Belinostat (PXD101)

Catalog No.S1085 Synonyms: NSC726630, PX-105684

Belinostat (PXD101) Chemical Structure

Molecular Weight(MW): 318.35

Belinostat (PXD101) is a novel HDAC inhibitor with IC50 of 27 nM in a cell-free assay, with activity demonstrated in cisplatin-resistant tumors.

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Cited by 17 Publications

8 Customer Reviews

  • A375DR and parental cells were seeded 50,000 cells per well in 6-well plates and treated with 1 mMvorinostat (Vor), 0.5 mMbelinostat (Bel), 5 nMpanobinostat (Pan), and/or combination of 5 nM trametinib and 0.125 mM dabrafenib.

    Cell, 2018, 173(6):1413-1425. Belinostat (PXD101) purchased from Selleck.

    (C) Cell lysates were harvested from lung SCC cells after treatment with increasing doses of belinostat (0.1, 0.2, 0.3, 1, 3 lM). Immunoblotting was performed to evaluate the changes in phosphorylated protein levels of the targets identified in 1D (ERK1/2, p38, B-Raf, MEK1/2) as well as PARP. b-Actin shown as loading control.

    Mol Oncol, 2017, 11(8):965-980. Belinostat (PXD101) purchased from Selleck.

  • (B) Western blotting for cyclin D1. Cells were treated for 48 h with 5 μM belinostat and/or 25 or 50 μM ritonavir. Actin was used for the loading control. Representative blots are shown.

    Oncol Res, 2016, 24(5):327-335. Belinostat (PXD101) purchased from Selleck.

    Inhibition of LSD1 activity by HDAC inhibitors. a MDA-MB-231 and MDA-MB-468 cells were exposed to indicated HDAC inhibitors for 24 h.

    Breast Cancer Res Treat 2012 131, 777-789. Belinostat (PXD101) purchased from Selleck.

  • LSD1 and HDAC inhibitors exhibit synergistic growth inhibition. Cells were simultaneously treated with pargyline or HDAC inhibitors for 48 h.

     

     

    Breast Cancer Res Treat 2010 131(3), 777-789. Belinostat (PXD101) purchased from Selleck.

    HDACIs That Simultaneously Inhibit HDACs 1 and 6 Showed Greater Antileukemic Activities than HDACIs that Don,t at Cmax Concentrations. THP-1 cells were treated with LBH-589, PXD101, SAHA, VPA, MS-275 and MGCD0103 at Cmax concentrations for 3 h and 24 h, respectively. The cells post 3 h treatments were washed three times with complete medium and divided into two halves. One half of the cells was resuspended in complete media and cultured for up to 24 h to determine the effects of the 3 h treatments on cell proliferation and apoptosis. The other half of the cells was used to prepare whole cell lysates. Whole cell lysates from the 3 h and 24 h treatments were extracted and subjected to Western blots probed by anti-ac-tubulin or-β-actin antibody (panels A&B), or subjected to HDAC1 enzymatic assays post IP as described in the Materials and Methods (Panels C&D). The effects of the 3 h and 24 h HDACI treatments on cell proliferation, as reflected by percent decrease of live cells relative to untreated cells (panel E), and apoptosis (panel F) were determined by flow cytometry analysis as described in the Materials and Methods.

     

     

    PLoS One 2011 6, e17138. Belinostat (PXD101) purchased from Selleck.

  • Induction of DNA Damage and Bim Is Critical for HDACI-Induced Apoptosis in Pediatric AML Cells. THP-1 cells were treated with the HDACIs at Cmax concentrations for 3 (panel A) and 24 h (panel B), respectively. Whole cell lysates were extracted and subjected to Western blots probed by anti-p21, -c-Myc, -cH2AX, -Bim, or -β-actin antibody.

     

     

    PLoS One 2011 6, e17138. Belinostat (PXD101) purchased from Selleck.

    MDA-MB-231 Breast cancer cells were pretreated with Acetyl-H3 and H3, and then treated with the indicated concentrations of  PXD101.

    Dr. Zhang of Tianjin Medical University. Belinostat (PXD101) purchased from Selleck.

