Discovery of novel DNA cytosine deaminase activities enables a nondestructive single-enzyme methylation sequencing method for base resolution high-coverage methylome mapping of cell-free and ultra-low input DNA

Vaisvila, Romualdas; Johnson, Sean R.; Yan, Bo; Dai, Nan; Bourkia, Billal M.; Chen, Minyong; Corrêa, Ivan R.; Yigit, Erbay; Sun, Zhiyi

doi:10.1101/2023.06.29.547047

Cited by 2 publications

(1 citation statement)

References 49 publications

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“…Recent biochemical studies conducted in vitro have shown that the enzyme SsdAtox possesses cytosine deamination activity on ssDNA. Interestingly, at elevated concentrations, SsdAtox also exhibits the ability to deaminate cytosine in dsDNA (14,33). To further explore the potential of SRE variant in mediating cytosine deamination within dsDNA genomes, we engineered fusions of SRE variant with TALE constructs, named TALE-SRE, akin to DdCBE systems, which is incorporating UGI and a nuclear localization signal (NLS) (5).…”

Section: The Versatility Of Sscbe1-srementioning

confidence: 99%

Efficient DNA base editing via an optimized DYW-like deaminase

Kweon,

Park,

Jeon

et al. 2024

Preprint

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CRISPR-based cytosine base editors enable precise genome editing without inducing double-stranded DNA breaks, yet traditionally depend on a limited selection of deaminases from the APOBEC/AID or TadA families. Here, we introduce SsCBE, a novel CRISPR-based cytosine base editor utilizing SsdAtox, a DYW-like deaminase derived from the toxin of Pseudomonas syringae. Strategic engineering of SsdAtox has led to remarkable improvements in the base editing efficiency (by up to 8.4-fold) and specificity for SsCBE, while concurrently reducing cytotoxicity. Exhibiting exceptional versatility, SsCBE was delivered and efficiently applied using diverse delivery methods, including the engineered virus-like particles (eVLPs). Its application has enabled targeted cytosine base editing in mouse zygotes and pioneering edits in mitochondrial DNA. The advent of SsCBE marks a significant advancement in the CRISPR toolkit, providing a versatile tool for advanced research and therapeutic strategies.

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Section: The Versatility Of Sscbe1-srementioning

confidence: 99%

Efficient DNA base editing via an optimized DYW-like deaminase

Kweon,

Park,

Jeon

et al. 2024

Preprint

View full text Add to dashboard Cite

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Enriched Methylomes of Low-input and Fragmented DNA Using Fragment Ligation EXclusive Methylation Sequencing (FLEXseq)

Yu,

Ahmann,

Yao

et al. 2024

Preprint

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Methylome profiling is an emerging clinical tool for tumor classification and liquid biopsies. Here, we developed FLEXseq, a genome-wide methylation profiler that enriches and sequences the fragments of DNA flanking the CCGG motif. FLEXseq strongly correlates (Pearson's r = 0.97) with whole genome bisulfite sequencing (WGBS) while enriching 18-fold. To demonstrate the broad applicability of FLEXseq, we verified its usage across cells, body fluids, and formalin-fixed paraffin-embedded (FFPE) tissues. DNA dilutions down to 250 pg decreased CpG coverage, but bias in methylation remained low (Pearson's r >= 0.90) compared to a 10 ng input. FLEXseq offers a cost-efficient, base-pair resolution methylome with potential as a diagnostic tool for tissue and liquid biopsies.

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Discovery of novel DNA cytosine deaminase activities enables a nondestructive single-enzyme methylation sequencing method for base resolution high-coverage methylome mapping of cell-free and ultra-low input DNA

Cited by 2 publications

References 49 publications

Efficient DNA base editing via an optimized DYW-like deaminase

Efficient DNA base editing via an optimized DYW-like deaminase

Enriched Methylomes of Low-input and Fragmented DNA Using Fragment Ligation EXclusive Methylation Sequencing (FLEXseq)

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