All of the 96 paired human GC tissues and matched NAT samples were obtained from patients who underwent radical resection of GC at The First Hospital of China Medical University between May 2009 and July 2010. The median age of the 96 patients with GC was 62 years (range, 30-81 years), with 70 males accounting for 72.9% and 26 females accounting for 27.1% of the cohort. Furthermore, 77 patients (80.2%) had lymph node metastasis (pN1-N3) and all of the 96 patients completed follow-up. The matched NAT samples were collected from tissues that were located ≥5 cm from the edge of the tumor. All of the samples were frozen immediately in liquid nitrogen and stored at −80°C until use. Two pathologists from The First Hospital of China Medical University (Shenyang, China) histopathologically confirmed each sample taken for diagnosis of GC. In addition, there was no radiotherapy or chemotherapy prior to resection. The histological grade of the samples was staged by following the standards set by the World Health Organization (14). The tumor stage was also evaluated on the basis of the 7th edition of the Tumor-Node-Metastasis (TNM) staging system (15). Overall survival (OS) was defined as the interval between the date of surgery and the date of mortality or the last follow-up examination. Disease-free survival (DFS) was defined as the interval between the date of surgery and the date of recovery from disease or the last follow-up examination.

The present study was performed according to the principles expressed in The Declaration of Helsinki. Tissue samples were collected once written informed consent was obtained from all 96 patients, and following institutional ethical guidelines that were reviewed and approved by the Research Ethics Committee of China Medical University (Shenyang, China).

According to the manufacturer's protocols, total RNA was isolated from frozen specimens of tumor and NATs using TRIzol^® (Invitrogen; Thermo Fisher Scientific, Inc., Waltham, MA, USA). The purity of the total RNA was verified by ultraviolet (UV) spectrophotometry (2.0>A260/A280>1.8) using a NanoPhotometer UV/Vis spectrophotometer (Implen GmbH, Münich, Germany). Using a PrimeScript RT reagent kit (Takara Biotechnology Co., Ltd., Dalian, China), RNA was reverse transcribed into cDNA for qPCR according to the manufacturer's protocol. For qPCR, according to the manufacturer's protocol, the 25 µl final volume contained 12.5 µl 2× SYBR^® Premix Ex Taq™ (Takara Biotechnology Co., Ltd.), 0.5 µl forward and reverse primers each (10 µM), 9.5 µl nuclease-free water, and 2 µl diluted of the reverse transcribed product The primers (Sangon Biotech Co., Ltd., Shanghai, China) used in the present study were as follows: GAPDH forward, 5′-CGGATTTGGTCGTATTGGG-3′ and reverse, 5′-CTGGAAGATGGTGATGGGATT-3′; AB007962 forward, 5′-TGTGCTCACGATGTTGAATG-3′ and reverse, 5′-AATGGAAATGGGACATGGAC-3′. The reaction was incubated in a 96-well optical plate and amplified for: 1 cycle of 95°C for 30 sec; and 45 cycles of 95°C for 5 sec and 60°C for 30 sec. Relative expression of AB007962 was normalized to GAPDH and calculated using the 2^−ΔΔCq method (16). ∆C_q is the difference in the C_q value between the target and endogenous reference (∆C_q=C_{q lncRNA}-C_{q GAPDH}). ∆∆C_q is the difference in ∆C_q values between the tumor cells and the control (∆∆C_q=∆C_{q tumor lncRNA}-∆C_{q NATs lncRNA}).

The expression of AB007962 in human gastric specimens was analyzed using publicly available TCGA Illumina RNA-Seq datasets (http://cancergenome.nih.gov) of 274 patients with GC, including their clinical parameters and follow-up data. The present study used the reads per kilobase of exon per million reads mapped (RPKM) value to represent the expression levels of AB007962 for each patient from TCGA datasets (17). Amongst these, matched tumor and non-tumor specimens were available for 29 patients with GC.

