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The Happy Hopping of Transposons: The Origins of V(D)J Recombination in Adaptive Immunity

Journal

FRONTIERS IN ECOLOGY AND EVOLUTION
Volume 10, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fevo.2022.836066

Keywords

transposable elements; V(D)J recombination; adaptive immunity; RAG recombinase; DNA transposons

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Nearly 50% of the human genome is derived from transposable elements, some of which can cause diseases when dysregulated, while others can generate new cellular functions. The adaptive immune system in jawed vertebrates is associated with Class II TEs, and the somatic rearrangement process in T and B cells is also influenced by TEs, laying the foundation for the generation of antibodies and receptors.
Nearly 50% of the human genome is derived from transposable elements (TEs). Though dysregulated transposons are deleterious to humans and can lead to diseases, co-opted transposons play an important role in generating alternative or new DNA sequence combinations to perform novel cellular functions. The appearance of an adaptive immune system in jawed vertebrates, wherein the somatic rearrangement of T and B cells generates a repertoire of antibodies and receptors, is underpinned by Class II TEs. This review follows the evolution of recombination activation genes (RAGs), components of adaptive immunity, from TEs, focusing on the structural and mechanistic similarities between RAG recombinases and DNA transposases. As evolution occurred from a transposon precursor, DNA transposases developed a more targeted and constrained mechanism of mobilization. As DNA repair is integral to transposition and recombination, we note key similarities and differences in the choice of DNA repair pathways following these processes. Understanding the regulation of V(D)J recombination from its evolutionary origins may help future research to specifically target RAG proteins to rectify diseases associated with immune dysregulation.

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