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Dive into the research topics where Kazimierz Grzeskowiak is active.

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Featured researches published by Kazimierz Grzeskowiak.


Journal of Molecular Biology | 1987

Binding of Hoechst 33258 to the minor groove of B-DNA.

Philip Pjura; Kazimierz Grzeskowiak; Richard E. Dickerson

An X-ray crystallographic structure analysis has been carried out on the complex between the antibiotic and DNA fluorochrome Hoechst 33258 and a synthetic B-DNA dodecamer of sequence C-G-C-G-A-A-T-T-C-G-C-G. The drug molecule, which can be schematized as: phenol-benzimidazole-benzimidazole-piperazine, sits within the minor groove in the A-T-T-C region of the DNA double helix, displacing the spine of hydration that is found in drug-free DNA. The NH groups of the benzimidazoles make bridging three-center hydrogen bonds between adenine N-3 and thymine O-2 atoms on the edges of base-pairs, in a manner both mimicking the spine of hydration and calling to mind the binding of the auti-tumor drug netropsin. Two conformers of Hoechst are seen in roughly equal populations, related by 180 degrees rotation about the central benzimidazole-benzimidazole bond: one form in which the piperazine ring extends out from the surface of the double helix, and another in which it is buried deep within the minor groove. Steric clash between the drug and DNA dictates that the phenol-benzimidazole-benzimidazole portion of Hoechst 33258 binds only to A.T regions of DNA, whereas the piperazine ring demands the wider groove characteristic of G.C regions. Hence, the piperazine ring suggests a possible G.C-reading element for synthetic DNA sequence-reading drug analogs.


Journal of Molecular Biology | 1992

Structure of a B-DNA decamer with a central T-A step: C-G-A-T-T-A-A-T-C-G.

Jordi Quintana; Kazimierz Grzeskowiak; Kazunori Yanagi; Richard E. Dickerson

The X-ray crystal structure analysis of the decamer C-G-A-T-T-A-A-T-C-G has been carried out to a resolution of 1.5 A. The crystals are space group P2(1)2(1)2(1), cell dimensions a = 38.60 A, b = 39.10 A, c = 33.07 A. The structure was solved by molecular replacement and refined with X-PLOR and NUCLSQ. The final R factor for a model with 404 DNA atoms, 108 water molecules and one magnesium hexahydrate cation is 15.7%. The double helix is essentially isostructural with C-G-A-T-C-G-A-T-C-G, with closely similar local helix parameters. The structure of the T-T-A-A center differs from that found in C-G-C-G-T-T-A-A-C-G-C-G in that the minor groove in our decamer is wide at the central T-A step rather than narrow, and the twist angle of the T-A step is small (31.1 degrees) rather than large. Whereas the tetrad model provides a convenient framework for discussing local DNA helix structure, it cannot be the entire story. The articulated helix model of DNA structure proposes that certain sequence regions of DNA show preferential twisting or bending properties, whereas other regions are less capable of deformation, in a manner that may be useful in sequence recognition by drugs and protein. Further crystal structure analyses should help to delineate the precise nature of sequence-dependent articulation in the DNA double helix.


Nucleosides, Nucleotides & Nucleic Acids | 1991

Polymorphism, Packing, Resolution, and Reliability in Single-Crystal DNA Oligomer Analyses

Richard E. Dickerson; Kazimierz Grzeskowiak; Maria Grzeskowiak; Mary L. Kopka; Teresa A. Larsen; Andrei A. Lipanov; Gilbert G. Privé; Jordi Quintana; Peter Schultze; Kazunori Yanagi; Hanna Yuan; Hyo-Chun Yoon

Abstract Synthetic double-helical B-DNA oligonucleotides crystallize in orthorhombic, monoclinic, and trigonal patterns that are determined by fine details of intermolecular contacts. Crystal packing apparently has relatively little influence on local helix structure, and noncrystallographic symmetry differences can be used to evaluate the quality of analyses.


Chemistry & Biology | 1996

Sequence-dependent structural variation in B-DNA

Kazimierz Grzeskowiak

Though fiber diffraction originally led to the belief that the structure of DNA would be a simple regular helix, X-ray crystallography of synthetic oligomers has shown that both deformability and structure depend on sequence. But the rules that determine these factors remain mysterious.


Biochemistry | 1996

Structure of the Escherichia coli response regulator NarL.

Igor Baikalov; Imke Schröder; Maria Kaczor-Grzeskowiak; Kazimierz Grzeskowiak; Robert P. Gunsalus; Richard E. Dickerson


Journal of Biomolecular Structure & Dynamics | 1989

The Structure of DAPI Bound to DNA

Teresa A. Larsen; David S. Goodsell; Duilio Cascio; Kazimierz Grzeskowiak; Richard E. Dickerson


Biochemistry | 1994

Crystal structure of a covalent DNA-drug adduct: anthramycin bound to C-C-A-A-C-G-T-T-G-G and a molecular explanation of specificity.

Mary L. Kopka; David S. Goodsell; Igor Baikalov; Kazimierz Grzeskowiak; Duilio Cascio; Richard E. Dickerson


Nature | 1988

X-ray structure of a DNA hairpin molecule.

Rajagopal Chattopadhyaya; Satoshi Ikuta; Kazimierz Grzeskowiak; Richard E. Dickerson


Biochemistry | 1995

Crystal structure of C-T-C-T-C-G-A-G-A-G. Implications for the structure of the Holliday junction.

David S. Goodsell; Kazimierz Grzeskowiak; Richard E. Dickerson


Biochemistry | 1993

Crystallographic analysis of C-C-A-A-G-C-T-T-G-G and its implications for bending in B-DNA.

Kazimierz Grzeskowiak; David S. Goodsell; Maria Kaczor-Grzeskowiak; Duilio Cascio; Richard E. Dickerson

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Hirofumi Ohishi

Taisho Pharmaceutical Co.

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Toshimasa Ishida

Osaka University of Pharmaceutical Sciences

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David S. Goodsell

Scripps Research Institute

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Duilio Cascio

University of California

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Igor Baikalov

University of California

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Jordi Quintana

University of California

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