To induce cells to make proteins that they do not normally produce, it is possible to introduce
heterologous mRNA into the
cytoplasm of the cell, bypassing the need for transcription. In other words, a blueprint for foreign proteins is "smuggled" into the cells. To achieve this goal, however, one must bypass cellular systems that prevent the penetration and translation of foreign mRNA. There are nearly-ubiquitous
enzymes called
ribonucleases (also called RNAses) that break down unprotected mRNA. There are also intracellular barriers against foreign mRNA, such as
innate immune system receptors,
toll-like receptor (TLR) 7 and
TLR8, located in
endosomal membranes. RNA sensors like TLR7 and TLR8 can dramatically reduce protein synthesis in the cell, trigger release of
cytokines such as
interferon and
TNF-alpha, and when sufficiently intense lead to
programmed cell death. The inflammatory nature of exogenous RNA can be masked by modifying the nucleosides in mRNA. For example, uridine can be replaced with a similar nucleoside such as
pseudouridine (Ψ) or
N1-methyl-pseudouridine (m1Ψ), and
cytosine can be replaced by
5-methylcytosine. while m1Ψ occurs naturally in
archaea. Inclusion of these modified nucleosides alters the
secondary structure of the mRNA, which can reduce recognition by the innate immune system while still allowing effective translation. == Significance of untranslated regions ==