Although enzymes of nonhuman origin
have been studied for a variety
of therapeutic and diagnostic applications, their use has been limited
by the immune responses generated against them. The described dual-porosity
hollow nanoparticle platform obviates immune attack on nonhuman enzymes
paving the way to in vivo applications including enzyme-prodrug therapies
and enzymatic depletion of tumor nutrients. This platform is manufactured
with a versatile, scalable, and robust fabrication method. It efficiently
encapsulates macromolecular cargos filled through mesopores into a
hollow interior, shielding them from antibodies and proteases once
the mesopores are sealed with nanoporous material. The nanoporous
shell allows small molecule diffusion allowing interaction with the
large macromolecular payload in the hollow center. The approach has
been validated in vivo using l-asparaginase to achieve l-asparagine depletion in the presence of neutralizing antibodies.
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