From Christian de Duve to Yoshinori Ohsumi: More to autophagy than just dining at home

Harnett, Margaret M.; Pineda, Miguel A.; Laté, Perle Latré de; Eason, Russell J.; Besteiro, Sébastien; Harnett, William; Langsley, Gordon

doi:10.1016/j.bj.2016.12.004

Cited by 51 publications

(38 citation statements)

References 170 publications

(246 reference statements)

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“…Consistent with this, ES-62 can rewire BM progenitors and stromal cells from CIA mice to an anti-inflammatory, regulatory or tissue repair phenotype 2,39,43,46,76,77 by subverting TLR4 signalling to prevent the up-regulation of the key TLR signal transducer, MyD88 observed during chronic inflammation 78,79 . Interestingly, therefore, given the increased incidence and severity of CIA in ES-62-ABX mice, we show that ES-62 dampening of aberrant MyD88 expression is abolished by ABX treatment and indeed, that MyD88 is expressed at equivalent levels in BM from PBS-CIA, PBS-ABX and ES-62-ABX mice (Fig.…”

Section: Es-62 Protects Against Gut Pathology In Ciasupporting

confidence: 55%

The parasitic worm product ES-62 normalises the gut microbiota/bone marrow axis in inflammatory arthritis

Doonan

Tarafdar

Pineda

et al. 2018

Preprint

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The human immune system has evolved in the context of our colonisation by bacteria, viruses, fungi and parasitic helminths. Reflecting this, the rapid eradication of pathogens appears to have resulted in reduced microbiome diversity and generation of chronically activated immune systems, presaging the recent rise of allergic, autoimmune and metabolic disorders. Certainly, gastrointestinal helminths can protect against gut and lung mucosa inflammatory conditions by modulating the microbiome and suppressing the chronic inflammation associated with dysbiosis. Here, we employ ES-62, an immunomodulator secreted by tissue-dwelling Acanthocheilonema viteae to show that modulation of the gut microbiome does not require live infection with gastrointestinal-based helminths nor is protection restricted to mucosal diseases.Specifically, subcutaneous administration of this defined parasitic worm product affords protection against joint disease in collagen-induced arthritis, a mouse model of rheumatoid arthritis, which is associated with normalisation of gut microbiota and prevention of loss of intestinal barrier integrity.

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Section: Es-62 Protects Against Gut Pathology In Ciasupporting

confidence: 55%

The parasitic worm product ES-62 normalises the gut microbiota/bone marrow axis in inflammatory arthritis

Doonan

Tarafdar

Pineda

et al. 2018

Preprint

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“…Lysosomes contain hydrolases that participate in the digestion of substrates that come either from outside or from inside the cell. Autophagy has been initially defined by Christian De Duve as a self-eating process, i.e., a process allowing cell to digest and recycle unnecessary or harmful intracellular components, in opposition with heterophagy, a process allowing cells to degrade extracellular material [76]. Although once considered an exclusive degradative process, it is now acknowledged that autophagy has also important signaling and metabolic function, being able to finely tune the degradation of specific substrates according to cellular needs.…”

Section: Secretory Autophagymentioning

confidence: 99%

Lysosomal Exocytosis, Exosome Release and Secretory Autophagy: The Autophagic- and Endo-Lysosomal Systems Go Extracellular

Buratta

Tancini

Sagini

et al. 2020

IJMS

235

162

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Beyond the consolidated role in degrading and recycling cellular waste, the autophagic-and endo-lysosomal systems play a crucial role in extracellular release pathways. Lysosomal exocytosis is a process leading to the secretion of lysosomal content upon lysosome fusion with plasma membrane and is an important mechanism of cellular clearance, necessary to maintain cell fitness. Exosomes are a class of extracellular vesicles originating from the inward budding of the membrane of late endosomes, which may not fuse with lysosomes but be released extracellularly upon exocytosis. In addition to garbage disposal tools, they are now considered a cell-to-cell communication mechanism. Autophagy is a cellular process leading to sequestration of cytosolic cargoes for their degradation within lysosomes. However, the autophagic machinery is also involved in unconventional protein secretion and autophagy-dependent secretion, which are fundamental mechanisms for toxic protein disposal, immune signalling and pathogen surveillance. These cellular processes underline the crosstalk between the autophagic and the endosomal system and indicate an intersection between degradative and secretory functions. Further, they suggest that the molecular mechanisms underlying fusion, either with lysosomes or plasma membrane, are key determinants to maintain cell homeostasis upon stressing stimuli. When they fail, the accumulation of undigested substrates leads to pathological consequences, as indicated by the involvement of autophagic and lysosomal alteration in human diseases, namely lysosomal storage disorders, age-related neurodegenerative diseases and cancer. In this paper, we reviewed the current knowledge on the functional role of extracellular release pathways involving lysosomes and the autophagic-and endo-lysosomal systems, evaluating their implication in health and disease.

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“…They facilitate degradation of extracellular material as well as intracellular components and contribute to many other key cellular processes such as plasma membrane repair, cholesterol homeostasis, antigen presentation, and cell death (Xu and Ren 2015). The fundamental pathophysiological relevance of lysosomal function is highlighted by the fact that the Nobel Prize for Physiology or Medicine has been granted twice for lysosomal research to Christian de Duve for their initial discovery as organelles (Bainton 1981) and, more recently, to Yoshinori Oshumi for elucidation of the process of autophagy (Harnett et al 2017).…”

Section: The Lysosomementioning

confidence: 99%

Characterizing Adversity of Lysosomal Accumulation in Nonclinical Toxicity Studies: Results from the 5th ESTP International Expert Workshop

et al. 2018

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Lysosomes have a central role in cellular catabolism, trafficking, and processing of foreign particles. Accumulation of endogenous and exogenous materials in lysosomes represents a common finding in nonclinical toxicity studies. Histologically, these accumulations often lack distinctive features indicative of lysosomal or cellular dysfunction, making it difficult to consistently interpret and assign adverse dose levels. To help address this issue, the European Society of Toxicologic Pathology organized a workshop where representative types of lysosomal accumulation induced by pharmaceuticals and environmental chemicals were presented and discussed. The expert working group agreed that the diversity of lysosomal accumulations requires a case-by-case weight-of-evidence approach and outlined several factors to consider in the adversity assessment, including location and type of cell affected, lysosomal contents, severity of the accumulation, and related pathological effects as evidence of cellular or organ dysfunction. Lysosomal accumulations associated with cytotoxicity, inflammation, or fibrosis were generally considered to be adverse, while those found in isolation (without morphologic or functional consequences) were not. Workshop examples highlighted the importance of thoroughly characterizing the biological context of lysosomal effects, including mechanistic data and functional in vitro readouts if available. The information provided here should facilitate greater consistency and transparency in the interpretation of lysosomal effects.

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From Christian de Duve to Yoshinori Ohsumi: More to autophagy than just dining at home

Cited by 51 publications

References 170 publications

The parasitic worm product ES-62 normalises the gut microbiota/bone marrow axis in inflammatory arthritis

The parasitic worm product ES-62 normalises the gut microbiota/bone marrow axis in inflammatory arthritis

Lysosomal Exocytosis, Exosome Release and Secretory Autophagy: The Autophagic- and Endo-Lysosomal Systems Go Extracellular

Characterizing Adversity of Lysosomal Accumulation in Nonclinical Toxicity Studies: Results from the 5th ESTP International Expert Workshop

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