Rigosertib (ON-01910)

Name: Rigosertib (ON-01910)
Brand: Selleck Chemicals
SKU: S1362
Rating: 5 (22 reviews)

For research use only.

Catalog No.S1362

22 publications

Rigosertib (ON-01910) Chemical Structure

Molecular Weight(MW): 473.47

Rigosertib (ON-01910) is a non-ATP-competitive inhibitor of PLK1 with IC50 of 9 nM in a cell-free assay. It shows 30-fold greater selectivity against Plk2 and no activity to Plk3. Phase 3.

Selleck's Rigosertib (ON-01910) has been cited by 22 publications

Nature, 2019, 10.1038/s41586-019-1607-3

PubMed: 31578521 ( click the link to review the publication )

Nature, 2019, 574(7777):268-272

PubMed: 31578521 ( click the link to review the publication )

Biology (Basel), 2020, 15;9(5):E99

PubMed: 32429320 ( click the link to review the publication )

Clin Cancer Res, 2019, 25(11):3384-3391

PubMed: 30846478 ( click the link to review the publication )

Toxicol Sci, 2019, 10.1093/toxsci/kfz123

PubMed: 31132080 ( click the link to review the publication )

Stem Cells Dev, 2019, 28(7):438-453

PubMed: 30667343 ( click the link to review the publication )

Neuron, 2018, 98(1):142-155

PubMed: 29551489 ( click the link to review the publication )

Pharmacol Res, 2018, 134:166-178

PubMed: 29944980 ( click the link to review the publication )

Sci Rep, 2018, 8(1):9991

PubMed: 29968772 ( click the link to review the publication )

Mol Cell, 2017, 68(1):210-223e6

PubMed: 28985505 ( click the link to review the publication )

Oncotarget, 2017, 8(58):97928-97940

PubMed: 29228663 ( click the link to review the publication )

Oncotarget, 2017, 9(13):10920-10933

PubMed: 29541386 ( click the link to review the publication )

Transl Res, 2016, 10.1016/j.trsl.2016.04.001

PubMed: 27150054 ( click the link to review the publication )

Cell Cycle, 2016, 15(15):2009-18

PubMed: 27249336 ( click the link to review the publication )

Exp Hematol, 2016, 44(4):247-56

PubMed: 26724640 ( click the link to review the publication )

J Control Release, 2015, 204:20-9

PubMed: 25681050 ( click the link to review the publication )

J Control Release, 2015, 204:20-29

PubMed: ( click the link to review the publication )

Endocr Relat Cancer, 2014, 13(5):1054-66

PubMed: 24748653 ( click the link to review the publication )

Sci Rep, 2014, 4:7310

PubMed: 25472472 ( click the link to review the publication )

Cancer Res, 2013, 73(20):6310-22

PubMed: 24067506 ( click the link to review the publication )

Stem Cells, 2013, 31(6):1051-63

PubMed: 23404835 ( click the link to review the publication )

PLoS One, 2013, 8(11):e79863

PubMed: 24223200 ( click the link to review the publication )

Purity & Quality Control

Choose Selective PLK Inhibitors

Biological Activity

Description

Rigosertib (ON-01910) is a non-ATP-competitive inhibitor of PLK1 with IC50 of 9 nM in a cell-free assay. It shows 30-fold greater selectivity against Plk2 and no activity to Plk3. Phase 3.

Targets

PLK1 ^[1] (Cell-free assay)	PDGFR ^[1] (Cell-free assay)	Bcr-Abl ^[1] (Cell-free assay)	Flt1 ^[1] (Cell-free assay)	Src ^[1] (Cell-free assay)	View More
9 nM	18 nM	32 nM	42 nM	155 nM	View More

In vitro

Rigosertib is non-ATP-competitive inhibitor to PLK1 with IC50 of 9 nM. Rigosertib also exhibits inhibition against PLK2, PDGFR, Flt1, BCR-ABL, Fyn, Src, and CDK1, with IC50 of 18-260 nM. Rigosertib shows cell killing activity against 94 different tumor cell lines with IC50 of 50-250 nM, including BT27, MCF-7, DU145, PC3, U87, A549, H187, RF1, HCT15, SW480, and KB cells. While in normal cells, such as HFL, PrEC, HMEC, and HUVEC, Rigosertib has little or no effect unless its concentration is greater than 5-10 μM. In HeLa cells, Rigosertib (100-250 nM) induces spindle abnormalities and apoptosis. ^[1] Rigosertib also inhibits several multidrug resistant tumor cell lines, including MES-SA, MES-SA/DX5a, CEM, and CEM/C2a, with IC50 of 50-100 nM. In DU145 cells, Rigosertib (0.25-5 μM) blocks cell cycle progression in G2/M phase, results in an accumulation of cells containing subG1 content of DNA, and activates apoptotic pathways. In A549 cells, Rigosertib (50 nM-0.5 μM) induces loss of viability and caspase 3/7 activation. ^[2] In a recent study, Rigosertib induces apoptosis in chronic lymphocytic leukemia (CLL) cells without toxicity against T-cells or normal B-cells. Rigosertib also abrogates the pro-survival effect of follicular dendritic cells on CLL cells and reduces SDF-1-induced migration of leukemic cells. ^[3]

