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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Cited by 27 Publications

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 Mn34R5l1d3irY3n0fUBie3OjeR?= NGPjfmV,OTBizszN M2nCOWlEPTB;MUKg{txO Mnv5NlI2PTN|NUW=
A2780cp20 MYfDfZRwgGmlaYT5JIF{e2G7 M1TWdJ4yOCEQvF2= MoHkTWM2OD15LkWg{txO MUSyNlU2OzN3NR?=
SKOV3ip1 NVzHSVdTS3m2b4jpZ4l1gSCjc4PhfS=> NEW2epR,OTBizszN NUPXXGpEUUN3ME2yOEDPxE1? M2W1U|IzPTV|M{W1
SKOV3TRip2 M{HWeGN6fG:6aXPpeJkh[XO|YYm= MVf+NVAh|ryP M4TBbWlEPTB;MUKg{txO M1LEOFIzPTV|M{W1
HeyA8 Mn74R5l1d3irY3n0fUBie3OjeR?= M3[xeJ4yOCEQvF2= NVTCS|N[UUN3ME2xPEDPxE1? M{LzblIzPTV|M{W1
HeyA8MDR NIfoZm1EgXSxeHnjbZR6KGG|c3H5 NH3W[md,OTBizszN NHHBcpNKSzVyPUig{txO MU[yNlU2OzN3NR?=
OS5 M3LLOWdzd3e2aDDpcohq[mm2b4L5JIF{e2G7 MV;+OUDPxE1? MonRdoVlfWOnczD0bIUheHKxbHnm[ZJifGmxbh?= NVzpO4xwOjN{NEO1PVU>
OS18 M{HtTGdzd3e2aDDpcohq[mm2b4L5JIF{e2G7 MVP+OUDPxE1? MonEdoVlfWOnczD0bIUheHKxbHnm[ZJifGmxbh?= MYeyN|I1OzV7NR?=
Glioblastoma initiating cells MlPrR5l1d3irY3n0fUBie3OjeR?= MojoglExKM7:TR?= NHfJXW1KdmirYnn0d{BE\WyuIG\pZYJqdGm2eR?= MVOyN|Q5OjZ5MR?=
Glioblastoma initiating cells NUfpOmxyTnWwY4Tpc44h[XO|YYm= M171Zp4yOCEQvF2= MXfpcohq[mm2czDu[ZVzd3OyaHXy[UBnd3KvYYTpc44> NYe2OFNiOjN2OEK2O|E>
Glioblastoma initiating cells NWH4VXhSS3m2b4jpZ4l1gSCjc4PhfS=> MWf+NVAh|ryP NHPuTItqdmS3Y3XzJIFxd3C2b4Ppdy=> M3yzbFI{PDh{Nkex
Glioblastoma initiating cells MYHGeY5kfGmxbjDhd5NigQ>? NEHF[IN,OTBizszN MVPkc5dvemWpdXzheIV{KHSqZTDTTGghe2mpbnHsbY5oKHCjdHj3ZZk> NFK0RYUzOzR6Mk[3NS=>
Glioblastoma initiating cells NXLUdnF[TnWwY4Tpc44h[XO|YYm= MUj+NVAh|ryP MoPRTY5pcWKrdIOgeIhmKEW6cILld5Nqd25ib3[gS4Vv\XNiSX72c4x3\WRiaX6gUYFqdnSjaX7pcochWGy3cnnwc5RmdmO7 NIPPVJkzOzR6Mk[3NS=>
Glioblastoma initiating cells Mn\3SpVv[3Srb36gZZN{[Xl? NVf2cGdphjFyIN88US=> M2P5S2lvcGmkaYTzJG1wfGmuaYT5MEBKdn[jc3nvckwh[W6mIF3p[5JifGmxbh?= NUDMfncyOjN2OEK2O|E>
LOX IMVI Ml74SpVv[3Srb36gZZN{[Xl? M173VFExKM7:TR?= MoO3SG1UVw>? MnHIbY5pcWKrdIOgTIVl\2Wqb3etS2xKKHCjdHj3ZZk> MlroNlM6OzV7MkW=
