Pathways of thymidine hypermodification

Author:

Lee Yan-Jiun1,Dai Nan1,Müller Stephanie I1ORCID,Guan Chudi1,Parker Mackenzie J1,Fraser Morgan E1,Walsh Shannon E1,Sridar Janani1,Mulholland Andrew1,Nayak Krutika1,Sun Zhiyi1,Lin Yu-Cheng1,Comb Donald G1,Marks Katherine1,Gonzalez Reyaz2,Dowling Daniel P2,Bandarian Vahe3ORCID,Saleh Lana1,Corrêa Ivan R1ORCID,Weigele Peter R1

Affiliation:

1. Research Department, New England Biolabs, Inc., 240 County Road, Ipswich, MA01938, USA

2. Chemistry Department, University of Massachusetts Boston, 100 William T. Morrissey Blvd. Boston, MA02125, USA

3. Department of Chemistry, University of Utah, 315 South 1400 East Salt Lake City, UT 84112, USA

Abstract

Abstract The DNAs of bacterial viruses are known to contain diverse, chemically complex modifications to thymidine that protect them from the endonuclease-based defenses of their cellular hosts, but whose biosynthetic origins are enigmatic. Up to half of thymidines in the Pseudomonas phage M6, the Salmonella phage ViI, and others, contain exotic chemical moieties synthesized through the post-replicative modification of 5-hydroxymethyluridine (5-hmdU). We have determined that these thymidine hypermodifications are derived from free amino acids enzymatically installed on 5-hmdU. These appended amino acids are further sculpted by various enzyme classes such as radical SAM isomerases, PLP-dependent decarboxylases, flavin-dependent lyases and acetyltransferases. The combinatorial permutations of thymidine hypermodification genes found in viral metagenomes from geographically widespread sources suggests an untapped reservoir of chemical diversity in DNA hypermodifications.

Funder

New England Biolabs

Publisher

Oxford University Press (OUP)

Subject

Genetics

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