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Literature DB >> 26440707

Sensitivity of plasma BRAFmutant and NRASmutant cell-free DNA assays to detect metastatic melanoma in patients with low RECIST scores and non-RECIST disease progression.

Gregory A Chang¹, Jyothirmayee S Tadepalli¹, Yongzhao Shao², Yilong Zhang², Sarah Weiss³, Eric Robinson¹, Cindy Spittle⁴, Manohar Furtado⁵, Dawne N Shelton⁵, George Karlin-Neumann⁵, Anna Pavlick³, Iman Osman¹, David Polsky⁶.

Abstract

Melanoma lacks a clinically useful blood-based biomarker of disease activity to help guide patient management. To determine whether measurements of circulating, cell-free, tumor-associated BRAF(mutant) and NRAS(mutant) DNA (ctDNA) have a higher sensitivity than LDH to detect metastatic disease prior to treatment initiation and upon disease progression we studied patients with unresectable stage IIIC/IV metastatic melanoma receiving treatment with BRAF inhibitor therapy or immune checkpoint blockade and at least 3 plasma samples obtained during their treatment course. Levels of BRAF(mutant) and NRAS(mutant) ctDNA were determined using droplet digital PCR (ddPCR) assays. Among patients with samples available prior to treatment initiation ctDNA and LDH levels were elevated in 12/15 (80%) and 6/20 (30%) (p = 0.006) patients respectively. In patients with RECIST scores <5 cm prior to treatment initiation, ctDNA levels were elevated in 5/7 (71%) patients compared to LDH which was elevated in 1/13 (8%) patients (p = 0.007). Among all disease progression events the modified bootstrapped sensitivities for ctDNA and LDH were 82% and 40% respectively, with a median difference in sensitivity of 42% (95% confidence interval, 27%-58%; P < 0.001). In addition, ctDNA levels were elevated in 13/16 (81%) instances of non-RECIST disease progression, including 10/12 (83%) instances of new brain metastases. In comparison LDH was elevated 8/16 (50%) instances of non-RECIST disease progression, including 6/12 (50%) instances of new brain metastases. Overall, ctDNA had a higher sensitivity than LDH to detect disease progression, including non-RECIST progression events. ctDNA has the potential to be a useful biomarker for monitoring melanoma disease activity.

Entities: Chemical Disease Gene Mutation Species

Keywords: BRAF; Biomarker; Circulating tumor DNA (ctDNA); Lactate dehydrogenase (LDH); Melanoma; NRAS

Mesh：

Substances：

Year: 2015 PMID： 26440707 PMCID： PMC4695284 DOI： 10.1016/j.molonc.2015.09.005

Source DB: PubMed Journal: Mol Oncol ISSN： 1574-7891 Impact factor: 6.603

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6. Circulating mutant DNA to assess tumor dynamics.

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Journal: Nat Med Date: 2007-07-31 Impact factor: 53.440

7. Sensitivity of plasma BRAFmutant and NRASmutant cell-free DNA assays to detect metastatic melanoma in patients with low RECIST scores and non-RECIST disease progression.

Authors: Gregory A Chang; Jyothirmayee S Tadepalli; Yongzhao Shao; Yilong Zhang; Sarah Weiss; Eric Robinson; Cindy Spittle; Manohar Furtado; Dawne N Shelton; George Karlin-Neumann; Anna Pavlick; Iman Osman; David Polsky
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8. Nivolumab plus ipilimumab in advanced melanoma.

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Journal: N Engl J Med Date: 2013-06-02 Impact factor: 91.245

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Authors: Meghna Das Thakur; Fernando Salangsang; Allison S Landman; William R Sellers; Nancy K Pryer; Mitchell P Levesque; Reinhard Dummer; Martin McMahon; Darrin D Stuart
Journal: Nature Date: 2013-01-09 Impact factor: 49.962

10. Monitoring response to therapy in melanoma by quantifying circulating tumour DNA with droplet digital PCR for BRAF and NRAS mutations.

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3. Isolation and Quantification of Plasma Circulating Tumor DNA from Melanoma Patients.

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4. The tumour trail left in blood.

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5. Clinical significance of BRAF^V600E mutation in circulating tumor DNA in Chinese patients with melanoma.

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Review 6. Current and Emerging Applications of Droplet Digital PCR in Oncology.

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Review 7. Pathologists and liquid biopsies: to be or not to be?

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8. Development of Novel Mutation-Specific Droplet Digital PCR Assays Detecting TERT Promoter Mutations in Tumor and Plasma Samples.

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10. Sensitivity of plasma BRAFmutant and NRASmutant cell-free DNA assays to detect metastatic melanoma in patients with low RECIST scores and non-RECIST disease progression.