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Photodynamic therapy of diseased bone

机译:患骨的光动力疗法

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Objective: Photodynamic therapy (PDT) defines the oxygen-dependent reaction that occurs upon light-mediated activation of a photosensitizing compound, culminating in the generation of cytotoxic, reactive oxygen species, predominantly, singlet oxygen. We are investigating PDT treatment of diseased bone. Methods: Using a rat model of human breast cancer (MT-1)-derived bone metastasis we confirmed the efficacy of benzoporphyrin-derivative monoacid (BPD-MA)-PDT for treating metastatic lesions within vertebrae or long bones. Results: Light administration (150 J) 15 mins after BPD-MA (2.5 mg/Kg, i.v.) into the lumbar (L3) vertebra of rats resulted in complete ablation of the tumour and surrounding bone marrow 48 hrs post-PDT without paralysis. Porcine vertebrae provided a model comparable to that of human for light propagation (at 150 J/cm) and PDT response (BPD-MA; 6 mg/m~2, i.v.) in non-tumour vertebrae. Precise fibre placement was afforded by 3-D cone beam computed tomography. Average penetration depth of light was 0.16 ± 0.04 cm, however, the necroticon-necrotic interface extended 0.6 cm out from the treatment fiber with an average incident fluence rate of 4.3 mW/cm~2. Non-necrotic tissue damage was evident 2 cm out from the treatment fiber. Current studies involving BPD-MA-PDT treatment of primary osteosarcomas in the forelimbs of dogs are very promising. Magnetic resonance imaging 24 hr post treatment reveal well circumscribed margins of treatment that encompass the entire 3-4 cm lesion. Finally, we are also interested in using 5-aminolevulinic acid (ALA) mediated PDT to treat osteomyelitis. Response to therapy was monitored as changes in bioluminescence signal of staphylococcus aureus (SA)-derived biofilms grown onto 0.5 cm lengths of wire and subjected to ALA-PDT either in vitro or in vivo upon implant into the intramedullary space of rat tibia. Transcutaneous delivery of PDT (75 J/cm~2) effectively eradicated SA-biofilms within bone. Conclusions: Results support the application of PDT to the treatment of primary or metastatic lesions within bone. Secondly, that ALA-PDT may be useful as a treatment for osteomyelitis. Further studies aim to optimize the parameters of delivering PDT into bone and explore imaging technologies that can be used for clinical PDT.
机译:目的:光动力疗法(PDT)定义了光敏化合物的光介导活化后发生的氧依赖性反应,最终产生细胞毒性,活性氧,主要是单线态氧。我们正在研究PDT治疗患病骨。方法:使用人类乳腺癌(MT-1)衍生的大鼠骨转移模型,我们证实了苯并卟啉衍生单酸(BPD-MA)-PDT治疗椎骨或长骨内转移性病变的有效性。结果:BPD-MA(2.5 mg / Kg,i.v.)注入BPD-MA后15分钟(150 J)进入大鼠的腰(L3)椎骨,导致PDT后48小时肿瘤和周围骨髓完全消融,而没有麻痹。猪椎骨为非肿瘤椎骨的光传播(150 J / cm)和PDT响应(BPD-MA; 6 mg / m〜2,静脉内注射)提供了与人类相当的模型。通过3D锥形束计算机断层扫描可以精确放置纤维。光的平均穿透深度为0.16±0.04cm,但是,坏死/非坏死界面从处理纤维伸出0.6cm,平均入射通量率为4.3mW / cm〜2。距治疗纤维2 cm处可见非坏死组织损伤。目前涉及BPD-MA-PDT治疗狗前肢原发性骨肉瘤的研究非常有前途。治疗后24小时的磁共振成像显示治疗边界清楚,包括整个3-4 cm病变。最后,我们也对使用5-氨基乙酰丙酸(ALA)介导的PDT治疗骨髓炎感兴趣。监测对治疗的反应,作为金黄色葡萄球菌(SA)来源的生物膜的生物发光信号的变化,该生物膜生长在0.5 cm长的金属丝上,并在植入大鼠胫骨髓腔内后进行体外或体内ALA-PDT处理。 PDT(75 J / cm〜2)的经皮递送有效消除了骨骼内的SA生物膜。结论:结果支持PDT在骨内原发性或转移性病变治疗中的应用。其次,ALA-PDT可能可用于治疗骨髓炎。进一步的研究旨在优化将PDT传递到骨骼中的参数,并探索可用于临床PDT的成像技术。

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