Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib

SIMPLE SUMMARY: Systemic therapy in advanced hepatocellular-carcinomas (HCC) has limited benefits, but some patients show partial responses (PR) and a few even a complete response (CR). Understanding the biological mechanisms could help clinicians in decision-making. Aim of this study was to develop...

Descripción completa

Detalles Bibliográficos
Autores principales: Colombatto, Piero, Demirtas, Coskun Ozer, Ricco, Gabriele, Civitano, Luigi, Boraschi, Piero, Scalise, Paola, Cavallone, Daniela, Oliveri, Filippo, Romagnoli, Veronica, Bleve, Patrizia, Coco, Barbara, Salvati, Antonio, Urbani, Lucio, Bonino, Ferruccio, Brunetto, Maurizia Rossana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8123288/
https://www.ncbi.nlm.nih.gov/pubmed/33922938
http://dx.doi.org/10.3390/cancers13092064
_version_ 1783692860010266624
author Colombatto, Piero
Demirtas, Coskun Ozer
Ricco, Gabriele
Civitano, Luigi
Boraschi, Piero
Scalise, Paola
Cavallone, Daniela
Oliveri, Filippo
Romagnoli, Veronica
Bleve, Patrizia
Coco, Barbara
Salvati, Antonio
Urbani, Lucio
Bonino, Ferruccio
Brunetto, Maurizia Rossana
author_facet Colombatto, Piero
Demirtas, Coskun Ozer
Ricco, Gabriele
Civitano, Luigi
Boraschi, Piero
Scalise, Paola
Cavallone, Daniela
Oliveri, Filippo
Romagnoli, Veronica
Bleve, Patrizia
Coco, Barbara
Salvati, Antonio
Urbani, Lucio
Bonino, Ferruccio
Brunetto, Maurizia Rossana
author_sort Colombatto, Piero
collection PubMed
description SIMPLE SUMMARY: Systemic therapy in advanced hepatocellular-carcinomas (HCC) has limited benefits, but some patients show partial responses (PR) and a few even a complete response (CR). Understanding the biological mechanisms could help clinicians in decision-making. Aim of this study was to develop a physic-mathematical model to investigate tumor dynamics using α-fetoprotein (AFP) and protein induced by vitamin K absence-II (PIVKA-II) measures combined with digital imaging. The model was set-up in three prototype patients with CR/PR to sorafenib and PR to regorafenib, and then applied in seven patients with different types of response. Overall, the rate constant of cancer cells production ranged between 0.250–0.372 C × day(−1). During therapy, neo-angiogenesis reduction was higher in four CR than in four PR or stable disease (SD) and in two non-responders (median: 83.2% vs. 29.4% vs. 2.0%). Tumor vasculature decay appeared accelerated in CR. We conclude that modeling serological and imaging biomarkers could help personalization of systemic therapy. ABSTRACT: In advanced HCC, tyrosine-kinase inhibitors obtain partial responses (PR) in some patients and complete responses (CR) in a few. Better understanding of the mechanism of response could be achieved by the radiomic approach combining digital imaging and serological biomarkers (α-fetoprotein, AFP and protein induced by vitamin K absence-II, PIVKA-II) kinetics. A physic-mathematical model was developed to investigate cancer cells and vasculature dynamics in three prototype patients receiving sorafenib and/or regorafenib and applied in seven others for validation. Overall four patients showed CR, two PR, two stable-disease (SD) and two progressive-disease (PD). The rate constant of cancer cells production was higher in PD than in PR-SD and CR (median: 0.398 vs. 0.325 vs. 0.316 C × day(−1)). Therapy induced reduction of neo-angiogenesis was greater in CR than in PR-SD and PD (median: 83.2% vs. 29.4% and 2.0%), as the reduction of cell-proliferation (55.2% vs. 7.6% and 0.7%). An additional dose-dependent acceleration of tumor vasculature decay was also observed in CR. AFP and cancer cells followed the same kinetics, whereas PIVKA-II time/dose dependent fluctuations were influenced also by tissue ischemia. In conclusion, pending confirmation in a larger HCC cohort, modeling serological and imaging biomarkers could be a new tool for systemic therapy personalization.
format Online
Article
Text
id pubmed-8123288
