Labeling proteins with fluorine-18 using N-succinimidyl 4-[18F]fluorobenzoate

## Abstract An efficient preparation of __N__‐succinimidyl 4‐[^18^F]fluorobenzoate ([^18^F]SFB) based on a convenient three‐step, one‐pot procedure is described. [^18^F]Fluorination of the precursor ethyl 4‐(trimethylammonium triflate)benzoate gave ethyl 4‐[^18^F]fluorobenzoate. Saponification of t

## Abstract Three G‐rich oligonucleotides (GROs) were conjugated with N‐succinimidyl 4‐[^18^F]fluorobenzoate (S^18^FB). The yields for GRO5, the shortest sequence among those three GROs being tested, were 42, 70, 84, and 99% at GRO5 concentration of 59, 118, 236, and 472 nmol/100 µl, respectively.

## Abstract The batch microfluidic technology is a promising system for sequential chemical steps combining the advantages of micro‐scale reactions, while addressing some shortcomings of flow‐through systems. We report herein the convenient three‐step, one‐pot synthesis and purification of [^18^F]S

## Abstract We have labeled proinsulin connecting peptide (C‐peptide) with fluorine‐18 (__t__~½~=109.7 min) in order to perform __in vivo__ biodistribution and pharmacokinetic studies with position emission tomography (PET). This study reports the optimization of the conjugation labeling in the N‐t

## Abstract The acylation reagent [^18^F]__N__‐succinimidyl‐4‐fluorobenzoate (^18^F‐SFB) has been prepared using a new two‐step approach. The starting material __p‐__[^18^F]fluorobenzaldehyde (^18^F‐FBA) was obtained by an improved radiosynthesis with a decay‐corrected radiochemical yield of 66±6 %