| Literature DB >> 28850629 |
Allan A Lima Pereira1, Maria Pia Morelli1, Michael Overman1, Bryan Kee1, David Fogelman1, Eduardo Vilar2, Imad Shureiqi1, Kanwal Raghav1, Cathy Eng1, Shanequa Manuel1, Shadarra Crosby1, Robert A Wolff1, Kimberly Banks3, Richard Lanman3, AmirAli Talasaz3, Scott Kopetz1, Van Morris1.
Abstract
BACKGROUND: Circulating cell-free DNA (cfDNA) isolated from the plasma of cancer patients (pts) has been shown to reflect the genomic mutation profile of the tumor. However, physician and patient assessment of clinical utility of these assays in patients with metastatic colorectal cancer (mCRC) has not been previously described.Entities:
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Year: 2017 PMID: 28850629 PMCID: PMC5574560 DOI: 10.1371/journal.pone.0183949
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Patient demographic characteristics.
| Characteristic | N = 128 (%) |
|---|---|
| Age (median/range) | 53 (27–76) |
| Gender | |
| Male | 65(50.8) |
| Female | 63 (49.2) |
| Race/Ethnicity | |
| Asian | 9 (7.0) |
| Black | 13 (10.2) |
| Hispanic | 7 (5.5) |
| Other | 2 (1.6) |
| White | 97 (75.8) |
| ECOG 0–1 | 128 (100) |
| 0 | 19 (14.8) |
| 1 | 108 (84.4) |
| 2 | 1 (0.8) |
| Primary tumor location | |
| Right colon | 34(26.6) |
| Transverse colon | 5 (3.9) |
| Left Colon | 69 (53.9) |
| Rectum | 20 (15.6) |
| Microsatellite Instability | |
| MSS / MSI-L | 110 (85.9) |
| MSI-H | 6 (4.7) |
| Unknown | 12 (9.4) |
| Systemic therapy (prior exposure) | |
| 5-FU or Capecitabine | 128 (100.0) |
| Irinotecan | 111 (86.7) |
| Oxaliplatin | 123 (96.1) |
| Anti-EGFR | 40 (31.3) |
| Anti-VEGF | 109 (85.2) |
| Regorafenib or TAS 102 | 16 (12.5) |
| Immunotherapy | 1 (0.8) |
| Other | 5 (3.9) |
| Sites of metastasis | |
| Liver | 85 (66.4) |
| Lung | 76 (59.4) |
| Peritoneum | 31 (24.2) |
| Pelvis | 3 (2.3) |
| Bone | 7 (5.5) |
| CNS | 1 (0.8) |
| Lymph nodes | 50 (39.1) |
| Other | 8 (6.3) |
| Site of collection tissue sample | |
| Primary tumor | 82(64.1) |
| Metastatic site | 46 (35.9) |
| Tissue sample location (metastatic site) | |
| Liver | 25 (54.3) |
| Lung | 5 (10.9) |
| Peritoneum/Omentum | 2 (4.4) |
| Other | 14 (30.4) |
MSS Microsatellite Stable; MSI-L: Microsatellite instability-Low; MSI-H: Microsatellite instability—High; 5-FU: 5-fluorouracil; EGFR: epidermal growth factor receptor; VEGF: vascular endothelial growth factor; CNS: Central Nervous System
*—Cetuximab or panitumumab
**—Bevacizumab or aflibercept
♯ - Experimental treatment in prior clinical trials
Fig 1Number of patients with genomic alterations detected by both FFPE and cfDNA analysis.
FFPE = formalin-fixed, paraffin-embedded tissue; cfDNA = cell-free DNA; Amplif = amplification.
Fig 2Clinical utility of cfDNA sequencing results.
(A) Detectable mutations and/or amplification were present in 78% of patients. (B) 50% of these patients (N = 50) had “potentially actionable” mutations and/or amplifications. (C) Among these, 60% (N = 30) patients had a clinical trial identified based on the matched biomarker detected from the cfDNA (D) 15 patients ultimately enrolled on a biomarker-based clinical trial. Pt = patient; MDACC = MD Anderson Cancer Center.
Additional findings noted in sequencing of historic FFPE specimens compared to cfDNA sequencing.
FFPE = formalin-fixed, paraffin-embedded tissue; cfDNA = cell-free DNA.
| Additional findings in FFPE—Physician Survey Response | N (%) |
|---|---|
| No additional findings were present | |
| Additional 'potentially actionable' amplifications were present in the tissue | |
| Additional 'potentially actionable' mutations were present in the tissue | |
| Both additional 'potentially actionable' amplifications and mutations were present in the tissue |
Fig 3Provider survery results.
Physician preference for convenience (A) and clinical utility (B) according to the sample detection method and a stated desire to incorporate sequencing results into clinical decisions. FFPE = formalin-fixed, paraffin-embedded tissue; cfDNA = cell-free DNA.
Fig 4The impact of the use of cfDNA in (A) quality of care and (B) patient satisfaction.