Wen-Shuo Cheng scite author profile

Wen-Shuo Cheng

4Publications

17Citation Statements Received

29Citation Statements Given

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150

Affiliations

Central South University, National Taiwan University, National Tsing Hua University

Publications

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Chiral electrokinetic chromatography‐electrospray ionization‐mass spectrometry using a double junction interface

et al. 2012

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A double junction interface was utilized to preserve separation efficiency and alleviate ion suppression from sulfated β-cyclodextrin (S-β-CD) in electrokinetic chromatography-electrospray ionization-mass spectrometry. The utility of the approach was demonstrated by chiral EKC-MS analysis of dihydroxyphenylalanine and methyldihydroxyphenylalanine enantiomers using either low concentration (counter-migration mode; 0.1% S-β-CD) or high concentration (carrier mode; 2% S-β-CD). In the counter-migration mode, S-β-CD anions were supplied continuously from the junction reservoir to the separation column so that the effective separation length was preserved. This interface is especially useful under carrier mode in which high concentration of S-β-CD will migrate toward the ESI source. With the use of the double junction interface, the S-β-CD exited the separation column will remain in the junction reservoir, whereas the analyte will flow toward the ESI source through a connecting column. As a result, no ion suppression was observed and the sensitivity was improved significantly.

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Phosphonium Ylide-Mediated Programmable Fluorination to Access Mono- and Difluoromethylarenes

Zheng

Xie

et al. 2021

Org. Lett.

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Compounds bearing fluorinated moieties are pervasive in a wide range of pharmaceuticals and agrochemicals. The installation of fluorinated units is a persistently vital task in synthetic chemistry, where facile and manipulable assays are highly demanding. Herein, we establish a general and programmable fluorination strategy for the modular assembly of mono- and difluoromethylarenes through the controllable deprotonation and fluorination of phosphonium ylides. Moreover, the rational combination of the reaction sequence allows the rapid construction of diversified fluorine-containing arenes.

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A chip-based method for studying the effects of exogenous proteins on neuronal axons

Hsu

Cheng

et al. 2012

Analytical Biochemistry

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Phosphine-Mediated Morita–Baylis–Hillman-Type/Wittig Cascade: Access to E-Configured 3-Styryl- and 3-(Benzopyrrole/furan-2-yl) Quinolinones

et al. 2022

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A phosphine-mediated, well-designed Morita–Baylis–Hillman-type/Wittig cascade for the rapid assembly of a quinolinone framework from benzaldehyde derivatives is developed for the first time. By rationally combining I2/NIS-mediated cyclization, biologically relevant 3-(benzopyrrole/furan-2-yl) quinolinones were facilely synthesized in a one-pot process by starting from 3-styryl-quinolinones bearing an o-hydroxy/amino group, significantly expanding the chemical space of this privileged skeleton. Further utility of this protocol is illustrated by successfully performing this transformation in a catalytic manner through in situ reduction of phosphine oxide by phenylsilane.

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Wen-Shuo Cheng

Chiral electrokinetic chromatography‐electrospray ionization‐mass spectrometry using a double junction interface

Phosphonium Ylide-Mediated Programmable Fluorination to Access Mono- and Difluoromethylarenes

A chip-based method for studying the effects of exogenous proteins on neuronal axons

Phosphine-Mediated Morita–Baylis–Hillman-Type/Wittig Cascade: Access to E-Configured 3-Styryl- and 3-(Benzopyrrole/furan-2-yl) Quinolinones

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