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包括通过瘤内注射胶体铬32P在内的各种治疗溶液对裸鼠体内AsPC-1人胰腺肿瘤异种移植瘤的肿瘤生理参数的影响。

The effect of various therapeutic solutions including colloidal chromic 32P via an intratumoral injection on the tumor physiological parameters of AsPC-1 human pancreatic tumor xenografts in nude mice.

作者信息

Lee I, Lee Y H

机构信息

Radiation Research Laboratory, Division of Radiation Research, UMDNJ-Robert Wood Johnson Medical School, Camden, New Jersey 08103, USA.

出版信息

Clin Cancer Res. 1999 Oct;5(10 Suppl):3139s-3142s.

Abstract

To overcome the physiological barrier in solid tumors (i.e., tumor hypertension), a large volume of material is required via an intratumoral injection. Alternatively, a method of reduction in tumor hypertension is also feasible. In this study, we focused on the physiological response after an intratumoral infusion of various therapeutic agents. Tumor interstitial fluid pressure (TIFP) was intermittently monitored for up to 7 days after treatment using AsPC-1 human pancreatic tumors in nude mice. Macroaggregated albumin (MAA), colloidal chromic 32P (32P-CP), albumin, dexamethasone, 5-fluoro-2'deoxyuridine, dextrose, saline, and trypan blue increased TIFP within approximately 5 min, and TIFP returned to the original level within 1 h, except in the case of MAA and 32P-CP. We also found that the maximal uptake for AsPC-1 tumors in both the exponential and plateau growth phases occurred at approximately 100 min postincubation; the maximum value in the exponential growth phase was approximately 2 times less than that of plateau growth phase (P < 0.01). Therefore, this study supports intralesional 32P-CP brachytherapy for nonresectional pancreatic cancer patients. This may offer a promising treatment modality for delivering high doses of tumor-selective radiation, mainly due to two physiological mechanisms: (a) the high adherence of 32P-CP to the infused regions; and (b) reduction in either tumor blood flow or TIFP by this therapeutic colloid.

摘要

为克服实体瘤中的生理屏障(即肿瘤高血压),通过瘤内注射需要大量物质。另外,降低肿瘤高血压的方法也是可行的。在本研究中,我们关注瘤内注入各种治疗剂后的生理反应。使用裸鼠体内的AsPC-1人胰腺肿瘤,在治疗后长达7天间歇性监测肿瘤间质液压力(TIFP)。大颗粒白蛋白(MAA)、胶体铬32P(32P-CP)、白蛋白、地塞米松、5-氟-2'-脱氧尿苷、葡萄糖、盐水和台盼蓝在约5分钟内使TIFP升高,除MAA和32P-CP外,TIFP在1小时内恢复到原始水平。我们还发现,AsPC-1肿瘤在指数生长期和平稳期的最大摄取量在孵育后约100分钟出现;指数生长期的最大值比平稳期约低2倍(P < 0.01)。因此,本研究支持对不可切除的胰腺癌患者进行瘤内32P-CP近距离放射治疗。这可能为提供高剂量的肿瘤选择性辐射提供一种有前景的治疗方式,主要归因于两种生理机制:(a)32P-CP对注入区域的高粘附性;以及(b)这种治疗性胶体使肿瘤血流或TIFP降低。

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