Abstract
Background
Patients with small-cell lung cancer (SCLC) patients demonstrate varied survival outcomes. Previous studies have reported that lipoproteins are associated with prognosis in various cancers; however, the role of low-density lipoprotein (LDL) and low-density lipoprotein- cholesterol (LDLR) in patients with SCLC has not been studied.
Methods
In this study, the impact of LDL and LDLR on the prognosis of SCLC patients was evaluated. A total of 601 patients with SCLC were retrospectively evaluated, in which 198 patients had adequate tissues for immunohistochemistry, and serum LDL and LDLR expression levels at baseline were tested. X-tile tool, and univariate and multivariate Cox analysis were used to assess the association between LDL, LDLR and overall survival (OS).
Results
Univariate analysis demonstrated that a lower LDL level was significantly associated with superior OS (P = 0.037). Similarly, LDLR also significantly predicted OS (P = 0.003). Multivariate Cox analyses confirmed that lower LDL and LDLR expression was independent prognostic factors associated with longer OS (P = 0.019 and P = 0.027, respectively).
Conclusions
This study showed that both LDL and LDLR are prognostic indexes for survival in patients with SCLC. Patients with high LDL or LDLR expression level may benefit from treatment that modulates lipoprotein combined with platinum-based chemotherapy.
Similar content being viewed by others
Background
Lung cancer remains the most common malignancy worldwide and accounts for the most cases of cancer related deaths in men and women [1]. Approximately 2.2 million new cases occur annually in the United States and 1.5 million people will die from this malignancy [2]. Up to 15% of newly diagnosed lung cancer in men and women are small-cell lung cancer (SCLC) [3–5]. SCLC is an aggressive subtype of lung cancer. About 60% of patients have extensive disease at diagnosis and many patients are at high risk for developing relapse disease [6]. Moreover, many patients with recurrent disease failed to respond effectively to chemotherapy due to developing resistance with treatment. The overall 5-year survival rate for SCLC patients with limited and extensive staging is 25 and 7.8%, respectively [7–9]. Therefore, patients with extensive SCLC have poor prognosis at initial diagnosis. Patients with SCLC patient have varied prognosis despite having similar staged disease. Therefore, identifying prognostic factors that are associated with clinical benefit may help guide treatment.
Cholesterol is a critical structural component of the cellular membrane in most cell types [10]. A number of studies have showed that cholesterol is associated with cell proliferation [11, 12], suggesting that abnormal cholesterol synthesis could play a role in the tumorigenesis of various tumor cells, including breast, colon, and nasopharyngeal [13–18]. The correlation between cholesterol and tumorigenesis in humans is currently an area of investigation; however, the mechanism by which abnormal cholesterol synthesis contributes to tumorigenesis remains unknown. Several studies have reported that cholesterol, particularly serum low-density lipoprotein (LDL), is abnormal in patients with cancer. Beyond the known functions of LDL as a key lipoprotein carrier of cholesterol, it is also a key factor in the signaling pathways of cancer cells [19]. Recently, LDL has been reported to promote cancer metastasis by regulating integrin transfer [20]. Otherwise, since tumor cells have more cholesterol requirements than normal cells, they may enhance their cholesterol content through receptor-mediated endocytosis of serum LDL by LDLR, which are able to recognize a series of ligands. Recent studies have demonstrated that low-density lipoprotein receptor (LDLR) play a role in cancer and is found overexpressed in various types of of human cancer cells [21, 22]. LDLR has also been reported to play an important role in tumor cancer growth and invasion by regulating NF-kB signaling [23].
Previous studies have indicated that LDL and LDLR are prognostic factors in pancreatic adenocarcinoma, which negatively correlated with clinical outcome [24]. However, the association of serum LDL and LDLR with clinical outcome in SCLC remained unknown. In this retrospective study, we explored the potential prognostic value of serum LDL and LDLR in SCLC patients. Moreover, we proposed that LDL and LDLR might be promising metabolic targets for anti-tumor therapy in SCLC.
