Lymphangiogenesis in Gastric Cancer regulated through Akt/mTOR-VEGF-C/VEGF-D axis

Akt/mTOR signaling pathway is an important intracellular pathway, which responds to cytokine signals, and is proved to play a major role in cell growth, metabolism and apoptosis [12,13]. Akt/mTOR pathway involves in various pathological mechanisms of colorectal cancer, gastric cancer, liver cancer, breast cancer and uterine cancer etc. [12-14]. Our previous study confirmed that p-Akt involved in angiogenesis of gastric adenocarcinoma and Akt activation may contribute to angiogenesis via VEGF-A up-regulation [15]. In this study, the positive staining rates of p-Akt and p-mTOR in 55 cases of gastric cancer were 74.54% and 85.45% respectively. Besides, p-Akt was positively correlated with p-mTOR (p < 0.01). This result was consistent with previous studies and confirmed the significant role of Akt/mTOR pathway in gastric cancer. The clinical prognosis of gastric cancer is also proposed to be associated with Akt pathway and VEGF pathway. For instance, Murakami et al. suggested that the prognosis of gastric cancer patients without p-Akt expression was always better than p-Akt positive ones, and the 5-year survival rates were 68% and 35% for patients with T3 or T4 stage tumors, respectively [16]. Besides, the Akt encoding gene PI3CA of upstream protein PI3K was associated with disease-free survival [17]. In addition, Wang et al. indicated that VEGF-C, VEGF-D and LVD of gastric cancer were related to tumor size and overall survival according to a study in 123 cases [18,19]. The correlation between VEGF-C/LVD and prognosis in tumor differentiation, T stage, lymph node metastasis, and distant metastasis were also confirmed [20]. Another study further suggested using the combination of VEGF-C/-D and CA199 to predict lymphatic vessel metastasis [21].

Given that Akt/mTOR pathway and VEGF-C/-D play a vital role in lymphatic metastasis and prognosis, our study aims to explore the relationship between two pathways and further promote the mechanism of lymphangiogenesis and metastasis. According to the results of staining in situ, p-Akt and p-mTOR were positively correlated with VEGF-C and VEGF-D (p < 0.01). In terms of LVD, D2-40 level of gastric carcinoma and normal tissues were examined at the same time. LVD in gastric cancer was four times higher than that of normal tissue. Besides, LVD was significantly correlated with p-Akt, p-mTOR, VEGF-C and VEGF-D (p < 0.05). Notably, LVD as well as VEGF-C/-D was obviously lower in patients with negative expression of p-Akt and p-mTOR than positive ones. It suggested that both Akt/mTOR pathway and VEGF pathway involved in lymphangiogenesis and lymphatic vessel metastasis in gastric cancer. Similar results were also confirmed by other studies. Yu et al. suggested that p-mTOR were highly consistent with lymph node metastasis and could be an independent predictor of lymphatic metastasis and prognosis of gastric cancer [22]. Besides, Onogawa et al. indicated that VEGF-C was highly correlated with lymphatic metastasis according to a study conducted in 140 cases of early gastric cancer [23]. VEGF-C as well as VEGF-D was also regarded as a predictor of lymphatic metastasis in patients with early gastric cancer [24]. In the study, we further confirmed the relationship of Akt/mTOR, VEGF-C/-D and LVD in gastric cancer in situ.

LY294002, as an Akt activation inhibitor, is confirmed with the anti-tumor effect and promoted the apoptosis of gastric cancer in vitro and in vivo [25]. Rapamycin known as an mTOR activation inhibitor is clinically used for its anti-tumor effect and immunomodulation [26]. The results of our study further verified that LY294002 and Rapamycin could efficiently inhibit the growth of SGC-7901 cells. Besides, LY294002 at 50 μM) and Rapamycin at 100 nM had the most effective inhibition rate of (52.53 ± 3.19) % and (48.72 ± 3.06) % at 24 h. When prolonging to 72 h, the inhibition rates were (68.76 ± 1.00) % and (68.50 ± 3.77) % respectively. Then, we observed the influence of phosphorylation inhibition of Akt and mTOR on lymphatic factors, VEGF-C and VEGF-D. High concentration of LY294002 (50 μM) and Rapamycin (100 nM) were used for the intervention study. According to the results, Rapamycin suppressed the expression of p-mTOR and LY294002 efficiently inhibited the expression of p-Akt as well as p-mTOR. It is noted that both inhibitors could efficiently inhibit the expression of VEGF-C/-D. Besides, the down-regulation of p-Akt/p-mTOR showed a high consistency with that of VEGF-C/-D. Therefore, Akt/mTOR pathway was proposed to be closely related to VEGF-C/-D. The similar results were also previously reported in other tumor models. For example, Zhang et al. decreased the insulin receptor by short hairpin RNA in cancer cell lines, LCC6 and T47D. The cell proliferation, angiogenesis, lymphangiogenesis and metastasis were also inhibited due to the down-regulation of p-Akt and inactivation of VEGF-D [27]. Besides, mTOR inhibition could suppress the expression of VEGF-C and effectively reduce lymphangiogenesis in pancreatic cancer mouse model [11]. In another study, VEGF-D was degraded by Honokiol to inhibit lymphangiogenesis of lung cancer xenograft [28]. IL-6 could also regulate VEGF-C at mRNA level through Akt/mTOR signaling pathway, which effectively decreased the lymphangiogenesis and metastasis in oral squamous cell carcinoma [29].