<scp>T</scp>rypanosoma brucei<scp>Orc</scp>1 is essential for nuclear <scp>DNA</scp> replication and affects both <scp>VSG</scp> silencing and <scp>VSG</scp> switching

Benmerzouga, Imaan; Concepción-Acevedo, Jeniffer; Kim, Hee Sook; Vandoros, Anthula V.; Cross, George A.M.; Klingbeil, Michele M.; Li, Bibo

doi:10.1111/mmi.12093

Cited by 62 publications

(68 citation statements)

References 76 publications

(130 reference statements)

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“…How stabilization might occur remains uncertain (103), in part because the trigger and timing of transcriptional VSG switching is unknown. DNA replication and segregation may provide a window for transcriptional change, which would be consistent with observations that RNAi targeting of factors involved in nuclear replication and chromatid cohesion functions can elevate levels of silent VSG expression and switching (104)(105)(106)(107). However, whether directed or random events can precipitate a transcriptional switch remains unknown.…”

Section: The Genomic Components Of Antigenic Variation In Trypanosomasupporting

confidence: 54%

“…5) have been limited to understanding the activation of intact VSGs (106,108,110,114,117,(127)(128)(129). This stems from the fact that these studies have used in vivo or in vitro selection strategies that detect the most frequently activated VSGs; the lack of detectable mosaic VSG formation in these studies may suggest that SGC is less efficient than intact VSG conversion, though a mechanistic switch during an infection cannot be currently ruled out.…”

Section: Activation Of Intact Vsgs Involves Homologous Recombinationmentioning

confidence: 91%

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DNA Recombination Strategies During Antigenic Variation in the African Trypanosome

2015

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Survival of the African trypanosome in its mammalian hosts has led to the evolution of antigenic variation, a process for evasion of adaptive immunity that has independently evolved in many other viral, bacterial and eukaryotic pathogens. The essential features of trypanosome antigenic variation have been understood for many years and comprise a dense, protective Variant Surface Glycoprotein (VSG) coat, which can be changed by recombination-based and transcription-based processes that focus on telomeric VSG gene transcription sites. However, it is only recently that the scale of this process has been truly appreciated. Genome sequencing of Trypanosoma brucei has revealed a massive archive of >1000 VSG genes, the huge majority of which are functionally impaired but are used to generate far greater numbers of VSG coats through segmental gene conversion. This chapter will discuss the implications of such VSG diversity for immune evasion by antigenic variation, and will consider how this expressed diversity can arise, drawing on a growing body of work that has begun to examine the proteins and sequences through which VSG switching is catalyzed. Most studies of trypanosome antigenic variation have focused on T. brucei , the causative agent of human sleeping sickness. Other work has begun to look at antigenic variation in animal-infective trypanosomes, and we will compare the findings that are emerging, as well as consider how antigenic variation relates to the dynamics of host–trypanosome interaction.

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Section: The Genomic Components Of Antigenic Variation In Trypanosomasupporting

confidence: 54%

Section: Activation Of Intact Vsgs Involves Homologous Recombinationmentioning

confidence: 91%

DNA Recombination Strategies During Antigenic Variation in the African Trypanosome

2015

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“…The precise underlying molecular mechanism is still not understood. Although several molecular players have been shown to be involved (8,(11)(12)(13)(14)(15)(16)(17)(18)(19)(20), depletion of any of these factors had only a moderate effect on the repression of silent VSG genes. Therefore, either a master regulator is still to be discovered or, alternatively, the process is controlled by multiple collaborative factors ensuring a cumulative tight lock.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, the level at which the control takes place is unknown: Whether the transcription control takes place at the initiation or elongation level is debated. Data reporting low levels of transcripts from silent ESs upon RNAi-mediated knockdown of various factors (8,(11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21) cannot resolve this issue, because the data are compatible with both models. Previous experiments pointed to mixed conclusions.…”

mentioning

confidence: 83%

“…The mechanism controlling the selective activity of a single ES at a time is still unknown, although several factors have been found to be involved, such as differential chromatin/histone acetylation and methylation between active and inactive ESs (6-8); nucleosome depletion in the active ES (9,10); and the influence of various negative transcription modulators such as a histone methylase, a high-mobility group protein, histone H1, NLP (a nucleoplasm-like protein), a FACT subunit (a chromatin remodeler), a SWI/SNF (a chromatin remodeling factor), ORC1 and MCM-BP (proteins involved in the initiation of DNA replication), RAP1 (a telomere-binding protein), histone chaperones, or a lamin-like protein (8,(11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21). However, no master ES regulator has been identified so far.…”

mentioning

confidence: 99%

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Transcription is initiated on silent variant surface glycoprotein expression sites despite monoallelic expression in Trypanosoma brucei

Kassem

Pays

Vanhamme

2014

Proc. Natl. Acad. Sci. U.S.A.

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Significance African trypanosomes are a major plague in sub-Saharan Africa. They cause sleeping sickness in humans and nagana in cattle, preventing extensive cattle raising. They escape the immune system of their host through frequent changes in their major surface antigen, the variant surface glycoprotein (VSG). The control of VSG expression is poorly understood, and the level at which it takes place has been a matter of debate for the last 25 y. A better understanding of the mechanism by which it works would facilitate the identification of the proteins involved and would provide putative targets for drug design. We report data indicating an unusual control level, namely after transcription initiation, suggesting transcription elongation or RNA processing as a control step.

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Epigenetic Regulation in T. brucei: Changing Coats Is a Chance to Survive

Pena

Aresta‐Branco

Figueiredo

2017

Epigenetics of Infectious Diseases

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Trypanosoma bruceiOrc1 is essential for nuclear DNA replication and affects both VSG silencing and VSG switching

Cited by 62 publications

References 76 publications

DNA Recombination Strategies During Antigenic Variation in the African Trypanosome

DNA Recombination Strategies During Antigenic Variation in the African Trypanosome

Transcription is initiated on silent variant surface glycoprotein expression sites despite monoallelic expression in Trypanosoma brucei

Epigenetic Regulation in T. brucei: Changing Coats Is a Chance to Survive

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