2022
DOI: 10.1002/pros.24331
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Clinical and pathological features associated with circulating tumor DNA content in real‐world patients with metastatic prostate cancer

Abstract: Background Liquid biopsy is a powerful tool that can enable treatment decisions for metastatic prostate cancer patients with difficult‐to‐biopsy tumors. However, the detection of genomic alterations via liquid biopsy is limited by the fraction (tumor fraction [TF]) of circulating tumor DNA (ctDNA) within the total cell‐free DNA content. While prior work has preliminarily correlated TF with clinical features of prostate cancer, we sought to validate and provide additional resolution, such that a clinical practi… Show more

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Cited by 11 publications
(8 citation statements)
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References 17 publications
(43 reference statements)
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“…Genomic sequencing techniques such as low-pass whole-genome sequencing may be able to identify genomic alterations (including homozygous deletions) in samples of low tumor fraction percentages (39); however, the evidence highlighting the clinical utility of such techniques in precision oncology is limited (40). Although there is considerable evidence related to the prognostic potential of ctDNA tumor fraction assessment in mCRPC (32,41,42), these data, as well as other research (43), highlight that additional work is needed to optimize and standardize quantification, particularly when tumor fraction/shedding rates are particularly low.…”
Section: Discussionmentioning
confidence: 99%
“…Genomic sequencing techniques such as low-pass whole-genome sequencing may be able to identify genomic alterations (including homozygous deletions) in samples of low tumor fraction percentages (39); however, the evidence highlighting the clinical utility of such techniques in precision oncology is limited (40). Although there is considerable evidence related to the prognostic potential of ctDNA tumor fraction assessment in mCRPC (32,41,42), these data, as well as other research (43), highlight that additional work is needed to optimize and standardize quantification, particularly when tumor fraction/shedding rates are particularly low.…”
Section: Discussionmentioning
confidence: 99%
“…LBx is therefore likely to be most useful in patients with an increased likelihood of ctDNA shed, generally patients with advanced cancer who are untreated or progressing on therapy higher levels of ctDNA shed were associated with a higher prostate-specific antigen level and collection of LBx within 60 days of new treatment initiation, whereas prostatespecific antigen , 5 was associated with lower ctDNA shed. 22 Optimal clinical use of LBx will require additional efforts to identify clinical features that identify patients who may be better served by tumor tissue profiling.…”
Section: Discussionmentioning
confidence: 99%
“…Publications with the highest level of evidence were selected for review. This yielded 60 articles for which full text evaluation was performed and included in the final review 12–71 . A flow diagram of the article evaluation process is shown in Figure 1.…”
Section: Methodsmentioning
confidence: 99%
“…Thus, a comparison of a major commercial ctDNA sequencing assay (Guardant360) with an academic laboratory-based gene panel identified very good concordance at 1% ctDNA fraction or above, below which alteration calls became considerably discordant/questionable 27 . When correlated to serum PSA, 4 of every 5 PCa patients with a PSA of >5 ng/mL were higher than the 1% ctDNA tumor fraction threshold, as opposed to fewer than half of patients with a PSA <5 ng/μL 26 . Comparison of ctDNA findings to those in matched, synchronous tissue biopsies as the benchmark method has continued to be studied.…”
Section: Evidence Synthesismentioning
confidence: 99%
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