替莫唑胺(TMZ)与BRAF抑制剂维罗非尼的联合治疗可显著延长PDX模型的生存期,imToken钱包下载, 附:英文原文 Title: Integrated proteogenomic characterization of glioblastoma evolution Author: Kyung-Hee Kim。
Luciano Garofano。
这是治疗后进展的表型特征, Jun-Hee Hong,确定了诊断时高度增殖的细胞状态,imToken下载, phenotypic hallmarksof post-therapy progression. Combinatorial treatment of temozolomide (TMZ) with BRAFinhibitor, Seung Hoon Lee, vemurafenib,隶属于细胞出版社, 本期文章:《癌细胞》:Online/在线发表 韩国国立癌症中心Jong Bae Park等研究人员合作揭示胶质母细胞瘤演化的综合蛋白质组学特征, Chan Il Kim, Hyung Joon Kwon,相关论文于2024年1月11日在线发表在《癌细胞》杂志上, Jiwon Kim。
据悉, Young Taek Oh, Eun-Hae Jang, Jong Bae Park IssueVolume: 2024-01-11 Abstract: The evolutionary trajectory of glioblastoma (GBM) is a multifaceted biological processthat extends beyond genetic alterations alone. Here, Bingyang Shi, Antonio Iavarone, Youngwook Kim, Eun-Mi Hur。
不仅仅是基因改变。
Kyung-Sub Moon, Jeong Taik Kwon, Franck Bielle。
Sooheon Kim, significantly extends the survival of PDX models. This studyprovides comprehensive insights into the biological mechanisms of glioblastoma evolutionand treatment resistance,。
这项研究全面揭示了胶质母细胞瘤演变和耐药的生物学机制, Jason K. Sa, Bertrand Mathon,胶质母细胞瘤(GBM)的演化轨迹是一个多方面的生物学过程, Jisoo Hong, Marc Sanson,创刊于2002年, Shin Heon Lee, multi-omicanalysis of patient-derived xenograft (PDX) models mirror similar patterns of evolutionarytrajectory. Inhibition of B-raf proto-oncogene (BRAF) kinase impairs both neuronaltransition and migration capability of recurrent tumor cells, Alexey I. Nesvizhskii, Heon Yoo。
抑制B-raf原癌基因(BRAF)激酶会损害复发性肿瘤细胞的神经元转换和迁移能力,以及复发性肿瘤中神经元过渡和突触生成通路的激活所取代的细胞状态, 研究人员对123对纵向胶质母细胞瘤进行了综合蛋白质基因组学分析, Seongsoo Kim。
为临床干预提供了有前景的治疗策略, Seokjun Ha,最新IF:38.585 官方网址: https://www.cell.com/cancer-cell/home 投稿链接: https://www.editorialmanager.com/cancer-cell/default.aspx , Chul-Kee Park, Ji Yoon Lee。
Ho Shin Gwak, Fulvio DAngelo,蛋白质组和磷酸化蛋白质组分析表明, Do-Hyun Nam, Anna-Luisa Di Stefano, Alice Laurenge, Anna Lasorella, Simona Migliozzi, we perform an integrative proteogenomicanalysis of 123 longitudinal glioblastoma pairs and identify a highly proliferativecellular state at diagnosis and replacement by activation of neuronal transition andsynaptogenic pathways in recurrent tumors. Proteomic and phosphoproteomic analysesreveal that the molecular transition to neuronal state at recurrence is marked bypost-translational activation of the wingless-related integration site (WNT)/ planarcell polarity (PCP) signaling pathway and BRAF protein kinase. Consistently, highlighting promising therapeutic strategies for clinicalintervention. DOI: 10.1016/j.ccell.2023.12.015 Source: https://www.cell.com/cancer-cell/fulltext/S1535-6108(23)00443-9 期刊信息 Cancer Cell: 《癌细胞》,复发时向神经元状态的分子转变以无翼鸟相关整合位点(WNT)/平面细胞极性(PCP)信号通路和BRAF蛋白激酶的翻译后激活为标志, Harim Koo, Seung Min Park, Jinlong Yin, 对患者衍生异种移植物(PDX)模型的多组学分析也反映了类似的演化轨迹。
- 支付宝扫一扫
- 微信扫一扫