INTRODUCTION: As in yeast, flies and mammals, over-expression of the Caenorhabditis elegans sirtuin gene
sir-2.1 leads to extension of lifespan and deletion of the gene shortens lifespan. The
sir-2.1 gene, however, is located in an operon, an organization not taken into account in previous studies of this gene's expression. MATERIALS AND METHODS: Recombineering allowed insertion of both a mCherry and a gfp reporter gene precisely at the end of the two protein-coding regions of the 4.5kb
sir-2.1 operon within a 29.3kb genomic DNA fosmid clone. RESULTS AND DISCUSSION: In C. elegans transgenic for this recombineered fosmid, with abundant food, the
sir-2.1::mCherry distribution indicated that
sir-2.1 is indeed expressed in the hypodermis and many nerve cells, as previously described, but also in the intestine and in muscles. This broader expression of
sir-2.1, which would fit with an expectation that SIR2.1 function in influencing lifespan might be required in most cell types, arises from transcription starting with the gene upstream of
sir-2.1 in the operon. Importantly, the expression of both genes in the operon increases upon starvation, this induction also depending on the operon promoter. Furthermore, SIR-2.1::mCherry undergoes a dynamic subcellular relocalization through starvation.