IgG trafficking in the adult pig small intestine: one- or bidirectional transfer across the enterocyte brush border?

Möller, Rebecca; Hansen, Gert H.; Danielsen, E. Michael

doi:10.1007/s00418-016-1492-x

Cited by 2 publications

(3 citation statements)

References 50 publications

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“…In the neonate, FcRn allows the ingested maternal IgG to be taken up from the gut lumen into the blood (see above, passive immunity). In the adult, the IgG produced in the intestinal Peyer’s patches uses this route to be released to the gut lumen as part of the mucosal defense [ 20 , 23 ]. After “gut closure”, milk polymeric IgA and IgM use the pIgR (polymeric immunoglobulin receptor) to cross the epithelial cells and reach the blood stream, or may stay in the gut lumen for surveillance.…”

Section: Maternal Antibodies and Leukocytes In The Suckling Infantmentioning

confidence: 99%

Maternal Vaccination. Immunization of Sows during Pregnancy against ETEC Infections

et al. 2017

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The immunology of pregnancy is an evolving consequence of multiple reciprocal interactions between the maternal and the fetal-placental systems. The immune response must warrant the pregnancy outcome (including tolerance to paternal antigens), but at the same time, efficiently respond to pathogenic challenges. Enterotoxigenic Escherichia coli (ETEC) strains are a major cause of illness and death in neonatal and recently weaned pigs. This review aims to give an overview of the current rationale on the maternal vaccination strategies for the protection of the newborn pig against ETEC. Newborn piglets are immunodeficient and naturally dependent on the maternal immunity transferred by colostrum for protection—a maternal immunity that can be obtained by vaccinating the sow during pregnancy. Our current knowledge of the interactions between the pathogen strategies, virulence factors, and the host immune system is aiding the better design of vaccination strategies in this particular and challenging host status. Challenges include the need for better induction of immunity at the mucosal level with the appropriate use of adjuvants, able to induce the most appropriate and long-lasting protective immune response. These include nanoparticle-based adjuvants for oral immunization. Experiences can be extrapolated to other species, including humans.

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Section: Maternal Antibodies and Leukocytes In The Suckling Infantmentioning

confidence: 99%

Maternal Vaccination. Immunization of Sows during Pregnancy against ETEC Infections

et al. 2017

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“…When IgG or albumin is taken up by polarized epithelial or endothelial cells, they are packaged into endosomes, which acidify as they traffic through the cell. 15 In this low-pH environment, histidines on albumin and the IgG Fc domain are protonated and binding to FcRn and its cognate light-chain β2 microglobulin (β2m) is enabled. 16 Association of β2m with FcRn is required for binding with IgG and albumin.…”

Section: ■ Introductionmentioning

confidence: 99%

“…In addition to mediating immune effector functions such as recruiting humoral and cellular responses, the Fc domain is also responsible for extending the serum half-life of antibodies via engagement with the neonatal Fc receptor (FcRn), promoting recycling rather than degradation of these long-lived serum proteins (Figure A). , FcRn also binds albumin in a similar way (but at an orthogonal binding site) (Figure B). When IgG or albumin is taken up by polarized epithelial or endothelial cells, they are packaged into endosomes, which acidify as they traffic through the cell . In this low-pH environment, histidines on albumin and the IgG Fc domain are protonated and binding to FcRn and its cognate light-chain β2 microglobulin (β2m) is enabled .…”

Section: Introductionmentioning

confidence: 99%

Short FcRn-Binding Peptides Enable Salvage and Transcytosis of scFv Antibody Fragments

Kelly

Sirk

2022

ACS Chem. Biol.

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Therapeutic antibodies have become one of the most widely used classes of biotherapeutics due to their unique antigen specificity and their ability to be engineered against diverse disease targets. There is significant interest in utilizing truncated antibody fragments as therapeutics, as their small size affords favorable properties such as increased tumor penetration as well as the ability to utilize lowercost prokaryotic production methods. Their small size and simple architecture, however, also lead to rapid blood clearance, limiting the efficacy of these potentially powerful therapeutics. A common approach to circumvent these limitations is to enable engagement with the half-life extending neonatal Fc receptor (FcRn). This is usually achieved via fusion with a large Fc domain, which negates the benefits of the antibody fragment's small size. In this work, we show that modifying antibody fragments with short FcRn-binding peptide domains that mimic native IgG engagement with FcRn enables binding and FcRn-mediated recycling and transmembrane transcytosis in cell-based assays. Further, we show that rational, single amino acid mutations to the peptide sequence have a significant impact on the receptor-mediated function and investigate the underlying structural basis for this effect using computational modeling. Finally, we report the identification of a short peptide from human serum albumin that enables FcRnmediated function when grafted onto a single-chain variable fragment (scFv) scaffold, establishing an approach for the rational selection of short-peptide domains from full-length proteins that could enable the transfer of non-native functions to small recombinant proteins without significantly impacting their size or structure.

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IgG trafficking in the adult pig small intestine: one- or bidirectional transfer across the enterocyte brush border?

Cited by 2 publications

References 50 publications

Maternal Vaccination. Immunization of Sows during Pregnancy against ETEC Infections

Maternal Vaccination. Immunization of Sows during Pregnancy against ETEC Infections

Short FcRn-Binding Peptides Enable Salvage and Transcytosis of scFv Antibody Fragments

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