Synthesis and antituberculosis activity of new fatty acid amides
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Montes D'Oca, Caroline Da Ros
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Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Montes D'Oca, Caroline Da Ros
[1
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Coelho, Tatiane
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Univ Fed Rio Grande, Fac Med, Lab Micobacteriol, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Coelho, Tatiane
[2
]
Marinho, Tamara Germani
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Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Marinho, Tamara Germani
[1
]
Lopes Hack, Carolina Rosa
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Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Lopes Hack, Carolina Rosa
[1
]
Duarte, Rodrigo da Costa
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Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Duarte, Rodrigo da Costa
[1
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da Silva, Pedro Almeida
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Univ Fed Rio Grande, Fac Med, Lab Micobacteriol, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
da Silva, Pedro Almeida
[2
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Montes D'Oca, Marcelo Goncalves
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Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, BrazilUniv Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
Montes D'Oca, Marcelo Goncalves
[1
]
机构:
[1] Univ Fed Rio Grande, Escola Quim & Alimentos, Lab Kolbe Sintese Organ, Rio Grande, RS, Brazil
[2] Univ Fed Rio Grande, Fac Med, Lab Micobacteriol, Rio Grande, RS, Brazil
This work reports the synthesis of new fatty acid amides from C16: 0, 18: 0, 18: 1, 18: 1 (OH), and 18: 2 fatty acids families with cyclic and acyclic amines and demonstrate for the first time the activity of these compounds as antituberculosis agents against Mycobacterium tuberculosis H(37)Rv, M. tuberculosis rifampicin resistance (ATCC 35338), and M. tuberculosis isoniazid resistance (ATCC 35822). The fatty acid amides derivate from ricinoleic acid were the most potent one among a series of tested compounds, with a MIC 6.25 mu g/mL for resistance strains. (C) 2010 Elsevier Ltd. All rights reserved.