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Loss of E cadherin in bladder cancer and its effects on lymphoepithelial interactionsCresswell, Joanne January 2002 (has links)
No description available.
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An evaluation of the chemosensitivity of superficial bladder cancer using the comet assayWalsh, Ian Kinsella January 1997 (has links)
No description available.
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Urinary Bladder Carcinoma – Studies of Outcome of Current Management and Experimental TherapyGårdmark, Truls January 2006 (has links)
<p>The thesis concerns the epidemiology, current and possible future treatment of urothelial cancer of the urinary bladder. The Swedish National Quality Registry for Bladder Cancer 1997-2001 was used to explore epidemiology, current therapies and outcome. More common in men, the incidence for Ta and T1 tumours peaks in the age range 70-79 years. There were differences in treatment activity between the reporting regions. An increasing activity was seen. Older patients received less intravesical treatment, which was also a tendency for women. The five year relative survival for all stages (Ta-T4) was 70%; 93% for Ta and 75% for T1. For Ta or T1 survival did not differ significantly between regions. Because the registry has only been running since 1997 a long term follow-up (ten years) of 250 patients comparing Bacillus Calmette-Guerin and Mitomycin-C, was performed. No differences regarding complementary treatment, progression or survival (overall or disease specific) were shown. Looking for new drugs, gemcitabine was tried for intravesical instillations. Patients were randomised to one of three dose schedules. The effect on a marker tumour lesion was evaluated after nine weeks. The overall complete response rate was 31% (9/29). Side effects were more common in women but generally mild; the most common was nausea. One patient stopped instillations (nausea and fever). No patients were excluded due to pathological changes in laboratory parameters. For metastasised disease, over-expression of the growth factor receptor HER2 on urothelial cancer cells was explored in primary tumours and metastases, aiming at radionuclide target therapy. With a new antigen retrieval procedure and evaluation protocol 80% of primary tumours overexpressed the receptor and 72% remained so in the metastases. In conclusion current therapies were increasingly used by clinicians. Superiority for BCG could not be proven. Prerequisites for new therapies have been explored and the way has been paved for future studies.</p>
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Urinary Bladder Carcinoma – Studies of Outcome of Current Management and Experimental TherapyGårdmark, Truls January 2006 (has links)
The thesis concerns the epidemiology, current and possible future treatment of urothelial cancer of the urinary bladder. The Swedish National Quality Registry for Bladder Cancer 1997-2001 was used to explore epidemiology, current therapies and outcome. More common in men, the incidence for Ta and T1 tumours peaks in the age range 70-79 years. There were differences in treatment activity between the reporting regions. An increasing activity was seen. Older patients received less intravesical treatment, which was also a tendency for women. The five year relative survival for all stages (Ta-T4) was 70%; 93% for Ta and 75% for T1. For Ta or T1 survival did not differ significantly between regions. Because the registry has only been running since 1997 a long term follow-up (ten years) of 250 patients comparing Bacillus Calmette-Guerin and Mitomycin-C, was performed. No differences regarding complementary treatment, progression or survival (overall or disease specific) were shown. Looking for new drugs, gemcitabine was tried for intravesical instillations. Patients were randomised to one of three dose schedules. The effect on a marker tumour lesion was evaluated after nine weeks. The overall complete response rate was 31% (9/29). Side effects were more common in women but generally mild; the most common was nausea. One patient stopped instillations (nausea and fever). No patients were excluded due to pathological changes in laboratory parameters. For metastasised disease, over-expression of the growth factor receptor HER2 on urothelial cancer cells was explored in primary tumours and metastases, aiming at radionuclide target therapy. With a new antigen retrieval procedure and evaluation protocol 80% of primary tumours overexpressed the receptor and 72% remained so in the metastases. In conclusion current therapies were increasingly used by clinicians. Superiority for BCG could not be proven. Prerequisites for new therapies have been explored and the way has been paved for future studies.
