Talazoparib (BMN 673)

Catalog No.S7048 Synonyms: LT-673

Molecular Weight(MW): 380.35

Talazoparib (BMN 673) is a novel PARP inhibitor with IC50 of 0.57 nM for PARP1 in a cell-free assay. It is also a potent inhibitor of PARP-2, but does not inhibit PARG and is highly sensitive to PTEN mutation. Phase 3.

5 Customer Reviews

DNA damage persists on withdrawal of PARPi in RNASEH2AKO cells. Wild-type and RNASEH2AKO HeLa cells were treated with talazoparib and released into fresh medium for the indicated times before being processed for γ-H2AX immunofluorescence and propidium iodide (PI) staining. The γ-H2AX immunofluorescence (pseudocolor plots) and cell cycle (histograms) FACS profiles shown are representative of three biologically independent experiments.

Nature, 2018, 559(7713):285-289. Talazoparib (BMN 673) purchased from Selleck.

Western blot assessment of effects on PAR, PARP, and dsDNA breaks mediated by IMMU-132 plus PARPi in TNBC tumor lines. Cells were plated overnight in 6-well plates before the addition of chemotherapeutics. After a 24-hour incubation, cells were harvested and cell lysates resolved and transferred for Western analysis as described in Materials and Methods. PAR and FL-PARP levels were determined on the same gel. Assessment of dsDNA breaks (p-H2A.X) was calculated as ratios relative to untreated control (Unt) normalized to b-actin protein loading control (Dp-H2A.X). B, HCC1806 cells exposed to rucaparib (Ruc) and IMMU-132 or to (C) talazoparib (Tala) and IMMU-132.

Clin Cancer Res, 2017, 23(13):3405-3415. Talazoparib (BMN 673) purchased from Selleck.
PARP inhibition prevents adhesion to and migration of monocytes across BMVEC monolayers preserving the barrier. Primary human monocytes were treated for 24 h with PARPi (AIQ, olaparib, EB47, talazoparib), calcein-labeled, washed, and then added to BMVEC monolayers (untreated or treated for 24 h with TNFα). Treatments were removed prior to the addition of monocytes. Adhesion to (a) and migration of (b) monocytes across blood-brain barrier models were measured and are presented as fold difference compared to TNFα-only control (mean ± SEM) for each treatment from at least quadruplicate determinations, which was assigned a value of 1 (7600 relative fluorescent units for adhesion or equivalent to 37 migrated cells). *P < 0.05, **P < 0.01 indicate significance vs. non-treated. TEER, an indicator of barrier integrity, was continuously measured in BMVEC monolayers treated with or without TNFα following the addition of primary human monocytes that had been treated with PARPi.

J Neuroinflammation, 2016, 13(1):254.. Talazoparib (BMN 673) purchased from Selleck.

BT-549 cells reconstituted with Vet, WT, 336* or PTEN WT HP1aKD were treated with BMN673. Relative cell viability was determined by MTT assay. The results were presented as mean of 3 independent experiments. Error bars indicate s.d.

Cell Cycle, 2015, 14(14): 2323-32. Talazoparib (BMN 673) purchased from Selleck.
We treated the FA defective and control lung cancer cell lines H1299D2-down/H1299E and A549D2 down/A549E with BMN673 (0.5 µM). MTT assay was used for the cell viability analysis and an averaged absorbance was recorded 24, 48 and 72 h post treatment.

Front Oncol, 2014, 4: 368. Talazoparib (BMN 673) purchased from Selleck.

Purity & Quality Control

Choose Selective PARP Inhibitors

Biological Activity

Description

Features

Most potent and selective PARPi reported thus far.

Targets

PARP1 ^[1]
(Cell-free assay)

0.57 nM

In vitro

BMN-673 selectively binds to PARP and prevents PARP-mediated DNA repair of single strand DNA breaks via the base-excision repair pathway. This enhances the accumulation of DNA strand breaks, promotes genomic instability and eventually leads to apoptosis. BMN 673 selectively kills cancer cells with BRCA-1 or BRCA-2 mutations. BMN 673 demonstrates single-agent cytotoxicityin BRCA-1 mutant (MX-1, IC50 = 0.3 nM) and BRCA-2 mutant cells (Capan-1, IC50 = 5 nM). In contrast, in MRC-5 normal human fibroblastand other tumor cell lines with wild-type BRCA-1 and BRCA-2 genes, IC50 of BMN 673 ranges between 90 nM and 1.9 μM. ^[1] In cultured human cancer cells, BMN 673 also significantly enhances the cytotoxic efficacy of both Temozolomide and SN-38. Off-target molecular screening did not identify significant non-specific activity for this class of PARP inhibitors. ^[2]

