Chemical Biology & Drug Design
RESEARCH LETTER
Full Access

Dual‐protected amino acid derivatives as new antitubercular agents

Pedro P. de Castro

Department of Chemistry, Federal University of Juiz de Fora, Minas Gerais, Brazil

Search for more papers by this author
Débora L. Campos

Department of Biological Sciences, School of Pharmaceutical Science, São Paulo State University, Araraquara, São Paulo, Brazil

Search for more papers by this author
Fernando R. Pavan

Department of Biological Sciences, School of Pharmaceutical Science, São Paulo State University, Araraquara, São Paulo, Brazil

Search for more papers by this author
Giovanni W. Amarante

Corresponding Author

E-mail address: giovanni.amarante@ufjf.edu.br

Department of Chemistry, Federal University of Juiz de Fora, Minas Gerais, Brazil

Correspondence

Giovanni W. Amarante, Department of Chemistry, Federal University of Juiz de Fora, Minas Gerais, Brazil.

Email: giovanni.amarante@ufjf.edu.br

Search for more papers by this author
First published: 20 April 2018
https://doi.org/10.1111/cbdd.13315
Citations: 4
Get access to the full version of this article. View access options below.
Institutional Login
Loading institution options...

If you have previously obtained access with your personal account, .

Purchase Instant Access
    • View the article PDF and any associated supplements and figures for a period of 48 hours.
    • Article can not be printed.
    • Article can not be downloaded.
    • Article can not be redistributed.
    • Unlimited viewing of the article PDF and any associated supplements and figures.
    • Article can not be printed.
    • Article can not be downloaded.
    • Article can not be redistributed.
    • Unlimited viewing of the article/chapter PDF and any associated supplements and figures.
    • Article/chapter can be printed.
    • Article/chapter can be downloaded.
    • Article/chapter can not be redistributed.
Check out

Abstract

Tuberculosis is an infectious disease with high incidence and growing drug‐resistant rates. In an attempt to develop new antitubercular agents, 35 compounds were synthesized, most of them bearing a carbamate and enantiopure amino acid moiety. These compounds had their activity evaluated toward a Mycobacterium tuberculosis strain (ATCC 27294) and cytotoxicity against fibroblast MRC‐5 cells (ATCC CCL‐171). Three of the prepared derivatives presented a good antimicrobial inhibition and two of them a moderate cytotoxicity. The lipophilicity seems to play a vital role in the cell growth activity, with best results for the derivatives with a higher logP.

The full text of this article hosted at iucr.org is unavailable due to technical difficulties.