Differential expression of IGF-1 mRNA isoforms in colorectal carcinoma and normal colon tissue

Kasprzak,Aldona; Szaflarski,Witold; Szmeja,Jacek; Andrzejewska,Małgorzata; Przybyszewska,Wiesława; Kaczmarek,Elżbieta; Koczorowska,Maria; Kościński,Tomasz; Zabel,Maciej; Drews,Michał

doi:10.3892/ijo.2012.1706

Differential expression of IGF-1 mRNA isoforms in colorectal carcinoma and normal colon tissue

Authors:
- Aldona Kasprzak
- Witold Szaflarski
- Jacek Szmeja
- Małgorzata Andrzejewska
- Wiesława Przybyszewska
- Elżbieta Kaczmarek
- Maria Koczorowska
- Tomasz Kościński
- Maciej Zabel
- Michał Drews
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Affiliations: Department of Histology and Embryology, Poznan University of Medical Sciences, Poznań, Poland, Department of Histology and Embryology, Poznan University of Medical Sciences, Poznań, Poland, Department of General, Gastroenterological and Endocrinological Surgery, Poznan University of Medical Sciences, Poznań, Poland, Department of Bioinformatics and Computational Biology, Chair of Pathology, Poznan University of Medical Sciences, Poznań, Poland, Department of Molecular Virology, Adam Mickiewicz University, Poznań, Poland
Published online on: November 19, 2012 https://doi.org/10.3892/ijo.2012.1706
Pages: 305-316

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Abstract

The insulin-like growth factor (IGF)-1 gene consists of 6 exons resulting in the expression of 6 variant forms of mRNA (IA, IB, IC, IIA, IIB and IIC) due to an alternative splicing. The mechanisms of IGF-1 gene splicing and the role of local expression manifested by IGF-1 mRNA variants in colorectal carcinoma (CRC) have not been extensively investigated. Therefore, the aim of our study was to analyse the expression of IGF-1 mRNA isoforms [A, B, C, P1 (class I) and P2 (class II)], as well as the protein expression in CRC and control samples isolated from 28 patients. The expression of Ki-67 was also analysed and clinical data were obtained. For this purpose, we used quantitative real-time PCR (qPCR) and immunocytochemistry. The expression of mRNAs coding for all splicing isoforms of IGF-1 was observed in every tissue sample studied, with a significantly lower expression noted in the CRC as compared to the control samples. The cytoplasmic expression of IGF-1 protein was found in 50% of the CRC and in ~40% of the non-tumor tissues; however, no significant quantitative inter-group differences were observed. The expression of the IGF-1 gene in the 2 groups of tissues was controlled by the P1 and P2 promoters in a similar manner. No significant differences were detected in the expression of the IGF-1 A and B isoforms; however, their expression was significantly higher compared to that of isoform C. No significant differences were observed between the expression of Ki-67 mRNA in the CRC and control tissue even though the expression of the Ki-67 protein was higher in the CRC compared to the control samples. Ki-67 protein expression was associated with the macroscopic and microscopic aspects of CRC. A significant positive correlation was found between the local production of total mRNA and isoform A and the expression of Ki-67 mRNA, although only in the non-tumor tissues. In CRC samples, the local expression of the total IGF-1 mRNA and all splicing isoforms of IGF-1 mRNA decreased as compared to the normal colon tissues, although however, with conservation of both gene promoter activities and with the continued principal splicing IGF-1 mRNA isoforms.