As neoplastic progression leading to the development of the tumorigenic phenotype is driven by molecular alterations, the analysis of these molecular features could contribute to the prediction of the
tumorigenic potential of cell substrates that evolve by Doxorubicin chemical structure spontaneous neoplastic development during cell culture. MicroRNAs are short RNA molecules that have been shown to be important regulators of biological functions [38]. Aberrations in miRNA expression can affect important cellular processes like the cell cycle, cell proliferation, or cell death by apoptosis [39]. These processes are known to be involved in neoplastic development and hence provide a direct link to tumor initiation and progression. The use of tissue miRNA expression profiles as diagnostic or prognostic biomarkers in cancer has been demonstrated by several studies [24] and [40]. We have shown that specific miRNA signatures were identified that correlated with the transition of VERO cells from a non-tumorigenic phenotype (low-passage cells, p148) to a tumorigenic phenotype (high-passage cells, p256) during serial tissue-culture passage [28]. We also demonstrated that the signature miRNAs identified see more in VERO cells grown
in FBS were the same as in the VERO cells adapted to grow in serum-free ALOX15 medium (SF-VERO). In the present study, we used quantitative RT-PCR to evaluate our initial observation that miRNA expression changes with the progress of neoplastic development of VERO cells during intervening passages. Compared with pAGMK cells, the expression levels of these signature miRNAs progressively increased in cells from LD 10–87 VERO cell banks established at every 10 passages from p151 to p256. Notably, the expression of these miRNAs peaked at p194 in LD 10–87 VERO cells. The correlation of the six selected miRNAs for the
tumorigenic phenotype of VERO cells was verified by assessing another independently-derived 10–87 VERO cell line that was developed by HD passaging. The trend in the expression of signature miRNAs was generally similar between the LD 10–87 VERO cell set and the HD 10–87 VERO cell set. Moreover, the over-expression of these miRNAs was also evident in another VERO cell line, A4497 VERO cells, that was also derived independently and has been shown to be tumorigenic in newborn and adult nude mice [10]. Similar to our previous report [28], the increased rate of migration of HD 10–87 VERO cells correlated with their capacity to form tumors in nude mice. The transition of non-tumorigenic phenotype to tumorigenic phenotype appeared to occur around p185 in 10–87 HD VERO cells and around p194 in LD 10–87 VERO cells.