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Avaliação do bacilo de Calmette-Guérin recombinante expressando o antígeno S1PT no tratamento do carcinoma urotelial de bexiga em modelo experimental / Evaluation of recombinant bacillus Calmette-Guérin expressing S1PT in the treatment of urothelial bladder carcinoma in an experimental modelChade, Daher Cezar 19 December 2008 (has links)
Introdução: A imunoterapia intravesical com o bacilo de Calmette-Guérin (BCG) é o tratamento adjuvante de escolha no câncer superficial de bexiga. Recentemente, os estudos do mecanismo imunoterápico do BCG têm permitido identificar as reações imunológicas e os genes associados ao efeito antitumoral, possibilitando a produção de vacinas recombinantes, possivelmente mais efetivas e com menos efeitos colaterais. Com esses objetivos, associou-se o componente pertussis (S1PT) ao BCG, criando uma variante recombinante (rBCG-S1PT) com capacidade para promover uma resposta imune direcionada ao tipo T helper 1 (Th1), o que poderá elevar a eficácia antitumoral do imunoterápico. Objetivo: Avaliar comparativamente o efeito antitumoral do rBCG-S1PT e do BCG no modelo experimental de carcinoma urotelial de bexiga. Métodos: O estabelecimento do modelo murino ortotópico e singênico de tumor vesical foi realizado através da implantação transuretral das células tumorais de bexiga da linhagem MB49 de camundongo C57BL/6. Experimento I Os animais (modelo experimental) foram divididos em três grupos, os quais receberam 4 aplicações semanais de rBCG-S1PT, BCG, ou soro fisiológico (grupo controle), por via intravesical. Após 7 dias da última aplicação, foram extraídos o baço e a bexiga, com o intuito de inferir o peso tumoral. Em seguida, as bexigas foram submetidas à avaliação do padrão de resposta imunológica e exame anátomo-patológico e imunohistoquímico. Experimento II Realizado como descrito no Experimento I, porém os animais foram acompanhados por 60 dias para análise de sobrevida. Experimento III Este ensaio foi realizado como descrito anteriormente, porém não foi realizada a implantação tumoral, para controle dos achados imunológicos e anátomo-patológicos. Resultados: A taxa média de implantação tumoral foi de aproximadamente 90% dos animais inoculados. Obtivemos redução das médias dos pesos vesicais dos grupos BCG e rBCG-S1PT (p<0,001). Nos dois grupos tratados com os imunoterápicos observou-se aumento significativo da expressão de TNF-, a qual foi mais intensa com o uso do rBCGS1PT (p<0,05). A IL-10 também teve aumento significante de sua expressão no grupo BCG recombinante (p<0,01). Os esplenócitos provenientes dos camundongos que foram tratados com imunoterápicos diminuíram a viabilidade das células tumorais MB49, sendo que este efeito foi mais intenso no grupo rBCG-S1PT. O grupo de animais tratados com rBCG-S1PT apresentou aumento significativo da sobrevida em relação aos outros grupos (Experimento II). As aplicações dos imunoterápicos em animais sem tumor (experimento III) não revelaram diferenças histológicas em relação ao grupo controle e o padrão de resposta imunológica encontrado sugere uma tendência à resposta Th1. Conclusão: Obtivemos sucesso no estabelecimento do modelo murino ortotópico singênico de tumor vesical. O imunoterápico rBCG-S1PT apresentou mais benefícios no tratamento do tumor vesical ortotópico em camundongos em relação ao BCG, como também maior redução da viabilidade das células tumorais in vitro. A cepa rBCG-S1PT apresentou elevação significativamente maior das citocinas da resposta imune Th1 em relação aos demais grupos. Concluimos, então, que os dados apresentados sugerem a possibilidade deste recombinante proporcionar melhor controle clínico do tumor vesical em humanos que a imunoterapia com BCG / Introduction: The intravesical immunotherapy with bacillus Calmette-Guérin (BCG) is the adjuvant treatment of choice in superficial bladder cancer. Recently, studies of the mechanism of BCG have identified the immune reactions favorable and the genes responsible for the antitumor effect, enabling the production of recombinant vaccines, possibly more effective and with fewer side effects. With those goals, the pertussis toxin (S1PT) was combined to BCG, creating a recombinant variant (rBCG-S1PT) with the capacity to promote an immune response targeted to the T helper type 1 (Th1), which may increase the effectiveness of its antitumor effect. Objective: Compare the antitumor effects of rBCG-S1PT and BCG in an experimental model of bladder cancer. Methods: The development of the animal model of bladder cancer was conducted by transurethral instillation of bladder tumor cell line MB49 of the mouse strain C57BL/6, setting the orthotopic and syngeneic murine model. Experiment I - The animal models were divided into three groups, which received 4 weekly intravesical applications of