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首页> 美国卫生研究院文献>other >Expression of the Chemokine Receptor CXCR7 in CXCR4-Expressing Human 143B Osteosarcoma Cells Enhances Lung Metastasis of Intratibial Xenografts in SCID Mice
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Expression of the Chemokine Receptor CXCR7 in CXCR4-Expressing Human 143B Osteosarcoma Cells Enhances Lung Metastasis of Intratibial Xenografts in SCID Mice

机译:趋化因子受体CXCR7在表达CXCR4的人143B骨肉瘤细胞中的表达增强SCID小鼠胫骨异种移植物的肺转移。

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More effective treatment of metastasizing osteosarcoma with a current mean 5-year survival rate of less than 20% requires more detailed knowledge on mechanisms and key regulatory molecules of the complex metastatic process. CXCR4, the receptor of the chemokine CXCL12, has been reported to promote tumor progression and metastasis in osteosarcoma. CXCR7 is a recently deorphanized CXCL12-scavenging receptor with so far not well-defined functions in tumor biology. The present study focused on a potential malignancy enhancing function of CXCR7 in interaction with CXCR4 in osteosarcoma, which was investigated in an intratibial osteosarcoma model in SCID mice, making use of the human 143B osteosarcoma cell line that spontaneously metastasizes to the lung and expresses endogenous CXCR4. 143B osteosarcoma cells stably expressing LacZ (143B-LacZ cells) were retrovirally transduced with a gene encoding HA-tagged CXCR7 (143B-LacZ-X7-HA cells). 143B-LacZ-X7-HA cells co-expressing CXCR7 and CXCR4 exhibited CXCL12 scavenging and enhanced adhesion to IL-1β-activated HUVEC cells compared to 143B-LacZ cells expressing CXCR4 alone. SCID mice intratibially injected with 143B-LacZ-X7-HA cells had significantly (p<0.05) smaller primary tumors, but significantly (p<0.05) higher numbers of lung metastases than mice injected with 143B-LacZ cells. Unexpectedly, 143B-LacZ-X7-HA cells, unlike 143B-LacZ cells, also metastasized with high incidence to the auriculum cordis. In conclusion, expression of the CXCL12 scavenging receptor CXCR7 in the CXCR4-expressing human 143B osteosarcoma cell line enhances its metastatic activity in intratibial primary tumors in SCID mice that predominantly metastasize to the lung and thereby closely mimic the human disease. These findings point to CXCR7 as a target, complementary to previously proposed CXCR4, for more effective metastasis-suppressive treatment in osteosarcoma.
机译:目前平均5年生存率低于20%的更有效的转移性骨肉瘤治疗,需要对复杂转移过程的机制和关键调节分子有更详细的了解。据报道,趋化因子CXCL12的受体CXCR4可促进骨肉瘤中的肿瘤进展和转移。 CXCR7是最近去孤儿的CXCL12清除受体,迄今为止在肿瘤生物学中尚无明确的功能。本研究集中于在骨肉瘤中CXCR7与CXCR4相互作用的潜在恶性增强功能,这在SCID小鼠的胫骨骨肉瘤模型中进行了研究,利用了人类143B骨肉瘤细胞系自发转移至肺部并表达内源性CXCR4 。用编码HA标签的CXCR7的基因(143B-LacZ-X7-HA细胞)逆转录病毒转导稳定表达LacZ的143B骨肉瘤细胞(143B-LacZ细胞)。与单独表达CXCR4的143B-LacZ细胞相比,共表达CXCR7和CXCR4的143B-LacZ-X7-HA细胞表现出CXCL12清除能力和对IL-1β激活的HUVEC细胞的粘附性增强。胫骨内注射143B-LacZ-X7-HA细胞的SCID小鼠的原发肿瘤明显小(p <0.05),但与转移143B-LacZ细胞的小鼠相比,肺转移的数目明显多(p <0.05)。出乎意料的是,与143B-LacZ细胞不同,143B-LacZ-X7-HA细胞也以高发生率转移到了耳道。总之,在表达CXCR4的人143B骨肉瘤细胞系中CXCL12清除受体CXCR7的表达增强了其在SCID小鼠胫内原发性肿瘤中的转移活性,该肿瘤主要转移至肺部,从而与人类疾病密切相似。这些发现指出,CXCR7是与先前提出的CXCR4互补的靶标,可以更有效地抑制骨肉瘤的转移。

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