Ozanimod (RPC1063) is a potent sphingosine‐1‐phosphate receptor‐1 (S1P<sub>1</sub>) and receptor‐5 (S1P<sub>5</sub>) agonist with autoimmune disease‐modifying activity

Scott, Fiona L.; Clemons, Bryan; Brooks, Jennifer L.; Brahmachary, Enugurthi; Powell, Rachel; Dedman, Harry; Desale, Hans; Timony, Gregg; Martinborough, Esther; Rosen, Hugh; Roberts, Edward; Boehm, Marcus F.; Peach, Robert

doi:10.1111/bph.13476

Cited by 227 publications

(219 citation statements)

References 57 publications

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“…Fourth, CYM-5442 therapy enhanced the expression of negative immune regulating surface molecules on autoreactive T cells, further limiting the ability of any autoimmune T-cell that might enter the islets from killing β cells. The selective and potent S1PR1 agonist CYM-5442 (27, 28) is a predecessor compound to the clinical agonist ozanimod (29), now completing phase 3 clinical trials for multiple sclerosis (30) and ulcerative colitis (31). S1PR1 agonists are clinically effective immunomodulators because of multistep interdiction of immunopathology.…”

Section: Comparable Gene Expression In the Pancreatic Islets Is Observedmentioning

confidence: 99%

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Marro

Ware

Zak

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Blockade of IFN-α but not IFN-β signaling using either an antibody or a selective S1PR1 agonist, CYM-5442, prevented type 1 diabetes (T1D) in the mouse Rip-LCMV T1D model. First, treatment with antibody or CYM-5442 limited the migration of autoimmune "antiself" T cells to the external boundaries around the islets and prevented their entry into the islets so they could not be positioned to engage, kill, and thus remove insulin-producing β cells. Second, CYM-5442 induced an exhaustion signature in antiself T cells by up-regulating the negative immune regulator receptor genes Pdcd1, Lag3, Ctla4, Tigit, and Btla, thereby limiting their killing ability. By such means, insulin production was preserved and glucose regulation maintained, and a mechanism for S1PR1 immunomodulation described.type I interferon | IFN-alpha | S1PR1 | type 1 diabetes T ype 1 diabetes (T1D) is an autoimmune disorder defined by infiltration of autoreactive lymphoid cells into the islets of Langerhans that destroy insulin-producing β cells (1). By the time of clinical diagnosis, T cells have destroyed 60-80% or more of total β cells, resulting in high blood glucose levels as a result of low insulin production. Prevention of ketoacidosis and death require lifelong delivery of exogenous insulin. However, daily insulin therapy is associated with increased prevalence of debilitating pathologies of cardiovascular, central and peripheral nervous, ophthalmic, and peripheral vascular systems among others.A role for type I IFN in autoimmune disease was first reported by Notkins' laboratory (2) and pancreata removed at necropsy from humans with T1D displayed significant increases in type I IFN (3, 4). Treatment of humans having hairy cell leukemia (5) or hepatitis C virus (6) with IFN-α was associated with induction or acceleration of the diabetogenic process, and recent longitudinal studies demonstrated that a IFN-I gene signature of individuals at risk for developing T1D preceded clinical onset (7,8). Direct evidence for an association of IFN-I with T1D was shown by Stewart et al. (9) in transgenic (tg) mice and strengthened in studies with NOD mice (10, 11). Unanue and coworkers (10) found IFN-I transcriptional signatures within the islets preceded T-cell activation. McDevitt and coworkers (11) reported treatment of 2-to 3-wk-old NOD mice with antibody to IFNAR1 delayed the onset and decreased the incidence of T1D. Using the virusinduced Rip-LCMV T1D model, Zinkernagel and coworkers (12) demonstrated that genetic ablation of Ifnar could delay onset of T1D. However, the mechanism of action by type I IFN was unknown. Here, we report studies that define the species of type I IFN and mechanism involved causing T1D and therapeutic approaches to prevent diabetes by preserving β-cell function. Results and DiscussionTo uncover the pathological role(s) of IFN-I, a viral mouse model of T1D (13) was used in which several parameters mimic immunological and histopathological components of human T1D and the "self" antigen recognized by specific autoimmune T cells ca...

