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Antigenic variation in A frican trypanosomes: the importance of chromosomal and nuclear context in VSG expression control
Author(s) -
Glover Lucy,
Hutchinson Sebastian,
Alsford Sam,
McCulloch Richard,
Field Mark C.,
Horn David
Publication year - 2013
Publication title -
cellular microbiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.542
H-Index - 138
eISSN - 1462-5822
pISSN - 1462-5814
DOI - 10.1111/cmi.12215
Subject(s) - biology , antigenic variation , chromatin , genetics , transcription (linguistics) , gene , epigenetics , homologous recombination , linguistics , philosophy
Summary African trypanosomes are lethal human and animal parasites that use antigenic variation for evasion of host adaptive immunity. To facilitate antigenic variation, trypanosomes dedicate approximately one third of their nuclear genome, including many minichromosomes, and possibly all sub‐telomeres, to variant surface glycoprotein ( VSG ) genes and associated sequences. Antigenic variation requires transcription of a single VSG by RNA polymerase I ( Pol ‐ I ), with silencing of other VSG s, and periodic switching of the expressed gene, typically via DNA recombination with duplicative translocation of a new VSG to the active site. Thus, telomeric location, epigenetic controls and monoallelic transcription by Pol ‐ I at an extranucleolar site are prominent features of VSG s and their expression, with telomeres, chromatin structure and nuclear organization all making vitally important contributions to monoallelic VSG expression control and switching. We discuss VSG transcription, recombination and replication control within this chromosomal and sub‐nuclear context.

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