Long non-coding RNA EGOT is associated with <sup>131</sup>iodine sensitivity and contributes to thyroid cancer progression by targeting miR-641/PTEN axis

Ming Wang; Zhengchao Wei; Shuang Wang; Wenjuan Feng; Lihua Shang; Xiaosong Sun

doi:doi:10.18632/aging.205284

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Research Paper Volume 15, Issue 22 pp 13542—13557

Long non-coding RNA EGOT is associated with ¹³¹iodine sensitivity and contributes to thyroid cancer progression by targeting miR-641/PTEN axis

Figure 6. EGOT regulates viability, apoptosis and DNA damage of 131I-resistant TC cells by targeting miR-641/PTEN axis. (A–E) The ¹³¹I -resistant TPC-1 and FTC-133 cells were treated with EGOT overexpression vectors, or co-treated with EGOT overexpression vectors and PTEN siRNA or miR-641 mimic. (A, B) CCK-8 analysis of cell viabilities. (C, D) Flow cytometry analysis of cell apoptosis in the cells. (E, F) Western blot analysis of γ-H2AX expression in the cells. mean ± SD, ** P < 0.01. Experiments were repeated at least biological triplicates.

Research Paper Volume 15, Issue 22 pp 13542—13557

Long non-coding RNA EGOT is associated with 131iodine sensitivity and contributes to thyroid cancer progression by targeting miR-641/PTEN axis

Long non-coding RNA EGOT is associated with ¹³¹iodine sensitivity and contributes to thyroid cancer progression by targeting miR-641/PTEN axis