Generation of New Glycoanalogues of Polyene Antibiotics by Synthetic Biology—Testing Current Technical Boundaries

Author:

Hogan Mark1ORCID,Song Yuhao1ORCID,Muldoon Jimmy2ORCID,Caffrey Patrick1ORCID

Affiliation:

1. School of Biomolecular and Biomedical Science, University College Dublin, D04 V1W8 Dublin, Ireland

2. School of Chemistry and Centre for Synthesis and Chemical Biology, University College Dublin, D04 V1W8 Dublin, Ireland

Abstract

A number of antifungal drugs are based on polyene macrolides that cause severe side effects. Most of these compounds contain a single aminodeoxysugar, D-mycosamine. Toxicity can be reduced by increasing the extent of glycosylation. The aromatic heptaene 67-121C and two analogues of the degenerate heptaene nystatin have a second sugar attached to the C4′ hydroxyl of mycosamine. Another nystatin analogue has L-digitoxose as a second sugar attached to C35 on the macrolactone ring. The pentaene selvamicin has 4-O-methyl-L-digitoxose at C27, the equivalent position. To assist the production of new antifungals by synthetic biology, we explore further the utility of three classes of polyene glycosyltransferase: extending glycosyltransferases that form disaccharide-containing polyenes, glycosyltransferases that add the L-digitoxose sugars of nystatin A3 and selvamicin, and mycosaminyltransferases that add the primary aminodeoxysugar. In addition, we combine enzymatic hyperglycosylation with a known chemical method for adding sugars to the C3′ amino group of mycosamine. This was used to convert the disaccharide-containing 67-121C heptaene to forms containing branched trisaccharide or tetrasaccharide chains. These analogues are of interest for testing as anti-Leishmania drugs.

Funder

Irish Research Council

SFI Research Infrastructure Programme

Biorbic—the SFI Bioeconomy Research Centre

School of Chemistry

UCD

Publisher

MDPI AG

Reference53 articles.

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3. Sterol profiling of Leishmania parasites using a new HPLC-tandem mass spectrometry-based method and antifungal azoles as chemical probes reveals a key intermediate sterol that supports a branched ergosterol biosynthetic pathway;Feng;Int. J. Parasitol. Drugs Drug Resist.,2022

4. Abu-Salah, K.M. (1996). Amphotericin B: An update. Br. J. Biomed. Sci., 53.

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