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依托硝唑在人脑肿瘤中的分布:对治疗高级别胶质瘤的意义。

Distribution of etanidazole into human brain tumors: implications for treating high grade gliomas.

作者信息

Hurwitz S J, Coleman C N, Riese N, Loeffler J S, Alexander E, Buswell L, Neben T Y, Shargel L, Kramer R A

机构信息

Joint Center of Radiation Therapy, Harvard Medical School, Boston, MA 02115.

出版信息

Int J Radiat Oncol Biol Phys. 1992;22(3):573-6. doi: 10.1016/0360-3016(92)90879-m.

Abstract

Etanidazole was developed as an oxygen-mimetic radiosensitizer less lipophilic than misonidazole. Sensitization depends on an adequate concentration of drug in the tumor at the time of irradiation. Therefore, due to the presence of the blood-brain barrier, brain tumors may theoretically be difficult to radiosensitize due to the hydrophilic characteristics of etanidazole. Based on previous reports of loss of BBB integrity in brain tumors, we investigated the ability of etanidazole to penetrate into malignant gliomas of patients receiving etanidazole as part of a Phase I continuous infusion protocol. The patients had completed previous external beam irradiation. Twenty-two patients were studied and their etanidazole plasma and biopsy data were compared to the 2-compartment model derived from a second group of 19 patients with bolus etanidazole. Etanidazole concentration in brain tumor biopsies varied widely and appeared to be clustered into a higher and a lower pharmacokinetic group having mean tumor to well-perfused second compartment ratios of 1 and 0.25, respectively. Both high and low etanidazole concentrations were evident in different biopsies obtained from the same patient. Correlations between histology and tissue concentrations suggested that the higher level correspond to malignant tissue. These data indicate that the blood brain barrier is disrupted to varying degrees by the brain tumor and/or prior irradiation and that etanidazole penetrates into brain tumors.

摘要

依托硝唑是作为一种比甲硝唑亲脂性更低的拟氧放射增敏剂而开发的。放射增敏作用取决于照射时肿瘤内药物的适当浓度。因此,由于血脑屏障的存在,理论上脑肿瘤可能因依托硝唑的亲水性特征而难以实现放射增敏。基于先前关于脑肿瘤血脑屏障完整性丧失的报道,我们研究了依托硝唑在作为I期持续输注方案一部分接受依托硝唑治疗的患者的恶性胶质瘤中的渗透能力。这些患者之前已完成外照射。对22名患者进行了研究,并将他们的依托硝唑血浆和活检数据与另一组19名接受大剂量依托硝唑治疗患者的二室模型数据进行了比较。脑肿瘤活检中的依托硝唑浓度差异很大,似乎聚集成一个较高和一个较低的药代动力学组,其平均肿瘤与灌注良好的第二室的比率分别为1和0.25。在同一患者的不同活检中,高和低依托硝唑浓度均很明显。组织学与组织浓度之间的相关性表明,较高水平对应于恶性组织。这些数据表明,血脑屏障因脑肿瘤和/或先前的照射而受到不同程度的破坏,并且依托硝唑可渗透到脑肿瘤中。

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