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黏液样脂肪肉瘤细胞系的高通量筛选:生存素对肿瘤生长至关重要。

High-Throughput Screening of Myxoid Liposarcoma Cell Lines: Survivin Is Essential for Tumor Growth.

作者信息

de Graaff Marieke A, Malu Shruti, Guardiola Irma, Kruisselbrink Alwine B, de Jong Yvonne, Corver Willem E, Gelderblom H, Hwu Patrick, Nielsen Torsten O, Lazar Alexander J, Somaiah Neeta, Bovée Judith V M G

机构信息

Department of Pathology, Leiden University Medical Center, Leiden, the Netherlands.

Department of Melanoma Medical Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.

出版信息

Transl Oncol. 2017 Aug;10(4):546-554. doi: 10.1016/j.tranon.2017.05.007. Epub 2017 Jun 24.

Abstract

Myxoid liposarcoma (MLS) is a soft tissue sarcoma characterized by a recurrent t(12;16) translocation. Although tumors are initially radio- and chemosensitive, the management of inoperable or metastatic MLS can be challenging. Therefore, our aim was to identify novel targets for systemic therapy. We performed an in vitro high-throughput drug screen using three MLS cell lines (402091, 1765092, DL-221), which were treated with 273 different drugs at four different concentrations. Cell lines and tissue microarrays were used for validation. As expected, all cell lines revealed a strong growth inhibition to conventional chemotherapeutic agents, such as anthracyclines and taxanes. A good response was observed to compounds interfering with Src and the mTOR pathway, which are known to be affected in these tumors. Moreover, BIRC5 was important for MLS survival because a strong inhibitory effect was seen at low concentration using the survivin inhibitor YM155, and siRNA for BIRC5 decreased cell viability. Immunohistochemistry revealed abundant expression of survivin restricted to the nucleus in all 32 tested primary tumor specimens. Inhibition of survivin in 402-91 and 1765-92 by YM155 increased the percentage S-phase but did not induce apoptosis, which warrants further investigation before application in the treatment of metastatic MLS. Thus, using a 273-compound drug screen, we confirmed previously identified targets (mTOR, Src) in MLS and demonstrate survivin as essential for MLS survival.

摘要

黏液样脂肪肉瘤(MLS)是一种软组织肉瘤,其特征为反复出现的t(12;16)易位。尽管肿瘤最初对放疗和化疗敏感,但不可切除或转移性MLS的治疗可能具有挑战性。因此,我们的目标是确定全身治疗的新靶点。我们使用三种MLS细胞系(402091、1765092和DL-221)进行了体外高通量药物筛选,这些细胞系在四种不同浓度下用273种不同药物进行处理。细胞系和组织微阵列用于验证。正如预期的那样,所有细胞系对传统化疗药物,如蒽环类药物和紫杉烷类药物,均表现出强烈的生长抑制作用。观察到对干扰Src和mTOR通路的化合物有良好反应,已知这些通路在这些肿瘤中受到影响。此外,BIRC5对MLS的存活很重要,因为使用survivin抑制剂YM155在低浓度下可观察到强烈的抑制作用,且针对BIRC5的小干扰RNA降低了细胞活力。免疫组织化学显示,在所有32个测试的原发性肿瘤标本中,survivin仅在细胞核中大量表达。YM155对402-91和1765-92细胞系中survivin的抑制增加了S期百分比,但未诱导凋亡,这在应用于转移性MLS治疗之前值得进一步研究。因此,通过273种化合物的药物筛选,我们在MLS中证实了先前确定的靶点(mTOR、Src),并证明survivin对MLS的存活至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/70f5/5487254/a25c40e38665/gr1.jpg

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