Infiltrated Macrophages Die of Pneumolysin-Mediated Necroptosis following Pneumococcal Myocardial Invasion

Gilley, Ryan P.; González-Juarbe, Norberto; Shenoy, A.T.; Reyes, Luis Felipe; Dube, Peter H.; Restrepo, Marcos I.; Orihuela, Carlos J.

doi:10.1128/iai.00007-16

Cited by 61 publications

(73 citation statements)

References 44 publications

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“…After crossing the vascular endothelium, S. pneumoniae damages the myocardium, creating bacterium-associated microlesions. Our published studies using immunofluorescence microscopy suggest that this begins with the interaction of a single pneumococcus with surrounding cardiomyocytes (15). A trypan blue exclusion assay showed that at a low multiplicity of infection (MOI), i.e., less than 10 bacteria per cardiomyocyte, S. pneumoniae was able to induce cell death in approximately 60% of HL-1 cardiomyocytes after 6 h of infection in vitro, without detachment (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…S2). Pneumolysin is a pore-forming toxin produced by S. pneumoniae (24), and its role in cardiomyocyte killing has already been demonstrated, albeit at late stages of microlesion formation or when administered extracellularly (13,15). In contrast, SpxB is a metabolic enzyme that generates H 2 O 2 as a result of converting pyruvate to acetylphosphate.…”

Section: Resultsmentioning

confidence: 99%

“…This most likely reflects the events that occur in the heart following bacterial translocation into the myocardium from the bloodstream and serves as a basis of a working model in which cardiomyocytes might serve as a protective niche, following cardiac invasion, that allows S. pneumoniae to replicate while avoiding immune system or host defenses. Ultimately, cardiomyocyte killing occurs from inside the cell, and as documented for mature lesions, bacteria that emerge are able to kill immune cells with extracellular release of pneumolysin (15).…”

Section: Discussionmentioning

confidence: 99%

“…pneumoniae is thought to invade the heart through the coronary circulation, as most pneumococci detected within the myocardium are close to the vascular network (13,15). Interaction of S. pneumoniae with endothelial cells has been extensively studied as a part of S. pneumoniae translocation across the blood-brain barrier (BBB), which occurs during the development of pneumococcal meningitis (16).…”

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Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

et al. 2018

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Streptococcus pneumoniae (the pneumococcus) is the leading cause of community-acquired pneumonia and is now recognized to be a direct contributor to adverse acute cardiac events. During invasive pneumococcal disease, S. pneumoniae can gain access to the myocardium, kill cardiomyocytes, and form bacterium-filled "microlesions" causing considerable acute and long-lasting cardiac damage. While the molecular mechanisms responsible for bacterial translocation into the heart have been elucidated, the initial interactions of heart-invaded S. pneumoniae with cardiomyocytes remain unclear. In this study, we used a model of low multiplicity of S. pneumoniae infection with HL-1 mouse cardiomyocytes to investigate these early events. Using adhesion/invasion assays and immunofluorescent and transmission electron microscopy, we showed that S. pneumoniae rapidly adhered to and invaded cardiomyocytes. What is more, pneumococci existed as intravacuolar bacteria or escaped into the cytoplasm. Pulse-chase assays with BrdU confirmed intracellular replication of pneumococci within HL-1 cells. Using endocytosis inhibitors, bacterial isogenic mutants, and neutralizing antibodies against host proteins recognized by S. pneumoniae adhesins, we showed that S. pneumoniae uptake by cardiomyocytes is not through the well-studied canonical interactions identified for vascular endothelial cells. Indeed, S. pneumoniae invasion of HL-1 cells occurred through clathrin-mediated endocytosis (CME) and independently of choline binding protein A (CbpA)/laminin receptor, CbpA/polymeric immunoglobulin receptor, or cell wall phosphorylcholine/platelet-activating factor receptor. Subsequently, we determined that pneumolysin and streptococcal pyruvate oxidasederived H 2 O 2 production were required for cardiomyocyte killing. Finally, we showed that this cytotoxicity could be abrogated using CME inhibitors or antioxidants, attesting to intracellular replication of S. pneumoniae as a key first step in pneumococcal pathogenesis within the heart. KEYWORDS Cardiac acute events, cardiomyocytes, invasive pneumococcal disease, Streptococcus pneumoniae, facultatively intracellular pathogens, oxidative stress S treptococcus pneumoniae (the pneumococcus) is a Gram-positive bacterium which typically colonizes the nasopharynx asymptomatically (1, 2). However, it is also an opportunistic pathogen, capable of causing a wide spectrum of human diseases, including otitis media, community-acquired pneumonia, bacteremia/sepsis, and meningitis (3-5). In 30% of adults with pneumococcal pneumonia, S. pneumoniae escapes the airway and causes bacteremia/invasive pneumococcal disease (IPD). This typically occurs in those who are Ն65 years of age and/or in some fashion immunocompromised (4). Despite development and use of multiple antipneumococcal vaccines for decades, S. pneumoniae remains a major cause of human morbidity and death worldwide (6).Approximately 20% of adults hospitalized for severe pneumococcal disease experience some sort of major adverse cardiac events (MA...

