Purpose: Treatment outcomes for hepatoblastoma have improved markedly in the contemporary treatment era, principally due to therapy intensification, with overall survival increasing from 35% in the 1970s to 90% at present. Unfortunately, these advancements are accompanied by an increased incidence of toxicities. A detailed analysis of age as a prognostic factor may support individualized risk-based therapy stratification. Methods: We evaluated 1605 patients with hepatoblastoma included in the CHIC database to assess the relationship between event-free survival (EFS) and age at diagnosis. Further analysis included the age distribution of additional risk factors and the interaction of age with other known prognostic factors. Results: Risk for an event increases progressively with increasing age at diagnosis. This pattern could not be attributed to the differential distribution of other known risk factors across age. Newborns and infants are not at increased risk of treatment failure. The interaction between age and other adverse risk factors demonstrates an attenuation of prognostic relevance with increasing age in the following categories: metastatic disease, AFP < 100 ng/mL, and tumor rupture. Conclusion: Risk for an event increased with advancing age at diagnosis. Increased age attenuates the prognostic influence of metastatic disease, low AFP, and tumor rupture. Age could be used to modify recommended chemotherapy intensity.

The importance of age as prognostic factor for the outcome of patients with hepatoblastoma. Analysis from the Children's Hepatic tumors International Collaboration (CHIC) database / Haeberle, B.; Rangaswami, A.; Krailo, M.; Czauderna, P.; Hiyama, E.; Maibach, R.; Lopez-Terrada, D.; Aronson, D. C.; Alaggio, R.; Ansari, M.; Malogolowkin, M. H.; Perilongo, G.; O'Neill, A. F.; Trobaugh-Lotrario, A. D.; Watanabe, K.; Schmid, I.; von Schweinitz, D.; Ranganathan, S.; Yoshimura, K.; Hishiki, T.; Tanaka, Y.; Piao, J.; Feng, Y.; Rinaldi, E.; Saraceno, D.; Derosa, M.; Meyers, R. L.. - In: PEDIATRIC BLOOD & CANCER. - ISSN 1545-5009. - 67:8(2020), pp. 1-8. [10.1002/pbc.28350]

The importance of age as prognostic factor for the outcome of patients with hepatoblastoma. Analysis from the Children's Hepatic tumors International Collaboration (CHIC) database

Alaggio R.;Perilongo G.;
2020

Abstract

Purpose: Treatment outcomes for hepatoblastoma have improved markedly in the contemporary treatment era, principally due to therapy intensification, with overall survival increasing from 35% in the 1970s to 90% at present. Unfortunately, these advancements are accompanied by an increased incidence of toxicities. A detailed analysis of age as a prognostic factor may support individualized risk-based therapy stratification. Methods: We evaluated 1605 patients with hepatoblastoma included in the CHIC database to assess the relationship between event-free survival (EFS) and age at diagnosis. Further analysis included the age distribution of additional risk factors and the interaction of age with other known prognostic factors. Results: Risk for an event increases progressively with increasing age at diagnosis. This pattern could not be attributed to the differential distribution of other known risk factors across age. Newborns and infants are not at increased risk of treatment failure. The interaction between age and other adverse risk factors demonstrates an attenuation of prognostic relevance with increasing age in the following categories: metastatic disease, AFP < 100 ng/mL, and tumor rupture. Conclusion: Risk for an event increased with advancing age at diagnosis. Increased age attenuates the prognostic influence of metastatic disease, low AFP, and tumor rupture. Age could be used to modify recommended chemotherapy intensity.
2020
age; CHIC; hepatoblastoma; pediatric liver tumor; prognostic factor
01 Pubblicazione su rivista::01a Articolo in rivista
The importance of age as prognostic factor for the outcome of patients with hepatoblastoma. Analysis from the Children's Hepatic tumors International Collaboration (CHIC) database / Haeberle, B.; Rangaswami, A.; Krailo, M.; Czauderna, P.; Hiyama, E.; Maibach, R.; Lopez-Terrada, D.; Aronson, D. C.; Alaggio, R.; Ansari, M.; Malogolowkin, M. H.; Perilongo, G.; O'Neill, A. F.; Trobaugh-Lotrario, A. D.; Watanabe, K.; Schmid, I.; von Schweinitz, D.; Ranganathan, S.; Yoshimura, K.; Hishiki, T.; Tanaka, Y.; Piao, J.; Feng, Y.; Rinaldi, E.; Saraceno, D.; Derosa, M.; Meyers, R. L.. - In: PEDIATRIC BLOOD & CANCER. - ISSN 1545-5009. - 67:8(2020), pp. 1-8. [10.1002/pbc.28350]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1626059
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