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通过降低血红蛋白亲和力实现肿瘤放射增敏作用。

Tumor radiosensitization through reductions in hemoglobin affinity.

作者信息

Siemann D W, Macler L M

出版信息

Int J Radiat Oncol Biol Phys. 1986 Aug;12(8):1295-7. doi: 10.1016/0360-3016(86)90157-4.

Abstract

Alterations in the oxygen (O2) distribution in a tumor due to changes in the quantity of O2 carried in the blood can affect the response of a tumor to radiation. For example, the blood hemoglobin (Hb) level has been shown to be an important prognostic and therapeutic factor in radiation therapy. Another factor affecting the delivery of O2 to tissues is the Hb affinity for O2. Changes in Hb affinity for O2 result in shifts of the Hb-O2 dissociation curve which increase or decrease tissue oxygenation. The aim of the present studies was to determine whether reductions in Hb affinity prior to irradiation could improve the resultant tumor response. KHT sarcomas were irradiated in female C3H/HeJ mice, possessing either normal or reduced Hb affinities for O2 at the time of treatment. Changes in Hb affinity for O2 were induced by keeping tumor-bearing mice in a 12% O2 environment for various periods of time. Erythrocyte 2,3-diphosphoglycerate (2,3 DPG) was measured as an indicator of Hb affinity for O2. After 36 hr of low O2 exposure, 2,3 DPG levels increased 20-30%. This change in 2,3 DPG reflected a proportional decrease in Hb affinity for O2. Following the exposure of 12% O2, the animals were removed from the low O2 chamber and their tumors locally irradiated while the mice breathed air. After irradiation, tumor cell survival was determined using an in vivo to in vitro excision assay. The results indicate that the fraction of hypoxic cells in tumors of mice whose Hb affinity had been reduced prior to irradiation was approximately 3%. By comparison, the hypoxic fraction in tumors irradiated in mice with normal Hb affinities was approximately 15%. Thus, reductions in Hb affinity prior to irradiation can yield significant radiation sensitization in tumors. These findings form the basis for future investigations of the use of pharmacologic methods for the in vivo alteration of the Hb-O2 dissociation curve to improve tumor oxygenation.

摘要

由于血液中携带的氧气(O2)量的变化而导致的肿瘤内氧气(O2)分布改变,会影响肿瘤对辐射的反应。例如,血液血红蛋白(Hb)水平已被证明是放射治疗中一个重要的预后和治疗因素。另一个影响氧气向组织输送的因素是Hb对O2的亲和力。Hb对O2亲和力的变化会导致Hb-O2解离曲线的移动,从而增加或减少组织的氧合作用。本研究的目的是确定照射前降低Hb亲和力是否能改善肿瘤的最终反应。在雌性C3H/HeJ小鼠中对KHT肉瘤进行照射,这些小鼠在治疗时Hb对O2的亲和力正常或降低。通过将荷瘤小鼠置于12% O2环境中不同时间段来诱导Hb对O2亲和力的变化。测量红细胞2,3-二磷酸甘油酸(2,3 DPG)作为Hb对O2亲和力的指标。在低氧暴露36小时后,2,3 DPG水平增加了20 - 30%。2,3 DPG的这种变化反映了Hb对O2亲和力成比例下降。在暴露于12% O2后,将动物从低氧舱中取出,在小鼠呼吸空气时对其肿瘤进行局部照射。照射后,使用体内到体外切除试验确定肿瘤细胞存活率。结果表明,照射前Hb亲和力降低的小鼠肿瘤中缺氧细胞的比例约为3%。相比之下,Hb亲和力正常的小鼠照射后肿瘤中的缺氧比例约为15%。因此,照射前降低Hb亲和力可在肿瘤中产生显著的放射增敏作用。这些发现为未来研究使用药理学方法在体内改变Hb-O2解离曲线以改善肿瘤氧合作用奠定了基础。

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