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Serum lactate dehydrogenase level predicts the prognosis in bladder cancer patients
BMC Urology volume 23, Article number: 65 (2023)
Abstract
Background
Recently, several studies investigated the association between lactate dehydrogenase (LDH) level and the prognosis of urothelial carcinoma. However, no studies explored the role of serum LDH level in the survival of overall bladder cancer (BC). In this study, we intended to address the association of LDH level with the prognosis of BC.
Methods
206 patients with BC were included in this study. The clinical data and blood samples of patients were collected. The overall survival and progression-free survival were used. Kaplan–Meier method and Log rank test were used to evaluate the effects of LDH level on the survival of BC. Univariate and multivariate Cox regression analyses were utilized to identify prognosis predictors of BC.
Results
Data indicated that serum LDH level in the BC patients was significantly higher than those in controls. In addition, this study suggested that serum LDH level was associated with T stage, N stage, tumor size, M stage, pathological type, and lymphovascular invasion. The Kaplan–Meier analysis found significant differences in the OS and PFS rate between lower and higher serum LDH level groups (LDH ≥ 225 U/L and < 225 U/L). Multivariate Cox regression indicated that pathological type, T2–3, and higher level of LDH were independently associated with adverse prognosis in BC patients.
Conclusion
The higher serum LDH level (≥ 225 U/L) is associated with poor prognosis in patients with BC. Serum LDH level could be used as a novel predictive biomarker for BC patients.
Introduction
Bladder cancer (BC) is a prevalent malignancy and is the fourth most main malignancy in men [1]. More than 430,000 BC patients were diagnosed globally every year, which brings a heavy burden for the society [2]. A host of risk factors including cigarette smoking, alcohol intake, diets low in fruits and vegetables, urban living, occupational exposure to carcinogens, and genetic factors were associated with the development of BC [3]. Among these factors, cigarette smoking is the most primary risk factor for BC. It is estimated that tobacco was responsible for approximately 50% of all BC patients [4]. The most common symptom of BC is haematuria [5]. However, some BC patients with microscopic haematuria were not easily detected [6]; and there were no effective screening methods for BC, except for the cystoscope. Thus, detecting novel prognostic and diagnostic biomarkers is urgently required for patients with BC.
Most cancer cells utilize glucose metabolism by glycolysis to produce enough ATP to promote the development of cancer, which is served as the Warburg effect [7]. Among the enzymes participating in glycolysis, lactate dehydrogenase (LDH), an oxidoreductase, could converts pyruvate to lactate at the end of glycolysis; thereby, LDH is regarded as a promising molecular target for the development of new glycolytic inhibitors used in cancer therapy [8]. LDH may be a biomarker of tumor development due to its association with tumor metabolic changes [9].Urothelial carcinoma (UC) mainly consists of urothelial carcinoma of the bladder (UCB) and upper tract urothelial carcinoma (UTUC). Recently, a host of studies investigated the link between LDH level and the prognosis of UC [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24]. Among these studies, no studies investigated the role of serum LDH level in the survival of overall BC; and previous studies mainly focused on UCB patients (the main type of BC). In this study, we intended to address the association of LDH level with clinicopathological markers of BC. In addition, we aimed to evaluate the ability of pretreatment serum LDH level in predicting the prognosis of BC patients.
Methods
Patients
This study was conducted after approval from the Ethics Committee of Huaian No.1 People’s Hospital. 206 consecutive BC patients were recruited between September 2014 and May 2017 from our Hospital. BC patients were divided into two groups, which was according to the pretherapeutic median levels of LDH. The diagnosis of BC patients was according to histological results. All relevant clinical and pathologic information was collected for each patient. Inclusion criteria for BC patients were as follows: one, patients with definite histologic evidence; two, patients older than 18 years; three, patients with complete data. Patients with other cancers, hepatitis, heart disease, and hemopathy were excluded. The informed consent form was provided by all subjects. This study was approved by the Ethics Committee of this hospital. This study was in consistent with the Declaration of Helsinki.
