Chemical Glycoproteomics

Palaniappan, Krishnan K.; Bertozzi, Carolyn R.

doi:10.1021/acs.chemrev.6b00023

Cited by 227 publications

(211 citation statements)

References 416 publications

Supporting

Mentioning

205

Contrasting

Unclassified

Order By: Relevance

“…[15] To target sialoglycoproteins specifically, cells are metabolically labeled with a modified peracetylated N -acetylmannosamine (Ac 4 ManNAc) analogue such as peracetylated N -azidoace-tylmannosamine (Ac 4 ManNAz, 1 ) [16] or its alkynyl counterpart, peracetylated N -pentynoylmannosamine (Ac 4 ManNAl). These compounds are converted by the Roseman–Warren pathway into the corresponding sialic acid derivatives, which are, in turn, incorporated into sialoglycoproteins.…”

mentioning

confidence: 99%

Bioorthogonal Labeling of Human Prostate Cancer Tissue Slice Cultures for Glycoproteomics

et al. 2017

Self Cite

View full text Add to dashboard Cite

Sialylated glycans are found at elevated levels in many types of cancer and have been implicated in disease progression. However, the specific glycoproteins that contribute to the cancer cell-surface sialylation are not well characterized, specifically in bona fide human disease tissue. Metabolic and bioorthogonal labeling methods have previously enabled the enrichment and identification of sialoglycoproteins from cultured cells and model organisms. Herein, we report the first application of this glycoproteomic platform to human tissues cultured ex vivo. Both normal and cancerous prostate tissues were sliced and cultured in the presence of the azide-functionalized sialic acid biosynthetic precursor Ac4ManNAz. The compound was metabolized to the azidosialic acid and incorporated into cell surface and secreted sialoglycoproteins. Chemical biotinylation followed by enrichment and mass spectrometry led to the identification of glycoproteins that were found at elevated levels or uniquely in cancerous prostate tissue. This work therefore extends the use of bioorthogonal labeling strategies to problems of clinical relevance.

show abstract

mentioning

confidence: 99%

Bioorthogonal Labeling of Human Prostate Cancer Tissue Slice Cultures for Glycoproteomics

et al. 2017

Self Cite

View full text Add to dashboard Cite

show abstract

“…6,7 Importantly, the number of eukaryotic proteins known to be glycosylated has dramatically increased in recent years owing, in major part, to improvements in glycoproteomic mass spectrometry methodologies. 8–10 …”

mentioning

confidence: 99%

Synthesis of rhamnosylated arginine glycopeptides and determination of the glycosidic linkage in bacterial elongation factor P

et al. 2017

View full text Add to dashboard Cite

show abstract

“…For purpose of improving MS detection sensitivity, many chemical derivatizations of free glycans have been developed to improve the detection sensitivity during MS analysis [24–26], including widely used permethylation [27], reductive amination with various type of hydrophobic aromatic amines [26], Michael's addiction with 1-phenyl-3-methyl-5-pyrazolone (PMP) [28] and acid catalyzed condensation with hydrazides or hydroxylamines to form hydrazones or oximes [29–32]. These derivatizations are usually applied to significant amounts of samples (μg to mg), often under relatively strong reaction conditions involving heating with acid or base.…”

Section: Introductionmentioning

confidence: 99%

Sensitive and robust MALDI-TOF-MS glycomics analysis enabled by Girard's reagent T on-target derivatization (GTOD) of reducing glycans

Zhang

Wang

Jin

et al. 2019

Analytica Chimica Acta

View full text Add to dashboard Cite

Sensitive glycomics analysis by matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF-MS) is of great importance but significantly hampered by their low ionization efficiency and labile sialic acid moieties. Chemical derivatization offers a viable way to improve both the ionization efficiency and analytical sensitivity of the glycans in MS analysis by altering their hydrophobicity or charge property. Here we employed Girard's reagent T (GT) for on-target derivatization (GTOD) of reducing glycan under mild acid condition to form stable hydrazones at room temperature, allowing rapid and sensitive identification of neutral and sialylated glycans in positive-ion mode as only permanently positive charged molecular ions without multiple ion adducts by MALDI-TOF-MS. The MS signal intensities of lactose, sialylated N-glycans derived from bovine fetuin and neutral N-glycans derived from RNaseB and ovalbumin were boosted by 7.44, 9.13, 12.96 and 13.47 folds on average (n = 3), respectively. More importantly, after GTOD strategy, unwanted desialylation of sialylated glycans during MS was suppressed. The detection limit of the assay is desirable since the nanogram of N-glycans derived from 0.16 μg ovalbumin could be detected. The assay demonstrated good stability (RSD≤2.95%, within 10 days), reliable reproducibility (RSD = 2.96%, n = 7) and a desirable linear dynamic range from 78 nmol/mL to 10 μmol/mL. The strategy has been successfully applied to MS analysis of reducing glycans from human milks, neutral and sialylated O-, N-glycans from glycoproteins, and reducing glycans derived from glycosphingolipids, presenting neater [M]+ signals which allow detection of more low-abundance glycans and assignation of Neu5Ac vs. Neu5Gc or fucose vs. hexose in glycans due to the absence of the ambiguous interpretation from multiple peaks (ion adducts [M+Na]+ and [M+K]+). Moreover, the GTOD assay prevents desialylation during MALDI-TOF-MS profiling and enables distinct linkage-specific characterization of terminal sialic acids of N-glycans derived from human serum protein when combines with an esterification.

show abstract

Chemical Glycoproteomics

Cited by 227 publications

References 416 publications

Bioorthogonal Labeling of Human Prostate Cancer Tissue Slice Cultures for Glycoproteomics

Bioorthogonal Labeling of Human Prostate Cancer Tissue Slice Cultures for Glycoproteomics

Synthesis of rhamnosylated arginine glycopeptides and determination of the glycosidic linkage in bacterial elongation factor P

Sensitive and robust MALDI-TOF-MS glycomics analysis enabled by Girard's reagent T on-target derivatization (GTOD) of reducing glycans

Contact Info

Product

Resources

About