Recent progress and challenges in screening and characterization of UGT1A1 inhibitors

Lv, Xia; Xia, Yangliu; Finel, Moshe; Wu, Jingjing; Ge, Guangbo; Yang, Ling

doi:10.1016/j.apsb.2018.09.005

Cited by 68 publications

(41 citation statements)

References 121 publications

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“…Similarly, several UGT1A1 substrates, like endogenous estradiol, bilirubin and clinical irinotecan, morphine, ezetimibe, all could be inhibited by CA and CA-containing herbal medicines, inducing clinical adverse reactions. Therefore, greater attention should be paid to avoid the potential risks of herbal medicines-drug interactions by considering the inhibitory effects of bioactive compounds on several human CYPs and UGTs (Lv et al, 2019;Zhou et al, 2019).…”

Section: Discussionmentioning

confidence: 99%

Metabolism and disposition of corylifol A from Psoralea corylifolia: metabolite mapping, isozyme contribution, species differences and identification of efflux transporters for corylifol A-O-glucuronide in HeLa1A1 cells

Yang

et al. 2020

Xenobiotica

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2020): Metabolism and disposition of corylifol A from Psoralea corylifolia: metabolite mapping, isozyme contribution, species differences, and identification of efflux transporters for corylifol A-O-glucuronide in HeLa1A1 cells, Xenobiotica, Abstract 1. Corylifol A (CA), a phenolic compound from Psoralea corylifolia, possessed several biological properties but poor bioavailability. Here we aimed to investigate the roles of cytochromes P450s (CYPs), UDP-glucuronosyltransferases (UGTs) and efflux transporters in metabolism and disposition of CA. 2. Metabolism of CA were evaluated in HLM, expressed CYPs and UGTs. Chemical inhibitors and shRNA-mediated gene siliencing of multidrug resistance-associated proteins (MRPs) and breast cancer resistance protein (BCRP) were performed to assess the roles of transporters in CA disposition. 3. Three oxidated metabolites (M1-M3) and two glucuronides (M4-M5) were detected. The intrinsic clearances (CL int ) values of M1 and M4 in HLM were 48.10 and 184.03 μL/min/mg, respectively. Additionally, CYP1A1, 2C8 and 2C19 were identified as main contributors with CL int values of 13.01~49.36 μL/min/mg, while UGT1A1, 1A7, 1A8 and 1A9 were with CL int values ranging form 85.01 to 284.07 μL/min/mg. Furthermore, activity correlation analysis proved CYP2C8, UGT1A1 and 1A9 were main active hepatic isozymes. Besides, rats and monkeys were appropriate model animals. Moreover, dipyridamole and MK571 both could significantly inhibit M4 efflux. Gene silencing results also indicated MRP4 and BCRP were major contributors in HeLa1A1 cells. 4. Taken together, CYPs, UGTs, MRP4 and BCRP were important determinants of CA A c c e p t e d M a n u s c r i p t pharmacokinetics.

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Section: Discussionmentioning

confidence: 99%

Metabolism and disposition of corylifol A from Psoralea corylifolia: metabolite mapping, isozyme contribution, species differences and identification of efflux transporters for corylifol A-O-glucuronide in HeLa1A1 cells

Yang

et al. 2020

Xenobiotica

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“…144 UGT1A1 inhibition has been suggested as the most likely cause of hyperbilirubinemia for several TKI. 143 Regorafenib and sorafenib were shown to strongly inhibit UGT1A1-mediated bilirubin glucuronidation which could have a significant effect on UGT1A1 activity in vivo, contrary to lapatinib and pazopanib. 145 Sorafenib, imatinib, and dasatinib were reported to inhibit UGT1A9-mediated paracetamol glucuronidation in vitro, inhibitions being also predicted to occur in vivo for sorafenib and imatinib.…”

Section: Inhibition Of Udp-glucuronosyltransferases By Tkimentioning

confidence: 99%

“…Particular attention is payed to UGT1A1 because of its involvement in bilirubin glucuronidation and its large interindividual variability due to UGT1A1*28 polymorphism . Regulatory agencies have thus recommended to assay the potential of new drugs to inhibit UGT1A1 prior approval to predict clinical hyperbilirubinemia . UGT1A1 inhibition has been suggested as the most likely cause of hyperbilirubinemia for several TKI .…”

