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首页> 外文期刊>Journal of Neurosurgery. Spine. >Delayed onset of paralysis and slowed tumor growth following in situ placement of recombinant human bone morphogenetic protein 2 within spine tumors in a rat model of metastatic breast cancer: Presented at the 2011 Spine Section Meeting - Laboratory investigation
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Delayed onset of paralysis and slowed tumor growth following in situ placement of recombinant human bone morphogenetic protein 2 within spine tumors in a rat model of metastatic breast cancer: Presented at the 2011 Spine Section Meeting - Laboratory investigation

机译:在转移性乳腺癌大鼠模型中将重组人骨形态发生蛋白2原位放置在脊柱肿瘤中后,麻痹的延迟发作和肿瘤生长减慢:在2011脊柱会议上进行-实验室研究

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Object. Recombinant human bone morphogenetic proteins (rhBMPs) are FDA-approved for specific spinal fusion procedures, but their use is contraindicated in spine tumor resection beds because of an unclear interaction between tumor tissue and such growth factors. Interestingly, a number of studies have suggested that BMPs may slow the growth of adenocarcinomas in vitro, and these lesions represent the majority of bony spine tumors. In this study, the authors hypothesized that rhBMP-2 placed in an intraosseous spine tumor in the rat could suppress tumor and delay the onset of paresis in such animals. Methods. Twenty-six female nude athymic rats were randomized into an experimental group (Group 1) or a positive control group (Group 2). Group 1 (tumor + 15 μg rhBMP-2 sponge, 13 rats) underwent transperitoneal exposure and implantation of breast adenocarcinoma (CRL-1666) into the L-6 spine segment, followed by the implantation of a bovine collagen sponge impregnated with 15 μg of rhBMP-2. Group 2 (tumor + 0.9% NaCl sponge, 13 rats) underwent transperitoneal exposure and tumor implantation in the lumbar spine but no local treatment with rhBMP-2. An additional 8 animals were randomized into 2 negative control groups (Groups 3 and 4). Group 3 (15 μg rhBMP-2 sponge, 4 rats) and Group 4 (0.9% NaCl sponge, 4 rats) underwent transperitoneal exposure of the lumbar spine along with the implantation of rhBMP-2- and saline-impregnated bovine collagen sponges, respectively. Neither of the negative control groups was implanted with tumor. The Basso-Beattie-Bresnahan (BBB) scale was used to monitor daily motor function regression and the time to paresis (BBB score ≤ 7). Results. In comparison with the positive control animals (Group 2), the experimental animals (Group 1) had statistically significant longer mean (25.8 ± 12.2 vs 13 ± 1.4 days, p d 0.001) and median (20 vs 13 days) times to paresis. In addition, the median survival time was significantly longer in the experimental animals (20 vs 13.5 days, p ≤ 0.0001). Histopathological analysis demonstrated bone growth and tumor inhibition in the experimental animals, whereas bone destruction and cord compression were observed in the positive control animals. Neither of the negative control groups (Groups 3 and 4) demonstrated any evidence of neurological deterioration, morbidity, or cord compromise on either gross or histological analysis. Conclusions. This study shows that the local administration of rhBMP-2 (15 μg, 10 μl of 1.5-mg/ml solution) in a rat spine tumor model of breast cancer not only fails to stimulate local tumor growth, but also decreases local tumor growth and delays the onset of paresis in rats. This preclinical experiment is the first to show that the local placement of rhBMP-2 in a spine tumor bed may slow tumor progression and delay associated neurological decline.
机译:目的。重组人骨形态发生蛋白(rhBMP)已获得FDA批准用于特定的脊柱融合手术,但由于肿瘤组织与此类生长因子之间的相互作用尚不清楚,因此禁止在脊柱肿瘤切除床上使用它们。有趣的是,许多研究表明BMPs可能会减慢体外腺癌的生长,这些病变代表了大多数骨脊柱肿瘤。在这项研究中,作者假设将rhBMP-2置于大鼠骨内脊柱肿瘤中可以抑制肿瘤并延缓此类动物的轻瘫发作。方法。将26只雌性裸性无胸腺大鼠随机分为实验组(第1组)或阳性对照组(第2组)。第一组(肿瘤+ 15μgrhBMP-2海绵,13只大鼠)经腹膜暴露,并将乳腺癌(CRL-1666)植入L-6脊柱节段,然后植入浸有15μg牛海绵的牛胶原海绵rhBMP-2。第2组(肿瘤+ 0.9%NaCl海绵,13只大鼠)经腹膜暴露并在腰椎植入肿瘤,但未使用rhBMP-2进行局部治疗。将另外8只动物随机分为2个阴性对照组(第3和第4组)。第3组(15μgrhBMP-2海绵,4只大鼠)和第4组(0.9%NaCl海绵,4只大鼠)分别经腰椎腹膜暴露于腰椎,并分别植入了rhBMP-2和盐水浸渍的牛胶原蛋白海绵。 。阴性对照组均未植入肿瘤。 Basso-Beattie-Bresnahan(BBB)量表用于监测每日运动功能的衰退和麻痹的时间(BBB评分≤7)。结果。与阳性对照动物(第2组)相比,实验动物(第1组)的平均麻痹时间(25.8±12.2 vs 13±1.4天,p d 0.001)和中位数(20 vs 13天)有统计学意义。此外,实验动物的中位生存时间明显更长(20天对13.5天,p≤0.0001)。组织病理学分析表明在实验动物中骨生长和肿瘤抑制,而在阳性对照动物中观察到骨破坏和脐带受压。阴性对照组(第3组和第4组)均未在肉眼或组织学分析中显示出任何神经系统恶化,发病率或脊髓损伤的证据。结论。这项研究表明,在乳腺癌的大鼠脊柱肿瘤模型中局部施用rhBMP-2(15μg,10μl1.5 mg / ml溶液)不仅不能刺激局部肿瘤的生长,而且会降低局部肿瘤的生长和延缓大鼠轻瘫的发作。该临床前实验首次表明,rhBMP-2在脊柱肿瘤床上的局部放置可能减慢肿瘤的进展并延迟相关的神经功能衰退。

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