Single base-pair mutations in centromere element III cause aberrant chromosome segregation in Saccharomyces cerevisiae.

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Mol Cell Biol. 1986 February; 6(2): 530-538

Single base-pair mutations in centromere element III cause aberrant chromosome segregation in Saccharomyces cerevisiae.

J McGrew, B Diehl and M Fitzgerald-Hayes

ABSTRACT

In this paper we show that a 211-base pair segment of CEN3 DNAis sufficient to confer wild-type centromere function in theyeast Saccharomyces cerevisiae. We used site-directed mutagenesisof the 211-base pair fragment to examine the sequence-specificfunctional requirements of a conserved 11-base pair segmentof centromere DNA, element III (5'-TGATTTATCCGAA-3'). ElementIII is the most highly conserved of the centromeric DNA sequences,differing by only a single adenine X thymine base pair amongthe four centromere DNAs sequenced thus far. All of the elementIII sequences contain specific cytosine X guanine base pairs,including a 5'-CCG-3' arrangement, which we targeted for singlecytosine-to-thymine mutations by using sodium bisulfite. Theeffects of element III mutations on plasmid and chromosome segregationwere determined by mitotic stability assays. Conversion of CCGto CTG completely abolished centromere function both in plasmidsand in chromosome III, whereas conversion of CCG to TCG decreasedplasmid and chromosome stability moderately. The other two guanineX cytosine base pairs in element III could be independentlyconverted to adenine X thymine base pairs without affectingplasmid or chromosome stability. We concluded that while somespecific nucleotides within the conserved element III sequenceare essential for proper centromere function, other conservednucleotides can be changed.

Mol Cell Biol. 1986 February; 6(2): 530-538

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