Small molecule protein kinase inhibitors (PKIs) have become an effective strategy for cancer patients. However, hepatotoxicity is a major safety concern of these drugs, since the majority are reported to increase transaminases, and few of them (Idelalisib, Lapatinib, Pazopanib, Pexidartinib, Ponatinib, Regorafenib, Sunitinib) have a boxed label warning. The exact rate of PKI-induced hepatoxicity is not well defined due to the fact that the majority of data arise from pre-registration or registration trials on fairly selected patients, and the post-marketing data are often based only on the most severe described cases, whereas most real practice studies do not include drug-related hepatotoxicity as an end point. Although these side effects are usually reversible by dose adjustment or therapy suspension, or by switching to an alternative PKI, and fatality is uncommon, all patients undergoing PKIs should be carefully pre-evaluated and monitored. The management of this complication requires an individually tailored reappraisal of the risk/benefit ratio, especially in patients who are responding to therapy. This review reports the currently available data on the risk and management of hepatotoxicity of all the approved PKIs.

Vigano, M., La Milia, M., Grassini, M., Pugliese, N., De Giorgio, M., Fagiuoli, S. (2023). Hepatotoxicity of Small Molecule Protein Kinase Inhibitors for Cancer. CANCERS, 15(6) [10.3390/cancers15061766].

Hepatotoxicity of Small Molecule Protein Kinase Inhibitors for Cancer

La Milia M.;Fagiuoli S.
Ultimo
2023

Abstract

Small molecule protein kinase inhibitors (PKIs) have become an effective strategy for cancer patients. However, hepatotoxicity is a major safety concern of these drugs, since the majority are reported to increase transaminases, and few of them (Idelalisib, Lapatinib, Pazopanib, Pexidartinib, Ponatinib, Regorafenib, Sunitinib) have a boxed label warning. The exact rate of PKI-induced hepatoxicity is not well defined due to the fact that the majority of data arise from pre-registration or registration trials on fairly selected patients, and the post-marketing data are often based only on the most severe described cases, whereas most real practice studies do not include drug-related hepatotoxicity as an end point. Although these side effects are usually reversible by dose adjustment or therapy suspension, or by switching to an alternative PKI, and fatality is uncommon, all patients undergoing PKIs should be carefully pre-evaluated and monitored. The management of this complication requires an individually tailored reappraisal of the risk/benefit ratio, especially in patients who are responding to therapy. This review reports the currently available data on the risk and management of hepatotoxicity of all the approved PKIs.
Articolo in rivista - Articolo scientifico
cancer; drug-induced liver injury; hepatitis; hepatotoxicity; liver failure; tyrosine kinase inhibitors;
English
14-mar-2023
2023
15
6
1766
open
Vigano, M., La Milia, M., Grassini, M., Pugliese, N., De Giorgio, M., Fagiuoli, S. (2023). Hepatotoxicity of Small Molecule Protein Kinase Inhibitors for Cancer. CANCERS, 15(6) [10.3390/cancers15061766].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/411275
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