Synthesis of cinnamic acid derivatives and leishmanicidal activity against Leishmania braziliensis

Rodrigues Michelle Peixoto; Tomaz Deborah Campos; de Souza Luciana Angelo; Onofre Thiago Souza; de Menezes Wemerson Aquiles; Almeida-Silva Juliana; Suarez-Fontes Ana Marcia; de Almeida Marcia Rogeria; Silva Adalberto Manoel; Bressan Gustavo Costa; Vannier-Santos Marcos Andre; Rangel Fietto Juliana Lopes; Teixeira Robson Ricardo

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Synthesis of cinnamic acid derivatives and leishmanicidal activity against Leishmania braziliensis

机译：对Leishmania Braziliensis的肉桂酸衍生物和Leishmanicidal活性的合成

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Leishmania braziliensis is one of the pathogenic agents of cutaneous and mucocutanoeous leishmaniasis. There are no validated vaccines to prevent the infection and the treatment relies on drugs that often present severe side effects, which justify the efforts to find new potential antileishmanial drugs. An alternative to promote the discovery of new drugs would be the association of different chemical groups of bioactive compounds. Here we describe the synthesis and bioactivity evaluation against L. braziliensis of cinnamic acid derivatives possessing isobenzofuranone and 1,2,3-triazole functionalities. We tested 25 compounds at 10 mu M concentration against extracellular promastigotes and intracellular amastigotes during macrophage infection. Most compounds were more active against amastigotes than to promastigotes. The derivatives (E)-3-oxo-1,3-dihydroisobenzofuran-5-yl-(3,4,5-trimethoxy) cinnamate (5c), (1-(3,4-difluorobenzyl)-1H-1,2,3-triazol-4-yl)methyl cinnamate (9g), and (1-(2-bromobenzyl)-1H-1,2,3triazol-4-yl)methyl cinnamate (91) were the most effective presenting over 80% toxicity on L braziliensis amastigotes. While compound 5c is a cinnamate with an isobenzofuranone portion, 9g and 9l are triazolic cinnamic acid derivatives. The action of these compounds was comparable to amphotericin B used as positive control. Ultrastructural analysis revealed that 5c-treated parasites showed impaired cytokinesis and apoptosis triggering. Taken together, these results highlight the potential of cinnamic acid derivatives in development of novel anti-leishmanial drugs. (C) 2019 Elsevier Masson SAS. All rights reserved.

机译：Leishmania Braziliensis是皮肤和粘蛋白的嗜利亚患者的病原体之一。没有经过验证的疫苗以防止感染，治疗依赖于往往呈现严重副作用的药物，这证明了寻找新的潜在抗野生药物的努力。促进新药的发现的替代方案将是生物活性化合物的不同化学类别的关联。在这里，我们描述了对具有异卵呋喃酮和1,2,3-三唑官能团的肉桂酸衍生物的L. Baziliensis的合成和生物活性评估。在巨噬细胞感染期间，我们在10亩浓度下以10μm浓度的浓度测试了25种化合物。巨噬细胞感染期间的细胞内春季。大多数化合物对Amastigotes更活跃而不是Promastigotes。衍生物（e）-3-氧代-1,3-二氢异洛呋喃-5-y1-（3,4,5-三甲氧基）肉桂酸（5℃），（1-（3,4-二氟苄基）-1H-1,2 ，3-三唑-4-基）肉桂酸甲酯（9g）和（1-（2-溴苄基）-1H-1,2,3trai唑-4-基）甲基肉桂酸甲（91）是最有效的呈现超过80％毒性在L Braziliensis Amastigotes。虽然化合物5c是肉桂酸二糖，但9g和9L是三唑型肉桂酸衍生物。这些化合物的作用与用作阳性对照的两性蛋白B相当。超微结构分析显示，5C处理的寄生虫显示细胞因子和细胞凋亡触发受损。总之，这些结果突出了肉桂酸衍生物在新型抗利尿药物发展中的潜力。（c）2019年Elsevier Masson SAS。版权所有。