Methods
Study population
This retrospective study involved data collection from SCLC patients between January 2004 to December 2011 at Sun Yat-Sen University Cancer Center (SYSUCC). All enrolled patients met the following criteria: (a) pathologically confirmed primary SCLC, (b) available clinical information, (c) normal liver function, and (d) detailed laboratory data, including cholesterol and LDL at diagnosis. In both groups, patients were recruited with lipid metabolism-related diseases, or currently treated for concomitant diseases that would influence serum lipids (i.e., diabetes, hyperlipidemia, or metabolic syndrome), patients with liver disease, or other types of cancer. A total 601 eligible patients were enrolled into the study. Among them, 198 cases have sufficient tumor specimens for immunohistochemistry (IHC). All patients were staged according to the Veterans Administration Lung Study Group (VALSG) staging system. Complete clinical information of all patients (i.e., demographics, performance status, treatments and laboratory tests) was recorded. Smokers were defined as patients who had more than 100 cigarettes. The study was approved by the Institutional Review Board of SYSUCC and written informed consent was obtained for each patient prior to sample collection.
Treatment
Most patients received four cycles of platinum plus etoposide as chemotherapy, and some patients also were subsequently treated with prophylactic cranial irradiation (PCI). Several patients underwent thorax radiotherapy (TRT) in accordance with chemotherapy.
LDLR immunohistochemistry and scoring
We performed IHC staining to evaluate the expression of LDLR in SCLC patients. Sections (thickness, 3–4 μm) were deparaffinized and rehydrated. For antigen retrieval, the slides were soaked in ethylene diamine tetraacetic acid (EDTA) and Aantigen Rretrieval Ssolution (3000 ml, pH 8.0), followed by heating in a pressure cooker for 12 min. Treated sections were then cooled to room temperature prior to immersing in distilled water for 2 min. To block the endogenous peroxidase activity and reduce non-specific assimilation, sections were treated with 3% H2O2 for 8 min, and further incubated in 5% bovine serum albumin for 30 min. Anti-LDLR (mouse LDLR antibody; R&D Systems; American) (1:400 dilution) was then added and incubated at 4 °C for 24 h. After washing with phosphate-buffered saline (PBS) for three cycles of 2 min, slides were incubated with secondary antibody (PV-9003 goat kit; ZSGB-Bio, Beijing, China) at 37 °C for 30 min. Afterwards, slides were washed with PBS thrice again. 3, 3′- diamino benzidine was applied for dyeing and hematoxylin was used to counterstain the sections. All sections were independently reviewed by two pathologists. Semi-quantitative scoring was used to evaluate immune reaction [25]. An IHC score, called HSCORE, was then applied to each sample based on the intensity of staining and the percentage of positive tumor cells. The HSCORE was calculated as following: HSCORE = Ʃ (I × PC). “I “means the intensity of staining and “PC” represents the percentage of positive tumor cells.
Follow-up
All the patients were carefully followed. Patients were evaluated every 2 months after completion of anti-tumor therapy. Routine follow-up examination was performed by computed tomography (CT) scan or/and Magnetic Resonance Imaging (MRI), including chest radiograph, abdominal ultrasonography and brain when clinically indicated. Anti-tumor response was assessed by radiologists according to the Response Evaluation Criteria in Solid Tumors (RECIST, version 1.1). Overall survival (OS) was defined as the months from the diagnosis to the death for any cause or last follow-up. Progression-free survival (PFS) was defined as the months from the diagnosis to the earliest occurrence of disease progression or death for any reasons. Patients who were alive at the time of last follow-up or lost to follow-up were censored. The last follow-up date was determine at May 31, 2015.
Statistical analysis
The primary outcome of the study was overall survival. Pearson correlation, Chi-square test, and Fisher exact test were used to compare continuous and categorical variables. The optimal cutoff values of LDL and LDLR level were determined using X-tile. Kaplan-Meier method was performed to estimate the relationship between overall survival (OS) and potential prognostic factors. Univariate analysis was performed to assess differences in survival by log-rank test. Cox proportional hazards model was used to estimate the predictive power. Potential prognostic factors included in the test model were age, sex, performance status (PS), cancer stage, LDL and LDLR. A P value of ≤0.05 was considered statistically significant. All of the statistical tests were two-tailed. Data analyses were carried out using the SPSS statistical software package (version 21.0, IBM, Armonk, NY).
