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Literature DB >> 21277202

Synthesis of GN8 derivatives and evaluation of their antiprion activity in TSE-infected cells.

Tsutomu Kimura¹, Junji Hosokawa-Muto, Yuji O Kamatari, Kazuo Kuwata.

Abstract

A series of GN8 derivatives were synthesized from various diamines, carboxylic acid derivatives, and nitrogen nucleophiles, and their antiprion activity was tested in TSE-infected mouse neuronal cells. We found that two ethylenediamine units, hydrophobic substituents on the nitrogen atoms, and the diphenylmethane scaffold were essential structural features responsible for the activity. Seven derivatives bearing substituents at the benzylic position exhibited an improved antiprion activity with the IC(50) values of 0.51-0.83 μM. Conformational analysis of model compounds suggested that the introduction of the substituent at the benzylic position restricted the conformational variability of the diphenylmethane unit.

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Year: 2011 PMID： 21277202 DOI： 10.1016/j.bmcl.2010.12.132

Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN： 0960-894X Impact factor: 2.823

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Cited

7 in total

1. Poly-L-histidine inhibits prion propagation in a prion-infected cell line.

Authors: Ryo Honda; Kei-Ichi Yamaguchi; Abdelazim Elsayed Elhelaly; Mitsuhiko Fuji; Kazuo Kuwata
Journal: Prion Date: 2018-08-17 Impact factor: 3.931

2. Characterizing antiprion compounds based on their binding properties to prion proteins: implications as medical chaperones.

Authors: Yuji O Kamatari; Yosuke Hayano; Kei-ichi Yamaguchi; Junji Hosokawa-Muto; Kazuo Kuwata
Journal: Protein Sci Date: 2012-11-19 Impact factor: 6.725

Synthesis of GN8 derivatives and evaluation of their antiprion activity in TSE-infected cells.

1. Poly-L-histidine inhibits prion propagation in a prion-infected cell line.

2. Characterizing antiprion compounds based on their binding properties to prion proteins: implications as medical chaperones.

Review 3. Pharmacological Agents Targeting the Cellular Prion Protein.

Review 4. Exploring Anti-Prion Glyco-Based and Aromatic Scaffolds: A Chemical Strategy for the Quality of Life.

5. Redox-triggered cascade dearomative cyclizations enabled by hexafluoroisopropanol.

6. Direct interaction of DNMT inhibitors to PrP^C suppresses pathogenic process of prion.

7. Anti-prion activity of an RNA aptamer and its structural basis.

Synthesis of GN8 derivatives and evaluation of their antiprion activity in TSE-infected cells.

1. Poly-L-histidine inhibits prion propagation in a prion-infected cell line.

2. Characterizing antiprion compounds based on their binding properties to prion proteins: implications as medical chaperones.

Review 3. Pharmacological Agents Targeting the Cellular Prion Protein.

Review 4. Exploring Anti-Prion Glyco-Based and Aromatic Scaffolds: A Chemical Strategy for the Quality of Life.

5. Redox-triggered cascade dearomative cyclizations enabled by hexafluoroisopropanol.

6. Direct interaction of DNMT inhibitors to PrPC suppresses pathogenic process of prion.

7. Anti-prion activity of an RNA aptamer and its structural basis.

6. Direct interaction of DNMT inhibitors to PrP^C suppresses pathogenic process of prion.