Clinical Response to Azacitidine in Myelodysplastic Neoplasms is Associated with Distinct DNA Methylation Changes in Haematopoietic Stem and Progenitor cells in vivo

Julie A.I. Thoms, Feng Yan, Henry R. Hampton, Sarah Davidson, Swapna Joshi, Jesslyn Saw, Chowdhury H. Sarowar, Xin Ying Lim, Andrea C. Nunez, Purvi M. Kakadia, Golam Sarower Bhuyan, Xiaoheng Zou, Mary Nguyen, Elaheh S. Ghodousi, Forrest C. Koch, Fatemeh Vafaee, Russell Pickford, Mark J. Raftery, Sally Hough, Griselda Buckland, Michelle Bailey, Yuvaraj Ghodke, Noorul Absar, Lachlin Vaughan, Leonardo Pasalic, Chun Y. Fong, Melita Kenealy, Devendra K. Hiwase, Rohanna I. Stoddart, Soma Mohammed, Linda Lee, Freda H. Passam, Stephen R. Larsen, Kevin J. Spring, Kristen K. Skarratt, Patricia Rebeiro, Peter Presgrave, William S. Stevenson, Silvia Ling, Campbell Tiley, Stephen J. Fuller, Fernando Roncolato, Anoop K. Enjeti, Dirk Hoenemann, Charlotte Lemech, Christopher J. Jolly, Stefan K. Bohlander, David J. Curtis, Jason W.H. Wong, Ashwin Unnikrishnan, Mark Hertzberg, Jake Olivier, Mark N. Polizzotto, John E. Pimanda
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Abstract

Hypomethylating agents are used as frontline therapy for myelodysplastic neoplasms (MDS), but clinical response is unpredictable. To determine whether response was associated with in vivo dynamics of DNA hypomethylation, we conducted a phase 2 trial for MDS using both injection and oral azacitidine (AZA). We established that global DNA methylation levels in peripheral blood and bone marrow mononuclear cells were comparable in AZA responders and non-responders during their course of treatment. However, there were distinct baseline and early drug induced differences in CpG methylation in haematopoietic stem and progenitor cells (HSPCs) in responders compared to non-responders that overlapped with regulatory regions of genes associated with tissue patterning, cell migration and myeloid differentiation. Following six cycles of therapy when clinical response typically manifests, differential hypomethylation in responder HSPCs pointed to marrow adaptation as a driver of enhanced haematopoiesis. Taken together, CpG methylation differences in HSPCs may explain variable response to AZA.
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骨髓增生异常肿瘤患者对阿扎胞苷的临床反应与体内造血干细胞和祖细胞不同的 DNA 甲基化变化有关
低甲基化药物被用作骨髓增生异常肿瘤(MDS)的一线疗法,但临床反应难以预测。为了确定反应是否与体内 DNA 低甲基化的动态有关,我们进行了一项治疗 MDS 的 2 期试验,同时使用注射和口服阿扎胞苷(AZA)。我们发现,在治疗过程中,AZA应答者和非应答者外周血和骨髓单核细胞中的DNA甲基化水平相当。然而,与非应答者相比,应答者造血干细胞和祖细胞(HSPCs)中的 CpG 甲基化存在明显的基线和早期药物诱导差异,这些差异与组织形态、细胞迁移和骨髓分化相关基因的调控区域重叠。在临床反应通常表现为六个周期的治疗后,反应者 HSPCs 中不同的低甲基化现象表明,骨髓适应是造血功能增强的驱动因素。综上所述,HSPCs 中的 CpG 甲基化差异可以解释对 AZA 的不同反应。
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