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A touch of Z en: post‐translational regulation of the L eishmania stress response
Author(s) -
Späth Gerald F.,
Drini Sima,
Rachidi Najma
Publication year - 2015
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.12440
Subject(s) - biology , microbiology and biotechnology , heat shock protein , chaperone (clinical) , heat shock , transcriptional regulation , hsp90 , transcription factor , cellular stress response , translational regulation , fight or flight response , genetics , gene , translation (biology) , medicine , pathology , messenger rna
Summary Across bacterial, archaeal and eukaryotic kingdoms, heat shock proteins ( HSPs ) are defined as a class of highly conserved chaperone proteins that are rapidly induced in response to temperature increase through dedicated heat shock transcription factors. While this transcriptional response governs cellular adaptation of fungal, plant and animal cells to thermic shock and other forms of stress, early‐branching eukaryotes of the kinetoplastid order, including trypanosomatid parasites, lack classical mechanisms of transcriptional regulation and show largely constitutive expression of HSPs , thus raising important questions on the function of HSPs in the absence of stress and the regulation of their chaperone activity in response to environmental adversity. Understanding parasite‐specific mechanisms of stress‐response regulation is especially relevant for protozoan parasites of the genus L eishmania that are adapted for survival inside highly toxic phagolysosomes of host macrophages causing the various immuno‐pathologies of leishmaniasis. Here we review recent advances on the function and regulation of chaperone activities in these kinetoplastid pathogens and propose a new model for stress‐response regulation through a reciprocal regulatory relationship between stress kinases and chaperones that may be relevant for parasite‐adaptive differentiation and infectivity.

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