Results
Patient characteristics
The patient baseline characteristics are presented in Table 1. A total of 601 patients with SCLC were enrolled in the study, with a median age of 60 years (range, 19–82 years). The majority of the patients were males (n = 529, 88%) and smokers (n = 505, 84.0%), and had a PS of 0–1 (n = 550, 91.7%). Among them, 254 (42.3%) patients had distant metastasis at the time of diagnosis and 347 (57.7%) patients were at limited stage. Most of the patients had prior treatment of two to four cycles of etoposide-based chemotherapy, while 22.1% (n = 133) patients received PCI and 37.8% (n = 227) had TRT. At last follow-up date, 433 (72%) patients had died. The median follow-up time was 31.75 months (range, 3.32 months to 117.41 months).
Correlation of LDL and LDLR with clinical features
Using X-tile [26], we determined that the optimal cutoff for serum LDL in assessing OS is 2.14 and 3.36. Patients were divided into three groups based on the cutoff value of LDL: (1) low-LDL group (LDL level ≤ 2.14 mmol/L, n = 66, 11.0%) (2) intermediate-LDL group (3.36 mmol/L < LDL level ≥ 2.14 mmol/L, n = 282, 46.9%) and (3) High-LDL group (LDL level > 3.36 mmol/L, n = 253, 42.1%) (Additional file 1: Figure S1).
The clinicopathological characteristics of SCLC patients based on LDL levels are presented in Table 2. More patients had low levels of serum LDL in the etoposide-based chemotherapy group compared with those in the non-etoposide-based chemotherapy group (P = 0.011, Table 2). However, the level of LDL was not significant associated with age (P = 0.648), gender (P = 0.918), PS (P = 0.119), smoking status (P = 0.411), and disease stage (P = 0.189) (Table 2).
Based on the results by X-tile, the 198 patients who had sufficient tumor samples for IHC were grouped as followed: (1) low-LDLR group (HSCORE ≤ 60, n = 145, 73.2%, Fig. 1a), and (2) high-LDLR group (HSCORE >60, n = 53, 26.8%, Fig. 1b) (Additional file 1: Figure S1).
Representative images of immunostaining of LDLR expression based on different levels of expression (Original magnification 200×). a Low LDLR expression, b High LDLR expression. LDLR, low-density lipoprotein
Among the 198 patients, 175 ones were males, ones were smokers, and ones had a PS of 0–1. The relationship between LDLR and clinical features have been analyzed. There were no obvious correlation of LDLR to gender (P = 0.565), PS (P = 0.118), and smoking status (P = 0.069).
Univariate Cox regression analysis of survival
The median OS for the 601 eligible patients was 15.43 months (range, 0.03–123.43 months). The median PFS for the entire cohort was 5.32 months (range, 0.03–71.79 months). A total of 66, 282, and 253 patients were categorized as low-LDL, intermediate-LDL, and high-LDL groups. Compared with the low-LDL group, patients with intermediate-LDL or high-LDL had lower survival outcome (low-LDL vs. intermediate-LDL vs. high-LDL, 29.27 vs. 16.70 vs. 17.23 months, respectively; P = 0.003) (Fig. 2a). When stratified by cancer stage, we found that LDL also showed a prognostic power in limited stage (P = 0.01, Fig. 2b). Moreover, baseline serum LDL value also had distinct significance in predicting PFS (P = 0.037, Fig. 2c).
Kaplein Meyer survival curves for patients with SCLC based on LDL levels. a Comparison of OS in overall patients based on LDL levels, b Comparison of OS in patients with limited stage based on LDL levels, c Comparison of PFS in patients based on LDL levels, d Comparison of OS in patients based on LDLR expression level. LDL: low-density lipoprotein; LDLR: low-density lipoprotein
To provide a significant control and a point of reference for LDLR expression, we also study the immune-staining of healthy lung tissue. The image shows that the expression of LDLR in healthy lung tissue is very low (Additional file 2: Figure S2). Moreover, patients with a lower expression of LDLR demonstrated significantly better OS (19.94 vs. 11.27 months, respectively; P = 0.003, Fig. 2d).
