2020
DOI: 10.1371/journal.pone.0229027
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R409K mutation prevents acid-induced aggregation of human IgG4

Abstract: Human immunoglobulin G isotype 4 (IgG4) antibodies are suitable for use in either the antagonist or agonist format because their low effector functions prevent target cytotoxicity or unwanted cytokine secretion. However, while manufacturing therapeutic antibodies, they are exposed to low pH during purification, and IgG4 is more susceptible to low-pH-induced aggregation than IgG1. Therefore, we investigated the underlying mechanisms of IgG4 aggregation at low pH and engineered an IgG4 with enhanced stability. B… Show more

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Cited by 10 publications
(8 citation statements)
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“…We first evaluated the cytotoxic activity of H22-dPBD against THP-1 cells, a monocytic leukemia cell line expressing CD64 ( Figure 2B ). In addition to H22-dPBD humanized with IgG1 (H22(IgG1)-dPBD) and the isotype matched control ADC [DNP(IgG1)-dPBD], we also tested the nullbody H22-dPBD [H22(Null)-dPBD], in which H22 is humanized with an IgG4 analogue having three mutations that stabilize the Ab and minimize non-specific binding to Fcγ receptors ( 39 ). Compared with DNP(IgG1)-dPBD, H22(IgG1)-dPBD had a more effective level of CD64-specific cytotoxicity.…”
Section: Resultsmentioning
confidence: 99%
“…We first evaluated the cytotoxic activity of H22-dPBD against THP-1 cells, a monocytic leukemia cell line expressing CD64 ( Figure 2B ). In addition to H22-dPBD humanized with IgG1 (H22(IgG1)-dPBD) and the isotype matched control ADC [DNP(IgG1)-dPBD], we also tested the nullbody H22-dPBD [H22(Null)-dPBD], in which H22 is humanized with an IgG4 analogue having three mutations that stabilize the Ab and minimize non-specific binding to Fcγ receptors ( 39 ). Compared with DNP(IgG1)-dPBD, H22(IgG1)-dPBD had a more effective level of CD64-specific cytotoxicity.…”
Section: Resultsmentioning
confidence: 99%
“…The alternative use of detergent is less straightforward and may affect yield to a greater extent than low pH [ 61 ]. While stabilizing mutations for IgG4 are known [ 62 ], IgG1 has significantly higher representation in marketed therapeutic antibodies; approximately 59% are IgG1 whereas IgG2 and IgG4 comprise 7% and 21%, respectively [ 63 ]. This may reflect a more straightforward manufacturing process and the favorable developability and functional profile of IgG1.…”
Section: Discussionmentioning
confidence: 99%
“…The scFv regions of KT112 (phage clone) were cloned in‐frame into an expression vector with a signal peptide and the human IgG4 Fc region (S228P/S235E/R409K) 17 . Immunoglobulin G4 (S228P/S235E/R409K) is a low‐effector‐activity Ab format that shows increased stability.…”
Section: Methodsmentioning
confidence: 99%
“…The scFv regions of KT112 (phage clone) were cloned in-frame into an expression vector with a signal peptide and the human IgG4 Fc region (S228P/S235E/R409K). 17 Immunoglobulin G4 (S228P/S235E/ R409K) is a low-effector-activity Ab format that shows increased stability. The V H and V L regions of KT112, AM1 (AbbVie), and DNP (negative control Ab) were each cloned in-frame into an expression vector with a signal peptide and human IgG4 constant region (S228P/S235E/ R409K).…”
Section: Construction and Expression Of Absmentioning
confidence: 99%