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Award details
Hybrid Nanopores for Single-Molecule Sensing
Reference
BB/M025373/1
Principal Investigator / Supervisor
Professor Hagan Bayley
Co-Investigators /
Co-Supervisors
Dr Stefan Howorka
Institution
University of Oxford
Department
Oxford Chemistry
Funding type
Research
Value (£)
726,202
Status
Completed
Type
Research Grant
Start date
01/10/2015
End date
30/09/2018
Duration
36 months
Abstract
Stochastic sensing with nanopores is a versatile single-molecule technology that can be used for the recognition and quantification of a wide range of analytes. Protein pores are advantageous in this respect, because they can be engineered with atomic precision and prepared in near homogeneous form. Until now, narrow protein pores have been used and therefore stochastic sensing has been confined to analytes of low mass or, in the case of nanopore DNA sequencing, to extended polymer chains. Here, we propose to make a new class of functional membrane-spanning nanopores, DNA-Protein hybrid nanopores, from DNA scaffolds to which peptide chains (either beta strands or alpha helices) are attached by bioorthogonal chemistry to form transmembrane barrel domains. This will be the first approach capable of producing pores of large internal diameter (5-30 nm) that are monodisperse and capable of precise site-specific modification: each pore will have an identical, predetermined number of subunits and no incomplete pores will be present. The DNA-protein hybrid nanopores will have several applications, for example to extend the scope of stochastic sensing to macromolecular analytes, e.g. for the recognition and quantification of large folded proteins, such as enzymes, receptors and antibodies. Our industrial partner is Oxford Nanopore Technologies, a company that exploits new developments in single-molecule sensing. Oxford Nanopore will evaluate and test our most promising DNA-Protein hybrid nanopores in their hand-held sensing devices, which are capable of monitoring the outputs of hundreds of pores in parallel.
Summary
Stochastic sensing with nanopores is a versatile technology that can be used for the recognition and quantification of a wide range of substances (known as analytes) through the detection of individual molecules. Our partner company, Oxford Nanopore Technologies, has been incorporating stochastic sensing into next-generation hand-held devices. The most highly developed application at Oxford Nanopore is cheap, extremely rapid DNA sequencing, which promises to revolutionise numerous areas of biology including aspects of medicine, ancestry and forensics. Currently, a portable sequencer is being tested at hundreds of sites worldwide. In stochastic sensing, analytes are detected as they enter and leave a single narrow pore perturbing a current that flows through it. The diameters of the pores, known as nanopores, are similar to those of a small molecule, about one-fifty thousandth of the diameter of a human hair, providing the basis for detection by current perturbation. Typically current changes of the order of one trillionth of an ampere are measured. Analytes have included drug molecules and small molecules found in the body that act as markers for disease. In the case of DNA sequencing, individual bases are detected as an extended DNA strand is threaded through a nanopore. Protein pores are advantageous for stochastic sensing, because they can be modified for particular applications with atomic precision and prepared in near homogeneous form. Until now, very narrow protein pores have been used and therefore stochastic sensing has been limited to analytes of small size or, in the case of DNA, to extended polymer chains. In the proposed work, we will endeavour to make a new class of functional nanopores, DNA-Protein hybrid nanopores. These pores will be constructed from folded DNA, known as DNA origami, and protein components. The DNA will act as a scaffold for the protein, ensuring that the new pores are up to fifteen times larger in internal diameter than the pores used before. Further, each pore will be of identical size and no incompletes pores will be present, a goal that has not be achieved previously. Finally, it will be possible to modify the new pores at precisely determined sites, which cannot be done with competing technologies, such as solid-state pores. The DNA-protein hybrid nanopores will enable a critical step forward for stochastic sensing by allowing the detection of a wide range of large biological molecules that can enter the pores, including proteins, DNAs and polymeric sugars. Conversely, it will also be possible to lodge these large molecules within the hybrid pores, where they will act as binding sites for a variety of additional analytes. In a futuristic application, it may prove possible to sequence double-stranded DNAs with hybrid pores, which will provide a significant advantage over the manipulations currently required for nanopore sequencing. Our industrial partner, Oxford Nanopore, will evaluate and test our most promising DNA-protein hybrid nanopores in their hand-held sensing devices, which are capable of monitoring the outputs of hundreds of pores in parallel, offering the prospect of step changes in sensing technology in areas including biological warfare defense, food authentication, plant and animal breeding and medical diagnostics.
Impact Summary
We envisage impact in five areas: (i) Academia; (ii) Training; (iii) the Research environment; (iv) the Economy; (v) Public engagement, and we summarize highlights here. From an academic viewpoint, the insight into a completely unexplored area of macromolecular engineering is of considerable interest to the wider community. From a practical viewpoint, the work will provide a new class of nanopores, which will allow large analytes, such as proteins, to be detected by stochastic sensing. This application will in turn require experimental exploration of fundamental issues, such as the behaviour of folded macromolecules in confinement. PDRAs taking part in the proposed work will be trained rigorously from a modern multidisciplinary perspective, at an internationally competitive level, in work requiring molecular engineering, cutting edge biophysics and high-level data analysis. They will be expected to plan and complete sub-projects, rather than merely participate in them. The researchers will also gain transferable skills through the demanding reporting and continuing education arrangements of the HB and SH groups, and courses provided by Oxford and UCL. The project will enhance the research environment at the group, local and collaborative level, as well as in a broader context. For example, we will welcome additional participants in the project area from the international research community. With this in mind, our results will be disseminated and discussed at meetings worldwide, and our materials and data will be freely available. The project is an Industrial Partnership Award in conjunction with Oxford Nanopore Technologies, a leader in single-molecule detection, which has committed £200,000 to the endeavour. The PDRAs will gain industrial experience through frequent visits to the company. Oxford Nanopore will explore applications of the best examples of our hybrid pores. They will be tested in their portable devices, which are capable of monitoring hundreds of pores in parallel. Therefore, there is a strong likelihood that our efforts will result in commercial products for personalised diagnosis, environmental protection, food testing or defense against bioterrorism. Both HB and SH enjoy and have significant experience in public engagement. They will continue to connect with the public through web sites, open days, visits to schools, and public lectures.
Committee
Research Committee D (Molecules, cells and industrial biotechnology)
Research Topics
Structural Biology, Synthetic Biology, Technology and Methods Development
Research Priority
X – Research Priority information not available
Research Initiative
X - not in an Initiative
Funding Scheme
Industrial Partnership Award (IPA)
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