Cell Data

Cell Lines	Assay Type	Concentration	Incubation Time	Activity Description	PMID
BR5FVB1-Akt	MYTHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?	MYmwMlEuOTByIH7N	MmPONlQwPDhxN{KgbC=>	MV;pcohq[mm2czDj[YxtKHC{b3zp[oVz[XSrb36g[I9{\SCmZYDlcoRmdnSueR?=	MlHUNlYxPDd4OUe=
BR5FVB1-Akt	M33I[2Fxd3C2b4Ppd{BCe3OjeR?=	MnX4NE4yNTFyMDDuUS=>	MmLqO\|IhcA>?	MlGybY5lfWOnczDhdI9xfG:\|aYO=	NWHybpU6OjZyNEe2PVc>
Capan-1	M1nDRmdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			MVHJR\|UxRTF4LkFihKnDueLCiUWuOQKBkcL3TdMg	NWPHVXhvOjV6NkS1PVA>
MIA PaCa-2	Mk[zS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			MkK4TWM2OD13OD6yN-KBkcLz4pEJPE4y6oDLwsXNxsA>	NEG3SIozPTh4NEW5NC=>
RD	MXjHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			M3SzTmlEPTB;OD63JI5O	NEfLcnQzPTJ4M{WzPS=>
Rh41	MXjHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			MnW1TWM2OD16LkGgcm0>	M2L6[VI2OjZ\|NUO5
Rh18	MVTHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			MUjJR\|UxRTRwOTDuUS=>	NVH4e2pXOjV{NkO1N\|k>
Rh30	MVrHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			NH:1RVNKSzVyPUOxMlEhdk1?	NV3iPWlnOjV{NkO1N\|k>
BT-12	M1TvVGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			M1PSWWlEPTB-4pEJNUwxODBibl2=	M1qxZlI2OjZ\|NUO5
CHLA-266	MoW4S5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			M3PkWmlEPTB-4pEJNUwxODBibl2=	NWjqUXlIOjV{NkO1N\|k>
TC-71	M3u5XGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			NXrX[YVRUUN3ME2zMlchdk1?	NGPCXlczPTJ4M{WzPS=>
CHLA-9	MmW3S5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			Mlr2TWM2OD16LkKgcm0>	MkKzNlUzPjN3M{m=
CHLA-10	MkSwS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			NXjDRnBOUUN3ME22O{45KG6P	Ml7lNlUzPjN3M{m=
CHLA-258	MWfHdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			NHjyZXdKSzVyPUSuOkBvVQ>?	M3fROlI2OjZ\|NUO5
SJ-GBM2	NGHyOGtIem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			NIHBR4NKSzVyPUG2MlIhdk1?	M1H2O\|I2OjZ\|NUO5
NB-1643	Mk[3S5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			M1zZXGlEPTB;MUiuOEBvVQ>?	Ml73NlUzPjN3M{m=
NB-EBc1	M3[3OWdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			NEn6bZRKSzVyPUK1Mlghdk1?	NHLOenozPTJ4M{WzPS=>
CHLA-90	M3TTTGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			M2G2RmlEPTB-4pEJNUwxODBibl2=	MWKyOVI3OzV\|OR?=
CHLA-136	MV3Hdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			NUfLOlB6UUN3ME2xOE4zKG6P	MYOyOVI3OzV\|OR?=
NALM-6	M2T1PWdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			NXeyW5d7UUN3ME20PUBvVQ>?	NGTSSW8zPTJ4M{WzPS=>
COG-LL-317	MlLtS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			NY\odVZiUUN3ME25MlQhdk1?	NFG4XWczPTJ4M{WzPS=>
RS4;11	NWP6VFR[T3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			MX\JR\|UxRTV{Lk[gcm0>	NFrtfG0zPTJ4M{WzPS=>
MOLT-4	NYPP[pNXT3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			MYXJR\|UxRTF4Lk[gcm0>	MonXNlUzPjN3M{m=
CCRF-CEM	NV7hRVA4T3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			MXTJR\|UxRTZ7Nz6zJI5O	MV6yOVI3OzV\|OR?=
Kasumi-1	NIXINVlIem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			NWC4cIFHUUN3ME23PFYvOiCwTR?=	MXSyOVI3OzV\|OR?=
Karpas-299	MX3Hdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			NWfXT5pkUUN3ME23OU44KG6P	M3TteVI2OjZ\|NUO5
Ramos-RA1	NEL3NoxIem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			MUDJR\|UxRTZ6LkOgcm0>	NXXvWpBqOjV{NkO1N\|k>
DT40	NF;NXoRIem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			NH\MXpZKSzVyPUSgcm0>	NGHHcmwzPDN3NkixNy=>
DU145	NEDTRmlIem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			NYrGW2MzUUN3ME2xNUBvVQ>?	NHe1SGMzPDN3NkixNy=>
H209	NVXEeJdlT3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			MYnJR\|UxRTFwNzDuUS=>	MmrONlQxPzd\|NUC=
H1048	NX[wR\|dIT3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			NYnMVYhFUUN3ME2yMlIhdk1?	NF\ue\|czPDB5N{O1NC=>
H524	MkLiS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			MXPJR\|UxRTNwMTDuUS=>	MXSyOFA4PzN3MB?=
H1930	MU\Hdo94fGhiSX7obYJqfGmxbjDBd5NigQ>?			MnvDTWM2OD12LkGgcm0>	NYnoU3FOOjRyN{ezOVA>
H69	NVjRZlY4T3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			MVjJR\|UxRTVwMjDuUS=>	M2r0dFI1ODd5M{Ww
H2081	M1PTPGdzd3e2aDDJcohq[mm2aX;uJGF{e2G7			MWLJR\|UxRTZwMzDuUS=>	MWiyOFA4PzN3MB?=
H2107	MlztS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			MX\JR\|UxRTdwMzDuUS=>	NIDHSXgzPDB5N{O1NC=>
H1092	NWiwWFViT3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			M1jQN2lEPTB;OD65JI5O	M{\MSlI1ODd5M{Ww
DMS-79	NXSzTIhNT3Kxd4ToJGlvcGmkaYTpc44hSXO\|YYm=			M{e3bWlEPTB;OT6zJI5O	NUXNc2dqOjRyN{ezOVA>
H446	NFPENI1Iem:5dHigTY5pcWKrdHnvckBCe3OjeR?=			MWDJR\|UxRTF\|IH7N	NIPsUlIzPDB5N{O1NC=>
COR-L279	Ml\jS5Jwf3SqIFnubIljcXSrb36gRZN{[Xl?			MVjJR\|UxRTF3IH7N	MknoNlQxPzd\|NUC=

