Circulating DNA as a Strong Multimarker Prognostic Tool for Metastatic Colorectal Cancer Patient Management Care

Messaoudi, Safia El; Moulière, Florent; Manoir, Stanislas du; Bascoul-Mollevi, Caroline; Gillet, Brigitte; Nouaille, Michelle; Fiess, Catherine; Lopez-Crapez, Evelyne; Bibeau, Frédéric; Theillet, Charles; Mazard, Thibault; Pezet, Denis; Mathonnet, Muriel; Ychou, Marc; Thierry, Alain R.

doi:10.1158/1078-0432.ccr-15-0297

Cited by 140 publications

(113 citation statements)

References 41 publications

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“…However, technological shortcomings and difficulty in finding the perfect markers to identify such CTCs or ctDNA have resulted in few studies of any clinically valuable difference in terms of survival outcomes or prediction[31]. Other studies appear promising, including one recent meta-analysis on the prognostic role of ctDNA[32], also for disease prediction but are small and need further validation[33-35]. …”

Section: Liquid Biopsies: Circulating Tumor Cells and Circulating Tummentioning

confidence: 99%

Can molecular biomarkers replace a clinical risk score for resectable colorectal liver metastasis?

Veen

Søreide

2017

WJGO

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In resectable colorectal liver metastasis (CRLM) the role and use of molecular biomarkers is still controversial. Several biomarkers have been linked to clinical outcomes in CRLM, but none have so far become routine for clinical decision making. For several reasons, the clinical risk score appears to no longer hold the same predictive value. Some of the reasons include the ever expanding indications for liver resection, which now increasingly tend to involve extrahepatic disease, such as lung metastases (both resectable and non-resectable) and the shift in indication from “what is taken out” (e.g., how much liver has to be resected) to “what is left behind” (that is, how much functional liver tissue the patient has after resection). The latter is amenable to modifications by using adjunct techniques of portal vein embolization and the associating liver partition and portal vein ligation for staged hepatectomy techniques to expand indications for liver resection. Added to this complexity is the increasing number of molecular markers, which appear to hold important prognostic and predictive information, for which some will be discussed here. Beyond characteristics of tissue-based genomic profiles will be liquid biopsies derived from circulating tumor cells and cell-free circulating tumor DNA in the blood. These markers are present in the peripheral circulation in the majority of patients with metastatic cancer disease. Circulating biomarkers may represent more readily available methods to monitor, characterize and predict cancer biology with future implications for cancer care.

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Section: Liquid Biopsies: Circulating Tumor Cells and Circulating Tummentioning

confidence: 99%

Can molecular biomarkers replace a clinical risk score for resectable colorectal liver metastasis?

Veen

Søreide

2017

WJGO

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“…Qualitative characteristics, such as methylated cfDNA levels have also been shown to independently predict OS in mCRC[62]. In the largest published prospective mCRC patient cohort ( n = 97), El Messaoudi et al[63] used qPCR and showed that cfDNA levels, higher specific mutation loads and the level of cfDNA fragmentation are strong prognostic factors; cfDNA levels were independent prognostic factors for the entire patient cohort and the level of fragmentation only for the KRAS/BRAF mutated subset. Specifically, a difference in OS of 10 mo was reported between the groups of high vs low cfDNA levels (18.07 mo vs 28.5 mo respectively, P = 0.0087)[63].…”

Section: Cell-free Dna As a Prognostic Markermentioning

confidence: 99%

“…In the largest published prospective mCRC patient cohort ( n = 97), El Messaoudi et al[63] used qPCR and showed that cfDNA levels, higher specific mutation loads and the level of cfDNA fragmentation are strong prognostic factors; cfDNA levels were independent prognostic factors for the entire patient cohort and the level of fragmentation only for the KRAS/BRAF mutated subset. Specifically, a difference in OS of 10 mo was reported between the groups of high vs low cfDNA levels (18.07 mo vs 28.5 mo respectively, P = 0.0087)[63]. Finally, Spindler et al[64] compared the prognostic value of the detection of KRAS mutations in the plasma compared to the primary tumor with the use of qPCR, with the former being an independent predictor for OS (HR = 2.98, 95%CI: 1.53-5.80, P = 0.001) and PFS (HR = 2.84, 95%CI: 1.46-5.53, P = 0.002), whereas the latter had no correlation with outcomes, which underscores the value of cfDNA qualitative testing.…”

