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给予甲基黄嘌呤衍生物后肿瘤的局部灌注与氧合

Regional perfusion and oxygenation of tumors upon methylxanthine derivative administration.

作者信息

Kelleher D K, Thews O, Vaupel P

机构信息

Institute of Physiology and Pathophysiology, University of Mainz, Germany.

出版信息

Int J Radiat Oncol Biol Phys. 1998 Nov 1;42(4):861-4. doi: 10.1016/s0360-3016(98)00318-6.

Abstract

PURPOSE

The use of methylxanthine derivatives has been postulated as a means of increasing tumor perfusion and thus ameliorating tumor hypoxia. The aim of this study was to quantify and compare the effects of three methylxanthine derivatives: pentoxifylline (PX), torbafylline (TB), and HWA 138 (HW) on tumor perfusion and oxygenation.

METHODS AND MATERIALS

Anesthetized Sprague Dawley rats with DS-sarcomas implanted subcutaneously onto the hind foot dorsum were used in this study. Mean arterial blood pressure (MABP) was measured throughout experiments. Regional red blood cell (RBC) flux was monitored using a multichannel laser Doppler device and tumor oxygenation on a more global level was assessed polarographically using an O2-sensitive catheter electrode. The methylxanthine derivatives were administered as a single dose intraperitoneally (for PX 50 mg/kg; for TB and HW 75 mg/kg).

RESULTS

Following drug administration, initial decreases in MABP down to 75% of baseline values were observed for all three substances. PX, HW, and TB caused initial transient reductions in mean RBC flux followed by gradual increases to values of 137 +/- 27%, 139 +/- 14%, and 122 + 14% respectively at t = 60 min. Following a small initial decrease upon drug administration, O2 partial pressure (pO2) rose to 160 +/- 31%, 153 +/- 34%, and 121 +/- 11% for PX, HW, and TB, respectively at t = 60 min. At the end of the observation period (t = 90 min), increases in RBC flux and pO2 were still evident. When individual tumors were considered, a variety of patterns (including opposing effects) for changes in RBC flux were seen, not necessarily reflected in the mean values. Thus, while the methylxanthine derivatives caused an increased average tumor perfusion, there is evidence suggesting that a redistribution of tumor blood flow occurs which may amplify preexisting heterogeneity.

CONCLUSIONS

Substantial improvements in tumor oxygenation and perfusion were observed after administration of the methylxanthine derivatives. These substances may therefore be of use during tumor therapies in which the outcome may be detrimentally affected by the presence of hypoxia.

摘要

目的

甲基黄嘌呤衍生物的使用被认为是增加肿瘤灌注从而改善肿瘤缺氧的一种方法。本研究的目的是量化并比较三种甲基黄嘌呤衍生物:己酮可可碱(PX)、托巴茶碱(TB)和HWA 138(HW)对肿瘤灌注和氧合的影响。

方法和材料

本研究使用了麻醉的Sprague Dawley大鼠,其在后足背皮下植入了DS - 肉瘤。在整个实验过程中测量平均动脉血压(MABP)。使用多通道激光多普勒装置监测局部红细胞(RBC)通量,并使用对O2敏感的导管电极通过极谱法在更全局的水平上评估肿瘤氧合。甲基黄嘌呤衍生物以单剂量腹腔注射给药(PX为50 mg/kg;TB和HW为75 mg/kg)。

结果

给药后,观察到所有三种物质的MABP最初下降至基线值的75%。PX、HW和TB导致平均RBC通量最初短暂降低,随后在t = 60分钟时逐渐增加,分别达到137 +/- 27%、139 +/- 14%和122 + 14%的值。给药后最初有小幅下降,O2分压(pO2)在t = 60分钟时分别升至PX为160 +/- 31%、HW为153 +/- 34%、TB为121 +/- 11%。在观察期结束时(t = 90分钟),RBC通量和pO2的增加仍然明显。当考虑单个肿瘤时,观察到RBC通量变化的多种模式(包括相反的效应),不一定反映在平均值中。因此,虽然甲基黄嘌呤衍生物导致平均肿瘤灌注增加,但有证据表明肿瘤血流发生了重新分布,这可能会放大先前存在的异质性。

结论

甲基黄嘌呤衍生物给药后观察到肿瘤氧合和灌注有显著改善。因此,这些物质可能在肿瘤治疗中有用,在这些治疗中,缺氧的存在可能会对结果产生不利影响。

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