Unpicking the Roles of DNA Damage Protein Kinases in Trypanosomatids.

Front Cell Dev Biol

The Wellcome Centre for Integrative Parasitology, Institute of Infection, Immunity and Inflammation, University of Glasgow, Glasgow, United Kingdom.

Published: August 2021

AI Article Synopsis

  • Cells have a complex system known as the DNA damage response (DDR) that activates to fix DNA damage through various repair pathways, with protein kinases (PKs) playing a key role in this process.
  • Research on model eukaryotes has revealed how these PKs regulate DNA repair and their connections to other cellular activities like DNA replication and transcription.
  • Kinetoplastid parasites, such as some that cause neglected tropical diseases, show unique DNA repair mechanisms and have raised questions about the roles of certain kinases, presenting opportunities for new treatments using kinase inhibitors.

Article Abstract

To preserve genome integrity when faced with DNA lesions, cells activate and coordinate a multitude of DNA repair pathways to ensure timely error correction or tolerance, collectively called the DNA damage response (DDR). These interconnecting damage response pathways are molecular signal relays, with protein kinases (PKs) at the pinnacle. Focused efforts in model eukaryotes have revealed intricate aspects of DNA repair PK function, including how they direct DDR pathways and how repair reactions connect to wider cellular processes, including DNA replication and transcription. The Kinetoplastidae, including many parasites like spp. and spp. (causative agents of debilitating, neglected tropical infections), exhibit peculiarities in several core biological processes, including the predominance of multigenic transcription and the streamlining or repurposing of DNA repair pathways, such as the loss of non-homologous end joining and novel operation of nucleotide excision repair (NER). Very recent studies have implicated ATR and ATM kinases in the DDR of kinetoplastid parasites, whereas DNA-dependent protein kinase (DNA-PKcs) displays uncertain conservation, questioning what functions it fulfills. The wide range of genetic manipulation approaches in these organisms presents an opportunity to investigate DNA repair kinase roles in kinetoplastids and to ask if further kinases are involved. Furthermore, the availability of kinase inhibitory compounds, targeting numerous eukaryotic PKs, could allow us to test the suitability of DNA repair PKs as novel chemotherapeutic targets. Here, we will review recent advances in the study of trypanosomatid DNA repair kinases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8377203PMC
http://dx.doi.org/10.3389/fcell.2021.636615DOI Listing

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