Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer

Edmund C.P. Chedgy; James Douglas; Jonathan L. Wright; Roland Seiler; Bas W.G. van Rhijn; Joost Boormans; Tilman Todenhöfer; Colin P. Dinney; Colin C. Collins; Michiel S. Van der Heijden; Peter C. Black

doi:10.1016/j.urolonc.2016.05.012

Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer

Edmund C.P. Chedgy, James Douglas, Jonathan L. Wright, Roland Seiler, Bas W.G. van Rhijn, Joost Boormans, Tilman Todenhöfer, Colin P. Dinney, Colin C. Collins, Michiel S. Van der Heijden, Peter C. Black

Urology

Research output: Contribution to journal › Review article › peer-review

9 Scopus citations

Abstract

Background Bladder cancer is a leading cause of morbidity and mortality. Despite recent advances in understanding its molecular biology, the 5-year survival for muscle-invasive disease (muscle-invasive bladder cancer [MIBC]) remains approximately 50%. Although neoadjuvant chemotherapy (NAC) offers an established 5% absolute survival benefit at 5 years, only the 40% of patients with a major tumor response appear to benefit. There remains, therefore, a critical unmet need for predictive markers to determine which patients are best managed with NAC, as well as for novel targeted therapies to overcome resistance to NAC. Methods The NAC paradigm offers the optimal clinical context for developing precision therapy for MIBC. Abundant tissue is available for analysis before NAC in all patients and after NAC in patients with residual MIBC. Technologic advances have enabled next-generation sequencing and gene expression microarray analysis of routinely collected and even archived tissue specimens. These technologies provide a foundation for the identification of markers of chemoresistance and for the development of rational cotargeting strategies. Results Modern computational methods allow for some measure of target validation, which can be enhanced by the use of patient-derived primary xenografts (PDX). These PDX can be established at the time of radical cystectomy after NAC if there is residual MIBC. By the time a patient recurs clinically, candidate drugs targeting specific molecular changes in the patient tumor and corresponding PDX would have been tested in the PDX model, and only the most efficacious drug(s) would be administered to the patient. Liquid biopsies in the form of circulating tumor DNA and circulating tumor cells allow noninvasive longitudinal monitoring of the molecular landscape of an advanced tumor as it is being treated with successive courses of systemic therapy. Conclusions These tools combined form the foundation of an evidence-based precision oncology strategy for MIBC.

Original language	English (US)
Pages (from-to)	469-476
Number of pages	8
Journal	Urologic Oncology: Seminars and Original Investigations
Volume	34
Issue number	10
DOIs	https://doi.org/10.1016/j.urolonc.2016.05.012
State	Published - Oct 1 2016

Keywords

Bladder cancer
Neoadjuvant chemotherapy
Radical cystectomy
Targeted therapy
Urothelial carcinoma

ASJC Scopus subject areas

Oncology
Urology

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10.1016/j.urolonc.2016.05.012

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Chedgy, E. C. P., Douglas, J., Wright, J. L., Seiler, R., van Rhijn, B. W. G., Boormans, J., Todenhöfer, T., Dinney, C. P., Collins, C. C., Van der Heijden, M. S., & Black, P. C. (2016). Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer. Urologic Oncology: Seminars and Original Investigations, 34(10), 469-476. https://doi.org/10.1016/j.urolonc.2016.05.012

Chedgy, ECP, Douglas, J, Wright, JL, Seiler, R, van Rhijn, BWG, Boormans, J, Todenhöfer, T, Dinney, CP, Collins, CC, Van der Heijden, MS & Black, PC 2016, 'Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer', Urologic Oncology: Seminars and Original Investigations, vol. 34, no. 10, pp. 469-476. https://doi.org/10.1016/j.urolonc.2016.05.012

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title = "Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer",

abstract = "Background Bladder cancer is a leading cause of morbidity and mortality. Despite recent advances in understanding its molecular biology, the 5-year survival for muscle-invasive disease (muscle-invasive bladder cancer [MIBC]) remains approximately 50%. Although neoadjuvant chemotherapy (NAC) offers an established 5% absolute survival benefit at 5 years, only the 40% of patients with a major tumor response appear to benefit. There remains, therefore, a critical unmet need for predictive markers to determine which patients are best managed with NAC, as well as for novel targeted therapies to overcome resistance to NAC. Methods The NAC paradigm offers the optimal clinical context for developing precision therapy for MIBC. Abundant tissue is available for analysis before NAC in all patients and after NAC in patients with residual MIBC. Technologic advances have enabled next-generation sequencing and gene expression microarray analysis of routinely collected and even archived tissue specimens. These technologies provide a foundation for the identification of markers of chemoresistance and for the development of rational cotargeting strategies. Results Modern computational methods allow for some measure of target validation, which can be enhanced by the use of patient-derived primary xenografts (PDX). These PDX can be established at the time of radical cystectomy after NAC if there is residual MIBC. By the time a patient recurs clinically, candidate drugs targeting specific molecular changes in the patient tumor and corresponding PDX would have been tested in the PDX model, and only the most efficacious drug(s) would be administered to the patient. Liquid biopsies in the form of circulating tumor DNA and circulating tumor cells allow noninvasive longitudinal monitoring of the molecular landscape of an advanced tumor as it is being treated with successive courses of systemic therapy. Conclusions These tools combined form the foundation of an evidence-based precision oncology strategy for MIBC.",