Data collection and follow-up
Clinical information was collected from the medical records, including age, sex (male and female), smoking status (yes and no), T stage, N stage (N0 and N1-N3), tumor size (< 3 cm and > 3 cm), M stage (M0 and M1), lymphovascular invasion (LVI) status, perineural invasion (PNI) status, pathological type, and multifocality (Unifocal and Multifocal). Serum LDH levels were collected from all BC patients before treatment. The cut-off value of LDH level was defined as 225 U/L, which was the upper limit of normal range in this hospital. Thus, we defined the high LDH level group was over 225 U/L, and the low LDH level group was lower than 225 U/L. Overall survival (OS) was defined as the survival duration from the date of initial diagnosis to death due to any reasons or last follow-up. Progression-free survival (PFS) referred to the time for BC patients to survive without progression or death after treatment. The follow-up strategies were as follows: every two months for the first 2 years, quarterly for the next 2 years, and then semiannually for the remaining time thereafter. The follow-up time ended in June 2021.
Statistical analysis
The correlation between serum LDH level and clinicopathological indexes was analyzed. We used the receiver operating characteristic (ROC) curve to assess the diagnostic ability of serum LDH level for detecting BC. The log-rank test was used to compare the OS and PFS between different groups. Univariate and Multivariate Cox regression analyses were conducted to identify prognostic variables associated with the survival of BC. Risk factors with a P value < 0.05 in univariate analysis were choose in further multivariate Cox regression analysis. 95% confidence interval (CI) and Hazard risk (HR) were figured out. Statistically significant Differences were set at P < 0.05. SPSS (version 19.0, Chicago, IL, USA), and Graphpad Prism (version 7.0, La Jolla, CA, USA), and MedCalc were used for statistical analyses.
Results
Clinicopathological variables of BC patients and LDH level
Clinicopathological variables for BC patients with LDH ≥ 225 U/L and < 225 U/L are shown in Table 1. 223 patients with BC were evaluated initially, and 206 cases were included finally (Fig. 1). Among the 206 BC patients, 149 cases were in the low LDH group and 57 cases were in the high LDH group. We found that LDH level was associated with T stage, N stage, tumor size, M stage, pathological type, and LVI status (Table 1). No significant differences were observed in two groups regarding age, sex, smoking status, PNI status, and multifocality status (Table 1).
The flow diagram of patients
Diagnostic value of LDH level for detecting BC
230 controls were included in this study. The detailed information for controls is summarized in Additional file 2: Table S1. We measured the serum level of LDH in BC patients and controls, and found that the LDH level in BC group were significantly higher than those in control group. We used the ROC curve to evaluate the diagnostic function of serum LDH level for BC (Fig. 2). The sensitivity and specificity were 47.57% and 71.74% with a cutoff value of 211.53 (Additional file 3: Table S2), respectively. The area under the curve was 0.615 (95%CI: 0.567–0.661, P < 0.001), suggesting that the diagnostic ability of serum LDH level for detecting BC was relatively moderate.
The receiver operating characteristic curve of LDH level for detecting bladder cancer
Correlation between LDH level and the prognosis in patients with BC
We divided all BC patients into two groups (LDH ≥ 225 U/L and < 225 U/L) according to the level of LDH. In order to evaluate the prognostic value of LDH in BC, Kaplan–Meier analysis was utilized to assess the association between LDH level and follow-up data, and the log-rank test was mainly used for analyzing statistical difference. The results showed that the high level of LDH was negatively correlated with OS and PFS (Figs. 3, 4), suggesting that the survival rate of BC patients with lower level of LDH were significantly higher than those with higher level of LDH. In addition, we compared the survival rates between UCB group and non-UCB group (squamous cell carcinoma and adenocarcinoma). Data indicated that the survival rate of BC patients with UCB was significantly higher than that in non-UCB group (Additional file 1: Figure S1 and S2).