UACC 257 MlTCSpVv[3Srb36gZZN{[Xl? M2rOO|ExKM7:TR?= NVjRTIhETE2VTx?= NF\SU2JqdmirYnn0d{BJ\WSpZXjv[{1IVElicHH0bJdigQ>? NIfQW2UzOzl|NUmyOS=>
LOX IMVI MWLGeY5kfGmxbjDhd5NigQ>? Mnn3NVAh|ryP MUTEUXNQ NEj5RYtqdmS3Y3XzJGcyKGOnbHygZ5lkdGViYYLy[ZN1 NHG0T28zOzl|NUmyOS=>
UACC 257 M4DQXmZ2dmO2aX;uJIF{e2G7 NWnM[ndGOTBizszN M{D4WWROW09? MWTpcoR2[2W|IFexJINmdGxiY4njcIUh[XK{ZYP0 MUOyN|k{PTl{NR?=
LOX IMVI MnX6R5l1d3irY3n0fUBie3OjeR?= NW\qSGFNOTBizszN NH7UR4FFVVOR M2jsPYRm[3KnYYPld{B1fW2xcjDj[YxtKH[rYXLpcIl1gQ>? M{Hxd|I{QTN3OUK1
UACC 257 Mo\tR5l1d3irY3n0fUBie3OjeR?= M4n2b|ExKM7:TR?= NFrnU2hFVVOR NXn6cWgx\GWlcnXhd4V{KHS3bX;yJINmdGxidnnhZoltcXS7 Mnz4NlM6OzV7MkW=
LOX IMVI M3;tSGFxd3C2b4Ppd{Bie3OjeR?= NGfMOIIyOCEQvF2= NH;uVm1FVVOR NWfGNItQcW6mdXPld{BieG:ydH;zbZM> M2C1XVI{QTN3OUK1
UACC 257 MmfiRZBweHSxc3nzJIF{e2G7 NGjoSnYyOCEQvF2= M1LVd2ROW09? NH\TNo1qdmS3Y3XzJIFxd3C2b4Ppdy=> M1q5SFI{QTN3OUK1
ACHN NYraSZVxT3Kxd4ToJIlvcGmkaYTvdpkh[XO|YYm= NY\1fXRFhjVizszN MYTEUXNQ Mk\WTWM2OD1{LURihKnPxE1? M4f3XlI2ODl|NEmx
769-P MWXHdo94fGhiaX7obYJqfG:{eTDhd5NigQ>? Ml[zglUh|ryP MYjEUXNQ MVfJR|UxRTJvM,MAje69VQ>? MoqyNlUxQTN2OUG=
786-O MoTZS5Jwf3SqIHnubIljcXSxcomgZZN{[Xl? Mn3PglUh|ryP MmqySG1UVw>? MYfJR|UxRTJvM,MAje69VQ>? NX3jZ2t5OjVyOUO0PVE>
786-O SuR MYHHdo94fGhiaX7obYJqfG:{eTDhd5NigQ>? NYO5N3dqhjVizszN MYPEUXNQ NYnLU41DUUN3ME2yMVPjiIoQvF2= M4TPZ|I2ODl|NEmx
SP53 M3z2fWZ2dmO2aX;uJIF{e2G7 M37DcVMxKM7:TR?= M4ThVGROW09? M1X5R4lvcGmkaYTzJINmdGxiYXTo[ZNqd25iYX7kJI1q\3KjdHnvci=> MUGyOlg5PTZyOB?=
SP53 NG\2WIlHfW6ldHnvckBie3OjeR?= M3rwfVMxKM7:TR?= NYPhcIh5TE2VTx?= MVnpcohq[mm2czD0bIUhXkyDND3t[YRq[XSnZDDGRWshe2mpbnHsbY5oKHCjdHj3ZZk> Mm\XNlY5QDV4MEi=
HS5 M{HFPWZ2dmO2aX;uJIF{e2G7 NYfSZ2trOzBizszN NYf4bms2TE2VTx?= NW\tUoNGcW6qaXLpeJMh[2WubDDh[Ihme2mxbjDhcoQhdWmpcnH0bY9v NWKyRWZ7OjZ6OEW2NFg>
HS27a NXPSUm92TnWwY4Tpc44h[XO|YYm= MmC2N|Ah|ryP MV;EUXNQ MoX1bY5pcWKrdIOgZ4VtdCCjZHjld4lwdiCjbnSgcYloemG2aX;u NEnxVWkzPjh6NU[wPC=>
SP53 M1iyTWN6fG:6aXPpeJkh[XO|YYm= NVfZeohCOzBizszN MoXMSG1UVw>? MmTrbY5lfWOnczDheZRweGijZ4m= NE\UWlczPjh6NU[wPC=>
Jeko MmDFR5l1d3irY3n0fUBie3OjeR?= M2XCUVMxKM7:TR?= NIDCSGJFVVOR M1j3colv\HWlZYOgZZV1d3CqYXf5 NVTHfGZGOjZ6OEW2NFg>

