| Literature DB >> 32053170 |
Taisho Abe1, Riku Nagai1, Shunta Shimazaki1, Shunta Kondo1, Satoshi Nishimura1, Yuriko Sakaguchi2, Tsutomu Suzuki2, Hiroaki Imataka3, Kozo Tomita1, Nono Takeuchi-Tomita1.
Abstract
We have recently developed an in vitro yeast reconstituted translation system, which is capable of synthesizing long polypeptides. Utilizing the system, we examined the role of eIF5A and its hypusine modification in translating polyproline sequence within long open reading frames. We found that polyproline motif inserted at the internal position of the protein arrests translation exclusively at low Mg2+ concentrations, and peptidylpolyproline-tRNA intrinsically destabilizes 80S ribosomes. We demonstrate that unmodified eIF5A essentially resolves such ribosome stalling; however, the hypusine modification drastically stimulates ability of eIF5A to rescue polyproline-mediated ribosome stalling and is particularly important for the efficient translation of the N-terminal or long internal polyproline motifs.Entities:
Keywords: zzm321990 in vitro translation; eIF5A; hypusine; intrinsic ribosome destabilization; polyproline
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Year: 2020 PMID: 32053170 DOI: 10.1093/jb/mvaa022
Source DB: PubMed Journal: J Biochem ISSN: 0021-924X Impact factor: 3.387