Competitive Cell Death Interactions in Pulmonary Infection: Host Modulation Versus Pathogen Manipulation

FitzGerald, Ethan S.; Luz, Nívea F.; Jamieson, Amanda M.

doi:10.3389/fimmu.2020.00814

Cited by 18 publications

(15 citation statements)

References 173 publications

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“…Ku et al demonstrated that cell fusion acts as a damage-associated molecular pattern (DAMP), triggering the cGAS-STING pathway that leads to autophagic cell death [ 34 ]. The presence of bacterial effectors that manipulate cell death pathways has not been established but it is likely that they exist in some capacity, based on the successful intracellular lifestyle of Bpm and the wide array of weaponry the pathogen uses within the cell [ 43 ]. The shift from active to persister bacteria would shut down the cytoprotection and manipulation exhibited by Bpm and cause the MNGC to undergo cell death, creating foci of necrosis and inflammation, similar to those seen at the center of the mature granuloma-like lesions of chronic melioidosis patients.…”

Section: Role Of Mngcs In Diseasementioning

confidence: 99%

Multinucleated Giant Cell Formation as a Portal to Chronic Bacterial Infections

Stockton

Torres

2020

Microorganisms

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This review provides a snapshot of chronic bacterial infections through the lens of Burkholderia pseudomallei and detailing its ability to establish multi-nucleated giant cells (MNGC) within the host, potentially leading to the formation of pyogranulomatous lesions. We explore the role of MNGC in melioidosis disease progression and pathology by comparing the similarities and differences of melioidosis to tuberculosis, outline the concerted events in pathogenesis that lead to MNGC formation, discuss the factors that influence MNGC formation, and consider how they fit into clinical findings reported in chronic cases. Finally, we speculate about future models and techniques that can be used to delineate the mechanisms of MNGC formation and function.

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Section: Role Of Mngcs In Diseasementioning

confidence: 99%

Multinucleated Giant Cell Formation as a Portal to Chronic Bacterial Infections

Stockton

Torres

2020

Microorganisms

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“…PcpA (pneumococcal choline-binding protein A) may also play a certain role [ 10 ]. Recent studies also demonstrated the ability of the pathogen to induce apoptosis, necroptosis and pyroptosis [ 15 ].…”

Section: Discussionmentioning

confidence: 99%

“…Although there are numerous studies on the molecular biology of the microbiological agents causing pneumonia, defense mechanisms of the host [ 1 , 7 – 15 ] and the treatment of the disease, studies on the pathology, cause, course and epidemiology of lobar pneumonia are lacking since the middle of the 1970s. The objectives of this work were therefore to re-study the lung changes in lobar pneumonia in relation to the cause and duration of the disease in a large number of autopsies.…”