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来源
《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2019年第2019期|共14页
作者
Rodrigues Michelle Peixoto; Tomaz Deborah Campos; de Souza Luciana Angelo; Onofre Thiago Souza; de Menezes Wemerson Aquiles; Almeida-Silva Juliana; Suarez-Fontes Ana Marcia; de Almeida Marcia Rogeria; Silva Adalberto Manoel; Bressan Gustavo Costa; Vannier-Santos Marcos Andre; Rangel Fietto Juliana Lopes; Teixeira Robson Ricardo;
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作者单位

Univ Fed Vicosa Dept Quim Vicosa MG Brazil;

Univ Fed Vicosa Dept Quim Vicosa MG Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Fiocruz MS Inst Oswaldo Cruz Rio De Janeiro RJ Brazil;

Fiocruz MS Inst Oswaldo Cruz Rio De Janeiro RJ Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Inst Fed Educ Ciencia &

Tecnol Catarinense Araquari SC Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Fiocruz MS Inst Oswaldo Cruz Rio De Janeiro RJ Brazil;

Univ Fed Vicosa Dept Bioquim &

Biol Mol Vicosa MG Brazil;

Univ Fed Vicosa Dept Quim Vicosa MG Brazil;

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原文格式 PDF
正文语种 eng
中图分类药学;
关键词
Cinnamic acid derivatives; Leishmanicidal activity; Leishmania braziliensis; Isobenzofuranone; 1; 2; 3-Triazole;

机译：肉桂酸衍生物;Leishmanicidal活动;Leishmania Braziliensis;isobenzofuranone;1;2;3-三唑;

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专利

1. Synthesis of cinnamic acid derivatives and leishmanicidal activity against Leishmania braziliensis [J] . Rodrigues Michelle Peixoto, Tomaz Deborah Campos, de Souza Luciana Angelo, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2019,第期

机译：对Leishmania Braziliensis的肉桂酸衍生物和Leishmanicidal活性的合成
2. In vitro leishmanicidal activity of imidazole- or pyrazole-based benzo(g)phthalazine derivatives against Leishmania infantum and Leishmania braziliensis species. [J] . Sanchez Moreno M, Gomez Contreras F, Navarro P, The Journal of Antimicrobial Chemotherapy . 2012,第2期

机译：咪唑或吡唑基苯并（g）酞嗪衍生物对婴儿利什曼原虫和巴西利什曼原虫的体外体外杀菌作用。
3. In vitro leishmanicidal activity of pyrazole-containing polyamine macrocycles which inhibit the Fe-SOD enzyme of Leishmania infantum and Leishmania braziliensis species [J] . NavarroP., Sánchez-MorenoM., MarínC., Parasitology . 2014,第8期

机译：含吡唑的多胺大环化合物的体外杀菌活性，抑制婴儿利什曼原虫和巴西利什曼原虫的Fe-SOD酶
4. Antifungal and Herbicidal Activities of Cinnamic Acid Derivatives [C] . Jun Zhu, Shinkichi Tawata 9th Japan-China Symposium on Pesticide Science October 26-28, 1998 Tian Jin China . 1998

机译：肉桂酸衍生物的抗真菌和除草活性
5. Structure and reactivity of cinnamic acid derivatives, analogs, and related metal complexes [D] . Snook, Julie Heather 2001

机译：肉桂酸衍生物，类似物和相关金属配合物的结构和反应性
6. In Vitro Leishmanicidal Activities of Sesquiterpene Lactones from Tithonia diversifolia against Leishmania braziliensis Promastigotes and Amastigotes [O] . Juliano S. de Toledo, Sergio R. Ambrósio, Carly H. G. Borges, 2014

机译：Tithonia diversifolia中倍半萜烯内酯对巴西利什曼原虫前鞭毛体和拟鞭毛体的体外利什曼杀菌活性。
7. Synthesis and leishmanicidal activity of cinnamic acid esters: structure–activity relationship [O] . Otero Elver, Robledo Sara M., Díaz Oltra Santiago, 2014

机译：肉桂酸酯的合成及其利什曼原虫活性：结构 - 活性关系

Synthesis of cinnamic acid derivatives and leishmanicidal activity against Leishmania braziliensis

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