Evolutionary Comparative Analyses of DNA-Editing Enzymes of the Immune System: From 5-Dimensional Description of Protein Structures to Immunological Insights and Applications to Protein Engineering

Ghorbani, Atefeh; Quinlan, Emma M; Larijani, Mani

doi:10.3389/fimmu.2021.642343

Cited by 8 publications

(8 citation statements)

References 216 publications

(260 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…To recognize conformational antigens, higher chordates have another mechanism of specificity enhancement called affinity maturation of BCRs after a low-specific interaction with the antigen ( Figure 2 ) [ 45 , 46 ]. Presently, this process or its analogs are not revealed in jawless vertebrates [ 29 , 47 , 48 , 49 , 50 ]. The emergence of the antigen-presenting system in higher chordates also solved the issue of the recognition of self/altered-self due to the mechanism of presentation of self-antigens in all the cells of an organism.…”

Section: Evolutionary Prerequisitesmentioning

confidence: 99%

Phylogeny, Structure, Functions, and Role of AIRE in the Formation of T-Cell Subsets

Shevyrev

Tereshchenko

Козлов

et al. 2022

Cells

View full text Add to dashboard Cite

It is well known that the most important feature of adaptive immunity is the specificity that provides highly precise recognition of the self, altered-self, and non-self. Due to the high specificity of antigen recognition, the adaptive immune system participates in the maintenance of genetic homeostasis, supports multicellularity, and protects an organism from different pathogens at a qualitatively different level than innate immunity. This seemingly simple property is based on millions of years of evolution that led to the formation of diversification mechanisms of antigen-recognizing receptors and later to the emergence of a system of presentation of the self and non-self antigens. The latter could have a crucial significance because the presentation of nearly complete diversity of auto-antigens in the thymus allows for the “calibration” of the forming repertoires of T-cells for the recognition of self, altered-self, and non-self antigens that are presented on the periphery. The central role in this process belongs to promiscuous gene expression by the thymic epithelial cells that express nearly the whole spectrum of proteins encoded in the genome, meanwhile maintaining their cellular identity. This complex mechanism requires strict control that is executed by several transcription factors. One of the most important of them is AIRE. This noncanonical transcription factor not only regulates the processes of differentiation and expression of peripheral tissue-specific antigens in the thymic medullar epithelial cells but also controls intercellular interactions in the thymus. Besides, it participates in an increase in the diversity and transfer of presented antigens and thus influences the formation of repertoires of maturing thymocytes. Due to these complex effects, AIRE is also called a transcriptional regulator. In this review, we briefly described the history of AIRE discovery, its structure, functions, and role in the formation of antigen-recognizing receptor repertoires, along with other transcription factors. We focused on the phylogenetic prerequisites for the development of modern adaptive immunity and emphasized the importance of the antigen presentation system.

show abstract

Section: Evolutionary Prerequisitesmentioning

confidence: 99%

Phylogeny, Structure, Functions, and Role of AIRE in the Formation of T-Cell Subsets

Shevyrev

Tereshchenko

Козлов

et al. 2022

Cells

View full text Add to dashboard Cite

show abstract

“…These data were obtained with bacterially expressed and purified GST-AID. Since this system has been used to demonstrate catalytic activity of many bony fish AID orthologs [71][72][73]80], it is unlikely but formally possible that the extreme enzymatic lethargy of Gm-AID is due to mis-folding when expressed in bacteria. To examine this possibility, we expressed Gm-AID in a different expression system (293 T cells), along with Dr-AID as a positive control.…”

Section: Deamination Catalysis By the Atlantic Cod Aid Is Several Ord...mentioning

confidence: 99%

Ancestral reconstruction reveals catalytic inactivation of activation-induced cytidine deaminase concomitant with cold water adaption in the Gadiformes bony fish

