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Title
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Production and characterization of monoclonal anti-sphingosine-1-phosphate antibodies.
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Authors
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N.O'Brien,
S.T.Jones,
D.G.Williams,
H.B.Cunningham,
K.Moreno,
B.Visentin,
A.Gentile,
J.Vekich,
W.Shestowsky,
M.Hiraiwa,
R.Matteo,
A.Cavalli,
D.Grotjahn,
M.Grant,
G.Hansen,
M.A.Campbell,
R.Sabbadini.
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Ref.
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J Lipid Res, 2009,
50,
2245-2257.
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PubMed id
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Abstract
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Sphingosine-1-phosphate (S1P) is a pleiotropic bioactive lipid involved in
multiple physiological processes. Importantly, dysregulated S1P levels are
associated with several pathologies, including cardiovascular and inflammatory
diseases and cancer. This report describes the successful production and
characterization of a murine monoclonal antibody, LT1002, directed against S1P,
using novel immunization and screening methods applied to bioactive lipids. We
also report the successful generation of LT1009, the humanized variant of
LT1002, for potential clinical use. Both LT1002 and LT1009 have high affinity
and specificity for S1P and do not cross-react with structurally related lipids.
Using an in vitro bioassay, LT1002 and LT1009 were effective in blocking
S1P-mediated release of the pro-angiogenic and prometastatic cytokine,
interleukin-8, from human ovarian carcinoma cells, showing that both antibodies
can out-compete S1P receptors in binding to S1P. In vivo anti-angiogenic
activity of all antibody variants was demonstrated using the murine choroidal
neovascularization model. Importantly, intravenous administration of the
antibodies showed a marked effect on lymphocyte trafficking. The resulting lead
candidate, LT1009, has been formulated for Phase 1 clinical trials in cancer and
age-related macular degeneration. The anti-S1P antibody shows promise as a
novel, first-in-class therapeutic acting as a "molecular sponge" to selectively
deplete S1P from blood and other compartments where pathological S1P levels have
been implicated in disease progression or in disorders where immune modulation
may be beneficial.
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