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Glycan chip based on structure-switchable DNA linker for on-chip biosynthesis of cancer-associated complex glycans.


ABSTRACT: On-chip glycan biosynthesis is an effective strategy for preparing useful complex glycan sources and for preparing glycan-involved applications simultaneously. However, current methods have some limitations when analyzing biosynthesized glycans and optimizing enzymatic reactions, which could result in undefined glycan structures on a surface, leading to unequal and unreliable results. In this work, a glycan chip is developed by introducing a pH-responsive i-motif DNA linker to control the immobilization and isolation of glycans on chip surfaces in a pH-dependent manner. On-chip enzymatic glycosylations are optimized for uniform biosynthesis of cancer-associated Globo H hexasaccharide and its related complex glycans through stepwise quantitative analyses of isolated products from the surface. Successful interaction analyses of the anti-Globo H antibody and MCF-7 breast cancer cells with on-chip biosynthesized Globo H-related glycans demonstrate the feasibility of the structure-switchable DNA linker-based glycan chip platform for on-chip complex glycan biosynthesis and glycan-involved applications.

SUBMITTER: Heo HR 

PROVIDER: S-EPMC7925590 | biostudies-literature | 2021 Mar

REPOSITORIES: biostudies-literature

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Glycan chip based on structure-switchable DNA linker for on-chip biosynthesis of cancer-associated complex glycans.

Heo Hye Ryoung HR   Joo Kye Il KI   Seo Jeong Hyun JH   Kim Chang Sup CS   Cha Hyung Joon HJ  

Nature communications 20210302 1


On-chip glycan biosynthesis is an effective strategy for preparing useful complex glycan sources and for preparing glycan-involved applications simultaneously. However, current methods have some limitations when analyzing biosynthesized glycans and optimizing enzymatic reactions, which could result in undefined glycan structures on a surface, leading to unequal and unreliable results. In this work, a glycan chip is developed by introducing a pH-responsive i-motif DNA linker to control the immobi  ...[more]

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