Metabolic functions of glycosomes in trypanosomatids

Michels, Paul A.M.; Bringaud, Frédéric; Herman, Murielle; Hannaert, Véronique

doi:10.1016/j.bbamcr.2006.08.019

Cited by 298 publications

(285 citation statements)

References 104 publications

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“…These include the glycosomes, peroxisome-related microbodies that contain enzymes of several important metabolic pathways including glycolysis, the pentose-phosphate pathway, b-oxidation of fatty acids, gluconeogenesis, purine salvage, and biosynthesis of pyrimidines, ether lipids and squalenes. 23 Compartmentalization of metabolic pathways in this manner prevents the accumulation of toxic intermediates which would otherwise damage the cell, 24 and is also thought to facilitate rapid metabolic adaptation in response to changing environments. 23 Studies in both Leishmania and trypanosomes have shown that proper biogenesis of glycosomes and the correct targeting of glycosomal enzymes are essential for parasite survival, [24][25][26][27][28][29] making these unique organelles an attractive drug target.…”

Section: Introductionmentioning

confidence: 99%

Glycosome turnover inLeishmania majoris mediated by autophagy

et al. 2014

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Abbreviations: ATG, autophagy-related; GFP, green fluorescent protein; mC, mCherry fluorescent protein; MVT, multivesicular tubule; RFP, red fluorescent protein; TEM, transmission electron microscopy.Autophagy is a central process behind the cellular remodeling that occurs during differentiation of Leishmania, yet the cargo of the protozoan parasite's autophagosome is unknown. We have identified glycosomes, peroxisome-like organelles that uniquely compartmentalize glycolytic and other metabolic enzymes in Leishmania and other kinetoplastid parasitic protozoa, as autophagosome cargo. It has been proposed that the number of glycosomes and their content change during the Leishmania life cycle as a key adaptation to the different environments encountered. Quantification of RFP-SQL-labeled glycosomes showed that promastigotes of L. major possess »20 glycosomes per cell, whereas amastigotes contain »10. Glycosome numbers were significantly greater in promastigotes and amastigotes of autophagy-defective L. major Datg5 mutants, implicating autophagy in glycosome homeostasis and providing a partial explanation for the previously observed growth and virulence defects of these mutants. Use of GFP-ATG8 to label autophagosomes showed glycosomes to be cargo in »15% of them; glycosome-containing autophagosomes were trafficked to the lysosome for degradation. The number of autophagosomes increased 10-fold during differentiation, yet the percentage of glycosome-containing autophagosomes remained constant. This indicates that increased turnover of glycosomes was due to an overall increase in autophagy, rather than an upregulation of autophagosomes containing this cargo. Mitophagy of the single mitochondrion was not observed in L. major during normal growth or differentiation; however, mitochondrial remnants resulting from stress-induced fragmentation colocalized with autophagosomes and lysosomes, indicating that autophagy is used to recycle these damaged organelles. These data show that autophagy in Leishmania has a central role not only in maintaining cellular homeostasis and recycling damaged organelles but crucially in the adaptation to environmental change through the turnover of glycosomes.

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Section: Introductionmentioning

confidence: 99%

Glycosome turnover inLeishmania majoris mediated by autophagy

et al. 2014

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“…The subcellular compartmentalization of glycolysis in trypanosomatids is fundamentally different than in all other eukaryotes, where glycolysis ensues cytoplasmically. In trypanosomatids, the majority of glycolytic enzymes are contained in unusual peroxisome-like organelles termed 'glycosomes'; only the terminal three glycolytic enzymes are cytosolic 48,49 (see Figure 3). Thus in trypanosomatids, GAPDH and enolase exist in distinct intracellular locales and are unassociated.…”

Section: Apoptotic Mimicrymentioning

confidence: 99%

“…This 'reversed' behavior was attributable genetically to E1B 19 K. That authentic Bcl-2 could substitute for E1B 19 K, but that it does not program such a reversed behavior in the context of Figure 3 Glycosomal localization of glycolytic enzymes. Enzymes and intermediates of glycolysis that are found within and without the glycosome 48,49 are diagrammed here. Glycosomes are intracellular peroxisome-like organelles of trypanosomatids, constrained by a single lipid bilayer membrane (represented by a double solid line), within which the proximal steps of glycolysis ensue.…”

Section: Reprogrammed Cell Deathmentioning

confidence: 99%

“…Glycosomal contents vary during the heteroxenous trypanosomatid life cycle, and other metabolic processes (including glycerol catabolism) also are localized within. 49 Intraglycosomal glycolytic enzymes are shown as darker (purple) boxes; extraglycosomal (cytosolic) glycolytic enzymes are shown as lighter (blue) boxes. Filled boxes denote those glycolytic enzymes whose mammalian homologs are externalized on the apoptotic cell surface (see Figure 1) uninfected mammalian cells suggests the additional contribution of other adenoviral gene(s).…”

Section: Reprogrammed Cell Deathmentioning

confidence: 99%

See 1 more Smart Citation

Exploiting death: apoptotic immunity in microbial pathogenesis

Ucker

2016

Cell Death Differ

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Innate immunity typically is responsible for initial host responses against infections. Independently, nucleated cells that die normally as part of the physiological process of homeostasis in mammals (including humans) suppress immunity. Specifically, the physiological process of cell death (apoptosis) generates cells that are recognized specifically by viable cells of all types and elicit a profound transient suppression of host immunity (termed 'innate apoptotic immunity' (IAI)). IAI appears to be important normally for the maintenance of self-tolerance and for the resolution of inflammation. In addition, pathogens are able to take advantage of IAI through a variety of distinct mechanisms, to enable their proliferation within the host and enhance pathogenicity. For example, the protist pathogen Leishmania amazonensis, at its infective stage, mimics apoptotic cells by expressing apoptotic-like protein determinants on the cell surface, triggering immunosuppression directly. In contrast, the pathogenic bacterium Listeria monocytogenes triggers cell death in host lymphocytes, relying on those apoptotic cells to suppress host immune control and facilitate bacterial expansion. Finally, although the inhibition of apoptotic cell death is a common attribute of many viruses which facilitates their extended replication, it is clear that adenoviruses also reprogram the non-apoptotic dead cells that arise subsequently to manifest apoptotic-like immunosuppressive properties. These three instances represent diverse strategies used by microbial pathogens to exploit IAI, focusing attention on the potency of this facet of host immune control. Further examination of these cases will be revealing both of varied mechanisms of pathogenesis and the processes involved in IAI control.

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“…Além disso, enzimas relacionadas a outras vias, como β-oxidação de ácidos graxos, recrutamento de purinas e vias biossintéticas para pirimidinas podem estar presentes nos glicossomos (Michels et al, 2006). Outras organelas encontradas no citoplasma de T. cruzi são os reservossomos e os acidocalcisomas.…”

Section: Ultraestruturaunclassified

Caracterização molecular e funcional da imidazolona propionase de <i>Trypanosoma cruzi</i>: uma enzima do metabolismo de histidina.

Melo¹

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Metabolic functions of glycosomes in trypanosomatids

Cited by 298 publications

References 104 publications

Glycosome turnover inLeishmania majoris mediated by autophagy

Glycosome turnover inLeishmania majoris mediated by autophagy

Exploiting death: apoptotic immunity in microbial pathogenesis

Caracterização molecular e funcional da imidazolona propionase de <i>Trypanosoma cruzi</i>: uma enzima do metabolismo de histidina.

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