... Click to View More Cell Line Experimental Data
Assay
Methods Test Index PMID
Western blot
Bcl2 / c-myc / Cyclin D1 / pERK / ERK / pJNK / JNK / Caspase 3 / Cleaved caspase 3 ; 

PubMed: 22821765     


Immunoblot experiment of protein lysate from OPM1 cells treated with NVP-LDE225 (5μM) for 12, 24, and 36 hours and fractionated by electrophoresis and stained with different Abs as shown in figure (left). Cells were treated with different concentrations o䲧疝Ỵ疞㧀疜膉痘 瘿⟸෕ᾰƌ෕Ð 㺣痖帉痖Ѐ瑖堘𢡄빢᎒෕Ð鑸᎒彿堙奋堙巫堙᎒ﻺ᎒彿堙ﻮ᎒塚堙ﻺ᎒ꍈ堞빢᎒學堙漸

Gli-1 / Gli-2 / p-Akt / Akt; 

PubMed: 25093491     


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

pp70S6K / P70s6k; 

PubMed: 25093491     


Percentage of survival of 786-O, 786-O SuR, and 769-P renal cancer cell lines treated with NVP-LDE225 and everolimus or their combination, as measured by the MTT assay. Data represent the mean (±s.d.) of three independent experiments, each performed in tr䲧疝Ỵ疞㧀疜膉痘 瘿뙠ෆᾰƌෆĀ 㺣痖帉痖Ѐ瑖堘𢡄빢᎒ෆĀ鑸᎒彿堙奋堙巫堙᎒ﻺ᎒彿堙ﻮ᎒塚堙ﻺ᎒ꍈ堞빢᎒學堙漸堞圔堙빢᎒圞堙圭堙𢡄玚Wᾰƌ ᾰƌ戤瘯Ɖ�෋䐺痖暼瘿�෋ᾰƌ �෋Ð㺣痖�෋€𢡄�෋€䀷痗�෋౴�෋㵶痗�෋뺖᎒泌Itemセ᎒Count﫨呂�෋猴፲�

p-p130CAS / p130CAS / p-FAK / FAK / p-Paxillin / Paxillin; 

PubMed: 25093491     


Western blot analysis of total cell lysates from 786-O, 786-O SuR, and 769-P human renal cancer cell lines treated with NVP-LDE225 (2.5 μm), everolimus (1 μm), and their combination. Densitometric measurements were normalised to β-actin and reported under䲧疝Ỵ疞㧀疜膉痘 

22821765 25093491
Immunofluorescence
GLI1; 

PubMed: 22821765     


U266 were cultured in the presence of control medium or NVP-LDE225 (5μM) for 24 hours. Immunocytochemical analysis was assessed using anti-Gli1 Ab, and 4,6-diamidino-2-phenylindole was used to stain nuclei. The cells were analyzed using an epifluorescence䲧疝Ỵ疞㧀疜膉痘 瘿⟸෕ᾰƌ෕Ð 㺣痖帉痖Ѐ瑖堘𢡄빢᎒෕Ð鑸᎒彿堙奋堙巫堙᎒ﻺ᎒彿堙ﻮ᎒塚堙ﻺ᎒ꍈ堞빢᎒學堙漸堞圔堙빢᎒圞堙圭堙𢡄玚Wᾰƌ ᾰƌ戤瘯Ɖ뙠ෆ䐺痖暼瘿뙠ෆᾰƌ 뙠ෆÐ㺣痖뙠ෆ€𢡄뙤ෆ€