keywords = "Bladder cancer, Neoadjuvant chemotherapy, Radical cystectomy, Targeted therapy, Urothelial carcinoma",

author = "Chedgy, {Edmund C.P.} and James Douglas and Wright, {Jonathan L.} and Roland Seiler and {van Rhijn}, {Bas W.G.} and Joost Boormans and Tilman Todenh{\"o}fer and Dinney, {Colin P.} and Collins, {Colin C.} and {Van der Heijden}, {Michiel S.} and Black, {Peter C.}",

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doi = "10.1016/j.urolonc.2016.05.012",

language = "English (US)",

volume = "34",

pages = "469--476",

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T1 - Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer

AU - Chedgy, Edmund C.P.

AU - Douglas, James

AU - Wright, Jonathan L.

AU - Seiler, Roland

AU - van Rhijn, Bas W.G.

AU - Boormans, Joost

AU - Todenhöfer, Tilman

AU - Dinney, Colin P.

AU - Collins, Colin C.

AU - Van der Heijden, Michiel S.

AU - Black, Peter C.

PY - 2016/10/1

Y1 - 2016/10/1

N2 - Background Bladder cancer is a leading cause of morbidity and mortality. Despite recent advances in understanding its molecular biology, the 5-year survival for muscle-invasive disease (muscle-invasive bladder cancer [MIBC]) remains approximately 50%. Although neoadjuvant chemotherapy (NAC) offers an established 5% absolute survival benefit at 5 years, only the 40% of patients with a major tumor response appear to benefit. There remains, therefore, a critical unmet need for predictive markers to determine which patients are best managed with NAC, as well as for novel targeted therapies to overcome resistance to NAC. Methods The NAC paradigm offers the optimal clinical context for developing precision therapy for MIBC. Abundant tissue is available for analysis before NAC in all patients and after NAC in patients with residual MIBC. Technologic advances have enabled next-generation sequencing and gene expression microarray analysis of routinely collected and even archived tissue specimens. These technologies provide a foundation for the identification of markers of chemoresistance and for the development of rational cotargeting strategies. Results Modern computational methods allow for some measure of target validation, which can be enhanced by the use of patient-derived primary xenografts (PDX). These PDX can be established at the time of radical cystectomy after NAC if there is residual MIBC. By the time a patient recurs clinically, candidate drugs targeting specific molecular changes in the patient tumor and corresponding PDX would have been tested in the PDX model, and only the most efficacious drug(s) would be administered to the patient. Liquid biopsies in the form of circulating tumor DNA and circulating tumor cells allow noninvasive longitudinal monitoring of the molecular landscape of an advanced tumor as it is being treated with successive courses of systemic therapy. Conclusions These tools combined form the foundation of an evidence-based precision oncology strategy for MIBC.

AB - Background Bladder cancer is a leading cause of morbidity and mortality. Despite recent advances in understanding its molecular biology, the 5-year survival for muscle-invasive disease (muscle-invasive bladder cancer [MIBC]) remains approximately 50%. Although neoadjuvant chemotherapy (NAC) offers an established 5% absolute survival benefit at 5 years, only the 40% of patients with a major tumor response appear to benefit. There remains, therefore, a critical unmet need for predictive markers to determine which patients are best managed with NAC, as well as for novel targeted therapies to overcome resistance to NAC. Methods The NAC paradigm offers the optimal clinical context for developing precision therapy for MIBC. Abundant tissue is available for analysis before NAC in all patients and after NAC in patients with residual MIBC. Technologic advances have enabled next-generation sequencing and gene expression microarray analysis of routinely collected and even archived tissue specimens. These technologies provide a foundation for the identification of markers of chemoresistance and for the development of rational cotargeting strategies. Results Modern computational methods allow for some measure of target validation, which can be enhanced by the use of patient-derived primary xenografts (PDX). These PDX can be established at the time of radical cystectomy after NAC if there is residual MIBC. By the time a patient recurs clinically, candidate drugs targeting specific molecular changes in the patient tumor and corresponding PDX would have been tested in the PDX model, and only the most efficacious drug(s) would be administered to the patient. Liquid biopsies in the form of circulating tumor DNA and circulating tumor cells allow noninvasive longitudinal monitoring of the molecular landscape of an advanced tumor as it is being treated with successive courses of systemic therapy. Conclusions These tools combined form the foundation of an evidence-based precision oncology strategy for MIBC.

KW - Bladder cancer

KW - Neoadjuvant chemotherapy

KW - Radical cystectomy

KW - Targeted therapy

KW - Urothelial carcinoma

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ER -

Using the neoadjuvant chemotherapy paradigm to develop precision therapy for muscle-invasive bladder cancer

Abstract

Keywords

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