Kinase-dependent control of DNA replication and repair as a drug target in Trypanosoma brucei

Lead Research Organisation: University of Glasgow
Department Name: School of Life Sciences

Abstract

The life of any living organism is dictated by the information contained in its genome, the genetic material that is contained within all cells and viruses. The propagation of an organism requires that the genome is copied, thereby generating offspring. This copying process is referred to as replication, and is a reaction that is carried out by specific proteins at a specific time during growth. The genome must also be protected from damage, which comes in many forms that can compromise the chemical composition of the genetic material. Protection is frequently due to reactions that repair damage that has already been inflicted, and these reactions are carried out, like replication, at specific times during growth. In fact, the two reactions can influence each other. The co-ordination of each reaction with growth is determined by a widely characterised set of enzymes, called protein kinases, which modify components of the cellular machineries that drive replication and repair. Trypanosomes are parasites that blight the health and economy of huge parts of the world and appear to have unconventional aspects of genome replication and repair. We wish to ask if we can identify the kinase enzymes that control these reactions, and thus understand if and how these reactions might be different from humans and other animals that are infected by the parasites. If we can identify these parasite protein kinases, we intend to try and find chemicals that will stop their activity and might then stop the growth of the parasites. If this is successful, we will have uncovered new strategies to treat the diseases caused by the parasites. These strategies will be robust because they target one of the most important aspects of the biology of any organism, and may be applicable to other parasites and infective organisms.

Technical Summary

DNA replication and repair are central processes in the transmission of all genomes. The activity of each process is regulated to occur at specific cell cycle stages, allowing the cell to monitor their success. In kinetoplastid organisms, including Trypanosoma species, no work to date has analysed the protein kinase-dependent checkpoints that link replication and repair to cell cycle progression. Unconventional aspects of cell division, the cell cycle, replication and repair have been detailed in kinetoplastid parasites, potentially making the protein kinases (PKs) that co-ordinate these central cell reactions viable drug targets. Identifying these PKs is a key step in understanding and validating this. To do this comprehensively, we propose to use a recently developed RNAi library that targets the complete repertoire of 183 PKs in T. brucei. PKs involved in DNA replication and repair will be identified by comparing, before and after RNAi induction, nucleotide incorporation rates, subcellular localisation of components of the replication machinery and the level of chromatin-association of replication components. PKs that act in repair will be identified by using cell imaging to evaluate when RNAi alters a conserved response to induced DNA breaks, the formation of subnuclear foci, and using next generation sequencing to identify those PKs whose RNAi targeting results in cell killing specifically in the presence of DNA damage. This work will reveal the network of PKs that regulate genome transmission in these diverged eukaryotes. To complement the above RNAi approach, and to move rapidly to the identification of compounds that target PKs that act in replication and repair, we will employ high-content cell imaging and assays developed above to screen available libraries of chemicals that have been designed to target PKs. Any compounds identified will be tested thoroughly for their mode and strength of anti-parasite activity and for the PKs that they target.

Planned Impact

The immediate beneficiaries (stakeholders) of this work will be academic researchers in the fields of parasitology, DNA replication and repair, and in cell cycle control. This will result from the fundamental findings that emerge from the screens that will be performed to identify protein kinases (PKs) that control DNA replication and repair in the parasite T. brucei, which will have relevance for such processes in other parasites, microbes and in all organisms. We anticipate, furthermore, that the novel approach we propose, linking medium-throughput genomic and compound screens with high content imaging, will be taken up by other researchers in the field, and that we will provide tools and expertise.

Integral to this approach is screens for compounds that inhibit T. brucei PKs, which may themselves be developed as anti-parasite therapies or provide the foundation for such therapies. This aspect of the project will have a wider impact, whose output will be realised at the end, and we will then consult on how this might be taken forward, either through the enrolment of a commercial pharmaceutical company, a not-for-profit organisation (e.g. the Drugs for Neglected Diseases Initiative) or a charity (e.g. the Wellcome Trust) as stakeholders in this development. This process could, then, contribute to local, national and international economies, as well as the health and wellbeing of the countries affected by these parasites.

The work on this project falls within the broad areas of genetics and microbial biology, which have a wide impact on the health of the population of the UK and beyond, and are frequently the subject of media discussion (e.g. through television programmes, such as Horizon or 'Monsters Inside Me', and in public science exhibits, such as at the Glasgow Science Centre). We will contribute to this discussion, throughout the course of the project, through public lectures and exhibits, school outreach programs and articles in local and national media.

Publications

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Briggs EM (2020) Next-Generation Analysis of Trypanosomatid Genome Stability and Instability. in Methods in molecular biology (Clifton, N.J.)

