BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Lung cancer, Liver, Laser capture microdissection, Clofibrate, rs7903146, DNMT1)
Bookmark Forward

Differences in Hydrolase Activities in the Liver and Small Intestine between Marmosets and Humans.

Shiori Honda, Tatsuki Fukami, Keiya Hirosawa, Takuya Tsujiguchi, Yongjie Zhang, Masataka Nakano, Shotaro Uehara, Yasuhiro Uno, Hiroshi Yamazaki, Miki Nakajima

Drug metabolism and disposition: the biological fate of chemicals 2021 Sep


filter terms:
  • callithrix (1)
  • CES 1 (6)
  • ces1 protein, human (1)
  • CES2 (6)
  • dogs (1)
  • drug- reactions (1)
  • ester (2)
  • humans (11)
  • hydrolases (8)
  • hydrolysis (2)
  • liver (10)
  • marmosets (14)
  • mice (1)
  • protein human (3)
  • protein levels (1)
  • rats (1)
  • rifabutin (1)
  • rifamycins (3)
  • small intestine (2)
  • species (2)
  • species specificity (1)
    • Sizes of these terms reflect their relevance to your search.

    For drug development, species differences in drug-metabolism reactions present obstacles for predicting pharmacokinetics in humans. We characterized the species differences in hydrolases among humans and mice, rats, dogs, and cynomolgus monkeys. In this study, to expand the series of such studies, we attempted to characterize marmoset hydrolases. We measured hydrolase activities for 24 compounds using marmoset liver and intestinal microsomes, as well as recombinant marmoset carboxylesterase (CES) 1, CES2, and arylacetamide deacetylase (AADAC). The contributions of CES1, CES2, and AADAC to hydrolysis in marmoset liver microsomes were estimated by correcting the activities by using the ratios of hydrolase protein levels in the liver microsomes and those in recombinant systems. For six out of eight human CES1 substrates, the activities in marmoset liver microsomes were lower than those in human liver microsomes. For two human CES2 substrates and three out of seven human AADAC substrates, the activities in marmoset liver microsomes were higher than those in human liver microsomes. Notably, among the three rifamycins, only rifabutin was hydrolyzed by marmoset tissue microsomes and recombinant AADAC. The activities for all substrates in marmoset intestinal microsomes tended to be lower than those in liver microsomes, which suggests that the first-pass effects of the CES and AADAC substrates are due to hepatic hydrolysis. In most cases, the sums of the values of the contributions of CES1, CES2, and AADAC were below 100%, which indicated the involvement of other hydrolases in marmosets. In conclusion, we clarified the substrate preferences of hydrolases in marmosets. SIGNIFICANCE STATEMENT: This study confirmed that there are large differences in hydrolase activities between humans and marmosets by characterizing marmoset hydrolase activities for compounds that are substrates of human CES1, CES2, or arylacetamide deacetylase. The data obtained in this study may be useful for considering whether marmosets are appropriate for examining the pharmacokinetics and efficacies of new chemical entities in preclinical studies. Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.

    Citation

    Shiori Honda, Tatsuki Fukami, Keiya Hirosawa, Takuya Tsujiguchi, Yongjie Zhang, Masataka Nakano, Shotaro Uehara, Yasuhiro Uno, Hiroshi Yamazaki, Miki Nakajima. Differences in Hydrolase Activities in the Liver and Small Intestine between Marmosets and Humans. Drug metabolism and disposition: the biological fate of chemicals. 2021 Sep;49(9):718-728

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 34135089

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.