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生成一氧化氮的亚硝基谷胱甘肽纳米颗粒作为对抗铜绿假单胞菌感染伤口的改进策略。

Nitrosoglutathione generating nitric oxide nanoparticles as an improved strategy for combating Pseudomonas aeruginosa-infected wounds.

作者信息

Chouake Jason, Schairer David, Kutner Allison, Sanchez David A, Makdisi Joy, Blecher-Paz Karin, Nacharaju Parimala, Tuckman-Vernon Chaim, Gialanella Phil, Friedman Joel M, Nosanchuk Joshua D, Friedman Adam J

机构信息

Department of Medicine, Division of Dermatology, Montefiore Medical Center, Bronx, NY, USA.

出版信息

J Drugs Dermatol. 2012 Dec;11(12):1471-7.


DOI:
PMID:23377518
Abstract

Pseudomonas aeruginosa is a community-acquired, nosocomial pathogen that is an important cause of human morbidity and mortality; it is intrinsically resistant to several antibiotics and is capable of developing resistance to newly developed drugs via a variety of mechanisms. P aeruginosa's ubiquity and multidrug resistance (MDR) warrants the development of innovative methods that overcome its ability to develop resistance. We have previously described a nitric oxide-releasing nanoparticle (NO-np) platform that effectively kills gram-positive and gram-negative organisms in vitro and accelerates clinical recovery in vivo in murine wound and abscess infection models. We have also demonstrated that when glutathione (GSH) is added to NO-np, the nitroso intermediate S-nitrosoglutathione (GSNO) is formed, which has greater activity against P aeruginosa and other gram-negative organisms compared with NO-np alone. In the current study, we evaluate the potential of NO-np to generate GSNO both in vitro and in vivo in a murine excisional wound model infected with an MDR clinical isolate of P aeruginosa. Whereas NO-np alone inhibited P aeruginosa growth in vitro for up to 8 hours, NO-np+GSH completely inhibited P aeruginosa growth for 24 hours. Percent survival in the NO-np+GSH-treated isolates was significantly lower than in the NO-np (36.1% vs 8.3%; P=.004). In addition, NO-np+GSH accelerated wound closure in P aeruginosa-infected wounds, and NO-np+GSH-treated wounds had significantly lower bacterial burden when compared to NO-np-treated wounds (P<.001). We conclude that GSNO is easily generated from our NO-np platform and has the potential to be used as an antimicrobial agent against MDR organisms such as P aeruginosa.

摘要

铜绿假单胞菌是一种社区获得性医院病原体,是导致人类发病和死亡的重要原因;它对多种抗生素具有内在抗性,并且能够通过多种机制对新开发的药物产生抗性。铜绿假单胞菌的广泛存在和多重耐药性(MDR)使得有必要开发创新方法来克服其产生抗性的能力。我们之前描述了一种释放一氧化氮的纳米颗粒(NO-np)平台,该平台在体外能有效杀死革兰氏阳性和革兰氏阴性生物体,并在小鼠伤口和脓肿感染模型中加速体内临床恢复。我们还证明,当将谷胱甘肽(GSH)添加到NO-np中时,会形成亚硝基中间体S-亚硝基谷胱甘肽(GSNO),与单独的NO-np相比,它对铜绿假单胞菌和其他革兰氏阴性生物体具有更强的活性。在当前研究中,我们在感染了铜绿假单胞菌多重耐药临床分离株的小鼠切除伤口模型中评估了NO-np在体外和体内产生GSNO的潜力。单独的NO-np在体外可抑制铜绿假单胞菌生长长达8小时,而NO-np+GSH可完全抑制铜绿假单胞菌生长24小时。经NO-np+GSH处理的分离株的存活率显著低于经NO-np处理的分离株(36.1%对8.3%;P=0.004)。此外,NO-np+GSH加速了铜绿假单胞菌感染伤口的愈合,与经NO-np处理的伤口相比,经NO-np+GSH处理的伤口细菌负荷显著更低(P<0.001)。我们得出结论,GSNO可轻易从我们的NO-np平台产生,并且有潜力用作针对铜绿假单胞菌等多重耐药生物体的抗菌剂。

相似文献

[1]
Nitrosoglutathione generating nitric oxide nanoparticles as an improved strategy for combating Pseudomonas aeruginosa-infected wounds.

J Drugs Dermatol. 2012-12

[2]
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[3]
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Adv Drug Deliv Rev. 2013-7-24

[4]
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Virulence. 2010

[5]
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Int J Biol Macromol. 2015-8

[6]
Antimicrobial photodynamic therapy on drug-resistant Pseudomonas aeruginosa-induced infection. An in vivo study.

Photochem Photobiol. 2012-3-30

[7]
Antimicrobial efficacy and toxicity of novel CAMPs against P. aeruginosa infection in a murine skin wound infection model.

BMC Microbiol. 2019-12-16

[8]
Antimicrobial and healing efficacy of sustained release nitric oxide nanoparticles against Staphylococcus aureus skin infection.

J Invest Dermatol. 2009-10

[9]
AB569, a Novel, Topical Bactericidal Gel Formulation, Kills Pseudomonas aeruginosa and Promotes Wound Healing in a Murine Model of Burn Wound Infection.

Infect Immun. 2021-10-15

[10]
In vitro activities of non-traditional antimicrobials alone or in combination against multidrug-resistant strains of Pseudomonas aeruginosa and Acinetobacter baumannii isolated from intensive care units.

Int J Antimicrob Agents. 2006-3

引用本文的文献

[1]
Roles and current applications of S-nitrosoglutathione in anti-infective biomaterials.

Mater Today Bio. 2022-9-6

[2]
Nanotechnology as a tool to advance research and treatment of non-oncologic urogenital diseases.

Ther Adv Urol. 2022-7-26

[3]
Nanomaterial Nitric Oxide Delivery in Traumatic Orthopedic Regenerative Medicine.

Front Bioeng Biotechnol. 2021-1-18

[4]
Hypoxia inducible factor-1 alpha stabilization for regenerative therapy in traumatic brain injury.

Neural Regen Res. 2017-5

[5]
Nanotechnology-Driven Therapeutic Interventions in Wound Healing: Potential Uses and Applications.

ACS Cent Sci. 2017-3-22

[6]
Nitric oxide therapy for dermatologic disease.

Future Sci OA. 2015-8-1

[7]
HbE/β-Thalassemia and Oxidative Stress: The Key to Pathophysiological Mechanisms and Novel Therapeutics.

Antioxid Redox Signal. 2017-5-10

[8]
Alternative antimicrobial approach: nano-antimicrobial materials.

Evid Based Complement Alternat Med. 2015-3-16

[9]
S-nitrosocaptopril nanoparticles as nitric oxide-liberating and transnitrosylating anti-infective technology.

Nanomedicine. 2014-11-15

[10]
Use of nitric oxide nanoparticulate platform for the treatment of skin and soft tissue infections.

Wiley Interdiscip Rev Nanomed Nanobiotechnol. 2013-5-9

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