The Evolutionary Landscape of Localized Prostate Cancers Drives Clinical Aggression

Espiritu, Shadrielle M. G.; Liu, Lydia; Rubanova, Yulia; Bhandari, Vinayak; Holgersen, Erle M.; Szyca, L; Fox, Natalie S.; Chua, Melvin L.K.; Yamaguchi, Takafumi N.; Heisler, Lawrence E.; Livingstone, Julie; Wintersinger, Jeff; Yousif, Fouad; Lalonde, Emilie; Rouette, Alexandre; Salcedo, Adriana; Houlahan, Kathleen E.; Li, Constance H.; Huang, Vincent; Fraser, Michael; Kwast, Theodorus van der; Morris, Quaid; Bristow, Robert G.; Boutros, Paul C.

doi:10.1016/j.cell.2018.03.029

Cited by 195 publications

(240 citation statements)

References 51 publications

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“…A deep sequencing study revealed that a proportion of Gleason grade 3 pattern carcinomas are monoclonal, whereas a subset is composed of multiple subclones. This may imply that the latter are subject to genetic evolutionary changes …”

Section: Isup 2014 Grading Of Prostate Cancermentioning

confidence: 99%

Grading of prostate cancer: a work in progress

2018

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Grading of prostate cancer has evolved substantially over time, not least because of major changes in diagnostic approach and concomitant shifts from late‐ to early‐stage detection since the adoption of PSA testing from the late 1980s. After the conception of the architecture‐based nine‐tier Gleason grading system more than 50 years ago, several changes were made in order to increase its prognostic impact, to reduce interobserver variation and to improve concordance between prostate needle biopsy and radical prostatectomy grading. This eventually resulted in the current five‐tier grading system, with a much more detailed description of the individual architectural patterns constituting the remaining three Gleason patterns (i.e. grades 3–5). Nevertheless, there is room for improvement. For instance, distinction of common grade 4 subpatterns such as ill‐formed and fused glands from the grade 3 pattern is challenging, blurring the division between low‐risk patients who could be eligible for deferred therapy and those who need curative therapy. The last few years have witnessed the publication of several studies on the prognostic impact of individual architectural subpatterns showing that, in particular, the cribriform pattern exceeded the prognostic impact of other grade 4 subpatterns. This review provides an overview of the changes in prostate cancer grading over time and provides a thorough description of the various Gleason subpatterns, the current evidence of their prognostic impact and areas of contention. Potential practical ways for improvements of the current grading system are also put forward.

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Section: Isup 2014 Grading Of Prostate Cancermentioning

confidence: 99%

Grading of prostate cancer: a work in progress

2018

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“…Numerous recent studies have explored the genomic basis for development of localized prostate cancer, showing distinct evolutionary paths in nonindolent versus indolent disease. The fate of tumors to progress from their somatic progenitors is set early, with alterations in ATM, PTEN, and MYC subclones having predictive power for the existence of higher grade disease including occult oligometastases at the time of radical prostatectomy [9][10][11][12][13]. As the vast majority of these alterations occur as copy number gains or deletions, the percentage of the genome affected by large chromosomal rearrangements is similarly predictive of biochemical recurrence and poor outcome [10,14,15].…”

Section: Introductionmentioning

confidence: 99%

Low Abundance of Circulating Tumor DNA in Localized Prostate Cancer

Hennigan

Trostel

Terrigino

et al. 2019

Preprint

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“…Despite being largely regarded as pursuing an indolent clinical course, aggressive behaviors like recurrence or metastasis have been observed and deaths also reported, highlighting the complex and yet poorly understood mechanism [5][6][7][8][9]. There have been extensive reports on the genomic features of common prostate cancer [10][11][12][13][14][15][16][17], and the molecular features of normal human prostate basal cells, prostate basal cell hyperplasia, and basal populations from human prostate cancer have also been reported [18][19][20], but the molecular profile of prostate BCC is still lacking. The mutational and transcriptomic features of this tumor sub-type will thus be valuable for understanding of its tumorigenesis mechanism and development of future clinical treatments.…”

Section: Introductionmentioning

confidence: 99%

Single-cell dissection of a rare human prostate basal cell carcinoma

Long

Jiang

et al. 2019

Preprint

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heading：Single-cell analysis of prostate basal cell carcinoma Abstract As a rare subtype of prostate carcinoma, basal cell carcinoma (BCC) has not been studied extensively and thus lacks systematic molecular characterization. Here we applied single-cell genomic amplification and RNA-Seq to a specimen of human prostate BCC (CK34βE12 + /P63 + /PAP -/PSA -). The mutational landscape was obtained via whole exome sequencing of the amplification mixture of 49 single cells, and the 5 putative driver genes mutated are CASC5, NUTM1, PTPRC, KMT2C and TBX3. The top 3 nucleotide substitutions are C>T, T>C and C>A, similar to common prostate cancer. The distribution of the variant allele frequency values indicated these single cells are from the same tumor clone. The transcriptomes of 69 single cells were obtained, and they were clustered into tumor, stromal and immune cells based on their global transcriptomic profiles. The tumor cells specifically express basal cell markers like KRT5, KRT14 and KRT23, and epithelial markers EPCAM, CDH1 and CD24.The transcription factor (TF) co-variance network analysis showed that the BCC tumor cells have distinct regulatory networks. By comparison with current prostate cancer datasets, we found that some of the bulk samples exhibit basal-cell signatures.Interestingly, at single-cell resolution the gene expression patterns of prostate BCC tumor cells show uniqueness compared with that of common prostate cancer-derived circulating tumor cells. This study, for the first time, discloses the comprehensive mutational and transcriptomic landscapes of prostate BCC, which lays a foundation 2 for the understanding of its tumorigenesis mechanism and provides new insights into prostate cancers in general.

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The Evolutionary Landscape of Localized Prostate Cancers Drives Clinical Aggression

Cited by 195 publications

References 51 publications

Grading of prostate cancer: a work in progress

Grading of prostate cancer: a work in progress

Low Abundance of Circulating Tumor DNA in Localized Prostate Cancer

Single-cell dissection of a rare human prostate basal cell carcinoma

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