Protein synthesis, inhibitors

Puromycin, though not a direct inhibitor of peptid-yl-transferase, inhibits normal peptide chain elongation by participating in the peptidyl transferase reaction. 

---

Lactam Antibiotics Ribosomal Protein Synthesis Inhibitors... 

Ribosomal Protein Synthesis Inhibitors. Figure 3 The chemical structure of tetracycline and possible interactions with 16S rRNA in the primary binding site. Arrows with numbers indicate distances (in A) between functional groups. There are no interactions obseived between the upper portion of the molecule and 16S rRNA consistent with data that these positions can be modified without affecting inhibitory action (from Brodersen et al. [4] with copynght permission). 

Ribosomal Protein Synthesis Inhibitors. Figure 4 The binding site of pactamycin on the 30S subunit. The positions of mRNA, the RNA elements H28, H23b, H24a, and the C-terminus of protein S7 are depicted in the E-site of the native 30S structure (left) and in the 30S-pactamycin complex (right). In the complex with pactamycin, the position of mRNA is altered (from Brodersen etal. [4] with copyright permission). 

Ribosomal Protein Synthesis Inhibitors. Figure 5 Nucleotides at the binding sites of chloramphenicol, erythromycin and clindamycin at the peptidyl transferase center. The nucleotides that are within 4.4 A of the antibiotics chloramphenicol, erythromycin and clindamycin in 50S-antibiotic complexes are indicated with the letters C, E, and L, respectively, on the secondary structure of the peptidyl transferase loop region of 23S rRNA (the sequence shown is that of E. coll). The sites of drug resistance in one or more peptidyl transferase antibiotics due to base changes (solid circles) and lack of modification (solid square) are indicated. Nucleotides that display altered chemical reactivity in the presence of one or more peptidyl transferase antibiotics are boxed. 

Gautier That is what we would like to do. I mentioned that when you increase the dose of protein synthesis inhibitor or irradiation up to 200 Gy, the onset is not moved. One of the experiments to do is to attempt to deplete the maternal store of IAPs, to see whether the cells enter apoptosis more rapidly. 

Mishra, N.P., Mishra, R.K. and Singhal, C.S. (1993). Changes in the activities of antioxidant enzymes during exposure of intact wheat leaves to strong visible light at different temperatures in the presence of protein synthesis inhibitors. Plant Physiology 102 903-910. 

Protein synthesis inhibitors Chloramphenicol Tetracyclines Macrolides Lincosamides Aminoglycosides... 

Elevated metallothionein levels are not necessarily indicative of heavy-metal insult. Starcher et al. (1980) show that liver metallothionein levels in mice are elevated following acute stress or starvation, and that this effect is blocked by actinomycin D, a protein synthesis inhibitor. It is further emphasized that not all zinc-binding proteins are metallothioneins (Webb etal. 1985 ... 

IL-6 expression can be activated in neutrophils upon exposure to GM-CSF and TNF, whilst IL-3, G-CSF, y-interferon and lymphotoxin do not induce expression of this cytokine. Expression of IL-6 has been identified by analysis of mRNA levels and by protein analysis. Following GM-CSF exposure, expression is detectable by 2 h, maximal by 6 h and then returns to base-line levels. LPS, PMA (but not fMet-Leu-Phe) and cycloheximide also induce IL-6 transcripts. The finding that this protein-synthesis inhibitor increases mRNA levels suggests either that transcription is regulated by a short-lived repressor, or else that decay of its mRNA may be regulated by a short-lived RNase. 

Messenger RNA molecules for both subunits of the cytochrome and the two cytosolic components are detectable in unstimulated bloodstream cells. Experiments involving incubation of neutrophil suspensions with the protein synthesis inhibitor cycloheximide indicate that constitutive expression of one or more components of the oxidase is required for the neutrophil to maintain its ability to generate reactive oxidants. For example, when neutrophils are incubated in vitro with cycloheximide, their ability to generate reactive oxidants declines more rapidly than in control cells, as they age in culture (Fig. 7.12). This decline in oxidase activity when protein biosynthesis is blocked is not due to cell death, because cells treated with cycloheximide for this time still exclude trypan blue. Furthermore, when protein biosynthesis is stimulated in neutrophils by the addition of GM-CSF for 24 h in vitro, the ability to generate reactive oxidants is enhanced considerably above the levels observed in untreated cells. 

Mahadevan LC, Willis AC, Barratt MJ (1991) Rapid histone H3 phosphorylation in response to growth factors, phorbol esters, okadaic acid, protein synthesis inhibitors. Cell 65(5) 775—783... 

---