Nanonewton scale adhesion force measurements on biotinylated microbeads with a robotic micropipette

Rita Ungai-Salánki; Benjamin Csippa; Tamás Gerecsei; Beatrix Péter; Robert Horvath; Bálint Szabó

doi:10.1016/j.jcis.2021.05.180

Nanonewton scale adhesion force measurements on biotinylated microbeads with a robotic micropipette

J Colloid Interface Sci. 2021 Nov 15:602:291-299. doi: 10.1016/j.jcis.2021.05.180. Epub 2021 Jun 3.

Authors

Rita Ungai-Salánki¹, Benjamin Csippa², Tamás Gerecsei³, Beatrix Péter⁴, Robert Horvath⁴, Bálint Szabó⁵

Affiliations

¹ ELTE Eötvös Loránd University, Department of Biological Physics, Budapest, Hungary; CellSorter Company for Innovations, Erdőalja út 174, H-1037 Budapest, Hungary.
² Budapest University of Technology and Economics, Department of Hydrodynamic System, Budapest, Hungary.
³ ELTE Eötvös Loránd University, Department of Biological Physics, Budapest, Hungary; Nanobiosensorics Laboratory, ELKH, Institute for Technical Physics and Materials Science, Centre for Energy Research, Budapest, Hungary.
⁴ Nanobiosensorics Laboratory, ELKH, Institute for Technical Physics and Materials Science, Centre for Energy Research, Budapest, Hungary.
⁵ ELTE Eötvös Loránd University, Department of Biological Physics, Budapest, Hungary; CellSorter Company for Innovations, Erdőalja út 174, H-1037 Budapest, Hungary. Electronic address: balint.szabo@ttk.elte.hu.

PMID: 34130175
DOI: 10.1016/j.jcis.2021.05.180

Abstract

Binding force between biomolecules has a crucial role in most biological processes. Receptor-ligand interactions transmit physical forces and signals simultaneously. Previously, we employed a robotic micropipette both in live cell and microbead adhesion studies to explore the adhesion force of biomolecules such as cell surface receptors including specific integrins on immune cells. Here we apply standard computational fluid dynamics simulations to reveal the detailed physical background of the flow generated by the micropipette when probing microbead adhesion on functionalized surfaces. Measuring the aspiration pressure needed to pick up the biotinylated 10 μm beads on avidin coated surfaces and converting it to a hydrodynamic lifting force on the basis of simulations, we found an unbinding force of 12 ± 2 nN, when targeting the beads manually; robotic targeting resulted in 9 ± 4 nN (mean ± SD). We measured and simulated the effect of the targeting offset, when the microbead was out of the axis (off-axis)of the micropipette. According to the simulations, the higher offset resulted in a higher lifting force acting on the bead. Considering this effect, we could readily correct the impact of the targeting offset to renormalize the experimental data. Horizontal force and torque also appeared in simulations in case of a targeting offset. Surprisingly, simulations show that the lifting force acting on the bead reaches a maximum at a flow rate of ~ 5 μl/s if the targeting offset is not very high (<5 μm). Further increasing the flow rate decreases the lifting force. We attribute this effect to the spherical geometry of the bead. We predict that higher flow rates cannot increase the hydrodynamic lifting force acting on the precisely targeted microbead, setting a fundamental force limit (16 nN in our setup) for manipulating microbeads with a micropipette perpendicular to the supporting surface. In order to extend the force range, we propose the offset targeting of microbeads.

Keywords: Adhesion force; Binding force; Computational fluid dynamics; Microbead; Micropipette.

MeSH terms

Cell Adhesion
Hydrodynamics
Microspheres
Robotic Surgical Procedures*