Dual Binding Mode of the Nascent Polypeptide-associated Complex Reveals a Novel Universal Adapter Site on the Ribosome

Pech, Markus; Spreter, Thomas; Beckmann, Roland; Beatrix, Birgitta

doi:10.1074/jbc.m109.092536

Cited by 53 publications

(66 citation statements)

References 47 publications

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“…However, different models suggest that SRP function is influenced by NAC and that this dynamic interplay is important for protein targeting to the ER (Zhang et al, 2012). Also, NAC has been shown to bind uL23 (Wegrzyn et al, 2006), although other studies identified eL31 as the major ribosomal binding site of NAC (Pech et al, 2010; Zhang et al, 2012). Therefore, it would be interesting to see if and how NatA may be involved in this process and what the consequences are for the acetylation status of proteins.…”

Section: Nata In Other Organismsmentioning

confidence: 99%

The biological functions of Naa10 — From amino-terminal acetylation to human disease

Dörfel

Lyon

2015

Gene

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N-terminal acetylation (NTA) is one of the most abundant protein modifications known, and the N-terminal acetyltransferase (NAT) machinery is conserved throughout all Eukarya. Over the past 50 years, the function of NTA has begun to be slowly elucidated, and this includes the modulation of protein–protein interaction, protein-stability, protein function, and protein targeting to specific cellular compartments. Many of these functions have been studied in the context of Naa10/NatA; however, we are only starting to really understand the full complexity of this picture. Roughly, about 40% of all human proteins are substrates of Naa10 and the impact of this modification has only been studied for a few of them. Besides acting as a NAT in the NatA complex, recently other functions have been linked to Naa10, including post-translational NTA, lysine acetylation, and NAT/KAT-independent functions. Also, recent publications have linked mutations in Naa10 to various diseases, emphasizing the importance of Naa10 research in humans. The recent design and synthesis of the first bisubstrate inhibitors that potently and selectively inhibit the NatA/Naa10 complex, monomeric Naa10, and hNaa50 further increases the toolset to analyze Naa10 function.

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Section: Nata In Other Organismsmentioning

confidence: 99%

The biological functions of Naa10 — From amino-terminal acetylation to human disease

Dörfel

Lyon

2015

Gene

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“…The NAC is a heterodimeric complex that associates with ribosomes near the polypeptide exit tunnel. 31 Although the function of the NAC is poorly defined, it is thought to have roles in co-translational protein folding 32 and in protein targeting to mitochondria 33 and the endoplasmic reticulum. 34 The RAC consists of the Heat Shock Protein (Hsp) 70/40 pair Ssz1/ Zuo1, 35 which is anchored to the ribosome in close proximity to the polypeptide exit tunnel via a charged C-terminal region of Zuo1.…”

Section: Introductionmentioning

confidence: 99%

The ribosome-associated complex antagonizes prion formation in yeast

Amor

Castanzo

Delany

et al. 2015

Prion

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ABSTRACT. The number of known fungal proteins capable of switching between alternative stable conformations is steadily increasing, suggesting that a prion-like mechanism may be broadly utilized as a means to propagate altered cellular states. To gain insight into the mechanisms by which cells regulate prion formation and toxicity we examined the role of the yeast ribosome-associated complex (RAC) in modulating both the formation of the [PSI C ] prion -an alternative conformer of Sup35 protein -and the toxicity of aggregation-prone polypeptides. The Hsp40 RAC chaperone Zuo1 anchors the RAC to ribosomes and stimulates the ATPase activity of the Hsp70 chaperone Ssb. We found that cells lacking Zuo1 are sensitive to over-expression of some aggregation-prone proteins, including the Sup35 prion domain, suggesting that co-translational protein misfolding increases in Dzuo1 strains. Consistent with this finding, Dzuo1 cells exhibit higher frequencies of spontaneous and induced prion formation. Cells expressing mutant forms of Zuo1 lacking either a C-terminal charged region required for ribosome association, or the J-domain responsible for Ssb ATPase stimulation, exhibit similarly high frequencies of prion formation. Our findings are consistent with a role for the RAC in chaperoning nascent Sup35 to regulate folding of the N-terminal prion domain as it emerges from the ribosome.

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“…NAC transiently associates with the large ribosomal subunit close to the peptide tunnel exit and binds a broad spectrum of ribosome-nascent chain complexes (RNCs) ( 3). In vitro NAC association sterically prevents indiscriminate binding of RNCs to the ER membrane, regardless of whether the nascent chain has a signal sequence or not ( 4,5). Addition of SRP, however, specifically rescues ER targeting of signal-containing RNCs ( 6).…”

mentioning

confidence: 95%

“…Finally, Gamerdinger et ( 4), and that NAC binds translating ribosomes, unless an emerging signal sequence provides a selective binding advantage to SRP. Other in vitro data suggest that there is an alternative NAC ribosome binding site near eL31 ( 5,12), and that both NAC and SRP concomitantly bind the ribosome ( 12). SRP could quickly scan translating ribosomes irrespective of NAC presence, until an emerging signal sequence triggers strong SRP binding and NAC release.…”

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confidence: 97%

“…For example, during the cell division cycle, a large multiprotein E3 ligase, the anaphase-promoting complex/cyclosome (APC/C), utilizes two E2 enzymes, UBE2C and UBE2S, to target proteins for destruction ( 3). On pages 199 and 200 of this issue, two Research Articles by Lu et al focus on these reactions and illuminate, at the single-molecule level, the process of ubiquitination by APC/C ( 4), as well as the recognition and subsequent destruction of APC/C substrates by proteasomes ( 5). Both studies substantially enrich our knowledge of ubiquitination and degradation, reveal new properties of APC/C and the proteasome, and challenge established concepts about the ubiquitin-proteasome system.…”

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confidence: 98%

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