Publications by authors named "Eng Piew Louis Kok"
Article Synopsis
- Researchers fused inactive Cas13 proteins with a modified human ADAR2 deaminase to create a new method for precise RNA editing without causing permanent changes in the genome.
- The new platform, called xPERT, was engineered to improve the balance between effective on-target editing and reduced off-target activity, addressing a major concern in existing RNA-editing technologies.
- Compared to previous systems (REPAIRv1 and REPAIRv2), xPERT demonstrates strong on-target editing while minimizing unintended alterations, making it a potentially safer option for customizing RNA and protein functions.
Inosine is a prevalent RNA modification in animals and is formed when an adenosine is deaminated by the ADAR family of enzymes. Traditionally, inosines are identified indirectly as variants from Illumina RNA-sequencing data because they are interpreted as guanosines by cellular machineries. However, this indirect method performs poorly in protein-coding regions where exons are typically short, in non-model organisms with sparsely annotated single-nucleotide polymorphisms, or in disease contexts where unknown DNA mutations are pervasive.
View Article and Find Full Text PDFAdenosine-to-inosine (A-to-I) RNA editing is a fundamental posttranscriptional mechanism that greatly diversifies the transcriptome in many living organisms, including mammals. Multiple studies have demonstrated the importance of this process not just in normal development and physiology but also in various human diseases. Importantly, the precise editing level of a site may have downstream consequences on cellular behavior.
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