Section: Introductionmentioning

confidence: 99%

Lobar (croupous) pneumonia: old and new data

et al. 2021

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Background and aim Pneumonia remains one of the most frequent death causes worldwide. Among the etiological factors S. pneumoniae -causing lobar pneumonia plays a leading role. According to current textbook knowledge at least three sequential stages of lobar pneumonia are distinguished: congestion, red hepatization and gray hepatization. However, there are no detailed data supporting this stage concept. There are also controversial views on its etiology. In this study, the lung changes in lobar pneumonia were related to the cause and duration of the disease. In addition, the complications of the disease were evaluated. PCR studies verified the etiology of pneumonia. Material and methods Lobar pneumonia was analyzed in 252 post mortem cases examined in a large hospital in Irkutsk. The pathology, etiology of pneumonia, course of disease and cause of death were recorded and correlated to its clinical course and duration. In the second part of the study, the results in 95 patients were analyzed in detail and related to PCR findings. Results Most patients were adult men of low social status who showed signs of severe alcoholism. Lobar pneumonia was observed in 85% of the patients, while the remaining patients showed sublobar (“lobular”, focal) lung involvement. Histologically, three patterns of inflammation were observed, which in most patients occurred concurrently in different parts of the involved lobe: “congestion”, characterized by serous exudation with multiple cocci (41% of cases), “red hepatization” (41% of cases) and “gray hepatization” (100% of cases). The latter pattern was subdivided into three subgroups according to the ratio of fibrin—neutrophils and the presence of macrophages. The mean number of different histological patterns observed per patient was 3.8. There was no correlation between the inflammatory patterns and the duration of the disease. In 23% of the patients, the cause of death was of pulmonary origin, while the remaining patients died of extrapulmonary complications (i.e. acute heart failure 26%, acute vascular insufficiency 15% purulent meningitis 11–24.3%. In 29/95 patients (20 with lobar and 9 with focal pneumonia) pneumococcal etiology of pneumonia was established by PCR. Conclusion Lobar pneumonia is a distinct clinico-pathological entity caused by S. pneumoniae , demonstrated by PCR testing and/or cytological examinations. Bacteriologic studies frequently give falsenegative results. Lobar pneumonia is characterized by three main histopathological patterns (congestion or microbeous edema, and red and gray hepatization) which usually occur side by side and not in chronological order. Early death is often related to heart failure and septic shock, while meningitis is a frequent complication later in the course.

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“…In cancer, anoikis resistance characterizes cancer cell anchorageindependent growth and EMT, contributing to cancer cell invasion and metastasis (62,64,65). In inflammatory diseases, as cardiovascular (66), pulmonary (67) and skin (49) diseases, and diabetes-related cardiovascular complications and retinopathy (62), aberrant anoikis is involved in excessive cell death and tissue injury.…”

Section: Granzyme B and Perforin-dependent And/or Perforin-independenmentioning

confidence: 99%

Granzyme B in Inflammatory Diseases: Apoptosis, Inflammation, Extracellular Matrix Remodeling, Epithelial-to-Mesenchymal Transition and Fibrosis

et al. 2020

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Inflammation is strictly interconnected to anti-inflammatory mechanisms to maintain tissue homeostasis. The disruption of immune homeostasis can lead to acute and chronic inflammatory diseases, as cardiovascular, pulmonary, metabolic diseases and cancer. The knowledge of the mechanisms involved in the development and progression of these pathological conditions is important to find effective therapies. Granzyme B (GrB) is a serine protease produced by a variety of immune, non-immune and tumor cells. Apoptotic intracellular and multiple extracellular functions of GrB have been recently identified. Its capability of cleaving extracellular matrix (ECM) components, cytokines, cell receptors and clotting proteins, revealed GrB as a potential multifunctional pro-inflammatory molecule with the capability of contributing to the pathogenesis of different inflammatory conditions, including inflammaging, acute and chronic inflammatory diseases and cancer. Here we give an overview of recent data concerning GrB activity on multiple targets, potentially allowing this enzyme to regulate a wide range of crucial biological processes that play a role in the development, progression and/or severity of inflammatory diseases. We focus our attention on the promotion by GrB of perforin-dependent and perforin-independent (anoikis) apoptosis, inflammation derived by the activation of some cytokines belonging to the IL-1 cytokine family, ECM remodeling, epithelial-to-mesenchymal transition (EMT) and fibrosis. A greater comprehension of the pathophysiological consequences of GrB-mediated multiple activities may favor the design of new therapies aim to inhibit different inflammatory pathological conditions such as inflammaging and age-related diseases, EMT and organ fibrosis.

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Competitive Cell Death Interactions in Pulmonary Infection: Host Modulation Versus Pathogen Manipulation

Cited by 18 publications

References 173 publications

Multinucleated Giant Cell Formation as a Portal to Chronic Bacterial Infections

Multinucleated Giant Cell Formation as a Portal to Chronic Bacterial Infections

Lobar (croupous) pneumonia: old and new data

Granzyme B in Inflammatory Diseases: Apoptosis, Inflammation, Extracellular Matrix Remodeling, Epithelial-to-Mesenchymal Transition and Fibrosis

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