Two‐point‐NGS analysis of cancer genes in cell‐free DNA of metastatic cancer patients

Palmieri, Maria; Baldassarri, Margherita; Fava, Francesca; Fabbiani, Alessandra; Gelli, Elisa; Tita, Rossella; Torre, Pamela; Petrioli, Roberto; Hadijstilianou, Theodora; Galimberti, Daniela; Cinotti, Élisa; Bengala, Carmelo; Mandalà, Marco; Piu, Pietro; Miano, Salvatora Tindara; Martellucci, Ignazio; Vannini, Agnese; Pinto, Anna Maria; Mencarelli, Maria Antonietta; Marsili, Stefania; Renieri, Alessandra; Frullanti, Elisa

doi:10.1002/cam4.2782

Cited by 9 publications

(7 citation statements)

References 21 publications

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“…In comparison with data from our previous study [5] , showing that at the beginning of tumor expansion there was a consistent, although variable, mutational burden from tens to hundreds, disease relapse is generally characterized by a "driver" clone that is responsible for metastases. The curve in Figure 2, simulating a Gaussian bell shape (similar to the typical population curve), underlines this concept.…”

Section: Discussionsupporting

confidence: 48%

“…cfDNA was extracted from 4 mL of plasma using AVENIO ctDNA Expanded Kit according to the manufacturer's instructions. cfDNA quality and quantity were verified as described in Palmieri et al [5] . cfDNA sequencing was performed using AVENIO circulating tumor DNA (ctDNA) Expanded Kit (Roche, Basel, Switzerland) on Illumina NextSeq 550 (Illumina, San Diego, CA, USA).…”

Section: Cfdna Extraction and Sequencingmentioning

confidence: 99%

“…New technologies such as the liquid biopsy of cell-free DNA (cfDNA) facilitate proper detection of somatic tumor mutations, which are the key mutation of specific cancer driver genes. The technique is non-invasive, is a valuable alternative to physical biopsies, and opens new avenues for personalized medicine [5] .…”

Section: Introductionmentioning

confidence: 99%

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Private somatic mutations identified with liquid biopsy lead tumor progression in solid cancers

Palmieri¹,

Baldassarri²,

Iuso³

et al. 2020

JCMT

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Section: Discussionsupporting

confidence: 48%

Section: Cfdna Extraction and Sequencingmentioning

confidence: 99%

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Private somatic mutations identified with liquid biopsy lead tumor progression in solid cancers

Palmieri¹,

Baldassarri²,

Iuso³

et al. 2020

JCMT

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“…Plasma sample from patient 2 was obtained as described in Palmieri et al. 9 Briefly, at least 10 ml of whole blood was collected in EDTA tubes. Plasma was separated within 5 h through two different centrifugation steps (10’ × 1600 g and 10’ × 3000 g at RT), obtaining at least 3 ml of plasma.…”

Section: Methodsmentioning

confidence: 99%

“…7,8 During the last years, next generation sequencing (NGS)–liquid biopsy has emerged as an innovative non-invasive technique for the identification of key mutations that are responsible for tumor growth allowing to optimize diagnosis, monitoring, and therapeutic choice. 9–11 Therefore, cell-free DNA (cfDNA) analysis overcomes the space-time profile constraint of physical biopsies and opens a new scenario for vascular malformations where tissue biopsy represents an invasive high risky, sometimes life-threatening, diagnostic procedure. The use of liquid biopsy would also improve the opportunities to check illness evolution on a molecular basis.…”

