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转铁蛋白修饰的石墨烯氧化物用于脑胶质瘤靶向药物传递:体外和体内评价。

Transferrin modified graphene oxide for glioma-targeted drug delivery: in vitro and in vivo evaluations.

机构信息

Neurosurgery Department, The Second Affiliated Hospital of Soochow University, 1055 Sanxiang Road, Suzhou, 215004, China.

出版信息

ACS Appl Mater Interfaces. 2013 Aug 14;5(15):6909-14. doi: 10.1021/am402128s. Epub 2013 Jul 24.


DOI:10.1021/am402128s
PMID:23883622
Abstract

Transferrin (Tf), an iron-transporting serum glycoprotein that binds to receptors overexpressed at the surface of glioma cells, was chosen as the ligand to develop Tf-conjugated PEGylated nanoscaled graphene oxide (GO) for loading and glioma targeting delivery of anticancer drug doxorubicin (Dox) (Tf-PEG-GO-Dox). Tf-GO with lateral dimensions of 100-400 nm exhibited a Dox loading ratio up to 115.4%. Compared with Dox-loaded PEGylated GO (PEG-GO-Dox) and free Dox, Tf-PEG-GO-Dox displayed greater intracellular delivery efficiency and stronger cytotoxicity against C6 glioma cells. A competition test showed that Tf was essential to glioma targeting in vitro. The HPLC assay for Dox concentration in tumor tissue and contrapart tissue of the brain demonstrated that Tf-PEG-GO-Dox could deliver more Dox into tumor in vivo. The life span of tumor bearing rats after the administration of Tf-PEG-GO-Dox was extended significantly compared to the rats treated with saline, Dox, and PEG-GO-Dox. In conclusion, we developed Tf-PEG-GO-Dox which exhibited significantly improved therapeutic efficacy for glioma both in vitro and in vivo.

摘要

转铁蛋白(Tf)是一种铁转运的血清糖蛋白,它与过度表达于神经胶质瘤细胞表面的受体结合,被选择作为配体来开发转铁蛋白-聚乙二醇化纳米氧化石墨烯(GO),用于装载和靶向神经胶质瘤的抗癌药物阿霉素(Dox)的递送(Tf-PEG-GO-Dox)。横向尺寸为 100-400nm 的 Tf-GO 具有高达 115.4%的 Dox 载药率。与载药的聚乙二醇化 GO(PEG-GO-Dox)和游离 Dox 相比,Tf-PEG-GO-Dox 显示出更高的细胞内递送效率和更强的对 C6 神经胶质瘤细胞的细胞毒性。竞争试验表明,Tf 是体外靶向神经胶质瘤所必需的。用于检测肿瘤组织和脑组织中 Dox 浓度的 HPLC 分析表明,Tf-PEG-GO-Dox 可以在体内将更多的 Dox 递送到肿瘤中。与给予生理盐水、Dox 和 PEG-GO-Dox 的大鼠相比,给予 Tf-PEG-GO-Dox 的荷瘤大鼠的寿命明显延长。总之,我们开发了 Tf-PEG-GO-Dox,它在体外和体内均显著提高了神经胶质瘤的治疗效果。

相似文献

[1]
Transferrin modified graphene oxide for glioma-targeted drug delivery: in vitro and in vivo evaluations.

ACS Appl Mater Interfaces. 2013-7-24

[2]
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Bioconjug Chem. 2011-5-11

[3]
Targeted delivery of doxorubicin using stealth liposomes modified with transferrin.

Int J Pharm. 2009-5-21

[4]
Transferrin-modified Doxorubicin-loaded biodegradable nanoparticles exhibit enhanced efficacy in treating brain glioma-bearing rats.

Cancer Biother Radiopharm. 2013-6-20

[5]
The targeted delivery of anticancer drugs to brain glioma by PEGylated oxidized multi-walled carbon nanotubes modified with angiopep-2.

Biomaterials. 2012-1-26

[6]
A dual-targeting nanocarrier based on poly(amidoamine) dendrimers conjugated with transferrin and tamoxifen for treating brain gliomas.

Biomaterials. 2012-2-23

[7]
PEGylated Poly(amidoamine) dendrimer-based dual-targeting carrier for treating brain tumors.

Biomaterials. 2010-10-8

[8]
Peptide-conjugated PAMAM for targeted doxorubicin delivery to transferrin receptor overexpressed tumors.

Mol Pharm. 2010-10-14

[9]
Lactoferrin modified doxorubicin-loaded procationic liposomes for the treatment of gliomas.

Eur J Pharm Sci. 2011-7-18

[10]
RGD-modified PEG-PAMAM-DOX conjugates: in vitro and in vivo studies for glioma.

Eur J Pharm Biopharm. 2011-4-8

引用本文的文献

[1]
Combined Strategies for Nanodrugs Noninvasively Overcoming the Blood-Brain Barrier and Actively Targeting Glioma Lesions.

Biomater Res. 2025-2-5

[2]
Targeting the undruggable in glioblastoma using nano-based intracellular drug delivery.

Med Oncol. 2024-10-29

[3]
Pathophysiological aspects of transferrin-A potential nano-based drug delivery signaling molecule in therapeutic target for varied diseases.

Front Pharmacol. 2024-3-4

[4]
Biomedical application of 2D nanomaterials in neuroscience.

J Nanobiotechnology. 2023-6-7

[5]
A receptor-mediated landscape of druggable and targeted nanomaterials for gliomas.

Mater Today Bio. 2023-5-19

[6]
The blood-brain barrier: structure, regulation, and drug delivery.

Signal Transduct Target Ther. 2023-5-25

[7]
Potential Role of Carbon Nanomaterials in the Treatment of Malignant Brain Gliomas.

Cancers (Basel). 2023-4-30

[8]
Graphene Oxide Nanoscale Platform Enhances the Anti-Cancer Properties of Bortezomib in Glioblastoma Models.

Adv Healthc Mater. 2023-1

[9]
Combinatorial delivery of CPI444 and vatalanib loaded on PEGylated graphene oxide as an effective nanoformulation to target glioblastoma multiforme: evaluation.

Front Oncol. 2022-8-16

[10]
Is Graphene Shortening the Path toward Spinal Cord Regeneration?

ACS Nano. 2022-9-27

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