Genomic and phenotypic heterogeneity in prostate cancer

Michael C. Haffner; Wilbert Zwart; Martine P. Roudier; Lawrence D. True; William G. Nelson; Jonathan I. Epstein; Angelo M. De Marzo; Peter S. Nelson; Srinivasan Yegnasubramanian

doi:10.1038/s41585-020-00400-w

Genomic and phenotypic heterogeneity in prostate cancer

Michael C. Haffner, Wilbert Zwart, Martine P. Roudier, Lawrence D. True, William G. Nelson, Jonathan I. Epstein, Angelo M. De Marzo, Peter S. Nelson, Srinivasan Yegnasubramanian

School of Medicine

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

3 Scopus citations

Abstract

From a clinical, morphological and molecular perspective, prostate cancer is a heterogeneous disease. Primary prostate cancers are often multifocal, having topographically and morphologically distinct tumour foci. Sequencing studies have revealed that individual tumour foci can arise as clonally distinct lesions with no shared driver gene alterations. This finding demonstrates that multiple genomically and phenotypically distinct primary prostate cancers can be present in an individual patient. Lethal metastatic prostate cancer seems to arise from a single clone in the primary tumour but can exhibit subclonal heterogeneity at the genomic, epigenetic and phenotypic levels. Collectively, this complex heterogeneous constellation of molecular alterations poses obstacles for the diagnosis and treatment of prostate cancer. However, advances in our understanding of intra-tumoural heterogeneity and the development of novel technologies will allow us to navigate these challenges, refine approaches for translational research and ultimately improve patient care.

Original language	English (US)
Pages (from-to)	79-92
Number of pages	14
Journal	Nature Reviews Urology
Volume	18
Issue number	2
DOIs	https://doi.org/10.1038/s41585-020-00400-w
State	Published - Feb 2021

ASJC Scopus subject areas

Urology

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10.1038/s41585-020-00400-w

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@article{1a690e2855844e538b36948388e2b5cf,

title = "Genomic and phenotypic heterogeneity in prostate cancer",

abstract = "From a clinical, morphological and molecular perspective, prostate cancer is a heterogeneous disease. Primary prostate cancers are often multifocal, having topographically and morphologically distinct tumour foci. Sequencing studies have revealed that individual tumour foci can arise as clonally distinct lesions with no shared driver gene alterations. This finding demonstrates that multiple genomically and phenotypically distinct primary prostate cancers can be present in an individual patient. Lethal metastatic prostate cancer seems to arise from a single clone in the primary tumour but can exhibit subclonal heterogeneity at the genomic, epigenetic and phenotypic levels. Collectively, this complex heterogeneous constellation of molecular alterations poses obstacles for the diagnosis and treatment of prostate cancer. However, advances in our understanding of intra-tumoural heterogeneity and the development of novel technologies will allow us to navigate these challenges, refine approaches for translational research and ultimately improve patient care.",

author = "Haffner, {Michael C.} and Wilbert Zwart and Roudier, {Martine P.} and True, {Lawrence D.} and Nelson, {William G.} and Epstein, {Jonathan I.} and {De Marzo}, {Angelo M.} and Nelson, {Peter S.} and Srinivasan Yegnasubramanian",

note = "Funding Information: S.Y., W.G.N. and A.M.D.M. are paid consultants to and received sponsored research funding from Cepheid. S.Y. and W.G.N. are co-inventors of intellectual property describing the use of DNA methylation changes as prostate cancer biomarkers and are eligible to earn royalties related to the future sale of any products using those technologies. S.Y. and A.M.D.M. receive sponsored research funding from Janssen. These arrangements have been reviewed and approved by the Johns Hopkins University in accordance with its conflict of interest policies. The other authors declare no competing interests. Funding Information: The authors thank C. Morrissey (University of Washington), T. Lotan (Johns Hopkins School of Medicine) and W. B. Isaacs (Johns Hopkins School of Medicine), as well as members of the Haffner, Yegnasubramanian and Nelson laboratories, for valuable discussions and suggestions on the manuscript. This work of the authors is supported by the NIH/NCI (P50CA097186, P50CA58236, U01 CA196390, P30 CA006973, R01CA183965), the US Department of Defense Prostate Cancer Research Program (W81XWH-20-1-0111, W81XWH-18-1-0406, W81XWH-18-2-0015), the Prostate Cancer Foundation, the Safeway Foundation, the Commonwealth Foundation and the Irving Hansen Memorial Foundation. Publisher Copyright: {\textcopyright} 2020, Springer Nature Limited.",

year = "2021",

month = feb,

doi = "10.1038/s41585-020-00400-w",

language = "English (US)",

volume = "18",

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journal = "Nature Reviews Urology",

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AU - Haffner, Michael C.

