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唑来膦酸和抗骨唾液蛋白II抗体对MDA-MB-231(绿色荧光蛋白)乳腺癌细胞的体外作用以及对该细胞系在裸鼠体内诱导产生的溶骨性病变的作用。

Effect of zoledronic acid and an antibody against bone sialoprotein II on MDA-MB-231(GFP) breast cancer cells in vitro and on osteolytic lesions induced in vivo by this cell line in nude rats.

作者信息

Peterschmitt Jenny, Bäuerle Tobias, Berger Martin R

机构信息

Toxicology and Chemotherapy Unit, Deutsches Krebsforschungszentrum Heidelberg, Im Neuenheimer Feld 280, 69120 Heidelberg, Germany.

出版信息

Clin Exp Metastasis. 2007;24(6):449-59. doi: 10.1007/s10585-007-9082-x. Epub 2007 Jul 18.

Abstract

The aim of this study was to investigate the combined effect of zoledronic acid and an antibody against bone sialoprotein II (BSPII) on proliferation and osteolytic activity of MDA-MB-231(GFP) breast cancer cells. For this purpose, the cells were exposed to zoledronic acid (10-20 microg/ml [25-50 microgM]) and an anti-BSPII IgY (10-100 microg/ml) for up to 5 days alone or in combination. The combined treatment showed synergistic antiproliferative effects at the higher dose of zoledronic acid. Following inoculation of 1 x 10(5) MDA-MB-231 (GFP) breast cancer cells into a branch of the femoral artery of nude rats, lytic lesions developed in the tibia, femur or fibula of the injected hind leg after approximately 30 days. The appearance and development of these lesions were monitored radiographically. Rats with lytic lesions were treated with zoledronic acid (60 microg/kg/week sc x 8; n = 10), zoledronic acid and an anti-BSPII IgY antibody (60 microg/kg/week sc x 8 + 10 mg/kg/week sc x 8; n = 10), or left untreated (n = 20). In addition, rats were treated for 4 weeks (n = 10) with both regimens starting right after tumor cell inoculation. Finally, ten rats were treated with zoledronic acid for 2 weeks before tumor cell inoculation (60 microg/kg/week sc x 2). The antiosteolytic effect of zoledronic acid was high as shown by inhibition of osteolytic growth. Addition of the anti-BSPII IgY further decreased the incidence of femoral osteolytic lesions (40% reduction), indicating remineralization, and reduced periosteal defects of cortical bone (20% reduction). These observations favor using the IgY-antibody in addition to zoledronic acid in order to stimulate osteoblast-induced remineralization.

摘要

本研究的目的是调查唑来膦酸和抗骨唾液蛋白II(BSPII)抗体对MDA-MB-231(绿色荧光蛋白)乳腺癌细胞增殖和溶骨活性的联合作用。为此,将细胞单独或联合暴露于唑来膦酸(10 - 20微克/毫升[25 - 50微摩尔])和抗BSPII IgY(10 - 100微克/毫升)中长达5天。联合治疗在较高剂量的唑来膦酸时显示出协同抗增殖作用。将1×10⁵个MDA-MB-231(绿色荧光蛋白)乳腺癌细胞接种到裸鼠股动脉分支后,大约30天后在注射后腿的胫骨、股骨或腓骨中出现溶骨性病变。通过放射学监测这些病变的出现和发展。对有溶骨性病变的大鼠用唑来膦酸(60微克/千克/周皮下注射×8;n = 10)、唑来膦酸和抗BSPII IgY抗体(60微克/千克/周皮下注射×8 + 10毫克/千克/周皮下注射×8;n = 10)治疗,或不治疗(n = 20)。此外,在肿瘤细胞接种后立即开始用两种方案对大鼠进行4周治疗(n = 10)。最后,10只大鼠在肿瘤细胞接种前用唑来膦酸治疗2周(60微克/千克/周皮下注射×2)。唑来膦酸的抗溶骨作用显著,表现为抑制溶骨生长。添加抗BSPII IgY进一步降低了股骨溶骨性病变的发生率(降低40%),表明有再矿化作用,并减少了皮质骨的骨膜缺损(降低20%)。这些观察结果支持除唑来膦酸外还使用IgY抗体以刺激成骨细胞诱导的再矿化。

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