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Biological Activity

Description Belinostat (PXD101) is a novel HDAC inhibitor with IC50 of 27 nM in a cell-free assay, with activity demonstrated in cisplatin-resistant tumors.
Features Lead compound of Topotarget.
Targets
HDAC [1]
(Cell-free assay)
27 nM
In vitro

Belinostat inhibits the growth of tumor cells (A2780, HCT116, HT29, WIL, CALU-3, MCF7, PC3 and HS852) with IC50 from 0.2-0.66 μM. PD101 shows low activity in A2780/cp70 and 2780AD cells, which are cisplatin and doxorubicin-resistant derivatives of A2780 cells. Belinostat could induce apoptosis through PARP cleavage and acetylation of histones H3/H4. [1] Belinostat inhibits bladder cancer cell growth, especially in 5637 cells, which shows accumulation of G0-G1 phase, decrease in S phase and increase in G2-M phase. [2] The growth inhibitory activity of belinostat on cell lines is not strongly influenced by the multidrug-resistant phenotype, whereas the activity of docetaxel is clearly affected. Belinostat could enhance the growth inhibitory activity of docetaxel or carboplatin in OVCAR-3 and A2780 cells. Belinostat also shows enhanced tubulin acetylation in ovarian cancer cell lines. [3] A recent study shows that Belinostat activates protein kinase A in a TGF-β signaling-dependent mechanism and decreases survivin mRNA. [4]

