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以及丁香酚抗隐孢子虫活性的评估。

and evaluation of the anti-cryptosporidial activity of eugenol.

作者信息

Gattan Hattan S, Wakid Majed H, Qahwaji Rowaid M, Altwaim Sarah, Mahjoub Haifaa A, Alfaifi Mashael S, Elshazly Hayam, Al-Megrin Wafa Abdullah I, Alshehri Eman Abdullah, Elshabrawy Hatem A, El-Kady Asmaa M

机构信息

Department of Medical Laboratory Sciences, Faculty of Applied Medical Sciences, King Abdulaziz University, Jeddah, Saudi Arabia.

Special Infectious Agents Unit, King Fahd Medical Research Center, Jeddah, Saudi Arabia.

出版信息

Front Vet Sci. 2024 Mar 7;11:1374116. doi: 10.3389/fvets.2024.1374116. eCollection 2024.

Abstract

BACKGROUND

Cryptosporidiosis is an opportunistic parasitic disease widely distributed worldwide. Although sp. causes asymptomatic infection in healthy people, it may lead to severe illness in immunocompromised individuals. Limited effective therapeutic alternatives are available against cryptosporidiosis in this category of patients. So, there is an urgent need for therapeutic alternatives for cryptosporidiosis. Recently, the potential uses of Eugenol (EUG) have been considered a promising novel treatment for bacterial and parasitic infections. Consequently, it is suggested to investigate the effect of EUG as an option for the treatment of cryptosporidiosis.

MATERIALS AND METHODS

The bioinformatics analysis was used to predict and determine the binding affinities and intermolecular interactions of EUG and Nitazoxanide (NTZ) toward several () lowa II target proteins. For animal study, five groups of immunosuppressed Swiss albino mice (10 mice each) were used. Group I was left uninfected (control), and four groups were infected with 1,000 oocysts of sp. The first infected group was left untreated. The remaining three infected groups received NTZ, EUG, and EUG + NTZ, respectively, on the 6th day post-infection (dpi). All mice were sacrificed 30 dpi. The efficacy of the used formulas was assessed by counting the number of oocysts excreted in stool of infected mice, histopathological examination of the ileum and liver tissues and determination of the expression of iNOS in the ileum of mice in different animal groups.

RESULTS

treatment with EUG resulted in a significant reduction in the number of oocysts secreted in stool when compared to infected untreated mice. In addition, oocyst excretion was significantly reduced in mice received a combination therapy of EUG and NTZ when compared with those received NTZ alone. EUG succeeded in reverting the histopathological alterations induced by infection either alone or in combination with NTZ. Moreover, mice received EUG showed marked reduction of the expression of iNOS in ileal tissues.

CONCLUSION

Based on the results, the present study signified a basis for utilizing EUG as an affordable, safe, and alternative therapy combined with NTZ in the management of cryptosporidiosis.

摘要

背景

隐孢子虫病是一种在全球广泛分布的机会性寄生虫病。虽然隐孢子虫在健康人群中可引起无症状感染,但在免疫功能低下的个体中可能导致严重疾病。对于这类患者的隐孢子虫病,有效的治疗选择有限。因此,迫切需要针对隐孢子虫病的治疗替代方案。最近,丁香酚(EUG)的潜在用途被认为是一种有前景的新型细菌和寄生虫感染治疗方法。因此,建议研究EUG作为治疗隐孢子虫病的一种选择的效果。

材料与方法

采用生物信息学分析来预测和确定EUG和硝唑尼特(NTZ)对几种()爱荷华II型靶蛋白的结合亲和力和分子间相互作用。对于动物研究,使用了五组免疫抑制的瑞士白化小鼠(每组10只)。第一组未感染(对照),其余四组感染1000个隐孢子虫卵囊。第一个感染组未接受治疗。其余三个感染组在感染后第6天(dpi)分别接受NTZ、EUG和EUG + NTZ治疗。所有小鼠在30 dpi时处死。通过计算感染小鼠粪便中排出的卵囊数量、回肠和肝脏组织的组织病理学检查以及测定不同动物组小鼠回肠中诱导型一氧化氮合酶(iNOS)的表达来评估所用配方的疗效。

结果

与未治疗的感染小鼠相比,EUG治疗导致粪便中分泌的卵囊数量显著减少。此外,与单独接受NTZ治疗的小鼠相比,接受EUG和NTZ联合治疗的小鼠卵囊排泄量显著降低。EUG成功逆转了单独或与NTZ联合感染引起的组织病理学改变。此外,接受EUG治疗的小鼠回肠组织中iNOS的表达明显降低。

结论

基于这些结果,本研究表明了将EUG作为一种经济实惠、安全的替代疗法与NTZ联合用于隐孢子虫病管理的依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c466/10954888/eef0b3d3c140/fvets-11-1374116-g001.jpg

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