Journal
JOURNAL OF IMMUNOLOGY
Volume 175, Issue 4, Pages 2331-2339Publisher
AMER ASSOC IMMUNOLOGISTS
DOI: 10.4049/jimmunol.175.4.2331
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- NCI NIH HHS [CA88053] Funding Source: Medline
- NICHD NIH HHS [HD38764] Funding Source: Medline
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Placental transfer of IgG from maternal circulation to that of the fetus is crucial for fetal and newborn immunity. This process requires that IgG broach two cellular layers of the placenta. IgG transport across the first layer, the syncytiotrophoblast, is almost certainly mediated by the MHC-related FcR for IgG, FcRn. The second layer, the villus endothelium, was until recently thought to allow IgG movement nonspecifically by constitutive transcytosis in caveolae. However, we recently showed that villus endothelium expressed a separate FcR for IgG, the inhibitory motif-bearing Fc gamma RIIb2 seen most notably on macrophages and as a minor fraction of the Fc gamma RIIb expressed on B cells. Now, by quantitative microscopy, we find Fc gamma RIIb2 to be expressed abundantly in an unidentifiable and likely novel organelle of the villus endothelium, unassociated with caveolae. About half of these Fc gamma RIIb2 organelles contain IgG; the remainder lack IgG. The majority fraction (similar to 80%) of IgG-containing organelles is associated with Fc gamma RIIb. No IgG-containing organelles are associated with caveolin. These findings are compatible with Fc gamma RIIb-mediated transfer of IgG across the villus endothelium, independent of caveolae.
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