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

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“…Several bacterial pathogens with pore-forming toxins induce macrophage necroptosis, a pro-inflammatory mode of cell death regulated by receptor interacting protein kinases RIP1 and RIP3 and mediated by the effector mixed-lineage kinase domain-like protein MLKL; macrophages deficient in MLKL are consequently resistant to pore-forming toxin-induced cell death. Treatment of mice with necrostatin-5, an inhibitor of RIP1 and/or GW806742X, an inhibitor of MLKL, reduced severity of Serratia marcescens pneumonia in mice, protecting alveolar macrophages from cell death and reducing bacterial burden [33]; necrostatin-5 also reduced pneumolysin-mediated macrophage necroptosis and cardiac damage following pneumococcal bacteremia and myocardial invasion [34]. …”

Section: Neutralization Of Virulence Factors: Disarming the Pathogenmentioning

confidence: 99%

Pharmacological Targeting of the Host–Pathogen Interaction: Alternatives to Classical Antibiotics to Combat Drug-Resistant Superbugs

Munguia

Nizet

2017

Trends in Pharmacological Sciences

105

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The rise of multidrug-resistant pathogens and the dearth of new antibiotic development place an existential strain on successful infectious disease therapy. Breakthrough strategies that go beyond classical antibiotic mechanisms are needed to combat this looming public health catastrophe. Reconceptualizing antibiotic therapy in the richer context of the host-pathogen interaction is required for innovative solutions. By defining specific virulence factors, the essence of a pathogen, and pharmacologically neutralizing their activities, one can block disease progression and sensitize microbes to immune clearance. Likewise, host-directed strategies to boost phagocyte bactericidal activity, enhance leukocyte recruitment, or reverse pathogen-induced immunosuppression seek to replicate the success of cancer immunotherapy in the field of infectious diseases. The answer to the threat of multidrug-resistant pathogens lies “outside-the-box” of current antibiotic paradigms.

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Consequences of Pneumonia in Older Adults

Orihuela

McElhaney

Bowdish

2021

Encyclopedia of Gerontology and Population Aging

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Infiltrated Macrophages Die of Pneumolysin-Mediated Necroptosis following Pneumococcal Myocardial Invasion

Cited by 61 publications

References 44 publications

Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

Pharmacological Targeting of the Host–Pathogen Interaction: Alternatives to Classical Antibiotics to Combat Drug-Resistant Superbugs

Consequences of Pneumonia in Older Adults

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Infiltrated Macrophages Die of Pneumolysin-Mediated Necroptosis following Pneumococcal Myocardial Invasion

Cited by 61 publications

References 44 publications

Cell Invasion and Pyruvate Oxidase-Derived H 2 O 2 Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

Cell Invasion and Pyruvate Oxidase-Derived H 2 O 2 Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

Pharmacological Targeting of the Host–Pathogen Interaction: Alternatives to Classical Antibiotics to Combat Drug-Resistant Superbugs

Consequences of Pneumonia in Older Adults

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Product

Resources

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Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing

Cell Invasion and Pyruvate Oxidase-Derived H ₂ O ₂ Are Critical for Streptococcus pneumoniae-Mediated Cardiomyocyte Killing