Preventing Viral Pandemic Associated Risk of Cancer Death Using Less Invasive Diagnostic Tests- Liquid Biopsies

Completed

• Conditions: Biliary Tract Neoplasms; Neoplasm, Bladder; Gastro Intestinal Stromal Tumour; Neoplasm, Colorectal; Neoplasm of Lung; Neoplasms Pancreatic
• Interventions: Other: ctDNA blood sampling

• Registration Number: NCT04566614
• Lead Sponsor: Royal Marsden NHS Foundation Trust

Brief Summary

The purpose of this study is to investigate the feasibility of using ctDNA to support cancer diagnosis and risk stratification where invasive aerosol generating testing (and/or tissue biopsy) is challenging due to infection risk, technical impracticalities and resource limitations, such as during the COVID-19 pandemic and the subsequent recovery period.

Detailed Description

This is a prospective, single-centre cohort pilot study using ctDNA informed treatment decisions. If the pilot study is successful within certain tumour types then this protocol may be extended to investigate further the benefit of ctDNA informed treatment decision in those tumour types.

Patients with suspected malignancy for whom invasive biopsy for definitive histological diagnosis is challenging either due to COVID-19-related resource limitations, infection control or technical feasibility will be considered for this study. In this setting liquid biopsy may be used in lieu of tissue biopsy to facilitate treatment or may be used to prioritise standard of care invasive diagnostic tests. The former includes patients who require repeat biopsies for genomic analysis following non-informative results where these would inform standard of care treatment (i.e. NICE (National Institute for Health and Care Excellence)/Cancer Drug Fund (CDF) approved drugs). Tumour types included in this study are therefore those where invasive aerosol generating diagnostic tests such as bronchoscopy, gastrointestinal endoscopy (including endoscopic ultrasound (EUS)) are part of the standard diagnostic pathway and where capacity for these tests has become severely constrained during (and likely after) the COVID-19 pandemic. Tumour types affected include some suspected biliary tract, bladder, colorectal, GIST, lung and pancreatic cancers.

The study is planned to continue until a total of 144 patients have been enrolled. This is anticipated to take up to 12-18 months. Follow-up will continue until patients have diagnosis made (based on ctDNA result) and treatment decision made (deferred or immediate).

Potential patients will be identified in and will usually at the multidisciplinary team (MDT) meeting. They will give consent to participate in the trial and offered a liquid biopsy (ctDNA) in lieu of a tissue biopsy if considered suitable for PREVAIL - ctDNA. This may include patients who require repeat biopsies for further genomic analyses when repeat biopsies are not feasible where liquid biopsy may support prioritisation for invasive diagnostics earlier. ctDNA analysis will involve copy number variant detection and low coverage whole genomic sequencing. ctDNA gene panels have already been validated against tissue based molecular diagnostics for paediatrics (ct_PAED) and colorectal cancer (ct_GI).

This analysis will be performed in an accredited clinical diagnostic laboratory (Translational Research Laboratory, Institute of Cancer Research). Patients will be stratified for treatment or further investigation based on their ctDNA result (either positive or negative), suspected tumour type, radiological (including PREVAIL-imaging risk stratification pathway) and clinical characteristics.

PREVAIL ctDNA- Part 2 Study:

PREVAIL part 2 is a multi-centre, prospective study assessing the impact of Guardant360© liquid biopsy in patients with radiologically suspicious pancreatic cancer (PC) and biliary tract cancer (BTC)without histological confirmation of malignancy.

Liquid biopsies will be implemented into the routine diagnostic pathway across 6 RMP sites for patients with radiologically suspicious stage III/IV PC/BTC as part of the ACCESS implementation programme. Over 12 months, approximately 650 patients will be identified at individual sites by the local team when seen for an invasive procedure and referred in parallel to the Guardant360© test. These patients will proceed through an invasive diagnostic pathway as is standard of care and have a liquid biopsy as a new standard of care. Most patients will undergo both invasive tissue biopsy and liquid biopsy.

Patients with informative liquid biopsy result, but without a histological diagnosis of cancer (either due to inconclusive biopsy result or if the invasive procedure hasn't been performed) will be considered suitable for the study. Only patients with detectable ctDNA without histological confirmation will be suitable for this study (approximately ¼ of patients entering the ACCESS programme). The study is planned to run parallel to the ACCESS implementation programme and it aims to enrole 150 patients.

As part of this study, treatment may be recommended based on the liquid biopsy result. Patients with an invasive biopsy result which is suitable to guide treatment will not be eligible.

ctDNA results will be discussed at the molecular tumour board (MTB) to provide clinical context and validity of the genomic result. In addition, all patients will be discussed at a central upper gastrointestinal cancer multidisciplinary team meeting (MDM) to discuss treatment based on ctDNA results. Treating clinicians will have access to the MTB outcome and patients may be treated based on the ctDNA result in the context of symptoms, tumour markers, and imaging results as a complete diagnostic package.

