Abstract
Background/Aim: Bladder cancer can spread from the sub-peritoneal space superior and posterolateral to the peritoneal cavity via the peritoneal lining. The aim of this study was to improve the identification of peritoneal spread from bladder urothelial carcinoma based on computed tomography (CT) scans. Materials and Methods: This is a retrospective study including patients selected with the following criteria: (i) pathology-confirmed urothelial carcinoma; (ii) peritoneal spread identified on CT scans from axial and corona views, either initially or after radical/partial cystectomy, concomitant chemoradiotherapy (CCRT), or radiotherapy. One hundred and fifty-nine cases met the selection criteria. Results: Routes of spread to the peritoneum included the superior to anterior direction in 59 patients (37%), the superior to posterolateral direction in 19 (12%), and the superior to both anterior and posterolateral directions in 81 (51%). Invasion of specific sites included the abdominal wall in 101 patients (70%), bowel/mesentery in 84 (53%), prostate, uterus, and rectum in 30 (19%), and circumferential tumors that outlined the whole bladder wall in 59 (37%). Initial modes of therapy were chemotherapy in 86 patients (54%), cystectomy in 55 (35%), CCRT in eight (5%), radiotherapy in two (1%), and no therapy in eight (5%). Peritoneal spread due to under-staging (clinical/pathological stage) after local therapy was found in 84 patients (53%). Conclusion: Initial pre-therapeutic staging is easily overlooked regarding peritoneal spread from bladder urothelial carcinoma. Combined axial and coronal views of CT scans can help identify peritoneal involvement.
The bladder is a sub-peritoneal organ, whereby the peritoneum covers the posterosuperior surface of the bladder. Along the lateral margins, the peritoneum passes onto the lateral walls of the pelvis, while the anterior, lateral, and lower parts of the posterior surface are devoid of peritoneum (1). The peritoneum is divided into two types: the visceral and parietal peritoneum. The parietal peritoneum is attached to the abdominal and the pelvic wall (1). Hence, bladder cancer can spread from the sub-peritoneal space superior and posterolateral to the peritoneal cavity via the peritoneal lining.
According to the 7th edition of the American Joint Committee on Cancer (AJCC) TNM system, stage T4b bladder cancer describes a tumor that has spread to the pelvic or abdominal wall (2). Tumors can enter the abdominal wall from the bladder dome and the peritoneum and can invade the pelvic sidewall from the posterolateral bladder wall and/or involve the peritoneal reflection (3, 4). Spread of bladder urothelial carcinoma to the peritoneum is encountered (3-8). Peritoneal involvement is a metastatic disease. According to EUA (European association of Urology) guideline, local therapy such as radical cystectomy, radiation or concomitant chemoradiotherapy (CCRT) are inadequate. Cisplatin-based combination chemotherapy is standard of mode in fit patients (9).
Computed tomography (CT) scans are useful for determining the stage or extent of bladder cancer (10-12). Lee et al. reported that accurate local staging of bladder urothelial carcinoma is crucial for management (10). Raman SP et al. reported the underrated role of CT scans in bladder malignancies (11). However, identifying peritoneal spread before treatment to determine the best course of action is difficult. In this case series study, bladder urothelial carcinoma with peritoneal involvement was investigated by retrospectively reviewing CT scans.
Materials and Methods
Study population. A retrospective case series study was conducted using data collected from patients with bladder cancer admitted to the oncology wards of Chang-Gung Memorial Hospital, Taoyuan, Taiwan, between January 2010 and December 2016. A single medical oncologist specializing in urological cancer provided most of the data, and the majority of the patients had urothelial carcinomas. They were all hospitalized patients because they needed to undergo chemotherapy. The criteria for inclusion were: (1) pathology-confirmed diagnosis of urothelial carcinoma and (2) peritoneal spread identified on CT scans from the axial and coronal views performed either initially or after radical/partial cystectomy, CCRT (concomitant chemoradiotherapy), or radiotherapy. All pre-therapy CT scans for each case were discussed in our urological cancer team meetings. Chemotherapy regimens included 5-fluorouracil, leucovorin, cisplatin, and gemcitabine (Gemmis; TTY, Taipei, Taiwan).
