在预先照射的小鼠模型中,氯喹可阻止三阴性乳腺癌细胞迁移和转移灶形成。
Stimulation of triple negative breast cancer cell migration and metastases formation is prevented by chloroquine in a pre-irradiated mouse model.
作者信息
Bouchard Gina, Therriault Hélène, Geha Sameh, Bérubé-Lauzière Yves, Bujold Rachel, Saucier Caroline, Paquette Benoit
机构信息
Centre for Research in Radiotherapy, Department of Nuclear Medicine and Radiobiology, Université de Sherbrooke, 3001, 12e Avenue Nord, Sherbrooke, Québec, J1H 5 N4, Canada.
Department of Pathology, Centre Hospitalier Universitaire de Sherbrooke, Sherbrooke, Canada.
出版信息
BMC Cancer. 2016 Jun 10;16:361. doi: 10.1186/s12885-016-2393-z.
BACKGROUND
Some triple negative breast cancer (TNBC) patients are at higher risk of recurrence in the first three years after treatment. This rapid relapse has been suggested to be associated with inflammatory mediators induced by radiation in healthy tissues that stimulate cancer cell migration and metastasis formation. In this study, the ability of chloroquine (CQ) to inhibit radiation-stimulated development of metastasis was assessed.
METHODS
The capacity of CQ to prevent radiation-enhancement of cancer cell invasion was assessed in vitro with the TNBC cell lines D2A1, 4T1 and MDA-MB-231 and the non-TNBC cell lines MC7-L1, and MCF-7. In Balb/c mice, a single mammary gland was irradiated with four daily doses of 6 Gy. After the last irradiation, irradiated and control mammary glands were implanted with D2A1 cells. Mice were treated with CQ (vehicle, 40 or 60 mg/kg) 3 h before each irradiation and then every 72 h for 3 weeks. Migration of D2A1 cells in the mammary gland, the number of circulating tumor cells and lung metastasis were quantified, and also the expression of some inflammatory mediators.
RESULTS
Irradiated fibroblasts have increased the invasiveness of the TNBC cell lines only, a stimulation that was prevented by CQ. On the other hand, invasiveness of the non-TNBC cell lines, which was not enhanced by irradiated fibroblasts, was also not significantly modified by CQ. In Balb/c mice, treatment with CQ prevented the stimulation of D2A1 TNBC cell migration in the pre-irradiated mammary gland, and reduced the number of circulating tumor cells and lung metastases. This protective effect of CQ was associated with a reduced expression of the inflammatory mediators interleukin-1β, interleukin-6, and cyclooxygenase-2, while the levels of matrix metalloproteinases-2 and -9 were not modified. CQ also promoted a blocking of autophagy.
CONCLUSION
CQ prevented radiation-enhancement of TNBC cell invasion and reduced the number of lung metastases in a mouse model.
背景
一些三阴性乳腺癌(TNBC)患者在治疗后的头三年复发风险较高。这种快速复发被认为与健康组织中辐射诱导的炎症介质有关,这些炎症介质会刺激癌细胞迁移和转移形成。在本研究中,评估了氯喹(CQ)抑制辐射刺激的转移发展的能力。
方法
用TNBC细胞系D2A1、4T1和MDA-MB-231以及非TNBC细胞系MC7-L1和MCF-7在体外评估CQ预防辐射增强癌细胞侵袭的能力。在Balb/c小鼠中,对单个乳腺每天照射4次,每次6 Gy。最后一次照射后,将D2A1细胞植入照射过的乳腺和对照乳腺。在每次照射前3小时用CQ(载体、40或60 mg/kg)处理小鼠,然后每72小时处理一次,持续3周。对乳腺中D2A1细胞的迁移、循环肿瘤细胞数量和肺转移进行定量,同时检测一些炎症介质的表达。
结果
照射后的成纤维细胞仅增加了TNBC细胞系的侵袭性,而CQ可阻止这种刺激。另一方面,非TNBC细胞系的侵袭性不受照射后成纤维细胞的增强作用影响,CQ对其也无明显改变。在Balb/c小鼠中,CQ治疗可防止照射前乳腺中D2A1 TNBC细胞迁移的刺激,并减少循环肿瘤细胞数量和肺转移。CQ的这种保护作用与炎症介质白细胞介素-1β、白细胞介素-6和环氧化酶-2的表达降低有关,而基质金属蛋白酶-2和-9的水平未改变。CQ还促进了自噬的阻断。
结论
在小鼠模型中,CQ可预防辐射增强的TNBC细胞侵袭并减少肺转移数量。
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