Fluorination Influences the Bioisostery of Myo‐Inositol Pyrophosphate Analogs

Author:

Hostachy Sarah1ORCID,Wang Huanchen2,Zong Guangning2,Franke Katy1,Riley Andrew M.3,Schmieder Peter1ORCID,Potter Barry V. L.3,Shears Stephen B.2,Fiedler Dorothea14ORCID

Affiliation:

1. Leibniz-Forschungsinstitut für Molekulare Pharmakologie (FMP) Robert-Rössle-Straße 10 13125 Berlin Germany

2. Inositol Signaling Group National Institutes of Health Research Triangle Park North Carolina 27709 USA

3. Medicinal Chemistry & Drug Discovery Department of Pharmacology University of Oxford Oxford OX1 3QT UK

4. Institut für Chemie Humboldt-Universität zu Berlin Brook-Taylor-Str. 2 12489 Berlin Germany

Abstract

AbstractInositol pyrophosphates (PP−IPs) are densely phosphorylated messenger molecules involved in numerous biological processes. PP−IPs contain one or two pyrophosphate group(s) attached to a phosphorylated myo‐inositol ring. 5PP−IP5 is the most abundant PP−IP in human cells. To investigate the function and regulation by PP−IPs in biological contexts, metabolically stable analogs have been developed. Here, we report the synthesis of a new fluorinated phosphoramidite reagent and its application for the synthesis of a difluoromethylene bisphosphonate analog of 5PP−IP5. Subsequently, the properties of all currently reported analogs were benchmarked using a number of biophysical and biochemical methods, including co‐crystallization, ITC, kinase activity assays and chromatography. Together, the results showcase how small structural alterations of the analogs can have notable effects on their properties in a biochemical setting and will guide in the choice of the most suitable analog(s) for future investigations.

Funder

Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung

German Academic Exchange Service

Wellcome Trust

Publisher

Wiley

Subject

General Chemistry,Catalysis,Organic Chemistry

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