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Chemo-enzymatic production of base-modified ATP analogues for polyadenylation of RNA.


ABSTRACT: Base-modified adenosine-5'-triphosphate (ATP) analogues are highly sought after as building blocks for mRNAs and non-coding RNAs, for genetic code expansion or as inhibitors. Current synthetic strategies lack efficient and robust 5'-triphosphorylation of adenosine derivatives or rely on costly phosphorylation reagents. Here, we combine the efficient organic synthesis of base-modified AMP analogues with enzymatic phosphorylation by a promiscuous polyphosphate kinase 2 class III from an unclassified Erysipelotrichaceae bacterium (EbPPK2) to generate a panel of C2-, N6-, or C8-modified ATP analogues. These can be incorporated into RNA using template independent poly(A) polymerase. C2-halogenated ATP analogues were incorporated best, with incorporations of 300 to >1000 nucleotides forming hypermodified poly(A) tails.

SUBMITTER: Mitton-Fry RM 

PROVIDER: S-EPMC11322958 | biostudies-literature | 2024 Aug

REPOSITORIES: biostudies-literature

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Chemo-enzymatic production of base-modified ATP analogues for polyadenylation of RNA.

Mitton-Fry Rachel M RM   Eschenbach Jannik J   Schepers Helena H   Rasche René R   Erguven Mehmet M   Kümmel Daniel D   Rentmeister Andrea A   Cornelissen Nicolas V NV  

Chemical science 20240716 32


Base-modified adenosine-5'-triphosphate (ATP) analogues are highly sought after as building blocks for mRNAs and non-coding RNAs, for genetic code expansion or as inhibitors. Current synthetic strategies lack efficient and robust 5'-triphosphorylation of adenosine derivatives or rely on costly phosphorylation reagents. Here, we combine the efficient organic synthesis of base-modified AMP analogues with enzymatic phosphorylation by a promiscuous polyphosphate kinase 2 class III from an unclassifi  ...[more]

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