RT Journal Article
SR Electronic
T1 MiR-146a wild-type 3’ sequence identity is dispensable for proper innate immune function <em>in vivo</em>
JF bioRxiv
FD Cold Spring Harbor Laboratory
SP 474791
DO 10.1101/474791
A1 Grant Bertolet
A1 Natee Kongchan
A1 Rebekah Miller
A1 Ravi K. Patel
A1 Antrix Jain
A1 Jong Min Choi
A1 Alexander Saltzman
A1 Amber Christenson
A1 Sung Yun Jung
A1 Anna Malovannaya
A1 Andrew Grimson
A1 Joel R. Neilson
YR 2018
UL http://biorxiv.org/content/early/2018/11/20/474791.abstract
AB The prevailing model of microRNA function is that the “seed” region (nucleotides 2-8) is typically sufficient to mediate target recognition and repression. However, numerous recent studies have challenged this model, either by demonstrating extensive 3’ pairing between physically defined miRNA-mRNA pairs or by showing in C. elegans that disrupted 3’ pairing can result in impaired function in vivo. To test the importance of miRNA 3’ pairing in a mammalian system in vivo, we engineered a mutant murine mir-146a allele in which the 5’ half of the mature microRNA retains its wild-type sequence, but the 3’ half has been altered to be anti-complementary. Mice homozygous or hemizygous for this mutant allele are phenotypically indistinguishable from wild-type controls and do not recapitulate any of the immunopathology previously described for mir-146a-null mice. Our results indicate that 3’ pairing is dispensable for the established myeloid function of this key mammalian microRNA.Summary Blurb 3’ sequence identity is dispensable for the established function of a mammalian miRNA in vivo.