Human umbilical cord mesenchymal stem cells promote carcinoma growth and lymph node metastasis when co-injected with esophageal carcinoma cells in nude mice.

[esophageal carcinoma]

Human umbilical cord blood derived-mesenchymal stem cells (hUCMSCs ) offer an attractive alternative to bone marrow-derived MSCs (BMMSCs ) for cell-based therapy as it is a less invasive source of biological material . However , limited studies have been conducted with hUCMSCs as compared to BMMSCs . The present study was conducted to evaluate the effects of hUCMSCs in esophageal carcinoma (EC ).hUCMSCs together with EC cells were transplanted subcutaneously into BALB /c nude mice to observe the effects of hUCMSCs on tumor establishment . hUCMSCs injected through the caudal vein to the mice with pre-established EC to observe the effects of hUCMSCs on tumor outgrowth . In order to elucidate the underlying mechanisms , we also performed in vitro experiments including directly co -culture , transwell assay , proliferation assay and western blotting analysis .hUCMSCs promoted EC formation in nude mice . In the in vivo model of pre-established EC , intravenously injected hUCMSCs potently promoted tumor growth . When in vitro co -cultured with hUCMSCs , EC cells proliferation increased . After co -cultured with hUCMSCs through transwell system , EC cells showed increased proliferation . Through transwell assay , we also observed that EC cells recruited MSCs , and MSCs promoted EC cells migration and invasion . Western blotting data showed that the expressions of proliferation related proteins Bcl-2 , survivin and metastasis related proteins MMP-2 and MMP-9 were up-regulated in the EC cells transwell co -cultured with hUCMSCs .Our results indicated that hUCMSCs could favor tumor growth in vivo and in vitro . Thus , the exploitation of hUCMSCs in new therapeutic strategies should be cautious under the malignant conditions .