Cell Data
Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID
NB4 MXnD[YxtKF[rYXLpcIl1gSCDc4PhfS=> NXXP[oJjOC5{L{NCpO69VQ>? NYTHfZRxOjRxNEivO|IhcA>? Mn7s[IVkemWjc3XzJINmdGxidnnhZoltcXS7IHnuJIJwfGhidHnt[UBidmRiZH;z[UBl\XCnbnTlcpQhdWGwbnXy NHrXR2UzPTh4NEezNi=>
HL-60  MVnD[YxtKF[rYXLpcIl1gSCDc4PhfS=> NYLubYF{OC5{L{NCpO69VQ>? M1fuWlI1NzR6L{eyJIg> M3jYSIRm[3KnYYPld{Bk\WyuII\pZYJqdGm2eTDpckBjd3SqIITpcYUh[W6mIHTvd4Uh\GWyZX7k[Y51KG2jbn7ldi=> NEjVc20zPTh4NEezNi=>
NB4 NHLYWG1HfW6ldHnvckBCe3OjeR?= M{LmPFLDqM7:TR?= Mmr2NlQwPDhiaB?= NGTncmpjdG:la4OgZ4VtdCCleXPs[UBqdiCVIIDoZZNm NGHCT2czPTh4NEezNi=>
HL-60  NHXC[ZZHfW6ldHnvckBCe3OjeR?= M3mwdlLDqM7:TR?= NVnOdWNOOjRxNEigbC=> NIXISmJjdG:la4OgZ4VtdCCleXPs[UBqdiCVIIDoZZNm NGHibFMzPTh4NEezNi=>
NB4 MVnGeY5kfGmxbjDBd5NigQ>? NIH0T5oxNjMEoN88US=> NFXX[IUzPC92OD:3NkBp MULlcohidmOnczDSRU1qdmS3Y3XkJIdz[W63bH;jfZRq[yCmaX\m[ZJmdnSrYYTpc44> MlvxNlU5PjR5M{K=
HL-60  MUPGeY5kfGmxbjDBd5NigQ>? MV2wMlLDqM7:TR?= MlfYNlQwPDhxN{KgbC=> NWLyTIFH\W6qYX7j[ZMhWkFvaX7keYNm\CCpcnHueYxw[3m2aXOg[Iln\mW{ZX70bYF1cW:w MoH3NlU5PjR5M{K=
PANC-1 NH\oVpBHfW6ldHnvckBCe3OjeR?= NYLuNoc{OTEEoN88US=> NF3MUVEzNzRxNjDo MoTjSG1UVw>? NV7US2E6cW6mdXPld{BCVVCNIHHjeIl3[XSrb36= NV;JTms{OjN5NEOxPVg>
PANC-1 NWD3cGZbS2WubDDWbYFjcWyrdImgRZN{[Xl? MlLsNU8yOMLizszN Mn7ZOFghcA>? MmHFSG1UVw>? NX7jZ|BX\GWlcnXhd4V{KGOnbHygeoli[mmuaYT5JIlvKGFiZH;z[UBl\XCnbnTlcpQhdWGwbnXy MVyyN|c1OzF7OB?=
PANC-1 M{fz[mZ2dmO2aX;uJGF{e2G7 NV\aXpd7OTEEoN88US=> NIrHPXkzNzRiaB?= MYTEUXNQ MnPzbY5kemWjc3XzJIlvfHKjY3XscJVt[XJiUl;TJIxmfmWu MVuyN|c1OzF7OB?=
H1666 NX;E[5hiT3Kxd4ToJGlvcGmkaYTpc44hSXO|YYm= MVK3NuKhcA>? MXjEUXNQ Ml;mTWM2OD5zMDFOwG0> M3;jdlI{PTF3N{Wy
H460 NWLDS5duT3Kxd4ToJGlvcGmkaYTpc44hSXO|YYm= Mo\PO|LDqGh? MmnrSG1UVw>? M4jxbWlEPTB;MD64OkDPxE1? M4XuVFI{PTF3N{Wy
H1299 Mor3S5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? NF3EVWI4OsLiaB?= MVnEUXNQ NYDuU2pwUUN3ME2xMlIh|ryP MoHFNlM2OTV5NUK=
H520 MnTTS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? NG\RXVY4OsLiaB?= NEW5THFFVVOR NYj4[4o2UUN3ME2wMlc2KM7:TR?= MWSyN|UyPTd3Mh?=
H1975 M4LoeGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7 NFzNfVI4OsLiaB?= NVHFeWtiTE2VTx?= NXHVU|V3UUN3ME2wMlY5KM7:TR?= M1rmbVI{PTF3N{Wy
H1650 Mn3kS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? MXG3NuKhcA>? MoL2SG1UVw>? M1uwU2lEPTB;MD64PEDPxE1? NX;uWZV4OjN3MUW3OVI>
