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直肠癌新辅助短期放疗后的Wnt信号传导与细胞凋亡

Wnt-signaling and apoptosis after neoadjuvant short-term radiotherapy for rectal cancer.

作者信息

Gassler Nikolaus, Herr Ingrid, Keith Martina, Autschbach Frank, Schmitz-Winnenthal Hubertus, Ulrich Alexis, Otto Herwart F, Kartenbeck Jürgen, Z'graggen Kaspar

机构信息

Department of Pathology, University of Heidelberg, Heidelberg, Germany.

出版信息

Int J Oncol. 2004 Dec;25(6):1543-9.

PMID:15547689
Abstract

Recent surgical concepts for primary rectal cancer include the combination of surgery and short-term neoadjuvant radiotherapy (STNR). This is usually given in a dose of 25 Gy over five days in order to reduce local recurrence rates. Clinical studies have shown that local recurrence is found in some patients despite STNR. We identified molecular patterns of the Wnt- and apoptosis pathways as well as expression of junction-associated molecules in rectal cancer specimens of patients who received STNR and in those who did not. Expression patterns were examined by immunohistochemistry and molecular techniques such as LightCycler RT-PCR and Western blot analysis in 25 sporadic rectal adenocarcinoma specimens derived from STNR-patients or non-pretreated donors, respectively. The molecular pattern in response to STNR was heterogeneous and was reflected by responders who show activation of apoptosis and cellular remodeling, whereas the group of non-responders from STNR did not show such reaction and was very similar to untreated controls. Enhanced expression of beta-catenin was generally mediated by STNR, but exclusively in the responder group impaired expression of c-Myc and junction-associated molecules as well as cleavage of poly-ADP-ribose polymerase and of the caspase substrate cytokeratin 19 were found. The molecular profile suggests that STNR interferes with Wnt-signaling and c-Myc expression. STNR in its present form is not suitable to fully complete the sequence of apoptosis in all rectal adenocarcinomas.

摘要

原发性直肠癌的最新手术理念包括手术与短期新辅助放疗(STNR)相结合。通常在五天内给予25 Gy的剂量,以降低局部复发率。临床研究表明,尽管进行了STNR,但仍有一些患者出现局部复发。我们确定了接受STNR和未接受STNR的患者直肠癌标本中Wnt和凋亡途径的分子模式以及连接相关分子的表达。分别通过免疫组织化学和分子技术,如LightCycler RT-PCR和蛋白质印迹分析,检测了25例源自接受STNR治疗的患者或未接受预处理供体的散发性直肠腺癌标本中的表达模式。对STNR的分子反应模式是异质性的,表现为显示凋亡激活和细胞重塑的反应者,而来自STNR的无反应者组未显示出这种反应,并且与未治疗的对照组非常相似。β-连环蛋白的表达增强通常由STNR介导,但仅在反应者组中发现c-Myc和连接相关分子的表达受损,以及聚ADP-核糖聚合酶和半胱天冬酶底物细胞角蛋白19的裂解。分子谱表明,STNR干扰Wnt信号传导和c-Myc表达。目前形式的STNR并不适合在所有直肠腺癌中完全完成凋亡序列。

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