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首页> 外文期刊>Clinical and experimental metastasis >Effect of zoledronic acid and amputation on bone invasion and lung metastasis of canine osteosarcoma in nude mice.
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Effect of zoledronic acid and amputation on bone invasion and lung metastasis of canine osteosarcoma in nude mice.

机译:唑来膦酸和截肢术对裸鼠犬骨肉瘤骨侵袭和肺转移的影响。

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摘要

Osteosarcoma (OSA) is an aggressive, highly metastatic and lytic primary bone neoplasm commonly affecting the appendicular skeleton of dogs and children. Current treatment options include amputation of the afflicted limb, limb-sparing procedures, or palliative radiation with or without adjunct chemotherapy. Therapies that inhibit bone resorption, such as the bisphosphonates, may be an effective palliative therapy by limiting the local progression of OSA in those patients that are not viable candidates for amputation. We have developed a mouse model of canine skeletal OSA following intratibial inoculation of OSCA40 cells that spontaneously metastasized to the lungs. We demonstrated that therapy with a nitrogen-containing bisphosphonate, zoledronic acid (Zol), reduced OSA-induced bone lysis; however, Zol monotherapy or in combination with amputation was not effective at inhibiting pulmonary metastasis. While not reaching statistical significance, amputation of the tumor-bearing limb reduced the average incidence of lung metastases; however, this effect was nullified when Zol was added to the treatment protocol. In untreated mice, the magnitude of proximal tibial lysis was significantly correlated with the incidence of metastasis. The data support amputation alone for the management of appendicular OSA rather than combining amputation with Zol. However, in patients that are not viable candidates for amputation, Zol may be a useful palliative therapy for OSA by reducing the magnitude of lysis and therefore bone pain, despite the risk of increased pulmonary metastasis.
机译:骨肉瘤(OSA)是一种侵袭性,高度转移性和溶解性的原发性骨肿瘤,通常会影响狗和儿童的阑尾骨骼。当前的治疗选择包括患肢的截肢,保留肢体的程序或有或没有辅助化疗的姑息性放疗。抑制骨吸收的疗法(例如双膦酸盐)可能是有效的姑息疗法,因为它可以限制那些无法行截肢的患者中OSA的局部进展。在胫骨内接种自发转移至肺部的OSCA40细胞后,我们已经开发了犬骨骼OSA的小鼠模型。我们证明了用含氮的双膦酸盐,唑来膦酸(Zol)治疗可减少OSA引起的骨溶解。但是,Zol单药治疗或联合截肢术不能有效抑制肺转移。虽然未达到统计学显着性,但截肢荷瘤的肢体降低了肺转移的平均发生率。但是,当将Zol添加到治疗方案中时,此效果无效。在未经治疗的小鼠中,胫骨近端溶解的程度与转移的发生率显着相关。数据支持截肢仅用于阑尾OSA的管理,而不是将截肢与Zol结合使用。但是,对于不能行截肢手术的患者,尽管有增加肺转移的风险,但通过降低溶解程度并因此降低骨痛,Zol可能是OSA的有用姑息疗法。

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