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Section: Comparable Gene Expression In the Pancreatic Islets Is Observedmentioning

confidence: 99%

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Marro

Ware

Zak

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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“…The compound is currently being evaluated for the treatment of immune-mediated inflammatory diseases,81 such as multiple sclerosis82 and IBD. In a recent double-blind, placebo-controlled phase II clinical trial (the TOUCHSTONE study), Sandborn et al evaluated the efficacy and safety of induction and maintenance therapy with ozanimod in patients with moderate-to-severe UC 83.…”

Section: Ozanimod and Other S1p Receptor Modulatorsmentioning

confidence: 99%

Next generation of small molecules in inflammatory bowel disease

Olivera

Danese

Peyrin–Biroulet

2016

Gut

127

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“…Ozanimod is an oral selective S1P 1/5 dual modulator, and induces lymphopenia and regulates immune response (Scott et al ., 2016). In three models of autoimmune diseases that is, experimental autoimmune encephalitis, TNBS-induced colitis, and CD4 + CD45RBhi T cell adaptive transfer colitis, oral ozanimod diminished inflammation parameters.…”

Section: Development Of S1p1 Receptor Modulatorsmentioning

confidence: 99%

“…In three models of autoimmune diseases that is, experimental autoimmune encephalitis, TNBS-induced colitis, and CD4 + CD45RBhi T cell adaptive transfer colitis, oral ozanimod diminished inflammation parameters. This finding supports the clinical development of ozanimod for multiple sclerosis (Cohen et al ., 2016a; Scott et al ., 2016). …”

Section: Development Of S1p1 Receptor Modulatorsmentioning

confidence: 99%

Sphingosine 1-Phosphate Receptor Modulators and Drug Discovery

Park

2017

Biomolecules & Therapeutics

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Initial discovery on sphingosine 1-phosphate (S1P) as an intracellular second messenger was faced unexpectedly with roles of S1P as a first messenger, which subsequently resulted in cloning of its G protein-coupled receptors, S1P1–5. The molecular identification of S1P receptors opened up a new avenue for pathophysiological research on this lipid mediator. Cellular and molecular in vitro studies and in vivo studies on gene deficient mice have elucidated cellular signaling pathways and the pathophysiological meanings of S1P receptors. Another unexpected finding that fingolimod (FTY720) modulates S1P receptors accelerated drug discovery in this field. Fingolimod was approved as a first-in-class, orally active drug for relapsing multiple sclerosis in 2010, and its applications in other disease conditions are currently under clinical trials. In addition, more selective S1P receptor modulators with better pharmacokinetic profiles and fewer side effects are under development. Some of them are being clinically tested in the contexts of multiple sclerosis and other autoimmune and inflammatory disorders, such as, psoriasis, Crohn’s disease, ulcerative colitis, polymyositis, dermatomyositis, liver failure, renal failure, acute stroke, and transplant rejection. In this review, the authors discuss the state of the art regarding the status of drug discovery efforts targeting S1P receptors and place emphasis on potential clinical applications.

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Ozanimod (RPC1063) is a potent sphingosine‐1‐phosphate receptor‐1 (S1P₁) and receptor‐5 (S1P₅) agonist with autoimmune disease‐modifying activity

Cited by 227 publications

References 57 publications

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Next generation of small molecules in inflammatory bowel disease

Sphingosine 1-Phosphate Receptor Modulators and Drug Discovery

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Ozanimod (RPC1063) is a potent sphingosine‐1‐phosphate receptor‐1 (S1P1) and receptor‐5 (S1P5) agonist with autoimmune disease‐modifying activity

Cited by 227 publications

References 57 publications

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Progression of type 1 diabetes from the prediabetic stage is controlled by interferon-α signaling

Next generation of small molecules in inflammatory bowel disease

Sphingosine 1-Phosphate Receptor Modulators and Drug Discovery

Contact Info

Product

Resources

About

Ozanimod (RPC1063) is a potent sphingosine‐1‐phosphate receptor‐1 (S1P₁) and receptor‐5 (S1P₅) agonist with autoimmune disease‐modifying activity