Kisaburo Deguchi scite author profile

Expression of the tumor suppressor p16INK4a after stable transfection can restore the susceptibility of epithelial tumor cells to anoikis. This property is linked to increases in the expression and cell-surface presence of the fibronectin receptor. Considering its glycan chains as pivotal signals, we assumed an effect of p16INK4a on glycosylation. To test this hypothesis for human Capan-1 pancreatic carcinoma cells, we combined microarray for selected glycosyltransferase genes with 2D chromatographic glycan profiling and plant lectin binding. Major differences between p16-positive and control cells were detected. They concerned expression of b1,4-galactosyltransferases (down-regulation of b1,4-galactosyltransferases-I ⁄ V and up-regulation of b1,4-galactosyltransferase-IV) as well as decreased a2,3-sialylation of O-glycans and a2,6-sialylation of N-glycans. The changes are compatible with increased b 1 -integrin maturation, subunit assembly and binding activity of the a 5 b 1 -integrin. Of further functional relevance in line with our hypothesis, we revealed differential reactivity towards endogenous lectins, especially galectin-1. As a result of reduced sialylation, the cells' capacity to bind galectin-1 was enhanced. In parallel, the level of transcription of the galectin-1 gene increased conspicuously in p16 INK4a-positive cells, and even figured prominently in a microarray on 1996 tumor-associated genes and in proteomic analysis. The cells therefore gain optimal responsiveness. The correlation between genetically modulated galectin-1 levels and anoikis rates in engineered transfectants inferred functional significance. To connect these findings to the fibronectin receptor, galectin-1 was shown to be co-immunoprecipitated. We conclude that p16 INK4aAbbreviations

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Vascular RAGE transports oxytocin into the brain to elicit its maternal bonding behaviour in mice

Yamamoto

et al. 2019

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Oxytocin sets the stage for childbirth by initiating uterine contractions, lactation and maternal bonding behaviours. Mice lacking secreted oxcytocin ( Oxt −/− , Cd38 −/− ) or its receptor ( Oxtr −/− ) fail to nurture. Normal maternal behaviour is restored by peripheral oxcytocin replacement in Oxt −/− and Cd38 −/− , but not Oxtr −/− mice, implying that circulating oxcytocin crosses the blood-brain barrier. Exogenous oxcytocin also has behavioural effects in humans. However, circulating polypeptides are typically excluded from the brain. We show that oxcytocin is transported into the brain by receptor for advanced glycation end-products (RAGE) on brain capillary endothelial cells. The increases in oxcytocin in the brain which follow exogenous administration are lost in Ager −/− male mice lacking RAGE, and behaviours characteristic to abnormalities in oxcytocin signalling are recapitulated in Ager −/− mice, including deficits in maternal bonding and hyperactivity. Our findings show that RAGE-mediated transport is critical to the behavioural actions of oxcytocin associated with parenting and social bonding.

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Simple separation of isomeric sialylated N‐glycopeptides by a zwitterionic type of hydrophilic interaction chromatography

Takegawa

Deguchi²,

Ito

et al. 2006

J of Separation Science

137

104

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Asparagine-linked oligosaccharides (N-glycans) usually show structural heterogeneity, especially in proteins with sialylated N-glycans and, therefore, their structural analysis is still very difficult. A zwitterionic type of hydrophilic interaction chromatography column with sulfobetaine functional groups (called a ZIC-HILIC column) was applied to the separation of tryptic peptides of alpha-1-acid glycoprotein. It was demonstrated that the ZIC-HILIC separation column has a selectivity for sialylated N-glycopeptides and a high capability for separation based on the structural recognition of sialylated N-glycan isomers as well as for the previously reported neutral N-glycans and N-glycopeptides. The retention characteristics of neutral and sialylated N-glycans derivatized with 2-aminopyridine (PA N-glycans) demonstrate that the retentions of the N-glycans are based primarily on hydrophilic interaction with the water-rich liquid layer generated on the surface of the ZIC-HILIC column. In addition, the electrostatic repulsion interaction shielded with counter ions effectively tunes the separation and recognition of sialylated N-glycan isomers.

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Separation of isomeric 2-aminopyridine derivatized N-glycans and N-glycopeptides of human serum immunoglobulin G by using a zwitterionic type of hydrophilic-interaction chromatography

Takegawa

Deguchi

Keira

et al. 2006

Journal of Chromatography A

122

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which are usually difficult to separate on NP and RP columns. In addition, it is noteworthy that IgG 9 glycopeptides consisting of isomeric N-glycans and the same peptide sequences can be sufficiently 10 separated on a ZIC-HILIC column. The latter feature (i.e., selectivity) was also demonstrated by 11 easily separating two peptide groups with/without N-glycans. Thus, we note that the ZIC-HILIC 12 column is highly promising for a simple analysis of N-glycans and N-glycopeptide samples.

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High‐Throughput Protein Glycomics: Combined Use of Chemoselective Glycoblotting and MALDI‐TOF/TOF Mass Spectrometry

et al. 2004

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