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virotherapy

Virotherapy is a therapeutic approach in oncology that uses viruses to treat cancer. It encompasses oncolytic virotherapy, which uses replication-competent viruses that preferentially infect and lyse cancer cells, and viroimmunotherapy, which aims to stimulate an anti-tumor immune response through viral oncolysis or by delivering immunomodulatory genes. Virus platforms include herpes simplex virus, adenovirus, vaccinia, reovirus, parvovirus, and others that are engineered for safety and tumor selectivity.

Mechanisms include selective replication in cancer cells with defective antiviral responses, direct oncolysis, and the release

Regulatory status and examples: The first and best-known approval is talimogene laherparepvec (T-VEC), a modified herpes

Challenges include delivering virus to tumors, especially after intravenous administration, pre-existing immunity that neutralizes the virus,

of
tumor
antigens
and
danger
signals
that
activate
dendritic
cells
and
T
cells.
Many
vectors
are
engineered
to
express
cytokines
such
as
GM‑CSF
to
boost
systemic
immunity.
Some
approaches
combine
virotherapy
with
immune
checkpoint
inhibitors
to
enhance
anti-tumor
responses.
simplex
virus,
for
advanced
melanoma
in
2015.
Other
oncolytic
viruses
have
gained
regulatory
approval
in
different
countries,
such
as
G47∆-based
therapies
(Delytact)
for
glioblastoma
in
Japan,
with
ongoing
trials
globally.
Numerous
agents
remain
in
clinical
trials
for
a
range
of
solid
tumors.
safety
concerns
about
infection
of
normal
tissues,
and
variable
efficacy
across
tumor
types.
Ongoing
research
explores
optimization
of
delivery
methods,
virus
engineering,
combination
strategies,
and
biomarkers
to
identify
responsive
patients.