Regiospecific, Controlled Synthesis of Structurally Defined Peptide Scaffolds
Lead Research Organisation:
Durham University
Department Name: Chemistry
Abstract
Noncovalent interactions between proteins are used in all living systems as an essential means of transferring and processing information and as such protein-protein interactions are fundamental to regulating life on a cellular level. Disruption of natural binding partners or alterations in the expression levels of a particular protein can perturb the balance of this signaling process and lead to the onset of a range of diseases. Altered protein-protein interactions are present in cancers, HIV, and Alzheimer's and inhibiting the abnormal protein-protein interactions associated with these diseases offers an exciting new avenue to develop highly selective drug molecules.
However, despite considerable research efforts, identifying inhibitors of disease-associated protein-protein interactions has proven to be very challenging. The large binding surfaces present in most protein-protein interactions has meant that effective inhibitors based on small molecules have been hard to identify, but larger compounds, such as cyclic peptides that can be used to mimic protein binding surfaces, have emerged as a promising therapeutics leads.
At the cutting edge of this field is the application of multicyclic peptide scaffolds, as the 3-dimensional structure of these compounds can be designed to allow multiple binding regions on a protein interface to be targeted simultaneously. But progress into designing new inhibitors of protein-protein interactions using this approach is severely hampered by a lack of viable synthetic routes to multicyclic peptide scaffolds.
Utilising novel fluoropyridine amino acids as the key building blocks we will develop synthetic strategies to access multicyclic peptide scaffolds, each with a defined 3-dimensional structure. The methodology developed will also permit the formation of the peptide scaffolds in a highly controlled and regionspecific manner which is something that is not currently possible using existing technologies. Having access to multicyclic peptide scaffolds will help to accelerate the discovery of inhibitors of protein-protein interactions and thus the development of new drug molecules to target diseases such as cancer.
However, despite considerable research efforts, identifying inhibitors of disease-associated protein-protein interactions has proven to be very challenging. The large binding surfaces present in most protein-protein interactions has meant that effective inhibitors based on small molecules have been hard to identify, but larger compounds, such as cyclic peptides that can be used to mimic protein binding surfaces, have emerged as a promising therapeutics leads.
At the cutting edge of this field is the application of multicyclic peptide scaffolds, as the 3-dimensional structure of these compounds can be designed to allow multiple binding regions on a protein interface to be targeted simultaneously. But progress into designing new inhibitors of protein-protein interactions using this approach is severely hampered by a lack of viable synthetic routes to multicyclic peptide scaffolds.
Utilising novel fluoropyridine amino acids as the key building blocks we will develop synthetic strategies to access multicyclic peptide scaffolds, each with a defined 3-dimensional structure. The methodology developed will also permit the formation of the peptide scaffolds in a highly controlled and regionspecific manner which is something that is not currently possible using existing technologies. Having access to multicyclic peptide scaffolds will help to accelerate the discovery of inhibitors of protein-protein interactions and thus the development of new drug molecules to target diseases such as cancer.
Planned Impact
Rising life expectancies have meant that many of us living in the UK will unfortunately suffer from some form of age-related illness. Two of the most common are cancer and Alzheimer's, and developing new drugs to treat these illness, would have a significant impact on the quality of life and health of the UK population. Finding new avenues to target disease is becoming increasingly difficult, but one promising area that is emerging as a new class of therapeutic targets are protein-protein interactions and this is the area in which the proposed work is focused.
We will develop new synthetic methodologies that will facilitate the synthesis of structurally defined multicyclic peptide scaffolds. These peptide scaffolds represent excellent templates for the rationale design of inhibitors of disease associated protein-protein interactions and they will be of considerable benefit to both industrial and academic researchers, who are searching for ways to design new therapies that target such interactions.
In addition to having an impact on the health and well-being of the UK population the proposed work will also generate new knowledge in the field of chemical-biology, which is an area of UK research strength and expertise as recognised by EPSRC. The creation of innovative technologies such as those proposed to access multicylic peptide scaffolds address a knowledge gap and this is critical in maintaining the UK at the forefront of research in the field of chemical-biology.
It is also recognised, that the pharmaceutical industry will benefit from the delivery of highly skilled researchers with expertise in peptide chemistry, as there is currently a skills shortage in this area within the UK. The project will also generate new technologies to prepare cyclic peptides. Such techniques can be exploited by industry to help them address a major stumbling block in the development of new peptide therapeutics, which is their susceptibility to in vivo degradation. Therefore, in the long term the proposed research could function as an enabling technology to help accelerate the development of peptide based drugs to market.
We will develop new synthetic methodologies that will facilitate the synthesis of structurally defined multicyclic peptide scaffolds. These peptide scaffolds represent excellent templates for the rationale design of inhibitors of disease associated protein-protein interactions and they will be of considerable benefit to both industrial and academic researchers, who are searching for ways to design new therapies that target such interactions.
