Library

Notes: Abstract The 20S proteasome (prosome) is a highly organized multiprotein complex with approximate molecular weight of about 700 kDa. Whilst the role of the proteasome in the processing and turnover of cellular proteins is becoming clearer, its relationship with RNA remains still obscure. Here we focus on the nature and function of proteasome associated endonuclease activity. Thus the involvement of a proteasome α-type subunit in RNA-degradation, the catalytic requirements, the interaction of proteasomes with their RNA-substrate and the identification of a well defined cleavage site in the 3-UTR of short-lived cellular mRNAs will be described in detail. All data indicate that proteasomes associated endonuclease activity could be involved in post-transcriptional gene control at the level of translation. Abbreviations: Hu – human; Mu – murine; β IFN – fibroblast interferon; γ IFN – lymphoblast interferon; c FOS – fos proto-oncogene; G-CSF – granulocyte colony stimulating factor.

Notes: Abstract The 20S proteasome (prosome) is a highly organized multi-protein complex with approximate molecular weight of about 700 kDa. Whilst the role of the proteasome in the processing and turnover of cellular proteins is becoming clearer, its relationship with RNA remains obscure. Over the last decade the possibility of association of proteasomes with specific RNAs or mRNPs have been particularly controversial. Proteasomes were reported to inhibit translation of viral mRNAs and to be tightly associated with RNase activity. It is possible that proteasomes are also involved in cellular RNA breakdown and RNA processing like prokaryotic RNase E.

Notes: Abstract Proteasomes (prosomes) are large multiprotein complexes. They are involved in protein degradation of ubiquitin-conjugated proteins and in the generation of MHC class I peptides. We gave further evidence that they interfere within vitro protein synthesis. Proteasomes inhibit the translation of Tobacco mosaic virus RNA. Analysis of cell-free systems by sucrose gradient centrifugation revealted that they prevent the formation of 80S initiation complexes but not the early phase of initiation.

Notes: In der vorliegenden Arbeit werden zunächst die in der Literatur auftretenden Widersprü:che über das Kalium-Rhenium(1V)-Chlorid geklärt.

Notes: Transcyclopropanation during the Tetrabromination of a Tricyclic Ketone to 3 exo, 4 endo, 6exo-Tribromo-7-bromomethyl-1,5-dimethyl-tricyclo[3.2.1.02,7]octan-8-oneBromination of the tricyclic ketone 1 with an excess of bromine at low temperature gives in approximately 30% yield the highly crystalline tricyclic tetrabromide 2 (Scheme 1). The structure of 2 was established by NMR.- and especially X-ray-analysis (Fig.1).Treatment of 1 with 1 mol-equ. of bromine gives an unstable dibromide, to which the structure 3 was assigned on the basis of its NMR.-spectrum and its further bromination to 2 (Scheme 1). In the course of the tetrabromination of 1 the original cyclopropane ring is opened in the first step (1 → 3) and another cyclopropane ring is formed in the second step (3 → 2) (cf. Scheme 3).

