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口服维生素D3与光动力疗法联合使用可增强皮肤鳞状细胞癌小鼠模型中的肿瘤细胞死亡。

Combination of oral vitamin D3 with photodynamic therapy enhances tumor cell death in a murine model of cutaneous squamous cell carcinoma.

作者信息

Anand Sanjay, Rollakanti Kishore R, Horst Ronald L, Hasan Tayyaba, Maytin Edward V

机构信息

Department of Biomedical Engineering, Cleveland Clinic, Cleveland, OH; Department of Dermatology, Cleveland Clinic, Cleveland, OH.

出版信息

Photochem Photobiol. 2014 Sep-Oct;90(5):1126-35. doi: 10.1111/php.12286. Epub 2014 May 26.

Abstract

Photodynamic therapy (PDT), in which 5-ALA (a precursor for protoporphyrin IX, PpIX) is administered prior to exposure to light, is a nonscarring treatment for skin cancers. However, for deep tumors, ALA-PDT is not always effective due to inadequate production of PpIX. We previously developed and reported a combination approach in which the active form of vitamin D3 (calcitriol) is given systemically prior to PDT to improve PpIX accumulation and to enhance PDT-induced tumor cell death; calcitriol, however, poses a risk of hypercalcemia. Here, we tested a possible strategy to circumvent the problem of hypercalcemia by substituting natural dietary vitamin D3 (cholecalciferol; D3 ) for calcitriol. Oral D3 supplementation (10 days of a 10-fold elevated D3 diet) enhanced PpIX levels 3- to 4-fold, and PDT-mediated cell death 20-fold, in subcutaneous A431 tumors. PpIX levels and cell viability in normal tissues were not affected. Hydroxylated metabolic forms of D3 were only modestly elevated in serum, indicating minimal hypercalcemic risk. These results show that brief oral administration of cholecalciferol can serve as a safe neoadjuvant to ALA-PDT. We suggest a clinical study, using oral vitamin D3 prior to PDT, should be considered to evaluate this promising new approach to treating human skin cancer.

摘要

光动力疗法(PDT)是一种用于治疗皮肤癌的无瘢痕治疗方法,该疗法在光照前给予5-氨基乙酰丙酸(原卟啉IX,PpIX的前体)。然而,对于深部肿瘤,由于PpIX产生不足,ALA-PDT并不总是有效。我们之前开发并报道了一种联合方法,即在PDT之前全身给予活性形式的维生素D3(骨化三醇),以改善PpIX的积累并增强PDT诱导的肿瘤细胞死亡;然而,骨化三醇存在高钙血症的风险。在此,我们测试了一种可能的策略,即通过用天然膳食维生素D3(胆钙化醇;D3)替代骨化三醇来规避高钙血症问题。口服补充D3(10天给予10倍剂量升高的D3饮食)可使皮下A431肿瘤中的PpIX水平提高3至4倍,PDT介导的细胞死亡增加20倍。正常组织中的PpIX水平和细胞活力不受影响。血清中D3的羟基化代谢形式仅适度升高,表明高钙血症风险极小。这些结果表明,短期口服胆钙化醇可作为ALA-PDT的安全新辅助治疗。我们建议应考虑进行一项临床研究,即在PDT之前使用口服维生素D3,以评估这种有前景的治疗人类皮肤癌的新方法。

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