H820 NF3xe5VIem:5dHigTY5pcWKrdHnvckBCe3OjeR?= MoHJO|LDqGh? NIDoVZNFVVOR NGLLOmtKSzVyPUCuOEDPxE1? MX[yN|UyPTd3Mh?=
PC9 NXrwTIk4T3Kxd4ToJGlvcGmkaYTpc44hSXO|YYm= NEGySWw4OsLiaB?= Mlz2SG1UVw>? M2PUOmlEPTB;MD6yPUDPxE1? NYfmWIRiOjN3MUW3OVI>
HCC2279 M4Dxb2dzd3e2aDDJcohq[mm2aX;uJGF{e2G7 MXq3NuKhcA>? MkTuSG1UVw>? Mlu4TWM2OD1yLkSg{txO MlXENlM2OTV5NUK=
HCC827 MW\Hdo94fGhiSX7obYJqfGmxbjDBd5NigQ>? MXy3NuKhcA>? MlrwSG1UVw>? NH6wb4NKSzVyPUCuNlkh|ryP M323PVI{PTF3N{Wy
HCC2935 NXzJd41UT3Kxd4ToJGlvcGmkaYTpc44hSXO|YYm= M4nFS|czyqCq M1rOSWROW09? MXfJR|UxRTBwOUeg{txO Ml\SNlM2OTV5NUK=
HCC4006 M2rQ[Gdzd3e2aDDJcohq[mm2aX;uJGF{e2G7 NIDTNo04OsLiaB?= NVHP[WliTE2VTx?= MmXUTWM2OD1yLkS2JO69VQ>? MWmyN|UyPTd3Mh?=
H460 MYPGeY5kfGmxbjDBd5NigQ>? NYDlOHc{PTBywrDuUS=> M37qV|I1yqCq MkTGSG1UVw>? M1PMT4Rm[3KnYYPld{BGT0[UIHX4dJJme3Orb36= NV\JVYdLOjN3MUW3OVI>
H1650 MlT2SpVv[3Srb36gRZN{[Xl? MWW1NFDDqG6P NFiyV4IzPMLiaB?= NGXjc2ZFVVOR M3Pv[IRm[3KnYYPld{BGT0[UIHX4dJJme3Orb36= MXeyN|UyPTd3Mh?=
PC9 NH7IcIFHfW6ldHnvckBCe3OjeR?= M{PVc|UxOMLibl2= MnzPNlTDqGh? M13YXGROW09? MWrk[YNz\WG|ZYOgSWdHWiCneIDy[ZN{cW:w NFHkc5ozOzVzNUe1Ni=>
H460 NHLpVlVHfW6ldHnvckBCe3OjeR?= M4nU[VAvPS9zL{Kg{txO MnzFOEBp MnH5SG1UVw>? MULpcohq[mm2czD0bIUhdGW4ZXzzJI9nKEGtdDCodE1Cc3RrIHHu[EBGT0[U NIOwSVkzOzVzNUe1Ni=>
H1650 M164NWZ2dmO2aX;uJGF{e2G7 MY[wMlUwOS9{IN88US=> MorlOEBp M3jRW2ROW09? MWLpcohq[mm2czD0bIUhdGW4ZXzzJI9nKEGtdDCodE1Cc3RrIHHu[EBGT0[U MlrVNlM2OTV5NUK=
PC9 M1rTOWZ2dmO2aX;uJGF{e2G7 NVHwcZZ4OC53L{GvNkDPxE1? M4nXTlQhcA>? NGrxeYhFVVOR MWfpcohq[mm2czD0bIUhdGW4ZXzzJI9nKEGtdDCodE1Cc3RrIHHu[EBGT0[U NFPZNnQzOzVzNUe1Ni=>
AsPc1 NHjH[lRIem:5dHigTY5pcWKrdHnvckBCe3OjeR?= NWfncI5yPDhiaB?= M1T0RmVEPTB;MD6zJO69VQ>? NHTxXlUzOzR5NU[5OS=>
Panc0327 NV3iRWYyT3Kxd4ToJGlvcGmkaYTpc44hSXO|YYm= M2HaelQ5KGh? NEHtVFBGSzVyPUCuOUDPxE1? MYqyN|Q4PTZ7NR?=
MiaPaCa2 M1W3WGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7 NXmyUHozPDhiaB?= NWixd5BlTUN3ME2wMlch|ryP MWeyN|Q4PTZ7NR?=
BxPc3 MXTHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>? NGHmNW41QCCq MU\FR|UxRTFwMDFOwG0> NXeyTXpMOjN2N{W2PVU>
Panc0403 Ml3YS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? M{DtfFQ5KGh? NW\JUG13TUN3ME2xMlEh|ryP MUeyN|Q4PTZ7NR?=
Panc1005 NHT1Z3JIem:5dHigTY5pcWKrdHnvckBCe3OjeR?= M2XYOVQ5KGh? NUXM[IdQTUN3ME2xMlEh|ryP NY\nPWMxOjN2N{W2PVU>
PL45 MX;Hdo94fGhiSX7obYJqfGmxbjDBd5NigQ>? MXu0PEBp M1LwV2VEPTB;MkCuPEDPxE1? MY[yN|Q4PTZ7NR?=
