1998
DOI: 10.1016/s1074-7613(00)80610-x
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Intracellular Neutralization of HIV Transcytosis across Tight Epithelial Barriers by Anti-HIV Envelope Protein dIgA or IgM

Abstract: Human immunodeficiency virus, generated during contact between HIV-infected cells and the apical surface of an epithelial cell, can cross a tight epithelial barrier by transcytosis. We show that transcytosis of primary HIV isolates is blocked by dimeric IgA or IgM against HIV envelope proteins. Neutralization occurs intracellularly within the apical recycling endosome, and immune complexes are specifically recycled to the mucosal surface. One epitope involved in neutralization is a conserved sequence of the gp… Show more

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Cited by 284 publications
(236 citation statements)
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“…In addition to the conventional neutralization activity mentioned, human IgA Ab has also been shown to be able to act intracellularly to block HIV transcytosis from the apical to the basolateral side of epithelial cell monolayers, suggesting the potential to inhibit spread of HIV from mucosal epithelium to the lamina propria (16,24,33,35,36). The ability of IgA Ab to act in this manner has been referred to as "intracellular neutralization" (16).…”
Section: Discussionmentioning
confidence: 99%
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“…In addition to the conventional neutralization activity mentioned, human IgA Ab has also been shown to be able to act intracellularly to block HIV transcytosis from the apical to the basolateral side of epithelial cell monolayers, suggesting the potential to inhibit spread of HIV from mucosal epithelium to the lamina propria (16,24,33,35,36). The ability of IgA Ab to act in this manner has been referred to as "intracellular neutralization" (16).…”
Section: Discussionmentioning
confidence: 99%
“…Neutralizing Ab D47A (anti-gp120), stained green with FITC, was distributed through all three horizontal sections (apical and middle more than basal) with the most intensity in the middle section. As shown in the merged images, HIV gp160 and D47A IgA were prominently colocalized in the apical and especially the middle sections (orange to yellow), suggesting the principle site, perhaps in the apical recycling endosome (16,46), of interaction between IgA Ab and HIV protein. Both non-neutralizing D10A (anti-gp41) and irrelevant IgA (anti-measles hemagglutinin) showed no colocalization with HIV protein, suggesting little or no interaction with HIV protein even though both IgAs were transported efficiently to the apical side.…”
Section: Intracellular Colocalization Of Iga Ab and Viral Agmentioning
confidence: 92%
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“…The exact mechanism by which these mucosal CTL could function is not yet clear. HIV-1 can cross into the submucosa by transcytosis across a tight epithelial barrier, a process that can be inhibited by HIV-specific IgA (30). Furthermore, CD4 ϩ and CCR5 ϩ cell populations, which are susceptible to productive HIV-1 infection, are present in this region (31,32).…”
Section: Discussionmentioning
confidence: 99%