Cell Data

Cell Lines	Assay Type	Concentration	Incubation Time	Activity Description	PMID
human K562 cells	M2D5W2N6fG:2b4jpZ:Kh[XO\|YYm=		NYDOR2o3QTZiaB?=	MnTMR5l1d3SxeHnjbZR6KGGpYXnud5QhcHWvYX6gT\|U3OiClZXzsd{Bi\nSncjC5OkBpenNiYomgeJJ6eGGwIHLseYUh\XilbIXzbY9vKGG\|c3H5MEBKSzVyPUeuOUBvVQ>?	NX;0NpNtOjF6MUK0NlE>
human T47D cells	M4DKeWN6fG:2b4jpZ:Kh[XO\|YYm=		NXfFfHRlPzJiaB?=	MmPmR5l1d3SxeHnjbZR6KGGpYXnud5QhcHWvYX6gWFQ4TCClZXzsd{Bi\nSncjC3NkBpenNiYomgUXRVKGG\|c3H5MEBIUTVyPUGwJI5O	Ml7rNlE1PjN7NES=
human HeLa cells	MW\Qdo9tcW[ncnH0bY9vKGG\|c3H5		MUm3NkBp	NV30RoJrSW62aYDyc4xq\mW{YYTpeoUh[WO2aY\peJkh[WejaX7zeEBpfW2jbjDI[WxiKGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeTygS2k2OD1zMjDuUS=>	NUK5NZdzOjR2N{G4O\|M>
human MDA468 cells	MmTmR5l1d3SxeHnjxsBie3OjeR?=		Mn\TO\|IhcA>?	MX3DfZRwfG:6aXPpeJkh[WejaX7zeEBpfW2jbjDNSGE1PjhiY3XscJMh[W[2ZYKgO\|IhcHK\|IHL5JG1VXCCjc4PhfUwhT0l3ME2yNEBvVQ>?	Ml7zNlE1PjN7NES=
human LNCAP cells	M4S0d3Bzd2yrZnXyZZRqd25iYYPzZZk>		MlzjO\|IhcA>?	M4PSVWFvfGmycn;sbYZmemG2aY\lJIFkfGm4aYT5JIFo[Wmwc4SgRXIheG:\|aYTpeoUhcHWvYX6gUG5ESVBiY3XscJMh[XO\|ZYPz[YQh[XNiY3XscEBoem:5dHigbY5pcWKrdHnvckBi\nSncjC3NkBpenNiYomgUXRVKGG\|c3H5MEBIUTVyPUK1JI5O	MVeyOFQ4OTh5Mx?=
human PANC1 cells	NWWyNXhVWHKxbHnm[ZJifGmxbjDhd5NigQ>?		NYnCfXJlPzJiaB?=	NIX3[2JCdnSrcILvcIln\XKjdHn2[UBi[3Srdnn0fUBi\2GrboP0JIh2dWGwIGDBUmMyKGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeTygS2k2OD1\|OTDuUS=>	MmC1NlQ1PzF6N{O=
human MCF7 cells	MU\Qdo9tcW[ncnH0bY9vKGG\|c3H5		MX:3NkBp	MmTURY51cXC{b3zp[oVz[XSrdnWgZYN1cX[rdImgZYdicW6\|dDDFVkBxd3OrdHn2[UBpfW2jbjDNR2Y4KGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeTygS2k2OD13MDDuUS=>	MUmyOFQ4OTh5Mx?=
human HCT116 cells	M{jJZWN6fG:2b4jpZ:Kh[XO\|YYm=		M1nOe\|czKGh?	MUPDfZRwfG:6aXPpeJkh[WejaX7zeEBpfW2jbjDIR3QyOTZiY3XscJMh[W[2ZYKgO\|IhcHK\|IHL5JG1VXCCjc4PhfUwhT0l3ME21NEBvVQ>?	NFLGUFAzOTR4M{m0OC=>
