Abstract
BackgroundDDP-based chemotherapy is one of the first-line treatment in GC. However, the therapeutic efficacy of DDP is limited due to side effects. Therefore, it is of great significance to develop novel adjuvants to synergize with DDP. We had demonstrated previously that rMV-Hu191 had antitumor activity in GC. Here we examined the synergism of rMV-Hu191 with DDP in vitro and in vivo.MethodsCellular proliferation, the synergistic effect and cell apoptosis were evaluated by CCK-8 assay, ZIP analysis and flow cytometry, respectively. The protein levels and location of ASMase were monitored by western blot and immunofluorescence assay. shRNA and imipramine were used to regulate the expression and activity of ASMase. MβCD was administrated to disrupt lipid rafts. Mice bearing GC xenografts were used to confirm the synergism in vivo.ResultsFrom our data, combinational therapy demonstrated synergistic cytotoxicity both in resistant GC cell lines from a Chinese patient and drug-nonresistant GC cell lines, and increased cell apoptosis, instead of viral replication. Integrity of lipid rafts and ASMase were required for rMV-Hu191- and combination-induced apoptosis. The ASMase was delivered to the lipid raft microdomains at the initial stage of rMV-Hu191 treatment. In vivo GC mice xenografts confirmed the synergism of combinational treatment, together with increased apoptosis and trivial side-effects.ConclusionsThis is the first study to demonstrate that rMV-Hu191 combined with DDP could be used as a potential therapeutic strategy in GC treatment and the ASMase and the integrity of lipid rafts are required for the synergistic effects.
Highlights
Gastric cancer (GC) is the fifth most common malignancy worldwide, and its overall mortality rate is the third highest in all types of cancers [1, 2]
Zero interaction potency (ZIP) analysis confirmed that the interaction between rMV-Hu191 and DDP was almost universally synergistic over all the dose–response matrix in GC cells (Fig. 1b)
For BGC-823 cells, the strongest synergistic effect was found within the region of dose combinations (MOI = 0.1 and DDP = 0.6 μM) with average ZIP
Summary
Gastric cancer (GC) is the fifth most common malignancy worldwide, and its overall mortality rate is the third highest in all types of cancers [1, 2]. The therapeutic efficacy of DDP treatment to GC patients is limited due to the toxicity induced by the relatively high dose applied in conventional chemotherapy, as well as the frequent development of drug resistance [5, 6]. Previous studies showed that combinational treatment with oncolytic measles vaccine viruses enhanced killing of therapy-induced senescent tumor cells including hepatoma, pancreatic cancer, and mammary gland carcinoma with chemotherapeutics including gemcitabine, doxorubicin, and paclitaxel [18]. Integrity of lipid rafts and ASMase were required for rMV-Hu191- and combination-induced apoptosis. In vivo GC mice xenografts confirmed the synergism of combinational treatment, together with increased apoptosis and trivial side-effects. Conclusions This is the first study to demonstrate that rMV-Hu191 combined with DDP could be used as a potential therapeutic strategy in GC treatment and the ASMase and the integrity of lipid rafts are required for the synergistic effects
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