 
Description Identification of multiple protein kinases that act in the response to DNA damage and in genome replication in the parasite Trypanosoma brucei
Exploitation Route Knowledge applicable to other parasites, potential drug targets
Sectors Education

 
Description A distinct mode of DNA replication initiation in trypanosomes?
Amount £756,872 (GBP)
Funding ID BB/W001101/1 
Organisation Biotechnology and Biological Sciences Research Council (BBSRC) 
Sector Public
Country United Kingdom
Start 04/2022 
End 09/2025
 
Description BBSRC DTP
Amount £100,000 (GBP)
Organisation Biotechnology and Biological Sciences Research Council (BBSRC) 
Sector Public
Country United Kingdom
Start 10/2012 
End 10/2016
 
Description Challenging trypanosome antigenic variation paradigms using natural systems
Amount £2,070,288 (GBP)
Funding ID 206815/Z/17/Z 
Organisation Wellcome Trust 
Sector Charity/Non Profit
Country United Kingdom
Start 04/2018 
End 01/2024
 
Description ESPRC studentship
Amount £100,000 (GBP)
Organisation Engineering and Physical Sciences Research Council (EPSRC) 
Sector Public
Country United Kingdom
Start 10/2014 
End 10/2017
 
Description FAPESP-Glasgow University Sprint
Amount £20,000 (GBP)
Organisation São Paulo Research Foundation (FAPESP) 
Sector Public
Country Brazil
Start 05/2017 
End 05/2019
 
Description Glasgow MVLS college studentship
Amount £100,000 (GBP)
Organisation University of Glasgow 
Sector Academic/University
Country United Kingdom
Start 10/2017 
End 10/2021
 
Description MRC Precision Medicine PhD project
Amount £100,000 (GBP)
Organisation Medical Research Council (MRC) 
Sector Public
Country United Kingdom
Start 10/2018 
End 10/2022
 
Description Marie Cure Individual Fellowship
Amount € 189,454 (EUR)
Funding ID 750259 - RECREPEMLE 
Organisation European Union 
Sector Public
Country European Union (EU)
Start 05/2017 
End 05/2019
 
Description PhD studentship
Amount £10,000 (GBP)
Organisation Biotechnology and Biological Sciences Research Council (BBSRC) 
Sector Public
Country United Kingdom
Start 04/2015 
End 10/2018
 
Description PhD studentship, Ecuador
Amount $205,000 (USD)
Organisation SENECYST 
Sector Public
Country Ecuador
Start 09/2013 
End 09/2016
 
Description PhD studentship, Portugal
Amount € 100,000 (EUR)
Organisation Government of the Portugese Republic 
Department Foundation of Science and Technology (FCT)
Sector Public
Country Portugal
Start 04/2011 
End 04/2015
 
Description Precision Medicine PhD project
Amount £100,000 (GBP)
Organisation Medical Research Council (MRC) 
Sector Public
Country United Kingdom
Start 10/2020 
End 10/2023
 
Description Wellcome Investigator Award
Amount £1,655,328 (GBP)
Funding ID 224501/Z/21/Z 
Organisation Wellcome Trust 
Sector Charity/Non Profit
Country United Kingdom
Start 07/2022 
End 07/2027
 
Description Wellcome Trust Strategic Award
Amount £8,300,000 (GBP)
Funding ID 104111/Z/14/Z/A 
Organisation Wellcome Trust 
Sector Charity/Non Profit
Country United Kingdom
Start 10/2014 
End 01/2022
 
Title Genetic screen for repair factors, including kinases 
Description RNAi screen to provide information on T. brucei repair factors 
Type Of Material Technology assay or reagent 
Year Produced 2017 
Provided To Others? Yes  
Impact Information to guide research directions 
 
Title Mapping replication origins in two Leishmania species 
Description MFAseq of origins in L. major and L. mexicana 
Type Of Material Technology assay or reagent 
Year Produced 2015 
Provided To Others? Yes  
Impact publication; data available via tritrypdb 
URL http://tritrypdb.org
 
Title Replication origin and factor mapping in T. brucei genome 
Description ChIP and MFAseq next generation mapping pipelines to examine replication kinetoplastid genomes 
Type Of Material Technology assay or reagent 
Year Produced 2013 
Provided To Others? Yes  
Impact Public access via TriTryDB.org 
 
Title Replication timing mapping in T. brucei genome 
Description Mapping of replication within the telomeres of T. brucei 
Type Of Material Technology assay or reagent 
Year Produced 2016 
Provided To Others? Yes  
Impact Publication; data available via tritrypdb.org 
 
Title Origin and factor mapping in parasite genomes 
Description Localisation of regions of replication initiation, factor localisation and changes in gene expression after genetic perturbation in the genomes of Trypanosoma brucei and two Leishmania species. 
Type Of Material Database/Collection of data 
Year Produced 2013 
Provided To Others? Yes  
Impact Have provided the raw data to several labs worldwide 
URL http://tritrypdb.org/tritrypdb/
 
Title RNAi of repair factors in T. brucei 
Description Sequence data of effect of RNAi in the presence of DNA damage 
Type Of Material Database/Collection of data 
Year Produced 2017 
Provided To Others? Yes  
Impact Data to guide future research 
 
Title repklication timing in T. brucei genome 
Description MFAseq of T. brucei subtelomeres 
Type Of Material Database/Collection of data 
Year Produced 2016 
Provided To Others? Yes  
Impact publication, data available on tritrypdb 
 
