We established patient‑like models of lung cancer metastasis by orthotopically implanting human non‑small cell lung cancer cell lines into SCID mice. We evaluated the utilities of small‑animal computed tomography (CT) and positron‑emission tomography‑computed tomography (PET/CT) in these models to non‑invasively and repeatedly monitor the anticancer effects of cisplatin and erlotinib. We orthotopically implanted three non‑small cell lung cancer cell lines, A549, FT821 and PC‑9, into SCID mice. These mice were then divided into three groups: Control, cis‑diamminedichloroplatinum (II) (CDDP) (7‑mg/kg CDDP, single administration intraperitoneally), and erlotinib (25 mg/kg erlotinib/day, oral administration 5 days/week). After treatment initiation, we repeatedly performed PET/CT and CT measurements and assessed anticancer effects based on tumor volumes and FDG uptake. A549 tumors were not affected by CDDP or erlotinib. FT821 tumors were highly responsive to CDDP. PC‑9 tumors, which have an epidermal growth factor receptor mutation, were highly responsive to erlotinib. Histological results and metastatic rates correlated with the anticancer effects shown by CT. In our orthotopic SCID mouse lung cancer models, 18FDG‑PET/CT and CT imaging non‑invasively and repeatedly monitored the efficacies of cisplatin and erlotinib against not only implanted tumors, but also mediastinal lymph node metastases.

译文

:我们通过将人非小细胞肺癌细胞系原位移植到SCID小鼠中,建立了类似于肺癌的患者转移模型。我们在这些模型中评估了小动物计算机断层扫描(CT)和正电子发射断层扫描计算机断层扫描(PET / CT)的实用性,以无创且反复监测顺铂和厄洛替尼的抗癌作用。我们将三种非小细胞肺癌细胞系A549,FT821和PC‑9原位移植到SCID小鼠中。然后将这些小鼠分为三组:对照组,顺二氨二氯铂(II)(CDDP)(7‑mg / kg CDDP,腹膜内单次给药)和厄洛替尼(25 mg / kg厄洛替尼/天,口服5天/周)。治疗开始后,我们反复进行PET / CT和CT测量,并根据肿瘤体积和FDG摄取评估抗癌作用。 A549肿瘤不受CDDP或厄洛替尼的影响。 FT821肿瘤对CDDP高度敏感。具有表皮生长因子受体突变的PC‑9肿瘤对厄洛替尼具有高响应性。组织学结果和转移率与CT显示的抗癌作用相关。在我们的原位SCID小鼠肺癌模型中,18FDG‑PET / CT和CT成像无创且反复监测了顺铂和厄洛替尼不仅对植入的肿瘤,而且对纵隔淋巴结转移的疗效。

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