Inhibition of inflammasome activation by a clinical strain of Klebsiella pneumoniae impairs efferocytosis and leads to bacterial dissemination

Codo, Ana Campos; Saraiva, Amanda Correia; Santos, Leonardo Lima dos; Visconde, Marina Francisco; Gales, Ana Cristina; Zamboni, Dario S.; Medeiros, Alexandra I.

doi:10.1038/s41419-018-1214-5

Cited by 37 publications

(39 citation statements)

References 52 publications

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“…Furthermore, by S. aureus secretes alpha‐toxin that reduces CCN1 expression in the lung and alters surface localization of DD1α in aveolar macrophages, both of which reduce efferocytosis of infected neutrophils and thus promote bacterial dissemination 125 . K. pneumoniae on the other hand evades killing by inducing IL‐10 production, which reduces pyroptosis of infected cells and subsequent efferocytosis 126 . In summary, these findings reveal highly context depended outcomes for the efferocytosis of infected cells.…”

Section: Effector Mechanisms Of Cell Deathmentioning

confidence: 72%

Cross talk between intracellular pathogens and cell death

Demarco

Chen

Brož

2020

Immunological Reviews

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Infections with bacterial pathogens often results in the initiation of programmed cell death as part of the host innate immune defense, or as a bacterial virulence strategy. Induction of host cell death is controlled by an elaborate network of innate immune and cell death signaling pathways and manifests in different morphologically and functionally distinct forms of death, such as apoptosis, necroptosis, NETosis and pyroptosis. The mechanism by which host cell death restricts bacterial replication is highly cell‐type and context depended, but its physiological importance is highlighted the diversity of strategies bacterial pathogens use to avoid induction of cell death or to block cell death signaling pathways. In this review, we discuss the latest insights into how bacterial pathogens elicit and manipulate cell death signaling, how different forms of cell death kill or restrict bacteria and how cell death and innate immune pathway cross talk to guard against pathogen‐induced inhibition of host cell death.

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Section: Effector Mechanisms Of Cell Deathmentioning

confidence: 72%

Cross talk between intracellular pathogens and cell death

Demarco

Chen

Brož

2020

Immunological Reviews

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“…It is possible that coordination of macrophages with additional immune cells and cytokines in concert may be required for the full capability of antibody-mediated opsonophagocytosis to be realized (50)(51)(52)(53). Additionally, alveolar macrophages or inflammatory monocytes may have improved lysosomal capabilities relative to standard BMDMs (54), or macrophages may clear phagocytized bacteria self-destruction via autophagy or pyroptosis (50,51).…”

Section: Discussionmentioning

confidence: 99%

The Role of IgG Subclass in Antibody-Mediated Protection against Carbapenem-Resistant Klebsiella pneumoniae

Motley

Diago-Navarro

Banerjee

et al. 2020

mBio

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Monoclonal antibodies (MAbs) have the potential to assist in the battle against multidrug-resistant bacteria such as carbapenem-resistant Klebsiella pneumoniae (CR-Kp). However, the characteristics by which these antibodies (Abs) function, such as the role of antibody subclass, must be determined before such modalities can be carried from the bench to the bedside. We performed a subclass switch on anticapsular monoclonal murine IgG3 (mIgG3) hybridomas and identified and purified a murine IgG1 (mIgG1) hybridoma line through sib selection. We then compared the ability of the mIgG1 and mIgG3 antibodies to control CR-Kp sequence type 258 (ST258) infection both in vitro and in vivo. We found by enzyme-limited immunosorbent assay (ELISA) and flow cytometry that mIgG3 has superior binding to the CR-Kp capsular polysaccharide (CPS) and superior agglutinating ability compared to mIgG1. The mIgG3 also, predictably, had better complement-mediated serum bactericidal activity than the mIgG1 and also promoted neutrophil-mediated killing at concentrations lower than that of the mIgG1. In contrast, the mIgG1 had marginally better activity in improving macrophage-mediated phagocytosis. Comparing their activities in a pulmonary infection model with wild-type as well as neutropenic mice, both antibodies reduced organ burden in a nonlethal challenge, regardless of neutrophil status, with mIgG1 having the highest overall burden reduction in both scenarios. However, at a lethal inoculum, both antibodies showed reduced efficacy in neutropenic mice, with mIgG3 retaining the most activity. These findings suggest the viability of monoclonal Ab adjunctive therapy in neutropenic patients that cannot mount their own immune response, while also providing some insight into the relative contributions of immune mediators in CR-Kp protection. IMPORTANCE Carbapenem-resistant Klebsiella pneumoniae is an urgent public health threat that causes life-threatening infections in immunocompromised hosts. Its resistance to nearly all antibiotics necessitates novel strategies to treat it, including the use of monoclonal antibodies. Monoclonal antibodies are emerging as important adjuncts to traditional pharmaceuticals, and studying how they protect against specific bacteria such as Klebsiella pneumoniae is crucial to their development as effective therapies. Antibody subclass is often overlooked but is a major factor in how an antibody interacts with other mediators of immunity. This paper is the first to examine how the subclass of anticapsular monoclonal antibodies can affect efficacy against CR-Kp. Additionally, this work sheds light on the viability of monoclonal antibody therapy in neutropenic patients, who are most vulnerable to CR-Kp infection.

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“…However, we were unable to obtain tissue samples and had to concentrate on circulating monocytes, which are simple enough to obtain, and study gene expression rather than protein levels due to the lack of biological material. In addition to the inability of studying macrophages we must also add that unfortunately, only anecdotical reports (20,21) have dealt with the role of inflammasomes regarding strains of resistant bacteria, so our hypothesis of "abnormal normality" has to be verified with a more conspicuous number of patients.…”

Section: Discussionmentioning

confidence: 99%