Quantification of prospective type 2 diabetes mellitus biomarkers by stable isotope dilution with bi-labeled standard glycated peptides

Soboleva, Alena; Modzel, Maciej; Didio, Anna; Płóciennik, Halina; Kijewska, Monika; Grischina, Tatiana; Karonova, Tatiana; Bilova, Tatiana; Стефанов, В. Е.; Stefanowicz, Piotr; Frolov, Andrej

doi:10.1039/c6ay02483a

Cited by 25 publications

(25 citation statements)

References 37 publications

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“…However, the most important (if not the critical) improvement of the LC-MS/MS-based quantification methodology was done by combining it with the stable isotope dilution technique [ 139 ]. This approach ( Figure 4 A) allows direct determination of analyte concentration ( C A ) in experimental samples based on the ratio of analyte ( S A ) and internal standard ( S IS ) peak areas, multiplied by the concentration of the stable isotope-labeled internal standard ( IS ) spiked to the sample (C IS ) [ 159 ]:

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Section: Methods Of Amino Acid Analysis In Glycation Researchmentioning

confidence: 99%

“…Although the reagents, conventionally used in amino acid analysis might also produce such characteristic fragments (e.g., characteristic loss of 2,4,6-trinitrobenzene moiety from 2,4,6-trinitrobenzene sulfonate derivatives of amino acids [ 123 ]), unbiased profiling of protein enzymatic digests still needs to be performed. Recently, we successfully applied different variants of unbiased MS profiling to human plasma tryptic digests, aiming identification of specific protein glycation sites associated with type 2 diabetes mellitus (T2DM) [ 77 , 80 , 159 , 226 , 227 , 228 ]. We believe, that analogous experiments, performed at the amino acid level, might also reveal new disease-specific markers and characteristic indicators for the loss of food quality during storage and thermal treatment.…”

Section: Further Perspectivesmentioning

confidence: 99%

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Probing Protein Glycation by Chromatography and Mass Spectrometry: Analysis of Glycation Adducts

Soboleva

Vikhnina

Grishina

et al. 2017

IJMS

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Glycation is a non-enzymatic post-translational modification of proteins, formed by the reaction of reducing sugars and α-dicarbonyl products of their degradation with amino and guanidino groups of proteins. Resulted early glycation products are readily involved in further transformation, yielding a heterogeneous group of advanced glycation end products (AGEs). Their formation is associated with ageing, metabolic diseases, and thermal processing of foods. Therefore, individual glycation adducts are often considered as the markers of related pathologies and food quality. In this context, their quantification in biological and food matrices is required for diagnostics and establishment of food preparation technologies. For this, exhaustive protein hydrolysis with subsequent amino acid analysis is the strategy of choice. Thereby, multi-step enzymatic digestion procedures ensure good recoveries for the most of AGEs, whereas tandem mass spectrometry (MS/MS) in the multiple reaction monitoring (MRM) mode with stable isotope dilution or standard addition represents “a gold standard” for their quantification. Although the spectrum of quantitatively assessed AGE structures is continuously increases, application of untargeted profiling techniques for identification of new products is desired, especially for in vivo characterization of anti-glycative systems. Thereby, due to a high glycative potential of plant metabolites, more attention needs to be paid on plant-derived AGEs.

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…”

Section: Methods Of Amino Acid Analysis In Glycation Researchmentioning

confidence: 99%

Section: Further Perspectivesmentioning

confidence: 99%

Probing Protein Glycation by Chromatography and Mass Spectrometry: Analysis of Glycation Adducts

Soboleva

Vikhnina

Grishina

et al. 2017

IJMS

Self Cite

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“…The same approach was followed to synthesise [Asn 7 As control peptides, we synthesised the phosphorylated analogue [Ser 7 (PO 3 H 2 )]CSF114 (7) [33] (bearing the O-phosphoryl moiety on Ser7) and the corresponding non-glycosylated peptide CSF114 (8). We selected O-phosphorylation as control modification, because in previous studies we evaluated that dysregulation in protein expression can be involved in diabetes immune dysfunction [33].…”