human MCF7 cells	MWHDfZRwfG:6aXRCpIF{e2G7		NYnBNYNlPzJiaB?=	NEHJcJBEgXSxdH;4bYNqfHliYXfhbY5{fCCqdX3hckBOS0Z5IHPlcIx{KGGodHXyJFczKGi{czDifUBOXFRiYYPzZZktKEeLNUC9OVAhdk1?	NGf2flgzOTR4M{m0OC=>
human MDA-MB-231 cells	NXjCZZFvWHKxbHnm[ZJifGmxbjDhd5NigQ>?		M4LDfVczKGh?	NXHQTmhpSW62aYDyc4xq\mW{YYTpeoUh[WO2aY\peJkh[WejaX7zeEBGWiCwZXfheIl3\SCqdX3hckBOTEFvTVKtNlMyKGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeR?=	M1TKdVI1PDdzOEez
human A2780 cells	NVnuZ2x6WHKxbHnm[ZJifGmxbjDhd5NigQ>?		MWW3NkBp	NHLBRY5CdnSrcILvcIln\XKjdHn2[UBi[3Srdnn0fUBi\2GrboP0JIh2dWGwIFGyO\|gxKGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeTygS2k2OD14MjDuUS=>	NU\3bWlJOjR2N{G4O\|M>
human HCT116 cells	MWHQdo9tcW[ncnH0bY9vKGG\|c3H5		NXnxVpNSPzJiaB?=	NGO1NWRCdnSrcILvcIln\XKjdHn2[UBi[3Srdnn0fUBi\2GrboP0JIh2dWGwIFjDWFEyPiClZXzsd{Bie3Onc4Pl[EBieyClZXzsJIdzd3e2aDDpcohq[mm2aX;uJIFnfGW{IEeyJIhzeyCkeTDNWHQh[XO\|YYmsJGdKPTB;N{Cgcm0>	NVW4d5A6OjR2N{G4O\|M>
human DU145 cells	NW\DR\|VOWHKxbHnm[ZJifGmxbjDhd5NigQ>?		NXfTbYRxPzJiaB?=	MUfBcpRqeHKxbHnm[ZJifGm4ZTDhZ5Rqfmm2eTDh[4FqdnO2IFHSJI5m\2G2aY\lJIh2dWGwIFTVNVQ2KGOnbHzzJIF{e2W\|c3XkJIF{KGOnbHyg[5Jwf3SqIHnubIljcXSrb36gZYZ1\XJiN{KgbJJ{KGK7IF3UWEBie3OjeTygS2k2OD15NTDuUS=>	Mk[0NlQ1PzF6N{O=
human DU145 cells	NXmz[XdlS3m2b4TvfIlkyqCjc4PhfS=>		MWe5OkBp	NFfFTFZEgXSxdH;4bYNqfHliYXfhbY5{fCCqdX3hckBFXTF2NTDj[YxteyCjZoTldkA6PiCqcoOgZpkhfHK7cHHuJIJtfWViZYjjcJV{cW:wIHHzd4F6NCCLQ{WwQVc2KG6P	NFThW5QzOThzMkSyNS=>
human MDA468 cells	NWPxVldlS3m2b4TvfIlkyqCjc4PhfS=>		M1;QdFQ5KGh?	NULER21KS3m2b4TvfIlkcXS7IHHnZYlve3RiaIXtZY4hVUSDNE[4JINmdGy\|IHHmeIVzKDR6IHjyd{BjgSCPVGSgZZN{[XluIFfJOVA:OC5\|MEKg{txO	Mo[yNlE1PjN7NES=
human MRC5 cells	MYPDfZRwfG:6aXRCpIF{e2G7		M1myXlczKGh?	NHjMZndEgXSxdH;4bYNqfHliYXfhbY5{fCCqdX3hckBOWkN3IHPlcIx{KGGodHXyJFczKGi{czDifUBOXFRiYYPzZZktKEeLNUC9NE44OSEQvF2=	M3PpS\|IyPDZ\|OUS0
human A2780 cells	MkiySpVv[3Srb36gZZN{[Xl?	M3vjcFAvOjVizszN	MVqyOEBp	MlruVoVlfWO2aX;uJIlvKE2lbEGgcIV3\WxiaX6gbJVu[W5iQUK3PFAh[2WubIOgZZQhOC5{NTD1UUBi\nSncjCyOEBpenNiYomgW4V{fGW{bjDicI91KGGwYXz5d4l{	MnWwNlQ1PzF6N{O=

