Volume 3, 2024

Therapeutic drug monitoring of immunotherapies with novel Affimer–NanoBiT sensor construct

Abstract

Concentration–therapeutic efficacy relationships have been observed for several therapeutic monoclonal antibodies (TmAb), where low circulating levels can result in ineffective treatment and high concentrations can cause adverse reactions. Rapid therapeutic drug monitoring (TDM) of TmAb drugs would provide the opportunity to adjust an individual patient's dosing regimen to improve treatment results. However, TDM for immunotherapies is currently limited to centralised testing methods with long sample-collection to result timeframes. Here, we show four point-of-care (PoC) TmAb biosensors by combining anti-idiotypic Affimer proteins and NanoBiT split luciferase technology at a molecular level to provide a platform for rapid quantification (<10 minutes) for four clinically relevant TmAb (rituximab, adalimumab, ipilimumab and trastuzumab). The rituximab sensor performed best with 4 pM limit of detection (LoD) and a quantifiable range between 8 pM–2 nM with neglectable matrix effects in serum up to 1%. After dilution of serum samples, the resulting quantifiable range for all four sensors falls within the clinically relevant range and compares favourably with the sensitivity and/or time-to-result of current ELISA standards. Further development of these sensors into a PoC test may improve treatment outcome and quality of life for patients receiving immunotherapy.

Graphical abstract: Therapeutic drug monitoring of immunotherapies with novel Affimer–NanoBiT sensor construct

Supplementary files

Article information

Article type
Paper
Submitted
30 May 2023
Accepted
23 Oct 2023
First published
01 Nov 2023
This article is Open Access
Creative Commons BY license

Sens. Diagn., 2024,3, 104-111

Therapeutic drug monitoring of immunotherapies with novel Affimer–NanoBiT sensor construct

E. Campbell, H. Adamson, T. Luxton, C. Tiede, C. Wälti, D. C. Tomlinson and L. J. C. Jeuken, Sens. Diagn., 2024, 3, 104 DOI: 10.1039/D3SD00126A

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