A Mass Balance Study of [C]SHR6390 (dalpiciclib), a Selective and Potent CDK4/6 Inhibitor in Humans

Overview

Journal Front Pharmacol

Date 2023 Apr 17

PMID 37063263

Authors

Hua Zhang

Shu Yan

Yan Zhan

Sheng Ma

Yicong Bian

Shaorong Li

Junjun Tian

Guangze Li

Dafang Zhong

Xingxing Diao

Liyan Miao

Affiliations

Soon will be listed here.

Abstract

SHR6390 (dalpiciclib) is a selective and effective cyclin-dependent kinase (CDK) 4/6 inhibitor and an effective cancer therapeutic agent. On 31 December 2021, the new drug application was approved by National Medical Product Administration (NMPA). The metabolism, mass balance, and pharmacokinetics of SHR6390 in 6 healthy Chinese male subjects after a single oral dose of 150 mg [C]SHR6390 (150 µCi) in this research. The of SHR6390 was 3.00 h. In plasma, the of SHR6390 and its relative components was approximately 17.50 h. The radioactivity B/P (blood-to-plasma) AUC ratio was 1.81, indicating the preferential distribution of drug-related substances in blood cells. At 312 h after administration, the average cumulative excretion of radioactivity was 94.63% of the dose, including 22.69% in urine and 71.93% in stool. Thirteen metabolites were identified. In plasma, because of the low level of radioactivity, only SHR6390 was detected in pooled AUC plasma. Stool SHR6390 was the main component in urine and stool. Five metabolites were identified in urine, and 12 metabolites were identified in stool. Overall, faecal clearance is the main method of excretion.

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