Selenoprotein plays a crucial role in immune cells and
inflammatory
regulation. However, as a protein drug that is easily denatured or
degraded in the acidic environment of the stomach, efficient oral
delivery of selenoprotein is a great challenge. Herein, we innovated
an oral hydrogel microbeads-based biochemical strategy that can in
situ synthesize selenoproteins, therefore bypassing the necessity
and harsh conditions for oral protein delivery while effectively generating
selenoproteins for therapeutic applications. The hydrogel microbeads
were synthesized by coating hyaluronic acid-modified selenium nanoparticles
with a protective shell of calcium alginate (SA) hydrogel. We tested
this strategy in mice with inflammatory bowel disease (IBD), one of
the most representative diseases related to intestinal immunity and
microbiota. Our results revealed that hydrogel microbeads-mediated
in situ synthesis of selenoproteins could prominently reduce proinflammatory
cytokines secretion and mediate immune cells (e.g., reduce neutrophils
and monocytes and increase immune regulatory T cells) to effectively
relieve colitis-associated symptoms. This strategy was also able to
regulate gut microbiota composition (increase probiotics abundance
and suppress detrimental communities) to maintain intestinal homeostasis.
Considering intestinal immunity and microbiota widely associated with
cancers, infections, inflammations, etc., this in situ selenoprotein
synthesis strategy might also be possibly applied to broadly tackle
various diseases.
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