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Molecular Biology - The process of inflammation is the body’s natural defense response to the penetration of foreign substances and molecules from the outside. Many proteins, signaling... 相似文献
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Rafal Archacki Daniel Buszewicz Tomasz J. Sarnowski Elzbieta Sarnowska Anna T. Rolicka Takayuki Tohge Alisdair R. Fernie Yusuke Jikumaru Maciej Kotlinski Roksana Iwanicka-Nowicka Katarzyna Kalisiak Jacek Patryn Joanna Halibart-Puzio Yuji Kamiya Seth J. Davis Marta K. Koblowska Andrzej Jerzmanowski 《PloS one》2013,8(3)
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Components of the Human SWI/SNF Complex Are Enriched in Active Chromatin and Are Associated with the Nuclear Matrix 总被引:26,自引:0,他引:26
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Biochemical and genetic evidence suggest that the SWI/SNF complex is involved in the remodeling of chromatin during gene activation. We have used antibodies specific against three human subunits of this complex to study its subnuclear localization, as well as its potential association with active chromatin and the nuclear skeleton. Immunofluorescence studies revealed a punctate nuclear labeling pattern that was excluded from the nucleoli and from regions of condensed chromatin. Dual labeling failed to reveal significant colocalization of BRG1 or hBRM proteins with RNA polymerase II or with nuclear speckles involved in splicing. Chromatin fractionation experiments showed that both soluble and insoluble active chromatin are enriched in the hSWI/SNF proteins as compared with bulk chromatin. hSWI/SNF proteins were also found to be associated with the nuclear matrix or nuclear scaffold, suggesting that a fraction of the hSWI/SNF complex could be involved in the chromatin organization properties associated with matrix attachment regions. 相似文献
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Sebastian P. Sacharowski Dominika M. Gratkowska Elzbieta A. Sarnowska Paulina Kondrak Iga Jancewicz Aimone Porri Ernest Bucior Anna T. Rolicka Rainer Franzen Justyna Kowalczyk Katarzyna Pawlikowska Bruno Huettel Stefano Torti Elmon Schmelzer George Coupland Andrzej Jerzmanowski Csaba Koncz Tomasz J. Sarnowski 《The Plant cell》2015,27(7):1889-1906
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Smith CL Horowitz-Scherer R Flanagan JF Woodcock CL Peterson CL 《Nature structural biology》2003,10(2):141-145
Elucidating the mechanism of ATP-dependent chromatin remodeling is one of the largest challenges in the field of gene regulation. One of the missing pieces in understanding this process is detailed structural information on the enzymes that catalyze the remodeling reactions. Here we use a combination of subunit radio-iodination and scanning transmission electron microscopy to determine the subunit stoichiometry and native molecular weight of the yeast SWI/SNF complex. We also report a three-dimensional reconstruction of yeast SWI/SNF derived from electron micrographs. 相似文献
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Zofall M Persinger J Kassabov SR Bartholomew B 《Nature structural & molecular biology》2006,13(4):339-346
Chromatin-remodeling complexes regulate access to nucleosomal DNA by mobilizing nucleosomes in an ATP-dependent manner. In this study, we find that chromatin remodeling by SWI/SNF and ISW2 involves DNA translocation inside nucleosomes two helical turns from the dyad axis at superhelical location-2. DNA translocation at this internal position does not require the propagation of a DNA twist from the site of translocation to the entry/exit sites for nucleosome movement. Nucleosomes are moved in 9- to 11- or approximately 50-base-pair increments by ISW2 or SWI/SNF, respectively, presumably through the formation of DNA loops on the nucleosome surface. Remodeling by ISW2 but not SWI/SNF requires DNA torsional strain near the site of translocation, which may work in conjunction with conformational changes of ISW2 to promote nucleosome movement on DNA. The difference in step size of nucleosome movement by SWI/SNF and ISW2 demonstrates how SWI/SNF may be more disruptive to nucleosome structure than ISW2. 相似文献
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