Background
Bladder cancer is the fourth most common cancer in men, with approximately 60,000 new diagnoses each year [
1], ranking as the eighth leading cause of cancer-related deaths in the United States, with about 12,000 deaths annually [
1]. Specifically, in 2017, there were 79,030 cases of bladder cancer and 16,870 related deaths in the United States [
1]. Approximately 90–95% of all bladder cancer cases are urothelial cell carcinoma, with the minority consisting of non-urothelial cell carcinoma. During initial diagnosis, 70–80% of bladder cancers are diagnosed as non-invasive with the remaining 20–30% diagnosed as invasive. Most cases of non-invasive bladder cancer can be treated with transurethral removal of the bladder tumor (TURB) alone [
2,
3]. However, a high recurrence rate after TURB has been reported within 1 year (15–70%) and 5 years (7–40%) [
2,
3]. Therefore, continuous additional testing and repeated treatments are often needed. Indeed, in the United States, bladder cancer is reportedly one of the tumors for which patients incur a high costof [
2,
3].
Recently, a large-scale, detailed analysis of the molecular genetic characteristics of bladder cancer was reported through The Cancer Genome Atlas (TCGA) [
2,
3]. The TCGA study revealed that bladder cancer can be classified into several subtypes depending on the molecular characteristics of the genomes [
4‐
9]: luminal type, basal type, p53-like tumor, and small cell carcinoma-like tumor. Among these subtypes, the basal type is associated with a particularly poor prognosis [
4‐
9]. Moreover, the basal type and p53-like tumor are highly resistant to preoperative chemotherapy; thus, identifying the accurate subtype is an essential factor in clinical decision-making [
5]. Basal/squamous-like (BASQ) is a basal type of bladder cancer with a very poor prognosis and high rate of resistance to chemotherapy [
5]. It is immunohistochemically defined by CK5/6(+), CK14(+), GATA3(−) and FOXA1(−) expression [
5]. However, there is no report on the treatment response and prognosis of patients with bladder cancer when applying this new classification system. Therefore, in the present study, we evaluated the clinical efficacy and prognosis of MIBC according to the use of the BASQ classification system in clinical practice.
Methods
Ethics
This study was approved by the Institutional Review Board (IRB No. H-1806-081-951). We used the human bladder cancer materials stored in the cancer tissue bank (IRB No. H1307–084-505). We obtained informed consent from all research participants.
Patient populations
A total of 100 patients with muscle-invasive urothelial carcinoma (cT2-4 N0-3 M0) of the urinary bladder were included in the study. Patient selection was based on the availability of sufficient material for immunohistochemistry. All patients underwent TURB followed by radical cystectomy between 2000 and 2012 at Seoul National University Hospital.
Tissue microarray (TMA) construction
Hematoxylin and eosin slides were reviewed for confirmation of the pathologic diagnosis and various pathologic parameters, including invasion depth and grade. We constructed TMA blocks from formalin-fixed paraffin-embedded tissue blocks (Superbiochips Laboratories, Seoul, Korea). In brief, two representative tumor cores (2 mm in diameter) were selected from the viable tumor area. The cancer tissues of patients were examined microscopically by a skilled pathologist, and the TMA was prepared after selecting the most representative cancer tissues. Immunostaining was performed for CK5/6, CK14, FOXA1, and GATA3 antibodies on TMA slides from the 100 patient samples, and the expression patterns were quantitatively analyzed using a scanning program. Based on the expression patterns, the patients were divided according to the BASQ classification (CK5/6, CK14, FOXA1, and GATA3).
The prognostic value of the BASQ classification was determined based on clinical and pathological information such as age, body mass index, sex, American Society of Anesthesiologists (ASA) physical status, pathologic TNM stage, carcinoma in situ status, lymphovascular invasion, margin-positive status, lymph node dissection range, number of removed lymph nodes, number of positive lymph nodes, and neoadjuvant chemotherapy enforcement. We also collected various types of oncological data, including the recurrence, mortality, and cancer-related mortality rates.