Panc0203 MYfHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>? MlW1OFghcA>? MWPFR|UxRTJ{LkKg{txO MWWyN|Q4PTZ7NR?=
Panc0327 NH7QVnFCeG:ydH;zbZMhSXO|YYm= NVixRpFqOSEQvF2= M4ftUVI1KGh? M2HBfYlv\HWlZYOgZZBweHSxc3nz MWSyN|Q4PTZ7NR?=
Panc1005 MmTSRZBweHSxc3nzJGF{e2G7 NVfUZ5hTOSEQvF2= NV2wd4c3OjRiaB?= M1rPOIlv\HWlZYOgZZBweHSxc3nz NH3aZXEzOzR5NU[5OS=>
Panc0403 M3j4dmFxd3C2b4Ppd{BCe3OjeR?= NIPN[GgyKM7:TR?= MV[yOEBp MXvpcoR2[2W|IHHwc5B1d3Orcx?= M4LKN|I{PDd3Nkm1
AsPc1 M{\rc2Z2dmO2aX;uJGF{e2G7 MnPVNU8yOCEQvF2= NUXYb4tMOjRiaB?= M3rjU4lv\HWlZYOgJIdzd3e2aDDhdpJme3SnZDDpckBIOi:P NGH6RWYzOzR5NU[5OS=>
MiaPaCa2 NXv1NVFETnWwY4Tpc44hSXO|YYm= MYWxM|ExKM7:TR?= NI[5OZczPCCq NFvJPZpqdmS3Y3XzJEBoem:5dHigZZJz\XO2ZXSgbY4hTzJxTR?= M4\EcFI{PDd3Nkm1
T3M4 MlnmS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? NFWwRmoxNThyMDDuUS=> M1r5WFQ5KGh? M{XPcIlvcGmkaYTzJINmdGxicILvcIln\XKjdHnvckBqdiCjIHTvd4Uh\GWyZX7k[Y51KG2jbn7ldi=> NWPUNXJHOjJ4OEG2PVg>
AsPC-1 NIOxUFhIem:5dHigTY5pcWKrdHnvckBCe3OjeR?= M4C2U|AuQDByIH7N NH7wcmo1QCCq MX;pcohq[mm2czDj[YxtKHC{b3zp[oVz[XSrb36gbY4h[SCmb4PlJIRmeGWwZHXueEBu[W6wZYK= MWGyNlY5OTZ7OB?=
Panc-1  MnezS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? NHnsNVkxNThyMDDuUS=> MYW0PEBp MX3pcohq[mm2czDj[YxtKHC{b3zp[oVz[XSrb36gbY4h[SCmb4PlJIRmeGWwZHXueEBu[W6wZYK= M4HLNVIzPjhzNkm4
T3M4 M2fDbGFxd3C2b4Ppd{BCe3OjeR?= NUjxZmNNOTByL{WwNE8yODByIH7N NEXLcmU1QCCq NX3a[4d4cW6mdXPld{Bld3OnIHTldIVv\GWwdDDhdI9xfG:|aYO= NWjzToJrOjJ4OEG2PVg>
AsPC-1 MYnBdI9xfG:|aYOgRZN{[Xl? M{DQcVExOC93MECvNVAxOCCwTR?= M2jmVlQ5KGh? M2nZV4lv\HWlZYOg[I9{\SCmZYDlcoRmdnRiYYDvdJRwe2m| M33lO|IzPjhzNkm4
Panc-1  NIHjb3FCeG:ydH;zbZMhSXO|YYm= M{TROlExOC93MECvNVAxOCCwTR?= M1f6d|Q5KGh? M{C4TYlv\HWlZYOg[I9{\SCmZYDlcoRmdnRiYYDvdJRwe2m| MYqyNlY5OTZ7OB?=
HBL-2 MorvS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? M2fuRlI1KGh? NUntWWI5UUN3ME2wMlQh|ryP NYrwcHprOjByNkiwPFA>
Jeko-1 NETHbFlIem:5dHigTY5pcWKrdHnvckBCe3OjeR?= MX2yOEBp MY\JR|UxRTBwMjFOwG0> NUD4PVNHOjByNkiwPFA>
Granta-519 MYTHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>? MYqyOEBp MlvwTWM2OD13Nj6zJO69VQ>? M4LVR|IxODZ6MEiw
HCT116 Mle0S5Jwf3SqIFnubIljcXSrb36gRZN{[Xl? NYrRO29kPDhiaB?= NILyZYlGSzVyPUCuNlgh|ryP MlvuNVcyOjR3OUS=
HCT116 NXf2Z5MzTnWwY4Tpc44hSXO|YYm= MX:wMlnDqM7:TdMg NH3odIYzPCCq NVLPeGVs\G:5bj3y[Yd2dGG2czDUV{Bxem:2ZXnuJIxmfmWuczDh[pRmeiB4wrDoJIlv[3WkYYTpc44> NELLOmIyPzF{NEW5OC=>