22821765
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]
- Collapse
  • 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]
- Collapse
  • 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 interventions Conditions Sponsor/Collaborators Start Date Phases
NCT02254551 Terminated Drug: LDE225|Drug: Bortezomib Multiple Myeloma SCRI Development Innovations LLC|Novartis January 2015 Phase 2
NCT02138929 Active not recruiting Drug: Everolimus|Drug: LDE 225 Esophageal Cancer M.D. Anderson Cancer Center|Novartis|National Cancer Institute (NCI) November 10 2014 Phase 1
NCT02195973 Completed Drug: LDE225 Recurrent Ovarian Cancer University of Alabama at Birmingham|Novartis Pharmaceuticals September 2014 Phase 1
NCT02027376 Completed Drug: LDE225|Drug: Docetaxel Advanced Breast Cancer Spanish Breast Cancer Research Group|Novartis May 2014 Phase 1
NCT02111187 Completed Drug: LDE225 Prostate Cancer Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins April 2014 Phase 1
NCT02086513 Terminated Drug: LDE225 Graft Versus Host Disease Massachusetts General Hospital|Novartis April 2014 Phase 1

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Hedgehog/Smoothened Signaling Pathway Map

Hedgehog/Smoothened Inhibitors with Unique Features

  • Selective Smoothened inhibitor

    PF-5274857 : Smoothened-selective, IC50=5.8 nM.

  • Smoothened Inhibitor in Clinical Trial

    LDE225 (NVP-LDE225,Erismodegib) : Phase III for Hh-pathway activated relapsed Medulloblastoma (MB).

  • Newest Smoothened Inhibitor

    GANT61 : Inhibitor for GLI1 as well as GLI2-induced transcription, inhibits hedgehog with IC50 of 5 μM, displays selectivity over other pathways, such as TNF and glucocorticoid receptor gene transactivation.

  • Smoothened Activator

    Purmorphamine : Directly binds and activates Smoothened, and blocks BODIPY-cyclopamine binding to Smo with IC50 of ~ 1.5 μM.

Related Hedgehog/Smoothened Products

  • Smoothened Agonist (SAG) HCl New

    Smoothened Agonist (SAG) HCl is a cell-permeable Smoothened (Smo) agonist with EC50 of 3 nM in Shh-LIGHT2 cells.

  • SB225002 New

    SB225002 is a potent, and selective CXCR2 antagonist with IC50 of 22 nM for inhibiting interleukin IL-8 binding to CXCR2, > 150-fold selectivity over the other 7-TMRs tested.

  • SB-334867 New

    SB-334867 is a selective orexin-1 (OX1) receptor antagonist.

  • Vismodegib (GDC-0449)

    Vismodegib (GDC-0449) is a potent, novel and specific hedgehog inhibitor with IC50 of 3 nM and also inhibits P-gp with IC50 of 3.0 μM in a cell-free assay.

  • Cyclopamine

    Cyclopamine is a specific Hedgehog (Hh) signaling pathway antagonist of Smoothened (Smo) with IC50 of 46 nM in TM3Hh12 cells.

  • GANT61

    GANT61 is an inhibitor for GLI1 as well as GLI2-induced transcription, inhibits hedgehog with IC50 of 5 μM in GLI1 expressing HEK293T cell, displays selectivity over other pathways, such as TNF and glucocorticoid receptor gene transactivation.

  • Purmorphamine

    Purmorphamine, which directly binds and activates Smoothened, blocks BODIPY-cyclopamine binding to Smo with IC50 of ~ 1.5 μM in HEK293T cell and also is an inducer of osteoblast differentiation with EC50 of 1 μM.

  • Taladegib (LY2940680)

    Taladegib (LY2940680) binds to the Smoothened (Smo) receptor and potently inhibits Hedgehog (Hh) signaling. Phase 1/2.

  • Glasdegib (PF-04449913)

    Glasdegib (PF-04449913) is a potent, and orally bioavailable Smoothened (Smo) inhibitor with IC50 of 5 nM. Phase 2.

  • SANT-1

    SANT-1 directly binds to Smoothened (Smo) receptor with Kd of 1.2 nM and inhibits Smo agonist effects with IC50 of 20 nM.

    Features:Attenuates SAG stimulation of Shh-LIGHT2 cells to a greater extent relative to other antagonists.

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Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID