JAK2 inhibitor blocks the inflammation and growth of esophageal squamous cell carcinoma in vitro through the JAK/STAT3 pathway.

[esophageal squamous cell carcinoma]

Recent research indicates that the Janus kinase /signal transducer and activator of transcription 3 (JAK /STAT 3 ) pathway may play an important role in chronic inflammation which promotes cancer progression , yet the mechanism is not clear . The present study aimed to investigate the role of the JAK /STAT 3 pathway in the growth and cancer -related inflammation (CRI ) of esophageal squamous cell carcinoma (ESCC ) by studying the crosstalk between the JAK /STAT 3 pathway and nuclear factor -κ B (NF-κB ) and cyclooxygenase-2 (COX -2 ) which are important inflammatory factors associated with tumorigenesis . Cell growth and the cell cycle were assessed by CCK -8 assays and flow cytometry , respectively . The protein levels of STAT 3 , phosphorylated STAT 3 , VEGF , NF-κB p 65 , phosphorylated NF-κB p 65 and COX -2 in ESCC cells following treatment with JAK 2 inhibitor for 48 h or interleukin-6 (IL -6 ) for 24 h were detected . RT-PCR was performed to study the interaction among STAT 3 , NF-κB and COX -2 by transfection of siRNAs targeted at STAT 3 and NF-κB . STAT 3 was activated in 3 ESCC cell lines at different levels . Blocking the JAK /STAT 3 pathway inhibited cancer growth through regulation of cell growth , cell cycle and angiogenesis . Likewise , abrogation of the JAK /STAT 3 pathway decreased CRI by downregulating levels of NF-κB p 65 phosphorylation , COX -2 and IL -6 concentration . In addition , CRI and cancer growth were accelerated by IL -6 through stimulation of the JAK /STAT 3 and NF-κB p 65 pathway . Moreover , STAT 3 and NF-κB both regulated COX -2 as a downstream gene . The JAK /STAT 3 pathway is an important pathway which links CRI and cancer growth through IL -6 and crosstalk with the NF-κB p 65 subunit and COX -2 . The STAT 3 pathway could be a novel target both for cancer treatment and prevention in ESCC .