Alternative lengthening of telomere-based immortalization renders H3G34R -mutant diffuse hemispheric glioma hypersensitive to PARP inhibitor combination regimens.

IF 16.4 1区医学 Q1 CLINICAL NEUROLOGY Neuro-oncology Pub Date : 2024-11-18 DOI:10.1093/neuonc/noae228

Anna Laemmerer, Christian Lehmann, Lisa Mayr, Katharina Bruckner, Lisa Gabler, Daniel Senfter, Philipp Meyer, Theresa Balber, Christine Pirker, Carola N Jaunecker, Dominik Kirchhofer, Petra Vician, Michelle Griesser, Sabine Spiegl-Kreinecker, Maria T Schmook, Tatjana Traub-Weidinger, Peter Kuess, Franziska Eckert, Aniello Federico, Sibylle Madlener, Natalia Stepien, Bernhard Robl, Alicia Baumgartner, Johannes A Hainfellner, Karin Dieckmann, Christian Dorfer, Karl Roessler, Nina S Corsini, Klaus Holzmann, Wolfgang M Schmidt, Andreas Peyrl, Amedeo A Azizi, Christine Haberler, Alexander Beck, Stefan M Pfister, Julia Schueler, Daniela Loetsch-Gojo, Jürgen A Knoblich, Walter Berger, Johannes Gojo

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Abstract

Background: Diffuse hemispheric glioma, H3G34R/V-mutant (DHG-H3G34) is characterized by poor prognosis and lack of effective treatment options. DHG-H3G34R further harbor deactivation of Alpha-Thalassemia/Mental Retardation Syndrome X-linked protein (ATRX; DHG-H3G34R_ATRX) suggesting a unique interaction of these two oncogenic alterations. In this study, we dissect their cell biological interplay, investigate the impact on telomere stabilization and, consequently, validate a targeted therapy approach.

Methods: We characterized patient-derived primary pediatric high-grade glioma (pHGG) models for telomere-maintenance mechanisms, DNA damage stress (including protein expression, pH2AX/Rad51 foci, cell-cycle arrest) and their sensitivity towards poly-ADP polymerase inhibitor (PARPi) combinations. Human induced pluripotent stem cells (iPSCs) were used for modelling the disease. The anticancer activity of PARPi combinations in vivo was studied in Chorioallantoic Membrane (CAM) and orthotopic in vivo experiments. Finally, we treated a DHG-H3G34R_ATRX patient with a PARPi combination therapy.

Results: We elaborate that alternative lengthening of telomeres (ALT) is a key characteristic of DHG-H3G34R_ATRX. A dominant cooperative effect between H3G34R and ATRX loss in ALT activation also became apparent in iPSCs, which endogenously exert telomerase activity. In both, patient-derived DHG-H3G34R_ATRX models and H3G34R+/ATRX- iPSCs, the ALT phenotype was associated with increased basal DNA damage stress, mediating synergistic susceptibility towards PARPi (talazoparib, niraparib) combinations with topoisomerase-I inhibitors (topotecan, irinotecan). In a first-of-its-kind case, treatment of a DHG-H3G34R_ATRX patient with the brain-penetrant PARP inhibitor niraparib and topotecan resulted in a significant tumor reduction.

Conclusion: Our preclinical and clinical data strongly support the further development of PARPis together with DNA damage stress-inducing treatment regimens for DHG-H3G34R_ATRX.

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基于端粒永生的替代性延长使H3G34R突变的弥漫性半球胶质瘤对PARP抑制剂联合疗法不敏感。

背景：弥漫性大脑半球胶质瘤、H3G34R/V-突变体（DHG-H3G34）的特点是预后不良和缺乏有效的治疗方案。DHG-H3G34R还携带α-地中海贫血/智力迟钝综合征X连锁蛋白（ATRX；DHG-H3G34R_ATRX）的失活，这表明这两种致癌改变之间存在独特的相互作用。在这项研究中，我们剖析了它们在细胞生物学上的相互作用，研究了它们对端粒稳定的影响，从而验证了一种靶向治疗方法：方法：我们对源自患者的原发性儿科高级别胶质瘤（pHGG）模型的端粒维持机制、DNA损伤应激（包括蛋白质表达、pH2AX/Rad51病灶、细胞周期停滞）及其对多聚ADP聚合酶抑制剂（PARPi）组合的敏感性进行了鉴定。人类诱导多能干细胞（iPSCs）被用于建立疾病模型。在绒毛膜（CAM）和正位体内实验中研究了 PARPi 组合的体内抗癌活性。最后，我们用PARPi联合疗法治疗了一名DHG-H3G34R_ATRX患者：结果：我们阐述了端粒替代性延长（ALT）是DHG-H3G34R_ATRX的一个关键特征。在内源性端粒酶活性的 iPSCs 中，H3G34R 和 ATRX 缺失在 ALT 激活过程中的优势合作效应也很明显。在患者衍生的 DHG-H3G34R_ATRX 模型和 H3G34R+/ATRX- iPSCs 中，ALT 表型与基础 DNA 损伤应激的增加有关，它介导了 PARPi（他拉唑帕利、尼拉帕利）与拓扑异构酶-I 抑制剂（拓扑替康、伊立替康）的协同易感性。在一个首例病例中，DHG-H3G34R_ATRX患者接受脑穿透性PARP抑制剂尼拉帕利和拓博替康治疗后，肿瘤明显缩小：我们的临床前和临床数据有力地支持了针对 DHG-H3G34R_ATRX 的 PARPis 和 DNA 损伤应激诱导治疗方案的进一步发展。

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

Neuro-oncology 医学-临床神经学

CiteScore

27.20

自引率

6.30%

发文量

1434

审稿时长

3-8 weeks

期刊介绍： Neuro-Oncology, the official journal of the Society for Neuro-Oncology, has been published monthly since January 2010. Affiliated with the Japan Society for Neuro-Oncology and the European Association of Neuro-Oncology, it is a global leader in the field. The journal is committed to swiftly disseminating high-quality information across all areas of neuro-oncology. It features peer-reviewed articles, reviews, symposia on various topics, abstracts from annual meetings, and updates from neuro-oncology societies worldwide.