posted on 2022-12-20, 23:51authored bySC-H Tsao, R Vaidyanathan, S Dey, LG Carrascosa, C Christophi, Jonathan Cebon, MJA Shiddiky, Andreas BehrenAndreas Behren, M Trau
With new systemic therapies becoming available for metastatic melanoma such as BRAF and PD-1 inhibitors, there is an increasing demand for methods to assist with treatment selection and response monitoring. Quantification and characterisation of circulating melanoma cells (CMCs) has been regarded as an excellent non-invasive candidate but a sensitive and efficient tool to do these is lacking. Herein we demonstrate a microfluidic approach for melanoma cell capture and subsequent on-chip evaluation of BRAF mutation status. Our approach utilizes a recently discovered alternating current electrohydrodynamic (AC-EHD)-induced surface shear forces, referred to as nanoshearing. A key feature of nanoshearing is the ability to agitate fluid to encourage contact with surface-bound antibody for the cell capture whilst removing nonspecific cells from the surface. By adjusting the AC-EHD force to match the binding affinity of antibodies against the melanoma-associated chondroitin sulphate proteoglycan (MCSP), a commonly expressed melanoma antigen, this platform achieved an average recovery of 84.7% from biological samples. Subsequent staining with anti-BRAF V600E specific antibody enabled on-chip evaluation of BRAFV600E mutation status in melanoma cells. We believe that the ability of nanoshearing-based capture to enumerate melanoma cells and subsequent on-chip characterisation has the potential as a rapid screening tool while making treatment decisions.
Funding
This work was supported by the NHMRC CDF (APP1088966) and ARC DECRA (DE120102503). Although not directly involved in this work, our lab is receiving support from the National Breast Cancer Foundation of Australia (CG-12-07). This grant has significantly contributed to the environment to stimulate the research described here. We would also like to acknowledge the Victorian State Government Operational Infrastructure Support Program for partial funding of the parts of the project based at the Olivia Newton-John Cancer Research Institute. S.C.T is funded by the Australia Postgraduate Award and the Australasian College of Surgeons Foundation for Surgery ANZ journal of Surgery research scholarship.
History
Publication Date
2016-01-27
Journal
Scientific Reports
Volume
6
Issue
1
Article Number
19709
Pagination
10p.
Publisher
Nature Publishing Group
ISSN
2045-2322
Rights Statement
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