Results from IMMUNOMICS-VHIO platform’s first study demonstrate the efficacy of ultrasensitive liquid biopsy in predicting and monitoring immunotherapy response

Results from IMMUNOMICS-VHIO platform’s first study demonstrate the efficacy of  ultrasensitive liquid biopsy in predicting and monitoring immunotherapy response

• Co-led by Rodrigo Toledo and Elena Garralda, IMMUNOMICS-VHIO is a platform for the discovery and validation of liquid biopsy biomarkers of immunotherapy outcomes.
• Published today in Clinical Cancer Research, results from this project’s first study show that ultrasensitive circulating tumor DNA analysis can predict immunotherapy response in patients with advanced cancer across diverse tumor types and could potentially optimize patient management and therapeutic decision-making.
• IMMUNOMICS-VHIO is part of one of VHIO’s institutional programs, the BBVA Foundation Comprehensive Program of Cancer Immunotherapy and Immunology (CAIMI), funded by the Fundación BBVA.

 

Published today in Clinical Cancer Research, findings from a study led by investigators at the Vall d’Hebron Institute of Oncology (VHIO), which forms part of the Vall d’Hebron Campus, underscore the efficacy of analyzing circulating tumor DNA (ctDNA) using a highly sensitive liquid biopsy platform for evaluating early response, predicting survival and tumor progression in patients with advanced cancers who received treatment with immunotherapy in the context of phase 1 clinical trials.

These are the first results from IMMUNOMICS-VHIO, a project-platform for the discovery and validation of liquid biopsy biomarkers of response to immunotherapy. IMMUNOMICS-VHIO has been developed as part of the BBVA Foundation Comprehensive Program of Cancer Immunotherapy and Immunology (CAIMI), funded by the Fundación BBVA. Rodrigo Toledo’s laboratory is also supported by the Fundación FERO, and this present work counted on the collaboration of the PREDICT project (Personalized REsponse Imaging biomarker for Cancer immunotherapy).

This work has also been conducted as part of the EU-funded Cancer Core Europe Building Data Rich Clinical Trials (CCE-DART) project, and the UpSMART Accelerator Consortium which is co-funded by the Asociación Española Contra el Cáncer (AECC).

The need for robust biomarkers in cancer immunotherapy

Immunotherapy has transformed cancer treatment by leveraging the patient’s own immune system to recognize and eliminate tumor cells. The approval of  the first  immune checkpoint inhibitor (ICI) in 2011 for metastatic melanoma marked a paradigm shift in cancer therapy, leading to the subsequent development of various antibodies targeting key immune checkpoints.

“Despite these advances, overall response rates to immune checkpoint inhibitors remains modest, typically ranging from 10 % to 20 %,” observed Elena Garralda, Director of VHIO’s Research Unit for Molecular Therapy of Cancer (UITM) – CaixaResearch, and co-corresponding author of this present study. “This spotlights the urgent need to identify robust, predictive biomarkers of immunotherapy response to optimize personalized treatment and maximize patient benefits.”

Ultrasensitive ctDNA monitoring

The detection of tumor-derived DNA fragments in blood (ctDNA) by liquid biopsy has emerged as a minimally invasive technique to help predict patients' response to immunotherapy and potentially optimize treatment selection. Analyzing ctDNA before treatment, and serially throughout the course of the disease, allows for the identification of genetic changes occurring in a tumor and enables a better understanding of its evolution.

“In our laboratory we use different approaches to sequence, capture, and monitor the evolution of tumors in cancer patients undergoing immunotherapy,” said Rodrigo Toledo, co-corresponding author, Head of VHIO’s Biomarkers and Clonal Dynamics Group, and Coordinator of the CIBERONC (Spanish Biomedical Research Centre in Cancer) network’s Liquid Biopsy and Biomarker Working Module.

 “With this work, we have evaluated the utility of next-generation ultrasensitive liquid biopsy and characterized specific patterns of ctDNA that correlate with response or resistance to therapy.”

The investigators analyzed 1,455 longitudinal plasma ctDNA samples serialized over time from a  primary/retrospective cohort of 136 patients with refractory metastatic solid tumors across 24 cancer types, who received 1 to 3 successive lines of immunotherapy in the context of phase 1 clinical trials, followed by an independent prospective validation cohort of 66 patients (374 samples).

A promising biomarker for predicting and monitoring response to immunotherapy 

Lower levels of ctDNA at baseline associated with higher progression-free survival and overall survival. At three weeks after initiating treatment, changes in ctDNA levels correlated with improved survival and disease control, and complete clearance of ctDNA from blood at any time strongly associated with radiological response and prolonged survival. Additionally, ctDNA dynamics distinguished true progression from pseudoprogression and predicted outcomes in patients receiving continued immunotherapy beyond initial progression.

“In conclusion,” added Rodrigo Toledo, “our comprehensive analysis of ultrasensitive ctDNA in patients with advanced cancers undergoing treatment with immunotherapy has demonstrated notable utility for early patient stratification, treatment response monitoring, and detection of disease progression. In addition to the ongoing IMMUNOMICS-VHIO project, our laboratory continues to develop new liquid biopsy techniques that can complement, or even reduce, the use of traditional imaging techniques for monitoring therapeutic responses.”

Moving forward,  the investigators will validate the utility of data generated by ultrasensitive liquid biopsy in predicting whether the treatment under study will likely yield clinical benefits for the patient, prior to performing imaging response assessment according to established evaluation criteria in phase one clinical trials.

“Anticipating response to therapy is key to optimizing patient management and therapeutic decision-making. It also enables us to more rapidly assess whether it is advisable for the patient to continue participating in the clinical trial or, if not, whether we should propose a new therapeutic strategy,” concluded Garralda.

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About VHIO

The Vall d’Hebron Institute of Oncology (VHIO), established in 2006 and located within the Vall d’Hebron Campus, is a reference comprehensive cancer center for personalized medicine in oncology. Through our purely translational and multidisciplinary research model, we aim to improve the prevention, early diagnosis and treatment of cancer by transforming the latest scientific discoveries made in the laboratory into early phase clinical trials for the development of more effective therapies to improve the quality of life and survival  of cancer patients.

VHIO forms part of the CERCA – Research Centres of Catalonia system and is accredited as a Severo Ochoa Center of Excellence.

Research at VHIO would not be possible without the support received from our patrons –Generalitat de Catalunya, Fundació Privada CELLEX, "La Caixa" Foundation, Fundación FERO, Fundación BBVA and the CRIS Cancer Foundation– and the public funding it receives as well as the generous support from institutional supporters, private institutions, companies, associations, societies, and individual donors. Only with such continued support will VHIO continue to advance personalized and targeted therapies against cancer.

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