rBCG-S1PT, BCG, or saline (SF - control group). After 7 days of the last instillation, splenectomy was performed for splenocyte culture and the bladders extracted and weighed in order to infer the tumor weight. Then, the bladders were divided into two pieces. The first was used for molecular analysis to assess the pattern of immune response. The second was sent to histopathological analysis. Experiment II - Held as described in Experiment I, but the animals were monitored for 60 days for analysis of survival. Experiment III - This test was carried out as previously described (Experiment I), but with no tumor cells instillation. Results: The rate of tumor implantation was 90% of the animals submitted to tumor inoculation. We obtained reduction of the average weights of bladder in groups BCG and rBCG-S1PT ((p<0,001). In both groups treated with immunotherapy, there was an increase of expression of interleukins TNF-, which was more intense in the group treated with rBCG-S1PT (p<0,05). There was also increased expression of IL-10 in the recombinant BCG (p<0,01). The splenocytes from animals that received immunotherapies had reduced tumor cells viability, more intensely demonstrated in the rBCG-S1PT group. The analysis of survival showed a significant increase in the group of animals treated with rBCGS1PT (Experiment II). The instillation of immunotherapeutic agents in animals without tumor did not demonstrate histological differences when compared to the control group and the immunological response pattern was similar to that of Experiment I (Experiment III). Conclusion: The establishment of the syngeneic orthotopic animal model was successful. The immunotherapy with rBCG-S1PT demonstrated more benefits than BCG in the treatment of bladder cancer in mice, reducing the bladder weight, increasing survival, and reducing tumor cells viability in vitro. The immune response obtained with the rBCG-S1PT expressed higher cytokines related to Th1. All this data may indicate that this recombinant agent may promote better bladder tumor control than BCG imunotherapy
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Avaliação do bacilo de Calmette-Guérin recombinante expressando o antígeno S1PT no tratamento do carcinoma urotelial de bexiga em modelo experimental / Evaluation of recombinant bacillus Calmette-Guérin expressing S1PT in the treatment of urothelial bladder carcinoma in an experimental modelDaher Cezar Chade 19 December 2008 (has links)
Introdução: A imunoterapia intravesical com o bacilo de Calmette-Guérin (BCG) é o tratamento adjuvante de escolha no câncer superficial de bexiga. Recentemente, os estudos do mecanismo imunoterápico do BCG têm permitido identificar as reações imunológicas e os genes associados ao efeito antitumoral, possibilitando a produção de vacinas recombinantes, possivelmente mais efetivas e com menos efeitos colaterais. Com esses objetivos, associou-se o componente pertussis (S1PT) ao BCG, criando uma variante recombinante (rBCG-S1PT) com capacidade para promover uma resposta imune direcionada ao tipo T helper 1 (Th1), o que poderá elevar a eficácia antitumoral do imunoterápico. Objetivo: Avaliar comparativamente o efeito antitumoral do rBCG-S1PT e do BCG no modelo experimental de carcinoma urotelial de bexiga. Métodos: O estabelecimento do modelo murino ortotópico e singênico de tumor vesical foi realizado através da implantação transuretral das células tumorais de bexiga da linhagem MB49 de camundongo C57BL/6. Experimento I Os animais (modelo experimental) foram divididos em três grupos, os quais receberam 4 aplicações semanais de rBCG-S1PT, BCG, ou soro fisiológico (grupo controle), por via intravesical. Após 7 dias da última aplicação, foram extraídos o baço e a bexiga, com o intuito de inferir o peso tumoral. Em seguida, as bexigas foram submetidas à avaliação do padrão de resposta imunológica e exame anátomo-patológico e imunohistoquímico. Experimento II Realizado como descrito no Experimento I, porém os animais foram acompanhados por 60 dias para análise de sobrevida. Experimento III Este ensaio foi realizado como descrito anteriormente, porém não foi realizada a implantação tumoral, para controle dos achados imunológicos e anátomo-patológicos. Resultados: A taxa média de implantação tumoral foi de aproximadamente 90% dos animais inoculados. Obtivemos redução das médias dos pesos vesicais dos grupos BCG e rBCG-S1PT (p<0,001). Nos dois grupos tratados com os imunoterápicos observou-se aumento significativo da expressão de TNF-, a qual foi mais intensa com o uso do rBCGS1PT (p<0,05). A IL-10 também teve aumento significante de sua expressão no grupo BCG recombinante (p<0,01). Os esplenócitos provenientes dos camundongos que foram tratados com imunoterápicos diminuíram a viabilidade das células tumorais MB49, sendo que este efeito foi mais intenso no