Dutta, Palash K. Zhang, Yun Blanchard, Aaron T. Ge, Chenghao Rushdi, Muaz Weiss, Kristin Zhu, Cheng Ke, Yonggang Salaita, Khalid Programmable Multivalent DNA-Origami Tension Probes for Reporting Cellular Traction Forces Mechanical forces are central to most, if not all, biological processes, including cell development, immune recognition, and metastasis. Because the cellular machinery mediating mechano-sensing and force generation is dependent on the nanoscale organization and geometry of protein assemblies, a current need in the field is the development of force-sensing probes that can be customized at the nanometer-length scale. In this work, we describe a DNA origami tension sensor that maps the piconewton (pN) forces generated by living cells. As a proof-of-concept, we engineered a novel library of six-helix-bundle DNA-origami tension probes (DOTPs) with a tailorable number of tension-reporting hairpins (each with their own tunable tension response threshold) and a tunable number of cell-receptor ligands. We used single-molecule force spectroscopy to determine the probes’ tension response thresholds and used computational modeling to show that hairpin unfolding is semi-cooperative and orientation-dependent. Finally, we use our DOTP library to map the forces applied by human blood platelets during initial adhesion and activation. We find that the total tension signal exhibited by platelets on DOTP-functionalized surfaces increases with the number of ligands per DOTP, likely due to increased total ligand density, and decreases exponentially with the DOTP’s force-response threshold. This work opens the door to applications for understanding and regulating biophysical processes involving cooperativity and multivalency. tailorable number;DNA origami tension sensor;Reporting Cellular Traction Forces Mechanical forces;protein assemblies;DOTP-functionalized surfaces increases;Programmable Multivalent DNA-Origami Tension Probes;DOTP library;single-molecule force spectroscopy;blood platelets;six-helix-bundle DNA-origami tension probes;tension signal;nanoscale organization;tension-reporting hairpins;nanometer-length scale;tunable tension response threshold;tunable number;novel library;force-sensing probes;force generation;cell-receptor ligands;ligand density;cell development 2018-06-18
    https://acs.figshare.com/articles/media/Programmable_Multivalent_DNA-Origami_Tension_Probes_for_Reporting_Cellular_Traction_Forces/6743441
10.1021/acs.nanolett.8b01374.s003