... Click to View More Cell Line Experimental Data

In vivo

In rat pharmacokinetic studies, BMN 673 displays >50% oralbioavailability and pharmacokinetic properties that enable singledaily dosing. In MX-1 xenograft tumor model studies, daily oral dosingof BMN 673 significantly enhances the antitumor effects ofcytotoxic therapies in a dose-dependent manner. ^[2]

Protocol

Animal Research: ^[2]	+ Expand Animal Models: MX-1 model (BRCA-1 deficient) Formulation: -- Dosages: 0.33 mg/kg/day, once daily Administration: Oral (Only for Reference)

References

Solubility (25°C)

In vitro	DMSO	38 mg/mL warmed (99.9 mM)
	Water	Insoluble
	Ethanol	Insoluble

* 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	380.35
Formula	C₁₉H₁₄F₂N₆O
CAS No.	1207456-01-6
Storage	3 years -20°C powder
Storage	2 years -80°C in solvent
Synonyms	LT-673

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Clinical Trial Information (data from https://clinicaltrials.gov, updated on 2018-11-16)

NCT Number	Recruitment	Conditions	Sponsor/Collaborators	Start Date	Phases
NCT03672773	Not yet recruiting	Recurrent Extensive Stage Small Cell Lung Carcinoma\|Refractory Extensive Stage Small Cell Lung Carcinoma	Jonsson Comprehensive Cancer Center\|Translational Research in Oncology\|National Cancer Institute (NCI)	November 1 2018	Phase 2
NCT03637491	Recruiting	Pancreatic Cancer\|Non-Small Cell Lung Cancer\|Cancer	Pfizer\|Array BioPharma	August 15 2018	Phase 2
NCT03499353	Recruiting	Early Breast Cancer	Pfizer	August 27 2018	Phase 2
NCT03642132	Recruiting	Ovarian Cancer	Pfizer	July 19 2018	Phase 3
NCT03565991	Recruiting	Locally Advanced or Metastatic Solid Tumors\|Genes BRCA 1	Pfizer	June 18 2018	Phase 2
NCT03426254	Enrolling by invitation	Advanced or Recurrent Solid Tumors\|Breast Neoplasm	Center Trials & Treatment\|BioGene Pharmaceutical	February 8 2018	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.