Section: Introductionmentioning

confidence: 99%

A pilot study of next generation sequencing–liquid biopsy on cell-free DNA as a novel non-invasive diagnostic tool for Klippel–Trenaunay syndrome

et al. 2020

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Objectives Somatic mosaicism of PIK3CA gene is currently recognized as the molecular driver of Klippel–Trenaunay syndrome. However, given the limitation of the current technologies, PIK3CA somatic mutations are detected only in a limited proportion of Klippel–Trenaunay syndrome cases and tissue biopsy remains an invasive high risky, sometimes life-threatening, diagnostic procedure. Next generation sequencing liquid biopsy using cell-free DNA has emerged as an innovative non-invasive approach for early detection and monitoring of cancer. This approach, overcoming the space-time profile constraint of tissue biopsies, opens a new scenario also for others diseases caused by somatic mutations. Methods In the present study, we performed a comprehensive analysis of seven patients (four females and three males) with Klippel–Trenaunay syndrome. Blood samples from both peripheral and efferent vein from malformation were collected and cell-free DNA was extracted from plasma. Tissue biopsies from vascular lesions were also collected when available. Cell-free DNA libraries were performed using Oncomine™ Pan-Cancer Cell-Free Assay. Ion Proton for sequencing and Ion Reporter Software for analysis were used (Life Technologies, Carlsbad, CA, USA). Results Cell-free circulating DNA analysis revealed pathogenic mutations in PIK3CA gene in all patients. The mutational load was higher in plasma obtained from the efferent vein at lesional site (0.81%) than in the peripheral vein (0.64%) leading to conclude for a causative role of the identified variants. Tissue analysis, available for one amputated patient, confirmed the presence of the mutation at the malformation site at a high molecular frequency (14–25%), confirming its causative role. Conclusions Our data prove for the first time that the cell-free DNA-next generation sequencing–liquid biopsy, which is currently used exclusively in an oncologic setting, is indeed the most effective tool for Klippel–Trenaunay syndrome diagnosis and tailored personalized treatment.

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Leveraging the Fragment Length of Circulating Tumour DNA to Improve Molecular Profiling of Solid Tumour Malignancies with Next-Generation Sequencing: A Pathway to Advanced Non-invasive Diagnostics in Precision Oncology?

Underhill

2021

Mol Diagn Ther

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Circulating cell-free DNA (ccfDNA) has emerged as a promising diagnostic tool in oncology. Identification of tumour-derived ccfDNA (i.e. circulating tumour DNA [ctDNA]) provides non-invasive access to a malignancy's molecular landscape to diagnose, inform therapeutic strategies, and monitor treatment efficacy. Current applications of ccfDNA to detect somatic mutations, however, have been largely constrained to tumour-informed searches and identification of common mutations because of the interaction between ctDNA signal and next-generation sequencing (NGS) noise. Specifically, the low allele frequency of ctDNA associated with non-metastatic and early-stage lesions may be indistinguishable from artifacts that accrue during sample preparation and NGS. Thus, using ccfDNA to achieve non-invasive and personalized molecular profiling to optimize individual patient care is a highly sought goal that remains limited in clinical practice. There is growing evidence, however, that further advances in the field of ccfDNA diagnostics may be achieved by improving detection of somatic mutations through leveraging the inherently shorter fragment lengths of ctDNA compared to non-neoplastic ccfDNA. Here, the origins and rationale for seeking to improve the mutation-based detection of ctDNA by using ccfDNA size profiling are reviewed. Subsequently, in vitro and in silico methods to enrich for a target ccfDNA fragment length are detailed to identify current practices and provide perspective into the potential of using ccfDNA size profiling to impact clinical applications in oncology.

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Two‐point‐NGS analysis of cancer genes in cell‐free DNA of metastatic cancer patients

Cited by 9 publications

References 21 publications

Private somatic mutations identified with liquid biopsy lead tumor progression in solid cancers

Private somatic mutations identified with liquid biopsy lead tumor progression in solid cancers

A pilot study of next generation sequencing–liquid biopsy on cell-free DNA as a novel non-invasive diagnostic tool for Klippel–Trenaunay syndrome

Leveraging the Fragment Length of Circulating Tumour DNA to Improve Molecular Profiling of Solid Tumour Malignancies with Next-Generation Sequencing: A Pathway to Advanced Non-invasive Diagnostics in Precision Oncology?

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