Comparison of overall survival rate between high LDH level group and low LDH level group
Comparison of progress-free survival rate between high LDH level group and low LDH level group
Identification of prognostic factors of OS and PFS
Univariate and multivariate Cox analyses were used to identify prognostic factors of BC patients. Univariate analysis showed that older age, T2–3 stage, N1–3 stage, M1 stage, LVI, PNI, non-UCB, and higher level of LDH were significantly associated with reduced OS (Table 2), while smoking, T2–3 stage, N1–3 stage, M1 stage, tumor size ≥ 3 cm, LVI, PNI, non-UCB, and higher level of LDH negatively correlated with PFS (Table 3). Multivariate analysis indicated that T2–3 stage, non-UCB, and higher level of LDH were independent predictive factors for worse OS and PFS. In addition, we identified prognostic factors for BC patients with UCB, and found that T2–3 stage, and higher LDH level were prognostic factors for worse OS (Additional file 4: Table S3). Furthermore, we observed that T2–3 stage, M1 stage, tumor size ≥ 3 cm were adverse factors for PFS in UCB (Additional file 5: Table S4).
Discussion
This study suggested that serum LDH level was associated with T stage, N stage, tumor size, M stage, pathological type, and LVI status. Serum LDH level had a moderate diagnostic value in detecting BC patients. Multivariate Cox regression indicated that non-UCB, T2–3, and higher level of LDH were independently associated with adverse prognosis in BC patients (including OS and PFS). Therefore, this study provided evidence that higher LDH level was associated with worse prognosis in BC and could be a prognostic indicator of BC patients.
Hannisdal et al. from Denmark first showed that UCB patients with LDH > 400 U/L showed shorter survival comparing to those with LDH < 400 U/L [11]. Two Japanese studies found that higher LDH level was negatively associated with the OS of UCB after radical cystectomy [12] or postcystectomy recurrent UCB [13]. However, a study by Yang et al. from Taiwan indicated that serum LDH level was not related with the disease-specific survival of UCB in their population [10], which was not consistent with previous findings [11,12,13]. We assumed the following factors may provide evidence for these conflicting points. One, the results of Taiwanese study was obtained by the univariate analysis [10], which may underpower the credibility of results. Two, clinical heterogeneity should not be ignored. Two Japanese studies investigated the recurrent UCB [12, 13], while the Taiwanese study explored invasive UCB [10]. Three, their indicators evaluating survival differed, such as OS or disease-free survival (DFS). Four, their varied treatment therapies may also contribute to their contradictory results concerning the survival. It is of note that Yang et al. conducted another study [14], and found that serum LDH level ranging from 200 to 300 U/L was an independent factor associated with UTUC after multivariate analysis, but not for UCB. Obviously, the tumor location may be a crucial reason for explaining their contradictory results by Yang et al. [10, 14] Last but not least, the cut-off values of serum LDH level were diverse, which may exert effects on the final results.
Regarding UTUC, other studies [15,16,17] also delineated the association between serum LDH level and the prognosis of UTUC. Zhang et al. showed that preoperative serum LDH level was as a negative predictor of OS and DFS [15], while Tan et al. indicated that preoperative LDH was not an independent prognostic indicator for patients with UTUC [15]. However, Tan et al. suggested that elevated LDH level correlated with worse OS in UTUC patients with localized disease [16]. Kluth et al. also indicated that serum LDH level was not associated with the survival of UTUC [18]. As for the Japanese study by Ito et al., they observed that LDH ≥ 210 IU/L were significantly related with extraurothelial recurrence in N0M0 patients with renal pelvic cancer [17], but not OS or DFS.
Besides UCB and UTUC, some researchers shed light on the investigation of serum LDH level and UC survival. Sengelov et al. showed that LDH level were related significantly to the survival of UC by univariate analyses [19], similar to the findings by Japanese studies via multivariate analyses [20,21,22]. In addition, two studies from Japan [23] and Spain [24] indicated that serum LDH level was not a prognostic factor in UC patients. We hypothesized that the negative results in the Spanish study [24] may due to its limited sample size (only 56 UC cases). Additionally, they utilized univariate analyses to obtain these results [24], which underpowered the reliability of their results.
