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A novel form of the DNA double helix imposed on the TATA-box by the TATA-binding protein

Gali Guzikevich-Guerstein
Zippora Shakked
Research01 Jan 1996
Nature Structural Biology

Volume: 3, P: 32-37
The conformation of the DNA double helix in the crystal is dependent on its environment

Zippora Shakked
Gali Guerstein-Guzikevich
Dov Rabinovich
Research01 Nov 1989
Nature

Volume: 342, P: 456-460
X-ray study of the rubidium salt of ADP

M. A. VISWAMITRA
M. V. HOSUR
OLGA KENNARD
Research01 Jul 1976
Nature

Volume: 262, P: 234-236
Structural basis of reactivation of oncogenic p53 mutants by a small molecule: methylene quinuclidinone (MQ)

The tumor suppressor p53 is mutated in more than half of human cancers and the compound methylene quinuclidinone (MQ) was shown to reactivate p53 mutants by binding covalently to cysteine residues. Here, the authors present crystal structures of wild-type and cancer related p53 mutant core domains bound to MQ alone and in complex with their DNA response elements and observe that MQ is bound to several cysteine residues located at the surface of the core domain.

Oksana Degtjarik
Dmitrij Golovenko
Zippora Shakked
ResearchOpen Access03 Dec 2021
Nature Communications

Volume: 12, P: 1-17
Diversity in DNA recognition by p53 revealed by crystal structures with Hoogsteen base pairs

High-resolution structures of p53 core domain tetramer bound to DNA containing 2 contiguous half-sites reveal a non-canonical Hoogsteen base-pairing at the center, which allows enhanced protein-DNA and protein-protein interactions. This distinct mode of recognition likely contributes to the different affinities shown by p53-regulated promoters and their different cellular outcomes.

Malka Kitayner
Haim Rozenberg
Zippora Shakked
Research04 Apr 2010
Nature Structural & Molecular Biology

Volume: 17, P: 423-429
Structure of Type-I Mycobacterium tuberculosis fatty acid synthase at 3.3 Å resolution

The type-I fatty acid synthase (FAS-I) complex is essential for Mycobacterium tuberculosis (Mtb) and mediates the production of C₂₆ fatty acids that are precursors for the synthesis of mycolic acids. Here the authors present the 3.3 Å resolution cryo-EM structure of Mtb FAS-I, which is of interest for tuberculosis drug development.

Nadav Elad
Szilvia Baron
Ron Diskin
ResearchOpen Access24 Sept 2018
Nature Communications

Volume: 9, P: 1-6
DNA binding and 3′–5′ exonuclease activity in the murine alternatively-spliced p53 protein

Zippora Shakked
Michael Yavnilovitch
Tali E Haran
Research29 Jul 2002
Oncogene

Volume: 21, P: 5117-5126
Post-translational regulation of p53 function through 20S proteasome-mediated cleavage

Hilla Solomon
Bastian Bräuning
Michal Sharon
Research08 Sept 2017
Cell Death & Differentiation

Volume: 24, P: 2187-2198

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A novel form of the DNA double helix imposed on the TATA-box by the TATA-binding protein

The conformation of the DNA double helix in the crystal is dependent on its environment

X-ray study of the rubidium salt of ADP

Structural basis of reactivation of oncogenic p53 mutants by a small molecule: methylene quinuclidinone (MQ)

Diversity in DNA recognition by p53 revealed by crystal structures with Hoogsteen base pairs

Structure of Type-I Mycobacterium tuberculosis fatty acid synthase at 3.3 Å resolution

DNA binding and 3′–5′ exonuclease activity in the murine alternatively-spliced p53 protein

Post-translational regulation of p53 function through 20S proteasome-mediated cleavage

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