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四(间羟基苯基)二氢卟吩在仓鼠颊囊肿瘤模型中的药代动力学和药效学:与临床测量结果的比较

Pharmacokinetics and pharmacodynamics of tetra(m-hydroxyphenyl)chlorin in the hamster cheek pouch tumor model: comparison with clinical measurements.

作者信息

Glanzmann T, Forrer M, Blant S A, Woodtli A, Grosjean P, Braichotte D, van den Bergh H, Monnier P, Wagnières G

机构信息

Institute of Environmental Engineering, Swiss Federal Institute of Technology (EPFL), Lausanne, Switzerland.

出版信息

J Photochem Photobiol B. 2000 Aug;57(1):22-32. doi: 10.1016/s1011-1344(00)00069-5.

Abstract

The pharmacokinetics (PK) of the photosensitizer tetra(m-hydroxyphenyl)chlorin (mTHPC) was measured by optical fiber-based light-induced fluorescence spectroscopy (LIFS) in the normal and tumoral cheek pouch mucosa of 29 Golden Syrian hamsters with chemically induced squamous cell carcinoma. Similar measurements were carried out on the normal oral cavity mucosa of five patients up to 30 days after injection. The drug doses were between 0.15 and 0.3 mg per kg of body weight (mg/kg), and the mTHPC fluorescence in the tissue was excited at 420 nm. The PK in both human and hamster exhibited similar behavior although the PK in the hamster mucosa was slightly delayed in comparison with that of its human counterpart. The mTHPC fluorescence signal of the hamster mucosa was smaller than that of the human mucosa by a factor of about 3 for the same injected drug dose. A linear correlation was found between the fluorescence signal and the mTHPC dose in the range from 0.075 to 0.5 mg/kg at times between 8 and 96 h after injection. No significant selectivity in mTHPC fluorescence between the tumoral and normal mucosa of the hamsters was found at any of the applied conditions. The sensitivity of the normal and tumoral hamster cheek pouch mucosa to mTHPC photodynamic therapy as a function of the light dose was determined by light irradiation at 650 nm and 150 mW/cm2, 4 days after the injection of a drug dose of 0.15 mg/kg. These results were compared with irradiations of the normal oral and normal and tumoral bronchial mucosa of 37 patients under the same conditions. The reaction to PDT of both types of human mucosae was considerably stronger than that of the hamster cheek pouch mucosa. The sensitivity to PDT became comparable between hamster and human mucosa when the drug dose for the hamster was increased to 0.5 mg/kg. A significant therapeutic selectivity between the normal and neoplastic hamster cheek pouch was observed. Less selectivity was found following irradiations of normal mucosa and early carcinomas in the human bronchi. The pharmacodynamic behavior of mTHPC was determined by test irradiations of the normal mucosa of hamsters and patients between 6 h and 8 days after injection of 0.5 and 0.15 mg/kg in the hamsters and the patients, respectively. The normal hamster cheek pouch showed a maximum response to irradiation 6 h after injection and then decreased continuously to no observable reaction at 8 days after injection. The reaction of the normal human oral mucosa, however, showed an increasing sensitivity to the applied light between 6 h and 4 days after mTHPC injection and then decreased again at 8 days. The hamster model with the chemically induced early squamous cell cancer in the cheek pouch thus showed some similarity to the early squamous cell cancer of the human oral mucosa considering the PK. However, a quantitative difference in fluorescence signal for identical mTHPC doses as well as a significant difference in pharmacodynamic behavior were also observed. The suitability of this animal model for the optimization of PDT parameters in the clinic is therefore limited. Hence great care must be taken in screening new dyes for PDT of early squamous cell cancer of the upper aerodigestive tract based upon observables in the hamster cheek pouch model.

摘要

采用基于光纤的光诱导荧光光谱法(LIFS),测定了29只化学诱导产生鳞状细胞癌的金黄叙利亚仓鼠正常及肿瘤性颊囊黏膜中光敏剂四(间羟基苯基)氯卟啉(mTHPC)的药代动力学(PK)。对5例患者在注射后长达30天的正常口腔黏膜进行了类似测量。药物剂量为每千克体重0.15至0.3毫克(mg/kg),组织中的mTHPC荧光在420纳米处激发。人与仓鼠的PK表现出相似的行为,尽管仓鼠黏膜中的PK与其人类对应物相比略有延迟。对于相同的注射药物剂量,仓鼠黏膜的mTHPC荧光信号比人类黏膜小约3倍。在注射后8至96小时之间,荧光信号与mTHPC剂量在0.075至0.5 mg/kg范围内呈线性相关。在任何应用条件下,均未发现仓鼠肿瘤和正常黏膜之间mTHPC荧光有明显选择性。在注射0.15 mg/kg药物剂量4天后,通过650纳米、150 mW/cm²的光照,测定了正常和肿瘤性仓鼠颊囊黏膜对mTHPC光动力疗法的敏感性与光剂量的关系。将这些结果与37例患者在相同条件下对正常口腔、正常及肿瘤性支气管黏膜的照射结果进行了比较。两种类型的人类黏膜对光动力疗法的反应明显强于仓鼠颊囊黏膜。当仓鼠的药物剂量增加到0.5 mg/kg时,仓鼠和人类黏膜对光动力疗法的敏感性变得相当。观察到正常和肿瘤性仓鼠颊囊之间有显著的治疗选择性。在照射人类支气管的正常黏膜和早期癌时,发现选择性较小。分别给仓鼠和患者注射0.5和0.15 mg/kg后,通过对仓鼠和患者正常黏膜在注射后6小时至8天的测试照射,确定了mTHPC的药效学行为。正常仓鼠颊囊在注射后6小时对照射表现出最大反应,然后在注射后8天持续下降至无明显反应。然而,正常人类口腔黏膜的反应在mTHPC注射后6小时至4天对施加的光的敏感性增加,然后在8天再次下降。因此,颊囊中化学诱导早期鳞状细胞癌的仓鼠模型在PK方面与人口腔黏膜早期鳞状细胞癌有一些相似之处。然而,对于相同的mTHPC剂量,荧光信号存在定量差异,药效学行为也有显著差异。因此,这种动物模型在临床上优化光动力疗法参数的适用性有限。因此,在基于仓鼠颊囊模型的观察结果筛选用于上消化道早期鳞状细胞癌光动力疗法的新染料时,必须格外小心。

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