Sphingosine‐1‐phosphate antibodies as potential agents in the treatment of cancer and age‐related macular degeneration

Sabbadini, Roger A.

doi:10.1111/j.1476-5381.2010.01118.x

Cited by 76 publications

(69 citation statements)

References 124 publications

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“…In addition to FTY720, a promising drug to target this pathway, is an antibody against S1P ligand, which has been shown to effectively inhibit primary tumor growth in various mouse models and has recently entered clinical trials for other indications. 35,40 Another possibility is the use of a novel in vivo siRNA delivery technology, CpG oligonucelotide-conjugated siRNA, to specifically target Toll-like receptor 9-positive cells. 41,42 Toll-like receptor 9-positive cells include normal macrophages and B cells and various types of malignant myeloid and B cells, including ABC-DLBCL.…”

mentioning

confidence: 99%

S1PR1 is an effective target to block STAT3 signaling in activated B cell–like diffuse large B-cell lymphoma

Liu¹,

Deng²,

Wang³

et al. 2012

Blood

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STAT3 plays a crucial role in promoting progression of human cancers, including several types of B-cell lymphoma. However, as a transcription factor lacking its own enzymatic activity, STAT3 remains difficult to target with small-molecule drugs in the clinic. Here we demonstrate that persistent activated STAT3 colocalizes with elevated expression of S1PR1, a G-protein-coupled receptor for sphingosine-1-phosphate (S1P), in the tumor cells of the activated B cell-like subtype of diffuse large B-cell lymphoma patient specimens. Inhibition of S1PR1 expression by shRNA in the lymphoma cells validates that blocking S1PR1 affects expression of STAT3 downstream genes critically involved in tumor cell survival, proliferation, tumor invasion, and/or immunosuppression. Using S1PR1 shRNA, or FTY720, an antagonist of S1P that is in the clinic for other indications, we show that inhibiting S1PR1 expression down-regulates STAT3 activity and causes growth inhibition of the lymphoma tumor cells in vitro and in vivo. Our results suggest that targeting S1P/ S1PR1 using a clinically relevant and available drug or other approaches is potentially an effective new therapeutic modality for treating the activated B celllike subtype of diffuse large B-cell lymphoma, a subset of lymphoma that is less responsive to current available therapies. (Blood. 2012;120(7):1458-1465) IntroductionDiffuse large B-cell lymphoma (DLBCL) is a heterogeneous disease, including subtypes with diverse origins and gene expression profiles. [1][2][3][4][5][6] One of the most aggressive histologies, activated B cell-like DLBCL (ABC-DLBCL) remains a challenge for effective therapy, despite extensive studies of morphology and gene expression patterns. [5][6][7][8][9][10] In vitro, cells of the ABC-DLBCL subtype have gene expression patterns similar to those of activated peripheral blood B cells, such as the NF-B downstream genes IRF4, CD44, and cyclin D2. 11 At the same time, these tumor cells also secrete IL-6 and IL-10 through autocrine/paracrine pathways. 12 Consistent with this, the constitutive activation of NF-B and Janus kinase (JAK) is shown to promote tumorigenicity of malignant B-cell lymphoma, including ABC-DLBCL. 13 One promising candidate for ABC-DLBCL targeted therapy is signal transducer and activator of transcription 3 (STAT3). STAT3 is a transcriptional factor that is constitutively activated in many types of cancer, contributing to tumor progression via several mechanisms. 14-20 STAT3 is shown to be activated in the ABC-DLBCL subtype. 20,21 Approximately one-third of ABC-DLBCL patients have gain-of-function mutations in the adaptor protein MYD88, which leads to JAK and STAT3 activation, as well as IL-6 and IL-10 secretion. 13 IL-6 and IL-10 secretion can further increase STAT3 activation levels within tumor cells via an autocrine feedback loop. 14 IL-6-activated STAT3 is crucial for survival of several types of cancer cells, including multiple myeloma, a plasmacytic B-cell malignancy. 14,22 IL-10 is also important for STAT3-mediated immune suppre...

