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Literature DB >> 15802643

The crystal structure of a partial mouse Notch-1 ankyrin domain: repeats 4 through 7 preserve an ankyrin fold.

Olga Y Lubman¹, Raphael Kopan, Gabriel Waksman, Sergey Korolev.

Abstract

Folding and stability of proteins containing ankyrin repeats (ARs) is of great interest because they mediate numerous protein-protein interactions involved in a wide range of regulatory cellular processes. Notch, an ankyrin domain containing protein, signals by converting a transcriptional repression complex into an activation complex. The Notch ANK domain is essential for Notch function and contains seven ARs. Here, we present the 2.2 A crystal structure of ARs 4-7 from mouse Notch 1 (m1ANK). These C-terminal repeats were resistant to degradation during crystallization, and their secondary and tertiary structures are maintained in the absence of repeats 1-3. The crystallized fragment adopts a typical ankyrin fold including the poorly conserved seventh AR, as seen in the Drosophila Notch ANK domain (dANK). The structural preservation and stability of the C-terminal repeats shed a new light onto the mechanism of hetero-oligomeric assembly during Notch-mediated transcriptional activation.

Entities: Gene Species

Mesh：

Substances：

Year: 2005 PMID： 15802643 PMCID： PMC2253258 DOI： 10.1110/ps.041184105

Source DB: PubMed Journal: Protein Sci ISSN： 0961-8368 Impact factor: 6.725

44 in total

1. SKIP, a CBF1-associated protein, interacts with the ankyrin repeat domain of NotchIC To facilitate NotchIC function.

Authors: S Zhou; M Fujimuro; J J Hsieh; L Chen; A Miyamoto; G Weinmaster; S D Hayward
Journal: Mol Cell Biol Date: 2000-04 Impact factor: 4.272

Review 2. Notch signaling: cell fate control and signal integration in development.

Authors: S Artavanis-Tsakonas; M D Rand; R J Lake
Journal: Science Date: 1999-04-30 Impact factor: 47.728

3. Nuclear localization of CBF1 is regulated by interactions with the SMRT corepressor complex.

Authors: S Zhou; S D Hayward
Journal: Mol Cell Biol Date: 2001-09 Impact factor: 4.272

4. The origin of the ankyrin repeat region in Notch intracellular domains is critical for regulation of HES promoter activity.

Authors: P Beatus; J Lundkvist; C Oberg; K Pedersen; U Lendahl
Journal: Mech Dev Date: 2001-06 Impact factor: 1.882

5. LAG-3 is a putative transcriptional activator in the C. elegans Notch pathway.

Authors: A G Petcherski; J Kimble
Journal: Nature Date: 2000-05-18 Impact factor: 49.962

6. The N- and C-terminal regions of RBP-J interact with the ankyrin repeats of Notch1 RAMIC to activate transcription.

Authors: S Tani; H Kurooka; T Aoki; N Hashimoto; T Honjo
Journal: Nucleic Acids Res Date: 2001-03-15 Impact factor: 16.971

7. Biologic and biochemical analyses of p16(INK4a) mutations from primary tumors.

Authors: W G Yarbrough; R A Buckmire; M Bessho; E T Liu
Journal: J Natl Cancer Inst Date: 1999-09-15 Impact factor: 13.506

8. Conservation of the biochemical mechanisms of signal transduction among mammalian Notch family members.

Authors: T Mizutani; Y Taniguchi; T Aoki; N Hashimoto; T Honjo
Journal: Proc Natl Acad Sci U S A Date: 2001-07-17 Impact factor: 11.205

9. The notch 3 intracellular domain represses notch 1-mediated activation through Hairy/Enhancer of split (HES) promoters.

Authors: P Beatus; J Lundkvist; C Oberg; U Lendahl
Journal: Development Date: 1999-09 Impact factor: 6.868

10. Vanilloid receptor-related osmotically activated channel (VR-OAC), a candidate vertebrate osmoreceptor.

Authors: W Liedtke; Y Choe; M A Martí-Renom; A M Bell; C S Denis; A Sali; A J Hudspeth; J M Friedman; S Heller
Journal: Cell Date: 2000-10-27 Impact factor: 41.582

14 in total

1. Crystal structure of a Tankyrase-Axin complex and its implications for Axin turnover and Tankyrase substrate recruitment.

Authors: Seamus Morrone; Zhihong Cheng; Randall T Moon; Feng Cong; Wenqing Xu
Journal: Proc Natl Acad Sci U S A Date: 2012-01-17 Impact factor: 11.205

The crystal structure of a partial mouse Notch-1 ankyrin domain: repeats 4 through 7 preserve an ankyrin fold.

1. SKIP, a CBF1-associated protein, interacts with the ankyrin repeat domain of NotchIC To facilitate NotchIC function.

Review 2. Notch signaling: cell fate control and signal integration in development.

3. Nuclear localization of CBF1 is regulated by interactions with the SMRT corepressor complex.

4. The origin of the ankyrin repeat region in Notch intracellular domains is critical for regulation of HES promoter activity.

5. LAG-3 is a putative transcriptional activator in the C. elegans Notch pathway.

6. The N- and C-terminal regions of RBP-J interact with the ankyrin repeats of Notch1 RAMIC to activate transcription.

7. Biologic and biochemical analyses of p16(INK4a) mutations from primary tumors.

8. Conservation of the biochemical mechanisms of signal transduction among mammalian Notch family members.

9. The notch 3 intracellular domain represses notch 1-mediated activation through Hairy/Enhancer of split (HES) promoters.

10. Vanilloid receptor-related osmotically activated channel (VR-OAC), a candidate vertebrate osmoreceptor.

1. Crystal structure of a Tankyrase-Axin complex and its implications for Axin turnover and Tankyrase substrate recruitment.

2. Notch2, but not Notch1, is required for proximal fate acquisition in the mammalian nephron.

3. A proline repeat domain in the Notch co-activator MAML1 is important for the p300-mediated acetylation of MAML1.

4. High-resolution crystal structure of the human Notch 1 ankyrin domain.

5. Conformational locking upon cooperative assembly of notch transcription complexes.

6. Assembly of a Notch transcriptional activation complex requires multimerization.

7. Quantitative dissection of the Notch:CSL interaction: insights into the Notch-mediated transcriptional switch.

Review 8. Functional diversity of ankyrin repeats in microbial proteins.

9. Analysis of repeat-protein folding using nearest-neighbor statistical mechanical models.

Review 10. The molecular logic of Notch signaling--a structural and biochemical perspective.