Claude Reiss scite author profile

To investigate the possible influence of the local rates of translation on protein folding, 16 consecutive rare (in Escherichia coli) codons in the chloramphenicol acetyltransferase (CAT) gene have been replaced by frequent ones. Site-directed silent mutagenesis reduced the pauses in translation of CAT in E. coli S30 extract cell-free system and led to the acceleration of the overall rate of CAT protein synthesis. At the same time, the silently mutated protein (with unaltered protein sequence) synthesized in the E. coli S30 extract system was shown to possess 20% lower specific activity. The data suggest that kinetics of protein translation can affect the in vivo proteinfolding pathway, leading to increased levels of protein misfolding.z 1999 Federation of European Biochemical Societies.

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Silent mutations affect in vivo protein folding in Escherichia coli

Cortazzo

Červeñanský

Marı́n

et al. 2002

Biochemical and Biophysical Research Communications

162

112

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Simple models of non-linearDNA dynamics

et al. 1994

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Common features of polyomavirus mutants selected on PCC4 embryonal carcinoma cells.

Melin¹,

Pinon²,

Reiss

et al. 1985

The EMBO Journal

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The genomic rearrangements of six polyomavirus mutants selected on PCC4 embryonal carcinoma cells have been compared and their common characteristics pointed out. All mutants show a duplication which includes at least the adenovirus type 5 (Ad5) ElA-like enhancer core sequence plus a deletion of variable size and location. The presence of the second enhancer core sequence, the SV40-like enhancer, is not required for expression of the PyEC PCC4 phenotype. Two of these mutants are also able to express polyomavirus T antigen on F9 and LT1 cells. Multiadaptation seems to require the duplication of the Ad5 ElA-like core sequence, the maintenance of the SV40-like core sequence and a local change in DNA stability.

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Claude Reiss

Synonymous codon substitutions affect ribosome traffic and protein folding during in vitro translation

Silent mutations affect in vivo protein folding in Escherichia coli

Simple models of non-linearDNA dynamics

Common features of polyomavirus mutants selected on PCC4 embryonal carcinoma cells.

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