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confidence: 99%

S1PR1 is an effective target to block STAT3 signaling in activated B cell–like diffuse large B-cell lymphoma

Liu¹,

Deng²,

Wang³

et al. 2012

Blood

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“…It has high affinity and specificity for S1P and blocks S1P-mediated release of the proangiogenic factors IL-8, IL-6, and VEGF from tumor cells in vitro and in vivo, out-competing S1P receptors in binding to S1P [60,[73][74][75]. Sonepcizumab (or it murine counterpart Sphingomab) has demonstrated antipermeability (reduced vascular leakage) and antiangiogenic activity after IVT administration in murine CNV models [67,68,74] and antiangiogenic activity in several mouse and human cancer models, where it retarded the progression of several orthotopic and SC human tumors implanted in nude mice [60].…”

Section: Anti-s1pmentioning

confidence: 99%

“…It has shown better efficacy than bevacizumab, tyrosine kinase inhibitors, and paclitaxel in mouse models of renal cell carcinoma (RCC), and ovarian and lung cancer, respectively (www.LPath.com). Regarding safety, 4 weeks after intraocular injection of up to 1.8 mg of sonepcizumab in non-human primate (NHPs), electroretinograms and fluorescein angiograms were normal, and light microscopy of ocular sections showed no evidence of structural damage [75]. Safety was further supported by toxicology studies in NHPs and mice (with Shingomab) with no adverse events observed at high-dose levels and only a slight decrease in blood lymphocytes at 100 mg kg −1 , expected because of the role of S1P in controlling lymphocyte trafficking [75].…”

Section: Anti-s1pmentioning

confidence: 99%

“…Regarding safety, 4 weeks after intraocular injection of up to 1.8 mg of sonepcizumab in non-human primate (NHPs), electroretinograms and fluorescein angiograms were normal, and light microscopy of ocular sections showed no evidence of structural damage [75]. Safety was further supported by toxicology studies in NHPs and mice (with Shingomab) with no adverse events observed at high-dose levels and only a slight decrease in blood lymphocytes at 100 mg kg −1 , expected because of the role of S1P in controlling lymphocyte trafficking [75]. However, another study showed sphingomab to cause B-and T-cell lymphopenia [77] and hence limiting systemic exposure in AMD through IVT injection should reduce concerns around systemic immunosuppression.…”

Section: Anti-s1pmentioning

confidence: 99%

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mAbs Targeting Apoptosis, Angiogenesis Inhibitors, and Other mAbs in Phase 1 and 2 Clinical Studies for Immunological Disorders

Brennan

2014

Handbook of Therapeutic Antibodies

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“…While intracellular targets such as histone deacetylases 1 and 2 (7) as well as TRAF2 (8) have been described, most of the described effects of S1P on cellular processes have been associated with the extracellular functions of S1P mediated through signaling events employing the S1P GPCRs. Thus, one potential therapeutic intervention point is to target the bioactive lipid directly so that it no longer acts as a ligand for its cognate GPCRs or other sites of action (9,10). One way that has been employed to block S1P actions involves the generation of monoclonal antibodies (mAbs) that could act as a molecular sponges to neutralize the bioactive lipid and prevent ligand-receptor signaling (11,12).…”

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confidence: 99%

Antibodies to Bioactive Lysophospholipids

Sabbadini

Wojciak

Moreno

et al. 2013

Lysophospholipid Receptors

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Sphingosine‐1‐phosphate antibodies as potential agents in the treatment of cancer and age‐related macular degeneration

Cited by 76 publications

References 124 publications

S1PR1 is an effective target to block STAT3 signaling in activated B cell–like diffuse large B-cell lymphoma

S1PR1 is an effective target to block STAT3 signaling in activated B cell–like diffuse large B-cell lymphoma

mAbs Targeting Apoptosis, Angiogenesis Inhibitors, and Other mAbs in Phase 1 and 2 Clinical Studies for Immunological Disorders

Antibodies to Bioactive Lysophospholipids

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