首页> 外文期刊>In Vitro Cellular and Developmental Biology. Animal: Journal of the Tissues Culture Association >Establishment of novel patient-derived models of dermatofibrosarcoma protuberans: two cell lines, NCC-DFSP1-C1 and NCC-DFSP2-C1
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Establishment of novel patient-derived models of dermatofibrosarcoma protuberans: two cell lines, NCC-DFSP1-C1 and NCC-DFSP2-C1

机译:建立Dermatofibrosarcoma蛋白酶的新型患者衍生模型:两种细胞系,NCC-DFSP1-C1和NCC-DFSP2-C1

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摘要

Dermatofibrosarcoma protuberans (DFSP) is a common type of dermal sarcoma, characterized by the presence of the unique collagen type I alpha 1 chain (COL1A1)-PDGFB translocation, which causes constitutive activation of the platelet-derived growth factor (PDGFB) signaling pathway. Patients with DFSP exhibit frequent local recurrence, and novel therapeutic approaches are required to achieve better clinical outcomes. Patient-derived cancer cell lines are essential in the preclinical research. Here, we established novel patient-derived DFSP cell lines from two patients with DFSP and designated these cell lines NCC-DFSP1-C1 and NCC-DFSP2-C1. Tumors of the two patients with DFSP had COL1A1-PDGFB translocations with distinct COL1A1 breakpoints, e.g., in exons 33 and 15, and the translocations were preserved in the established cell lines. NCC-DFSP1-C1 and NCC-DFSP2-C1 cells exhibited similar morphology and limited capability of proliferation in vitro, forming spheroids when seeded on low-attachment tissue culture plates. In contrast, NCC-DFSP1-C1 cells had considerably higher invasive capability than NCC-DFSP2-C1 cells. Overall proteome contents were similar between NCC-DFSP1-C1 and NCC-DFSP2-C1 cells. Notably, in vitro screening studies identified anticancer drugs that showed antiproliferative effects at considerably low concentrations in the DFSP cell lines. Bortezomib, mitoxantrone, ponatinib, and romidepsin were more cytotoxic to NCC-DFSP1-C1 cells than to NCC-DFSP2-C1 cells. These cell lines will be useful tools for developing novel therapeutic strategies to treat DFSP.
机译:Dermatofibrosarcoma protuberans(DFSP)是一种常见的皮肤肉瘤,其特征在于,其特征在于独特的胶原型Iα1链(COL1A1)-PDGFB易位,这导致血小板衍生的生长因子(PDGFB)信号通路的组成型激活。 DFSP患者表现出频繁的局部复发,并且需要新的治疗方法来实现更好的临床结果。患者衍生的癌细胞系在临床前研究中是必不可少的。在这里,我们从两种DFSP患者建立了新的患者衍生的DFSP细胞系,并指定了这些细胞系NCC-DFSP1-C1和NCC-DFSP2-C1。两种DFSP患者的肿瘤具有COL1A1-PDGFB易位,具有不同的COL1A1断点,例如在外显子33和15中,并在已建立的细胞系中保存易位。 NCC-DFSP1-C1和NCC-DFSP2-C1细胞在体外表现出类似的体态和有限的增殖能力,在低附着组织培养板上播种时形成球状体。相反,NCC-DFSP1-C1细胞具有比NCC-DFSP2-C1细胞更高的侵入性能力。 NCC-DFSP1-C1和NCC-DFSP2-C1细胞之间的总体蛋白质组含量相似。值得注意的是,体外筛选研究确定了DFSP细胞系中以相当低浓度的抗增殖作用显示出抗增殖药物。 Bortezomib,Mitoxantrone,Ponatinib和Romidepsin对NCC-DFSP1-C1细胞的细胞毒性比对于NCC-DFSP2-C1细胞更多。这些细胞系将是制定新的治疗DFSP的新疗效策略的有用工具。

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