Beta-lactam antibiotics modulate T-cell functions and gene expression via covalent binding to cellular albumin

Mor, Felix; Cohen, Irun R.

doi:10.1073/pnas.1215722110

Cited by 22 publications

(21 citation statements)

References 46 publications

(42 reference statements)

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“…While the first report from 2011 was verified and germ free mice showed either complete resistance or attenuation of EAE in several experimental paradigms 46–48 , using antibiotic cocktails to deplete gut microbiota has provided controversial results. Even though most of the antibiotic administration studies have shown an amelioration of EAE pointing to a disease promoting effect of gut bacteria 49–51 , experimental evidence suggests that certain bacterial strains have a beneficial effect on EAE development and protect from exacerbated disease, as shown in treatment experiments using the macrolide antibiotics clarithromycine and azithromycin or the cephalosporine cefuroxime 52,53 .…”

Section: The Gut Microbiome and Dietary Factorsmentioning

confidence: 99%

Environmental control of autoimmune inflammation in the central nervous system

Rothhammer

Quintana

2016

Current Opinion in Immunology

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Summary Multiple Sclerosis (MS) is a chronic autoimmune inflammatory demyelinating disorder of the central nervous system (CNS), which causes severe disability and requires extensive medical attention and treatment. While the infiltration of pathogenic immune cells into the CNS leads to the formation of inflammatory lesions in its initial relapsing-remitting stage, late stages of MS are characterized by progressive neuronal loss and demyelination even without continued interaction with the peripheral immune compartment. Several genetic and environmental factors modulate and influence these processes on multiple levels. Genetic variants confer a predisposition for the development of MS, but are not accessible to therapeutic intervention as of today. However, migration studies suggest that environmental factors influence disease development, activity and progression. This article reviews mechanisms of disease pathogenesis in MS and their modulation by environmental factors such as geographical localization, the gut microbiome and the diet.

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Section: The Gut Microbiome and Dietary Factorsmentioning

confidence: 99%

Environmental control of autoimmune inflammation in the central nervous system

Rothhammer

Quintana

2016

Current Opinion in Immunology

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“…Interestingly, ceftriaxone has had no impact on the EAAT2 protein expression levels in several brain areas as well as on the glutamate uptake rate suggesting that in this model the positive effects of the antibiotic are not mediated through the modulation of glutamate concentration. Moreover, it seems that even the individual antibiotics within the β-lactam group may display differential immunomodulatory properties (Mor and Cohen, 2013). This mechanism operates via covalent binding of various β-lactams to cellular albumin and subsequent modulation of T cell function and gene expression.…”

Section: β-Lactamsmentioning

confidence: 99%

Biotic acts of antibiotics

Aminov¹

2013

Front. Microbiol.

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Biological functions of antibiotics are not limited to killing. The most likely function of antibiotics in natural microbial ecosystems is signaling. Does this signaling function of antibiotics also extend to the eukaryotic – in particular mammalian – cells? In this review, the host modulating properties of three classes of antibiotics (macrolides, tetracyclines, and β-lactams) will be briefly discussed. Antibiotics can be effective in treatment of a broad spectrum of diseases and pathological conditions other than those of infectious etiology and, in this capacity, may find widespread applications beyond the intended antimicrobial use. This use, however, should not compromise the primary function antibiotics are used for. The biological background for this inter-kingdom signaling is also discussed.

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“…In this context, it is thought that some antibiotic compounds may directly stimulate the host immune system [16,17]. The current TB chemotherapy contains four first-line antibiotics namely, rifampicin, ethambutol, pyrazinamide and isoniazid.…”

Section: Introductionmentioning

confidence: 99%

“…In addition to antibiotics, which are major therapeutic tools to promote further suppression of mycobacterial growth [13], host-targeted interventions have also been proposed as novel approaches to enhance control of TB [14,15]. In this context, it is thought that some antibiotic compounds may directly stimulate the host immune system [16,17] [27]. In that study, the authors have demonstrated a role for host autophagy as an essential requirement to the bactericidal activity of INH in H37Rv-infected murine macrophages.…”

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confidence: 99%

Isoniazid‐induced control of Mycobacterium tuberculosis by primary human cells requires interleukin‐1 receptor and tumor necrosis factor

et al. 2016

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Proinflammatory cytokines are critical mediators that control Mycobacterium tuberculosis (Mtb) growth during active tuberculosis (ATB). To further inhibit bacterial proliferation in diseased individuals, drug inhibitors of cell wall synthesis such as isoniazid (INH) areemployed. However, whether INH presents an indirect effect on bacterial growth by regulating host cytokines during ATB is not well known. To examine this hypothesis, we used an in vitro human granuloma system generated with primary leukocytes from healthy donors adapted to model ATB. Intense Mtb proliferation in cell cultures was associated with monocyte/macrophage activation and secretion of IL-1β and TNF. Treatment with INH significantly reduced Mtb survival, but altered neither T-cell-mediated Mtb killing, nor production of IL-1β and TNF. However, blockade of both IL-1R1 and TNF signaling rescued INH-induced killing, suggesting synergistic roles of these cytokines in mediating control of Mtb proliferation. Additionally, mycobacterial killing by INH was highly dependent upon drug activation by the pathogen catalase-peroxidase KatG and involved a host PI3K-dependent pathway. Finally, experiments using coinfected (KatG-mutated and H37Rv strains) cells suggested that active INH does not directly enhance host-mediated killing of Mtb. Our results thus indicate that Mtb-stimulated host IL-1 and TNF have potential roles in TB chemotherapy.Keywords: Human r IL-1 r TNF r Isoniazid r Leukocytes r Mycobacterium tuberculosis Additional supporting information may be found in the online version of this article at the publisher's web-site IntroductionUpon Mycobacterium tuberculosis (Mtb) exposure, it is estimated that 5-10% of human subjects will develop active tuberculosis Correspondence: Prof. André Báfica e-mail: andre.bafica@ufsc.br (TB) [1], which is characterized by intense pathogen proliferation associated with cellular activation and cell death. Cellular structures known as necrotic granulomas may promote bacterial dissemination and enhance Mtb transmission [2,3]. On the other hand, counter balance is supported by host recognition of Mtb, which induces cytokines such as IL-1β and TNF [4,5], two potent inflammatory mediators that suppress Mtb growth [4,6]. It has C 2016 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim www.eji-journal.eu Eur. J. Immunol. 2016. 46: 1936-1947 Immunity to infection 1937 been shown that these cytokines regulate intracellular bacterial growth in human macrophages, whether by recruitment of antimicrobial effector molecules [7] or induction of apoptotic cell death [8]. In conjunction with 9], IL-1β, and TNF can provide signals to help differentiation and antigen presentation by macrophages [6,10,11]. Moreover, the adverse outcome of latent TB reactivation observed in clinical trials with anti-TNF therapies, additionally confirmed the essential role of TNF for controlling Mtb growth in humans [12]. In addition to antibiotics, which are major therapeutic tools to promote further suppression of mycobacterial growth [13], host-targeted i...

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Beta-lactam antibiotics modulate T-cell functions and gene expression via covalent binding to cellular albumin

Cited by 22 publications

References 46 publications

Environmental control of autoimmune inflammation in the central nervous system

Environmental control of autoimmune inflammation in the central nervous system

Biotic acts of antibiotics

Isoniazid‐induced control of Mycobacterium tuberculosis by primary human cells requires interleukin‐1 receptor and tumor necrosis factor

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