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Frequently Asked Questions

Question 1:
Which solvent do you recommend to dilute the inhibitor for in vivo study in mice?
Answer:
BMN673 (S7048) can be dissolved in vehicle (10% DMAc, 6% Solutol, and 84% PBS) according to the paper: http://clincancerres.aacrjournals.org/content/19/18/5003.full. Quote from Method and Material section "Xenograft experiments: BMN 673 (various doses as indicated), or vehicle (10% DMAc, 6% Solutol, and 84% PBS) was administered by oral gavage"

PARP Signaling Pathway Map

PARP Inhibitors with Unique Features

Selective PARP Inhibitors

AG-14361 : PARP1-selective, K_i<5 nM.
Selective PARP Inhibitors

UPF 1069 : PARP2-selective, IC50=0.3 μM.
Most Potent PARP Inhibitor

MK-4827 (Niraparib) : PARP1, IC50=3.8 nM; PARP2, IC50=2.1 nM.
PARP Inhibitor in Clinical Trial

Iniparib (BSI-201) : Phase III for solid tumors.
Newest PARP Inhibitor

PJ34 HCl ^New : PARP inhibitor with EC50 of 20 nM and is equally potent to PARP1/2.

Related PARP Products5

G007-LK ^New

G007-LK is a potent and selective tankyrase inhibitor with IC50 of 46 nM and 25 nM for TNKS1/2, respectively.
NU1025 ^New

NU1025 is a potent PARP inhibitor with IC50 of 400 nM.
SCR7 ^New

SCR7 is a specific DNA Ligase IV inhibitor, which blocks nonhomologous end-joining (NHEJ). It increases the efficiency of HDR-mediated genome editing up to 19-fold using CRISPR/Cas9 in mammalian cells and mouse embryos.
Olaparib (AZD2281, Ku-0059436)

Olaparib (AZD2281, KU0059436) is a selective inhibitor of PARP1/2 with IC50 of 5 nM/1 nM in cell-free assays, 300-times less effective against tankyrase-1.

Features:A potent PARP inhibitor (currently in late stage clinical trials).
Veliparib (ABT-888)

Veliparib (ABT-888) is a potent inhibitor of PARP1 and PARP2 with K_i of 5.2 nM and 2.9 nM in cell-free assays, respectively. It is inactive to SIRT2. Phase 3.

Features:Increases the efficacy of common cancer therapies such as radiation and alkylating agents.
Rucaparib (AG-014699,PF-01367338) phosphate

Rucaparib (AG-014699, PF-01367338) is an inhibitor of PARP with K_i of 1.4 nM for PARP1 in a cell-free assay, also showing binding affinity to eight other PARP domains. Phase 3.

Features:The first PARP inhibitor used in clinical trials combined with temozolomide.
Iniparib (BSI-201)

Iniparib (BSI-201) is a PARP1 inhibitor with demonstrated effectiveness in triple-negative breast cancer (TNBC). Phase 3.
PJ34 HCl

PJ34 HCl is the hydrochloride salt of PJ34, which is a PARP inhibitor with EC50 of 20 nM and is equally potent to PARP1/2.

Features:Water-soluble PARP1/2 inhibitor with >10,000-fold potentcy vs. 3-aminobenzamide (prototypical PARP inhibitor). Potential uses in cardiovascular diseases (stroke, cerebral ischemia, & myocardial ischemia).
AG-14361

AG14361 is a potent inhibitor of PARP1 with K_i of <5 nM in a cell-free assay. It is at least 1000-fold more potent than the benzamides.

Features:The 1st high-potency PARP-1 inhibitor with the specificity & in vivo activity to enhance chemotherapy and radiation therapy of human cancers.
A-966492

A-966492 is a novel and potent inhibitor of PARP1 and PARP2 with K_i of 1 nM and 1.5 nM, respectively.

Features:A promising, structurally diverse benzimidazole analogue that is being further characterized preclinically.

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Talazoparib (BMN 673)