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histonetargeted

Histone-targeted refers to therapeutic and research strategies that aim to modulate histones or their post-translational modifications to influence chromatin structure and gene expression. Histones are the core proteins around which DNA is wound to form nucleosomes; their modifications, including acetylation, methylation, phosphorylation, and ubiquitination, help regulate access to genetic information and control cellular processes.

Targets in histone targeting include histone-modifying enzymes (writers that add marks, erasers that remove marks) and

Approaches in histone targeting encompass small-molecule inhibitors, peptides, and degrader technologies. Examples of established or influential

Applications of histone-targeted strategies are broadly focused on oncology, with ongoing research into neurodegenerative and inflammatory

histone-binding
proteins
that
recognize
specific
marks,
known
as
readers.
Writers
and
erasers
include
histone
acetyltransferases
and
deacetylases,
as
well
as
methyltransferases
and
demethylases.
Readers
include
bromodomain-containing
proteins
that
interpret
acetylation
marks.
Therapeutic
efforts
also
explore
histone
chaperones
and
histone
variants
that
influence
nucleosome
dynamics.
modalities
include
histone
deacetylase
inhibitors,
which
are
approved
for
certain
lymphomas
and
other
cancers,
and
EZH2
inhibitors
that
target
a
key
methyltransferase
involved
in
gene
silencing.
Bromodomain
inhibitors
(BET
inhibitors)
have
been
widely
studied
in
clinical
trials
for
cancer
and
other
diseases.
More
recently,
targeted
protein
degradation
approaches
(PROTACs)
and
epigenome
editing
strategies
using
programmable
nucleases
fused
to
histone
modifiers
have
been
explored
to
achieve
precise
chromatin
modulation.
diseases.
Challenges
include
achieving
selectivity
among
closely
related
enzymes,
managing
toxicity,
and
addressing
redundancy
in
histone
modification
networks.
The
field
continues
to
evolve
as
new
targets,
molecules,
and
delivery
approaches
emerge.