Out of the 206 hospitalized bladder cancer patients reviewed, 159 (77%) met the inclusion criteria of this study because they needed to be admitted for chemotherapy. Routes of peritoneal spread, including superior to anterior, superior to posterolateral, and superior to both anterior and posterolateral, and specific site involvement, such as invasion into the abdominal wall, bowel/mesentery, prostate, uterus, and rectum, and circumferential tumors that outlined the whole bladder wall, were determined. The bladder cancer pre-therapeutic tumor extent and stage evaluation was mainly determined from CT scans. Only tumor extent and stage of two patients were determined by magnetic resonance imaging studies. The stage was evaluated according to the 7th edition of the AJCC TNM staging system (2). Peritoneal involvement was detected either initially or after local therapy and usually was symptomatic.
Initial modes of therapy included chemotherapy only, radical/partial cystectomy, CCRT, radiotherapy only, and no therapy. Chemotherapy regimens were 5-fluorouracil, leucovorin, cisplatin, and gemcitabine (Gemmis®; TTY, Taipei, Taiwan). When renal function impairment occurred (serum creatinine greater than 2 mg/dl), chemotherapy with continuous maintenance was administered with carboplatin replacing cisplatin. The schedule of initial CCRT combined radiotherapy with chemotherapy. Radiotherapy of the bladder and pelvic lymphatics used a 10- or 15-MV X-ray dose with a parallel-opposed anteroposterior or four-field box beam. The total dose was 44-45 Gy in 22-26 fractions and further boosted to a total dose of 60-61.2 Gy.
Results
One hundred and fifty-nine consecutive bladder cancer patients, including 104 men and 55 women (range=40–93 years; median age: 69), met the selection criteria for this study. The patients' clinical characteristics are shown in Table I. These patients had peritoneal involvement with various tumor extents. Routes of spread to the peritoneum included the superior to anterior direction in 59 patients (37%), superior to posterolateral in 19 (12%), and superior to both anterior and posterolateral in 81 (51%). For invasion of specific sites, 101 patients (70%) had a tumor in the abdominal wall, 84 (53%) in the bowel/mesentery, 30 (19%) in the prostate, uterus, and rectum, and 59 (37%) had a circumferential tumor that outlined the whole bladder wall.
Different types of spread were diagnosed. CT scans from axial and coronal views can help detect peritoneal spread. Bladder tumor spread in the superior to anterior direction are demonstrated in Figures 1, 2 and 3. A bladder tumor with intestinal and abdominal wall invasion is shown in Figure 1. Figure 2 shows a bladder tumor with intestinal invasion and urine leakage into the abdominal cavity. A bladder tumor with mesenteric metastasis is seen in Figure 3 and bladder tumor spread in the superior to posterolateral direction in Figures 4 and 5. A bladder tumor with obvious superior and posterolateral invasion is shown in Figure 4, a bladder tumor with mesenteric metastasis in Figure 5, and a bladder tumor spread in the superior to both anterior and posterolateral directions in Figures 6 and 7. A bladder tumor with prostate invasion shown in Figure 6 reveals a circumferential bladder tumor that outlines the entire bladder wall (Figure 7).
The study included 7 patients with simultaneous bladder and renal pelvis urothelial carcinoma and 12 patients with upper urinary tract urothelial carcinoma who had previously undergone nephroureterectomy. Three cases that have had prior renal transplantation were included in this study.
Initial modes of therapy included chemotherapy in 86 patients (54%), cystectomy in 55 (35%), CCRT in eight (5%), radiotherapy in two (1%), and no therapy in eight (5%). Peritoneal spread due to under-staging (clinical/pathological stage) after radical/partial cystectomy, CCRT, or radiotherapy was found in 84 patients (53%) despite the fact that cases had been discussed at urological cancer team meetings. Tumor staging was determined as T1 in five patients, T2 in 23, T3 in 26, T4a in 19, N1 in eight, and N2 in three.
