Literature DB >> 28817122

Single-cell mechanogenetics using monovalent magnetoplasmonic nanoparticles.

Ji-Wook Kim1,2,3, Daeha Seo4,5, Jung-Uk Lee1,2,3, Kaden M Southard4,6, Yongjun Lim1,2,3, Daehyun Kim1,2,3, Zev J Gartner5,6, Young-Wook Jun1,2,4, Jinwoo Cheon1,2,3.   

Abstract

Spatiotemporal interrogation of signal transduction at the single-cell level is necessary to answer a host of important biological questions. This protocol describes a nanotechnology-based single-cell and single-molecule perturbation tool, termed mechanogenetics, that enables precise spatial and mechanical control over genetically encoded cell-surface receptors in live cells. The key components of this tool are a magnetoplasmonic nanoparticle (MPN) actuator that delivers defined spatial and mechanical cues to receptors through target-specific one-to-one engagement and a micromagnetic tweezers (μMT) that remotely controls the magnitude of force exerted on a single MPN. In our approach, a SNAP-tagged cell-surface receptor of interest is conjugated with a single-stranded DNA oligonucleotide, which hybridizes to its complementary oligonucleotide on the MPN. This protocol consists of four major stages: (i) chemical synthesis of MPNs, (ii) conjugation with DNA and purification of monovalent MPNs, (iii) modular targeting of MPNs to cell-surface receptors, and (iv) control of spatial and mechanical properties of targeted mechanosensitive receptors in live cells by adjusting the μMT-to-MPN distance. Using benzylguanine (BG)-functionalized MPNs and model cell lines expressing either SNAP-tagged Notch or vascular endothelial cadherin (VE-cadherin), we provide stepwise instructions for mechanogenetic control of receptor clustering and for mechanical receptor activation. The ability of this method to differentially control spatial and mechanical inputs to targeted receptors makes it particularly useful for interrogating the differential contributions of each individual cue to cell signaling. The entire procedure takes up to 1 week.

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Year:  2017        PMID: 28817122      PMCID: PMC5742362          DOI: 10.1038/nprot.2017.071

Source DB:  PubMed          Journal:  Nat Protoc        ISSN: 1750-2799            Impact factor:   13.491


  56 in total

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4.  Piezo1 and Piezo2 are essential components of distinct mechanically activated cation channels.

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Journal:  Nano Lett       Date:  2019-05-03       Impact factor: 11.189

Review 2.  Development of Integrated Systems for On-Site Infection Detection.

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Review 3.  Magnetic Nanotweezers for Interrogating Biological Processes in Space and Time.

Authors:  Ji-Wook Kim; Hee-Kyung Jeong; Kaden M Southard; Young-Wook Jun; Jinwoo Cheon
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4.  Fast detection of SARS-CoV-2 RNA via the integration of plasmonic thermocycling and fluorescence detection in a portable device.

Authors:  Jiyong Cheong; Hojeong Yu; Chang Yeol Lee; Jung-Uk Lee; Hyun-Jung Choi; Jae-Hyun Lee; Hakho Lee; Jinwoo Cheon
Journal:  Nat Biomed Eng       Date:  2020-12-03       Impact factor: 25.671

Review 5.  Biophysical Approaches for Applying and Measuring Biological Forces.

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6.  Valence-controlled protein conjugation on nanoparticles via re-arrangeable multivalent interactions of tandem repeat protein chains.

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7.  Introducing stimulogenetics, unraveling pertinent semantic ambiguity, and determining clinical relevance among novel neuromodulation strategies.

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  7 in total

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