Immunohistochemistry (IHC)
IHC staining was performed on 4-μm-thick sections from TMA blocks using the Benchmark XT autostainer (Ventana Medical Systems, Tucson, AZ, USA). The sections were incubated with the following primary antibodies: mouse monoclonal antibodies against CK5/6 (64 min; 1:50; Dako, Glostrup, Denmark), CK14 (32 min; 1:50; Cell Marque, Rocklin, CA, USA), and GATA3 (32 min; 1:500; clone 156-3C11; Cell Marque), and rabbit polyclonal antibody against FOXA1 (16 min; 1:700; ThermoFisher Scientific, Rockford, IL, USA). To interpret the IHC results, the percentage of positively stained tumor cells was semi-quantitatively evaluated into three categories; 0, no positive cells; 1+, 1–10% positive cells; 2+, 11–25% positive cells; 3+, > 25% positive cells.
Statistical analysis
Continuous variables are presented as the median value and interquartile ranges (IQRs) or average value and standard deviations (SDs). Nominal variables are presented as the frequency of events (%). The primary endpoint of the study was the overall survival (OS) rate, and the secondary endpoints were cancer-specific survival (CSS) and recurrence-free survival (RFS). The Kaplan-Meier method was used to predict all survival outcomes, and significance among groups was determined using log-rank tests. Cox proportional hazards regression analysis was used for analysis of various oncology outcomes and predictors. All statistical tests were performed using IBM SPSS Statistics version 22.0 (IBM, Armonk, NY, USA) and STATA version 14 (StataCorp LP, College Station, Texas). A p-value < 0.05 was considered statistically significant.
Discussion
Several recent studies have shown that in addition to the well-known Clinic factors, various antropometric factors have an effect on the outcome of the bladder cancer [
10‐
13]. The recurrence rate of bladder cancer is reported to be significantly higher in obese patients than in normal weight patients [
10,
13]. Metabolic features such as obesity and associated insulin resistance have also been reported to affect prognosis [
13]. High BMI also helps to predict poor prognosis, such as lymph node metastasis [
10]. Immunological and inflammation markers such as basophil count, neutrophil and lymphocyte count, and C-reactive protein are also helpful in predicting recurrence after cystectomy or intravesical Bacillus Calmette-Guérin (BCG) treatment [
11,
12].
In addition to these various antropometric factors, histologic features have been reported to be helpful in predicting the prognosis of bladder cancer. Recent molecular studies have provided new insight into the factors contributing to bladder cancer development and progression. TMAs have been used to analyze genome expression, and immunohistochemical expression patterns are used to classify unique molecular types of bladder cancer. The gene mutations identified to date include genes related to chromatin regulation, cell cycle regulation, and kinase signaling pathways. In particular, molecular insight has been gained with respect to the cell and molecular biology of the urothelium, with 32 gene mutations significantly and repeatedly observed in urothelial cell carcinoma, including genes related to cell cycle regulation, chromatin regulation, and kinase signaling pathways [
5]. In particular, tumor protein 53 (TP53), fibroblast growth factor receptor-3 (FGFR3) mutations, and genes involved in the phosphatidylinositol-3-OH kinase (Pl3K)/protein kinase B (Akt)/mammalian target of rapamycin (mTOR) pathway were found to be associated with the prognosis of bladder cancer [
5].
Besides the specific mutations and pathways, the discovery of molecular subtypes of urothelial cell carcinoma represents another important advance obtained through molecular studies. Several studies on genome expression profiles have reported that bladder cancer can be categorized into two intrinsic molecular types: luminal and basal, which are similar to those in breast cancer [
5,
14,
15]. The molecular subtype of urothelial carcinoma is related to cell differentiation [
16]. Basal type and luminal type are distinguished by keratin markers. The basal type has keratins representing the basal/stem-cell compartment, and the luminal type has keratins representing the umbrella cell layer [
6,
15]. Basal type keratins are associated with the transcription factor ΔNP63, which is related to a poor prognosis of muscle-invasive bladder cancer [
15,
16].
