A low pKa ligand inhibits cancer-associated pain in mice by activating peripheral mu-opioid receptors

被引:11
作者
Baamonde, Ana [1 ]
Menendez, Luis [1 ]
Gonzalez-Rodriguez, Sara [1 ]
Lastra, Ana [1 ]
Seitz, Viola [2 ,3 ]
Stein, Christoph [2 ]
Machelska, Halina [2 ]
机构
[1] Univ Oviedo, Lab Farmacol, Inst Invest Sanitaria Principado Asturias ISPA, Inst Univ Oncol Principado Asturias IUOPA,Fac Med, C Julian Claveria 6, Oviedo 33006, Asturias, Spain
[2] Charite Univ Med Berlin, Dept Expt Anesthesiol, Campus Benjamin Franklin, Hindenburgdamm 30, D-12203 Berlin, Germany
[3] Univ Potsdam, Inst Biochem & Biol, Karl Liebknecht Str 24-25, D-14474 Potsdam, Germany
关键词
INTRATIBIAL INOCULATION; SENSITIVE METHOD; MURINE MODEL; NCTC; 2472; HYPERALGESIA; FENTANYL; CELLS; ANTINOCICEPTION; LOPERAMIDE; MORPHINE;
D O I
10.1038/s41598-020-75509-4
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
The newly designed fentanyl derivative [(+/-)-N-(3-fluoro-1-phenethylpiperidine-4-yl)-N-phenyl propionamide] (NFEPP) was recently shown to produce analgesia selectively via peripheral mu-opioid receptors (MOR) at acidic pH in rat inflamed tissues. Here, we examined the pH-dependency of NFEPP binding to brain MOR and its effects on bone cancer-induced pain in mice. The IC50 of NFEPP to displace bound [H-3]-DAMGO was significantly higher compared to fentanyl at pH 7.4, but no differences were observed at pH 5.5 or 6.5. Intravenous NFEPP (30-100 nmol/kg) or fentanyl (17-30 nmol/kg) inhibited heat hyperalgesia in mice inoculated with B16-F10 melanoma cells. The peripherally-restricted opioid receptor antagonist naloxone-methiodide reversed the effect of NFEPP (100 nmol/kg), but not of fentanyl (30 nmol/kg). The antihyperalgesic effect of NFEPP was abolished by a selective MOR- (cyprodime), but not delta- (naltrindole) or kappa- (nor-binaltorphimine) receptor antagonists. Ten-fold higher doses of NFEPP than fentanyl induced maximal antinociception in mice without tumors, which was reversed by the non-restricted antagonist naloxone, but not by naloxone-methiodide. NFEPP also reduced heat hyperalgesia produced by fibrosarcoma- (NCTC 2472) or prostate cancer-derived (RM1) cells. These data demonstrate the increased affinity of NFEPP for murine MOR at low pH, and its ability to inhibit bone cancer-induced hyperalgesia through peripheral MOR. In mice, central opioid receptors may be activated by ten-fold higher doses of NFEPP.
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页数:10
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