Literature DB >> 17066446

Aclarubicin-loaded cationic albumin-conjugated pegylated nanoparticle for glioma chemotherapy in rats.

Wei Lu1, Jin Wan, Qing Zhang, Zhenjue She, Xinguo Jiang.   

Abstract

Traditional glioma chemotherapy with those second-line drugs such as anthracyclines usually failed because they are inaccessible to blood-brain barrier (BBB) in tumor. In our study, we incorporated aclarubicin (ACL) into cationic albumin-conjugated pegylated nanoparticle (CBSA-NP-ACL) to determine its therapeutic potential of rats with intracranially implanted C6 glioma cells. When labeled with fluorescent probe, 6-coumarin, CBSA-NP was shown to accumulate much more in tumor mass than nanoparticle without conjugated CBSA (NP) 1 hr post intravenous injection, as well as better retention after 24 hr. Tumor drug concentration of CBSA-NP-ACL displayed 2.6- and 3.3-fold higher than that of NP-ACL and ACL solution 1 hr post injection, while 2.7 and 6.6-fold higher after 24 hr, respectively. Moreover, using tumor microdialysis sampling, AUC(0-24 hr) of free drug amount in tumor interstitium delivered by CBSA-NP-ACL was about 2.0- and 2.7-fold higher than that of NP-ACL and ACL solutions, respectively. When the tumor rat model was subjected to 4 cycles of 2 mg/kg of ACL in different formulations, a significant increase of median survival time was found in the group of CBSA-NP-ACL compared with that of saline control animals, animals treated with NP-ACL and ACL solution. By terminal deoxynucleotidyl transferase-mediated dUTP nick-end-labeling, CBSA-NP-ACL can extensively make the tumor cell apoptosis. Histochemical evaluation by periodic acid Shiff staining and biochemical analysis depicted that the incorporation of ACL into CBSA-NP reduced its toxicity to liver, kidney and heart. Besides, CBSA-NP-ACL was not shown to open tight junction evaluated by BBB coculture. It was concluded that CBSA-NP-ACL could have a therapeutic potential for treatment of glioma. (c) 2006 Wiley-Liss, Inc.

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Year:  2007        PMID: 17066446     DOI: 10.1002/ijc.22296

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  15 in total

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3.  Liposome size and charge optimization for intraarterial delivery to gliomas.

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4.  Specific targeting of brain tumors with an optical/magnetic resonance imaging nanoprobe across the blood-brain barrier.

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Review 5.  Therapeutic nanomedicine for brain cancer.

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6.  Hydrogel matrix entrapping PLGA-paclitaxel microspheres: drug delivery with near zero-order release and implantability advantages for malignant brain tumour chemotherapy.

Authors:  Sudhir Hulikal Ranganath; Irene Kee; William B Krantz; Pierce Kah-Hoe Chow; Chi-Hwa Wang
Journal:  Pharm Res       Date:  2009-06-20       Impact factor: 4.200

7.  Irradiation induced fluorescence enhancement in PEGylated cyanine-based NIR nano- and mesoscale GUMBOS.

Authors:  Chengfei Lu; Susmita Das; Paul K S Magut; Min Li; Bilal El-Zahab; Isiah M Warner
Journal:  Langmuir       Date:  2012-09-25       Impact factor: 3.882

Review 8.  Nanoplatforms for constructing new approaches to cancer treatment, imaging, and drug delivery: what should be the policy?

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Journal:  Neuroimage       Date:  2010-02-10       Impact factor: 7.400

Review 9.  Peptide and protein nanoparticle conjugates: versatile platforms for biomedical applications.

Authors:  Christopher D Spicer; Coline Jumeaux; Bakul Gupta; Molly M Stevens
Journal:  Chem Soc Rev       Date:  2018-05-21       Impact factor: 54.564

Review 10.  Drug-loaded nanoparticle systems and adult stem cells: a potential marriage for the treatment of malignant glioma?

Authors:  Brenda Auffinger; Ramin Morshed; Alex Tobias; Yu Cheng; Atique U Ahmed; Maciej S Lesniak
Journal:  Oncotarget       Date:  2013-03
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