In addition to having an impact on the health and well-being of the UK population the proposed work will also generate new knowledge in the field of chemical-biology, which is an area of UK research strength and expertise as recognised by EPSRC. The creation of innovative technologies such as those proposed to access multicylic peptide scaffolds address a knowledge gap and this is critical in maintaining the UK at the forefront of research in the field of chemical-biology.
It is also recognised, that the pharmaceutical industry will benefit from the delivery of highly skilled researchers with expertise in peptide chemistry, as there is currently a skills shortage in this area within the UK. The project will also generate new technologies to prepare cyclic peptides. Such techniques can be exploited by industry to help them address a major stumbling block in the development of new peptide therapeutics, which is their susceptibility to in vivo degradation. Therefore, in the long term the proposed research could function as an enabling technology to help accelerate the development of peptide based drugs to market.
Organisations
People |
ORCID iD |
| Steven Cobb (Principal Investigator) |
Publications
Gimenez D
(2017)
2,2,2-Trifluoroethanol as a solvent to control nucleophilic peptide arylation.
in Organic & biomolecular chemistry
Gimenez D
(2017)
The application of perfluoroheteroaromatic reagents in the preparation of modified peptide systems.
in Organic & biomolecular chemistry
Tatum N
(2015)
Synthesis, Ni(II) Schiff base complexation and structural analysis of fluorinated analogs of the ligand (S)-2-[N-(N'-benzylprolyl)amino]benzophenone (BPB)
in Journal of Fluorine Chemistry
Webster A
(2014)
A mild method for the synthesis of a novel dehydrobutyrine-containing amino acid
in Tetrahedron
| Description | The key aim of the project was to develop a technology platform that could be used to be prepare stable well defined peptide scaffolds that could be used in future drug development applications. We have been able to do this and we have also been able to use the methods developed to develop new bio-conjugation methods that can be used to link different classes of bio-molecules. For example, the method can be used to link peptides to sugars to make glyco-peptides. |
| Exploitation Route | Two patent applications based on this work were filed in 2014 and we have these have now seen these patents granted in the US and EU/ UK (granted in 2018). Follow on funding from the EPSRC IAA fund was awarded to continue this work. In Dec 2015 we were awarded funding via ICURe (HEFCE/ Innovate UK) to support additional work to build a business case for commercialization of the patented technology. in 2019 we set up the University spinout Pepmotec. We are now looking for investment to develop the company further. |
| Sectors | Healthcare,Pharmaceuticals and Medical Biotechnology |
| URL | https://www.dur.ac.uk/chemistry/staff/profile/?id=5553 |
| Description | We have used the primary data to support research publications and two UK patent applications (filed in 2014 and published in 2016). In Dec 2015 we were awarded funding via the ICURe program to look at developing a commercial pathway for the technology first developed on the EPSRC funded project. International Patents Europe and US were granted in 2018. We have set up a spin out company - Pepmotec in 2019 and are now looking for first stage investment. |
| First Year Of Impact | 2014 |
| Sector | Healthcare,Pharmaceuticals and Medical Biotechnology |
| Impact Types | Societal,Economic |
| Description | EPSRC IAA follow on funding |
| Amount | £67,000 (GBP) |
| Organisation | Durham University |
| Sector | Academic/University |
| Country | United Kingdom |
| Start | 06/2014 |
| End | 09/2015 |
| Description | ICURe (Innovation-to-Commercialisation of University Research programme) |
| Amount | £45,000 (GBP) |
| Organisation | Innovate UK |
| Sector | Public |
| Country | United Kingdom |
| Start | 12/2015 |
| End | 04/2016 |
| Title | CHEMICALLY MODIFYING PEPTIDES |
| Description | A method for chemically modifying a peptide, derivative or analogue thereof is described. The method comprises contacting a peptide, derivative or analogue thereof with a fluoro-heteroaromatic compound to activate the peptide, derivative or analogue thereof. The activated peptide, derivative or analogue thereof is then contacted with a nucleophile or base to create a chemically modified peptide, derivative or analogue thereof. |
| IP Reference | WO2015181544 |
| Protection | Patent application published |
| Year Protection Granted | 2015 |
| Licensed | No |
| Impact | We are looking to use the patent to underpin a Durham University spin-out company. |
| Title | CYCLISING PEPTIDES |
| Description | A method for preparing a cyclic peptide, derivative or analogue thereof is described. The method comprises contacting a peptide, derivative or analogue thereof with a fluoro-heteroaromatic compound to cyclise the peptide, derivative or analogue thereof. |
| IP Reference | WO2015181545 |
| Protection | Patent application published |
| Year Protection Granted | 2015 |
| Licensed | No |
| Impact | We will use patent to underpin a Durham spin-out company. |
| Company Name | PEPMOTEC LIMITED |
| Description | Set up as a University spin-out in 2019. Based on the peptide technology platforms developed as part of an EPSRC first grant led by Steven Cobb (grant PI). |
| Year Established | 2019 |
| Impact | The company has a strong IP position (two patents granted in the US and EU/ UK) and we are currently looking for initial investment to setup a research lab. |