Secreted cyclophilin A mediates G1/S phase transition of cholangiocarcinoma cells via CD147/ERK1/2 pathway.

[cholangiocarcinoma]

Cyclophilin A (CypA ) was shown to be upregulated in human cholangiocarcinoma (CCA ) tissues . Suppression of intracellular CypA (inCypA ) significantly reduces cell proliferation in vitro and tumor growth in nude mice . In the present study , the effect and potential mechanism of secreted CypA (sCypA ) on cell proliferation of CCA cell lines were further investigated . CCA cells were treated with sCypA-containing conditioned media (CM ) or with purified recombinant human CypA (rhCypA ). Cell proliferation , cell cycle , ERK 1 /2 , p 38 MAPK , NF-κB , and STAT 3 activities were examined by MTS assay , flow cytometry , and Western blot . sCypA was detected in CM from MMNK 1 (an immortalized human cholangiocyte cell line ) and six CCA cell lines . The sCypA levels corresponded to the inCypA levels indicating the intracellular origin of sCypA . Both sCypA-containing CM and rhCypA significantly increased proliferation of CCA cells . CD 14 7 depletion by shRNA-knockdown or neutralizing with a CD 14 7 -monoclonal antibody significantly reduced sCypA-, and rhCypA-mediated cell proliferation . Upon rhCypA treatment , ERK 1 /2 was rapidly phosphorylated ; whereas neutralizing CD 14 7 inhibited ERK 1 /2 phosphorylation . Cell cycle analysis showed a significant increase in S phase and decrease in G 1 population in rhCypA-treated cells . The expression levels of cyclin D 1 and phosphorylated-retinoblastoma protein in the rhCypA-treated cells were increased compared with those in the non-treated control cells . p 38 MAPK pathway was shown to be suppressed in siCypA-treated cells . In summary , CypA is secreted from CCA cells and enhances cell proliferation in an autocrine /paracrine manner , at least via direct binding with CD 14 7 , which may activate the ERK 1 /2 and p 38 MAPK signaling pathways .