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使用氧分压组织成像技术检测和表征肿瘤缺氧情况。

Detection and characterization of tumor hypoxia using pO2 histography.

作者信息

Vaupel Peter, Höckel Michael, Mayer Arnulf

机构信息

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

出版信息

Antioxid Redox Signal. 2007 Aug;9(8):1221-35. doi: 10.1089/ars.2007.1628.

DOI:10.1089/ars.2007.1628
PMID:17536958
Abstract

Data from 125 studies describing the pretreatment oxygenation status as measured in the clinical setting using the computerized Eppendorf pO2 histography system have been compiled in this article. Tumor oxygenation is heterogeneous and severely compromised as compared to normal tissue. Hypoxia results from inadequate perfusion and diffusion within tumors and from a reduced O2 transport capacity in anemic patients. The development of tumor hypoxia is independent of a series of relevant tumor characteristics (e.g., clinical size, stage, histology, and grade) and various patient demographics. Overall median pO2 in cancers of the uterine cervix, head and neck, and breast is 10 mm Hg with the overall hypoxic fraction (pO2 <or= 2.5 mm Hg) being approx. 25%. Metastatic lesions do not substantially deviate from the oxygenation status of (their) primary tumors. Whereas normal tissue oxygenation is independent of the hemoglobin level over the range of 8-15 g/dL, hypoxia is more pronounced in anemic patients and above this range in some cancers. Identification of tumor hypoxia may allow an assessment of a tumor's potential to develop an aggressive phenotype or acquired treatment resistance, both of which lead to poor prognosis. Detection of hypoxia in the clinical setting may therefore be helpful in selecting high-risk patients for individual and/or more intensive treatment schedules.

摘要

本文汇总了125项研究的数据,这些研究使用计算机化的Eppendorf pO2组织血氧定量分析系统描述了临床环境中测量的预处理氧合状态。与正常组织相比,肿瘤氧合是异质性的且严重受损。缺氧是由于肿瘤内灌注和扩散不足以及贫血患者氧气运输能力降低所致。肿瘤缺氧的发生与一系列相关的肿瘤特征(如临床大小、分期﹑组织学和分级)以及各种患者人口统计学特征无关。子宫颈癌、头颈癌和乳腺癌的总体中位pO2为10 mmHg,总体缺氧分数(pO2≤2.5 mmHg)约为25%。转移灶的氧合状态与原发肿瘤基本无差异。正常组织氧合在8-15 g/dL的血红蛋白水平范围内与血红蛋白水平无关,而在贫血患者中缺氧更为明显,在某些癌症中超过此范围时也是如此。识别肿瘤缺氧可能有助于评估肿瘤发展为侵袭性表型或获得性治疗耐药性的可能性,这两者都会导致预后不良。因此,在临床环境中检测缺氧可能有助于选择高危患者进行个体化和/或更强化的治疗方案。

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