Circulating Tumor DNA Analysis and Functional Imaging Provide Complementary Approaches for Comprehensive Disease Monitoring in Metastatic Melanoma

Mark A. Dawson; Anthony T. Papenfuss; Mark Shackleton; Rodney J. Hicks; Grant A. McArthur; Shahneen Sandhu; Sarah‐Jane Dawson; Stephen Q. Wong; Jeanette Raleigh; Jason Callahan; Ismael A. Vergara; Sarah Ftouni; Athena Hatzimihalis; Andrew J. Colebatch; Jason Li; Timothy Semple; Kenneth Doig; Christopher Mintoff; Devbarna Sinha; Paul Yeh; Maria João Silva; Kathryn Alsop; Heather Thorne; David D.L. Bowtell; David Gyorki; Gisela Mir Arnau; Carleen Cullinane; Damien Kee; Benjamin Brady; Fergal C. Kelleher

doi:10.1200/po.16.00009

Abstract

1 min read

Circulating tumor DNA (ctDNA) allows noninvasive disease monitoring across a range of malignancies. In metastatic melanoma, the extent to which ctDNA reflects changes in metabolic disease burden assessed by 18F-labeled fluorodeoxyglucose positron emission tomography (FDG-PET) is unknown. We assessed the role of ctDNA analysis in combination with FDG-PET to monitor tumor burden and genomic heterogeneity throughout treatment.We performed a comprehensive analysis of serial ctDNA and FDG-PET in 52 patients who received systemic therapy for metastatic melanoma. Next-generation sequencing and digital polymerase chain reaction were used to analyze plasma samples from the cohort.ctDNA levels were monitored across patients with mutant BRAF, NRAS, and BRAF/NRAS wild type disease. Mutant BRAF and NRAS ctDNA levels correlated closely with changes in metabolic disease burden throughout treatment. TERT promoter mutant ctDNA levels also paralleled changes in tumor burden, which provide an alternative marker for disease monitoring. Of note, subcutaneous and cerebral disease sites were not well represented in plasma. Early changes in ctDNA and metabolic disease burden were important indicators of treatment response. Patients with an early decrease in ctDNA post-treatment had improved progression-free survival compared with patients in whom ctDNA levels remained unchanged or increased over time (hazard ratio, 2.6; P = .05). ctDNA analysis contributed key molecular information through the identification of putative resistance mechanisms to targeted therapy. A detailed comparison of the genomic architecture of plasma and multiregional tumor biopsy specimens at autopsy revealed the ability of ctDNA to comprehensively capture genomic heterogeneity across multiple disease sites.The findings highlight the powerful role of ctDNA in metastatic melanoma as a complementary modality to functional imaging that allows real-time monitoring of both tumor burden and genomic changes throughout therapy.

Related publications

Article2016

Circulating tumor DNA (ctDNA) to track responses and to capture the genomic heterogeneity of metastatic melanoma.

Shahneen Sandhu, Stephen Q. Wong, Ismael A. Vergara, Jeanette Raleigh, Jason Callahan, Sarah Ftouni, Athena Hatzimihalis, Devbarna Sinha, Ken Doig, Andrew J. Colebatch, Gisela Mir-Arnau, Carleen Cullinane, David Gyorki, Damien Kee, Benjamin Brady, Mark Shackleton, Anthony T. Papenfuss, Rodney J. Hicks, Grant A. McArthur, Sarah‐Jane Dawson

Article2015

Circulating tumor DNA to monitor treatment response and detect acquired resistance in patients with metastatic melanoma

Elin S. Gray, Helen Rizos, Anna Reid, Suzanah C. Boyd, Michelle R. Pereira, Johnny Lo, Varsha Tembe, James Freeman, Jenny Lee, Richard A Scolyer, Kelvin Shenq Woei Siew, Chris Lomma, Adam Cooper, Muhammad A. Khattak, Tarek Meniawy, Georgina V. Long, Matteo S. Carlino, Michael Millward, Mel Ziman

Article2019

Analysis of the Whole-Exome Sequencing of Tumor and Circulating Tumor DNA in Metastatic Melanoma

Russell J. Diefenbach, Jenny Lee, Dario Strbenac, Jean Yang, Alexander M. Menzies, Matteo S. Carlino, Georgina V. Long, Andrew J. Spillane, Jonathan R. Stretch, Robyn P.M. Saw, John F. Thompson, Sydney Ch’ng, Richard A Scolyer, Richard Kefford, Helen Rizos

Article2022

Anchored Multiplex PCR Custom Melanoma Next Generation Sequencing Panel for Analysis of Circulating Tumor DNA

Russell J. Diefenbach, Jenny Lee, Ashleigh Stewart, Alexander M. Menzies, Matteo S. Carlino, Robyn P.M. Saw, Jonathan R. Stretch, Georgina V. Long, Richard A Scolyer, Helen Rizos

Article2019

Hypermethylation of Circulating Free DNA in Cutaneous Melanoma

Russell J. Diefenbach, Jenny Lee, David Chandler, Yinan Wang, Christian Pflueger, Georgina V. Long, Richard A Scolyer, Matteo S. Carlino, Alexander M. Menzies, Richard Kefford, Helen Rizos