Notes: Photochemical Generation and Reactions of Benzonitrile-benzylideThe low temperature irradiation of 2,3-diphenyl-2H-azirine (1) in DMBP-glass at -196° has been reinvestigated. It was possible to convert 1 nearly quantitatively into the dipolar species benzonitrile-benzylide (3, Φ3 = 0,78), which exhibits UV.-absorptions at 344 (∊ = 48000) and 244 nm (∊ = 28500) (Fig. 1, Tab. 1). Irradiation of 3 with 345 nm light at -196° resulted in almost complete reconversion to the azirine 1 (Φ = 0,15; Fig. 2). When the solution of 3 in the DMBP-glass was warmed up to about -160° a quantitative dimerization to 1,3,4, 6-tetraphenyl-2,5-diaza-1,3,5-hexatriene (8) occurred. This proves that 8 is not only formed by the indirect route 3 + 1 → 7 \documentclass{article}\pagestyle{empty}\begin{document}$ \mathop {\longrightarrow }\limits^{hv} $\end{document} 11 → 8 known before (Scheme 1), but also by dimerization of 3 either by direct head to head coupling or via the intermediate e (p. 2675), followed by a fast thermal hydrogen transfer reaction.The occurrence of the dipolar intermediate 11 in the photochemical conversion of the bicyclic compound 7 to 8 could also be demonstrated by low temperature experiments: On irradiation at -196° 7 gave the cherry red dipolar intermediate 11 (λmax = 520 nm), which at -120° isomerizes to 8. It should be noted, that neither 7 nor 11 are formed by dimerization reactions of 3.Experiments carried out at room temperature demonstrate, that both processes for the formation of 8 may compete: Irradiation of a solution of 1 (DMBP, c = 8 × 10-4 to 5 × 10-3M) with 350 nm light of high intensity (which does not excite the bicyclic compound 7) leads to a relative high photostationary concentration of the dipolar species 3. Under these conditions the formation of 8 is due to dimerization of 3 (Φ8 = 0,19). With low light intensity only a very low stationary concentration of 3 can be obtained. Therefore the reaction of 3 with 1, leading to the bicyclic intermediate 7, becomes now predominant (Φ-1 = 1,55, which corresponds with the expected value of 2 × 0,8). Irradiation of 1 at -130° with 350 nm light of high intensity gives 8 with a quantum yield of 0,44. This is in agreement with the theoretical value Φ8 = 0,4 for an exclusive formation of 8 by dimerization of 3. The lower quantum yield for the formation of 8 at room temperature makes probable that under these conditions 3 not only dimerizes to 8, but also to another, so far unidentified dimer, e.g. 2,3,5,6-Tetraphenyl-2,5-dihydropyrazine.By flash photolysis of a solution of 1 (cyclohexane, c = 10-4M, 25°) the disappearance of 3 could directly be measured by UV.-spectroscopy: At relative high concentrations (c ≥ 10-7M) 3 disappeared according to a second order reaction with the rate constant k = 5 × 107M-1S-1. At lower concentrations (c ≤ 10-7M) the rate of disappearance of 3 follows first order kinetics. The rate constant of this pseudo first order reaction (3 + 1 → 7) has been determined to be 1 → 104M-1S-1.Using Padwa's table of relative rates for the cycloaddition of the dipolar species 3 to various dipolarophiles, including the azirine 1, an absolute rate constant of k ≈ 8 × 108M-1S-1 for the addition of 3 to the most active dipolarophile fumaronitrile could be estimated. In cyclohexane at room temperature, the diffusion controlled rate constant equals 6,6 × 109M-1S-1.In Table 1 the UV.-maxima of several nitrile-ylides, among them a purely aliphatic one, are given.

Notes: 3-Alkyl-1-benzoxepin-5-one derivatives and 2-alkyl-1,4-naphtoquinones from 2-acylaryl propargyl ethers.It was found that 3-alkyl-1-benzoxepin-5(2H)-ones of type B can be synthesized by treating 2-acylaryl propargyl ethers of type A with sodium methylsulfinyl methide (NaMSM, dimesyl sodium) (Scheme 13). Oxepinone derivatives of type B undergo ring contraction with base (also NaMSM) to yield the quinol derivatives C which, oxidize (during work-up), if R2 = H, to the 1,4-naphthoquinones D (Scheme 13).The propargyl ethers used are listed in Scheme 1. The naphthalene derivatives 1 and 3 give oxepinones (E-9 and a mixture of 14/15 respectively), whereas the expected oxepinone from 2 is transformed directly into the quinone 11 (Scheme 2, 3 and 5). Isomerizations of 2-acetylphenyl propargyl ethers (4, 5 and 6) (Schemes 6, 7 and 8) are less successful because of side reactions. If however the acetyl group is replaced by a propionyl or substituted propionyl group (as in ethers 7 and 8) oxepinones are obtained again in good yield (Scheme 9).The mechanistic pathway for the transformation of naphthyl propargyl ethers (and phenyl derivatives) under influence of NaMSM is shown in Scheme 10. The base-catalysed conversion of 4-phenyl-l-benzoxepin-5(2H)-one,benzo[f]furo[2,3-c](10 H)-oxepin-4-oncsand 3-methoxy-G,11- dihydro-dibenzo[b, e]loxepin-11-oneinto thc corresponding quinones has been reported [13] [20] [21].The conversion of 2-acylaryl propargyl others via the isolable benzoxepin-5-one derivativcs or directly into the specifically substituted 1,4-naphthoquinone derivatives is of synthetic interest.