HIRA protects telomeres against R-loop-induced instability in ALT cancer cells.

IF 7.5 1区 生物学 Q1 CELL BIOLOGY
Michelle Lee Lynskey, Emily E Brown, Ragini Bhargava, Anne R Wondisford, Jean-Baptiste Ouriou, Oliver Freund, Ray W Bowman, Baylee A Smith, Santana M Lardo, Sandra Schamus-Hayes, Sarah J Hainer, Roderick J O'Sullivan
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引用次数: 0

Abstract

Inactivating mutations in chromatin modifiers, like the α-thalassemia/mental retardation, X-linked (ATRX)-death domain-associated protein (DAXX) chromatin remodeling/histone H3.3 deposition complex, drive the cancer-specific alternative lengthening of telomeres (ALT) pathway. Prior studies revealed that HIRA, another histone H3.3 chaperone, compensates for ATRX-DAXX loss at telomeres to sustain ALT cancer cell survival. How HIRA rescues telomeres from the consequences of ATRX-DAXX deficiency remains unclear. Here, using an assay for transposase-accessible chromatin using sequencing (ATAC-seq) and cleavage under targets and release using nuclease (CUT&RUN), we establish that HIRA-mediated deposition of new H3.3 maintains telomeric chromatin accessibility to prevent the detrimental accumulation of nucleosome-free single-stranded DNA (ssDNA) in ATRX-DAXX-deficient ALT cells. We show that the HIRA-UBN1/UBN2 complex deposits new H3.3 to prevent TERRA R-loop buildup and transcription-replication conflicts (TRCs) at telomeres. Furthermore, HIRA-mediated H3.3 incorporation into telomeric chromatin links productive ALT to the phosphorylation of serine 31, an H3.3-specific amino acid, by Chk1. Therefore, we identify a critical role for HIRA-mediated H3.3 deposition that ensures the survival of ATRX-DAXX-deficient ALT cancer cells.

在 ALT 癌细胞中,HIRA 保护端粒免受 R 环诱导的不稳定性的影响。
染色质修饰因子的失活突变,如α-地中海贫血/智力低下,X-连锁(ATRX)-死亡结构域相关蛋白(DAXX)染色质重塑/组蛋白H3.3沉积复合物,推动了癌症特异性端粒替代性延长(ALT)途径。先前的研究发现,另一种组蛋白 H3.3 合子 HIRA 可补偿端粒上 ATRX-DAXX 的损失,以维持 ALT 癌细胞的存活。目前还不清楚HIRA是如何从ATRX-DAXX缺失的后果中拯救端粒的。在这里,我们利用测序(ATAC-seq)和靶标裂解及核酸酶释放(CUT&RUN)对转座酶可访问染色质进行检测,确定了由HIRA介导的新H3.3沉积可维持端粒染色质的可访问性,以防止无核苷酸单链DNA(ssDNA)在ATRX-DAXX缺陷的ALT细胞中的有害积累。我们发现,HIRA-UBN1/UBN2复合物会沉积新的H3.3,以防止端粒上TERRA R环的堆积和转录-复制冲突(TRC)。此外,HIRA 介导的 H3.3 并入端粒染色质与 Chk1 对丝氨酸 31(H3.3 的特异性氨基酸)的磷酸化有关。因此,我们确定了 HIRA 介导的 H3.3 沉积在确保 ATRX-DAXX 缺陷 ALT 癌细胞存活方面的关键作用。
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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来源期刊
Cell reports
Cell reports CELL BIOLOGY-
CiteScore
13.80
自引率
1.10%
发文量
1305
审稿时长
77 days
期刊介绍: Cell Reports publishes high-quality research across the life sciences and focuses on new biological insight as its primary criterion for publication. The journal offers three primary article types: Reports, which are shorter single-point articles, research articles, which are longer and provide deeper mechanistic insights, and resources, which highlight significant technical advances or major informational datasets that contribute to biological advances. Reviews covering recent literature in emerging and active fields are also accepted. The Cell Reports Portfolio includes gold open-access journals that cover life, medical, and physical sciences, and its mission is to make cutting-edge research and methodologies available to a wide readership. The journal's professional in-house editors work closely with authors, reviewers, and the scientific advisory board, which consists of current and future leaders in their respective fields. The advisory board guides the scope, content, and quality of the journal, but editorial decisions are independently made by the in-house scientific editors of Cell Reports.
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