... Click to View More Cell Line Experimental Data
In vivo Belinostat indicates significant tumor growth delay in A2780 and A2780/cp70 xenograft at a dose of 10mg/kg with no effects on the body weight. [1] Belinostat also induces p21WAF1, HDAC core and cell communication genes in mouse bladder tumors. [2] Belinostat monotherapy induces dose-proportional antitumor effects with TGI of 47% at a dose of 100mg/kg in A2780 xenograft. The combination of Belinostat (100 mg/kg) with carboplatin (40 mg/kg) could delay tumor growth from 18.6 days to 22.5 days. [3] Combining with bortezomib, Belinostat results in great tumor inhibition and gastrointestinal toxicity in mice with bortezomib-resistant UMSCC-11A xenograft. [5]

Protocol

Kinase Assay:[1]
+ Expand

Histone Deacetylase Activity:

Subconfluent cultures are harvested and washed twice in ice cold PBS and pelleted by centrifugation at 200 × g for 5 min. The cell pellet is resuspended in two volumes of lysis buffer [60 mM Tris buffer (pH 7.4) containing 30% glycerol and 450 mM NaCl] and lysed by three freeze (dry ice) thaw (30 °C water bath) cycles. Cell debris is removed by centrifugation at 1.2 × 104 g for 5 min, and the supernatant is stored at −80 °C. Histone H4 peptide (sequence SGRGKGGKGLGKGGAKRHRK corresponding to the 20 NH2-terminal residues) is acetylated by a recombinant protein containing the hypoxanthine-aminopterin-thymidine domain of p300, using [3H]acetyl CoA as a source of acetate. H4 peptide (100 μg) is mixed with hypoxanthine-aminopterin-thymidine buffer (50 mM Tris HCl pH 8.0, 5% glycerol, 50 mM KCl, and 0.1 mM EDTA), 1 mM DTT, 1 mM 4-(2-aminoethyl) benzenesulfonylfluoride, 1 × complete protease inhibitors, 50 μL of purified p300, and 1.85 m [3H]acetyl CoA (4.50Ci/mmol) in a final volume of 300 μL and incubated at 30 °C for 45 min. The p300 protein is removed by incubation with 20 μL of 50% Ni-agaroase beads for 1 hour at 4 °C and centrifugation. The supernatant is applied to a 2 mL Sephadex G15 column, and the flow through is collected. One milliliter of distilled H2O is gently applied, and three drop fractions are collected; this is repeated until 4–5 mL of distilled H2O has been added, and ∼40 fractions are collected. Three microliters of each fraction are diluted in 2 mL of scintillation fluid and counted in a scintillation counter to identify the fractions containing the labeled peptide. These fractions are pooled, and 1 μL of the combined sample is measured to assess the radioactivity in every peptide batch (3-7×103 cpm/μL). For activity assays, the reaction is carried out in a total volume of 150 μL of buffer [60 mM Tris (pH 7.4) containing 30% glycerol] containing 2 μL of cell extract and, where used, 2 μL of belinostat. The reaction is started by the addition of 2 μL of [3H] labeled substrate (acetylated histone H4 peptide corresponding to the 20 NH2-terminal residues). Samples are incubated at 37 °C for 45 min, and the reaction stopped by the addition of HCl and acetic acid (0.72 and 0.12 M final concentrations, respectively). Released [3H]acetate is extracted into 750 μL of ethyl acetate, and samples are centrifuged at 1.2× 104 g for 5 min. The upper phase (600 μL) is transferred to 3 mL of scintillation fluid and counted.
Cell Research:[1]
+ Expand
  • Cell lines: A2780, A2780/cp70, 2780AD, HCT116, HT29, WIL, CALU-3, MCF7, PC3 and HS852
  • Concentrations: 0.016 - 10 μM
  • Incubation Time: 24 hours
  • Method: Tumor cell lines are seeded in 5 mL of medium at a density of 8 × 104 cells/25 cm2 flask and incubated for 48 hours. Cells are exposed to Belinostat (0.016 to 10 μM) for 24 hours. The medium is removed, and 1 mL of trypsin/EDTA is added to each flask. Once the cells have detached, 1 mL of medium is added, the cells are resuspended, and those from the control untreated flask are counted. Cells are diluted and plated into 6-cm Petri dishes (three per flask) at a density of 0.5-2× 103 cells/dish depending on the cell line. Cells from the drug-treated flasks are diluted and plated as for the control flasks. Dishes are incubated for 10–15 days at 37 °C. Cells are washed with PBS, fixed in methanol, and stained with crystal violet, and colonies that contained ≥50 cells counted. Sensitivity is expressed as the IC50 defined as the concentration of belinostat required to reduce the number of colonies to 50% of that of the control untreated cells.
    (Only for Reference)
Animal Research:[1]
+ Expand
  • Animal Models: A2780, A2780/cp70 and HCT116 cells are injected s.c. into the right flank of CD1 nu/nu mice.
  • Formulation: Dissolved in DMSO and then diluted in water to give a final concentration of DMSO of 10%
  • Dosages: ≤40 mg/kg
  • Administration: Administered via i.p.
    (Only for Reference)

