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1. Chp1 is a dedicated chaperone at the ribosome that safeguards eEF1A biogenesis

2. Balanced activities of Hsp70 and the ubiquitin proteasome system underlie cellular protein homeostasis

3. DENR promotes translation reinitiation via ribosome recycling to drive expression of oncogenes including ATF4

4. Cellular sequestrases maintain basal Hsp70 capacity ensuring balanced proteostasis

5. Chaperone-Mediated Protein Disaggregation Triggers Proteolytic Clearance of Intra-nuclear Protein Inclusions

6. Hormesis enables cells to handle accumulating toxic metabolites during increased energy flux

7. Small heat shock proteins sequester misfolding proteins in near-native conformation for cellular protection and efficient refolding

8. Two-Step Activation Mechanism of the ClpB Disaggregase for Sequential Substrate Threading by the Main ATPase Motor

9. The C-terminal tail of the bacterial translocation ATPase SecA modulates its activity

10. Accurate prediction of cellular co-translational folding indicates proteins can switch from post- to co-translational folding

11. Regulatory coiled-coil domains promote head-to-head assemblies of AAA+ chaperones essential for tunable activity control

12. Evolution of an intricate J-protein network driving protein disaggregation in eukaryotes

13. The Rqc2/Tae2 subunit of the ribosome-associated quality control (RQC) complex marks ribosome-stalled nascent polypeptide chains for aggregation

14. Head-to-tail interactions of the coiled-coil domains regulate ClpB activity and cooperation with Hsp70 in protein disaggregation

15. Monitoring protein misfolding by site-specific labeling of proteins in vivo.

16. Functional analysis of Hsp70 inhibitors.

18. Hsp110 chaperones regulate prion formation and propagation in S. cerevisiae by two discrete activities.

22. Ko-translationale Assemblierung von Proteinkomplexen

24. Translational Activity Controls Ribophagic Flux and Turnover of Distinct Ribosome Pools

25. Molecular dissection of amyloid disaggregation by human HSP70

26. The cytoprotective sequestration activity of small heat shock proteins is evolutionarily conserved

28. DENR promotes translation reinitiation via ribosome recycling to drive expression of oncogenes including ATF4

29. Processive extrusion of polypeptide loops by a Hsp100 disaggregase

30. Cellular sequestrases maintain basal Hsp70 capacity ensuring balanced proteostasis

31. Combinations of slow-translating codon clusters can increase mRNA half-life in

32. Cooperative Amyloid Fibre Binding and Disassembly by the Hsp70 disaggregase

33. The Hsp70 chaperone network

34. Interactions between nascent proteins translated by adjacent ribosomes drive homomer assembly

36. Pairs of amino acids at the P- and A-sites of the ribosome predictably and causally modulate translation-elongation rates

37. The Diverse Functions of Small Heat Shock Proteins in the Proteostasis Network

38. Chaperone-Mediated Protein Disaggregation Triggers Proteolytic Clearance of Intra-nuclear Protein Inclusions

39. Disassembly of Tau fibrils by the human Hsp70 disaggregation machinery generates small seeding-competent species

40. Disassembly of Tau fibrils by the human Hsp70 disaggregation machinery generates small seeding-competent species

41. N

42. Translational regulation of Pmt1 and Pmt2 by Bfr1 affects unfolded protein O-mannosylation

43. Nα-terminal acetylation of proteins by NatA and NatB serves distinct physiological roles in Saccharomyces cerevisiae

44. The HSP110/HSP70 disaggregation system generates spreading-competent toxic α-synuclein species

45. Selective 40S footprinting reveals that scanning ribosomes remain cap-tethered in human cells

46. HSP110 dependent HSP70 disaggregation machinery mediates prion-like propagation of amyloidogenic proteins in metazoa

47. Protein Disaggregation in Multicellular Organisms

48. A prion-like domain in Hsp42 drives chaperone-facilitated aggregation of misfolded proteins

49. Cellular Handling of Protein Aggregates by Disaggregation Machines

50. Hormesis enables cells to handle accumulating toxic metabolites during increased energy flux

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