Alterations in the adenine-plus-thymine-rich region of CEN3 affect centromere function in Saccharomyces cerevisiae.

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Mol Cell Biol. 1987 January; 7(1): 68-75

Alterations in the adenine-plus-thymine-rich region of CEN3 affect centromere function in Saccharomyces cerevisiae.

A Gaudet and M Fitzgerald-Hayes

ABSTRACT

Centromere DNA from 11 of the 16 chromosomes of the yeast Saccharomycescerevisiae have been analyzed and reveal three sequence elementscommon to each centromere, referred to as conserved centromereDNA elements (CDE). The adenine-plus-thymine (A + T)-rich centralcore element, CDE II, is flanked by two short conserved sequences,CDE I (8 base pairs [bp]) and CDE III (25 bp). Although no consensussequence exists among the different CDE II regions, they dohave three common features of sequence organization. First,the CDE II regions are similar in length, ranging from 78 to86 bp measured from CDE I to the left boundary of CDE III. Second,the base composition is always greater than 90% A + T. Finally,the A and T residues in these segments are often arranged inruns of A and runs of T residues, sometimes with six or sevenbases in a stretch. We constructed insertion, deletion, andreplacement mutations in the CDE II region of the centromerefrom chromosome III, CEN3, designed to investigate the lengthand sequence requirements for function of the CDE II regionof the centromere. We analyzed the effect of these altered centromereson plasmid and chromosome segregation in S. cerevisiae. Ourresults show that increasing the length of CDE II from 84 to154 bp causes a 100-fold increase in chromosome nondisjunction.Deletion mutations removing segments of the A + T-rich CDE IIDNA also cause aberrant segregation. In some cases partial functioncould be restored by replacing the deleted DNA with fragmentswhose primary sequence or base composition is very differentfrom that of the wild-type CDE II DNA. In addition, we foundthat identical mutations introduced into different positionsin CDE II have very similar effects.

Mol Cell Biol. 1987 January; 7(1): 68-75

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