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Jun Haginaka

Researcher at Mukogawa Women's University

Publications -  225
Citations -  6576

Jun Haginaka is an academic researcher from Mukogawa Women's University. The author has contributed to research in topics: Molecularly imprinted polymer & High-performance liquid chromatography. The author has an hindex of 43, co-authored 221 publications receiving 6287 citations.

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Separation and sensing based on molecular recognition using molecularly imprinted polymers

TL;DR: Recent developments in molecularly imprinted polymers are described with their applications as separation media in liquid chromatography, capillary electrophoresis, solid-phase extraction, and membranes.
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Protein-based chiral stationary phases for high-performance liquid chromatography enantioseparations.

TL;DR: The enantioseparations of various compounds using proteins as the chiral selectors in high-performance liquid chromatography (HPLC) are considered in this review.
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Molecularly imprinted polymers as affinity‐based separation media for sample preparation

TL;DR: An over view of two types of MIPs used for the sample preparation and modes of molecularly imprinted SPE (online mode, offline mode, on-column extraction, SPME, and microextraction in packed syringe) are given, focusing on the advantages and disadvantages of these types and modes.
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Monodispersed, molecularly imprinted polymers as affinity-based chromatography media

TL;DR: This review article deals with preparation methods for spherical and monodispersed molecularly imprinted polymers (MIPs) in micrometer sizes, which include suspension polymerization in water, liquid perfluorocarbon and mineral oil, seed polymerization and dispersion/precipitation polymerization.
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Enantiomer separation of drugs by capillary electrophoresis using proteins as chiral selectors.

TL;DR: The separation of drug enantiomers using proteins as the chiral selectors in capillary electrophoresis (CE) is considered in this review and the advantages and limitations of the two modes and the factors affecting theChiral separations of various drugs by protein-based CE are discussed.