Transformable Nanomaterials as an Artificial Extracellular Matrix for Inhibiting Tumor Invasion and Metastasis

Transformable Nanomaterials as an Artificial Extracellular Matrix for Inhibiting Tumor Invasion and Metastasis

Tumor metastasis is one of the big challenges in cancer treatment and is often associated with high patient mortality. Until now, there is an agreement that tumor invasion and metastasis are related to degradation of extracellular matrix (ECM) by enzymes. Inspired by the formation of natural ECM and...

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Bibliographic Details
Published in:ACS nano Vol. 11; no. 4; pp. 4086 - 4096
Main Authors: Hu, Xiao-Xue, He, Ping-Ping, Qi, Guo-Bin, Gao, Yu-Juan, Lin, Yao-Xin, Yang, Chao, Yang, Pei-Pei, Hao, Hongxun, Wang, Lei, Wang, Hao
Format: Journal Article
Language:English
Published: United States American Chemical Society 25-04-2017
Subjects:
Animals
Antineoplastic Agents - administration & dosage
Antineoplastic Agents - chemistry
Cell Line, Tumor
Cell Membrane - metabolism
Cell Survival - drug effects
Extracellular Matrix - chemistry
Humans
Laminin - chemistry
Lung Neoplasms - pathology
Lung Neoplasms - therapy
Mice
Molecular Mimicry
Nanofibers - chemistry
Nanoparticles - chemistry
Neoplasm Invasiveness
Neoplasm Metastasis
Particle Size
Peptides - administration & dosage
Peptides - chemistry
Permeability
Pyrenes - chemistry
self-assembly
peptide
metastasis
tumor
therapy
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Summary:Tumor metastasis is one of the big challenges in cancer treatment and is often associated with high patient mortality. Until now, there is an agreement that tumor invasion and metastasis are related to degradation of extracellular matrix (ECM) by enzymes. Inspired by the formation of natural ECM and the in situ self-assembly strategy developed in our group, herein, we in situ constructed an artificial extracellular matrix (AECM) based on transformable Laminin (LN)-mimic peptide 1 (BP-KLVFFK-GGDGR-YIGSR) for inhibition of tumor invasion and metastasis. The peptide 1 was composed of three modules including (i) the hydrophobic bis-pyrene (BP) unit for forming and tracing nanoparticles; (ii) the KLVFF peptide motif that was inclined to form and stabilize fibrous structures through intermolecular hydrogen bonds; and (iii) the Y-type RGD-YIGSR motif, derived from LN conserved sequence, served as ligands to bind cancer cell surfaces. The peptide 1 formed nanoparticles (1-NPs) by the rapid precipitation method, owing to strong hydrophobic interactions of BP. Upon intravenous injection, 1-NPs effectively accumulated in the tumor site due to the enhanced permeability and retention (EPR) effect and/or targeting capability of RGD-YIGSR. The accumulated 1-NPs simultaneously transformed into nanofibers (1-NFs) around the solid tumor and further entwined to form AECM upon binding to receptors on the tumor cell surfaces. The AECM stably existed in the primary tumor site over 72 h, which consequently resulted in efficiently inhibiting the lung metastasis in breast and melanoma tumor models. The inhibition rates in two tumor models were 82.3% and 50.0%, respectively. This in vivo self-assembly strategy could be widely utilized to design effective drug-free biomaterials for inhibiting the tumor invasion and metastasis.
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ISSN:1936-0851
1936-086X
DOI:10.1021/acsnano.7b00781