Zou Yiyu, Fu Hao, Ghosh Sukhen, Farquhar David, Klostergaard Jim
Department of Oncology, Albert Einstein College of Medicine, Bronx, New York, USA.
Clin Cancer Res. 2004 Nov 1;10(21):7382-91. doi: 10.1158/1078-0432.CCR-04-0334.
Paclitaxel (Taxol) has demonstrated clinical activity in non-small-cell lung cancer (NSCLC), but its use has not led to marked improvements in survival. This ineffectiveness can in part be attributed to inadequate delivery of effective drug levels to the lung via systemic administration and to drug resistance mechanisms. Locoregional drug administration and the use of drug copolymers are possible approaches to address these issues. In this study, we evaluated the activity of a poly(L-glutamic acid)-paclitaxel (PGA-TXL) formulation administered by intratracheal injection to mice bearing orthotopic human NSCLC tumors (H460, H358). H460 cells were found to be sensitive to paclitaxel and PGA-TXL in vitro, in a time- and concentration-dependent manner. In preliminary acute toxicity studies, PGA-TXL administered by intratracheal injection was found to be much less toxic than paclitaxel, as anticipated. Mice into which H460 cells had been implanted by intratracheal injection were given single-dose intratracheal treatments with paclitaxel (1.2 or 2.4 mg/kg) or with PGA-TXL (15 mg/kg, paclitaxel equivalents) 1 week later. When the mice were sacrificed at up to 65 days after tumor implantation, they were evaluated grossly for tumor at bronchial, neck, and lung sites. Control mice had tumors in 60% of all three sites, and all of the control mice had tumors in at least one site. The low- and high-dose Taxol groups had fewer incidences at these three sites (27-33%) and 60-80% of these mice had tumors in at least one site. The PGA-TXL mice displayed a low (13%) incidence at these sites, and only 40% had detectable tumors. In a subsequent survival study with the intratracheal H358 model, control mice had a mean life span of 95 days, whereas both the intratracheal Taxol (2.5 mg/kg, every 7th day for three doses) and the intratracheal PGA-TXL (20 mg/kg, paclitaxel equivalents, every 7th day for three doses) groups had improved survival (mean life spans: 133.5 and 136.5 days, respectively). In pilot studies intended to compare the feasibility of the development of paclitaxel aerosols suitable for clinical application, based either on Cremophor solutions or on PGA backbones, only the latter gave acceptable particle size distributions and flow rates. These results encourage the development and application of Cremophor-free copolymer formulations of paclitaxel for locoregional treatment (e.g., as aerosol) of endobronchial malignant diseases.
紫杉醇(泰素)已在非小细胞肺癌(NSCLC)中显示出临床活性,但其使用并未带来生存率的显著提高。这种无效性部分可归因于通过全身给药向肺部输送有效药物水平不足以及耐药机制。局部区域给药和使用药物共聚物是解决这些问题的可能方法。在本研究中,我们评估了通过气管内注射给予携带原位人非小细胞肺癌肿瘤(H460、H358)的小鼠的聚(L-谷氨酸)-紫杉醇(PGA-TXL)制剂的活性。发现H460细胞在体外对紫杉醇和PGA-TXL敏感,呈时间和浓度依赖性。在初步急性毒性研究中,如预期的那样,发现通过气管内注射给予的PGA-TXL的毒性比紫杉醇小得多。在通过气管内注射植入H460细胞的小鼠1周后,分别给予单剂量气管内紫杉醇(1.2或2.4mg/kg)或PGA-TXL(15mg/kg,紫杉醇当量)治疗。当在肿瘤植入后长达65天处死小鼠时,对其支气管、颈部和肺部部位的肿瘤进行大体评估。对照小鼠在所有三个部位中的60%有肿瘤,并且所有对照小鼠至少在一个部位有肿瘤。低剂量和高剂量紫杉醇组在这三个部位的发生率较低(27 - 33%),并且这些小鼠中有60 - 80%至少在一个部位有肿瘤。PGA-TXL组小鼠在这些部位的发生率较低(13%),只有40%有可检测到的肿瘤。在随后使用气管内H358模型的生存研究中,对照小鼠的平均寿命为95天,而气管内紫杉醇组(2.5mg/kg,每7天一次,共三剂)和气管内PGA-TXL组(20mg/kg,紫杉醇当量,每7天一次,共三剂)的生存率均有所提高(平均寿命分别为:133.5天和136.5天)。在旨在比较基于聚氧乙烯蓖麻油溶液或基于PGA主链开发适合临床应用的紫杉醇气雾剂可行性的初步研究中,只有后者给出了可接受的粒径分布和流速。这些结果鼓励开发和应用不含聚氧乙烯蓖麻油的紫杉醇共聚物制剂用于支气管内恶性疾病的局部区域治疗(例如作为气雾剂)。