Due to these conflicting findings concerning UCB, UTUC or UC, Wu et al. conducted a meta-analysis to address this issue [25]. They suggested that a high pretreatment serum LDH level was linked with an inferior OS, cancer-specific survival, and DFS in UC patients [25]. Subgroup analyses revealed that high serum LDH level was associated with a poor OS and DFS in UTUC, and a short OS in UCB [25]. It is noticeable that the meta-analysis by Wu et al. did not include a study [18], which was in line with inclusion criteria of this meta-analysis. Another meta-analysis by Zhang et al. also indicated that a high LDH level was associated with an adverse prognosis in many solid tumors [26].
In this study, we included 206 BC patients, and found that a higher pretreatment serum LDH level was associated with an unfavorable prognosis in BC patients. Abovementioned studies primarily investigated the survival of UCB patients (the main type of BC), while this study explored the prognosis of overall BC with UCB, squamous cell carcinoma, and adenocarcinoma. We compared the survival rates between UCB group and non-UCB group, and found that the survival rate of BC patients with UCB was significantly higher than that in non-UCB group, which was not investigated in other studies. Furthermore, multivariate analysis indicated that pathological type (non-UCB vs UCB) was an independent predictive factor for worse OS and PFS.
This study had several limitations. First, the sample size of this study was not large enough. Second, some confounding factors affecting the survival of BC may not be investigated in this study, thereby exerting effects on final results. Third, the findings observed by this study were only yielded in one single center; thus, multi-center studies are urgently needed to verify these findings. Fourth, UTUC patients were not investigated in this study. Fifth, diverse treatment strategies may affect the survival analysis, thereby interfering the effect of serum LDH level on the prognosis of BC patients. Last, regarding for the ROC curve (Fig. 2), the AUC value was 0.615, indicating that there was no clear cut differentiation. High LDH level might just be another marker for poor performance.
Conclusions
Totally, this study observes that a higher pretreatment serum LDH level is associated with adverse prognosis in BC patients. In addition, serum LDH level may predict the occurrence of BC patients. Thus, LDH level could be served as a prognostic biomarker for BC patients.
Availability of data and materials
All data generated or analyzed during this study are included in this published article [and its supplementary information files].
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Acknowledgements
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This study did not receive any funding in any form.
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Contributions
SG and CY: study design. CY: data collection. SG and CY: manuscript writing. SG and CY: critical revision of the manuscript. SG supervision. Both authors read and approved the final manuscript.
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Ethics approval and consent to participate
This study was approved by the Ethics Committee of The Affiliated Huaian No.1 People's Hospital of Nanjing Medical University. This study was in consistent with the Declaration of Helsinki. Informed consent was obtained from all subjects and/or their legal guardian.
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Supplementary Information
Additional file 1. Supplementary Figure 1.
Comparison of overall survival rate between UCB group and non-UCB group. Supplementary Figure 2. Comparison of progress-free survival rate between UCB group and non-UCB group.
Additional file 2. Supplement Table 1.
Demographics between BC patients and controls.
Additional file 3. Supplementary Table 2.
ROC curves for predictive values of serum LDH level in UCB.
Additional file 4. Supplementary Table 3.
Univariate and multivariate cox regression analysis for overall patient survival in transitional cell carcinoma.
Additional file 5. Supplementary Table 4.
Univariate and multivariate cox regression analysis for progression-free survival in transitional cell carcinoma.
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Gu, S., Yang, C. Serum lactate dehydrogenase level predicts the prognosis in bladder cancer patients. BMC Urol 23, 65 (2023). https://doi.org/10.1186/s12894-023-01239-0
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DOI: https://doi.org/10.1186/s12894-023-01239-0