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Ribosome-Mediated Specificity in Hox mRNA Translation and Vertebrate Tissue Patterning
Author(s) -
Nadya Kondrashov,
Aya D. Pusic,
Craig R. Stumpf,
Kunihiko Shimizu,
Andrew C. Hsieh,
Shifeng Xue,
Junko Ishijima,
Toshihiko Shiroishi,
Maria Barna
Publication year - 2011
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2011.03.028
Subject(s) - biology , translation (biology) , ribosome , genetics , hox gene , microbiology and biotechnology , homeobox , messenger rna , homeotic gene , ribosomal protein , protein biosynthesis , gene expression , gene , rna
Historically, the ribosome has been viewed as a complex ribozyme with constitutive rather than regulatory capacity in mRNA translation. Here we identify mutations of the Ribosomal Protein L38 (Rpl38) gene in mice exhibiting surprising tissue-specific patterning defects, including pronounced homeotic transformations of the axial skeleton. In Rpl38 mutant embryos, global protein synthesis is unchanged; however the translation of a select subset of Homeobox mRNAs is perturbed. Our data reveal that RPL38 facilitates 80S complex formation on these mRNAs as a regulatory component of the ribosome to confer transcript-specific translational control. We further show that Rpl38 expression is markedly enriched in regions of the embryo where loss-of-function phenotypes occur. Unexpectedly, a ribosomal protein (RP) expression screen reveals dynamic regulation of individual RPs within the vertebrate embryo. Collectively, these findings suggest that RP activity may be highly regulated to impart a new layer of specificity in the control of gene expression and mammalian development.

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