grupo rBCG-S1PT. O grupo de animais tratados com rBCG-S1PT apresentou aumento significativo da sobrevida em relação aos outros grupos (Experimento II). As aplicações dos imunoterápicos em animais sem tumor (experimento III) não revelaram diferenças histológicas em relação ao grupo controle e o padrão de resposta imunológica encontrado sugere uma tendência à resposta Th1. Conclusão: Obtivemos sucesso no estabelecimento do modelo murino ortotópico singênico de tumor vesical. O imunoterápico rBCG-S1PT apresentou mais benefícios no tratamento do tumor vesical ortotópico em camundongos em relação ao BCG, como também maior redução da viabilidade das células tumorais in vitro. A cepa rBCG-S1PT apresentou elevação significativamente maior das citocinas da resposta imune Th1 em relação aos demais grupos. Concluimos, então, que os dados apresentados sugerem a possibilidade deste recombinante proporcionar melhor controle clínico do tumor vesical em humanos que a imunoterapia com BCG / Introduction: The intravesical immunotherapy with bacillus Calmette-Guérin (BCG) is the adjuvant treatment of choice in superficial bladder cancer. Recently, studies of the mechanism of BCG have identified the immune reactions favorable and the genes responsible for the antitumor effect, enabling the production of recombinant vaccines, possibly more effective and with fewer side effects. With those goals, the pertussis toxin (S1PT) was combined to BCG, creating a recombinant variant (rBCG-S1PT) with the capacity to promote an immune response targeted to the T helper type 1 (Th1), which may increase the effectiveness of its antitumor effect. Objective: Compare the antitumor effects of rBCG-S1PT and BCG in an experimental model of bladder cancer. Methods: The development of the animal model of bladder cancer was conducted by transurethral instillation of bladder tumor cell line MB49 of the mouse strain C57BL/6, setting the orthotopic and syngeneic murine model. Experiment I - The animal models were divided into three groups, which received 4 weekly intravesical applications of rBCG-S1PT, BCG, or saline (SF - control group). After 7 days of the last instillation, splenectomy was performed for splenocyte culture and the bladders extracted and weighed in order to infer the tumor weight. Then, the bladders were divided into two pieces. The first was used for molecular analysis to assess the pattern of immune response. The second was sent to histopathological analysis. Experiment II - Held as described in Experiment I, but the animals were monitored for 60 days for analysis of survival. Experiment III - This test was carried out as previously described (Experiment I), but with no tumor cells instillation. Results: The rate of tumor implantation was 90% of the animals submitted to tumor inoculation. We obtained reduction of the average weights of bladder in groups BCG and rBCG-S1PT ((p<0,001). In both groups treated with immunotherapy, there was an increase of expression of interleukins TNF-, which was more intense in the group treated with rBCG-S1PT (p<0,05). There was also increased expression of IL-10 in the recombinant BCG (p<0,01). The splenocytes from animals that received immunotherapies had reduced tumor cells viability, more intensely demonstrated in the rBCG-S1PT group. The analysis of survival showed a significant increase in the group of animals treated with rBCGS1PT (Experiment II). The instillation of immunotherapeutic agents in animals without tumor did not demonstrate histological differences when compared to the control group and the immunological response pattern was similar to that of Experiment I (Experiment III). Conclusion: The establishment of the syngeneic orthotopic animal model was successful. The immunotherapy with rBCG-S1PT demonstrated more benefits than BCG in the treatment of bladder cancer in mice, reducing the bladder weight, increasing survival, and reducing tumor cells viability in vitro. The immune response obtained with the rBCG-S1PT expressed higher cytokines related to Th1. All this data may indicate that this recombinant agent may promote better bladder tumor control than BCG imunotherapy
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Prolonged Modulation of the Micturition Reflex by Electrical StimulationJiang, Chong-He January 1999 (has links)
