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患者来源的横纹肌肉瘤细胞概括了原发性肿瘤的基因和转录组图谱。

Patient-derived rhabdomyosarcoma cells recapitulate the genetic and transcriptomic landscapes of primary tumors.

作者信息

Hu Yuxiang, He Ziqi, Liu Shuangai, Ying Wenwen, Chen Yifan, Zhao Manli, He Min, Wu Xuan, Tang Yinbing, Gu Weizhong, Ying Meidan, Wang Jinhu, Tao Ting

机构信息

Pediatric Cancer Research Center, National Clinical Research Center for Child Health, Hangzhou 310052, China.

Department of Surgical Oncology, Children's Hospital Zhejiang University School of Medicine, National Clinical Research Center for Child Health, Hangzhou 310052, China.

出版信息

iScience. 2024 Aug 31;27(10):110862. doi: 10.1016/j.isci.2024.110862. eCollection 2024 Oct 18.

Abstract

Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in childhood and adolescence. The availability of appropriate and well-characterized preclinical models for RMS is limited, posing a challenge for investigating the molecular mechanisms and evaluating new targeted compounds in preclinical settings. Here, we collected 51 RMS specimens (referred to as ZJUCH-RMS cohort) and established 9 patient-derived cells (PDCs) and validated the identity of these cells by the expression of RMS-specific markers. Whole-transcriptome analysis identified high-confidence mutations in ZJUCH-RMS cohort including , , , , and . Further studies showed that RMS PDCs retained the genetic alterations and the expression of RMS hallmark and dependency genes in matched primary tumors and acted as valuable tools to assess drug responses and pharmacogenomic interactions. Our study provides unique PDCs that are available for preclinical studies of RMS and further advances the feasibility of RMS PDCs as valuable tools for developing personalized treatments for patients.

摘要

横纹肌肉瘤(RMS)是儿童和青少年中最常见的软组织肉瘤。用于RMS的合适且特征明确的临床前模型有限,这给在临床前环境中研究分子机制和评估新的靶向化合物带来了挑战。在这里,我们收集了51个RMS标本(称为ZJUCH-RMS队列),建立了9个患者来源的细胞(PDC),并通过RMS特异性标志物的表达验证了这些细胞的身份。全转录组分析确定了ZJUCH-RMS队列中的高置信度突变,包括 , , , ,和 。进一步的研究表明,RMS PDC保留了匹配的原发性肿瘤中的基因改变以及RMS标志性和依赖性基因的表达,并作为评估药物反应和药物基因组相互作用的有价值工具。我们的研究提供了可用于RMS临床前研究的独特PDC,并进一步提高了RMS PDC作为为患者开发个性化治疗的有价值工具的可行性。

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