Evolution of Castration-Resistant Prostate Cancer in ctDNA during Sequential Androgen Receptor Pathway Inhibition

Annala, Matti; Taavitsainen, Sinja; Khalaf, Daniel; Vandekerkhove, Gillian; Beja, Kevin; Sipola, Joonatan; Warner, Evan W.; Herberts, Cameron; Wong, Amanda; Fu, Simon; Finch, Daygen L.; Oja, Conrad D.; Vergidis, Joanna; Zulfiqar, Muhammad; Eigl, Bernhard J.; Kollmansberger, Christian K.; Nykter, Matti; Gleave, Martin; N., Kim; Wyatt, Alexander W.

doi:10.1158/1078-0432.ccr-21-1625

Cited by 48 publications

(65 citation statements)

References 45 publications

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“…TF for WES was estimated using manually fitted ploidy models for copy number and heterozygous SNP deviation, as described previously. 25…”

Section: Methodsmentioning

confidence: 99%

“…Targeted DNA sequencing was performed on all samples using an established targeted panel capturing the exons of 73 prostate cancer-relevant genes, according to the published methodology. [23][24][25] Whole-exome sequencing (WES) was performed on 28 tumor samples (and matched gDNAs) using the same protocol as for targeted DNA sequencing except that hybridization capture was carried out with the Roche Nimblegen SeqCap EZ MedExome kit. A detailed description of somatic and germline mutation calling and copy number evaluation is given in the Data Supplement.…”

Section: Dna Sequencing and Variant Detectionmentioning

confidence: 99%

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Genomic Features of Lung-Recurrent Hormone-Sensitive Prostate Cancer

Eecken

Fonseca

Herberts

et al. 2022

JCO Precision Oncology

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PURPOSE Pulmonary involvement is rare in metastatic hormone-sensitive prostate cancer (mHSPC) that recurs after treatment for localized disease. Guidelines recommend intensive systemic therapy, similar to patients with liver metastases, but some lung-recurrent mHSPC may have good outcomes. Genomic features of lung metastases may clarify disease aggression, but are poorly understood since lung biopsy is rarely performed. We present a comparative assessment of genomic drivers and heterogeneity in metachronous prostate tumors and lung metastases. METHODS We leveraged a prospective functional imaging study of 208 biochemically recurrent prostate cancers to identify 10 patients with lung-recurrent mHSPC. Histologic diagnosis was attained via thoracic surgery or fine-needle lung biopsy. We retrieved clinical data and performed multiregion sampling of primary tumors and metastases. Targeted and/or whole-exome sequencing was applied to 46 primary and 32 metastatic foci. RESULTS Unusually for mHSPC, all patients remained alive despite a median follow-up of 11.5 years. Several patients experienced long-term freedom from systemic treatment. The genomic landscape of lung-recurrent mHSPC was typical of curable prostate cancer with frequent PTEN, SPOP, and chromosome 8p alterations, and there were no deleterious TP53 and DNA damage repair gene mutations that characterize aggressive prostate cancer. Despite a long median time to recurrence (76.8 months), copy number alterations and clonal mutations were highly conserved between metastatic and primary foci, consistent with intrapatient homogeneity and limited genomic evolution. CONCLUSION In this retrospective hypothesis-generating study, we observed indolent genomic etiology in selected lung-recurrent mHSPC, cautioning against grouping these patients together with liver or bone-predominant mHSPC. Although our data do not generalize to all patients with lung metastases, the results encourage prospective efforts to stratify lung-recurrent mHSPC by genomic features.

