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Query: UMLS:C0024312 (
lymphopenia
)
4,859
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Immunotherapeutic drugs that mimic sphingosine 1-phosphate (S1P) disrupt lymphocyte trafficking and cause T helper and T effector cells to be retained in secondary lymphoid tissue and away from sites of inflammation. The prototypical therapeutic agent, 2-alkyl-2-amino-1,3-propanediol (FTY720), stimulates S1P signaling pathways only after it is phosphorylated by one or more unknown kinases. We generated
sphingosine kinase 2
(
SPHK2
) null mice to demonstrate that this kinase is responsible for FTY720 phosphorylation and thereby its subsequent actions on the immune system. Both systemic and lymphocyte-localized sources of
SPHK2
contributed to FTY720 induced
lymphopenia
. Although FTY720 was selectively activated in vivo by
SPHK2
, other S1P pro-drugs can be phosphorylated to cause
lymphopenia
through the action of additional sphingosine kinases. Our results emphasize the importance of
SPHK2
expression in both lymphocytes and other tissues for immune modulation and drug metabolism.
...
PMID:Sphingosine kinase 2 is required for modulation of lymphocyte traffic by FTY720. 1609 48
FTY720, a potent immunomodulatory drug in phase 2/3 clinical trials, induces rapid and reversible sequestration of lymphocytes into secondary lymphoid organs, thereby preventing their migration to sites of inflammation. As prerequisite for its function, phosphorylation of FTY720 to yield a potent agonist of the sphingosine-1-phosphate receptor S1P(1) is required in vivo, catalyzed by an as-yet-unknown kinase. Here, we report on the generation of
sphingosine kinase 2
(
SPHK2
) knockout mice and demonstrate that this enzyme is essential for FTY720 phosphate formation in vivo. Consequently, administration of FTY720 does not induce
lymphopenia
in
SPHK2
-deficient mice. After direct dosage of FTY720 phosphate,
lymphopenia
is only transient in this strain, indicating that
SPHK2
is constantly required to maintain FTY720 phosphate levels in vivo.
...
PMID:Sphingosine kinase type 2 is essential for lymphopenia induced by the immunomodulatory drug FTY720. 1622 73
The new immunosuppressant FTY720 (fingolimod), an analog of the endogenous lipid sphingosine, induces transient
lymphopenia
through the sequestration of lymphocytes in secondary lymphoid organs. Phosphorylation of FTY720 by
sphingosine kinase 2
(SphK2) yields the active metabolite FTY720-phosphate (FTY-P), which induces
lymphopenia
through agonism of the sphingosine 1-phosphate receptor S1P(1) on endothelial cells and lymphocytes. Dephosphorylation of circulating FTY-P creates an equilibrium between FTY720 and its phosphate, and results with human patients indicate that phosphorylation of FTY720 could be rate limiting for efficacy. We report that the FTY720 derivative 2-amino-4-(4-heptyloxyphenyl)-2-methylbutanol [AAL(R)] is phosphorylated much more rapidly than FTY720 in cultured human cells and whole blood. The K(cat) for AAL(R) with recombinant SphK2 is 8-fold higher than for FTY720, whereas the K(m) for the two substrates is very similar, indicating that the increased rate of phosphorylation results from faster turnover by SphK2 rather than a higher binding affinity. Consequently, treating cells with AAL(R), but not FTY720, triggers an apoptotic pathway that is dependent on excessive intracellular accumulation of long-chain base phosphates. In agreement with the in vitro results, phosphorylation of AAL(R) is more complete than that of FTY720 in vivo (mice), and AAL(R) is a more potent inducer of
lymphopenia
. These differences may be magnified in humans, because phosphorylation of FTY720 is much less efficient in humans compared with rodents. Our results suggest that AAL(R) is a better tool than FTY720 for in vivo studies with S1P analogs and would probably be a more effective immunosuppressant than FTY720.
...
PMID:Elimination of a hydroxyl group in FTY720 dramatically improves the phosphorylation rate. 2061 Jul 34
FTY720 is a recently approved first line therapy for relapsing forms of multiple sclerosis. In this context, FTY720 is a pro-drug, with its anti-multiple sclerosis, immunosuppressive effects largely elicited following its phosphorylation by
sphingosine kinase 2
and subsequent modulation of G protein-coupled sphingosine 1-phosphate (S1P) receptor 1 that induces
lymphopenia
by altering lymphocyte trafficking. A number of other biological effects of FTY720 have, however, been described, including considerable evidence that this drug also has anti-cancer properties. These other effects of FTY720 are independent of S1P receptors, and appear facilitated by modulation of a range of other recently described protein targets by nonphosphorylated FTY720. Here, we review the direct targets of FTY720 that contribute to its anti-cancer properties. We also discuss other recently described protein effectors that, in combination with S1P receptors, appear to contribute to its immunosuppressive effects.
...
PMID:Molecular targets of FTY720 (fingolimod). 2283 25