... Click to View More Cell Line Experimental Data

Assay

Methods	Test Index	PMID
Western blot	pAbl / Abl / PCrk-L / Crk-L / Cleaved caspase3 / Cleaved PARP / pHistone H2A.X; PubMed: 26008977 Oncotarget Ba/F3 T315I cells were treated with rigosertib at the indicated concentrations for 24 h. Total extracts were examined via immunoblotting with anti-phospho ABL, phospho-Crk-L, phosphohistone H2A.X, cleaved caspase 3, cleaved-PARP, ABL, Crk-L, and β-actin antibodies (abs). ABL, Abelson; PARP, poly (ADP-ribose) polymerase; abs, antibodies.	26008977
Immunofluorescence	p-ATF / COX IV; PubMed: 27764820 Oncotarget Representative confocal microscopy images of FaDu, UMSCC 47 and D-HMVEC cells treated with rigosertib (1.0 μM) or ON 01911.Na (1.0 μM) for 24 h before fixing, staining with indicated antibodies, and capturing images. Green: p-ATF; Red: Cox IV (mitochondrial marker); Blue: DAPI (nuclear marker).	27764820
Growth inhibition assay	GI50; PubMed: 29108241 Oncotarget The GI50 values of BI2536, rigosertib, and poloxin were determined in both parental and volasertib-resistant R-MOLM14 and R-HL-60. Error bars represent the mean values ± S.D. of at least three independent experiments. Cell viability; PubMed: 27764820 Oncotarget Cell viability as measured by MTS. FaDu, Detroit 562, UMSCC 1, UMSCC 47 and UMSCC 104 cells were treated with increasing concentrations of rigosertib for 48 h, and cell viability was assessed. 50% growth inhibition (IC50) is recorded for each cell line in μM in the legend. Untreated cells were considered 100% viable and percent viability of cells treated with rigosertib was calculated vs. this control. Data represent the mean +/− SD of 3 independent experiments.	29108241 27764820

In vivo

In mouse xenograft models of Bel-7402, MCF-7, and MIA-PaCa cells, Rigosertib (250 mg/kg) markedly inhibits tumor growth. ^[1] Rigosertib (200 mg/kg) shows inhibition on tumor growth in a mouse xengraft model of BT20 cells. ^[2]

Protocol

Kinase Assay:^[1]	- Collapse In vitro enzyme assays for PLK1: Recombinant PLK1 (10 ng) is incubated with different concentrations of Rigosertib in a 15 µL reaction mixture (50 mM HEPES, 10 mM MgCl₂, 1 mM EDTA, 2 mM Dithiothreitol, 0.01% NP-40 [pH 7.5]) for 30 min at room temperature. Kinase reactions are performed for 20 min at 30 °C in a volume of 20 µL (15 µL enzyme + inhibitor, 2 µL 1 mM ATP), 2 µL of γ³²P-ATP (40 μCi), and 1 µL of recombinant Cdc25C (100 ng) or casein (1 μg) substrates. Reactions are terminated by boiling for 2 min in 20 µL of 2× Laemmli buffer. Phosphorylated substrates are separated by 18% SDS-PAGE. The gels are dried and exposed to X-ray film for 3-10 min.
Cell Research:^[2]	- Collapse Cell lines: A number of tumor cell lines, including BT20, MCF-7, DU145, PC3, U87, A549, H187, RF1, HCT15, HeLa, and Raji cells Concentrations: 1 nM - 10 μM, dissolved in DMSO as stock solution. Incubation Time: 96 hours Method: Cells are grown in either DMEM or RPMI supplemented with 10% fetal bovine serum and 1 unit/mL penicillin-streptomycin solution. Tumor cells are plated into six-well dishes at a density of 1 × 10⁵cells/mL/well, and Rigosertib is added 24 hours later at various concentrations. Cell counts are determined from duplicate wells after 96-hour of treatment. The total number of viable cells is determined by trypan blue exclusio (Only for Reference)
Animal Research:^[1]	- Collapse Animal Models: Mouse (female athymic, NCR-nu/nu) xenograft models of Bel-7402, MCF-7, and MIA-PaCa cells Dosages: 250 mg/kg Administration: Intraperitonially (Only for Reference)

References

Solubility (25°C)

In vitro	DMSO	95 mg/mL (200.64 mM)
	Water	95 mg/mL (200.64 mM)
	Ethanol	Insoluble
In vivo	Add solvents to the product individually and in order(Data is from Selleck tests instead of citations): water For best results, use promptly after mixing.	95mg/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 Download Rigosertib (ON-01910) SDF

Molecular Weight	473.47
Formula	C₂₁H₂₄NNaO₈S
CAS No.	1225497-78-8
Storage	3 years -20°C powder
Storage	2 years -80°C in solvent
Synonyms	N/A
Smiles	[Na+].COC1=CC(=C(\C=C\[S](=O)(=O)CC2=CC=C(OC)C(=C2)NCC([O-])=O)C(=C1)OC)OC

