Inhibition of a protein-protein interaction between INI1 and c-Myc by small 
peptidomimetic molecules inspired by Helix-1 of c-Myc: identification of a new 
target of potential antineoplastic interest

Bagnasco, L.; Tortolina, L.; Biasotti, B.; Castagnino, N.; Ponassi, R.; Tomati, V.; Nieddu, E.; Stier, Gunter; Malacarne, D.; Parodi, S.

doi:10.1096/fj.06-7082com

Local TagsRelease HistoryDetailsSummary

Inhibition of a protein-protein interaction between INI1 and c-Myc by small peptidomimetic molecules inspired by Helix-1 of c-Myc: identification of a new target of potential antineoplastic interest

Bagnasco, L., Tortolina, L., Biasotti, B., Castagnino, N., Ponassi, R., Tomati, V., et al. (2007). Inhibition of a protein-protein interaction between INI1 and c-Myc by small peptidomimetic molecules inspired by Helix-1 of c-Myc: identification of a new target of potential antineoplastic interest. The FASEB Journal, 21(4), 1256-1263. doi:10.1096/fj.06-7082com.

Item is Released

show all hide all

Basic

show hide

Item Permalink: https://hdl.handle.net/11858/00-001M-0000-002C-AB9A-D Version Permalink: https://hdl.handle.net/11858/00-001M-0000-002C-AB9B-B

Genre: Journal Article

Alternative Title : Inhibition of a protein-protein interaction between INI1 and c-Myc by small peptidomimetic molecules inspired by Helix-1 of c-Myc: identification of a new target of potential antineoplastic interest

Files

show Files

hide Files

:

FASEBJ_21_2007_1256.pdf (Any fulltext), 255KB

File Permalink:
-

Name:
FASEBJ_21_2007_1256.pdf

Description:
-

OA-Status:

Visibility:
Restricted (Max Planck Institute for Medical Research, MHMF; )

MIME-Type / Checksum:
application/pdf

Technical Metadata:

Copyright Date:
-

Copyright Info:
-

License:
-

Locators

show

hide

Locator:
http://www.fasebj.org/content/21/4/1256.full.pdf+html (Any fulltext) Open Access status unknown

Description:
-

OA-Status:

Locator:
https://dx.doi.org/10.1096/fj.06-7082com (Any fulltext) Open Access status unknown

Description:
-

OA-Status:

Creators

show

hide

Creators:
Bagnasco, L., Author
Tortolina, L., Author
Biasotti, B., Author
Castagnino, N., Author
Ponassi, R., Author
Tomati, V., Author
Nieddu, E., Author
Stier, Gunter¹, Author
Malacarne, D., Author
Parodi, S., Author

Affiliations:
1Department of Biomolecular Mechanisms, Max Planck Institute for Medical Research, Max Planck Society, ou_1497700

Content

show

hide

Free keywords: inhibitors

Abstract: c-Myc is a transcription modulator proto-oncogene. When overexpressed, it becomes an important contributor to the multi-hit process of malignant transformation. In two earlier papers in this journal (see refs. 19 , 20) we reported that retro-inverso peptidomimetic molecules inspired by the Helix-1 of c-Myc motif could be sequence-specific antiproliferative agents active in the low micromolar range. We also found that our peptides were not opening the four-alpha-helix Myc:Max bundle. Their antiproliferative activity in cancer cell lines needs the presence of side chains projecting outside of the bundle in the corresponding native H1 motif. This observation suggested interference with an external partner. In this study we investigated the INI1:Myc interaction. INI1 is a subunit of the SWI/SNF complex (component of the enhanceosome surrounding Myc:Max heterodimer). The INI1:Myc interaction was confirmed via pull down, ELISA, and fluorescence anisotropy assays. According to the length of INI1 fragments used, we calculated Kds ranging between 1.3x10(-6) and 4.8x10(-7) M. The three different techniques applied showed that the INI1:Myc interaction was also the target of our retro-inverso peptidomimetic molecules, which seem to bind specifically at INI1. A Myc binding, 21aa INI1 fragment (minimum interacting sequence), could inspire the synthesis of a new class of more selective c-Myc inhibitors.

Details

show

hide

Language(s): eng - English

Dates: Submitted: 2006-08-18Accepted: 2006-11-09Published Online: 2007-01-10Date issued: 2007-04-01

Publication Status: Issued

Pages: 8

Publishing info: -

Table of Contents: -

Rev. Type: Peer

Identifiers: eDoc: 664850
DOI: 10.1096/fj.06-7082com
URI: http://www.ncbi.nlm.nih.gov/pubmed/17215484
URI: http://www.fasebj.org/content/21/4/1256.full
URI: http://www.fasebj.org/content/21/4/1256.full.pdf+html
Other: 7998

Degree: -

Event

show

Legal Case

show

Project information

show

Source 1

show

hide

Title: The FASEB Journal

Other : FASEB J.

Source Genre: Journal

Creator(s):

Affiliations:

Publ. Info: Bethesda, Md. : The Federation

Pages: - Volume / Issue: 21 (4) Sequence Number: - Start / End Page: 1256 - 1263 Identifier: ISSN: 0892-6638
CoNE: https://pure.mpg.de/cone/journals/resource/954927535970_1