Importance of introns for expression of mouse ribosomal protein gene rpL32.

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Mol Cell Biol. 1989 May; 9(5): 2075-2082

Importance of introns for expression of mouse ribosomal protein gene rpL32.

S Chung and R P Perry

Institute for Cancer Research, Fox Chase Cancer Center, Philadelphia, Pennsylvania 19111.

ABSTRACT

The importance of intronic sequences for expression of the mouseribosomal protein gene rpL32 was evaluated by transfection experimentswith a series of mutant constructs in which one or more of thethree rpL32 introns was totally or partially deleted. When transientlytransfected into monkey kidney (COS) cells or stably transfectedinto mouse L cells, a mutant that lacked all three introns wascompletely inactive. Constructs that contained intron 1, eitheralone or in combination with another intron, were expressedas efficiently as was the normal intact rpL32 gene. Constructsthat lacked intron 1 but contained another spliceable intron,even one from a foreign gene, were expressed at about 10 to20% of the maximum level. These results indicated that intron1 contains an element that increases the level of expressionby 5- to 10-fold. A comparison of internal deletion mutantslocalized the element to within the first 27 base pairs of intron1. Nuclear run-on experiments with stably transfected COS cellsdemonstrated that this element functions at the transcriptionallevel. The element was inactive when translocated to a positionupstream of the transcriptional start site or to a positionwithin intron 3, which indicated that it does not have the propertiesof a typical enhancer. From these and other results, we concludethat introns have both a general and a specific role in rpL32expression. The general role, which can be satisfied by anyspliceable intron, is to ensure an efficient yield of RNA transcripts.The specific role is uniquely attributable to intron 1, whichcontains a transcriptional regulatory element near its 5' end.

Mol Cell Biol. 1989 May; 9(5): 2075-2082

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