APR-246 (PRIMA-1MET)

Name: APR-246 (PRIMA-1MET)
Brand: Selleck Chemicals
SKU: S7724
Rating: 5 (0 reviews)

For research use only. Not for use in humans.

Catalog No.S7724

Molecular Weight(MW): 199.25

APR-246, also known as PRIMA-1MET, is a small organic molecule that has been shown to restore tumour-suppressor function primarily to mutant p53 and also to induce cell death in various cancer types.

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5mg	USD 97	In stock
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Biological Activity

Description

Targets

Mutant p53 ^[2]
()

In vitro

APR-246 (PRIMA-1MET) is the first clinical-stage compound that reactivates mutant p53 and induces apoptosis. APR-246 is a prodrug that is converted to the active compound methylene quinuclidinone (MQ), a Michael acceptor that binds to cysteine residues in mutant p53 and restores its wild-type conformation. APR-246 completely restores the cisplatin and doxorubicin sensitivity to p53-mutant drug-resistant ovarian cancer cells. It not only reactivates p53 but also decreases intracellular glutathione levels in a dose-dependent manner. APR-246 can trigger apoptosis in a p53-independent manner by inducing ROS and endoplasmic reticulum (ER) stress and by inhibiting thioredoxin reductase 1 (TrxR1). It was also reported that APR-246 induces cell death in myeloma cells independently of p53 status by impairing the GSH/ROS balance^[1]. PRIMA-1Met/APR-246 efficiently inhibited the growth of the SCLC cell lines expressing mutant p53 in vitro and induced apoptosis, associated with increased fraction of cells with fragmented DNA, caspase-3 activation, PARP cleavage, Bax and Noxa upregulation and Bcl-2 downregulation in the cells^[2].

