This study retrospectively analyzed 152 surgical HCC patients treated by surgical resection from the period January 2016 to December 2019. The screening of patients was based on the following criteria: (1) those who had a pathological diagnosis of primary HCC, (2) those primarily treated by surgical resection, (3) those who had retrievable tumor and adjacent tissues that were fresh-frozen in liquid nitrogen, and (4) those whose preoperative clinical data, laboratory test data, as well as survival data were accessible and available. The following patients were omitted: (1) those who had tumor or adjacent tissue specimens were not eligible for RNA isolation due to improper preservation, (2) those who had a history of other cancers, and (3) those who had failed to follow-up within 3 months after surgery. Ethical approval was acquired from the Ethics Committee. Written informed consent was required from either the patients or their families.

All patients’ tumor and adjacent tissues (stored in liquid nitrogen) were acquired from the hospital specimen library. All samples were cryopreserved and feasible for reverse transcription-quantitative polymerase chain reaction (RT-qPCR) assay. In addition, patients’ clinical data, including basic information, tumor features, liver function indexes, and tumor markers, were also abstracted from their medical records. The CNLC stage of the patients was retrospectively assessed according to the documented tumor features (16). Moreover, overall survival (OS) time up to June 2021 was calculated on the basis of follow-up records. Apart from surgical resection, 8 patients received neoadjuvant sorafenib, 13 patients received neoadjuvant transarterial chemoembolization (TACE), and 37 patients received adjuvant treatment (such as TACE, chemotherapy, and interferon).

RT-qPCR was carried out to detect lnc-MAFG-AS1 in the tumor and adjacent tissues. The RT-qPCR procedures were implemented as described in a previous study (17), using the following kits: TRIzol™ Reagent (Invitrogen™, Carlsbad, CA, USA) for total RNA extraction; iScript™ cDNA Synthesis Kit (Bio-Rad, Hercules, CA, USA) for cDNA Synthesis; QuantiNova SYBR Green PCR Kit (Qiagen, Duesseldorf, Nordrhein-Westfalen, Germany) for qPCR. glyceraldehyde-3-phosphate dehydrogenase (GAPDH) was applied as a reference gene. The relative expression of lnc-MAFG-AS1was calculated using the 2^−ΔΔCt method. RT-qPCR was performed in triplicate. The primers were constructed according to the previous study (17): lnc-MAFG-AS1: 5′-ATGACGACCCCCAATAAAGGG-3′ (sense); 5′-CACCGACATGGTTACCAGC-3′ (antisense). GAPDH: 5′-GAAGGTGAAGGTCGGAGT-3′ (sense); 5′-GAAGATGGTGACTGGGATTT-3′ (antisense).

A comparison of lnc-MAFG-AS1 expression was done by using the Wilcoxon matched-pairs signed rank test or the Wilcoxon rank-sum test. The accuracy of lnc-MAFG-AS1 in identifying the different tissues was analyzed using the receiver operator characteristic curve. When evaluating the correlation between lnc-MAFG-AS1 and OS, the patients were classified into lnc-MAFG-AS1 high and low groups on the basis of the median expression of lnc-MAFG-AS1 in the total tumor tissue. The Kaplan–Meier curve for OS was analyzed using the log-rank test. Prognostic factor analysis was performed using univariable and multivariable Cox’s proportional hazard regression. A p-value below 0.05 indicated statistical significance. SPSS 24.0 (IBM Corp., Armonk, NY, USA) and GraphPad Prism 7.01 (GraphPad Software Inc., San Diego, CA, USA) were used for analysis and graphing, respectively.

Analyzed HCC patients showed an age of 57.3 ± 8.9 years; among them, 86.8% were males, and 13.2% were females (Table 1). The BCLC and CNLC stages were assessed according to ECOG PS, Child–Pugh, tumor nodule number, tumor size, etc. It was found that 1.3%, 48.7%, 20.4%, and 29.6% patients belonged to the BCLC stage 0, A, B, and C, respectively; 18.4%, 41.4%, 24.4%, and 15.8% patients belonged to the CNLC stage Ia, Ib, IIa, and IIb, respectively. Detailed information on these patients’ features is given in Table 1.

Lnc-MAFG-AS1 was higher in HCC tumor tissue than in adjacent tissue [median (interquartile range): 2.730 (1.685–4.198) vs. 0.990 (0.703–1.468), p < 0.001] (Figure 1A). Besides, lnc-MAFG-AS1 distinguished HCC tumor tissue from adjacent tissue with an AUC of 0.889 [95% confidence interval (CI): 0.854–0.924] (Figure 1B).

In terms of disease conditions and tumor properties, lnc-MAFG-AS1 expression was related to multifocal nodules (p < 0.001), increased BCLC stage (p = 0.018), and elevated CNLC stage (p = 0.008) (Table 2). From the perspective of liver function indexes and tumor markers, lnc-MAFG-AS1 expression was associated with an abnormal alpha-fetoprotein (AFP) level (p = 0.004) (Table 3). However, lnc-MAFG-AS1 was not linked with other disease conditions, tumor properties, liver function indexes, or tumor markers in HCC patients.

During a median follow-up of 30 months (range: 5–60 months) in this study, unfortunately 71 (46.7%) patients died. It was then observed that patients with a high expression of lnc-MAFG-AS1 exhibited worse OS than those with a low expression of lnc-MAFG-AS1 [median (95% CI): 34.0 (24.5–43.5) vs. 48.0 (41.5–54.5) months] (p = 0.011) (Figure 2). In detail, the 1-, 2-, 3-, and 4-year OS rates of patients with low lnc-MAFG-AS1 were 97.4%, 90.4%, 70.3%, and 47.8%, respectively. The 1-, 2-, 3-, and 4-year OS rates of those with high lnc-MAFG-AS1 were 94.6%, 65.0%, 47.5%, and 34.3%, respectively.

In addition, univariate Cox’s analysis found that lnc-MAFG-AS1 expression (high vs. low) correlated with unfavorable OS [hazard ratio (HR) = 1.827, p = 0.013] (Figure 3A). Subsequent multivariate Cox’s analysis identified that lnc-MAFG-AS1 expression (high vs. low) related to a less-prolonged OS (HR = 1.697, p = 0.040) (Figure 3B).

Furthermore, subgroup analysis was conducted, which disclosed that high lnc-MAFG-AS1 was not related to OS in BCLC 0/A patients (p = 0.118) (Figure 4A) but was linked with worse OS in BCLC B/C patients (p = 0.010) (Figure 4B).