Haase Michael, Gmach Christine C, Eke Iris, Hehlgans Stephanie, Baretton Gustavo B, Cordes Nils
OncoRay-Center for Radiation Research in Oncology, Medical Faculty Carl Gustav Carus, Dresden University of Technology, Fetscherstrasse 74/PF 86, 01307 Dresden, Germany.
J Histochem Cytochem. 2008 Sep;56(9):819-29. doi: 10.1369/jhc.2008.951095. Epub 2008 May 27.
Integrin-linked kinase (ILK), a mediator of beta integrin signals, has emerged as a therapeutic target in malignant tumors. Because malignant transformation is accompanied by dedifferentiation, ILK expression was evaluated in diverse normal and tumor tissue samples with regard to tissue differentiation. In single sections and in a tissue microarray (323 tumor tissues, 181 normal tissues), immunohistochemistry was performed [ILK, Akt, phospho-Akt-S473, loricrin, transforming growth factor beta2 (TGFbeta2)], and staining intensities were semiquantitatively scored. Increased ILK expression was clearly associated with increased differentiation in normal gastrointestinal, neural, bone marrow, renal tissue, and in more differentiated areas of malignant tumors. ILK colocalized with its putative downstream target Akt and with loricrin or TGFbeta2. Our findings clearly show that elevated levels of ILK are associated with cellular differentiation in high turnover tissues but not generally with a malignant phenotype. Our study indicates that ILK is not a general molecular target for cancer therapy but rather an indicator of differentiation. This manuscript contains online supplemental material at http://www.jhc.org. Please visit this article online to view these materials.
整合素连接激酶(ILK)是β整合素信号的介导因子,已成为恶性肿瘤的治疗靶点。由于恶性转化伴随着去分化,因此针对组织分化情况,在多种正常和肿瘤组织样本中评估了ILK的表达。在单张切片和组织芯片(323个肿瘤组织、181个正常组织)中进行了免疫组织化学检测[ILK、Akt、磷酸化Akt-S473、loricrin、转化生长因子β2(TGFβ2)],并对染色强度进行了半定量评分。在正常胃肠道、神经、骨髓、肾组织以及恶性肿瘤的高分化区域中,ILK表达增加明显与分化增加相关。ILK与其假定的下游靶点Akt以及loricrin或TGFβ2共定位。我们的研究结果清楚地表明,ILK水平升高与高代谢组织中的细胞分化相关,但一般与恶性表型无关。我们的研究表明,ILK不是癌症治疗的通用分子靶点,而是分化的一个指标。本文包含在线补充材料,网址为http://www.jhc.org。请在线访问本文以查看这些材料。
