PREDICTING RESPONSE TO THERAPY: DETECTION OF ORAL CANCER

预测治疗反应：口腔癌的检测

• 批准号: 6523882
• 负责人: THOMAS E. CAREY
• 金额: $ 39.11万
• 依托单位: UNIVERSITY OF MICHIGAN AT ANN ARBOR
• 依托单位国家: 美国
• 财政年份: 1999
• 资助国家: 美国
• 起止时间: 1999-09-30 至 2004-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6523882
• 关键词: antibody; apoptosis; cis platinum compound; clinical research; gene expression; genetic markers; head /neck neoplasm; human subject; human therapy evaluation; neoplasm /cancer chemotherapy; neoplasm /cancer radiation therapy; neoplasm /cancer relapse /recurrence; neoplastic cell; oral pharyngeal neoplasm; p53 gene /protein; prognosis; tissue /cell culture; tissue /organ preservation; tumor suppressor genes

A critical research goal in head and neck oncology is to define the use of chemotherapy plus radiation regimens that allow organ preservation and preserve quality of life. Progress has been limited by the failure of some tumors to respond to chemoradiation, and the lack of predictive markers for identifying those likely to respond. Furthermore, persistent or recurrent disease is often detected late when the effectiveness of salvage treatment options is limited. Oral cancer is a devastating disease for which better therapies are needed. Surgery is effective in some patients but the surgical defects can be functionally and cosmetically unacceptable and many patients recur after surgery. Thus, the development of predictive markers to select patients for appropriate therapy is needed. Our preliminary results suggest that p53 expression or mutation and expression of the apoptosis-blocking proteins, Bcl-2 and Bcl-x, interact to determine responsiveness to chemoradiation. We propose to determine in patients with oral cancers whether chemotherapy response, organ preservation and/or survival is predicted by p53 overexpression and gene mutation, and we will determine how this is influenced by the expression of Bcl-2 and Bcl-x. Our preliminary in vivo and in vitro data support the concept that tumors with mutant p53 are susceptible to cisplatin-based chemotherapy regimens but that those with wild type p53 are resistant. We will test our hypotheses in tumor samples obtained from patients before and after organ sparing therapy and we will test these hypotheses with in vitro experiments using cell lines with known p53 and Bcl-2/Bcl-x status. Specimens from patients undergoing conventional treatment will also be tested to determine how expression and mutation of these genes may influence outcome in the absence of organ sparing procedures. Furthermore, our preliminary data indicate that the presence and persistence of serum antibodies to p53 in patients with head and neck cancer is associated with poor outcome. However, we have also observed that following successful treatment the antibodies disappear and may reappear with relapse. Thus, we plan to investigate the value of antibodies to p53 as a predictive marker for persistence, recurrence, and successful therapy as well as to correlate p53 antibody data with p53 mutation data. The information developed in this work should result in new trials that employ predictive markers to select the most appropriate and effective treatment for oral cancer. This together with close monitoring for early recurrence should in turn lead to improved overall survival.

头颈部肿瘤学的一个关键研究目标是确定化疗加放疗方案的使用，以保存器官并保持生活质量。由于一些肿瘤对放化疗没有反应，以及缺乏识别那些可能有反应的肿瘤的预测标记物，进展受到限制。此外，持续性或复发性疾病往往发现较晚，此时抢救治疗方案的有效性有限。口腔癌是一种毁灭性的疾病，需要更好的治疗方法。手术对一些患者是有效的，但手术缺陷可能在功能和美容上是不可接受的，许多患者术后复发。因此，需要开发预测标记物来选择适当治疗的患者。我们的初步结果表明，p53的表达或突变与凋亡阻断蛋白Bcl-2和Bcl-x的表达相互作用，决定了对放化疗的反应性。我们建议在口腔癌患者中确定p53过表达和基因突变是否预测化疗反应、器官保存和/或生存，我们将确定Bcl-2和Bcl-x的表达如何影响这一点。我们初步的体内和体外数据支持突变型p53的肿瘤对顺铂化疗方案敏感，而野生型p53的肿瘤对顺铂化疗方案有耐药性。我们将在器官保留治疗前后从患者获得的肿瘤样本中测试我们的假设，我们将使用已知p53和Bcl-2/Bcl-x状态的细胞系进行体外实验来测试这些假设。还将对接受常规治疗的患者标本进行测试，以确定在没有器官保留手术的情况下，这些基因的表达和突变如何影响结果。此外，我们的初步数据表明，头颈癌患者血清中p53抗体的存在和持续存在与预后不良有关。然而，我们也观察到，在成功治疗后，抗体消失，并可能复发。因此，我们计划研究p53抗体作为持续性、复发和成功治疗的预测标志物的价值，并将p53抗体数据与p53突变数据相关联。在这项工作中发展的信息应该导致新的试验，使用预测标记来选择最合适和有效的口腔癌治疗方法。这与密切监测早期复发应反过来提高总生存率。