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建立并鉴定了两种新型的患者来源的黏液样脂肪肉瘤细胞系。

Establishment and characterization of two novel patient-derived myxoid liposarcoma cell lines.

机构信息

Division of Rare Cancer Research, National Cancer Center Research Institute, 5-1-1 Tsukiji, Chuo-ku, Tokyo, 104-0045, Japan.

Division of Diagnostic Pathology, Tochigi Cancer Center, 4-9-13 Yohnan, Utsunomiya, Tochigi, 320-0834, Japan.

出版信息

Hum Cell. 2022 Jul;35(4):1279-1289. doi: 10.1007/s13577-022-00717-1. Epub 2022 May 30.

Abstract

Myxoid liposarcoma (MLPS) is a lipogenic sarcoma, characterized by myxoid appearance histology and the presence of the FUS-DDIT3 fusion gene. MLPS shows frequent recurrence and poor prognosis after standard treatments, such as surgery. Therefore, novel therapeutic approaches for MLPS are needed. Development of novel treatments requires patient-derived cell lines to study the drug responses and their molecular backgrounds. Presently, only three cell lines of MLPS have been reported, and no line is available from public cell banks. Thus, this study aimed to establish and characterize novel MLPS cell lines. Using surgically resected tumor tissue from two patients with MLPS, two novel lines NCC-MLPS2-C1 and NCC-MLPS3-C1 were established. The presence of FUS-DDIT3 fusion, slow growth, spheroid formation, and invasive capability in these cell lines was confirmed. Growth retardation was monitored for 213 anti-cancer agents using NCC-MLPS2-C1 and NCC-MLPS3-C1 cells, and the results were integrated with the response to treatments in an MLPS cell line, NCC-MLPS1-C1, which was previously established in our laboratory. We found that romidepsin suppressed cell proliferation at considerably low concentrations in all three examined cell lines. NCC-MLPS2-C1 and NCC-MLPS3-C1 cell lines developed here represent a useful tool for basic and preclinical studies of MLPS.

摘要

黏液样脂肪肉瘤(MLPS)是一种脂肪源性肉瘤,其特征是组织学上呈黏液样外观,并存在 FUS-DDIT3 融合基因。MLPS 在接受标准治疗(如手术)后常复发且预后不良。因此,需要为 MLPS 寻找新的治疗方法。开发新的治疗方法需要使用患者来源的细胞系来研究药物反应及其分子背景。目前,仅报道了三种 MLPS 细胞系,且没有可从公共细胞库获得的细胞系。因此,本研究旨在建立和鉴定新型 MLPS 细胞系。本研究使用两名 MLPS 患者手术切除的肿瘤组织,建立了两个新型细胞系 NCC-MLPS2-C1 和 NCC-MLPS3-C1。证实了这些细胞系中存在 FUS-DDIT3 融合、生长缓慢、球体形成和侵袭能力。使用 NCC-MLPS2-C1 和 NCC-MLPS3-C1 细胞监测了 213 种抗癌药物的生长抑制情况,并将结果与我们实验室之前建立的 MLPS 细胞系 NCC-MLPS1-C1 的治疗反应进行了整合。我们发现罗米地辛在所有三种检测的细胞系中以相当低的浓度抑制细胞增殖。本研究中建立的 NCC-MLPS2-C1 和 NCC-MLPS3-C1 细胞系为 MLPS 的基础和临床前研究提供了有用的工具。

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