The Spliced Leader RNA Silencing (SLS) Pathway in Trypanosoma brucei Is Induced by Perturbations of Endoplasmic Reticulum, Golgi Complex, or Mitochondrial Protein Factors: Functional Analysis of SLS-Inducing Kinase PK3

Okalang, Uthman; Bar-Ner, Bar Mualem; Rajan, K. Shanmugha; Friedman, Nehemya; Aryal, Saurav; Egarmina, Katarina; Hope, Ronen; Khazanov, Netaly; Senderowitz, Hanoch; Alon, Assaf; Fass, Deborah; Michaeli, Shulamit

doi:10.1128/mbio.02602-21

Cited by 3 publications

(5 citation statements)

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“…Furthermore, these authors argued that DTT was lethal to parasites by causing a strong redox stress, at all concentrations tested, making it unsuitable for use as an ER-stressor (Tiengwe et al, 2015;Sandes et al, 2019). The discrepancy in the phenotypes found following DTT treatment may be attributed to differences in the drug concentrations used in these studies as well as the distinct susceptibility existing between the evolutive forms of this parasite (Goldshmidt et al, 2010;Goldshmidt and Michaeli, 2011;Okalang et al, 2021). In A. deanei TM treatment at higher concentrations caused a decrease in proliferation at higher concentrations.…”

Section: Er-quality Control and Er-response To Stress In Trypanosomatidsmentioning

confidence: 87%

“…PK3 kinase have demonstrated to be essential in this process and its activation during persisting ER stress induces PCD and consequently the parasite elimination. Thus, small molecules that selectively activate PK3 could be considered an attractive drug target ( Okalang et al, 2021 ). Finally, but not least, a better understanding of how the ERQC and UPR work, as well as the mechanisms underlying cell death caused by persistent ER stress in trypanosomatids, can reveal molecular peculiarities, opening new avenues for the development of more effective and less toxic drugs to combat the devastating illness caused by these protozoans.…”

Section: Discussionmentioning

confidence: 99%

“…Consequently, expression levels are primarily controlled by mRNA stability ( Tiengwe et al., 2015 ). Because UPR activation in higher eukaryotes is performed by increased transcription of specific mRNA, it is unlikely that trypanosomatids have a classical UPR machinery ( Hope et al., 2014 ; Tiengwe et al., 2015 ; Okalang et al., 2021 ). However, trypanosomatids are able to respond ER stress by upregulating BiP, triggering the splice leader silencing (SLS) that in turn, inhibits SL RNA transcription.…”

Section: The Er-response To Stress: a Delicate Equilibrium Between Li...mentioning

confidence: 99%

“…The ER-stress induced by SEC63 silencing or low pH results in the translocation of PK3 from the ER to the nucleus where it phosphorylates the TATA-binding TRF4, causing the shutoff of SL RNA transcription, followed by induction of programmed cell death. The loss of PK3 function attenuates the programmed cell death triggered by ER stress, indicating that SLS may contribute to programmed cell death activation in T. brucei ( Bindereif and Preußer, 2014 ; Hope et al., 2014 ; Okalang et al, 2021 ).…”

Section: The Er-response To Stress: a Delicate Equilibrium Between Li...mentioning

confidence: 99%

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The endoplasmic reticulum of trypanosomatids: An unrevealed road for chemotherapy

Sandes

Figueiredo²

2022

Front. Cell. Infect. Microbiol.

