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混合金属氧化物纳米颗粒抑制结核分枝杆菌在THP-1细胞中的生长。

Mixed metal oxide nanoparticles inhibit growth of Mycobacterium tuberculosis into THP-1 cells.

作者信息

Jafari A R, Mosavi T, Mosavari N, Majid A, Movahedzade F, Tebyaniyan M, Kamalzadeh M, Dehgan M, Jafari S, Arastoo S

机构信息

Rasoul-e-Akram Hospital, Antimicrobial Resistance Research Center, Iran University of Medical Sciences, Tehran, Iran.

Rasoul-e-Akram Hospital, Antimicrobial Resistance Research Center, Iran University of Medical Sciences, Tehran, Iran.

出版信息

Int J Mycobacteriol. 2016 Dec;5 Suppl 1:S181-S183. doi: 10.1016/j.ijmyco.2016.09.011. Epub 2016 Nov 5.

Abstract

OBJECTIVE/BACKGROUND: Humans have been in a constant battle with tuberculosis (TB). Currently, overuse of antibiotics has resulted in the spread of multidrug-resistant Mycobacterium tuberculosis (MDR), leading to antibiotic ineffectiveness at controlling the spread of TB infection in host cells and especially macrophages. Additionally, the Mycobacterium tuberculosis (Mtb) has developed methods to evade the immune system and survive. With the discovery of nanoparticle (NP)-based drugs, it is necessary to research their anti-mycobacterial properties and bactericidal mechanisms. In this study, we synthesized mixed metal oxide NPs and tested their ability to inhibit Mtb growth into macrophages and investigated the cytotoxic effects of NPs in THP-1 cells.

METHODS

Silver (Ag) NPs and zinc oxide (ZnO) NPs were synthesized by chemical reduction and chemical deposition in aqueous solution, and the diffraction light scattering, scanning electron microscopy, transmission electron microscopy, and ultraviolet-visible light-absorption spectra were used to identify NP properties. Ag and ZnO NPs were mixed together at a ratio of 8/2 and diluted into Löwenstein-Jensen medium followed by the addition of bacteria and incubation for 28days at 37°C. The toxicity of NPs to THP-1 cells was assessed by MTT test, and macrophages were infected with Mtb for 4h at 37°C under 5% CO.

RESULTS

Nano-sized particles were estimated at ∼30-80nm, and the initial concentration of Ag NPs and ZnO NPs were estimated at ∼20ppm and ∼60ppm. The minimal inhibitory concentration ratio of 8/2 NPs against Mtb was detected at ∼1/32 of the initial concentration. Ag NPs in the range of concentrations exhibited no anti-Mtb effects, whereas ZnO NPs showed potent antibacterial activity at ∼1/128 of the initial concentration. ZnO NPs at all concentrations showed cytotoxic activity, whereas 100% of THP-1 cells remained viable in the presence of Ag NPs at ∼1/32 and ∼1/64 of the initial concentrations. However, at ratios of 8/2, ∼39.94% of the cells at ∼1/16 of the initial concentration remained viable, with 100% of THP-1 cells at ∼1/32 of the initial concentration remaining viable.

CONCLUSION

Although Ag NPs exhibited low cytotoxicity, they were unable to inhibit Mtb growth in vitro. ZnO NPs exhibited strong anti-Mtb activity and inhibited bacterial growth, but exhibited high cytotoxicity to human macrophage cells. By mixing Ag and ZnO NPs at a ratio of 8/2, we acquired a mixture that exhibited potent antibacterial activity against Mtb and no cytotoxic effects on THP-1 cells, resulting in inhibition of both in vitro and ex vivo Mtb growth Figs. 1-3, Tables 1-3.

摘要

目的/背景:人类一直在与结核病(TB)进行持续斗争。目前,抗生素的过度使用导致了耐多药结核分枝杆菌(MDR)的传播,致使抗生素在控制宿主细胞尤其是巨噬细胞中结核感染传播方面失效。此外,结核分枝杆菌(Mtb)已形成逃避免疫系统并存活的方法。随着基于纳米颗粒(NP)药物的发现,有必要研究其抗分枝杆菌特性及杀菌机制。在本研究中,我们合成了混合金属氧化物NP,并测试了它们抑制Mtb在巨噬细胞中生长的能力,还研究了NP对THP - 1细胞的细胞毒性作用。

方法

通过化学还原和化学沉积在水溶液中合成银(Ag)NP和氧化锌(ZnO)NP,并利用衍射光散射、扫描电子显微镜、透射电子显微镜以及紫外 - 可见光吸收光谱来鉴定NP特性。将Ag和ZnO NP按8/2的比例混合,稀释到罗 - 琴培养基中,随后加入细菌并在37°C孵育28天。通过MTT试验评估NP对THP - 1细胞的毒性,在5%CO₂条件下于37°C让巨噬细胞感染Mtb4小时。

结果

估计纳米颗粒大小约为30 - 80nm,Ag NP和ZnO NP的初始浓度估计分别约为20ppm和60ppm。8/2比例的NP对Mtb的最低抑菌浓度比在初始浓度的约1/32处检测到。一定浓度范围内的Ag NP未表现出抗Mtb作用,而ZnO NP在初始浓度的约1/128时显示出强大的抗菌活性。所有浓度的ZnO NP均表现出细胞毒性活性,而在初始浓度的约1/32和1/64时,100%的THP - 1细胞在存在Ag NP的情况下仍保持存活。然而,在8/2比例下,初始浓度约1/16时约39.94%的细胞存活,初始浓度约1/32时100%的THP - 1细胞存活。

结论

尽管Ag NP表现出低细胞毒性,但它们在体外无法抑制Mtb生长。ZnO NP表现出强大的抗Mtb活性并抑制细菌生长,但对人巨噬细胞具有高细胞毒性。通过按8/2的比例混合Ag和ZnO NP,我们获得了一种对Mtb具有强大抗菌活性且对THP - 1细胞无细胞毒性作用的混合物,并导致体外和体内Mtb生长均受到抑制(图1 - 3,表1 - 3)。

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