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Effects of U0126 and MK2206 on cell growth and re-growth of endometriotic stromal cells grown on substrates of varying stiffness

机译:U0126和MK2206对不同刚度基底生长的细胞生长及肝脏重新生长的影响

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Endometriosis is a common gynecological disorder responsible for infertility and pelvic pain. A complete cure for patients with endometriosis awaits new targets and strategies. Here we show that U0126 (a MEK inhibitor) and MK2206 (an AKT inhibitor) synergistically inhibit cell growth of deep endometriotic stromal cells (DES) grown on polyacrylamide gel substrates (PGS) of varying stiffness (2 or 30 kilopascal [kPa]) or plastic in vitro. No significant differences in cell proliferation were observed among DES, endometrial stromal cells of patients with endometriosis (EES) from the proliferative phase (P), EES-S (secretory phase) and EES-M (menstrual phase) compared to cells grown on a substrate of the same stiffness at both higher (U0126 [30?μM] and MK2206 [9?μM]) and lower (U0126 [15?μM] and MK2206 [4.5?μM]) combined doses. However, cell re-growth of DES after drug discontinuation was higher than that of EES-P and EES-S when cells were grown on rigid substrates at both combined doses. Combination U0126 and MK2206 treatment is more effective than each drug alone in cell growth inhibition of DES. However, further studies are required to investigate the mechanisms underlying high cell survival and proliferation after drug discontinuation for developing target therapies that prevent recurrence.
机译:子宫内膜异位症是一种常见的妇科疾病,负责不孕症和骨盆疼痛。对子宫内膜异位症患者的完全治愈等待新的目标和策略。在这里,我们表明U0126(MEK抑制剂)和MK2206(AKT抑制剂)协同抑制在不同刚度(2或30kka)的聚丙烯酰胺凝胶基材(PGS)上生长的深内静脉肌基质细胞(DES)的细胞生长塑料体外。与在A的细胞相比,在增殖相(P),EES-S(分泌阶段)和EES-M(月经阶段)的子宫内膜异位症(EES)的子宫内膜体细胞中没有观察到细胞增殖的显着差异。与在a上生长的细胞相比在较高(U0126 [30≤μm]和MK2206 [9≤μm])和更低的相同刚度的基材(U0126 [15?μm]和MK2206 [4.5μm])组合剂量。然而,当药物停止后,DES的细胞重新生长高于EES-P和EES-S,当在两个组合剂量上在刚性基板上生长细胞时,ees-P和EES-S。组合U0126和MK2206处理比单独的药物在细胞生长抑制中更有效。然而,需要进一步的研究来探讨药物停止后高细胞存活率和增殖的机制,用于制定预防复发的靶疗法。

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