Overexpressed HDAC4 is associated with poor survival and promotes tumor progression in esophageal carcinoma

Li-Si Zeng; Xian-Zi Yang; Yue-Feng Wen; Shi-Juan Mai; Meng-He Wang; Mei-Yin Zhang; X.F. Steven Zheng; Hui-Yun Wang

doi:doi:10.18632/aging.100980

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Research Paper Volume 8, Issue 6 pp 1236—1248

Overexpressed HDAC4 is associated with poor survival and promotes tumor progression in esophageal carcinoma

Figure 4. Down-regulation of HDAC4 inhibits the migration of EC cells. (A) Knockdown of HDAC4 reduces migration of KYSE30 and EC/CUHK1 cells. EC cells were transiently transfected with HDAC4 siRNA or a control siRNA. The number of migrated cells is decreased in cells (x100 magnification) transfected with HDAC4 siRNAs compared with those transfected with a control siRNA. Wound healing assay demonstrates that down-regulation of HDAC4 inhibits cell migration at 12 h and 24 h in (B) KYSE30 and (C) EC/CUHK1 cells (magnification, x100). (D) Western blot analysis indicates that knockdown of HDAC4 increases the expression of E-cadherin and α-catenin, and decreases the expression of Vimentin.