Section: The Phb-lys(phb)-chemmatrix ® Rink Resin Is Specific For Deomentioning

confidence: 99%

“…Reactive dicarbonyls, glyoxal, methylglyoxal, and 3-deoxyglucosone are potent glycation agents, highly reactive more than the glucose itself and thus originate glycation chain reactions on more and more protein sites [1][2][3]. AGEs and their concentration levels are considered, in the clinics, relevant for diagnosis of diabetes complications and proteomics technologies are proposed for their characterisation [4][5][6][7]. However the possibility to trap early glycation adducts (i.e., deoxyfructosylated proteins) and the corresponding peptides by efficient mass spectrometry technology is a challenge to anticipate AGEs formation.…”

Section: Introductionmentioning

confidence: 99%

“…Therefore, efficient methods for isolation, enrichment, and recognition of glycated proteins are of current research interest. Hereof, boronate affinity materials (BAMs) have gained increasing attention in recent years [9], because of the specificity of the reaction of boronic acid that has been demonstrated efficient for the separation of a wide variety of cis diol-containing compounds, including catechols, nucleosides, nucleotides, nucleic acids, carbohydrates [10], glycoproteins [6,7,11], and enzymes [12]. In particular, boronic acid forms with cis diols esters (in aqueous solution under basic conditions) that can be easily hydrolysed under acidic conditions.…”

Section: Introductionmentioning

confidence: 99%

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An Optimised Di-Boronate-ChemMatrix Affinity Chromatography to Trap Deoxyfructosylated Peptides as Biomarkers of Glycation

et al. 2020

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We report herein a novel ChemMatrix® Rink resin functionalised with two phenylboronate (PhB) moieties linked on the N-α and N-ε amino functions of a lysine residue to specifically capture deoxyfructosylated peptides, compared to differently glycosylated peptides in complex mixtures. The new PhB-Lys(PhB)-ChemMatrix® Rink resin allows for exploitation of the previously demonstrated ability of cis diols to form phenylboronic esters. The optimised capturing and cleavage procedure from the novel functionalised resin showed that only the peptides containing deoxyfructosyl-lysine moieties can be efficiently and specifically detected by HR-MS and MS/MS experiments. We also investigated the high-selective affinity to deoxyfructosylated peptides in an ad hoc mixture containing unique synthetic non-modified peptides and in the hydrolysates of human and bovine serum albumin as complex peptide mixtures. We demonstrated that the deoxyfructopyranosyl moiety on lysine residues is crucial in the capturing reaction. Therefore, the novel specifically-designed PhB-Lys(PhB)-ChemMatrix® Rink resin, which has the highest affinity to deoxyfructosylated peptides, is a candidate to quantitatively separate early glycation peptides from complex mixtures to investigate their role in diabetes complications in the clinics.

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New Approaches for Absolute Quantification of Stable‐Isotope‐Labeled Peptide Standards for Targeted Proteomics Based on a UV Active Tag

et al. 2020

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Targeted proteomics depends on the availability of stable isotope labeled (SIL) peptide standards, which for absolute protein quantification need to be absolutely quantified. In the present study, three new approaches for absolute quantification of SIL peptides are developed. All approaches rely on a quantification tag (Qtag) with a specific UV absorption. The Qtag is attached to the peptide during synthesis and is removed by tryptic digestion under standard proteomics workflow conditions. While one quantification method (method A) is designed to allow the fast and economic production of absolutely quantified SIL peptides, two other methods (methods B and C) are developed to enable the straightforward re-quantification of SIL peptides after reconstitution to control and monitor known problems related to peptide solubility, precipitation, and adhesion to vials. All methods yield consistent results when compared to each other and when compared to quantification by amino acid analysis. The precise quantitation methods are used to characterize the in vivo specificity of the H3 specific histone methyltransferase EZH2.

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Quantification of prospective type 2 diabetes mellitus biomarkers by stable isotope dilution with bi-labeled standard glycated peptides

Cited by 25 publications

References 37 publications

Probing Protein Glycation by Chromatography and Mass Spectrometry: Analysis of Glycation Adducts

Probing Protein Glycation by Chromatography and Mass Spectrometry: Analysis of Glycation Adducts

An Optimised Di-Boronate-ChemMatrix Affinity Chromatography to Trap Deoxyfructosylated Peptides as Biomarkers of Glycation

New Approaches for Absolute Quantification of Stable‐Isotope‐Labeled Peptide Standards for Targeted Proteomics Based on a UV Active Tag

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