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依伐普酶(efaproxiral)对小鼠皮下RIF-1肿瘤氧合作用及放疗介导的肿瘤生长抑制增强作用的影响。

The effects of Efaproxyn (efaproxiral) on subcutaneous RIF-1 tumor oxygenation and enhancement of radiotherapy-mediated inhibition of tumor growth in mice.

作者信息

Hou Huagang, Khan Nadeem, Grinberg Oleg Y, Yu Hongsheng, Grinberg Stalina A, Lu Shiyi, Demidenko Eugene, Steffen Robert P, Swartz Harold M

机构信息

Department of Diagnostic Radiology, Dartmouth Medical School, Hanover, NH 03755, USA.

出版信息

Radiat Res. 2007 Aug;168(2):218-25. doi: 10.1667/RR0962.1.

Abstract

Efaproxiral, an allosteric modifier of hemoglobin, reduces hemoglobin-oxygen binding affinity, facilitating oxygen release from hemoglobin, which is likely to increase tissue pO(2). The purpose of this study was to determine the effect of efaproxiral on tumor oxygenation and growth inhibition of RIF-1 tumors that received X radiation (4 Gy) plus oxygen breathing compared to radiation plus oxygen plus efaproxiral daily for 5 days. Two lithium phthalocyanine (LiPc) deposits were implanted in RIF-1 tumors in C3H mice for tumor pO(2) measurements using EPR oximetry. Efaproxiral significantly increased tumor oxygenation by 8.4 to 43.4 mmHg within 5 days, with maximum increases at 22-31 min after treatment. Oxygen breathing alone did not affect tumor pO(2). Radiation plus oxygen plus efaproxiral produced tumor growth inhibition throughout the treatment duration, and inhibition was significantly different from radiation plus oxygen from day 3 to day 5. The results of this study provide unambiguous quantitative information on the effectiveness of efaproxiral to consistently and reproducibly increase tumor oxygenation over the course of 5 days of treatment, modeling the clinical use of efaproxiral. Also, based on the tumor growth inhibition, the study shows the efaproxiral-enhanced tumor oxygenation was radiobiologically significant. This is the first study to demonstrate the ability of efaproxiral to increase tumor oxygenation and to increase the tumor growth inhibition of radiotherapy over 5 days of treatment.

摘要

依氟普胺是一种血红蛋白变构调节剂,可降低血红蛋白与氧的结合亲和力,促进氧从血红蛋白释放,这可能会增加组织的氧分压(pO₂)。本研究的目的是确定依氟普胺对接受X射线照射(4 Gy)并吸氧的RIF-1肿瘤的肿瘤氧合作用及生长抑制的影响,并与每天接受辐射加氧气加依氟普胺共5天的情况进行比较。在C3H小鼠的RIF-1肿瘤中植入两个锂酞菁(LiPc)沉积物,用于使用电子顺磁共振波谱法进行肿瘤pO₂测量。依氟普胺在5天内可使肿瘤氧合作用显著增加8.4至43.4 mmHg,治疗后22 - 31分钟时增加幅度最大。单独吸氧对肿瘤pO₂没有影响。辐射加氧气加依氟普胺在整个治疗期间均产生肿瘤生长抑制作用,从第3天到第5天,其抑制作用与辐射加氧气组有显著差异。本研究结果提供了明确的定量信息,表明依氟普胺在5天的治疗过程中能够持续且可重复地增加肿瘤氧合作用,模拟了依氟普胺的临床应用。此外,基于肿瘤生长抑制情况,该研究表明依氟普胺增强的肿瘤氧合作用具有放射生物学意义。这是第一项证明依氟普胺在5天治疗过程中能够增加肿瘤氧合作用并增强放疗对肿瘤生长抑制作用的研究。

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