卵巢癌细胞释放的微颗粒进入腹水并促进细胞迁移。

Microparticles from ovarian carcinomas are shed into ascites and promote cell migration.

机构信息

Division of Gynecologic Oncology, Department of Obstetrics and Gynecology, University of Washington School of Medicine, Seattle, WA, USA.

出版信息

Int J Gynecol Cancer. 2012 May;22(4):546-52. doi: 10.1097/IGC.0b013e318241d9b9.

DOI:10.1097/IGC.0b013e318241d9b9

PMID:22315094

Abstract

OBJECTIVE

Microparticles are cellular-derived vesicles (0.5-1.0 μm) composed of cell membrane components, which are actively shed from the surface of various cells, including epithelial cells. We compared microparticles in ascites between women with ovarian carcinoma and women with benign ovarian pathology, and isolated tumor-derived (epithelial cell adhesion molecule [EpCAM]-positive) microparticles for functional analysis and proteomics.

MATERIALS AND METHODS

Cases included 8 patients with benign ovarian neoplasms and 41 with ovarian carcinoma. Ascites from a high-grade stage III serous carcinoma was used for functional and proteomic analysis. Cancer cells were isolated using EpCAM-coated beads, microparticles were isolated by ultracentrifugation/flow cytometry, and sorting was achieved using markers (eg, EpCAM). Binding and migrations assays were performed with 3 ovarian cancer cell lines. Proteomic analysis of EpCAM-positive microparticles and ascites cancer cells was performed by mass spectrometry.

RESULTS

Microparticles in benign pelvic fluid were similar to early and advanced-stage ascites (2.4 vs 2.8 vs 2.0 × 10⁶ microparticles/mL). Advanced stage had a greater proportion of EpCAM-positive microparticles than early or benign disease (13.3% vs 2.5% vs 2.1%; P = 0.001), and serous histology had more than endometrioid (13.2% vs 1.8%; P = 0.01). Microparticles bound to the surface of 3 cultured cell lines, and were internalized into the EpCAM-positive microparticles, resulting in more cell migration than buffer alone or EpCAM-negative microparticles (P = 0.007). A dose-dependent increase was seen with increasing numbers of EpCAM-positive microparticles. Proteomics revealed that most proteins in EPCAM-positive microparticles were shared with cancer cells, and many are associated with cell motility and invasion, such as fibronectin, filamin A, vimentin, myosin-9, and fibrinogen.

CONCLUSIONS

Ascites from advanced-stage and serous ovarian carcinomas contain large numbers of tumor-derived microparticles. In vitro, these microparticles bind to cancer cells and stimulate migration. Tumor-derived microparticles in ascites could mediate the predilection for peritoneal spread in serous ovarian carcinomas.

摘要

目的

微粒体是由细胞膜成分组成的细胞来源的小泡（0.5-1.0μm），从各种细胞表面主动脱落，包括上皮细胞。我们比较了卵巢癌患者和良性卵巢病理患者的腹水之间的微粒体，并分离了肿瘤衍生的（上皮细胞黏附分子[EpCAM]阳性）微粒体进行功能分析和蛋白质组学分析。

材料与方法

病例包括 8 例良性卵巢肿瘤患者和 41 例卵巢癌患者。高级别 III 期浆液性癌腹水用于功能和蛋白质组学分析。使用 EpCAM 包被珠分离癌细胞，超速离心/流式细胞术分离微粒体，并用标志物（如 EpCAM）进行分选。进行了 3 种卵巢癌细胞系的结合和迁移试验。采用质谱法对 EpCAM 阳性微粒体和腹水癌细胞进行蛋白质组学分析。

结果

良性盆腔液中的微粒体与早期和晚期腹水（2.4 对 2.8 对 2.0×10⁶微粒体/mL）相似。晚期比早期或良性疾病有更多的 EpCAM 阳性微粒体（13.3%对 2.5%对 2.1%；P=0.001），浆液性组织学比子宫内膜样组织学有更多（13.2%对 1.8%；P=0.01）。微粒体与 3 种培养的细胞系表面结合，并被内化到 EpCAM 阳性微粒体中，导致细胞迁移比缓冲液单独或 EpCAM 阴性微粒体更多（P=0.007）。随着 EpCAM 阳性微粒体数量的增加，观察到剂量依赖性增加。蛋白质组学显示，EpCAM 阳性微粒体中的大多数蛋白质与癌细胞共享，许多与细胞运动和侵袭有关，如纤维连接蛋白、纤维蛋白原、肌球蛋白-9 和纤连蛋白。