Radiodynamic Therapy with Acridine Orange Is an Effective Treatment for Bone Metastases

被引:3
作者
Di Pompo, Gemma [1 ]
Kusuzaki, Katsuyuki [2 ]
Ponzetti, Marco [3 ]
Leone, Vito Ferdinando [4 ]
Baldini, Nicola [1 ,5 ]
Avnet, Sofia [5 ]
机构
[1] IRCCS Ist Ortoped Rizzoli, Biomed Sci & Technol & Nanobiotechnol Lab, I-40136 Bologna, Italy
[2] Takai Hosp, Dept Musculoskeletal Oncol, Tenri, Nara 6320372, Japan
[3] Univ Aquila, Dept Biotechnol & Appl Clin Sci, I-67100 Laquila, Italy
[4] Ctr Oncol Vet, I-40037 Bologna, Italy
[5] Univ Bologna, Dept Biomed & Neuromotor Sci, I-40126 Bologna, Italy
关键词
radiodynamic therapy; acridine orange; tumor acidosis; bone metastases; tumor microenvironment; PROTON PUMP INHIBITORS; LIMB SALVAGE SURGERY; LOW-DOSE RADIATION; PHOTODYNAMIC THERAPY; H+-ATPASE; MUSCULOSKELETAL SARCOMAS; FLUORESCENCE MICROSCOPY; K+-ATPASE; V-ATPASE; PH;
D O I
10.3390/biomedicines10081904
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Current multimodal treatment of bone metastases is partially effective and often associated with side effects, and novel therapeutic options are needed. Acridine orange is a photosensitizing molecule that accumulates in acidic compartments. After photo- or radiodynamic activation (AO-PDT or AO-RDT), acridine orange can induce lysosomal-mediated cell death, and we explored AO-RDT as an acid-targeted anticancer therapy for bone metastases. We used osteotropic carcinoma cells and human osteoclasts to assess the extracellular acidification and invasiveness of cancer cells, acridine orange uptake and lysosomal pH/stability, and the AO-RDT cytotoxicity in vitro. We then used a xenograft model of bone metastasis to compare AO-RDT to another antiacid therapeutic strategy (omeprazole). Carcinoma cells showed extracellular acidification activity and tumor-derived acidosis enhanced cancer invasiveness. Furthermore, cancer cells accumulated acridine orange more than osteoclasts and were more sensitive to lysosomal death. In vivo, omeprazole did not reduce osteolysis, whereas AO-RDT promoted cancer cell necrosis and inhibited tumor-induced bone resorption, without affecting osteoclasts. In conclusion, AO-RDT was selectively toxic only for carcinoma cells and effective to impair both tumor expansion in bone and tumor-associated osteolysis. We therefore suggest the use of AO-RDT, in combination with the standard antiresorptive therapies, to reduce disease burden in bone metastasis.
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页数:19
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