Study Timeline

• Study First Submitted: 2020-06-02
• Study Start: 2020-06-18
• Study First Submitted QC: 2020-09-25
• Study First Posted: 2020-09-28
• Primary Completion: 2023-07-31
• Study Completion: 2025-01-31
• Status Verified: 2025-04
• Last Update Submitted: 2025-04-02
• Last Update Posted: 2025-04-06

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 128

Inclusion Criteria

• Participants aged ≥18 years old
• Patients with suspected malignancies of early stage colorectal cancer (FIT intermediate and high risk), early and late stage pancreatic cancer, biliary tract cancer, gastro-intestinal stromal tumours, lung cancer or bladder cancer, without a definitive histological diagnosis (including those with inconclusive biopsy result) or
• Patients with histological diagnosis of lung cancer without adequate tissue for NHS genomic test directory predictive biomarker testing
• Ability to provide informed consent.
• Patients with performance status suitable for oncological treatments (ECOG performance status 0-2).

Exclusion criterion:

• Patients with an established histological diagnosis adequate to support standard of care treatment

PART 2:

Inclusion criteria

• Included in the ACCESS implementation programme
• Has detectable ctDNA on Guardant360© assay
• Discussion at molecular tumour board and central multi-disciplinary meeting confirming ctDNA variant is supportive of diagnosis of PC/BTC (diagnostic or consistent with)
• Performance status suitable for oncological treatment
• Ability to provide informed consent

Exclusion criteria

1. Previously diagnosed invasive or haematological malignancy within the past 3 years
2. Outcome at the molecular tumour board not supportive of cancer diagnosis (possibly consistent or not consistent)

Exclusion Criteria

Not provided

Study & Design

• Study Type: OBSERVATIONAL
• Study Design: Not specified

Arm && Interventions

Group	Intervention	Description
Bladder Cancer Cohort	ctDNA blood sampling	Patients with suspected bladder cancer (localised and metastatic) will be offered ctDNA to support their diagnosis, in cases where cystoscopy and biopsy are difficult to obtain due to the COVID-19 pandemic. Patients with histological diagnosis will not be eligible for this study. A positive ctDNA result will be supportive of a diagnosis of bladder cancer, their treatment may be prioritised and decided based on this result in conjunction with radiological findings, patient presentation and after discussion between the treating physician and patient
Gastrointestinal Stromal Tumour Cohort	ctDNA blood sampling	Those with suspected Gastrointestinal Stromal Tumour Cohort (GIST) are eligible for this study. KIT and PDGFR mutation detected using ctDNA in conjunction with radiological features will be supportive of a diagnosis of GIST. This may allow for the use of directed targeted therapy, or prioritise surgical resection in some cases. Patients with histological diagnosis will not be eligible for this study. However, patients with inadequate tissue for KIT/PDGFR analysis will be eligible for PREVAIL-ctDNA to confirm the diagnosis of GIST and help guide treatment decisions
Biliary Tract Cohort	ctDNA blood sampling	Patients with suspected biliary tract cancer will be offered ctDNA to support a diagnosis in patients with suspected early stage, locally advanced and advanced disease. This includes patients with tumours that are technically challenging to access with invasive biopsy or due to limitations in endoscopic ultrasound due to the COVID-19 pandemic. Patients with histological diagnosis will not be eligible for this study. Patients with suspected cancer will have ctDNA result (positive or negative) discussed at MDT in conjunction with PREVAIL-imaging risk stratification pathway to risk stratify in terms of cancer risk (low, intermediate and high risk), serum tumour markers and patient presentation which will dictate the appropriate treatment. Those with metastatic disease will have their treatment decision based on ctDNA result, radiology and patient characteristics after discussion between the treating clinician and patient
Colorectal Cancer Cohort	ctDNA blood sampling	Patients with suspected colorectal cancer will often be referred following either suspicion on imaging or faecal immunochemical testing (FIT). FIT testing results will be used to prioritise patients for screening colonoscopy, in conjunction with the PREVAIL-imaging risk stratification pathway
Pancreatic Cancer Cohort	ctDNA blood sampling	Patients with suspected pancreatic cancer will be offered ctDNA to support a diagnosis in patients with suspected early stage, locally advanced and advanced disease. This includes patients with tumours that are technically challenging to access with invasive biopsy or due to limitations in endoscopic ultrasound due to the COVID-19 pandemic. Patients with histological diagnosis will not be eligible for this study. Patients with suspected cancer will have ctDNA result (positive or negative) discussed at MDT in conjunction with PREVAIL-imaging risk stratification pathway to risk stratify in terms of cancer risk (low, intermediate and high risk), serum tumour markers and patient presentation which will dictate the appropriate treatment. Those with metastatic disease will have their treatment decision based on ctDNA result, radiology and patient characteristics after discussion between the treating clinician and patient
Lung Cancer Cohort	ctDNA blood sampling	The use of ctDNA in the diagnosis and adaptive management of patients with lung cancer is well established, however not funded by NHS. As aerosol-generating bronchoscopy procedures have reduced due to the COVID-19 pandemic, patients with suspected lung cancer may be offered ctDNA to support the diagnosis. A positive ctDNA result in conjunction with radiological findings will assist in prioritising those suitable for upfront surgical resection, radiotherapy or systemic anti-cancer treatment. It may provide sufficient genotypic information to guide standard of care targeted therapies (usually two tests are required - biopsy and then next generation sequencing of extracted DNA), including in patients without sufficient tissue for EGFR and ALK testing which can be detected using ctDNA. The use of ctDNA to guide treatment decisions in this cohort will not require signed consent as it is considered a standard approach (not yet NHS funded)

