| Literature DB >> 28111097 |
Pan Wu1, Dan Wan1, Gudan Xu1, Gui Wang1, Hongmin Ma1, Tingting Wang1, Yaojie Gao1, Jianzhao Qi1, Xiaoxia Chen2, Jian Zhu2, Yong-Quan Li3, Zixin Deng1, Wenqing Chen4.
Abstract
Pentostatin (PTN, deoxycoformycin) and arabinofuranosyladenine (Ara-A, vidarabine) are purine nucleoside antibiotics used clinically to treat hematological cancers and human DNA virus infections, respectively. PTN has a 1,3-diazepine ring, and Ara-A is an adenosine analog with an intriguing epimerization at the C-2' hydroxyl group. However, the logic underlying the biosynthesis of these interesting molecules has long remained elusive. Here, we report that the biosynthesis of PTN and Ara-A employs an unusual protector-protégé strategy. To our surprise, we determined that a single gene cluster governs PTN and Ara-A biosynthesis via two independent pathways. Moreover, we verified that PenB functions as a reversible oxidoreductase for the final step of PTN. Remarkably, we provided the first direct biochemical evidence that PTN can protect Ara-A from deamination by selective inhibition of the host adenosine deaminase. These findings expand our knowledge of natural product biosynthesis and open the way for target-directed genome mining of Ara-A/PTN-related antibiotics.Entities:
Keywords: arabinofuranosyladenine; biosynthesis; gene cluster; pentostatin; protector-protégé strategy; purine nucleoside antibiotics
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Year: 2017 PMID: 28111097 DOI: 10.1016/j.chembiol.2016.12.012
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116