Statistical analysis was performed using the SPSS 21.0 software package (IBM Corp., Armonk, NY, USA). A paired Student's t-test was used to evaluate the difference in AB007962 expression between tumor tissues and NATs and the expression levels from TCGA datasets between groups were calculated by a nonparametric test (Wilcoxon test). The association between AB007962 expression and clinicopathological factors was analyzed using the Mann-Whitney U test for two groups and the Kruskal-Wallis test for three or more groups. Survival curves were evaluated by the Kaplan-Meier method and the log-rank test was used to determine whether there was a statistically significant difference between survival curves. Cox proportional hazards analysis was performed to calculate the hazard ratio (HR) and the 95% confidence interval (CI) to estimate the association between AB007962 expression level and OS and DFS survival time. P<0.05 was considered to indicate a statistically significant difference.

The expression level of AB007962 in 96 paired cancerous and matched NATs was examined by RT-qPCR. The results demonstrated that AB007962 expression levels were reduced in cancerous tissues, compared with matched NATs (paired Student's t-test; P<0.05; Fig. 1). Furthermore, the AB007962 expression levels in 58/96 (60.4%) GC tissues were downregulated, compared with matched NATs. The AB007962 relative gene expression were further analyzed in patients with GC from the TCGA gene expression datasets, and the results demonstrated that there was no statistical differences of AB007962 expression in cancerous tissues, compared with NATs [read per kilobase of transcript per million mapped reads (RPKM)_GC, 0.379±0.078; RPKM_NATs, 0.400±0.095; Wilcoxon test, P=0.633].

The association between the expression level of AB007962 and clinicopathological factors in 96 patients with GC was investigated, including sex, age, tumor size, tumor location, macroscopic type, histological grade and TNM stage. No significant associations were identified between AB007962, and sex (P=0.154), age (P=0.772), tumor location (P=0.515), tumor size (P=0.078) macroscopic type (P=0.241), histological differentiation (P=0.492), pathological (p)T stage (P=0.756), pN stage (P=0.070), pTNM stage (P=0.978) or invasion into the lymphatic vessels (P=0.820). Furthermore, through the use of TCGA gene expression datasets, no significant associations were identified between AB007962 expression and clinicopathological factors, including sex (P=0.726), Lauren type (P=0.152), histological differentiation (P=0.532), pT stage (P=0.250), pN stage (P=0.472) or pTNM stage (P=0.092).

In order to investigate whether the expression level of AB007962 was associated with the prognosis of the 96 patients with GC, survival data on the patients following gastrectomy was collected. The median ratio of relative AB007962 expression in the 96 patients with GC was used as the cut-off value to divide the 96 patients into groups with high and low AB007962 expression. Kaplan-Meier analysis and the log-rank test were used to evaluate the association between AB007962 expression, and OS and DFS. The results demonstrated that there was no significant difference in OS (P=0.147; Fig. 2A) or DFS (P=0.370; Fig. 2B) between the two groups.

However, among 28 patients with intestinal-type GC, those with increased AB007962 expression had significantly increased OS (P=0.006; Fig. 2C) and DFS (P=0.004; Fig. 2D) compared with the reduced expression group. The univariate survival analysis for OS and DFS indicated that AB007962 expression (P=0.016) and tumor location (P=0.026) were prognostic factors for OS, and AB007962 expression (P=0.015) and tumor size (P=0.033) were significant prognostic factors for DFS (Table I). P<0.05 was considered to indicate a statistically significant difference for multivariate Cox analysis, and the multivariate analysis confirmed that AB007962 expression levels were retained as an independent prognostic indicator for OS (HR=6.185; 95% CI, 1.331-28.732; P=0.020) and DFS (HR=7.982; 95% CI, 1.638-38.894; P=0.010) (Table II) of patients with intestinal-type GC.

Nevertheless, from TCGA gene expression datasets, no significant association was identified between AB007962 expression, and the OS and DFS of patients with intestinal-type GC.