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(Referência obtida automaticamente do Web of Science, por meio da informação sobre o financiamento pela FAPESP e o número do processo correspondente, incluída na publicação pelos autores.)

Improvement of paclitaxel therapeutic index by derivatization and association to a cholesterol-rich microemulsion: in vitro and in vivo studies

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Autor(es):
Rodrigues, Debora G. ; Maria, Durvanei A. ; Fernandes, Denise C. ; Valduga, Claudete ; Couto, Ricardo D. ; Ibañez, Olga Célia Martinez ; Maranhão, Raul C. [7]
Número total de Autores: 7
Tipo de documento: Artigo Científico
Fonte: Cancer Chemotherapy and Pharmacology; v. 55, n. 6, p. 565-576, Jun. 2005.
Área do conhecimento: Ciências da Saúde - Medicina
Assunto(s):Oncologia   Neoplasias   Colesterol   Emulsões gordurosas intravenosas
Resumo

A cholesterol-rich microemulsion or nanoparticle termed LDE concentrates in cancer tissues after injection into the bloodstream. Here the cytotoxicity, pharmacokinetics, toxicity to animals and therapeutic action of a paclitaxel lipophilic derivative associated to LDE is compared with those of the commercial paclitaxel. Results show that LDE-paclitaxel oleate is stable. The cytostatic activity of the drug in the complex is diminished compared with the commercial paclitaxel due to the cytotoxicity of the vehicle Cremophor EL used in the commercial formulation. Competition experiments in neoplastic cultured cells show that paclitaxel oleate and LDE are internalized together by the LDL receptor pathway. LDE-paclitaxel oleate arrests the G2/M phase of cell cycle, similarly to commercial paclitaxel. Tolerability to mice is remarkable, such that the lethal dose (LD50) was ninefold greater than that of the commercial formulation (LD50 = 326 M and 37 M, respectively). LDE concentrates paclitaxel oleate in the tumor roughly fourfold relative to the normal adjacent tissues. At equimolar doses, the association of paclitaxel oleate with LDE results in remarkable changes in the drug pharmacokinetic parameters when compared to commercial paclitaxel (t1/2=218 min and 184 min, AUC=1,334 g h/ml and 707 g h/ml and CL=0.125 ml/min and 0.236 ml/min, respectively). Finally, the therapeutic efficacy of the complex is pronouncedly greater than that of the commercial paclitaxel, as indicated by the reduction in tumor growth, increase in survival rates and % cure of treated mice. In conclusion, LDE-paclitaxel oleate is a stable complex and compared with paclitaxel toxicity is considerably reduced and activity is enhanced, which may lead to improved therapeutic index in clinical use. (AU)

Processo FAPESP: 99/01229-2 - Lipoproteínas artificiais na investigação das dislipidemias e no tratamento do câncer
Beneficiário:Raul Cavalcante Maranhao
Modalidade de apoio: Auxílio à Pesquisa - Temático