Drug discovery to counteract antinociceptive tolerance with mu-opioid receptor endocytosis

Author:

Chao Po-KuanORCID,Ke Yi-Yu,Chang Hsiao-Fu,Huang Yi-Han,Ou Li-Chin,Chuang Jian-Ying,Lin Yen-Chang,Lee Pin-Tse,Chang Wan-Ting,Chen Shu-Chun,Ueng Shau-Hua,Hsu John Tsu-An,Tao Pao-Luh,Law Ping-Yee,Loh Horace H.,Shih Chuan,Yeh Shiu-HwaORCID

Abstract

AbstractMorphine antinociceptive tolerance is highly correlated with its poor ability to promote mu-opioid– receptor (MOR) endocytosis. Our objective was to discover a novel positive allosteric modulator of MOR to enhance morphine-induced MOR endocytosis. We used high-throughput screening to identify several cardiotonic steroids as positive allosteric modulators of morphine-induced MOR endocytosis having high potency and efficacy, independently of Na+/K+-ATPase inhibition. Convallatoxin was found to enhance morphine-induced MOR endocytosis through an adaptor protein 2/clathrin-dependent mechanism without regulating G protein- or β-arrestin-mediated pathways. Both F243 and I292 residues of MOR were essential to the effect of convallatoxin on MOR endocytosis. Co-treatment with chronic morphine and convallatoxin reduced morphine tolerance in animal models of acute thermal pain and chronic inflammatory pain. Acute convallatoxin administration reversed morphine tolerance in morphine-tolerant mice. These findings suggest that cardiotonic steroids are potentially therapeutic for morphine side effects and open a new avenue for the study of MOR trafficking.

Publisher

Cold Spring Harbor Laboratory

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