Sonidegib (Erismodegib, NVP-LDE225)

Catalog No.S2151

Sonidegib (Erismodegib, NVP-LDE225) Chemical Structure

Molecular Weight(MW): 485.5

Sonidegib (Erismodegib, NVP-LDE225) is a Smoothened (Smo) antagonist, inhibiting Hedgehog (Hh) signaling with IC50 of 1.3 nM (mouse) and 2.5 nM (human) in cell-free assays, respectively. Phase 3.

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3 Customer Reviews

  • RU-SKI 43 blocks Shh signaling. (a) RU-SKI 43 blocks Gli activation. NIH 3T3 cells were cotransfected with vectors encoding 8× Gli-binding site (GliBS)-Firefly luciferase (unless indicated otherwise), Renilla luciferase reporter (pRL-TK) and Shh. Confluent cells were treated with DMSO, 10 μM LDE225, 10 μM RU-SKI 43 or 10 μM C-2. The firefly luciferase (FL)/Renilla luciferase (RL) ratio in cell lysates was calculated and normalized to that measured in DMSO-treated samples; error bars represent mean ± s.d. (n = 2–3). 

    Nat Chem Biol 2013 9, 247-9. Sonidegib (Erismodegib, NVP-LDE225) purchased from Selleck.

    Western blot analysis on total cell lysates from renal cancer cell lines treated with NVP-LDE225 at different concentrations. Densitometric measurements were normalised to b-actin and reported under western blot images.

    Br J Cancer 2014 111(6), 1168-79. Sonidegib (Erismodegib, NVP-LDE225) purchased from Selleck.

  • NVP-LDE225, everolimus, sunitinib, and their combination interfere with actin and with intracellular organisation of focal adhesion points. Cytoskeleton organisation of 786-O SuR treated with NVP-LDE225 ( 2.5 uM ), everolimus (1 uM ), sunitinib (1 uM ), and their combination for 24 h was analysed by confocal microscopy. Actin-based structures were revealed by rhodaminated phalloidin staining (red fluorescence). Localisation of focal adhesion points was obtained by immunofluorescent staining of p-paxillin (green fluorescence). Merged row images show overlapping of p-paxillin and actin signals. Moreover, all captures were shown in transmitted light. Scale bars, 10 um.

    Br J Cancer 2014 111(6), 1168-79. Sonidegib (Erismodegib, NVP-LDE225) purchased from Selleck.

Purity & Quality Control

Choose Selective Hedgehog/Smoothened Inhibitors

Biological Activity

Description Sonidegib (Erismodegib, NVP-LDE225) is a Smoothened (Smo) antagonist, inhibiting Hedgehog (Hh) signaling with IC50 of 1.3 nM (mouse) and 2.5 nM (human) in cell-free assays, respectively. Phase 3.
Targets
Smo (mouse) [1]
(Cell-free assay)
Smo (human) [1]
(Cell-free assay)
1.3 nM 2.5 nM
In vitro

Sonidegib (Erismodegib, NVP-LDE225) inhibits TM3 luciferized cell line with 0.6 nM and 8 nM, at the presence of 1 nM and 25 nM Hh agonist Ag1.5, respectively. [1]