Discussion
Patterns of bladder urothelial carcinoma with peritoneal involvement are rarely mentioned. Lymph nodes, bones, lung, liver, and peritoneum are the most common sites of metastasis from bladder cancer (5, 6) and T4b bladder cancers are likely to already involve the peritoneum (2-4). However, identifying peritoneal spread before treatment to determine the best course of action is difficult because of a dirty and/or thickened peritoneum don't represent tumor involvement. Black et al. reported that long-term survival can be achieved in some patients with cT4b bladder cancer undergoing chemotherapy and extirpative surgery (13). However, Liberman et al. mentioned that radical cystectomy of pT4b patients had higher cancer-specific mortality (14).
CT scans have a role in the local staging of urothelial carcinoma (10, 11) and are important in the diagnosis of peritoneal spread (7-9). Hence, understanding the anatomy of the peritoneum and bladder is crucial (1). Based on our study, bladder tumors can spread from the bladder dome in a superior to anterior and/or posterolateral direction. Tumors that spread from the superior and anterior extent can invade the intestine/mesentery and abdominal wall, while tumors that spread posterolateral can invade the prostate, uterus, or rectum. Tumors can also be circumferential and outline the whole bladder wall. CT scans from axial and coronal views helped in the detection of peritoneal spread in our cases.
CT scans can influence the initial therapy modality. More than half of our patients had under-staging and underwent local therapy with radical/partial cystectomy, CCRT, or radiotherapy. Patients with clinical under-staging experienced incomplete removal of the bladder tumor or had peritoneal lesions outside the radiation field. These tumors usually progress after local therapy. This is inconsistent with the results of our study, which suggested that CCRT is a feasible and promising treatment for invasive bladder cancer (15). However, recently published articles show that these patients benefit from continuous maintenance of cisplatin-based chemotherapy.
Despite the fact that cases are discussed at urological cancer team meetings, incorrect clinical staging, especially under-staging, is a serious problem in bladder cancers patients, and improvements of the staging process are needed to achieve more accuracy (16, 17). Pathological under-staging of patients is often seen because the cancer is mistaken as T3b (macroscopic extravesicular spread) or T4a (prostate, uterus, or rectum involvement). CT scans with combined axial and coronal views can reduce clinical under-staging, especially regarding peritoneal involvement.
The tumor microenvironment has been shown to impact tumor progression, and key factors have been detected in bladder cancer tissues (18). Evidence suggests that the critical factors of the tumor microenvironment are immune and inflammatory cells, blood and lymphatic vascular networks, fibroblasts, and the extracellular matrix (18). Cancer-associated fibroblasts (CAFs), a major component of the cancer stroma, have a prominent role in the progression, growth, and spread of cancers (19, 20), and can be involved in angiogenesis and the response to injury. A dirty and thickened peritoneum represented cancer cells in the peritoneum; however, the burden of cancer cells and their fibrotic tissue could not be determined.
Our study has several important limitations. First, the data were collected mainly from one physician as a retrospective case cohort study in a single center. Second, the diagnosis of peritoneal involvement was not verified by tissue confirmation.
Conclusion
Initial pre-therapeutic staging is easy to overlook for peritoneal spread from bladder urothelial carcinoma. Combined axial and coronal views of CT scans can help identify peritoneal involvement and avoid clinical under-staging of bladder cancer.
Acknowledgments
The Authors wish to acknowledge the oncology nurse staff for providing the best care for these patients.
Footnotes
This article is freely accessible online.
Conflicts of Interest
The Authors declare no potential conflicts of interest.
- Received March 31, 2018.
- Revision received April 24, 2018.
- Accepted April 25, 2018.
- Copyright© 2018, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved