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. 2017 Apr 13;13(6):5009–5015. doi: 10.3892/ol.2017.6033

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Figure 2. — Effects of miR-10b on proliferation, migration and invasion of cervical cancer cells. (A) Expression levels of miR-10b in SiHa cells transfected with miR-10b mimics or NC, and HeLa cells transfected with miR-10b inhibitor or NC inhibitor. (B) miR-10b mimics inhibited proliferation of SiHa cells, and miR-10b inhibitor prompted proliferation of HeLa cells. (C) Migration and invasion assays demonstrated that numbers of migrated and invaded SiHa cells transfected with miR-10b mimic were lower compared with cells transfected with NC. Numbers of migrated and invaded HeLa cells transfected with miR-10b inhibitor were higher than cells transfected with NC inhibitor (magnification, ×200). *P<0.05. miR-10b, microRNA-10b; NC, negative control.

Figure 2. — Effects of miR-10b on proliferation, migration and invasion of cervical cancer cells. (A) Expression levels of miR-10b in SiHa cells transfected with miR-10b mimics or NC, and HeLa cells transfected with miR-10b inhibitor or NC inhibitor. (B) miR-10b mimics inhibited proliferation of SiHa cells, and miR-10b inhibitor prompted proliferation of HeLa cells. (C) Migration and invasion assays demonstrated that numbers of migrated and invaded SiHa cells transfected with miR-10b mimic were lower compared with cells transfected with NC. Numbers of migrated and invaded HeLa cells transfected with miR-10b inhibitor were higher than cells transfected with NC inhibitor (magnification, ×200). *P<0.05. miR-10b, microRNA-10b; NC, negative control.