Cell Data
Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID
A2780ip2 MnLhR5l1d3irY3n0fUBie3OjeR?= NXGzN4lThjFyIN88US=> Ml;DTWM2OD1zMjFOwG0> MkfONlI2PTN|NUW=
A2780cp20 MYXDfZRwgGmlaYT5JIF{e2G7 MmDBglExKM7:TR?= MVLJR|UxRTdwNTFOwG0> NXLGbItkOjJ3NUOzOVU>
SKOV3ip1 Ml:2R5l1d3irY3n0fUBie3OjeR?= NGXkZnR,OTBizszN MYfJR|UxRTJ2IN88US=> MWiyNlU2OzN3NR?=
SKOV3TRip2 MWrDfZRwgGmlaYT5JIF{e2G7 MVT+NVAh|ryP M{\GWmlEPTB;MUKg{txO NGD6b|czOjV3M{O1OS=>
HeyA8 MWjDfZRwgGmlaYT5JIF{e2G7 M1Pkfp4yOCEQvF2= NF;UfVdKSzVyPUG4JO69VQ>? NUPBN|JHOjJ3NUOzOVU>
HeyA8MDR MXLDfZRwgGmlaYT5JIF{e2G7 NY\EfmhWhjFyIN88US=> MoDoTWM2OD16IN88US=> NYjaRmZbOjJ3NUOzOVU>
OS5 MUHHdo94fGhiaX7obYJqfG:{eTDhd5NigQ>? NVWxW2NvhjVizszN MoPadoVlfWOnczD0bIUheHKxbHnm[ZJifGmxbh?= M33DfFI{OjR|NUm1
OS18 NX35VGNtT3Kxd4ToJIlvcGmkaYTvdpkh[XO|YYm= NXn3foVZhjVizszN MWny[YR2[2W|IITo[UBxem:uaX\ldoF1cW:w MVWyN|I1OzV7NR?=
Glioblastoma initiating cells NX7rc2JMS3m2b4jpZ4l1gSCjc4PhfS=> NIXTTYd,OTBizszN M{jtSGlvcGmkaYTzJGNmdGxiVnnhZoltcXS7 NY\hR5EzOjN2OEK2O|E>
Glioblastoma initiating cells NVPjfWZDTnWwY4Tpc44h[XO|YYm= M3exOp4yOCEQvF2= NHf6W5BqdmirYnn0d{Bv\XW{b4PwbIVz\SCob4LtZZRqd25? M3:xe|I{PDh{Nkex
Glioblastoma initiating cells MUfDfZRwgGmlaYT5JIF{e2G7 NGLLSld,OTBizszN M4jNZYlv\HWlZYOgZZBweHSxc3nz Mn;iNlM1QDJ4N{G=
Glioblastoma initiating cells NIPBTY1HfW6ldHnvckBie3OjeR?= MWD+NVAh|ryP M{noWoRwf26{ZXf1cIF1\XNidHjlJHNJUCC|aXfuZYxqdmdicHH0bJdigQ>? NYPsXppnOjN2OEK2O|E>
Glioblastoma initiating cells NGDRNHlHfW6ldHnvckBie3OjeR?= NYjCWWVThjFyIN88US=> NUTaZ45XUW6qaXLpeJMhfGinIFX4dJJme3Orb36gc4YhT2WwZYOgTY53d2y4ZXSgbY4hVWGrboThbY5qdmdiUHz1dolxd3SnbnP5 M{j5clI{PDh{Nkex
Glioblastoma initiating cells M2Pyc2Z2dmO2aX;uJIF{e2G7 M4TaXp4yOCEQvF2= M4rONGlvcGmkaYTzJG1wfGmuaYT5MEBKdn[jc3nvckwh[W6mIF3p[5JifGmxbh?= MV2yN|Q5OjZ5MR?=
LOX IMVI NVv3OYFHTnWwY4Tpc44h[XO|YYm= NXm2[WsxOTBizszN NV\GR|RPTE2VTx?= MUPpcohq[mm2czDI[YRo\WixZz3HUGkheGG2aIfhfS=> MnLNNlM6OzV7MkW=
UACC 257 MlfzSpVv[3Srb36gZZN{[Xl? NVq1ZZYxOTBizszN NGnRXo1FVVOR M{XNcolvcGmkaYTzJGhm\GenaH;nMWdNUSCyYYToe4F6 MoXkNlM6OzV7MkW=
