Publications by authors named "Jan Mach"

Iron, as an essential micronutrient, plays a crucial role in host-pathogen interactions. In order to limit the growth of the pathogen, a common strategy of innate immunity includes withdrawing available iron to interfere with the cellular processes of the microorganism. Against that, unicellular parasites have developed powerful strategies to scavenge iron, despite the effort of the host.

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Primary amoebic meningoencephalitis is a rare but fatal central nervous system (CNS) disease caused by the "brain-eating amoeba" Naegleria fowleri. A major obstacle is the requirement for drugs with the ability to cross the blood-brain barrier, which are used in extremely high doses, cause severe side effects, and are usually ineffective. We discovered that the 4-aminomethylphenoxy-benzoxaborole AN3057 exhibits nanomolar potency against N.

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Unlabelled: The model pennate diatom is able to assimilate a range of iron sources. It therefore provides a platform to study different mechanisms of iron processing concomitantly in the same cell. In this study, we follow the localization of three iron starvation induced proteins (ISIPs) in vivo, driven by their native promoters and tagged by fluorophores in an engineered line of .

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Many of the currently available anti-parasitic and anti-fungal frontline drugs have severe limitations, including adverse side effects, complex administration, and increasing occurrence of resistance. The discovery and development of new therapeutic agents is a costly and lengthy process. Therefore, repurposing drugs with already established clinical application offers an attractive, fast-track approach for novel treatment options.

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Acanthamoeba castellanii is a ubiquitously distributed amoeba that can be found in soil, dust, natural and tap water, air conditioners, hospitals, contact lenses and other environments. It is an amphizoic organism that can cause granulomatous amoebic encephalitis, an infrequent fatal disease of the central nervous system, and amoebic keratitis, a severe corneal infection that can lead to blindness. These diseases are extremely hard to treat; therefore, a more comprehensive understanding of this pathogen's metabolism is essential for revealing potential therapeutic targets.

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Article Synopsis
  • Investigations into how phytoplankton handle iron stress are complex because iron concentrations don't always indicate how available the iron is for them to use.
  • Previous studies have focused on either single species or field samples, making the results difficult to interpret. This study used a cocultivation model to assess competition between species based on different iron levels and forms, as well as nutritional conditions.
  • The research found that a specific dinoflagellate can utilize iron from hydroxamate siderophores, giving it an ecological advantage, and identified a candidate protein related to this iron acquisition strategy, which is not well understood in other eukaryotic phytoplankton.
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The productivity of the ocean is largely dependent on iron availability, and marine phytoplankton have evolved sophisticated mechanisms to cope with chronically low iron levels in vast regions of the open ocean. By analyzing the metabarcoding data generated from the Oceans expedition, we determined how the global distribution of the model marine chlorarachniophyte varies across regions with different iron concentrations. We performed a comprehensive proteomics analysis of the molecular mechanisms underpinning the adaptation of to iron scarcity and report on the temporal response of cells to iron enrichment.

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The transition of free-living organisms to parasitic organisms is a mysterious process that occurs in all major eukaryotic lineages. Parasites display seemingly unique features associated with their pathogenicity; however, it is important to distinguish ancestral preconditions to parasitism from truly new parasite-specific functions. Here, we sequenced the genome and transcriptome of anaerobic free-living Mastigamoeba balamuthi and performed phylogenomic analysis of four related members of the Archamoebae, including Entamoeba histolytica, an important intestinal pathogen of humans.

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Copper is a trace metal that is necessary for all organisms but toxic when present in excess. Different mechanisms to avoid copper toxicity have been reported to date in pathogenic organisms such as Cryptococcus neoformans and Candida albicans. However, little if anything is known about pathogenic protozoans despite their importance in human and veterinary medicine.

