Nucleic Acids Research, 2000, Vol. 28, No. 21 4068-4075
© 2000 Oxford University Press
Biochemical characterisation of cappoly(A) synergy in rabbit reticulocyte lysates: the eIF4GPABP interaction increases the functional affinity of eIF4E for the capped mRNA 5'-end
Unité de Génétique Moléculaire des Virus Respiratoires, CNRS URA 1966, Institut Pasteur, 25 Rue du Dr Roux, 75724 Paris Cedex 15, France
The 5' cap and 3' poly(A) tail of eukaryotic mRNAs cooperate to synergistically stimulate translation initiation in vivo. We recently described mammalian cytoplasmic extracts which, following ultracentrifugation to partially deplete them of ribosomes and associated initiation factors, reproduce cappoly(A) synergy in vitro. Using these systems, we demonstrate that synergy requires interaction between the poly(A)-binding protein (PABP) and the eukaryotic initiation factor (eIF) 4F holoenzyme complex, which recognises the 5' cap. Here we further characterise the requirements and constraints of cappoly(A) synergy in reticulocyte lysates by evaluating the effects of different parameters on synergy. The extent of extract depletion and the amounts of different initiation factors in depleted extracts were examined, as well as the effects of varying the concentrations of KCl, MgCl2 and programming mRNA and of adding a cap analogue. The results presented demonstrate that maximal cappoly(A) synergy requires: (i) limiting concentrations of ribosome-associated initiation factors; (ii) precise ratios of mRNA to translation machinery (low concentrations of ribosome-associated initiation factors and low, non-saturating mRNA concentrations); (iii) physiological concentrations of added KCl and MgCl2. Additionally, we show that the eIF4GPABP interaction on mRNAs which are capped and polyadenylated significantly increases the affinity of eIF4E for the 5' cap.
* To whom correspondence should be addressed. Tel: +33 1 40 61 33 55; Fax: +33 1 40 61 30 45; Email: kathiemb@pasteur.fr
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