Title replication origin mapping in Leishmania 
Description MFAseq of origins in L. major and L. mexicana 
Type Of Material Database/Collection of data 
Year Produced 2015 
Provided To Others? Yes  
Impact publication; data available via tritrypdb.org 
URL http://tritrypdb.org
 
Description Joint Wellcome Trust collaboratiev award 
Organisation University of Edinburgh
Country United Kingdom 
Sector Academic/University 
PI Contribution Writing and securing award; foundation data in support of the award
Collaborator Contribution Writing and securing award; foundation data in support of the award
Impact None to date
Start Year 2018
 
Description Joint Wellcome Trust collaboratiev award 
Organisation University of Liverpool
Country United Kingdom 
Sector Academic/University 
PI Contribution Writing and securing award; foundation data in support of the award
Collaborator Contribution Writing and securing award; foundation data in support of the award
Impact None to date
Start Year 2018
 
Description Visiting professor, Federal University Of Minas Gerais 
Organisation Federal University of Minas Gerais
Country Brazil 
Sector Academic/University 
PI Contribution Formal arrangement, funded by CAPES Print programme, for me to visit UFMG and teach and develop ongoing research collaborations; established after British Council-funded visit to UFMG in November 2018
Collaborator Contribution Colleagues in UFMG applied for an received Print funding for the collaboration
Impact Exchange of teaching expertise, improved research collaboration
Start Year 2020
 
Description Craft Critters 
Form Of Engagement Activity Participation in an activity, workshop or similar
Part Of Official Scheme? No
Geographic Reach National
Primary Audience Public/other audiences
Results and Impact A hands-on activity for all ages involving the construction of parasite toys, which are taken as gifts.
Year(s) Of Engagement Activity 2014,2015,2016
 
Description Glasgow Science Week 
Form Of Engagement Activity Participation in an open day or visit at my research institution
Part Of Official Scheme? No
Geographic Reach National
Primary Audience Schools
Results and Impact Hands on research experience for near school leavers thinking about attending university
Year(s) Of Engagement Activity 2018
 
Description Glasgow science festival 
Form Of Engagement Activity Participation in an activity, workshop or similar
Part Of Official Scheme? Yes
Geographic Reach Regional
Primary Audience Schools
Results and Impact Talk inspired discussions on microbiology and careers with pupils

None
Year(s) Of Engagement Activity 2014
 
Description Meeting between Glasgow University and Federal University of Minas Gerais 
Form Of Engagement Activity A formal working group, expert panel or dialogue
Part Of Official Scheme? No
Geographic Reach International
Primary Audience Policymakers/politicians
Results and Impact A week of discussion meetings to determine future directions of collaborations between the UK and Brazil institutions
Year(s) Of Engagement Activity 2017
 
Description Meeting between University fo Glasgow and Federal University of Minas Gerais 
Form Of Engagement Activity A formal working group, expert panel or dialogue
Part Of Official Scheme? No
Geographic Reach International
Primary Audience Postgraduate students
Results and Impact Meeting to consider presence of University of Glasgow in upcoming UFM Print award for staff mobility.
Year(s) Of Engagement Activity 2018
 
Description Pathogen investigation 
Form Of Engagement Activity A talk or presentation
Part Of Official Scheme? No
Geographic Reach Regional
Primary Audience Schools
Results and Impact A series of experiments for secondary school pupils who are pursuing their highers and considering whether or not to apply for university. The pupils were given a short talk on pathogen biology and then conducted a series of pre-arranged experiments to gain insight into how science is pursued.
Year(s) Of Engagement Activity 2013,2014,2015,2016,2017
 
Description School visit 
Form Of Engagement Activity A talk or presentation
Part Of Official Scheme? No
Geographic Reach Regional
Primary Audience Schools
Results and Impact Visit and presentation to local school
Year(s) Of Engagement Activity 2017
 
Description Secondary school visit 
Form Of Engagement Activity A talk or presentation
Part Of Official Scheme? No
Geographic Reach Regional
Primary Audience Schools
Results and Impact Secondary school pupils visited the host laboratory and were allowed to conduct controlled experiments and view ongoing experiments.
Year(s) Of Engagement Activity 2013,2014,2015,2016,2017
 
Description Visiting local school 
Form Of Engagement Activity A talk or presentation
Part Of Official Scheme? No
Geographic Reach Regional
Primary Audience Schools
Results and Impact Visit to local school to discuss microbiology
Year(s) Of Engagement Activity 2018
 
Description hosting visiting school 
Form Of Engagement Activity A talk or presentation
Part Of Official Scheme? No
Geographic Reach Regional
Primary Audience Schools
Results and Impact hosting local school, hands-on 'taster' activities in science
Year(s) Of Engagement Activity 2017
 
Description open day 
Form Of Engagement Activity Participation in an open day or visit at my research institution
Part Of Official Scheme? No
Geographic Reach National
Primary Audience Schools
Results and Impact Open day to provide information on degrees at Glasgow University
Year(s) Of Engagement Activity 2017