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-81232882021-05-16 Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib Colombatto, Piero Demirtas, Coskun Ozer Ricco, Gabriele Civitano, Luigi Boraschi, Piero Scalise, Paola Cavallone, Daniela Oliveri, Filippo Romagnoli, Veronica Bleve, Patrizia Coco, Barbara Salvati, Antonio Urbani, Lucio Bonino, Ferruccio Brunetto, Maurizia Rossana Cancers (Basel) Article SIMPLE SUMMARY: Systemic therapy in advanced hepatocellular-carcinomas (HCC) has limited benefits, but some patients show partial responses (PR) and a few even a complete response (CR). Understanding the biological mechanisms could help clinicians in decision-making. Aim of this study was to develop a physic-mathematical model to investigate tumor dynamics using α-fetoprotein (AFP) and protein induced by vitamin K absence-II (PIVKA-II) measures combined with digital imaging. The model was set-up in three prototype patients with CR/PR to sorafenib and PR to regorafenib, and then applied in seven patients with different types of response. Overall, the rate constant of cancer cells production ranged between 0.250–0.372 C × day(−1). During therapy, neo-angiogenesis reduction was higher in four CR than in four PR or stable disease (SD) and in two non-responders (median: 83.2% vs. 29.4% vs. 2.0%). Tumor vasculature decay appeared accelerated in CR. We conclude that modeling serological and imaging biomarkers could help personalization of systemic therapy. ABSTRACT: In advanced HCC, tyrosine-kinase inhibitors obtain partial responses (PR) in some patients and complete responses (CR) in a few. Better understanding of the mechanism of response could be achieved by the radiomic approach combining digital imaging and serological biomarkers (α-fetoprotein, AFP and protein induced by vitamin K absence-II, PIVKA-II) kinetics. A physic-mathematical model was developed to investigate cancer cells and vasculature dynamics in three prototype patients receiving sorafenib and/or regorafenib and applied in seven others for validation. Overall four patients showed CR, two PR, two stable-disease (SD) and two progressive-disease (PD). The rate constant of cancer cells production was higher in PD than in PR-SD and CR (median: 0.398 vs. 0.325 vs. 0.316 C × day(−1)). Therapy induced reduction of neo-angiogenesis was greater in CR than in PR-SD and PD (median: 83.2% vs. 29.4% and 2.0%), as the reduction of cell-proliferation (55.2% vs. 7.6% and 0.7%). An additional dose-dependent acceleration of tumor vasculature decay was also observed in CR. AFP and cancer cells followed the same kinetics, whereas PIVKA-II time/dose dependent fluctuations were influenced also by tissue ischemia. In conclusion, pending confirmation in a larger HCC cohort, modeling serological and imaging biomarkers could be a new tool for systemic therapy personalization. MDPI 2021-04-25 /pmc/articles/PMC8123288/ /pubmed/33922938 http://dx.doi.org/10.3390/cancers13092064 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Colombatto, Piero
Demirtas, Coskun Ozer
Ricco, Gabriele
Civitano, Luigi
Boraschi, Piero
Scalise, Paola
Cavallone, Daniela
Oliveri, Filippo
Romagnoli, Veronica
Bleve, Patrizia
Coco, Barbara
Salvati, Antonio
Urbani, Lucio
Bonino, Ferruccio
Brunetto, Maurizia Rossana
Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title_full Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title_fullStr Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title_full_unstemmed Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title_short Modeling Hepatocellular Carcinoma Cells Dynamics by Serological and Imaging Biomarkers to Explain the Different Responses to Sorafenib and Regorafenib
title_sort modeling hepatocellular carcinoma cells dynamics by serological and imaging biomarkers to explain the different responses to sorafenib and regorafenib
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8123288/
https://www.ncbi.nlm.nih.gov/pubmed/33922938
http://dx.doi.org/10.3390/cancers13092064
work_keys_str_mv AT colombattopiero modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT demirtascoskunozer modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT riccogabriele modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT civitanoluigi modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT boraschipiero modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT scalisepaola modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT cavallonedaniela modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT oliverifilippo modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT romagnoliveronica modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT blevepatrizia modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT cocobarbara modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT salvatiantonio modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT urbanilucio modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT boninoferruccio modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib
AT brunettomauriziarossana modelinghepatocellularcarcinomacellsdynamicsbyserologicalandimagingbiomarkerstoexplainthedifferentresponsestosorafenibandregorafenib

Ejemplares similares