Borgatti-Jeffreys Antonella, Hooser Stephen B, Miller Margaret A, Lucroy Michael D
Department of Veterinary Clinical Sciences, School of Veterinary Medicine, Purdue University, West Lafayette, IN 47907, USA.
Am J Vet Res. 2007 Apr;68(4):399-404. doi: 10.2460/ajvr.68.4.399.
To determine the threshold for acute toxicosis of parenterally administered zinc phthalocyanine tetrasulfonate (ZnPcS(4)), a candidate second-generation photosensitizer, in mice and evaluate the compound's safety in a phase I clinical trial of ZnPcS(4)-based photodynamic therapy (PDT) in pet dogs with naturally occurring tumors.
Male Swiss-Webster mice and client-owned dogs with naturally occurring neoplasms.
For the study of acute toxicosis, mice were given graded doses of ZnPcS(4). To determine safety, a rapid-titration phase I clinical trial of ZnPcS(4)-based PDT in tumor-bearing dogs was conducted.
In mice, administration of >or= 100 mg of ZnPcS(4)/kg resulted in renal tubular necrosis 24 hours after IP injection. In tumor-bearing dogs, ZnPcS(4) doses <or= 4 mg/kg induced no signs of toxicosis and resulted in partial to complete tumor responses in 10 of 12 dogs 4 weeks after PDT. Tumor remission was observed with ZnPcS(4) doses as low as 0.25 mg/kg.
A conservative starting dose of ZnPcS(4) was arrived at on the basis of mouse toxicosis findings. Zinc phthalocyanine tetrasulfonate-based PDT was tolerated well by all dogs and warrants further study. The identification of the maximum tolerated dose through traditional phase I clinical trials may be unnecessary for evaluating novel PDT protocols.
确定第二代光敏剂候选药物静脉注射四磺化酞菁锌(ZnPcS(4))在小鼠体内的急性中毒阈值,并在一项针对患有自然发生肿瘤的宠物狗的基于ZnPcS(4)的光动力疗法(PDT)的I期临床试验中评估该化合物的安全性。
雄性瑞士韦伯斯特小鼠和患有自然发生肿瘤的客户拥有的狗。
为研究急性中毒,给小鼠给予分级剂量的ZnPcS(4)。为确定安全性,对荷瘤狗进行了基于ZnPcS(4)的PDT的快速滴定I期临床试验。
在小鼠中,腹腔注射后24小时,给予≥100 mg ZnPcS(4)/kg会导致肾小管坏死。在荷瘤狗中,ZnPcS(4)剂量≤4 mg/kg未引起中毒迹象,并且在PDT后4周,12只狗中有10只出现部分至完全肿瘤反应。观察到低至0.25 mg/kg的ZnPcS(4)剂量可使肿瘤缓解。
根据小鼠中毒结果得出了ZnPcS(4)的保守起始剂量。所有狗对基于四磺化酞菁锌的PDT耐受性良好,值得进一步研究。通过传统I期临床试验确定最大耐受剂量对于评估新型PDT方案可能没有必要。
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