Nanoparticulate Cationic Poly(amino acid)s Block Cancer Metastases by Destructing Neutrophil Extracellular Traps.
Huiyi LiangYibo DuChenxu ZhuZhaoqiang ZhangGuiqing LiaoLixin LiuYongming ChenPublished in: ACS nano (2023)
Cancer metastasis that is resistant to conventional therapies has become a major cause of patient death. Recent reports indicate that the neutrophil extracellular trap (NET) is closely associated with cancer distant metastases, and the cell-free DNA of NETs has been identified as the ligand of the transmembrane protein CCDC25 of cancer cells, acting as a chemokine to induce cancer cell migration to distant organs. In this work, we present the poly(aspartic acid) based-cationic materials to interfere with the interaction between NET-DNA and CCDC25, and furthermore to inhibit NET-DNA-mediated cancer cell chemotaxis and migration. Because of a stronger binding affinity to DNA and favorable retention in the liver, nanoparticulate poly(aspartic acid) derivatives (cANP) efficiently reduce the level of hepatic NET-DNA infiltration, leading to a significant suppression of cancer metastases in mice and several human metastatic models. Moreover, the cANP exhibits no toxicity to organs of animals during the entire treatment. Thus, this work suggests a strategy for controlling cancer metastases, which will benefit patients in clinics.
Keyphrases
- papillary thyroid
- squamous cell
- primary care
- circulating tumor
- lymph node
- squamous cell carcinoma
- endothelial cells
- cell migration
- cell free
- young adults
- emergency department
- skeletal muscle
- newly diagnosed
- metabolic syndrome
- single molecule
- prognostic factors
- ejection fraction
- adipose tissue
- childhood cancer
- binding protein
- smoking cessation
- nucleic acid
- circulating tumor cells