LOX IMVI NX:0RpBTTnWwY4Tpc44h[XO|YYm= NFnEZVMyOCEQvF2= NUS5UnZUTE2VTx?= Mk\PbY5lfWOnczDHNUBk\WyuIHP5Z4xmKGG{cnXzeC=> NGPPSWIzOzl|NUmyOS=>
UACC 257 NE\WcVRHfW6ldHnvckBie3OjeR?= NH\xflYyOCEQvF2= MWjEUXNQ MUjpcoR2[2W|IFexJINmdGxiY4njcIUh[XK{ZYP0 M4rsO|I{QTN3OUK1
LOX IMVI MlH1R5l1d3irY3n0fUBie3OjeR?= M{nZOlExKM7:TR?= NF3VNFVFVVOR NIixOppl\WO{ZXHz[ZMhfHWvb4KgZ4VtdCC4aXHibYxqfHl? MV:yN|k{PTl{NR?=
UACC 257 MoLHR5l1d3irY3n0fUBie3OjeR?= M4TKcVExKM7:TR?= Mm\JSG1UVw>? MWnk[YNz\WG|ZYOgeJVud3JiY3XscEB3cWGkaXzpeJk> M2jnc|I{QTN3OUK1
LOX IMVI M{\lPWFxd3C2b4Ppd{Bie3OjeR?= MWCxNEDPxE1? MmjJSG1UVw>? NHvyU5RqdmS3Y3XzJIFxd3C2b4Ppdy=> M16zRVI{QTN3OUK1
UACC 257 NGPsZ2RCeG:ydH;zbZMh[XO|YYm= M1\GT|ExKM7:TR?= M1jGfWROW09? NIjYbXdqdmS3Y3XzJIFxd3C2b4Ppdy=> NU[4SppjOjN7M{W5NlU>
ACHN NIrvT5JIem:5dHigbY5pcWKrdH;yfUBie3OjeR?= M3HTOp42KM7:TR?= MnTWSG1UVw>? M2LMZmlEPTB;Mj2z5qCK|ryP MXiyOVA6OzR7MR?=
769-P MWTHdo94fGhiaX7obYJqfG:{eTDhd5NigQ>? M1rRSp42KM7:TR?= NVfueWtLTE2VTx?= NVm0Z3FpUUN3ME2yMVPjiIoQvF2= M3vTXVI2ODl|NEmx
786-O NHrsV3BIem:5dHigbY5pcWKrdH;yfUBie3OjeR?= M{H2NZ42KM7:TR?= NX3X[VJxTE2VTx?= Ml;0TWM2OD1{LURihKnPxE1? MYKyOVA6OzR7MR?=
786-O SuR NVzwcFdLT3Kxd4ToJIlvcGmkaYTvdpkh[XO|YYm= MnHGglUh|ryP NYSz[mRtTE2VTx?= NEXkZYlKSzVyPUKtN-KBkc7:TR?= MmfMNlUxQTN2OUG=
SP53 NIrZSXRHfW6ldHnvckBie3OjeR?= NEnOelg{OCEQvF2= MXrEUXNQ M4PPSolvcGmkaYTzJINmdGxiYXTo[ZNqd25iYX7kJI1q\3KjdHnvci=> M1zVS|I3QDh3NkC4
SP53 M2nDdWZ2dmO2aX;uJIF{e2G7 MUWzNEDPxE1? NFPzdVJFVVOR Mn7hbY5pcWKrdIOgeIhmKF[OQUStcYVlcWG2ZXSgSmFMKHOrZ37hcIlv\yCyYYToe4F6 MlfQNlY5QDV4MEi=
HS5 M1LCcGZ2dmO2aX;uJIF{e2G7 MUKzNEDPxE1? MoPHSG1UVw>? NGGzVGpqdmirYnn0d{Bk\WyuIHHkbIV{cW:wIHHu[EBucWe{YYTpc44> NV3vemNQOjZ6OEW2NFg>
HS27a MVTGeY5kfGmxbjDhd5NigQ>? MlPwN|Ah|ryP M2G5UGROW09? MXnpcohq[mm2czDj[YxtKGGmaHXzbY9vKGGwZDDtbYdz[XSrb36= NFTGcFMzPjh6NU[wPC=>
SP53 NVP3[I5WS3m2b4jpZ4l1gSCjc4PhfS=> M4TyZVMxKM7:TR?= M17m[2ROW09? MXTpcoR2[2W|IHH1eI9xcGGpeR?= MmrmNlY5QDV4MEi=
Jeko NVzlXYw6S3m2b4jpZ4l1gSCjc4PhfS=> MVuzNEDPxE1? NVzp[Wt6TE2VTx?= M3PMdolv\HWlZYOgZZV1d3CqYXf5 NXfyS5R2OjZ6OEW2NFg>

