Koukourakis Michael I, Giatromanolaki Alexandra, Sivridis Efthimios, Simopoulos Constantinos, Turley Helen, Talks Kate, Gatter Kevin C, Harris Adrian L
Department of Radiotherapy/Oncology, Democritus University of Thrace, Alexandroupolis, Greece.
Int J Radiat Oncol Biol Phys. 2002 Aug 1;53(5):1192-202. doi: 10.1016/s0360-3016(02)02848-1.
Hypoxia-inducible factors HIF1alpha and HIF2alpha (HIFalphas) regulate the expression of a variety of genes encoding proteins related to angiogenesis and to anaerobic metabolism of cells exposed to hypoxic stress. Their putative role as markers of clinically relevant hypoxia and, therefore, as predictors of response to chemoradiotherapy is herein examined.
Using immunohistochemistry, we assessed the expression of HIFalphas in normal head-neck mucosa and in 75 cancer specimens from patients with locally advanced squamous cell head-and-neck cancer (SCHNC), treated with concurrent carboplatin chemoradiotherapy.
Head-and-neck mucosa from normal individuals did not show any HIF1alpha or HIF2alpha reactivity. SCHNC showed a varying expression of HIFalphas ranging through negative reactivity, to weak or focally strong cytoplasmic reactivity, or to strong diffuse cytoplasmic/nuclear reactivity. Fifty-two percent and 33% of cancer samples showed the latter expression pattern for HIF1alpha and HIF2alpha, respectively, and were considered to bear "high" HIF reactivity. Bone/cartilage involvement was more frequent in tumors with high HIF1alpha expression (p = 0.05). HIF1alpha and HIF2alpha overexpression were significantly associated with high microvessel density (p = 0.002 and 0.02, respectively) and with VEGF expression (p = 0.01 and 0.005, respectively). HIF1alpha was related to high thymidine phosphorylase expression (p = 0.03), whereas VEGF/KDR-activated tumor vasculature was significantly more frequent in HIF2alpha-overexpressing tumors (p = 0.02). High HIF1alpha and HIF2alpha were associated with incomplete response to chemoradiation (p = 0.007 and p = 0.02, respectively). In univariate analysis, high HIF1alpha and HIF2alpha expression were significantly associated with poor local relapse-free survival (p = 0.003 and 0.003, respectively) and with poor overall survival (p = 0.05 and 0.001, respectively). In multivariate models, HIF2alpha expression was an independent prognostic factor. In biopsies performed after the delivery of 20 Gy of radiotherapy, upregulation of HIFalphas was noted in some cases.
It is concluded that the overexpression of HIFalphas in SCHNC is related to locally aggressive behavior, to intensification of angiogenesis, and to an important resistance to carboplatin chemoradiotherapy.
缺氧诱导因子HIF1α和HIF2α(HIFαs)可调节多种基因的表达,这些基因编码与血管生成以及暴露于缺氧应激的细胞无氧代谢相关的蛋白质。本文研究了它们作为临床相关缺氧标志物的假定作用,以及作为放化疗反应预测指标的作用。
我们采用免疫组织化学方法,评估了HIFαs在正常头颈黏膜以及75例局部晚期头颈鳞状细胞癌(SCHNC)患者癌组织标本中的表达,这些患者接受了卡铂同步放化疗。
正常个体的头颈黏膜未显示任何HIF1α或HIF2α反应性。SCHNC中HIFαs的表达各不相同,范围从无反应性,到弱或局灶性强的细胞质反应性,或强弥漫性细胞质/核反应性。分别有52%和33%的癌样本显示HIF1α和HIF2α呈后一种表达模式,被认为具有“高”HIF反应性。HIF1α高表达的肿瘤中骨/软骨受累更为常见(p = 0.05)。HIF1α和HIF2α的过表达分别与高微血管密度(p = 0.002和0.02)以及VEGF表达(p = 0.01和0.005)显著相关。HIF1α与高胸苷磷酸化酶表达相关(p = 0.03),而VEGF/KDR激活的肿瘤血管在HIF2α过表达的肿瘤中显著更常见(p = 0.02)。HIF1α和HIF2α高表达与放化疗反应不完全相关(分别为p = 0.007和p = 0.02)。在单因素分析中,HIF1α和HIF2α高表达分别与较差的局部无复发生存率(分别为p = 0.003和0.003)以及较差的总生存率(分别为p = 0.05和0.001)显著相关。在多变量模型中,HIF2α表达是一个独立的预后因素。在放疗20 Gy后进行的活检中,部分病例出现了HIFαs上调。
得出结论,SCHNC中HIFαs的过表达与局部侵袭性行为、血管生成增强以及对卡铂放化疗的重要抗性相关。
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