et al. 2022

Self Cite

View full text Add to dashboard Cite

Background Antibody affinity maturation in vertebrates requires the enzyme activation-induced cytidine deaminase (AID) which initiates secondary antibody diversification by mutating the immunoglobulin loci. AID-driven antibody diversification is conserved across jawed vertebrates since bony and cartilaginous fish. Two exceptions have recently been reported, the Pipefish and Anglerfish, in which the AID-encoding aicda gene has been lost. Both cases are associated with unusual reproductive behavior, including male pregnancy and sexual parasitism. Several cold water fish in the Atlantic cod (Gadinae) family carry an aicda gene that encodes for a full-length enzyme but lack affinity-matured antibodies and rely on antibodies of broad antigenic specificity. Hence, we examined the functionality of their AID. Results By combining genomics, transcriptomics, immune responsiveness, and functional enzymology of AID from 36 extant species, we demonstrate that AID of that Atlantic cod and related fish have extremely lethargic or no catalytic activity. Through ancestral reconstruction and functional enzymology of 71 AID enzymes, we show that this enzymatic inactivation likely took place relatively recently at the emergence of the true cod family (Gadidae) from their ancestral Gadiformes order. We show that this AID inactivation is not only concordant with the previously shown loss of key adaptive immune genes and expansion of innate and cell-based immune genes in the Gadiformes but is further reflected in the genomes of these fish in the form of loss of AID-favored sequence motifs in their immunoglobulin variable region genes. Conclusions Recent demonstrations of the loss of the aicda gene in two fish species challenge the paradigm that AID-driven secondary antibody diversification is absolutely conserved in jawed vertebrates. These species have unusual reproductive behaviors forming an evolutionary pressure for a certain loss of immunity to avoid tissue rejection. We report here an instance of catalytic inactivation and functional loss of AID rather than gene loss in a conventionally reproducing vertebrate. Our data suggest that an expanded innate immunity, in addition to lower pathogenic pressures in a cold environment relieved the pressure to maintain robust secondary antibody diversification. We suggest that in this unique scenario, the AID-mediated collateral genome-wide damage would form an evolutionary pressure to lose AID function.

show abstract

“…Cas9 engagement impacts DNA deaminase strand capture. There are multiple hypotheses addressing how AID targets both Ig strands in B-cells, 19 including antisense transcription, DNA topology, and R-loop collapse by endogenous RNAse H digestion, all of which would expose both strands as ssDNA. However, how Cas9 binding could create the right environment for AID to access either the NTS or TS has not yet been studied.…”

Section: Modulating Intrinsic Aid Activity Tunes Be Activitymentioning

confidence: 99%

“…AID naturally functions to drive somatic hypermutation (SHM) in B-cells where it generates clustered mutations on the immunoglobulin (Ig) locus by acting on either strand in a processive fashion (18, 19). In addition to being processive, AID activity can be tuned as its deamination activity has been highly constrained (20), as evidenced by the isolation of various hyperactivating mutations that shift the balance towards increased genomic instability in B-cells (21, 22). Similar to the opportunity offered by systematically altering AID, perturbing Cas9 cleavage activity can offer a means to alter downstream replication and repair, and analyzing BE off-targets can provide a means to assess the impact of Cas9 engagement.…”

Section: Introductionmentioning

confidence: 99%

Cooperativity between Cas9 and hyperactive AID establishes broad and diversifying mutational footprints in base editors

Berríos

Barka

Gill

et al. 2022

Preprint

View full text Add to dashboard Cite

The partnership of DNA deaminase enzymes with CRISPR-Cas nucleases is now a well-established method to enable targeted genomic base editing. However, an understanding of how Cas9 and DNA deaminases collaborate to shape base editor (BE) outcomes has been lacking. Here, we employ a range of hyperactive AID base editors (hBEs) to deduce a novel mechanistic model that reveals multiple layers of previously underappreciated cooperativity in BE steps. These include: (1) Cas9 binding can potentially expose both DNA strands for capture by the deaminase, a feature enhanced by guide mismatches; (2) after strand capture, intrinsic deaminase activity can tune window size and base editing activity; and (3) non-canonical base edits can be further elicited by modulating Cas9 nicking activity. Leveraging insights from our mechanistic model, we create novel hBEs that can remarkably generate simultaneous C>T and G>A transitions over >65 bp with the potential for gene diversification.

show abstract

Evolutionary Comparative Analyses of DNA-Editing Enzymes of the Immune System: From 5-Dimensional Description of Protein Structures to Immunological Insights and Applications to Protein Engineering

Cited by 8 publications

References 216 publications

Phylogeny, Structure, Functions, and Role of AIRE in the Formation of T-Cell Subsets

Phylogeny, Structure, Functions, and Role of AIRE in the Formation of T-Cell Subsets

Ancestral reconstruction reveals catalytic inactivation of activation-induced cytidine deaminase concomitant with cold water adaption in the Gadiformes bony fish

Cooperativity between Cas9 and hyperactive AID establishes broad and diversifying mutational footprints in base editors

Contact Info

Product

Resources

About