Clinical validation of a tissue-agnostic genome-wide methylome enrichment molecular residual disease assay for head and neck malignancies

Liu, G.; Huang, S.H.; Ailles, L.; Rey-McIntyre, K.; Melton, C.A.; Shen, S.Y.; Burgener, J.M.; Brown, B.; Zhang, J.; Min, J.; Wang, Y.; Hall, O.; Jones, J.T.; Budhraja, K.; Provance, J.B.; Sosa, E.V.; Licon, A.; Williams, A.; Bratman, S.V.; Allen, B.A.; Zhang, J.; Hartman, A.-R.; De Carvalho, D.D.

doi:10.1016/j.annonc.2024.08.2348

Cited by 2 publications

References 32 publications

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Postoperative Lymphatic Exudate is a Proximal Source of ctDNA and Detects Recurrence in HPV-negative Head and Neck Cancer

Lazare,

Gu,

Earland

et al. 2024

Preprint

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Relapse is a major cause of failure after surgery in HPV-human papillomavirus (HPV) negative head and neck squamous cell carcinoma (HNSCC),), with up to 50% of patients recurring within 2 years. While clinicopathologic criteria exist for adjuvant treatment, these criteria are imprecise and have not changed for decades. However, no reliable method exists to tailor adjuvant therapy for individual patients based on risk of recurrence after surgery. Using an ultra-sensitive targeted sequencing approach, we demonstrate that circulating tumor DNA (ctDNA) in lymphatic exudate collected via surgical drains ("lymph") 24 hours after surgery accurately identifies MRD and outperforms plasma in an initial cohort of 36 HNSCC patients. We then applied the lymph ctDNA test to an independent, multi-site cohort of 37 HNSCC patients, replicating the original finding. Lymph performance was particularly enhanced in locoregional relapse in both cohorts and generalized to early stage (I-II) patients. Analysis of matched plasma collected at this early timepoint was not predictive of recurrence. We demonstrate a liquid biopsy approach using a historically overlooked biofluid to potentially enable precision adjuvant therapy and achieve superior oncologic outcomes. SIGNIFICANCE Postoperative lymphatic exudate represents a novel proximal analyte for MRD detection in HPV- HNSCC designed specifically for use in the immediate post-surgical window when adjuvant therapy decisions must be made. Accurate MRD identification at this early timepoint has potential to augment traditional pathology and personalize adjuvant treatment paradigms in HPV-negative HNSCC.

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Postoperative Lymphatic Exudate is a Proximal Source of ctDNA and Detects Recurrence in HPV-negative Head and Neck Cancer

Lazare,

Gu,

Earland

et al. 2024

Preprint

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Differential methylation of circulating free DNA assessed through cfMeDiP as a new tool for breast cancer diagnosis and detection of BRCA1/2 mutation

Grisolia,

Tufano,

Iannarone

et al. 2024

J Transl Med

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Background Recent studies have highlighted the importance of the cell-free DNA (cfDNA) methylation profile in detecting breast cancer (BC) and its different subtypes. We investigated whether plasma cfDNA methylation, using cell-free Methylated DNA Immunoprecipitation and High-Throughput Sequencing (cfMeDIP-seq), may be informative in characterizing breast cancer in patients with BRCA1/2 germline mutations for early cancer detection and response to therapy. Methods We enrolled 23 BC patients with germline mutation of BRCA1 and BRCA2 genes, 19 healthy controls without BRCA1/2 mutation, and two healthy individuals who carried BRCA1/2 mutations. Blood samples were collected for all study subjects at the diagnosis, and plasma was isolated by centrifugation. Cell-free DNA was extracted from 1 mL of plasma, and cfMeDIP-seq was performed for each sample. Shallow whole genome sequencing was performed on the immuno-precipitated samples. Then, the differentially methylated 300-bp regions (DMRs) between 25 BRCA germline mutation carriers and 19 non-carriers were identified. DMRs were compared with tumor-specific regions from public datasets to perform an unbiased analysis. Finally, two statistical classifiers were trained based on the GLMnet and random forest model to evaluate if the identified DMRs could discriminate BRCA-positive from healthy samples. Results We identified 7,095 hypermethylated and 212 hypomethylated regions in 25 BRCA germline mutation carriers compared to 19 controls. These regions discriminate tumors from healthy samples with high accuracy and sensitivity. We show that the circulating tumor DNA of BRCA1/2 mutant breast cancers is characterized by the hypomethylation of genes involved in DNA repair and cell cycle. We uncovered the TFs associated with these DRMs and identified that proteins of the Erythroblast Transformation Specific (ETS) family are particularly active in the hypermethylated regions. Finally, we assessed that these regions could discriminate between BRCA positives from healthy samples with an AUC of 0.95, a sensitivity of 88%, and a specificity of 94.74%. Conclusions Our study emphasizes the importance of tumor cell-derived DNA methylation in BC, reporting a different methylation profile between patients carrying mutations in BRCA1, BRCA2, and wild-type controls. Our minimally invasive approach could allow early cancer diagnosis, assessment of minimal residual disease, and monitoring of response to therapy. Supplementary Information The online version contains supplementary material available at 10.1186/s12967-024-05734-2.

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Clinical validation of a tissue-agnostic genome-wide methylome enrichment molecular residual disease assay for head and neck malignancies

Cited by 2 publications

References 32 publications

Postoperative Lymphatic Exudate is a Proximal Source of ctDNA and Detects Recurrence in HPV-negative Head and Neck Cancer

Postoperative Lymphatic Exudate is a Proximal Source of ctDNA and Detects Recurrence in HPV-negative Head and Neck Cancer

Differential methylation of circulating free DNA assessed through cfMeDiP as a new tool for breast cancer diagnosis and detection of BRCA1/2 mutation

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