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Clinical Trial Information (data from https://clinicaltrials.gov, updated on 2020-05-15)

NCT Number	Recruitment	interventions	Conditions	Sponsor/Collaborators	Start Date	Phases
NCT04177498	Not yet recruiting	Drug: Rigosertib Sodium\|Other: Quality-of-Life Assessment	Recessive Dystrophic Epidermolysis Bullosa	Thomas Jefferson University\|Onconova Therapeutics Inc.	December 31 2019	Early Phase 1
NCT02075034	Suspended	Drug: rigosertib	Myelodysplastic Syndrome	Onconova Therapeutics Inc.	May 2014	Phase 1
NCT02030639	Completed	Drug: rigosertib	Healthy	Onconova Therapeutics Inc.	January 2014	Phase 1
NCT01928537	Active not recruiting	Drug: rigosertib sodium	Myelodysplastic Syndromes\|Refractory Anemia With Excess Blasts\|Chronic Myelomonocytic Leukemia\|Cytopenia	Onconova Therapeutics Inc.	August 2013	Phase 3
NCT01807546	Completed	Drug: rigosertib	Head and Neck Squamous Cell Carcinoma\|Anal Squamous Cell Carcinoma\|Lung Squamous Cell Carcinoma\|Cervical Squamous Cell Carcinoma\|Esophageal Squamous Cell Carcinoma\|Skin Squamous Cell Carcinoma\|Penile Squamous Cell Carcinoma	Onconova Therapeutics Inc.	March 2013	Phase 2
NCT01168011	Completed	Drug: rigosertib	Solid Tumor	Onconova Therapeutics Inc.	July 2010	Phase 1

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PLK Signaling Pathway Map

PLK Inhibitors with Unique Features

Pan Plk Inhibitors

BI 2536 : Pan-Plk1, Plk1, IC50=0.83 nM; Plk2, IC50=3.5 nM; Plk3, IC50=9 nM.
Most Potent Plk Inhibitor

BI 2536 : Plk1, IC50=0.83 nM.
Plk Inhibitor in Clinical Trial

Volasertib (BI 6727) : Phase III for acute myeloid leukaemia.
Newest Plk Inhibitor

Ro3280 ^New : Potent, highly selective inhibitor of Polo-like kinase 1 (PLK1) with IC50 of 3 nM.

Related PLK Products

SBE 13 HCl ^New

SBE 13 HCl is a potent and selective PLK1 inhibitor with IC50 of 200 pM, >4000-fold selectivity over Aurora A kinase, Plk2 and Plk3.
Ro-3306 ^New

RO-3306 is an ATP-competitive, and selective CDK1 inhibitor with K_i of 20 nM, >15-fold selectivity against a diverse panel of human kinases.
CCG-1423 ^New

CCG-1423 is a specific RhoA pathway inhibitor, which inhibits SRF-mediated transcription.
BI 2536

BI2536 is a potent Plk1 inhibitor with IC50 of 0.83 nM in a cell-free assay. It shows 4- and 11-fold greater selectivity against Plk2 and Plk3. Phase 2.

Features:The first potent and selective Plk1 inhibitor that induces all hallmarks of Plk1 inhibition.
HMN-214

HMN-214 is a prodrug of HMN-176, which alters the cellular spatial orientation of Plk1.
GSK461364

GSK461364 inhibits purified Plk1 with K_i of 2.2 nM in a cell-free assay. It is more than 1000-fold selective against Plk2/3. Phase 1.

Features:Demonstrates >390-fold selectivity for Plk1 relative to Plk2 and Plk3.
Volasertib (BI 6727)

Volasertib (BI 6727) is a highly potent Plk1 inhibitor with IC50 of 0.87 nM in a cell-free assay. It shows 6- and 65-fold greater selectivity against Plk2 and Plk3. Phase 3.

Features:A high volume of distribution, indicating good tissue penetration, and a long terminal half-life.
MLN0905

MLN0905 is a potent inhibitor of PLK1 with IC50 of 2 nM.
Ro3280

RO3280 is a potent, highly selective inhibitor of Polo-like kinase 1 (PLK1) with IC50 of 3 nM.

Features:A selective PLK1 inhibitor. Demonstrates greater potency than BI2536. Potential use in nasopharyngeal carcinomas.
onvansertib (NMS-P937)

onvansertib (NMS-P937) is an orally available, selective Polo-like Kinase 1 (PLK1) inhibitor with IC50 of 2 nM, 5000-fold selectivity over PLK2/PLK3. Phase 1.

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Rigosertib (ON-01910)