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“…TF for WES was estimated using manually fitted ploidy models for copy number and heterozygous SNP deviation, as described previously. 25…”

Section: Methodsmentioning

confidence: 99%

Section: Dna Sequencing and Variant Detectionmentioning

confidence: 99%

Genomic Features of Lung-Recurrent Hormone-Sensitive Prostate Cancer

Eecken

Fonseca

Herberts

et al. 2022

JCO Precision Oncology

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“…In castration‐resistant disease, AR gene amplification is the dominant genomic mechanism contributing to increased AR expression 11,14 . More recently, whole genome sequencing has helped define the existence of a critical transcriptional enhancer 600−700 kb upstream of the AR gene body, with coamplification of both the AR gene body and associated enhancer representing the most common genomic pattern observed in mCRPC clinical samples 13,15,20–22 …”

Section: Overview Of Ar Genotype In Prostate Cancermentioning

confidence: 99%

Androgen receptor genomic alterations and treatment resistance in metastatic prostate cancer

Kwan

Wyatt

2022

The Prostate

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Background Genomic alterations to the androgen receptor (AR) are common in metastatic castration‐resistant prostate cancer (mCRPC). AR copy number amplifications, ligand‐binding domain missense mutations, and intronic structural rearrangements can all drive resistance to approved AR pathway inhibitors and their detection via tissue or liquid biopsy is linked to clinical outcomes. With an increasingly crowded treatment landscape, there is hope that AR genomic alterations can act as prognostic and/or predictive biomarkers to guide patient management. Methods In this review, we evaluate the current evidence for AR genomic alterations as clinical biomarkers in mCRPC, focusing on correlative studies that have used plasma circulating tumor DNA to characterize AR genotype. Results We highlight data that demonstrates the complexity of AR genotype within individual patients, and suggest that future studies should account for cancer clonal heterogeneity and variable tumor content in liquid biopsy samples. Given the potential for cooccurrence of multiple AR genomic alterations in the same or competing subclones of a patient, it is distinctly challenging to attribute blanket clinical significance to any individual alteration. This challenge is further complicated by the varied treatment exposures in contemporary patients, and the fact that AR genotype continues to evolve in the mCRPC setting across sequential lines of systemic therapy. Conclusions As treatment access and liquid biopsy technology continues to improve, we posit that real‐time measures of AR biology are likely to play a key role in emerging precision oncology strategies for metastatic prostate cancer.

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“…Another study exploiting dynamic ctDNA analysis to monitor genetic evolutions during ensartinib treatment in NSCLC showed that TP53 mutations promoted tumor evolution and accelerated occurrence of resistance, thus indicating TP53 mutations at baseline were independently correlated with worse clinical outcomes [87]. Deep targeted and whole-exome sequencing of ctDNA in metastatic castration-resistant prostate cancer patients for comparison of base-line and posttreatment showed that the dominant androgen receptor (AR) genotype continues to evolve during sequential lines of AR inhibition and drives acquired resistance [88].…”

Section: Detection Of Ctdna Mutations For Cancer Monitoring and Assessment Of Minimal Residual Diseasementioning

confidence: 99%

Liquid Biopsy, ctDNA Diagnosis through NGS

Chen

Liu

Zheng

et al. 2021

Life

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Liquid biopsy with circulating tumor DNA (ctDNA) profiling by next-generation sequencing holds great promise to revolutionize clinical oncology. It relies on the basis that ctDNA represents the real-time status of the tumor genome which contains information of genetic alterations. Compared to tissue biopsy, liquid biopsy possesses great advantages such as a less demanding procedure, minimal invasion, ease of frequent sampling, and less sampling bias. Next-generation sequencing (NGS) methods have come to a point that both the cost and performance are suitable for clinical diagnosis. Thus, profiling ctDNA by NGS technologies is becoming more and more popular since it can be applied in the whole process of cancer diagnosis and management. Further developments of liquid biopsy ctDNA testing will be beneficial for cancer patients, paving the way for precision medicine. In conclusion, profiling ctDNA with NGS for cancer diagnosis is both biologically sound and technically convenient.

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Evolution of Castration-Resistant Prostate Cancer in ctDNA during Sequential Androgen Receptor Pathway Inhibition

Cited by 48 publications

References 45 publications

Genomic Features of Lung-Recurrent Hormone-Sensitive Prostate Cancer

Genomic Features of Lung-Recurrent Hormone-Sensitive Prostate Cancer

Androgen receptor genomic alterations and treatment resistance in metastatic prostate cancer

Liquid Biopsy, ctDNA Diagnosis through NGS

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