Literature DB >> 19966540

Pulmonary targeting microparticulate camptothecin delivery system: anticancer evaluation in a rat orthotopic lung cancer model.

Piyun Chao1, Manjeet Deshmukh, Hilliard L Kutscher, Dayuan Gao, Sujata Sundara Rajan, Peidi Hu, Debra L Laskin, Stanley Stein, Patrick J Sinko.   

Abstract

Large (>6 microm) rigid microparticles (MPs) become passively entrapped within the lungs after intravenous (i.v.) injection making them an attractive and highly efficient alternative to inhalation for pulmonary delivery. In this study, PEGylated 6 microm polystyrene MPs with multiple copies of the norvaline (Nva) alpha-amino acid prodrug of camptothecin (CPT) were prepared. Surface morphology was characterized using a scanning electron microscope. CPT was released from the CPT-Nva-MPs over 24 h in rat plasma at 37 degrees C. In-vivo CPT plasma concentrations were low (approximately 1 ng/ml or less) and constant over a period of 4 days after a single i.v. injection of CPT-Nva-MPs as compared with high but short-lived systemic exposures after an i.v. injection of free CPT. This suggests that sustained local CPT concentrations were achieved in the lung after administration of the MP delivery system. Anticancer efficacy was evaluated in an orthotopic lung cancer animal model and compared with a bolus injection of CPT. Animals receiving free CPT (2 mg/kg) and CPT-Nva-MPs (0.22 mg/kg CPT and 100 mg/kg MPs) were found to have statistically significant smaller areas of lung cancer (P<0.05 and 0.01, respectively) than untreated animals. In addition, 40% of the animals receiving CPT-Nva-MPs were found to be free of cancer. The CPT dose using targeted MPs was 10 times lower than after i.v. injection of free CPT, but was more effective in reducing the amount of cancerous areas. In conclusion, CPT-Nva-MPs were able to achieve effective local lung and low systemic CPT concentrations at a dose that was 10 times lower than systemically administered CPT resulting in a significant improvement in anticancer efficacy in an orthotopic rat model of lung cancer.

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Year:  2010        PMID: 19966540      PMCID: PMC3859198          DOI: 10.1097/CAD.0b013e328332a322

Source DB:  PubMed          Journal:  Anticancer Drugs        ISSN: 0959-4973            Impact factor:   2.248


  51 in total

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4.  Capillary recruitment and transit time in the rat lung.

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5.  Validation of an orthotopic model of human lung cancer with regional and systemic metastases.

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Review 7.  Quantitation of camptothecin and related compounds.

Authors:  M Palumbo; C Sissi; B Gatto; S Moro; G Zagotto
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Authors:  Gergely Szakács; Jill K Paterson; Joseph A Ludwig; Catherine Booth-Genthe; Michael M Gottesman
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2.  Novel monodisperse PEGtide dendrons: design, fabrication, and evaluation of mannose receptor-mediated macrophage targeting.

Authors:  Jieming Gao; Peiming Chen; Yashveer Singh; Xiaoping Zhang; Zoltan Szekely; Stanley Stein; Patrick J Sinko
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Review 3.  Recent trends on hydrogel based drug delivery systems for infectious diseases.

Authors:  Arti Vashist; Ajeet Kaushik; Atul Vashist; Rahul Dev Jayant; Asahi Tomitaka; Sharif Ahmad; Y K Gupta; Madhavan Nair
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Review 4.  Bioavailability enhancers of herbal origin: an overview.

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6.  Gelation chemistries for the encapsulation of nanoparticles in composite gel microparticles for lung imaging and drug delivery.

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7.  Nano-Engineered Mesenchymal Stem Cells Increase Therapeutic Efficacy of Anticancer Drug Through True Active Tumor Targeting.

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Review 8.  Polymeric nanoparticles in development for treatment of pulmonary infectious diseases.

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9.  Toxicodynamics of rigid polystyrene microparticles on pulmonary gas exchange in mice: implications for microemboli-based drug delivery systems.

Authors:  H L Kutscher; D Gao; S Li; C B Massa; J Cervelli; M Deshmukh; L B Joseph; D L Laskin; P J Sinko
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10.  Biodistribution and renal clearance of biocompatible lung targeted poly(ethylene glycol) (PEG) nanogel aggregates.

Authors:  Manjeet Deshmukh; Hilliard L Kutscher; Dayuan Gao; Vasanthi R Sunil; Rama Malaviya; Kinal Vayas; Stanley Stein; Jeffrey D Laskin; Debra L Laskin; Patrick J Sinko
Journal:  J Control Release       Date:  2012-10-03       Impact factor: 9.776

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