Intravesical electrical stimulation (IVES) has been used in treatment of patients with urinary bladder dysfunctions for more than four decades. While some investigators have reported excellent results others have observed less convincing effects or outright failures. The discrepancies may reflect differences in patient selection or stimulation procedure. A better theoretical understanding of the IVES working mechanism might help to improve the success rate of the treatment. The aims of the present study were to provide such information. Experiments were performed on adult female cats and rats under /alpha/-chloralose anesthesia. IVES was delivered by a catheter electrode in the bladder. At proper intensity and frequency, IVES evoked reflex detrusor contractions that were abolished by bilateral rhizotomy of sacral dorsal roots. Stimulation parameters and response characteristics revealed that bladder mechanoreceptor A/delta/ afferents were activated by the IVES, the same afferents that drive the normal micturition reflex. Five minutes of continues IVES at 20 Hz induced a prolonged, significant decrease in the micturition threshold volume of anesthetized rats. Similarly, selective bladder A/delta/ afferent stimulation induced a long-lasting enhancement of micturition reflex discharges in cats. A comparable prolonged inhibitory effect on the micturition reflex was demonstrated after ano-genital afferent stimulation. Both modulatory effects occurred without changes in response sensitivity of stimulated afferents. The IVES induced modulation was prevented by transient exposure of the bladder to a local anesthetic and by systemic administration of a glutamate NMDA receptor antagonist. In conclusion, IVES induces a prolonged modulation of the micturition reflex by an LTP like enhancement of excitatory synaptic transmission in the central micturition reflex pathway. The findings provide an experimental explanation for the neuronal mechanisms underlying the curative effect of IVES in patients with bladder evacuation problems. / On the day of the public defence the status of article V was: Accepted.
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Mechanisms of Resistance to BCG Immunotherapy in Bladder Cancer / Mécanismes de résistance au BCG des cancers de la vessieRouanne, Mathieu 23 October 2019 (has links)
Le cancer de la vessie est le 9ème cancer le plus fréquent avec 435 000 nouveaux cas diagnostiqués chaque année et 165 000 décès par an dans le monde. Au diagnostic, 70-80% des cancers de la vessie sont tumeurs superficielles n’infiltrant pas le muscle vésical (TVNIM). Depuis près de 40 ans, les instillations intra-vésicales de bacille de Calmette-Guérin (BCG) sont le traitement de référence des TVNIM ayant un risque élevé de progression (T1, carcinome in situ, Ta haut grade). Malgré un traitement bien conduit, le taux de récidive est d'environ 50%, et la progression vers une tumeur infiltrant le muscle est estimé à 20%-30% dans les 5 ans. Jusqu’à 15% des patients développent des métastases de leur carcinome urothélial. Aujourd’hui, aucun biomarqueur ne permet de prédire la réponse au BCG, ni l’évolution métastatique de la maladie. La cystectomie totale reste le traitement de référence en cas de non-réponse au BCG. Plusieurs essais cliniques évaluent des traitements immuno-modulateurs ciblant les points de contrôle immunitaires PD1, PD-L1 en 2° ligne de traitement après échec du BCG. Les instillations endo-vésicales d’adénovirus recombinant, de virus oncolytique ou d'agoniste de la voie STING sont des stratégies thérapeutiques en cours d'évaluation. L'objectif de ce travail était d'étudier les mécanismes de résistance intrinsèques des cellules tumorales exposées au BCG afin d'identifier de nouvelles cibles thérapeutiques. / Bladder cancer is a heterogeneous disease that displays invasive and non-invasive histological features, and a wide spectrum of molecular alterations and subtypes. Treatment of non-invasive tumors with high-risk features (carcinoma in situ, high-grade Ta, T1) includes trans-urethral resection of the tumor, followed by intravesical instillations of bacillus Calmette-Guérin (BCG). Despite a multitude of evidence for anti-tumor efficacy, 50% of patients with high-risk NMIBC develop tumor recurrence and 20-30% disease progression. Ultimately, 10-15% of patients die of metastatic disease. New therapeutic strategies are currently in clinical development to treat BCG-unresponsive tumors including antagonistic antibodies directed against the T-cell immune checkpoints PD-1, PD-L1 and CTLA-4, but also recombinant adenovirus interferon α (Ad-IFNα/Syn3), oncolytic virus and STING agonists. Although recent studies have identified potential immune parameters that could impact clinical response, mechanisms of tumor resistance to BCG immunotherapy remain poorly understood. Additionally, tumor heterogeneity and plasticity of cancer cells undermine our attempts to precise dynamics of immune escape under selective pressure. How cancer cells evade to the anti-tumor immune response, and whether cancer cells acquire intrinsic undesirable characteristics upon BCG exposure remain unknown. Altogether, this highlights the crucial need to better understand the mechanisms of tumor resistance that occur during BCG immunotherapy in order to identify new targetable pathways and treatment strategies.
