Expression of epithelial-Mesenchymal transition related markers in Plasmacytoid Urothelial carcinoma of the urinary bladder

Plasmacytoid urothelial carcinoma (PUC) of the urinary bladder was first reported in 1991 as a similar histological type to plasma cell [1]. The World Health Organization (WHO) working group classified PUC as a variant of urothelial carcinoma (UC). These tumor cells have eosinophilic cytoplasm and eccentrically placed, enlarged hyperchromatic nuclei with small nucleoli [2]. The prognosis of PUC of the bladder is worse than that of conventional UC [3]. However, why PUC is more aggressive is unknown.

Later inquire about proposes that the epithelial-mesenchymal transition (EMT) is a vital figure related to tumor progression and metastasis [4, 5]. EMT could be a handle at first watched in embryonic improvement in which cells lose epithelial characteristics and pick up mesenchymal properties to extend motility and invasion [4]. Besides, a later ponder detailed that Snail could be a key controller of EMT [6]. Snail is a superfamily of zinc-finger transcription factors that was, to begin with distinguished in Drosophila melanogaster [7]. Snail actuates EMT, in portion, by straighforwardly repressing epithelial markers such as E-cadherin and by upregulating mesenchymal markers such as N-cadherin, Vimentin, and Fibronectin. Immunohistochemistry has appeared downregulated or negative E-cadherin expression in the majority of PUC [3, 8]. Hence, PUC may actuate EMT. Therefore, EMT may be associated with PUC progression. The present study examined the expression status of EMT-related markers (E-cadherin, N-cadherin, Vimentin, Fibronectin and Snail) in PUC.

Whether survival is related to the proportion of plasmacytoid variant histology is unknown. Thus, we assessed the association between the proportion of plasmacytoid variant histology and survival in PUC patients. Furthermore, we also report clinical outcome information.

PUC is recognized as a rare and aggressive variant of UC, which often presents at a high stage and carries a poor prognosis [3]. Sahin et al. first described this tumor in 1991 [1]. Mai et al. reported an incidence of 2.7% of PUC in a series of muscle invasive UC [9]. In this study, 9 of 12 tumors were invasive. 9 of 12 PUC patients died during follow-up. The median age at diagnosis was 71 years, a finding similar to other recent reports. We recognized that the poor prognoses of these cases are due to the high invasion and the high clinical stage at presentation [3]. However, it is unclear how often PUC shows high invasion.

EMT is an essential step amid epithelial tumor metastasis [10]. EMT causes changes in cell-cell and cell-extracellular matrix interactions coming about in transmigration of cancer cells, in this way driving to metastasis [11, 12]. E-cadherin may be a cell-cell intersection protein that is regularly downregulated or misplaced amid EMT, while expression of N-cadherin, Vimentin, Fibronectin, and Snail are obtained amid this process. In this study, E-cadherin expression was largely negative, while N-cadherin, Vimentin, Fibronectin and Snail were mostly positive. The present study reported a possibility of EMT in PUC.

E-cadherin is a key structure protein in maintaining both the stability of adhesion between epithelial cells and the stability of tissues [13]. Recent studies have demonstrated that loss of E-cadherin expression may correlate with high grade and advanced stage of UC [14, 15]. Other studies reported that the majority of PUC cases show low E-cadherin expression [3, 8]. Keck et al. reported that most PUC with loss of membranous E-cadherin show a nuclear accumulation of E-cadherin. E-cadherin also serves as an independent prognostic factor for reduced overall survival of patients with muscle-invasive bladder cancer who were treated with radical cystectomy and adjuvant chemotherapy [16]. In this study, 10 of 12 cases (83.3%) showed largely negative membranous E-cadherin.

Snail is considered a fundamental controller of EMT and, thus, of tumor movement. Bruyere et al. detailed that Snail expression predicts tumor recurrence in superficial bladder cancer [17]. Kosaka et al. reported that Snail expression might be a prognostic indicator of disease-free survival and disease-specific survival in upper urinary tract UC [18]. We moreover already detailed that Snail expression may anticipate poor results in bladder cancer patients treated with neoadjuvant chemotherapy [19]. In this study, Snail was mostly positive in 83.3%. PUC also may predict the poor outcome by Snail. Further studies with a large cohort of PUC patients are needed to confirm this result.

Fibronectin is an essential component of extracellular matrix. It has been found highly expressed in a few kinds of cancer, indicating a potential role in progression [20, 21]. Malmstrom et al. reported the level of urine fibronectin in bladder cancer patients were significantly higher than that in patients with benign urothelial diseases and the health groups [22]. Furthermore, muscle invasive bladder cancer patients have a significantly higher level of urine fibronectin [23]. In this study, fibronectin was all negative in the patient had no progression. Although our study is the small number of cases, fibronectin may predict the recurrence of PUC patients.

CD138 expression has been reported as a specific marker for PUC. However, Goto et al. reported the frequency of CD138 positivity in PUC was relatively low, compared with that observed in the conventional types and other variants [24]. In this study, CD138 was negative in all cases. Therefore, PUC should be correctly diagnosed using their characteristic cytomorphology.

Whether survival is related to the proportion of plasmacytoid variant histology has been unknown. Here we assessed the association between the proportion of plasmacytoid variant histology and survival in PUC patients. Analysis of the correlation between the amount of PUC and outcome revealed that the three patients with < 10% plasmacytoid component did not die from cancer, while eight of the nine patients (88.9%) with > 10% plasmacytoid component died from disease. This result may demonstrate the importance in identifying the amount of PUC.

It remains unknown how PUC patients should be treated. Qiang et al. reported PUC was not associated with worse overall mortality compared with pure UC on multivariable analysis in a large cohort of patients treated with radical cystectomy [25]. Radical cystectomy may improve survival for patients with PUC. In this study, only four PUC patients underwent radical cystectomy and three patients underwent only TURBT. Radical cystectomy should be considered as the first line choice for PUC.

Our study is the first to elucidate immunohistochemical evidence of EMT in PUC. PUC may induce EMT and may be associated with high invasion. More detailed studies are needed to address this question.