Literature DB >> 34073316

TP53 Targeted Deep Sequencing of Cell-Free DNA in Esophageal Squamous Cell Carcinoma Using Low-Quality Serum: Concordance with Tumor Mutation.

Dariush Nasrollahzadeh1,2, Gholamreza Roshandel3, Tiffany Myriam Delhomme2,4, Patrice Hodonou Avogbe2, Matthieu Foll2, Farrokh Saidi1, Hossein Poustchi1, Masoud Sotoudeh1, Reza Malekzadeh1, Paul Brennan2, James Mckay2, Pierre Hainaut5, Behnoush Abedi-Ardekani2.   

Abstract

Circulating cell-free DNA (cfDNA) is emerging as a potential tumor biomarker. CfDNA-based biomarkers may be applicable in tumors without an available non-invasive screening method among at-risk populations. Esophageal squamous cell carcinoma (ESCC) and residents of the Asian cancer belt are examples of those malignancies and populations. Previous epidemiological studies using cfDNA have pointed to the need for high volumes of good quality plasma (i.e., >1 mL plasma with 0 or 1 cycles of freeze-thaw) rather than archival serum, which is often the main available source of cfDNA in retrospective studies. Here, we have investigated the concordance of TP53 mutations in tumor tissue and cfDNA extracted from archival serum left-over from 42 cases and 39 matched controls (age, gender, residence) in a high-risk area of Northern Iran (Golestan). Deep sequencing of TP53 coding regions was complemented with a specialized variant caller (Needlestack). Overall, 23% to 31% of mutations were concordantly detected in tumor and serum cfDNA (based on two false discovery rate thresholds). Concordance was positively correlated with high cfDNA concentration, smoking history (p-value = 0.02) and mutations with a high potential of neoantigen formation (OR; 95%CI = 1.9 (1.11-3.29)), suggesting that tumor DNA release in the bloodstream might reflect the effects of immune and inflammatory context on tumor cell turnover. We identified TP53 mutations in five controls, one of whom was subsequently diagnosed with ESCC. Overall, the results showed that cfDNA mutations can be reliably identified by deep sequencing of archival serum, with a rate of success comparable to plasma. Nonetheless, 70% non-identifiable mutations among cancer patients and 12% mutation detection in controls are the main challenges in applying cfDNA to detect tumor-related variants when blindly targeting whole coding regions of the TP53 gene in ESCC.

Entities:  

Keywords:  TP53; circulating cell-free DNA; circulating tumor DNA; deep sequencing; esophageal squamous cell carcinoma; liquid biopsy; neoantigen; tumor mutation; variant caller

Year:  2021        PMID: 34073316     DOI: 10.3390/ijms22115627

Source DB:  PubMed          Journal:  Int J Mol Sci        ISSN: 1422-0067            Impact factor:   5.923


  32 in total

1.  Robust inference in the negative binomial regression model with an application to falls data.

Authors:  William H Aeberhard; Eva Cantoni; Stephane Heritier
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2.  Systemic inflammation induces release of cell-free DNA from hematopoietic and parenchymal cells in mice and humans.

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Journal:  J Am Acad Dermatol       Date:  2020-05-07       Impact factor: 11.527

5.  Circulating tumor DNA detection in head and neck cancer: evaluation of two different detection approaches.

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Journal:  Oncotarget       Date:  2017-08-07

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Authors:  Leila Jahangiri; Tara Hurst
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7.  Tea drinking habits and oesophageal cancer in a high risk area in northern Iran: population based case-control study.

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Journal:  BMJ       Date:  2009-03-26

8.  Genomic comparison of esophageal squamous cell carcinoma and its precursor lesions by multi-region whole-exome sequencing.

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Journal:  Nat Commun       Date:  2017-09-12       Impact factor: 14.919

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Review 1.  A Review of Circulating Tumor DNA in the Diagnosis and Monitoring of Esophageal Cancer.

Authors:  Jiang Min; Huilin Zhou; Su Jiang; Hong Yu
Journal:  Med Sci Monit       Date:  2022-02-25
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