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antiCD33

AntiCD33 refers to therapeutic approaches that target the CD33 antigen, a sialic acid–binding immunoglobulin-like lectin expressed on most myeloid cells, including many acute myeloid leukemia (AML) blasts, as well as on normal monocytes and granulocytes. Because CD33 is broadly present on malignant myeloid cells but not on hematopoietic stem cells, it has been explored as a means to selectively deliver cytotoxic effects to leukemic cells while attempting to preserve other tissues. Therapeutic strategies include naked monoclonal antibodies against CD33, antibody–drug conjugates (ADCs) that release a toxin after internalization, and bispecific T-cell engagers that recruit T cells to CD33-expressing targets. On-target, off-tumor toxicity to normal myeloid cells and associated cytopenias are important considerations in development and clinical use.

Gemtuzumab ozogamicin (GO, Mylotarg) is a prominent anti-CD33 ADC in clinical history. It consists of an anti-CD33

In summary, antiCD33 encompasses a range of strategies aimed at exploiting CD33 as a therapeutic target in

antibody
linked
to
the
cytotoxic
agent
calicheamicin.
GO
was
approved
for
AML
in
2000,
withdrawn
in
2010
due
to
safety
concerns
and
overall
survival
signals,
and
reintroduced
in
2017
at
a
lower
dose
with
restricted
indications
in
several
regions.
Other
anti-CD33
programs
have
included
lintuzumab,
a
naked
anti-CD33
monoclonal
antibody,
and
vadastuximab
talirine
(SGN-CD33A),
an
ADC.
Development
of
vadastuximab
talirine
was
halted
after
unfavorable
safety
outcomes
in
late-stage
trials,
and
the
program
was
not
continued.
AML
and
related
myeloid
disorders,
with
mixed
clinical
success
and
ongoing
evaluation
of
safety,
dosing,
and
patient
selection.