Section: Inhibition Of Udp‐glucuronosyltransferases By Tkimentioning

confidence: 99%

“…Regulatory agencies have thus recommended to assay the potential of new drugs to inhibit UGT1A1 prior approval to predict clinical hyperbilirubinemia . UGT1A1 inhibition has been suggested as the most likely cause of hyperbilirubinemia for several TKI . Regorafenib and sorafenib were shown to strongly inhibit UGT1A1‐mediated bilirubin glucuronidation which could have a significant effect on UGT1A1 activity in vivo, contrary to lapatinib and pazopanib .…”

Section: Inhibition Of Udp‐glucuronosyltransferases By Tkimentioning

confidence: 99%

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Identifying the reactive metabolites of tyrosine kinase inhibitors in a comprehensive approach: Implications for drug‐drug interactions and hepatotoxicity

Paludetto

Puisset

Chatelut

et al. 2019

Medicinal Research Reviews

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Tyrosine kinase inhibitors (TKI) are small heterocyclic molecules targeting transmembrane and cytoplasmic tyrosine kinases that have met with considerable success in clinical oncology. TKI are associated with toxicities including liver injury that may be serious and even life‐threatening. Many of them require warnings in drug labeling against liver injury, and five of them have Black Box Warning (BBW) labels. Although drug‐induced liver injury is a matter of clinical and industrial concern, little is known about the underlying mechanisms that likely involve reactive metabolites (RM). RM are electrophiles or radicals originating from the metabolic activation of particular functional groups, known as structural alerts or toxicophores. RM are able to covalently bind to proteins and macromolecules, causing cellular damage and even cell death. If the adducted protein is the enzyme involved in RM formation, time‐dependent inhibition of the enzyme—also called mechanism‐based inhibition (MBI) or inactivation—can occur and lead to pharmacokinetic drug‐drug interactions. To mitigate RM liabilities, common practice in drug development includes avoiding structural alerts and assessing RM formation via RM trapping screens with soft and hard nucleophiles (glutathione, potassium cyanide, and methoxylamine) in liver microsomes. RM‐positive derivatives are further optimized to afford drug candidates with blocked or minimized bioactivation potential. However, different structural alerts are still commonly used scaffolds in drug design, including in TKI structures. This review focuses on the current state of knowledge of the relations among TKI structures, bioactivation pathways, RM characterization, and hepatotoxicity and cytochrome P450 MBI in vitro.

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“…[10][11][12] Inhibition of human CYP or UGT functions can not only trigger potentially adverse clinical DDIs, but could also result in metabolic disorders for endogenous molecules. [13][14][15] Considering the potential co-administration of PI-103 with other chemotherapeutic drugs, it is crucial to evaluate the potential risks of DDI in clinics.…”

Section: Introductionmentioning

confidence: 99%

An investigation of the metabolic activity, isozyme contribution, species differences and potential drug–drug interactions of PI-103, and the identification of efflux transporters for PI-103-O-glucuronide in HeLa1A9 cells

et al. 2020

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Recent progress and challenges in screening and characterization of UGT1A1 inhibitors

Cited by 68 publications

References 121 publications

Metabolism and disposition of corylifol A from Psoralea corylifolia: metabolite mapping, isozyme contribution, species differences and identification of efflux transporters for corylifol A-O-glucuronide in HeLa1A1 cells

Metabolism and disposition of corylifol A from Psoralea corylifolia: metabolite mapping, isozyme contribution, species differences and identification of efflux transporters for corylifol A-O-glucuronide in HeLa1A1 cells

Identifying the reactive metabolites of tyrosine kinase inhibitors in a comprehensive approach: Implications for drug‐drug interactions and hepatotoxicity

An investigation of the metabolic activity, isozyme contribution, species differences and potential drug–drug interactions of PI-103, and the identification of efflux transporters for PI-103-O-glucuronide in HeLa1A9 cells

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