Loss of expression of <i>N</i>‐acetylglucosaminyltransferase Va results in altered gene expression of glycosyltransferases and galectins

Guo, Hua-Bei; Nairn, Alison V.; Harris, Kyle; Randolph, Matthew; Álvarez-Manilla, Gerardo; Moremen, Kelley W.; Pierce, Michael

doi:10.1016/j.febslet.2008.01.015

Cited by 19 publications

(9 citation statements)

References 28 publications

(63 reference statements)

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“…Many published studies have reported statistically and biologically significant microarray data using a low cutoff rate similar to that used in the present study 21-26. Moreover, many differential gene expression studies have shown low changes in glycogenes, specifically glycosyltransferases, to be biologically relevant 27-30. For example, Comelli et al29 showed that a 1.3- to 1.5-fold decrease in ST3GalI expression between fresh and activated T cells (and B cells) is sufficient to cause hyposialylation of O-glycans.…”

Section: Discussionmentioning

confidence: 83%

Detection of Differentially Expressed Wound-Healing–Related Glycogenes in Galectin-3–Deficient Mice

Saravanan

Cao

Head

et al. 2009

Invest. Ophthalmol. Vis. Sci.

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Purpose A prior study showed that exogenous galectin-3 (Gal-3) stimulates re-epithelialization of corneal wounds in wild-type (Gal-3+/+) mice but, surprisingly, not in galectin-3–deficient (Gal-3−/−) mice. In an effort to understand why the injured corneas of Gal-3−/− mice are unresponsive to exogenous Gal-3, the present study was designed to determine whether genes encoding the enzymes that regulate the synthesis of glycan ligands of Gal-3 are differentially expressed in Gal-3−/− corneas compared with the Gal-3+/+ corneas. Methods Glycogene microarray technology was used to identify differentially expressed glycosyltransferases in healing Gal-3+/+ and Gal-3−/− corneas. Results Of ~2000 glycogenes on the array, the expression of 8 was upregulated and that of 14 was downregulated more than 1.3-fold in healing Gal-3−/− corneas. A galactosyltransferase, β3GalT5, which has the ability to synthesize Gal-3 ligands was markedly downregulated in healing Gal-3−/− corneas. The genes for polypeptide galactosaminyltransferases (ppGalNAcT-3 and -7) that are known to initiate O-linked glycosylation and N-aspartyl-β-glucosaminidase, which participates in the removal of N-glycans, were found to be upregulated in healing Gal-3−/− corneas. Microarray data were validated by qRT-PCR. Conclusions Based on the known functions of the differentially expressed glycogenes, it appears that the glycan structures on glycoproteins and glycolipids, synthesized as a result of the differential glycogene expression pattern in healing Gal-3−/− corneas may lead to the downregulation of specific counterreceptors for Gal-3. This may explain, at least in part, why, unlike healing Gal-3+/+ corneas, the healing Gal-3−/− corneas are unresponsive to the stimulatory effect of exogenous Gal-3 on re-epithelialization of corneal wounds.

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Section: Discussionmentioning

confidence: 83%

Detection of Differentially Expressed Wound-Healing–Related Glycogenes in Galectin-3–Deficient Mice

Saravanan

Cao

Head

et al. 2009

Invest. Ophthalmol. Vis. Sci.

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“…1-β-1,4-GalT V). As ablation of the N -acetylglucosaminyltransferase Va gene in mice affected the expression of several other glycosyltransferase genes [37], the expression levels of the β-1,4-GalT I, II, III, IV and VI genes were examined by RT-PCR. The results showed that no significant changes in their expression levels are observed among three samples (Fig.…”

Section: Resultsmentioning

confidence: 99%

Involvement of murine β-1,4-galactosyltransferase V in lactosylceramide biosynthesis

et al. 2010

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Human β-1,4-galactosyltransferase (β-1,4-GalT) V was shown to be involved in the biosynthesis of N-glycans, O-glycans and lactosylceramide (Lac-Cer) by in vitro studies. To determine its substrate specificity, enzymatic activity and its products were analyzed using mouse embryonic fibroblast (MEF) cells from β-1,4-GalT V (B4galt5)-mutant mice. Analysis of expression levels of the β-1,4-GalT I-VI genes revealed that the expression of the β-1,4-GalT V gene in B4galt5+/−- and B4galt5−/−-derived MEF cells are a half and null when compared to that of B4galt5+/+-derived MEF cells without altering the expression levels of other β-1,4-GalT genes. These MEF cells showed no apparent difference in their growth. When β-1,4-GalT activities were determined towards GlcNAcβ-S-pNP, no significant difference in its specific activity was obtained among B4galt5+/+-, B4galt5+/−- and B4galt5−/−-derived MEF cells. No significant differences were obtained in structures and amounts of N-glycans and lectin bindings to membrane glycoproteins among B4galt5+/+-, B4galt5+/−- and B4galt5−/−-derived MEF cells. However, when cell homogenates were incubated with glucosylcer-amide in the presence of UDP-[3H]Gal, Lac-Cer synthase activity in B4galt5+/−- and B4galt5−/−-derived MEF cells decreased to 41% and 11% of that of B4galt5+/+-derived MEF cells. Consistent with this, amounts of Lac-Cer and its derivative GM3 in B4galt5−/−-derived MEF cells decreased remarkably when compared with those of B4galt5+/+ derived MEF cells. These results indicate that murine β-1,4-GalT V is involved in Lac-Cer biosynthesis.

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“…It has been already known that β1,6GlcNAc branching of N-glycans is often increased [26] and the chain length of mucintype O-glycans is generally shorten in cancer patients, notably "aberrant O-glycans" [27]. Branching N-glycan structures, such as bisecting GlcNAc and third branching1,6GlcNAc are produced by enzymes GlcNAc-transferase-III (GnT-III) and GlcNAc-transferase-IV or -V (GnT-IV or -V), respectively.…”

Section: Discussionmentioning

confidence: 99%

N- and O-glycome analysis of serum and urine from bladder cancer patients using a high-throughput glycoblotting method

Amano¹

2013

J Glycomics Lipidomics

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Loss of expression of N‐acetylglucosaminyltransferase Va results in altered gene expression of glycosyltransferases and galectins

Cited by 19 publications

References 28 publications

Detection of Differentially Expressed Wound-Healing–Related Glycogenes in Galectin-3–Deficient Mice

Detection of Differentially Expressed Wound-Healing–Related Glycogenes in Galectin-3–Deficient Mice

Involvement of murine β-1,4-galactosyltransferase V in lactosylceramide biosynthesis

N- and O-glycome analysis of serum and urine from bladder cancer patients using a high-throughput glycoblotting method

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