Other than LDL and LDLR, PS score (P < 0.001), smoking status (P < 0.001), and disease stage (P < 0.001) were also significantly associated with OS. Patients who received TRT (P < 0.001) or PCT (P = 0.001) also were associated with better OS (Fig. 3). However, there were no distinct associations between OS and gender (P = 0.438) and age (P = 0.424) (Table 1). In addition, patients with a lower PS score and in limited stage demonstrated significantly better PFS (P = 0.002 and P < 0.001, respectively).
Overall survival curves of patients with SCLC a Good vs bad PS, b Limited stage vs extensive stage, c Received TRT vs none, d Received PCI vs none. PS: performance status; TRT: thorax radiotherapy; PCI: prophylactic cranial irradiation
Multivariate Cox regression analysis of potential prognostic factors
Multivariate analyses, was performed to test for correlation among the different prognostic variables. We observed that higher LDL level was a significantly independent prognostic factor for poorer OS (P = 0.019, Table 3). Patients in intermediate LDL group were estimated to have 1.42-fold higher risk of death compared with those in the low LDL group (HR, 1.42; 95% CI: 1.08–2.03; P = 0.015). Patients with a LDL level of >3.36 had 1.64-fold higher risk of death than those in the low LDL group. Similarly, the multivariate analyses demonstrated that LDLR expression independently predicted OS in patients with SCLC (P = 0.027, Table 3). Compared with patients with a HSCORE ≤ 60, those with a HSCORE >60 had a 1.538 higher risk of death. Moreover, PS score (P < 0.001), cancer stage (P < 0.001), PCI (P = 0.011), and TRT (P = 0.007) were also independent predictors of survival outcome in patients with SCLC (Table 3).
Discussion
Cholesterol plays a critical role in maintaining the structural integrity of the plasma cell membrane [27, 28]. In addition, cholesterol also accumulates in specific domains of the membrane and associates with proteins that are involved in various cellular signaling pathways [29]. A study by Guillaumond et al. found that cholesterol uptake is significantly increased in pancreatic adenocarcinoma [24]. Several studies indicated that cholesterol modulates the development and progression of various cancers [30, 31]. Moreover, a recent study identified that cholesterol could be a prognostic index for patients with metastatic nasopharyngeal carcinoma [17].
LDL is a component of cholesterol and is involved in cholesterol transportation. A recent study has indicated that LDL level is associated with increased risk of developing hepatocellular carcinoma [32]. Rodrigues et al. demonstrated that LDL level was an adverse predictor of disease-free survival in breast cancer patients [33]. In CRC patients, LDL was also identified as an independent prognostic factor [34]. Nevertheless, the mechanism by which LDL levels are associated with cancer development remains unclear. LDLR, a receptor for LDL, can activate signaling pathways involved in inflammation, cellular transformation, and cell growth. Previous studies demonstrated that LDLR has a pro-tumorigenic effect [35]. Studies have also demonstrated that the expression of LDLR in tumor cells is higher than in normal cells, and has been reported to promote cancer progression by increasing proliferation and migration of tumor cells [24, 36, 37].
Although studies have suggested a significant relationship between LDL, LDLR and cancer, levels of LDL and LDLR expression are varied across patients of different tumor types. Thus, in this study, we assessed the prognostic impact of LDL and LDLR expression levels in SCLC patients. To our knowledge, this is the first large-scale cohort study to explore the prognostic value of LDL and LDLR levels in SCLC patients. Based on cutoff value of LDL levels at diagnosis, we observed that 89% (n = 535) of SCLC patients had elevated serum LDL. We next evaluated the effects of LDL levels on OS. Univariate analysis demonstrated that high levels of LDL were associated with poorer survival in SCLC patients. Consistently, multivariate analysis demonstrated that LDL was also an independent prognostic factor in SCLC. Our study also suggested that lower LDLR was significantly associated with longer OS, compared with higher LDLR. Additionally, we showed that LDLR is also an independent predictor for OS. The stratification of patients according to disease stage showed that LDL level is a predictor of limited stage and not extensive stage. While the reason for this observation remains unclear, we speculate that an abnormal metabolic microenvironment in patients with extensive disease may influence LDL levels. Low LDL level was a predictor of longer PFS, which was consistent with the findings by previous published studies.
