The early stage peptidoglycan biosynthesis Mur enzymes are antibacterial and antisporulation drug targets for recurrent Clostridioides difficile infection

Sapkota Madhab; Marreddy Ravi K. R.; Wu Xiaoqian; Kumar Manish; Hurdle Julian G.

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The early stage peptidoglycan biosynthesis Mur enzymes are antibacterial and antisporulation drug targets for recurrent Clostridioides difficile infection

机译：早期的肽蛋白生物合成的混合物酶是复发性梭菌差异感染的抗菌和防治药物靶标

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Sporulation during Clostridioides difficile infection (CDI) contributes to recurrent disease. Cell division and sporulation both require peptidoglycan biosynthesis. We show C. difficile growth and sporulation is attenuated by antisenses to murA and murC or the MurA inhibitor fosfomycin. Thus, targeting the early steps of peptidoglycan biosynthesis might reduce the onset of recurrent CDI. (C) 2019 Elsevier Ltd. All rights reserved.

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《Anaerobe》 |2020年第2020期|共4页
作者
Sapkota Madhab; Marreddy Ravi K. R.; Wu Xiaoqian; Kumar Manish; Hurdle Julian G.;
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作者单位

Univ Texas Arlington Dept Biol Arlington TX 76019 USA;

Texas A&

M Univ Hlth Sci Ctr Biosci &

Technol Houston TX 77030 USA;

Texas A&

M Univ Hlth Sci Ctr Biosci &

Technol Houston TX 77030 USA;

Univ Texas Arlington Dept Biol Arlington TX 76019 USA;

Texas A&

M Univ Hlth Sci Ctr Biosci &

Technol Houston TX 77030 USA;

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原文格式 PDF
正文语种 eng
中图分类微生物学;
关键词
Peptidoglycan; Mur ligases; Antibiotic drug-targets; Heat-resistant spore cortex;

机译：肽聚糖;MUR连接酶;抗生素药物靶标;耐热孢子皮质;

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专利

1. The early stage peptidoglycan biosynthesis Mur enzymes are antibacterial and antisporulation drug targets for recurrent Clostridioides difficile infection [J] . Sapkota Madhab, Marreddy Ravi K. R., Wu Xiaoqian, Anaerobe . 2020,第期

机译：早期的肽蛋白生物合成的混合物酶是复发性梭菌差异感染的抗菌和防治药物靶标
2. Differential requirements for conserved peptidoglycan remodeling enzymes during Clostridioides difficile Clostridioides difficile spore formation [J] . Ribis John W., Fimlaid Kelly A., Shen Aimee Molecular Microbiology . 2018,第3期

机译：梭肽梭梭梭梭梭梭梭梭梭梭菌差异要求进行差异要求锥形孢子形成
3. Identification of i >O/i>O ‐acetylhomoserine sulfhydrylase, a putative enzyme responsible for methionine biosynthesis in i >Clostridioides difficile/i>Clostridioides difficile : Gene cloning and biochemical characterizations [J] . Kulikova Vitalia V., Revtovich Svetlana V., Bazhulina Natalia P., IUBMB life . 2019,第11期

机译：鉴定＆ i> o-sacetylhomoserine磺氢羟基磺酸盐，其负责蛋氨酸酸纤维胺酸纤维梭菌的甲硫氨酸生物合成的推定酶
4. Macrophage-Targeted Antibacterial Polymeric Prodrug for Controlled Drug Pharmacokinetics Against Alveolar Pulmonary Intracellular Infections [C] . Debashish Roy, Fang-Yi Su, Selvi Srinivasan, Society for Biomaterials annual meeting and exposition . 2019

机译：巨噬细胞靶向抗菌聚合前药对肺泡肺细胞内感染的控制药物药代动力学。
5. Use of Shotgun Metagenomic Sequencing to Determine How the Human Gut Microbiome and Antibiotic Resistome Influence the Risk of Recurrent Clostridioides difficile Infection [D] . ?Correa, Maria Alexandra 2020

机译：使用霰弹枪偏测元素测序以确定人体肠道微生物组和抗生素抵抗如何影响复发性梭氧化物差异感染的风险
6. Mapping Epitopes of a Novel Peptidoglycan Cross-Linking Enzyme Cwp22 Recognized by Human Sera Obtained from Patients with Clostridioides difficile Infection and Cord Blood [O] . Agnieszka Razim, Katarzyna Pacyga, Gajane Martirosian, 2019

机译：从难辨梭状芽孢杆菌感染和脐带血患者获得的人类血清识别的新型肽聚糖交联酶Cwp22的表位定位。
7. Cationic biaryl 1,2,3-triazolyl peptidomimetic amphiphiles targeting Clostridioides (Clostridium) difficile: Synthesis, antibacterial evaluation and an in vivo C. difficile infection model [O] . Andrew J. Tague, Papanin Putsathit, Melanie L. Hutton, 2019

机译：阳离子纤维素1,2,3-三唑基拟肽两亲靶向梭菌（Clostridium）差异：合成，抗菌评估和体内C.艰难梭菌感染模型

The early stage peptidoglycan biosynthesis Mur enzymes are antibacterial and antisporulation drug targets for recurrent Clostridioides difficile infection

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