Highlights d Circadian depletion of GCs is required for reactivation of GR target genes d Ultradian and constant hormone treatments result in distinct RNA bursting patterns d The GR dwell time and bound fraction determine RNA burst duration and frequency d Stimulation with GCs induces co-bursting of proximal and distal transcription sites
The
electrophilic natural product parthenolide has generated significant
interest as a model for potential chemotherapeutics. Similar to other
α,β-unsaturated carbonyl electrophiles, parthenolide induces
the heat shock response in leukemia cells, potentially through covalent
adduction of heat shock proteins. Other thiol-reactive electrophiles
have also been shown to induce the heat shock response as well as
to covalently adduct members of the heat shock protein family, such
as heat shock protein 72 (Hsp72). To identify sites of modification
of Hsp72 by parthenolide, we used high-resolution tandem mass spectrometry
to detect 10 lysine, histidine, and cysteine residues of recombinant
Hsp72 as modified in vitro by 10 and 100 μM parthenolide. To
further ascertain that modification of Hsp72 by parthenolide occurs
inside cells and not simply as an in vitro artifact, an alkyne-labeled
derivative of parthenolide was synthesized to enable enrichment and
detection of protein targets of parthenolide using copper-catalyzed
[3 + 2] azide–alkyne cycloaddition. The alkyne-labeled parthenolide
derivative displays an half maximal inhibitory concentration (IC50) in undifferentiated acute monocytic leukemia cells (THP-1)
of 13.1 ± 1.1 μM, whereas parthenolide has an IC50 of 4.7 ± 1.1 μM. Concentration dependence of protein
modification by the alkyne–parthenolide derivative was demonstrated,
as well as in vitro adduction of Hsp72. Following treatment of THP-1
cells in culture by the alkyne–parthenolide, adducted proteins
were isolated with neutravidin resin and detected by immunoblotting
in the enriched protein fraction. Hsp70 proteins were detected in
the enriched proteins, indicating that Hsp70 proteins were adducted
intracellularly by the alkyne–parthenolide derivative.
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