Based on the findings of this study, we speculate that higher serum LDL and LDLR expression level could be attributed to active tumor cells secreting high levels of cholesterol. Therefore, our findings support the notion that lipoprotein treatment may be a promising anti-tumor agent in patients with high LDL or LDLR expression level. Moreover, combination therapies of LDL-lowering agent with platinum-based chemotherapy may improve clinical outcome of patients. Nonetheless, there remains a need for identifying effective agents to improve the clinical outcomes of patients with SCLC, such as evaluating whether LDLR is a potential therapeutic target.
Our study does have several limitations. First, it is a retrospective study with clinical data primarily derived from a single institution. Future studies will involve patients from multiple centers to validate our findings. Second, it remains unclear the mechanism by which increased LDL level occurs in patients with SCLC. Additional studies will be needed to elucidate this.
Conclusions
In summary, our results suggest that the serum LDL and LDLR expression level at diagnosis could serve as a significant prognostic factor in patients with SCLC. Serum LDL and LDLR expression in tumor cells at diagnosis could help identify patients susceptible to disease progression. Furthermore, the development of LDL-lowering agents combined with platinum-based chemotherapy may be a new and promising therapeutic strategy for SCLC patients. Therefore, baseline LDL and LDLR expression level could be routinely applied to guide treatment decisions in patients with SCLC.
Abbreviations
- CT:
-
Computed tomography
- EDTA:
-
Ethylene diamine tetraacetic acid
- IHC:
-
Immunohistochemistry
- LDL:
-
Low-density lipoprotein
- LDLR:
-
Low-density lipoprotein- cholesterol
- MRI:
-
Magnetic Resonance Imaging
- OS:
-
Overall survival
- PBS:
-
Phosphate-buffered saline
- PCI:
-
Prophylactic cranial irradiation
- PFS:
-
Progression-free survival
- PS:
-
Performance status
- RECIST:
-
Response Evaluation Criteria in Solid Tumors
- SCLC:
-
Small-cell lung cancer
- SYSUCC:
-
Sun Yat-Sen University Cancer Center
- TRT:
-
Thorax radiotherapy
- VALSG:
-
the Veterans Administration Lung Study Group
References
Jemal A, Siegel R, Xu J, Ward E. Cancer statistics, 2010. CA Cancer J Clin. 2010;60(5):277–300.
Siegel RL, Miller KD, Jemal A. Cancer statistics, 2015. CA Cancer J Clin. 2015;65(1):5–29.
Govindan R, Page N, Morgensztern D, Read W, Tierney R, Vlahiotis A, et al. Changing epidemiology of small-cell lung cancer in the United States over the last 30 years: analysis of the surveillance, epidemiologic, and end results database. J Clin Oncol. 2006;24(28):4539–44.
Herbst RS, Heymach JV, Lippman SM. Lung cancer. N Engl J Med. 2008;359(13):1367–80.
Lally BE, Urbanic JJ, Blackstock AW, Miller AA, Perry MC. Small cell lung cancer: have we made any progress over the last 25 years? Oncologist. 2007;12(9):1096–104.
Peeters M, Price TJ, Cervantes A, Sobrero AF, Ducreux M, Hotko Y, et al. Randomized phase III study of panitumumab with fluorouracil, leucovorin, and irinotecan (FOLFIRI) compared with FOLFIRI alone as second-line treatment in patients with metastatic colorectal cancer. J Clin Oncol. 2010;28(31):4706–13.
Gralla RJ. Quality-of-life considerations in patients with advanced lung cancer: effect of topotecan on symptom palliation and quality of life. Oncologist. 2004;9(Suppl 6):14–24.
Sugiyama T, Hirose T, Hosaka T, Kusumoto S, Nakashima M, Yamaoka T, et al. Effectiveness of intensive follow-up after response in patients with small cell lung cancer. Lung Cancer. 2008;59(2):255–61.
Hann CL, Rudin CM. Management of small-cell lung cancer: incremental changes but hope for the future. Oncology. 2008;22:1486–92.
Brameshuber M, Sevcsik E, Rossboth BK, Manner C, Deigner HP, Peksel B, et al. Oxidized phospholipids inhibit the formation of cholesterol-dependent plasma membrane nanoplatforms. Biophys J. 2016;110(1):205–13.
