Literature DB >> 30382184

Metabolism and disposition of pyrotinib in healthy male volunteers: covalent binding with human plasma protein.

Jian Meng1, Xiao-Yun Liu1, Sheng Ma2,3, Hua Zhang2,3, Song-da Yu1, Yi-Fan Zhang1, Mei-Xia Chen4, Xiao-Yu Zhu4, Yi Liu4, Ling Yi2,3, Xiao-Liang Ding2,3, Xiao-Yan Chen1, Li-Yan Miao5,6, Da-Fang Zhong7.   

Abstract

Pyrotinib is a novel irreversible EGFR/HER2 dual tyrosine kinase inhibitor that is used to treat HER2-positive breast cancer. In this study we investigated the metabolism and disposition of pyrotinib in six healthy Chinese men after a single oral dose of 402 mg of [14C]pyrotinib. At 240 h postdose, the mean cumulative excretion of the dose radioactivity was 92.6%, including 1.7% in urine and 90.9% in feces. In feces, oxidative metabolites were detected as major drug-related materials and the primary metabolic pathways were O-depicoline (M1), oxidation of pyrrolidine (M5), and oxidation of pyridine (M6-1, M6-2, M6-3, and M6-4). In plasma, the major circulating entities identified were pyrotinib, SHR150980 (M1), SHR151468 (M2), and SHR151136 (M5), accounting for 10.9%, 1.9%, 1.0%, and 3.0%, respectively, of the total plasma radioactivity based on the AUC0-∞ ratios. Approximately 58.3% of the total plasma radioactivity AUC0-∞ was attributed to covalently bound materials. After incubation of human plasma with [14C]pyrotinib at 37 °C for 2, 5, 8, and 24 h, the recovery of radioactivity by extraction was 97.4%, 91.8%, 69.6%, and 46.7%, respectively, revealing covalent binding occurred independently of enzymes. A group of pyrotinib adducts, including pyrotinib-lysine and pyrotinib adducts of the peptides Gly-Lys, Lys-Ala, Gly-Lys-Ala, and Lys-Ala-Ser, was identified after HCl hydrolysis of the incubated plasma. Therefore, the amino acid residue Lys190 of human serum albumin was proposed to covalently bind to pyrotinib via Michael addition. Finally, the covalently bound pyrotinib could dissociate from the human plasma protein and be metabolized by oxidation and excreted via feces.

Entities:  

Keywords:  EGFR/HER2 dual tyrosine kinase inhibitor; breast cancer; covalent binding; drug disposition; drug metabolism; human plasma; pyrotinib

Mesh:

Substances:

Year:  2018        PMID: 30382184      PMCID: PMC6786348          DOI: 10.1038/s41401-018-0176-6

Source DB:  PubMed          Journal:  Acta Pharmacol Sin        ISSN: 1671-4083            Impact factor:   6.150


  23 in total

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5.  Discovery and development of pyrotinib: A novel irreversible EGFR/HER2 dual tyrosine kinase inhibitor with favorable safety profiles for the treatment of breast cancer.

Authors:  Xin Li; Changyong Yang; Hong Wan; Ge Zhang; Jun Feng; Lei Zhang; Xiaoyan Chen; Dafang Zhong; Liguang Lou; Weikang Tao; Lianshan Zhang
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6.  Efficacy and Risk Factors of Pyrrotinib in Second- and Third-Line Treatments for HER2-Positive Advanced Breast Cancer.

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7.  Prediction of pyrotinib exposure based on physiologically-based pharmacokinetic model and endogenous biomarker.

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8.  Neoadjuvant Pyrotinib plus Trastuzumab and Chemotherapy for Stage I-III HER2-Positive Breast Cancer: A Phase II Clinical Trial.

Authors:  Juncheng Xuhong; Xiaowei Qi; Peng Tang; Linjun Fan; Li Chen; Fan Zhang; Xuanni Tan; Wenting Yan; Ling Zhong; Cheng He; Yan Liang; Lin Ren; Minghao Wang; Yi Zhang; Jun Jiang
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9.  Multiple Administrations of Itraconazole Increase Plasma Exposure to Pyrotinib in Chinese Healthy Adults.

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