Your search keyword '"N. Masque-Soler"' showing total 3 results

1. Longitudinal tracking of 97 esophageal adenocarcinomas using liquid biopsy sampling

Author

J M J Weaver, N. Masque Soler, Christopher C.W. Hughes, Rebecca C. Fitzgerald, K Lehovsky, Elizabeth C Smyth, Nicola Grehan, E. Ococks, Ginny Devonshire, H. Coles, Alexander M. Frankell, A. Northrop, A. Redmond, Adrienn Blasko, and Barbara Nutzinger

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Esophageal Neoplasms, medicine.medical_treatment, Adenocarcinoma, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Biomarkers, Tumor, medicine, Humans, Peripheral blood cell, Prospective Studies, Liquid biopsy, Survival rate, Aged, Chemotherapy, business.industry, Incidence (epidemiology), Hazard ratio, Liquid Biopsy, Cancer, Hematology, medicine.disease, Confidence interval, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Neoplasm Recurrence, Local, business

Abstract

The incidence of esophageal adenocarcinoma (EAC) is rapidly rising and has a 5-year survival rate of20%. Beyond TNM (tumor-node-metastasis) staging, no reliable risk stratification tools exist and no large-scale studies have profiled circulating tumor DNA (ctDNA) at relapse in EAC. Here we analyze the prognostic potential of ctDNA dynamics in EAC, taking into account clonal hematopoiesis with indeterminate potential (CHIP).A total of 245 samples from 97 patients treated with neoadjuvant chemotherapy and surgery were identified from the prospective national UK Oesophageal Cancer Clinical and Molecular Stratification (OCCAMS) consortium data set. A pan-cancer ctDNA panel comprising 77 genes was used. Plasma and peripheral blood cell samples were sequenced to a mean depth of 7082× (range 2196-28 524) and ctDNA results correlated with survival.Characteristics of the 97 patients identified were as follows: 83/97 (86%) male, median age 68 years (SD 9.5 years), 100% cT3/T4, 75% cN+. EAC-specific drivers had higher variant allele fractions than passenger mutations. Using stringent quality criteria 16/79 (20%) were ctDNA positive following resection; recurrence was observed in 12/16 (75%) of these. As much as 78/97 (80%) had CHIP analyses that enabled filtering for CHIP variants, which were found in 18/78 (23%) of cases. When CHIP was excluded, 10/63 (16%) patients were ctDNA positive and 9/10 of these (90%) recurred. With correction for CHIP, median cancer-specific survival for ctDNA-positive patients was 10.0 months versus 29.9 months for ctDNA-negative patients (hazard ratio 5.55, 95% confidence interval 2.42-12.71; P = 0.0003). Similar outcomes were observed for disease-free survival.We demonstrate in a large, national, prospectively collected data set that ctDNA in plasma following surgery for EAC is prognostic for relapse. Inclusion of peripheral blood cell samples can reduce or eliminate false positives from CHIP. In future, post-operative ctDNA could be used to risk stratify patients into high- and low-risk groups for intensification or de-escalation of adjuvant chemotherapy.

Published

2021

2. Assessing the clinical utility of circulating tumour DNA through longitudinal liquid biopsy sampling in oesophageal adenocarcinoma

Author

Christopher C.W. Hughes, Rebecca C. Fitzgerald, A. Frankell, Elizabeth C Smyth, E. Ococks, Ginny Devonshire, Nicola Grehan, A. Northrop, Adrienn Blasko, and N. Masque-Soler

Subjects

Oncology, Whole genome sequencing, medicine.medical_specialty, business.industry, Cancer, Hematology, Disease, Esophageal cancer, medicine.disease, Minimal residual disease, CDKN2A, Internal medicine, medicine, Liquid biopsy, business, Survival rate

Abstract

Background Oesophageal cancer is the eighth most frequently diagnosed form of cancer and has a dismal 5-year survival rate of 12%, with Oesophageal adenocarcinoma (OAC) being the most common sub-type in western countries (Ferlay et al., 2012). Previous studies in many cancer types have demonstrated potential clinical utility of circulating tumour DNA (ctDNA) for detecting minimal residual disease and tumour evolution through therapy, but there has been little investigation of this technology in large cohorts of OAC patients. Consequently, the aim of this study is to evaluate the clinical potential of longitudinal liquid biopsy sampling using 100 OAC cases. Methods Our approach uses the Roche-Avenio expanded panel and ultra-deep sequencing to detect genomic aberrations across 77 cancer genes in the ctDNA of OAC cases. All cases are late disease stage (T3 /T4) and have at least one plasma sample taken before surgery and on average two other samples taken at time points of clinical interest. One third of cases have associated whole genome sequencing of the primary tumour. Results Our results demonstrate that in spite of OAC being a low ctDNA shedding cancer type, ctDNA can be consistently detected in late disease cases. At least one mutation in OAC driver genes was identified in 69% of cases, some of which include TP53, SMAD4, and CDKN2A (Frankell et al., 2019). TP53 was the most frequently mutated gene, which is also observed in whole-genome sequencing (WGS) data. In addition, other OAC driver genes were mutated to a similar extent to the WGS data. Clinically relevant variants were identified in the plasma samples, such as SMAD4 which has been shown to be a prognostic biomarker in OAC. Therapeutically actionable targets not detected in the primary tumour were also captured, including ALK and PIK3CA. Moreover, minimal residual disease was detected after surgery in the majority of patients that went on to relapse. Conclusions These data suggest that ctDNA can be routinely detected in OAC and that clinically relevant alterations can also be identified at late stage of disease, which is when the majority of patients present. Overall our results indicate that there is potential for using targeted sequencing of ctDNA in the clinic. Legal entity responsible for the study The authors. Funding Educational grant from Roche for the library prep kits. Disclosure All authors have declared no conflicts of interest.

Published

2019

3. Optimising TNFRSF agonism and checkpoint blockade with a novel CD137/PD-L1 bispecific antibody

Author

S. Pechouckova, Emma Goodman, Mihriban Tuna, Michelle Morrow, Jose Munoz-Olaya, A. Knudsen, C. Gradinaru, Daniel Gliddon, Simon J. Marshall, Neil Brewis, Alexander Koers, Matthew Lakins, Deborah A. Jones, Raffaella Giambalvo, Carrie L. Hall, Sarah Batey, M. Davies, Mateusz Wydro, Francisca Wollerton, and N. Masque Soler

Subjects

Bispecific antibody, Oncology, biology, business.industry, PD-L1, CD137, biology.protein, Cancer research, Medicine, Agonism, Hematology, business, Blockade

Published

2018