2013
DOI: 10.1074/jbc.m113.468397
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IgG1 Thioether Bond Formation in Vivo

Abstract: Background: Thioethers have been observed in therapeutic antibodies, with increasing levels upon storage. Results: IgG1 thioether bond formation is naturally occurring, but the formation rate depends on light chain type. Conclusion: Slower thioether bond formation on IgG1 is caused by dehydrogenation impairment through its light chain. Significance: Safety concerns associated with thioether control on therapeutic antibodies are diminished by its natural production.

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Cited by 43 publications
(59 citation statements)
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“…The thioether bond formed at this position can be detected as a non-reducible species possessing the combined mass of the LC and HC by reducing capillary electrophoresis or reducing RP-HPLC/MS, or can be detected by peptide mapping (5). Peptide mapping under non-reducing conditions has been used to characterize this species as well as quantify the relative levels (10). Digestions of a previously stressed IgG1 antibody containing a light chain (IgG1) with the protease Lys-C generates a thioether-linked peptide of the sequence (H)SC*DK/(L)SFNRGEC*, where the asterisks represent positions of the modified cystine linkage, also called a lanthionine, and the letters in parentheses represent the antibody polypeptide chains (H for heavy chain, L for light chain).…”
Section: Resultsmentioning
confidence: 99%
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“…The thioether bond formed at this position can be detected as a non-reducible species possessing the combined mass of the LC and HC by reducing capillary electrophoresis or reducing RP-HPLC/MS, or can be detected by peptide mapping (5). Peptide mapping under non-reducing conditions has been used to characterize this species as well as quantify the relative levels (10). Digestions of a previously stressed IgG1 antibody containing a light chain (IgG1) with the protease Lys-C generates a thioether-linked peptide of the sequence (H)SC*DK/(L)SFNRGEC*, where the asterisks represent positions of the modified cystine linkage, also called a lanthionine, and the letters in parentheses represent the antibody polypeptide chains (H for heavy chain, L for light chain).…”
Section: Resultsmentioning
confidence: 99%
“…Recently, we explored the base-catalyzed thioether bond formation in human IgG1s (10). Formation rates were faster in antibodies containing light chains over those with the more common light chains.…”
mentioning
confidence: 99%
“…Bottom-up LC-MS, at reducing and non-reducing conditions [86][87][88] Aggregates and fragments SEC with light scattering detection, nanoparticle tracking analysis, light obscuration, micro-flow imaging Large size range needs to be covered. Multiple methods are required [102] [47] This direct connection between the amount of sialylated glycoforms present for a given antibody sample and the anti-inflammatory effect of IgG is also supported by the fact that steady-state serum IgG shows sialylation to a higher extent than serum IgG produced in response to a challenge with a specific antigen.…”
Section: N-glycosylationmentioning
confidence: 99%
“…The state of the art methods for analyzing these variants are RP-LC and MS-based peptide map both under non-reducing conditions. [86] Using a mass tag or a fluorescent dye for labeling before the tryptic digest of the protein also allows the detection of free SH-groups in non-reduced peptide map. [87][88][89] …”
Section: Disulfide Bond Variantsmentioning
confidence: 99%
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