Hoffmann Andreas-Claudius, Mori Ryutaro, Vallbohmer Daniel, Brabender Jan, Klein Ellen, Drebber Uta, Baldus Stephan E, Cooc Janine, Azuma Mizutomo, Metzger Ralf, Hoelscher Arnulf H, Danenberg Kathleen D, Prenzel Klaus L, Danenberg Peter V
Department of Biochemistry and Molecular Biology and Norris Comprehensive Cancer Center, University of Southern California, Los Angeles, CA 90033, USA.
Neoplasia. 2008 Jul;10(7):674-9. doi: 10.1593/neo.08292.
Pancreatic cancer still has one of the worst prognoses in gastrointestinal cancers with a 5-year survival rate of 5%, making it necessary to find markers or gene sets that would further classify patients into different risk categories and thus allow more individually adapted multimodality treatment regimens. In this study, we investigated the prognostic values of HIF1a, bFGF, VEGF, and PDGFA gene expressions as well as their interrelationships.
Formalin-fixed paraffin-embedded tissue samples were obtained from 41 patients with pancreatic adenocarcinoma (age, 65; range, 34-85 years). After laser capture microdissection, direct quantitative real-time reverse transcription-polymerase chain reaction assays were performed in triplicates to determine HIF1a, PDGFA, VEGF, and bFGF gene expression levels. Multivariate Cox proportional hazards regression analysis was used to assess the impact of HIF1a gene expression on prognosis.
HIF1a was significantly correlated to every gene we tested: bFGF (P = .04), VEGF (P = .02), and PDGFA (P = .03). Tumor size, P = .04, and high HIF1a mRNA expression (cutoff, 75th percentile) had a significant impact on survival, P = .009 (overall model fit, P = .02). High HIF1a expression had a sensitivity of 87.1% and a specificity of 55.6% for the diagnosis short (<6 months) versus long (6-60 months) survival.
Measuring PDGFA, bFGF, and HIF1a expression may contribute to a better understanding of the prognosis of patients with pancreatic cancer and may even play a crucial role for the distribution of patients to multimodal therapeutic regimens. Larger studies including patients treated with actual chemotherapeutics seem to be warranted.
胰腺癌仍是胃肠道癌症中预后最差的癌症之一,5年生存率仅为5%,因此有必要寻找能够将患者进一步分为不同风险类别的标志物或基因集,从而制定更具个性化的多模式治疗方案。在本研究中,我们调查了HIF1a、bFGF、VEGF和PDGFA基因表达的预后价值及其相互关系。
从41例胰腺腺癌患者(年龄65岁;范围34 - 85岁)获取福尔马林固定石蜡包埋组织样本。经过激光捕获显微切割后,进行三次重复的直接定量实时逆转录 - 聚合酶链反应测定,以确定HIF1a、PDGFA、VEGF和bFGF基因表达水平。采用多变量Cox比例风险回归分析评估HIF1a基因表达对预后的影响。
HIF1a与我们检测的每个基因均显著相关:bFGF(P = .04)、VEGF(P = .02)和PDGFA(P = .03)。肿瘤大小(P = .04)和高HIF1a mRNA表达(临界值为第75百分位数)对生存率有显著影响(P = .009;总体模型拟合,P = .02)。高HIF1a表达对诊断短期(<6个月)与长期(6 - 60个月)生存的敏感性为87.1%,特异性为55.6%。
检测PDGFA、bFGF和HIF1a表达可能有助于更好地了解胰腺癌患者的预后,甚至可能在将患者分配至多模式治疗方案中发挥关键作用。似乎有必要开展包括接受实际化疗患者的更大规模研究。