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6T59

Structure of rabbit 80S ribosome translating beta-tubulin in complex with tetratricopeptide protein 5 and nascent chain-associated complex

This is a non-PDB format compatible entry.
Summary for 6T59
Entry DOI10.2210/pdb6t59/pdb
EMDB information10380
DescriptorRibosomal protein L8, Ribosomal protein L11, eL13, ... (55 entities in total)
Functional Keywordstubulin, nascent chain-associated complex, ribosome-nascent chain, tetratricopeptide protein 5, autoregulation, ribosome
Biological sourceHomo sapiens (Human)
More
Total number of polymer chains53
Total formula weight2262178.98
Authors
Lin, Z.,Gasic, I.,Chandrasekaran, V.,Peters, N.,Shao, S.,Ramakrishnan, V.,Mitchison, T.J.,Hegde, R.S. (deposition date: 2019-10-15, release date: 2019-11-27, Last modification date: 2020-01-15)
Primary citationLin, Z.,Gasic, I.,Chandrasekaran, V.,Peters, N.,Shao, S.,Mitchison, T.J.,Hegde, R.S.
TTC5 mediates autoregulation of tubulin via mRNA degradation.
Science, 367:100-104, 2020
Cited by
PubMed Abstract: Tubulins play crucial roles in cell division, intracellular traffic, and cell shape. Tubulin concentration is autoregulated by feedback control of messenger RNA (mRNA) degradation via an unknown mechanism. We identified tetratricopeptide protein 5 (TTC5) as a tubulin-specific ribosome-associating factor that triggers cotranslational degradation of tubulin mRNAs in response to excess soluble tubulin. Structural analysis revealed that TTC5 binds near the ribosome exit tunnel and engages the amino terminus of nascent tubulins. TTC5 mutants incapable of ribosome or nascent tubulin interaction abolished tubulin autoregulation and showed chromosome segregation defects during mitosis. Our findings show how a subset of mRNAs can be targeted for coordinated degradation by a specificity factor that recognizes the nascent polypeptides they encode.
PubMed: 31727855
DOI: 10.1126/science.aaz4352
PDB entries with the same primary citation
Experimental method
ELECTRON MICROSCOPY (3.11 Å)
Structure validation

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