Lindgren et al. [
8] first classified samples from 144 patients with urothelial cell carcinoma according to gene expression patterns. They divided the urobasal group into two subgroups: urobasal A and B, according to their molecular characteristics. Urobasal A was mostly a non-muscle invasive bladder cancer; however, patients with urobasal B showed a progressive phenotype with increased cell cycle activity and basal cell-related keratin expression [
7].
The MD Anderson cohort was classified into basal and luminal types, which included 98 patients with invasive bladder cancers and 34 patients with superficial bladder cancers. The luminal type showed strong expression of markers such as CD24, FOXA1, GATA3, CK20, and XBP1, whereas the basal type was characterized by high-molecular-weight keratins (CK5 and CK14) and strong expression of CDH3 and CD44 [
5,
17].
Thus, the molecular characteristics of urothelial carcinoma can be used to predict the therapeutic effect and prognosis of the patient. McConkey et al.[18] reported that these molecular characteristics could predict the benefits of treatment such as chemotherapy or target agent therapy. Specifically, basal subtypes have been shown to be beneficial in neoadjuvant settings.[18].
Our present study also showed a tendency for a better prognosis in cancers with FOXA1 or GATA3 expression. Conversely, some of the CK14 and CK5/6-positive cases showed a tendency to be correlated with a poor prognosis. CK 14 negatively correlated with OS, CSS, and RFS, and FOXA1 positively correlated with OS and CSS. The expression of CK14 and FOXA1 subtypes seemed to be correlated with oncologic outcomes compared to those of CK56 and GATA3. Indeed, CK14 and FOXA1 expression may be a sensitive criterion for further differentiating urothelial carcinoma. However, our study was limited to 100 subjects and the results may be due to these limited subjects.
The difference in survival outcomes according to the degree of subtype expression was not significantly correlated with oncologic outcomes. However, CK14 and FOXA1 expression was correlated with oncologic outcomes at some yields. FOXA1 expression in the between 1 and 10% group was positively correlated with OS compared to that in the lesser than 1% group, OS (
p = 0.007), CSS (
p = 0.001), and RFS (
p = 0.025) (Fig.
3).
CK14 also showed differences in oncologic outcome of OS and CSS according to subtype expression levels. There was a difference in the oncologic outcomes between the less than 1%, between 11 and 25%, and more than 25% groups. CK14 is negatively correlated with OS, CSS, and RFS according to subtype expression level (Fig.
3).
Even if FOXA1 is statistically significant in multivariate Cox regression analysis, the odd ratio is 0.08 and its impact is unclear. However, CK14 expression was associated with oncologic outcome of OS and CSS. (Table
3).
In the case of basal type cancers (CK14+, CK5/6+, FOXA1-, GATA3-), CK5/6+ and GATA3- were significantly correlated with a poor OS when the CK5/6+ expression rate was > 10%. CK5/6+ and FOXA1- were also significantly correlated with a poor OS and RFS when the CK5/6+ expression rate was > 10 and > 25%. When we defined the basal type according to the new consensus, we found a significant correlation with poor OS, and a tendency toward an association with RFS. This somewhat unclear correlation is likely due to the insufficient number of specimens analyzed in our study. However, this finding suggests a clear relationship between the basal type and a poor prognosis.
This study has some limitations. This study had a retrospective design, and the sample size was relatively small. Therefore, more extensive and prospective studies are needed to verify the observed associations. And we did not consider the number of TURBs or intravesical treatments that could affect the outcome. Nevertheless, it is meaningful that this study applied the newly established BASQ classification to the evaluation of clinical specimens from patients diagnosed with bladder cancer and related the BASQ classification to prognosis. We could also confirm that the basal and luminal types in the BASQ classification are closely related to patient prognosis.
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