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邓宁R3327H前列腺腺癌对放疗和各种化疗药物的反应。

Response of the Dunning R3327H prostatic adenocarcinoma to radiation and various chemotherapeutic drugs.

作者信息

Mador D, Ritchie B, Meeker B, Moore R, Elliott F G, McPhee M S, Chapman J D, Lakey W H

出版信息

Cancer Treat Rep. 1982 Oct;66(10):1837-43.

PMID:6889915
Abstract

Dunning R3327H prostatic adenocarcinoma was bilaterally transplanted in the flanks of animals at the Papanicolaou Institute in Miami, and the animals were received at the Cross Cancer Institute (Edmonton, Alberta, Canada) each month. The animal flanks were palpated weekly, and when tumor volumes reached a size of approximately 300 mm3 the animals were randomized into treatment groups for the assessment of various therapies. Tumor volumes were determined each week before and after various treatments, and tumor growth was compared to that in untreated controls. Ionizing radiation at relatively small single doses completely inhibits tumor growth for a period of up to 6 months. Some interesting characteristics of this radiation-induced growth arrest are that tumors do not die and shrink away as with some other tumor models but remain static in size and show histologic evidence of viable tumor cells. The hypoxic cell radiosensitizer misonidazole potentiates radiation response in this tumor model. Cisplatin, vincristine, etoposide, and estramustine phosphate administered in drug doses approaching their toxic limits have a partial effect on tumor growth.

摘要

邓宁R3327H前列腺腺癌被双侧移植到迈阿密帕潘尼古拉乌研究所动物的胁腹处,每月将这些动物送到加拿大艾伯塔省埃德蒙顿市的十字癌症研究所。每周对动物的胁腹进行触诊,当肿瘤体积达到约300立方毫米时,将动物随机分为治疗组以评估各种疗法。在各种治疗前后每周测定肿瘤体积,并将肿瘤生长情况与未治疗的对照组进行比较。相对小剂量的单次电离辐射可完全抑制肿瘤生长长达6个月。这种辐射诱导的生长停滞的一些有趣特征是,肿瘤不会像其他一些肿瘤模型那样死亡并缩小,而是保持大小不变,并显示出存活肿瘤细胞的组织学证据。缺氧细胞放射增敏剂米索硝唑可增强该肿瘤模型中的辐射反应。以接近其毒性极限的药物剂量给予顺铂、长春新碱、依托泊苷和磷酸雌莫司汀对肿瘤生长有部分作用。

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