Detail information
| ID | ENOM00107 | ||||||||||||||||||||||||||||
| Accession | GSE6578 | ||||||||||||||||||||||||||||
| Status | Public on Mar 14, 2007 | ||||||||||||||||||||||||||||
| Title | Analgesia of naloxone in wild-type and NY1DD transgenic mouse model of sickle cell anemia using BMAP cDNA microarrays | ||||||||||||||||||||||||||||
| Organism | Mus musculus | ||||||||||||||||||||||||||||
| Experiment type | Expression profiling by array | ||||||||||||||||||||||||||||
| Summary |
Sickle cell disease is the most common genetic disorder in African-Americans. The opioid analgesic, morphine, has long been the treatment for the severe pain associated with this disease. Here we reveal that the opioid antagonist, naloxone, possesses potent analgesic activity in two strains of sickle cell mice (NY1DD and hBERK1) and not in their respective controls (ICR-CD1 and C57BL/6J) when administered by three parenteral routes. In the NY1DD sickle mice, naloxone (i.c.v.) possessed ~300-fold greater potency than morphine (i.c.v.). Other opioid antagonists (naltrexone, norbinaltorphimine, naltrindole) were substantially less effective in producing analgesia. Naloxone and morphine were synergistic in NY1DD mice, suggesting that analgesia was mediated via different receptor systems. Since microarray analysis suggested naloxone-induced down-regulation of the CCR5 chemokine receptor in NY1DD mice but not in control mice, the role of its endogenous ligand, CCL5 (RANTES), was investigated.
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| Platform | GPL4464: UMN Mouse 11K V 11_22_04 BMAP | ||||||||||||||||||||||||||||
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| Download | Download data in GEO database |