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XB-ART-37009
Mol Cell 2007 Dec 28;286:1029-44. doi: 10.1016/j.molcel.2007.10.010.
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A NASP (N1/N2)-related protein, Sim3, binds CENP-A and is required for its deposition at fission yeast centromeres.

Dunleavy EM , Pidoux AL , Monet M , Bonilla C , Richardson W , Hamilton GL , Ekwall K , McLaughlin PJ , Allshire RC .


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A defining feature of centromeres is the presence of the histone H3 variant CENP-A(Cnp1). It is not known how CENP-A(Cnp1) is specifically delivered to, and assembled into, centromeric chromatin. Through a screen for factors involved in kinetochore integrity in fission yeast, we identified Sim3. Sim3 is homologous to known histone binding proteins NASP(Human) and N1/N2(Xenopus) and aligns with Hif1(S. cerevisiae), defining the SHNi-TPR family. Sim3 is distributed throughout the nucleoplasm, yet it associates with CENP-A(Cnp1) and also binds H3. Cells defective in Sim3 function have reduced levels of CENP-A(Cnp1) at centromeres (and increased H3) and display chromosome segregation defects. Sim3 is required to allow newly synthesized CENP-A(Cnp1) to accumulate at centromeres in S and G2 phase-arrested cells in a replication-independent mechanism. We propose that one function of Sim3 is to act as an escort that hands off CENP-A(Cnp1) to chromatin assembly factors, allowing its incorporation into centromeric chromatin.

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Species referenced: Xenopus
Genes referenced: adh1 brsk2 cenpa fbp1 frzb2 fubp1 isyna1 myc nasp rasgrf1 septin7 tpr yes1


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References [+] :
Ahmad, The histone variant H3.3 marks active chromatin by replication-independent nucleosome assembly. 2002, Pubmed