Development of a Novel Co-Amorphous Curcumin and L-Arginine (1:2): Structural Characterization, Biological Activity and Pharmacokinetics

被引:0
|
作者
Mancillas-Quiroz, Jose Antonio [1 ]
Carrasco-Portugal, Miriam del Carmen [2 ]
Mondragon-Vasquez, Karina [3 ]
Huerta-Cruz, Juan Carlos [2 ]
Rodriguez-Silverio, Juan [1 ]
Rodriguez-Vera, Leyanis [4 ]
Reyes-Garcia, Juan Gerardo [1 ]
Flores-Murrieta, Francisco Javier [1 ,2 ]
Dominguez-Chavez, Jorge Guillermo [3 ]
Rocha-Gonzalez, Hector Isaac [1 ]
机构
[1] Inst Politecn Nacl, Escuela Super Med, Ciudad De Mexico 11340, Mexico
[2] Inst Nacl Enfermedades Resp, Ciudad De Mexico 14080, Mexico
[3] Univ Veracruzana, Fac Bioanal Veracruz, Veracruz 91700, Mexico
[4] CTI Clin Trial & Consulting Clin Res Ctr, Norwood, OH 45212 USA
关键词
bioavailability; co-amorphous; curcumin; cytokines; inflammation; L-arginine; nociception; pharmacokinetics; solubility; stability; BIOAVAILABILITY; PIPERINE; EFFICACY; SAFETY; PAIN;
D O I
10.3390/pharmaceutics17010011
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Background: Curcumin appears to be well tolerated and effective for managing chronic inflammatory pain, but its poor oral bioavailability has been a hurdle in its use as a therapeutic agent. The current study was performed to characterize a novel co-amorphous compound based on curcumin/L-arginine 1:2 (CAC12). Methods: Stability, solubility and structural characterization of the CAC12 were carried out by spectrometry techniques and in vitro assays, whereas the antinociceptive and anti-inflammatory effects were evaluated by CFA or carrageenan models. The mechanism of action was determined by cytokine quantification, and pharmacokinetic parameters were obtained through UPLC-MS/MS. The co-amorphous compound was prepared by fast solvent evaporation. Powder XRD, 13C-NMR, ATR-FTIR and TGA/DSC thermal analysis showed a 1:2 stoichiometry for the CAC12. Results: CAC12 was 1000 times more soluble than curcumin, and it was stable for 1 month at 40 degrees C and 75% relative humidity or for 60 min in physiological medium at pH 4.5-6.8. Co-amorphous curcumin/L-arginine, but not curcumin + L-arginine, decreased carrageenan- or CFA-induced inflammation and nociception by decreasing IL-1 alpha, IL-1 beta, IL-6, TNF-alpha, MCP-1 and CXCL1 cytokines. The bioavailability of free plasmatic curcumin increased about 22.4 times when it was given as CAC12 relative to a phytosome formulation at the equivalent dose. Conclusions: Results suggest the possible use of CAC12 to treat inflammatory pain disorders in human beings.
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页数:24
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