AI Article Synopsis

  • IgG glycosylation is crucial for immune system function, but factors influencing its variability among individuals are not fully understood.
  • A study of 95 strains of mice revealed that the genetic variation in IgG glycosylation among mouse strains exceeded that of humans, with five genetic loci linked to this variation.
  • The research also found that certain glycosylation patterns, typically not seen in lab mice, suggest that common mouse strains may not be the best models for investigating the role of glycosylation on IgG function.

Article Abstract

Immunoglobulin G (IgG) glycosylation is essential for function of the immune system, but the genetic and environmental factors that underlie its inter-individual variability are not well defined. The Collaborative Cross (CC) genetic resource harnesses over 90% of the common genetic variation of the mouse. By analyzing the IgG glycome composition of 95 CC strains, we made several important observations: (i) glycome variation between mouse strains was higher than between individual humans, despite all mice having the same environmental influences; (ii) five genetic loci were found to be associated with murine IgG glycosylation; (iii) variants outside traditional glycosylation site motifs affected glycome variation; (iv) bisecting N-acetylglucosamine (GlcNAc) was produced by several strains although most previous studies have reported the absence of glycans containing the bisecting GlcNAc on murine IgGs; and (v) common laboratory mouse strains are not optimal animal models for studying effects of glycosylation on IgG function.

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Source
http://dx.doi.org/10.1038/s41589-018-0034-3DOI Listing

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