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Neural progenitor cell-mediated delivery of osteoprotegerin limits disease progression in a preclinical model of neuroblastoma bone metastasis.

机译:在神经母细胞瘤骨转移的临床前模型中,神经祖细胞介导的骨保护素传递限制了疾病进展。

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PURPOSE: Osteoprotegerin (OPG) inhibits osteoclast activation and reduces osteolysis in bone tumors. We hypothesized that tumor-tropic neural progenitor cells (NPCs) engineered to express OPG would reduce neuroblastoma disease burden in the bone. METHODS: Stable expression of green fluorescent protein (NPC-GFP) and OPG (NPC-OPG) was established in human NPCs by lentivirus-mediated transduction. Bone disease was established by intrafemoral injection of luciferase-expressing human neuroblastoma (CHLA-255) cells into 20 SCID mice. Three weeks later, mice began receiving intravenous injection of 2 x 10(6) NPC-OPG or NPC-GFP (control) every 10 days x 3 doses. Disease was monitored with quantitative bioluminescence imaging and x-ray images, which were evaluated on a scale of 0 to 4. These studies were approved by the Institutional Animal Care and Use Committee. RESULTS: Osteoprotegerin treatment in vitro produced no direct toxicity to tumor cells. Coculture of tumor cells with bone marrow significantly increased
机译:目的:骨保护素(OPG)抑制破骨细胞活化并减少骨肿瘤中的骨溶解。我们假设工程化以表达OPG的肿瘤嗜性神经祖细胞(NPC)将减少骨骼中的神经母细胞瘤疾病负担。方法:通过慢病毒介导的转导,在人鼻咽癌中建立了绿色荧光蛋白(NPC-GFP)和OPG(NPC-OPG)的稳定表达。通过向20只SCID小鼠股内注射表达荧光素酶的人神经母细胞瘤(CHLA-255)细胞来确定骨骼疾病。三周后,小鼠开始每10天x 3剂静脉注射2 x 10(6)NPC-OPG或NPC-GFP(对照)。通过定量的生物发光成像和X射线图像对疾病进行监控,并以0到4的等级进行评估。这些研究得到了机构动物护理和使用委员会的批准。结果:体外骨保护素对肿瘤细胞未产生直接毒性。肿瘤细胞与骨髓的共培养显着增加

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