Recurrent spontaneous miscarriages from sperm after ABVD chemotherapy in a patient with Hodgkin's lymphoma: sperm DNA and methylation profiling.

Gwendoline Lecuyer, Antoine D Rolland, Anne-Sophie Neyroud, Bertrand Evrard, Nathan Alary, Clemence Genthon, Nathalie Dejucq-Rainsford, Célia Ravel, Jessika Moreau, Nathalie Moinard, Mohamed Hadi Mohamed Abdelhamid, Christophe Klopp, Louis Bujan, Frédéric Chalmel
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Abstract

Abstract: Lymphomas represent one of the most common malignant diseases in young men and an important issue is how treatments will affect their reproductive health. It has been hypothesized that chemotherapies, similarly to environmental chemicals, may alter the spermatogenic epigenome. Here, we report the genomic and epigenomic profiling of the sperm DNA from a 31-year-old Hodgkin lymphoma patient who faced recurrent spontaneous miscarriages in his couple 11-26 months after receiving chemotherapy with adriamycin, bleomycin, vinblastine, and dacarbazine (ABVD). In order to capture the potential deleterious impact of the ABVD treatment on mutational and methylation changes, we compared sperm DNA before and 26 months after chemotherapy with whole-genome sequencing (WGS) and reduced representation bisulfite sequencing (RRBS). The WGS analysis identified 403 variants following ABVD treatment, including 28 linked to genes crucial for embryogenesis. However, none were found in coding regions, indicating no impact of chemotherapy on protein function. The RRBS analysis identified 99 high-quality differentially methylated regions (hqDMRs) for which methylation status changed upon chemotherapy. Those hqDRMs were associated with 87 differentially methylated genes, among which 14 are known to be important or expressed during embryo development. While no variants were detected in coding regions, promoter regions of several genes potentially important for embryo development contained variants or displayed an altered methylated status. These might in turn modify the corresponding gene expression and thus affect their function during key stages of embryogenesis, leading to potential developmental disorders or miscarriages.

霍奇金淋巴瘤患者ABVD化疗后精子复发性自发流产:精子DNA和甲基化分析
摘要:淋巴瘤是年轻男性最常见的恶性疾病之一,其治疗如何影响其生殖健康是一个重要问题。据推测,化疗与环境化学物质类似,可能改变生精表观基因组。在这里,我们报告了一名31岁霍奇金淋巴瘤患者的精子DNA的基因组和表观基因组分析,该患者在接受阿霉素、博来霉素、长春花碱和达卡巴嗪(ABVD)化疗后11-26个月出现了复发性自然流产。为了了解ABVD治疗对突变和甲基化变化的潜在有害影响,我们将化疗前和化疗后26个月的精子DNA与全基因组测序(WGS)和亚硫酸盐还原测序(RRBS)进行了比较。WGS分析确定了ABVD治疗后的403个变异,其中28个与胚胎发生至关重要的基因相关。然而,在编码区没有发现,表明化疗对蛋白质功能没有影响。RRBS分析确定了99个高质量的差异甲基化区域(hqDMRs),其甲基化状态在化疗后发生了变化。这些hqDRMs与87个差异甲基化基因相关,其中14个已知在胚胎发育过程中是重要的或表达的。虽然在编码区没有检测到变异,但对胚胎发育可能重要的几个基因的启动子区域包含变异或显示甲基化状态的改变。这些可能反过来改变相应的基因表达,从而影响其在胚胎发生的关键阶段的功能,导致潜在的发育障碍或流产。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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