Primary Outcome Measures

Name	Time	Method
ctDNA detection rate within different cancer types (and overall)	Throughout study completion, up to one year	The primary endpoint, ctDNA detection rate, overall and within different cancer types will be presented as a proportion of patients with a positive ctDNA test out of those tested, with 90% confidence intervals
PREVAIL ctDNA Part 2 Study	To run parallel for 12 months alongside the ACCESS implementation programme	Primary end point, Proportion of patients with detectable ctDNA which supports a diagnosis of malignancy and commence treatment

Secondary Outcome Measures

Name	Time	Method
PREVAIL ctDNA Part 2 Study secondary end point 5b	To run parallel for 12 months alongside the ACCESS implementation programme	Number of histopathology reviews
PREVAIL ctDNA Part 2 Study secondary end point 6c	To run parallel for 12 months alongside the ACCESS implementation programme	Number of hospital visits in diagnostic pathway
Proportion of patients with a positive ctDNA result which assisted in prioritising invasive diagnostic tests	Throughout study completion, up to one year	Proportion of patients with positive ctDNA result which assisted in prioritising invasive diagnostic tests will be presented as a proportion with 90% confidence intervals
PREVAIL ctDNA Part 2 Study secondary end point 3b- comparison with NHS targets	To run parallel for 12 months alongside the ACCESS implementation programme	Comparison of diagnostic pathway duration with 62 day wait target
PREVAIL ctDNA Part 2 Study secondary end point 4b	To run parallel for 12 months alongside the ACCESS implementation programme	Frequency of complications from invasive diagnostic procedures
PREVAIL ctDNA Part 2 Study secondary end point 5	To run parallel for 12 months alongside the ACCESS implementation programme	Number and type of invasive procedures performed
PREVAIL ctDNA Part 2 Study secondary end point 6b	To run parallel for 12 months alongside the ACCESS implementation programme	Cost per-quality adjusted-life-year of diagnostic pathway
Proportion of patients with a positive ctDNA result which identified a diagnosis and/or commenced treatment	Throughout study completion, up to one year	All secondary endpoints will be analysed in the patients diagnosed with suspected cancer, i.e. positive ctDNA result, unless stated. They will also be presented overall and by cancer type. The proportion of patients with positive ctDNA result which identified a diagnosis and/or commenced treatment will be presented as a proportion with 90% confidence intervals
PREVAIL ctDNA Part 2 Study secondary end point 1b	To run parallel for 12 months alongside the ACCESS implementation programme	Progression free survival
PREVAIL ctDNA Part 2 Study secondary end point 1c	To run parallel for 12 months alongside the ACCESS implementation programme	Overall survival
PREVAIL ctDNA Part 2 Study secondary end point 2	To run parallel for 12 months alongside the ACCESS implementation programme	Proportion of patients who undergo a repeated invasive procedure
PREVAIL ctDNA Part 2 Study secondary end point 4a	To run parallel for 12 months alongside the ACCESS implementation programme	Type of complications from invasive diagnostic procedures
PREVAIL ctDNA Part 2 Study secondary end point 6a	To run parallel for 12 months alongside the ACCESS implementation programme	Healthcare costs associated with diagnostic pathway
PREVAIL ctDNA Part 2 Study secondary end point 4c	To run parallel for 12 months alongside the ACCESS implementation programme	Severity of complications from invasive diagnostic procedures
The association of ctDNA result (positive versus negative) and the PREVAIL-imaging pathway scoring result	Throughout study completion, up to one year	The association between ctDNA result (positive versus negative) and the PREVAIL-imaging pathway scoring result will be assessed descriptively by presenting cross-tabulations and relevant proportions
Estimation of the cost of liquid biopsy in lieu of tissue biopsy as compared to standard of care investigations and treatments prioritisation	Throughout study completion, up to one year	Simple estimation of the cost of liquid biopsy in lieu of tissue biopsy as compared to standard of care investigations and treatments prioritisation will be performed
PREVAIL ctDNA Part 2 Study secondary end point 1a	To run parallel for 12 months alongside the ACCESS implementation programme	Treatment response objective response rate
PREVAIL ctDNA Part 2 Study secondary end point 3a- comparison with NHS targets	To run parallel for 12 months alongside the ACCESS implementation programme	Comparison of diagnostic pathway duration with NHS faster Diagnostic Standard (FDS)
PREVAIL ctDNA Part 2 Study secondary end point 5c	To run parallel for 12 months alongside the ACCESS implementation programme	Number of tissue based NGS performed
PREVAIL ctDNA Part 2 Study secondary end point 6d	To run parallel for 12 months alongside the ACCESS implementation programme	Length of hospital stay during diagnostic pathway

Trial Locations

Locations (1)

Royal Marsden Hospital; 🇬🇧 Sutton, Surrey, United Kingdom