Zhuang L, Kim J, Adam RM, Solomon KR, Freeman MR. Cholesterol targeting alters lipid raft composition and cell survival in prostate cancer cells and xenografts. J Clin Invest. 2005;115(4):959–68.
Cruz PM, Mo H, McConathy WJ, Sabnis N, Lacko AG. The role of cholesterol metabolism and cholesterol transport in carcinogenesis: a review of scientific findings, relevant to future cancer therapeutics. Front Pharmacol. 2013;4:119.
DeBerardinis RJ, Lum JJ, Hatzivassiliou G, Thompson CB. The biology of cancer: metabolic reprogramming fuels cell growth and proliferation. Cell Metab. 2008;7(1):11–20.
Lee BH, Taylor MG, Robinet P, Smith JD, Alermus JB, Sehayek E, et al. Dysregulation of cholesterol homeostasis in human prostate cancer through loss of ABCA1. Cancer Res. 2013;73(3):1211–8.
Calle EE, Rodriguez C, Walker-Thurmond K, Thun MJ. Overweight, obesity, and mortality from cancer in a prospectively studied cohort of U.S. adults. N Engl J Med. 2003;348(17):1625–38.
Michalaki V, Koutroulis G, Syrigos K, Piperi C, Kalofoutis A. Evaluation of serum lipids and high-density lipoprotein subfractions (HDL2, HDL3) in postmenopausal patients with breast cancer. Mol Cell Biochem. 2005;268(1–2):19–24.
Jiang R, Yang ZH, Luo DH, Guo L, Sun R, Chen QY, et al. Elevated apolipoprotein A-I levels are associated with favorable prognosis in metastatic nasopharyngeal carcinoma. Med Oncol. 2014;31(8):80.
Mandal CC, Rahman MM. Targeting intracellular cholesterol is a novel therapeutic strategy for cancer treatment. J Cancer Sci Ther. 2014;6(12):510–3.
Jeon JH, Kim SK, Kim HJ, Chang J, Ahn CM, Chang YS. Lipid raft modulation inhibits NSCLC cell migration through delocalization of the focal adhesion complex. Lung Cancer. 2010;69(2):165–71.
Reverter M, Rentero C, Garcia-Melero A, Hoque M, de Muga SV, Alvarez-Guaita A, et al. Cholesterol regulates Syntaxin 6 trafficking at trans-Golgi network endosomal boundaries. Cell Rep. 2014;7(3):883–97.
Hirsch HA, Iliopoulos D, Joshi A, Zhang Y, Jaeger SA, Bulyk M, et al. A transcriptional signature and common gene networks link cancer with lipid metabolism and diverse human diseases. Cancer Cell. 2010;17(4):348–61.
Damiano MG, Mutharasan RK, Tripathy S, McMahon KM, Thaxton CS. Templated high density lipoprotein nanoparticles as potential therapies and for molecular delivery. Adv Drug Deliv Rev. 2013;65(5):649–62.
Notarnicola M, Messa C, Orlando A, D'Attoma B, Tutino V, Rivizzigno R, et al. Effect of genistein on cholesterol metabolism-related genes in a colon cancer cell line. Genes Nutr. 2008;3(1):35–40.
Guillaumond F, Bidaut G, Ouaissi M, Servais S, Gouirand V, Olivares O, et al. Cholesterol uptake disruption, in association with chemotherapy, is a promising combined metabolic therapy for pancreatic adenocarcinoma. Proc Natl Acad Sci U S A. 2015;112(8):2473–8.
McCarty KS, Szabo E, Flowers JL, Cox EB, Leight GS, Miller L, et al. Use of a monoclonal anti-estrogen receptor antibody in the immunohistochemical evaluation of human tumors. Cancer Res. 1986;46(8 Suppl):4244s–8s.
Camp RL, Dolled-Filhart M, Rimm DL. X-tile: a new bio-informatics tool for biomarker assessment and outcome-based cut-point optimization. Clin Cancer Res. 2004;10(21):7252–9.
Patel PS, Shah MH, Jha FP, Raval GN, Rawal RM, Patel MM, et al. Alterations in plasma lipid profile patterns in head and neck cancer and oral precancerous conditions. Indian J Cancer. 2004;41(1):25–31.