AU - Zwart, Wilbert

AU - Roudier, Martine P.

AU - True, Lawrence D.

AU - Nelson, William G.

AU - Epstein, Jonathan I.

AU - De Marzo, Angelo M.

AU - Nelson, Peter S.

AU - Yegnasubramanian, Srinivasan

N1 - Funding Information: S.Y., W.G.N. and A.M.D.M. are paid consultants to and received sponsored research funding from Cepheid. S.Y. and W.G.N. are co-inventors of intellectual property describing the use of DNA methylation changes as prostate cancer biomarkers and are eligible to earn royalties related to the future sale of any products using those technologies. S.Y. and A.M.D.M. receive sponsored research funding from Janssen. These arrangements have been reviewed and approved by the Johns Hopkins University in accordance with its conflict of interest policies. The other authors declare no competing interests. Funding Information: The authors thank C. Morrissey (University of Washington), T. Lotan (Johns Hopkins School of Medicine) and W. B. Isaacs (Johns Hopkins School of Medicine), as well as members of the Haffner, Yegnasubramanian and Nelson laboratories, for valuable discussions and suggestions on the manuscript. This work of the authors is supported by the NIH/NCI (P50CA097186, P50CA58236, U01 CA196390, P30 CA006973, R01CA183965), the US Department of Defense Prostate Cancer Research Program (W81XWH-20-1-0111, W81XWH-18-1-0406, W81XWH-18-2-0015), the Prostate Cancer Foundation, the Safeway Foundation, the Commonwealth Foundation and the Irving Hansen Memorial Foundation. Publisher Copyright: © 2020, Springer Nature Limited.

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N2 - From a clinical, morphological and molecular perspective, prostate cancer is a heterogeneous disease. Primary prostate cancers are often multifocal, having topographically and morphologically distinct tumour foci. Sequencing studies have revealed that individual tumour foci can arise as clonally distinct lesions with no shared driver gene alterations. This finding demonstrates that multiple genomically and phenotypically distinct primary prostate cancers can be present in an individual patient. Lethal metastatic prostate cancer seems to arise from a single clone in the primary tumour but can exhibit subclonal heterogeneity at the genomic, epigenetic and phenotypic levels. Collectively, this complex heterogeneous constellation of molecular alterations poses obstacles for the diagnosis and treatment of prostate cancer. However, advances in our understanding of intra-tumoural heterogeneity and the development of novel technologies will allow us to navigate these challenges, refine approaches for translational research and ultimately improve patient care.

AB - From a clinical, morphological and molecular perspective, prostate cancer is a heterogeneous disease. Primary prostate cancers are often multifocal, having topographically and morphologically distinct tumour foci. Sequencing studies have revealed that individual tumour foci can arise as clonally distinct lesions with no shared driver gene alterations. This finding demonstrates that multiple genomically and phenotypically distinct primary prostate cancers can be present in an individual patient. Lethal metastatic prostate cancer seems to arise from a single clone in the primary tumour but can exhibit subclonal heterogeneity at the genomic, epigenetic and phenotypic levels. Collectively, this complex heterogeneous constellation of molecular alterations poses obstacles for the diagnosis and treatment of prostate cancer. However, advances in our understanding of intra-tumoural heterogeneity and the development of novel technologies will allow us to navigate these challenges, refine approaches for translational research and ultimately improve patient care.

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DO - 10.1038/s41585-020-00400-w

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JO - Nature Reviews Urology

JF - Nature Reviews Urology

IS - 2

ER -

Genomic and phenotypic heterogeneity in prostate cancer

Abstract

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