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Response of multiple recurrent TaT1 bladder cancer to intravesical apaziquone (EO9): Comparative analysis of tumour recurrence rates.Jain, A., Phillips, Roger M., Scally, Andy J., Lenaz, G., Beer, M., Puri, Rajiv January 2009 (has links)
No / Objectives
Previous studies have demonstrated that intravesical administration of apaziquone (EOquin) has ablative activity against superficial bladder cancer marker lesions with 8 out of 12 complete responses recorded. We present a comparison between the rates of tumor recurrence before and after treatment with apaziquone.
Methods
The rate of tumor recurrence after treatment with apaziquone was compared with each patient's historical record of recurrences obtained from a retrospective analysis of the patients' case notes. The time to each recurrence event before apaziquone treatment and the time to the first recurrence after apaziquone treatment were recorded, and the data were analyzed using a population-averaged linear regression model using Stata Release, version 9.2, software.
Results
Of the eight complete responses obtained in the Phase I study, tumor recurrence occurred in 4 patients and the remaining 4 patients remained disease free after a median follow-up of 31 months. The time to the first recurrence after apaziquone treatment was significantly longer (P <0.001) compared with the historical pattern and recurrence interval before apaziquone. Before apaziquone instillation, the mean ± SE recurrence rate and tumor rate per year was 1.5 ± 0.2 and 4.8 ± 1.2, respectively, and these decreased to 0.6 ± 0.25 and 1.5 ± 0.8, respectively, after apaziquone treatment (P <0.05).
Conclusions
The results of this study indicate that early recurrences after treatment with apaziquone are infrequent and the interval to recurrence is significantly greater compared with the historical recurrence times for these patients. Larger prospective randomised trials are warranted to confirm these results.
Aapaziquone (EOquin, USAN, E09, 3-hydroxy-5-aziridinyl-1-methyl-2[indole-4,7-dione]¿prop-¿-en-¿-ol) belongs to a class of anticancer agents known as bioreductive drugs that require metabolism by cellular reductases to generate a cytotoxic species.1 Although it is chemically related to mitomycin C, apaziquone has a distinctly different mechanism of action and preclinical activity profile.1 and 2 The initial optimism generated by its preclinical activity profile rapidly evaporated after the demonstration that intravenously administered apaziquone was clinically inactive against a range of solid tumors in Phase II clinical trials.3 and 4 Several possible explanations were considered for its lack of efficacy, but poor drug delivery to the tumor because of the rapid pharmacokinetic elimination of apaziquone in conjunction with relatively poor penetration through avascular tissue was considered to be the principal reason.5 On the basis of the rationale that intravesical administration would circumvent the problem of drug delivery and any apaziquone absorbed into the blood stream would be rapidly cleared,6 a Phase I-II clinical pilot study of intravesical administration of apaziquone to superficial bladder tumors was established.7 The results of that trial demonstrated that intravesically administered apaziquone has ablative activity against superficial bladder transitional cell carcinoma (TCC) marker lesions.7 These results were confirmed and extended in a Phase II clinical trial of 47 patients with superficial bladder TCC, in which complete responses were obtained in 67% of patients.8 Because all the enrolled patients in the original trial7 had had multiple recurrences after previous intravesical chemotherapy and/or immunotherapy, the purpose of the present study was, first, to report the recurrences that occurred after apaziquone treatment and, second, to study the effect of apaziquone instillation on the recurrence rate by statistically comparing these results with the historical pattern of recurrences for each patient before treatment with apaziquone.
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