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Article Synopsis
  • * Parasitic protists, which rely on their hosts for iron, face challenges in acquiring this nutrient since hosts can starve them by making iron inaccessible.
  • * The review discusses various human parasites' strategies for managing iron, including acquisition, storage, and detoxification, and highlights the potential of iron-targeting treatments for combating these infections.
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Naegleria fowleri is a single-cell organism living in warm freshwater that can become a deadly human pathogen known as a brain-eating amoeba. The condition caused by N. fowleri, primary amoebic meningoencephalitis, is usually a fatal infection of the brain with rapid and severe onset.

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Article Synopsis
  • * The study focused on the marine picoalga Ostreococcus tauri, revealing that it adapts to copper deficiency by altering its copper management without affecting its growth or overall physiology.
  • * Researchers identified a key iron uptake protein, Ot-Fea1, which relies on copper for its expression and function, suggesting that O. tauri may have an additional iron uptake system that doesn't depend on Fea1.
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Phytoplankton growth is limited in vast oceanic regions by the low bioavailability of iron. Iron fertilization often results in diatom blooms, yet the physiological underpinnings for how diatoms survive in chronically iron-limited waters and outcompete other phytoplankton when iron becomes available are unresolved. We show that some diatoms can use siderophore-bound iron, and exhibit a species-specific recognition for siderophore types.

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Article Synopsis
  • * Research identified a single ferritin in its genome and showed that its localization is in the mitochondria.
  • * Iron limitation significantly affects protein expression, with 229 proteins upregulated and 184 downregulated, including important proteins like hemerythrin and [FeFe]-hydrogenase, suggesting that N. gruberi adapts its metabolism based on iron availability with mitochondria playing a key role.
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Upon their translocation into the mitochondrial matrix, the N-terminal pre-sequence of nuclear-encoded proteins undergoes cleavage by mitochondrial processing peptidases. Some proteins require more than a single processing step, which involves several peptidases. Down-regulation of the putative Trypanosoma brucei mitochondrial intermediate peptidase (MIP) homolog by RNAi renders the cells unable to grow after 48 hours of induction.

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Pyruvate is a key product of glycolysis that regulates the energy metabolism of cells. In Trypanosoma brucei, the causative agent of sleeping sickness, the fate of pyruvate varies dramatically during the parasite life cycle. In bloodstream forms, pyruvate is mainly excreted, whereas in tsetse fly forms, pyruvate is metabolized in mitochondria yielding additional ATP molecules.

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Article Synopsis
  • * The study examined key enzymes in the anaerobic amoebozoan Mastigamoeba balamuthi, revealing that some enzymes related to energy metabolism have mitochondrial targeting sequences (MTS) while others do not, indicating parallel pathways.
  • * Phylogenetic analysis suggests that these energy metabolism components were acquired through LGT, supporting the idea that the hydrogenosome evolved from an ancestral organelle via gene duplication and the addition of MTS.
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Mitochondrial processing peptidase (MPP) consists of α and β subunits that catalyze the cleavage of N-terminal mitochondrial-targeting sequences (N-MTSs) and deliver preproteins to the mitochondria. In plants, both MPP subunits are associated with the respiratory complex bc1, which has been proposed to represent an ancestral form. Subsequent duplication of MPP subunits resulted in separate sets of genes encoding soluble MPP in the matrix and core proteins (cp1 and cp2) of the membrane-embedded bc1 complex.

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The bloodstream form of Trypanosoma brucei acquires iron from transferrin by receptor-mediated endocytosis. However, it is unknown how procyclic forms that cannot bind transferrin acquire iron. Here, we show that the procyclic form of T.

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Frataxin is a small conserved mitochondrial protein; in humans, mutations affecting frataxin expression or function result in Friedreich's ataxia. Much of the current understanding of frataxin function comes from informative studies with yeast models, but considerable debates remain with regard to the primary functions of this ubiquitous protein. We exploit the tractable reverse genetics of Trypanosoma brucei in order to specifically consider the importance of frataxin in an early branching lineage.

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