Solubility (25°C)

In vitro DMSO 64 mg/mL (201.03 mM)
Water Insoluble
Ethanol Insoluble
In vivo Add solvents to the product individually and in order(Data is from Selleck tests instead of citations):
2% DMSO+30% PEG 300+ddH2O
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 318.35
Formula

C15H14N2O4S
CAS No. 414864-00-9
Storage powder
in solvent
Synonyms NSC726630, PX-105684

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    C2=C1/X C2: LOG(C2):
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    C4=C3/X C4: LOG(C4):
    C5=C4/X C5: LOG(C5):
    C6=C5/X C6: LOG(C6):
    C7=C6/X C7: LOG(C7):
    C8=C7/X C8: LOG(C8):
Molecular Weight Calculator

Molecular Weight Calculator

Enter the chemical formula of a compound to calculate its molar mass and elemental composition:

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To calculate molar mass of a chemical compound, please enter its chemical formula and click 'Calculate'.

Definitions of molecular mass, molecular weight, molar mass and molar weight:

Molecular mass (molecular weight) is the mass of one molecule of a substance and is expressed in the unified atomic mass units (u). (1 u is equal to 1/12 the mass of one atom of carbon-12)
Molar mass (molar weight) is the mass of one mole of a substance and is expressed in g/mol.

Molarity Calculator

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Clinical Trial Information

NCT Number Recruitment Conditions Sponsor/Collaborators Start Date Phases
NCT03432741 Recruiting Breast Adenocarcinoma|Recurrent Breast Carcinoma|Recurrent Hodgkin Lymphoma|Recurrent Mycosis Fungoides|Recurrent Non-Hodgkin Lymphoma|Recurrent Primary Cutaneous T-Cell Non-Hodgkin Lymphoma|Refractory Hodgkin Lymphoma|Refractory Mycosis Fungoides|Refractory Nodal Marginal Zone Lymphoma|Refractory Non-Hodgkin Lymphoma|Refractory Primary Cutaneous T-Cell Non-Hodgkin Lymphoma|Stage IV Breast Cancer AJCC v6 and v7 Mayo Clinic|National Cancer Institute (NCI) March 27 2018 Phase 1
NCT02737046 Recruiting Adult T-cell Leukemia-Lymphoma|ATLL University of Miami December 12 2016 Phase 2
NCT02875002 Withdrawn Relapsed and Refractory Aggressive B- and T-cell Lymphomas|Lymphoma Yale University|Massey Cancer Center|Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins October 2016 Phase 1
NCT02701673 Withdrawn Lymphoma M.D. Anderson Cancer Center June 2016 Phase 1|Phase 2
NCT02680795 Recruiting Solid Tumors|Hematological Malignancies Spectrum Pharmaceuticals Inc March 2016 Phase 1
NCT02679131 Terminated Relapsed/Refractory Solid Tumors/Hematological Malignancies Spectrum Pharmaceuticals Inc March 2016 Phase 1

Tech Support

Answers to questions you may have can be found in the inhibitor handling instructions. Topics include how to prepare stock solutions, how to store inhibitors, and issues that need special attention for cell-based assays and animal experiments.

Handling Instructions

Tel: +1-832-582-8158 Ext:3

If you have any other enquiries, please leave a message.

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Frequently Asked Questions

  • Question 1:

    Could you please give some suggestions for the use of Belinostat in vivo (i.p. injection)?

  • Answer:

    For I.P. injection, S1085 Belinostat (PXD101) can be dissolved in 2% DMSO+30% PEG 300+ddH2O at 10 mg/ml clearly. When preparing the solution, please dissolve the compound in DMSO clearly first. Then add PEG, after they mixed well, then dilute with water. Hope this information is useful to you.

selleck catalog

HDAC Signaling Pathway Map

HDAC Inhibitors with Unique Features

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Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID