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Condensation of DNA and Chromatin by an SPKK-Containing Octapeptide Repeat Motif Present in the C-Terminus of Histone H1

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dc.contributor.author Khadake, Jyoti R
dc.contributor.author Rao, M R S
dc.date.accessioned 2012-03-06T11:21:37Z
dc.date.available 2012-03-06T11:21:37Z
dc.date.issued 1997-02-04
dc.identifier 0006-2960 en_US
dc.identifier.citation Biochemistry 36(5), 1041-1051 (1997) en_US
dc.identifier.uri https://libjncir.jncasr.ac.in/xmlui/10572/570
dc.description Restricted Access en_US
dc.description.abstract Several DNA binding motifs have been described in the C-terminus of histone H1 (Churchill & Travers, 1991), of these the S/TPKK repeat (Suzuki, 1989) often occurs as a part of an octapeptide repeat of the type XTPKKXKK. We have studied in detail the DNA and chromatin condensing properties of a consensus octapeptide KSPKKAKK (8 mer) present in many histone H1 subtypes and its imperfect repeat ATPKKSTKKTPKKAKK (16 mer TPKK) as it occurs in the C-tenminus of rat histone Hid. The 16 mer TPKK peptide containing two S/TPKK motifs was able to condense both rat oligonucleosomal (2-5 kbp) DNA and histone Hi-depleted chromatin as revealed by circular dichroism spectroscopy. The 8 mer peptide, however, was unable to condense either the DNA or the histone Hi-depleted chromatin. Both the 8 mer peptide and the 16 mer TPKK peptide displaced distamycin A from the drug-DNA complex, although with different efficiency, indicating that while these two peptides could bind DNA, only the 16 mer (TPKK) peptide could brine about condensation of DNA and histone Hi-depleted chromatin. A mutant 16 mer (TAKK) peptide wherein two proline residues are replaced by alanine, was ineffective in bringing about condensation of both DNA and histone Hi-depleted chromatin. These results suggest that the two p-turn structures present in the 16 mer (TPKK) peptide could be important in facilitating binding to different regions of duplex DNA thereby bringing about close packing and condensation. The condensation property of the 16 mer (TPKK) peptide was very similar to that of histone H1 in terms of (a) its preference for AT rich DNA, (b) cooperativity of condensation, and (c) salt dependence of condensation. The 16 mer (TPKK) peptide, but not the 8 mer peptide or the 16 mer (TAKK) peptide, could form complexes with a polynucleosomal 5S DNA core resulting in retarded mobility similar to the complexes formed with histone H1 on agarose gel electrophoresis. en_US
dc.description.uri http://dx.doi.org/10.1021/bi961617p en_US
dc.language.iso en en_US
dc.publisher American Chemical Society en_US
dc.rights © 1997 American Chemical Society en_US
dc.subject Higher-Order Structure en_US
dc.subject Agarose-Gel Electrophoresis en_US
dc.subject Circular-Dichroism en_US
dc.subject Linker-Length en_US
dc.subject Minor-Groove en_US
dc.subject Beta-Turns en_US
dc.subject H-1 en_US
dc.subject Binding en_US
dc.subject Fragments en_US
dc.subject Domain en_US
dc.title Condensation of DNA and Chromatin by an SPKK-Containing Octapeptide Repeat Motif Present in the C-Terminus of Histone H1 en_US
dc.type Article en_US


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