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Centromere localization and function of Mis18 requires Yippee‐like domain‐mediated oligomerization
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Abstract
Mis18 is a key regulator responsible for the centromere localization of the CENP‐A chaperone Scm3 in
Schizosaccharomyces pombe
and HJURP in humans, which establishes CENP‐A chromatin that defines centromeres. The molecular and structural determinants of Mis18 centromere targeting remain elusive. Here, by combining structural, biochemical, and yeast genetic studies, we show that the oligomerization of
S. pombe
Mis18, mediated via its conserved N‐terminal Yippee‐like domain, is crucial for its centromere localization and function. The crystal structure of the N‐terminal Yippee‐like domain reveals a fold containing a cradle‐shaped pocket that is implicated in protein/nucleic acid binding, which we show is required for Mis18 function. While the N‐terminal Yippee‐like domain forms a homodimer
in vitro
and
in vivo
, full‐length Mis18, including the C‐terminal α‐helical domain, forms a homotetramer
in vitro
. We also show that the Yippee‐like domains of human Mis18α/Mis18β interact to form a heterodimer, implying a conserved structural theme for Mis18 regulation.
Springer Science and Business Media LLC
Title: Centromere localization and function of Mis18 requires Yippee‐like domain‐mediated oligomerization
Description:
Abstract
Mis18 is a key regulator responsible for the centromere localization of the CENP‐A chaperone Scm3 in
Schizosaccharomyces pombe
and HJURP in humans, which establishes CENP‐A chromatin that defines centromeres.
The molecular and structural determinants of Mis18 centromere targeting remain elusive.
Here, by combining structural, biochemical, and yeast genetic studies, we show that the oligomerization of
S.
pombe
Mis18, mediated via its conserved N‐terminal Yippee‐like domain, is crucial for its centromere localization and function.
The crystal structure of the N‐terminal Yippee‐like domain reveals a fold containing a cradle‐shaped pocket that is implicated in protein/nucleic acid binding, which we show is required for Mis18 function.
While the N‐terminal Yippee‐like domain forms a homodimer
in vitro
and
in vivo
, full‐length Mis18, including the C‐terminal α‐helical domain, forms a homotetramer
in vitro
.
We also show that the Yippee‐like domains of human Mis18α/Mis18β interact to form a heterodimer, implying a conserved structural theme for Mis18 regulation.
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