P-gp substrate-induced neurotoxicity in an Abcb1a knock-in/Abcb1b knock-out mouse model with a mutated canine ABCB1 targeted insertion

被引:8
|
作者
Swain, M. D. [1 ]
Orzechowski, K. L. [1 ]
Swaim, H. L. [1 ]
Jones, Y. L. [1 ]
Robl, M. G. [2 ]
Tinaza, C. A. [2 ]
Myers, M. J. [1 ]
Jhingory, M. V. [1 ]
Buckely, L. E. [1 ]
Lancaster, V. A. [3 ]
Yancy, H. F. [1 ]
机构
[1] US FDA, Ctr Vet Med, Res Off, Laurel, MD 20708 USA
[2] US FDA, Ctr Food Safety & Appl Nutr, Off Appl Res & Safety Assessments, Laurel, MD 20708 USA
[3] US FDA, Ctr Vet Med, Off New Anim Drug Evaluat, Rockville, MD 20855 USA
关键词
P-glycoprotein; Collie; ABCB1-1; Delta; Mouse; Moxidectin; Doramectin; Digoxin; MULTIDRUG-RESISTANCE GENE; BLOOD-BRAIN-BARRIER; IVERMECTIN TOXICITY; DIAGNOSTIC-TEST; MDR1; MUTATION; GLYCOPROTEIN; DOGS; COLLIES; SENSITIVITY; MDR1-1-DELTA;
D O I
10.1016/j.rvsc.2012.10.025
中图分类号
S85 [动物医学(兽医学)];
学科分类号
0906 ;
摘要
Certain dog breeds, especially Collies, are observed to exhibit neurotoxicity to avermectin drugs, which are P-glycoprotein (P-gp) substrates. This neurotoxicity is due to an ABCB1 gene mutation (ABCB1-1 Delta) that results in non-functional P-gp expression. A developed Abcb1 a knock-in/Abcb1b knock-out mouse model expressing the ABCB1-1 Delta canine gene was previously reported and mice exhibited sensitivity upon ivermectin administration. Here, model and wild-type mice were administered P-gp substrates doramectin, moxidectin, and digoxin. While knock-in/knock-out mice exhibited ataxia, lethargy and tremor, wild-type mice remained unaffected. In addition, no neurotoxic clinical signs were observed in either mouse type administered domperidone, a P-gp substrate with no reported neurotoxicity in ABCB1-1 Delta Collies. Overall, neurotoxic signs displayed by model mice closely paralleled those observed in ivermectin-sensitive Collies. This model can be used to identify toxic P-gp substrates with altered safety in dog populations and may reduce dog use in safety studies that are part of the drug approval process. Published by Elsevier Ltd.
引用
收藏
页码:656 / 661
页数:6
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