| Literature DB >> 33922938 |
Piero Colombatto1, Coskun Ozer Demirtas2, Gabriele Ricco1, Luigi Civitano1, Piero Boraschi3, Paola Scalise3, Daniela Cavallone1,4, Filippo Oliveri1, Veronica Romagnoli1, Patrizia Bleve1, Barbara Coco1, Antonio Salvati1, Lucio Urbani5, Ferruccio Bonino6, Maurizia Rossana Brunetto1,4,5.
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.Entities:
Keywords: AFP; HCC; PIVKA-II; digital imaging; hepatocellular carcinoma; kinetics; mathematical modeling; regorafenib; sorafenib
Year: 2021 PMID: 33922938 DOI: 10.3390/cancers13092064
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639