Section: Cell-free Dna As a Prognostic Markermentioning

confidence: 99%

Role of circulating free DNA in colorectal cancer

Matikas¹,

Voutsina²,

Trypaki³

et al. 2016

WJGO

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The gradual elucidation of the underlying biology of colorectal cancer has provided new insights and therapeutic options for patients with metastatic disease which are selected according to predictive biomarkers. This precision medicine paradigm, however, is incomplete since not all eligible patients respond to these agents and prognostic stratification is largely based on clinicopathologic variants. Importantly, no robust data exist to help properly select patients with localized disease at high risk for recurrence and most likely to benefit from adjuvant chemotherapy. There is a rapidly expanding body of literature regarding the role of the qualitative and quantitative analysis of circulating free DNA in various neoplasms, which consistently outperforms traditional tumor markers both as a predictive and as a prognostic marker. Several lines of evidence suggest that circulating free DNA may exhibit a complementary role to existing modalities for the early diagnosis of colorectal cancer, the selection of patients for adjuvant chemotherapy, for the follow-up of treated patients, for the selection of treatment for advanced disease and the assessment of response and for determining the prognosis of patients. These data, which are reviewed here, illustrate the important role that circulating biomarkers may soon have at the daily clinical practice.

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“…The detection of ctDNA can be used for obtaining diagnostic, prognostic and theranostic information concerning cancer. The diagnostic utility of ctDNA primarily stems from the presence of somatic genomic alterations, such as in the KRAS , BRAF and EGFR genes, which are absent from DNA taken from matched normal cells and in the circulating cell-free DNA (ccfDNA) of healthy subjects [1,2,3,4,5,6]. …”

Section: Introductionmentioning

confidence: 99%

Evaluation of Methylation Biomarkers for Detection of Circulating Tumor DNA and Application to Colorectal Cancer

Mitchell

Brown

et al. 2016

Genes

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Solid tumors shed DNA into circulation, and there is growing evidence that the detection of circulating tumor DNA (ctDNA) has broad clinical utility, including monitoring of disease, prognosis, response to chemotherapy and tracking tumor heterogeneity. The appearance of ctDNA in the circulating cell-free DNA (ccfDNA) isolated from plasma or serum is commonly detected by identifying tumor-specific features such as insertions, deletions, mutations and/or aberrant methylation. Methylation is a normal cell regulatory event, and since the majority of ccfDNA is derived from white blood cells (WBC), it is important that tumour-specific DNA methylation markers show rare to no methylation events in WBC DNA. We have used a novel approach for assessment of low levels of DNA methylation in WBC DNA. DNA methylation in 29 previously identified regions (residing in 17 genes) was analyzed in WBC DNA and eight differentially-methylated regions (DMRs) were taken through to testing in clinical samples using methylation specific PCR assays. DMRs residing in four genes, BCAT1, GRASP, IKZF1 and IRF4, exhibited low positivity, 3.5% to 7%, in the plasma of colonoscopy-confirmed healthy subjects, with the sensitivity for detection of ctDNA in colonoscopy-confirmed patients with colorectal cancer being 65%, 54.5%, 67.6% and 59% respectively.

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Circulating DNA as a Strong Multimarker Prognostic Tool for Metastatic Colorectal Cancer Patient Management Care

Cited by 140 publications

References 41 publications

Can molecular biomarkers replace a clinical risk score for resectable colorectal liver metastasis?

Can molecular biomarkers replace a clinical risk score for resectable colorectal liver metastasis?

Role of circulating free DNA in colorectal cancer

Evaluation of Methylation Biomarkers for Detection of Circulating Tumor DNA and Application to Colorectal Cancer

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