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首页> 外文期刊>Turkish journal of biology >The promising effects of BMP2 transfected mesenchymal stem cells on human osteosarcoma
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The promising effects of BMP2 transfected mesenchymal stem cells on human osteosarcoma

机译:BMP2转染间充质干细胞对人骨瘤的有希望的影响

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Selective targeting of transfected mesenchymal stem cells (MSCs) carrying specific antioncogenes to the tumor was suggested as a treatment option. Bone morphogenetic protein-2 (BMP2) was shown to inhibit the proliferation and aggressiveness of osteosarcoma (OS) cells. Here, we aimed to assess the homing efficiency of intraperitoneally administered hMSCs transfected with BMP2 to the tumoral site and their effects on OS using an orthotopic xenograft murine model. Orthotopic xenograft murine model of OS in sixweek- old female NOD/SCID mice using 143B cells was established. hMSCs transfected with BMP2 (BMP2 + hMSC) were used. In vivo experiments performed on four groups of mice that received no treatment, or intraperitoneally administered BMP2, hMSCs, and BMP2+hMSCs. Histopathological and immunohistochemical studies were used to evaluate the pathological identification and to assess the dimensions and necrotic foci of the tumor, the features of lung metastases, and immunostaining against p27, Ki-67, and caspase-3 antibodies. The osteogenic differentiation markers BMP2, BMP4, COL1A1, OPN, OCN and PF4 evaluated using RT-PCR. The tumor dimensions in the hMSCs group were significantly higher than those of the remaining groups (p 0.01). The number of metastatic foci in the BMP2 + hMSCs group was significantly lower than those of the other groups (p 0.01). The current results showed that the intraperitoneal route could be efficiently used for targeting hMSCs to the tumoral tissues for effective BMP2 delivery. In this study, the effects of BMP2 transfected hMSCs on human OS and metastasis were promising for achieving osteogenic differentiation and reduced metastatic process.
机译:提出了将转染的间充质干细胞(MSCs)携带对肿瘤的转染的间充质干细胞(MSC)作为治疗方案。显示骨形态发生蛋白-2(BMP2)抑制骨肉瘤(OS)细胞的增殖和侵蚀性。在这里,我们旨在评估用原位异种移植小鼠模型对肿瘤部位转染的腹膜内给药的HMSCs的宿舍效率及其对OS的影响。建立了使用143B细胞的六周旧雌性点击/ SCID小鼠OS的原位异种移植鼠模型。使用用BMP2(BMP2 + HMSC)转染的HMSCs。体内实验在4组小鼠中进行,该小鼠没有治疗,或腹膜内给药BMP2,HMSCs和BMP2 + HMSC。组织病理学和免疫组化研究用于评估病理鉴定并评估肿瘤的尺寸和坏死焦点,肺转移的特征,以及针对P27,KI-67和Caspase-3抗体的免疫染色。使用RT-PCR评估的骨质发生分化标记BMP2,BMP4,COL1A1,OPN,OCN和PF4。 HMSC组中的肿瘤尺寸显着高于剩余基团的尺寸(P <0.01)。 BMP2 + HMSCs组中的转移性焦点的数量显着低于其他基团(P <0.01)。目前的结果表明,腹膜内途径可以有效地用于靶向HMSCs以肿瘤组织以有效BMP2递送。在该研究中,BMP2转染的HMSCs对人OS和转移的影响是为了实现骨质发生分化和降低的转移过程。

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