Girotti AW, Korytowski W. Cholesterol as a natural probe for free radical-mediated lipid peroxidation in biological membranes and lipoproteins. J Chromatogr B. 2016;1019:202–9.
Muntoni S, Atzori L, Mereu R, Satta G, Macis MD, Congia M, et al. Serum lipoproteins and cancer. Nutr Metab Cardiovasc Dis. 2009;19(3):218–25.
Tamura T, Inagawa S, Hisakura K, Enomoto T, Ohkohchi N. Evaluation of serum high-density lipoprotein cholesterol levels as a prognostic factor in gastric cancer patients. J Gastroenterol Hepatol. 2012;27(10):1635–40.
Danilo C, Frank PG. Cholesterol and breast cancer development. Curr Opin Pharmacol. 2012;12(6):677–82.
Saito N, Sairenchi T, Irie F, Iso H, Iimura K, Watanabe H, et al. Low serum LDL cholesterol levels are associated with elevated mortality from liver cancer in Japan: the Ibaraki prefectural health study. Tohoku J Exp Med. 2013;229(3):203–11.
Santos C, Fonseca I, Dias S, de Almeida JM. Plasma level of LDL-cholesterol at diagnosis is a predictor factor of breast tumor progression. BMC Cancer. 2014;14(1):132.
Liu YL, Qian HX, Qin L, Zhou XJ, Zhang B. Serum LDL-C and LDL-C/HDL-C ratio are positively correlated to lymph node stages in males with colorectal cancer. Hepato-Gastroenterol. 2011;58(106):383–7.
Migita T, Ruiz S, Fornari A, Fiorentino M, Priolo C, Zadra G, et al. Fatty acid synthase: a metabolic enzyme and candidate oncogene in prostate cancer. J Natl Cancer Inst. 2009;101(7):519–32.
Jiang L, Jiang S, Lin Y, Yang H, Zhao Z, Xie Z. Combination of body mass index and oxidized low density lipoprotein receptor 1 in prognosis prediction of patients with squamous non-small cell lung cancer. Oncotarget. 2015;6(26):22072–80.
Harisa GI, Alanazi FK. Low density lipoprotein bionanoparticles: from cholesterol transport to delivery of anti-cancer drugs. Saudi Pharmaceutical J. 2014;22(6):504–15.
Acknowledgements
Not applicable.
Funding
This work was supported by: Wu Jieping Medical Foundation Project (Grant No: 08-JC-003), Innovative drug R&D center based on real-time high-throughput cell-based screening platform and large capacity compound library (Grant No: 2013ZX09401003–002), National Natural Science Foundation of China (Grant No: 81,372,502), and National Natural Science Foundation of China (Grant No: 81,602,011). All the grand supporters have no roles in study design, data collection and analysis, and manuscript preparation.
Availability of data and materials
All data generated or analysed during this study are included in this published article and its supplementary information files.
Authors’ contributions
TZ, JZ and WF conceived of the study, and drafted the manuscript. YZ and YY participated in the design of the study. XH, ZZ and XH performed the statistical analysis. YZ and YH conceived of the study. LZ design study. All authors read and approved the final manuscript.
Competing interests
The authors declare that they have no competing interests.
Consent for publication
Not applicable.
Ethics approval and consent to participate
The study was approved by the Institutional Review Board of SYSUCC and written informed consent was obtained for each patient prior to sample collection. Patients were informed that the resected specimens were stored by the hospital and potentially used for scientific research, and that their privacy would be maintained.
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Author information
Authors and Affiliations
Corresponding author
Additional files
Additional file 1: Figure S1.
Bar plots of baseline serum LDL and LDLR expression levels of the SCLC patients base on the cutoff values. (TIFF 3195 kb)
Additional file 2: Figure S2.
Representative image of immunostaining of LDLR expression in healthy lung tissue (Original magnification 200×). (TIFF 6774 kb)
Rights and permissions
Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
About this article
Cite this article
Zhou, T., Zhan, J., Fang, W. et al. Serum low-density lipoprotein and low-density lipoprotein expression level at diagnosis are favorable prognostic factors in patients with small-cell lung cancer (SCLC). BMC Cancer 17, 269 (2017). https://doi.org/10.1186/s12885-017-3239-z
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/s12885-017-3239-z