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Rakesh N. Veedu

Researcher at Murdoch University

Publications -  113
Citations -  3251

Rakesh N. Veedu is an academic researcher from Murdoch University. The author has contributed to research in topics: Oligonucleotide & Locked nucleic acid. The author has an hindex of 25, co-authored 108 publications receiving 2292 citations. Previous affiliations of Rakesh N. Veedu include University of Oldenburg & University of Queensland.

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Progress, opportunity, and perspective on exosome isolation - efforts for efficient exosome-based theranostics.

TL;DR: A panoramic view of current exosome isolation techniques is provided, providing perspectives toward the development of novel approaches for high-efficient exosomes isolation from various types of biological matrices.
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Three decades of nucleic acid aptamer technologies: Lessons learned, progress and opportunities on aptamer development.

TL;DR: By analyzing key aspects of SELEX including initial library design, target preparation, PCR optimization, and single strand DNA separation, this work provides a comprehensive analysis of individual steps to facilitate researchers intending to develop personalized protocols to address many of the obstacles inSELEX.
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Locked nucleic acids: Promising nucleic acid analogs for therapeutic applications

TL;DR: This work highlights the applications of LNA nucleotides for controlling gene expression in different nucleic acid‐based therapeutic strategies both in vitro and in vivo.
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Locked nucleic acid as a novel class of therapeutic agents.

TL;DR: The uses of LNA for regulation of gene expression with emphasis on RNA targeting are highlighted, including applications within various gene silencing strategies both in vitro and in vivo.
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Systematic Screening of Commonly Used Commercial Transfection Reagents towards Efficient Transfection of Single-Stranded Oligonucleotides.

TL;DR: The transfection efficacy of Lipofectamine 2000 was compromised by its high toxicity, which may adversely affect its application in most cells, and RNAiMAX may be a better option for majority of cells when lower toxicity is desired.