... Click to View More Cell Line Experimental Data

In vivo Sonidegib (Erismodegib, NVP-LDE225) is highly bound to mouse, rat, and human plasma proteins (>99%) and moderately bound to dog and monkey plasma proteins (77 and 85%, respectively). LDE225 has high permeability (90.8% in man) in the PAMPA assay. LDE225 shows good oral bioavailability ranging from 69 to 102% in preclinical species when dosed in solution. LDE225 is a weak base with a measured pKa of 4.20 and exhibits relatively poor aqueous solubility. LDE225 demonstrates dose-related antitumor activity. At a dose of 5 mg/kg/day qd, LDE225 significantly inhibits tumor growth, corresponding to a T/C value of 33%. When dosed at 10 and 20 mg/kg/day qd, LDE225 gives rise to 51 and 83% regression, respectively. Gli1 mRNA inhibition correlates with tumor and plasma exposure of LDE225. LDE225 successfully penetrates the blood−brain barrier in tumor-bearing animals and results in tumor growth inhibition after 4 days of treatment. [1] LDE225 significantly reduces the tumor volume by 95.7% in Rip1-Tag2 mice. LDE225 prolongs survival in Rip1Tag2 mice. LDE225 decreases expression of stromal markers in the LDE225-treated mice. [2]

Protocol

Cell Research:

[1]

+ Expand
  • Cell lines: TM3Hh12 cells
  • Concentrations: ~10 μM
  • Incubation Time: 30 minutes
  • Method:

    LDE225 is prepared for assay by serial dilution in DMSO and then added to empty assay plates. TM3Hh12 cells (TM3 cells containing Hh-responsive reporter gene construct pTA-8xGli-Luc) are cultured in F12 Ham's/DMEM (1:1) containing 5% horse serum, 2.5% fetal bovine serum (FBS), and 15 mM HEPES, pH 7.3. Cells are harvested by trypsin treatment, resuspended in F12 Ham's/DMEM (1:1) containing 5% horse serum and 15 mM HEPES, pH 7.3, added to assay plates, and incubated with LDE225 for approximately 30 min at 37 °C in 5% CO2. Then 1 nM or 25 nM Ag1.5 is added to assay plates and incubated at 37 °C in the presence of 5% CO2. After 48 hours, either Bright-Glo or MTS reagent is added to the assay plates and luminescence or absorbance at 492 nm is determined. IC50 values, defined as the inflection point of the logistic curve, are determined by nonlinear regression of the Gli-driven luciferase luminescence or absorbance signal from MTS assay vs log10 (concentration) of LDE225 using the R statistical software pack


    (Only for Reference)
Animal Research:

[1]

+ Expand
  • Animal Models: Orthotopic Ptch+/-p53-/- medulloblastoma allograft model in athymic nude mice
  • Formulation: 0.5% sodium carboxymethyl cellulose
  • Dosages: 40 mg/kg/day
  • Administration: Administered via p.o. or b.i.d
    (Only for Reference)

Solubility (25°C)

In vitro DMSO 97 mg/mL (199.79 mM)
Ethanol 97 mg/mL warmed (199.79 mM)
Water Insoluble
In vivo Add solvents to the product individually and in order(Data is from Selleck tests instead of citations):
2% DMSO+corn oil
For best results, use promptly after mixing.
10mg/mL

* Please note that Selleck tests the solubility of all compounds in-house, and the actual solubility may differ slightly from published values. This is normal and is due to slight batch-to-batch variations.

Chemical Information

Molecular Weight 485.5
Formula

C26H26F3N3O3

CAS No. 956697-53-3
Storage powder
in solvent
Synonyms

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Clinical Trial Information

NCT Number Recruitment Conditions Sponsor/Collaborators Start Date Phases
NCT01787552 Completed Primary Myelofibrosis|Thrombocythemia Essential|Thrombocytosis|Myeloproliferative Disorders|Bone Marrow Diseases|Hematologic Diseases|Blood Coagulation Disorders|Blood Platelet Disorders|Hemorrhagic Disorders Novartis Pharmaceuticals|Novartis May 8 2013 Phase 1|Phase 2
NCT01708174 Completed Medulloblastoma Novartis Pharmaceuticals|Novartis May 6 2013 Phase 2
NCT02254551 Terminated Multiple Myeloma SCRI Development Innovations LLC|Novartis January 2015 Phase 2
NCT02195973 Completed Recurrent Ovarian Cancer University of Alabama at Birmingham|Novartis Pharmaceuticals September 2014 Phase 1
NCT02182622 Unknown status Prostate Cancer Martin Gutierrez|Novartis|Hackensack Meridian Health July 2014 Phase 1
NCT02151864 Active not recruiting Hepatocellular Carcinoma|Cirrhosis Jason K. Sicklick M.D.|Novartis Pharmaceuticals|University of California San Diego July 2014 Phase 1

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Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID