| Literature DB >> 34938910 |
Haicong Shen1, Rui Su2, Jiao Peng1, Lin Zhu1, Kunyue Deng1, Qi Niu3, Yanling Song1, Liu Yang1, Lingling Wu3, Zhi Zhu1, Chaoyong Yang1,3.
Abstract
Circulating tumor cells (CTCs), as important liquid biopsy target, can provide valuable information for cancer progress monitoring and individualized treatment. However, current isolation platforms incapable of balancing capture efficiency, specificity, cell viability, and gentle release have restricted the clinical applications of CTCs. Herein, inspired by the structure and functional merits of natural membrane interfaces, we established an antibody-engineered red blood cell (RBC-Ab) affinity interface on microfluidic chip for high-performance isolation and release of CTCs. The lateral fluidity, pliability, and anti-adhesion property of the RBC microfluidic interface enabled efficient CTCs capture (96.5%), high CTCs viability (96.1%), and high CTCs purity (average 4.2-log depletion of leukocytes). More importantly, selective lysis of RBCs by simply changing the salt concentration was utilized to destroy the affinity interface for efficient and gentle release of CTCs without nucleic acid contamination. Using this chip, CTCs were successfully detected in colon cancer samples with 90% sensitivity and 100% specificity (20 patients and 10 healthy individuals). After the release process, KRAS gene mutations of CTCs were identified from all the 5 cancer samples, which was consistent with the results of tissue biopsy. We expect this RBC interface strategy will inspire further biomimetic interface construction for rare cell analysis.Entities:
Keywords: Biomimetic interface; Circulating tumor cells; Colon cancer; Red blood cells
Year: 2021 PMID: 34938910 PMCID: PMC8661445 DOI: 10.1016/j.bioactmat.2021.09.034
Source DB: PubMed Journal: Bioact Mater ISSN: 2452-199X