Literature DB >> 31172184

A validated collection of mouse monoclonal antibodies to human glycosyltransferases functioning in mucin-type O-glycosylation.

Catharina Steentoft1, Zhang Yang1, Shengjun Wang1,2, Tongzhong Ju3,4, Malene B Vester-Christensen1,5, María F Festari1,6, Sarah L King1, Kelley Moremen7, Ida S B Larsen1, Christoffer K Goth1, Katrine T Schjoldager1, Lars Hansen1, Eric P Bennett1, Ulla Mandel1, Yoshiki Narimatsu1.   

Abstract

Complex carbohydrates serve a wide range of biological functions in cells and tissues, and their biosynthesis involves more than 200 distinct glycosyltransferases (GTfs) in human cells. The kinetic properties, cellular expression patterns and subcellular topology of the GTfs direct the glycosylation capacity of a cell. Most GTfs are ER or Golgi resident enzymes, and their specific subcellular localization is believed to be distributed in the secretory pathway according to their sequential role in the glycosylation process, although detailed knowledge for individual enzymes is still highly fragmented. Progress in quantitative transcriptome and proteome analyses has greatly advanced our understanding of the cellular expression of this class of enzymes, but availability of appropriate antibodies for in situ monitoring of expression and subcellular topology have generally been limited. We have previously used catalytically active GTfs produced as recombinant truncated secreted proteins in insect cells for generation of mouse monoclonal antibodies (mAbs) to human enzymes primarily involved in mucin-type O-glycosylation. These mAbs can be used to probe subcellular topology of active GTfs in cells and tissues as well as their presence in body fluids. Here, we present several new mAbs to human GTfs and provide a summary of our entire collection of mAbs, available to the community. Moreover, we present validation of specificity for many of our mAbs using human cell lines with CRISPR/Cas9 or zinc finger nuclease (ZFN) knockout and knockin of relevant GTfs.
© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.

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Keywords:  CRISPR Cas9; GalNAc-transferase; immunocytology; immunohistology; western blot

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Year:  2019        PMID: 31172184      PMCID: PMC6704369          DOI: 10.1093/glycob/cwz041

Source DB:  PubMed          Journal:  Glycobiology        ISSN: 0959-6658            Impact factor:   4.313


  70 in total

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Journal:  Glycobiology       Date:  2018-03-01       Impact factor: 4.313

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9.  Controls for immunohistochemistry: the Histochemical Society's standards of practice for validation of immunohistochemical assays.

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