Immunology, Genetics and Pathology, Science for Life Laboratory, Uppsala University, Uppsala, Sweden.
Int J Cancer. 2019 Jun 1;144(11):2695-2706. doi: 10.1002/ijc.31999. Epub 2019 Jan 15.
Chronic lymphocytic leukemia (CLL) stereotyped subsets #6 and #8 include cases expressing unmutated B cell receptor immunoglobulin (BcR IG) (U-CLL). Subset #6 (IGHV1-69/IGKV3-20) is less aggressive compared to subset #8 (IGHV4-39/IGKV1(D)-39) which has the highest risk for Richter's transformation among all CLL. The underlying reasons for this divergent clinical behavior are not fully elucidated. To gain insight into this issue, here we focused on epigenomic signatures and their links with gene expression, particularly investigating genome-wide DNA methylation profiles in subsets #6 and #8 as well as other U-CLL cases not expressing stereotyped BcR IG. We found that subset #8 showed a distinctive DNA methylation profile compared to all other U-CLL cases, including subset #6. Integrated analysis of DNA methylation and gene expression revealed significant correlation for several genes, particularly highlighting a relevant role for the TP63 gene which was hypomethylated and overexpressed in subset #8. This observation was validated by quantitative PCR, which also revealed TP63 mRNA overexpression in additional nonsubset U-CLL cases. BcR stimulation had distinct effects on p63 protein expression, particularly leading to induction in subset #8, accompanied by increased CLL cell survival. This pro-survival effect was also supported by siRNA-mediated downregulation of p63 expression resulting in increased apoptosis. In conclusion, we report that DNA methylation profiles may vary even among CLL patients with similar somatic hypermutation status, supporting a compartmentalized approach to dissecting CLL biology. Furthermore, we highlight p63 as a novel prosurvival factor in CLL, thus identifying another piece of the complex puzzle of clinical aggressiveness.
慢性淋巴细胞白血病(CLL)的刻板亚型 #6 和 #8 包括表达未突变 B 细胞受体免疫球蛋白(BcR IG)(U-CLL)的病例。与亚型 #8(IGHV4-39/IGKV1(D)-39)相比,亚型 #6(IGHV1-69/IGKV3-20)的侵袭性较低,而亚型 #8 是所有 CLL 中 Richter 转化风险最高的亚型。导致这种不同临床行为的根本原因尚未完全阐明。为了深入了解这一问题,我们在这里专注于表观基因组特征及其与基因表达的联系,特别是研究了亚型 #6 和 #8 以及其他不表达刻板 BcR IG 的 U-CLL 病例的全基因组 DNA 甲基化谱。我们发现,与所有其他 U-CLL 病例(包括亚型 #6)相比,亚型 #8 显示出独特的 DNA 甲基化谱。DNA 甲基化和基因表达的综合分析显示,有几个基因存在显著相关性,特别是强调了 TP63 基因的重要作用,该基因在亚型 #8 中呈低甲基化和过表达。这一观察结果通过定量 PCR 得到了验证,该实验还揭示了额外的非亚型 U-CLL 病例中 TP63 mRNA 的过表达。BcR 刺激对 p63 蛋白表达有明显的影响,特别是在亚型 #8 中诱导表达,同时增加 CLL 细胞的存活。这种促存活作用也得到了 siRNA 介导的 p63 表达下调导致细胞凋亡增加的支持。总之,我们报告说,即使在具有相似体细胞高突变状态的 CLL 患者中,DNA 甲基化谱也可能存在差异,支持对 CLL 生物学进行分区的方法。此外,我们强调 p63 是 CLL 中的一种新的促存活因子,从而确定了临床侵袭性这一复杂难题的另一个组成部分。