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The endoplasmic reticulum (ER) of higher eukaryotic cells forms an intricate membranous network that serves as the main processing facility for folding and assembling of secreted and membrane proteins. The ER is a highly dynamic organelle that interacts with other intracellular structures, as well as endosymbiotic pathogenic and non-pathogenic microorganisms. A strict ER quality control (ERQC) must work to ensure that proteins entering the ER are folded and processed correctly. Unfolded or misfolded proteins are usually identified, selected, and addressed to Endoplasmic Reticulum-Associated Degradation (ERAD) complex. Conversely, when there is a large demand for secreted proteins or ER imbalance, the accumulation of unfolded or misfolded proteins activates the Unfold Protein Response (UPR) to restore the ER homeostasis or, in the case of persistent ER stress, induces the cell death. Pathogenic trypanosomatids, such as Trypanosoma cruzi, Trypanosoma brucei and Leishmania spp are the etiological agents of important neglected diseases. These protozoans have a complex life cycle alternating between vertebrate and invertebrate hosts. The ER of trypanosomatids, like those found in higher eukaryotes, is also specialized for secretion, and depends on the ERAD and non-canonical UPR to deal with the ER stress. Here, we reviewed the basic aspects of ER biology, organization, and quality control in trypanosomatids. We also focused on the unusual way by which T. cruzi, T. brucei, and Leishmania spp. respond to ER stress, emphasizing how these parasites’ ER-unrevealed roads might be an attractive target for chemotherapy.

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Section: Er-quality Control and Er-response To Stress In Trypanosomatidsmentioning

confidence: 87%

Section: Discussionmentioning

confidence: 99%

Section: The Er-response To Stress: a Delicate Equilibrium Between Li...mentioning

confidence: 99%

Section: The Er-response To Stress: a Delicate Equilibrium Between Li...mentioning

confidence: 99%

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The endoplasmic reticulum of trypanosomatids: An unrevealed road for chemotherapy

Sandes

Figueiredo²

2022

Front. Cell. Infect. Microbiol.

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“…QSOX2, in contrast, is largely uncharacterized but, like QSOX1 [22][23][24][25], has been reported to be associated with cancer progression [26][27][28]. Golgi localization of QSOX1 was seen in multiple mammalian cell types [15] and in the unicellular parasite Trypanosoma brucei [29], suggesting a conserved and widespread function in this compartment. Correspondingly, QSOX1 has no detectable impact on oxidative protein folding in the ER [30].…”

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confidence: 99%

Disulfide bond formation and redox regulation in the Golgi apparatus

Reznik

Fass

2022

FEBS Letters

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Formation of disulfide bonds in secreted and cell‐surface proteins involves numerous enzymes and chaperones abundant in the endoplasmic reticulum (ER), the first and main site for disulfide bonding in the secretory pathway. Although the Golgi apparatus is the major station after the ER, little is known about thiol‐based redox activity in this compartment. QSOX1 and its paralog QSOX2 are the only known Golgi‐resident enzymes catalyzing disulfide bonding. The localization of disulfide catalysts in an organelle downstream of the ER in the secretory pathway has long been puzzling. Recently, it has emerged that QSOX1 regulates particular glycosyltransferases, thereby influencing a central activity of the Golgi. Surprisingly, a few important disulfide‐mediated multimerization events occurring in the Golgi were found to be independent of QSOX1. These multimerization events depend, however, on the low pH of the Golgi lumen and secretory granules. We compare and contrast disulfide‐mediated multimerization in the ER vs. the Golgi to illustrate the variety of mechanisms controlling covalent supramolecular assembly of secreted proteins.

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Effect of polyphenols against complications of COVID-19: current evidence and potential efficacy

Vajdi,

Karimi,

Hassanizadeh

et al. 2024

Pharmacol. Rep

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The Spliced Leader RNA Silencing (SLS) Pathway in Trypanosoma brucei Is Induced by Perturbations of Endoplasmic Reticulum, Golgi Complex, or Mitochondrial Protein Factors: Functional Analysis of SLS-Inducing Kinase PK3

Cited by 3 publications

References 86 publications

The endoplasmic reticulum of trypanosomatids: An unrevealed road for chemotherapy

The endoplasmic reticulum of trypanosomatids: An unrevealed road for chemotherapy

Disulfide bond formation and redox regulation in the Golgi apparatus

Effect of polyphenols against complications of COVID-19: current evidence and potential efficacy

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