Cell Data

Cell Lines	Assay Type	Concentration	Incubation Time	Activity Description	PMID
NALM-6	NGjIOYpE\WyuII\pZYJqdGm2eTDhd5NigQ>?			NUn1NFV3cGmpaDDz[Y5{cXSrdnn0fUBidmRiY3XscEBl\WG2aDDpcoR2[3Srb36gbY4h[WyuIGTQOVNufXRibHX1b4VucWG\|LDDieZQhdG:5IFHQVk0zPDZic3Xud4l1cX[rdImgbY4hXFB3M4f0JGFNVA>?	MXuzNVA4OzB5Nh?=
UoCB-6	NXGwVpBJS2WubDD2bYFjcWyrdImgZZN{[Xl?			NFzoOnRpcWeqIIPlcpNqfGm4aYT5JIFv\CClZXzsJIRm[XSqIHnu[JVkfGmxbjDpckBidGxiVGC1N412fCCuZYXr[Y1q[XNuIHL1eEBtd3diQWDSMVI1PiC\|ZX7zbZRqfmm2eTDpckBVWDV\|d4SgRWxN	NX7KTGpmOzFyN{OwO\|Y>
EU-3	NHLWb5JE\WyuII\pZYJqdGm2eTDhd5NigQ>?			M1viW4hq\2hic3Xud4l1cX[rdImgZY5lKGOnbHyg[IVifGhiaX7keYN1cW:wIHnuJIFtdCCWUEWzcZV1KGyndXvlcYlieyxiYoX0JIxwfyCDUGKtNlQ3KHOnboPpeIl3cXS7IHnuJHRRPTO5dDDBUGw>	MkjPN\|ExPzNyN{[=
MUTZ-5	Mlj2R4VtdCC4aXHibYxqfHliYYPzZZk>			MX\obYdpKHOnboPpeIl3cXS7IHHu[EBk\WyuIHTlZZRpKGmwZIXjeIlwdiCrbjDhcIwhXFB3M331eEBt\XWtZX3pZZMtKGK3dDDsc5chSVCULUK0OkB{\W6\|aYTpeol1gSCrbjDUVFU{f3RiQVzM	NG\xXHo{OTB5M{C3Oi=>
KOPN-8	NGnTU5dE\WyuII\pZYJqdGm2eTDhd5NigQ>?			MmPsbIlocCC\|ZX7zbZRqfmm2eTDhcoQh[2WubDDk[YF1cCCrbnT1Z5Rqd25iaX6gZYxtKFSSNUPteZQhdGW3a3XtbYF{NCCkdYSgcI94KEGSUj2yOFYhe2Wwc3n0bZZqfHliaX6gWHA2O3e2IFHMUC=>	NWDDcII3OzFyN{OwO\|Y>
RS4;11	M4rIVWNmdGxidnnhZoltcXS7IHHzd4F6			NV7Ne5p5cGmpaDDz[Y5{cXSrdnn0fUBidmRiY3XscEBl\WG2aDDpcoR2[3Srb36gbY4h[WyuIGTQOVNufXRibHX1b4VucWG\|LDDieZQhdG:5IFHQVk0zPDZic3Xud4l1cX[rdImgbY4hXFB3M4f0JGFNVA>?	NYLSe5ZQOzFyN{OwO\|Y>
SKBR3	NVPZ[oZRS2WubDDjfYNt\SCjc4PhfS=>	NV;ObFl{PSEEtV2=	M3\4[FIhf2Wna4O=	MkD4cIFx[XSrbnniJIlvKGOxbXLpcoF1cW:wIIfpeIghSVCULUK0OkBk[XW\|ZXSgZUBtd3encjDs[ZZmdCCxZjDHNUBienKnc4SgZY5lKGGwIHnuZ5Jm[XOnIHnuJJRp\SC\|dXKtS\|Eh\nKjY4Tpc44>	M{PtflMxPzR\|OUm2
BT549	NHXDU49E\WyuII\pZYJqdGm2eTDhd5NigQ>?			MmXYTWM2OD1\|LkGg{txO	MnTLN\|AyQTZ{M{[=
MDA-MB-468	NI\OTnVE\WyuII\pZYJqdGm2eTDhd5NigQ>?			NVvxUGFxUUN3ME21JO69VQ>?	MnjZN\|AyQTZ{M{[=
MDA-MB-231	NUTsZZIxS2WubDD2bYFjcWyrdImgZZN{[Xl?			NV\KdVhuUUN3ME20MlEh\|ryP	NWXRb\|hIOzBzOU[yN\|Y>
HCC1143	MlvyR4VtdCC4aXHibYxqfHliYYPzZZk>			NUTRb4NQUUN3ME22Mlgh\|ryP	MX6zNFE6PjJ\|Nh?=
MDA-MB-453	NX\qfGpoS2WubDD2bYFjcWyrdImgZZN{[Xl?			NIfUNIRKSzVyPUCuPUDPxE1?	M4\CV\|MxOTl4MkO2
SKBR3	NIG0O25E\WyuII\pZYJqdGm2eTDhd5NigQ>?			Mnn5TWM2OD13LkGg{txO	MknNN\|AyQTZ{M{[=
UACC812	MXfD[YxtKH[rYXLpcIl1gSCjc4PhfS=>			MVzJR\|UxRTFzLkOg{txO	NGi5[48{ODF7NkKzOi=>
MCF7	NHS3SJdE\WyuII\pZYJqdGm2eTDhd5NigQ>?			MmDpTWM2OD1\|MT6xJO69VQ>?	M2PUe\|MxOTl4MkO2
MCF10A	NEjvTpNE\WyuII\pZYJqdGm2eTDhd5NigQ>?			MlnnTWM2OD13LkKg{txO	NXeyTI0yOzBzOU[yN\|Y>
UMSCC10A	NGDldZZE\WyuII\pZYJqdGm2eTDhd5NigQ>?	MUewMVUxKM7:TR?=	MnP3O\|IhcA>?	MWrzeZBxemW\|c3XkJINmdGxic4Xyeol3[WxiYX7kJIJwemViYTDtc4Rme3RiZX\m[YN1KG:wIITo[UBscWyuaX7nJI9nKEiQU1PDJINmdGy\|	MXmyPVM1QDR4Mh?=
FaDu	NFjL[5ZE\WyuII\pZYJqdGm2eTDhd5NigQ>?	NX[4c5hiOC13MDFOwG0>	MVG3NkBp	MWTzeZBxemW\|c3XkJINmdGxic4Xyeol3[WxiYX7kJIJwemViYTDtc4Rme3RiZX\m[YN1KG:wIITo[UBscWyuaX7nJI9nKEiQU1PDJINmdGy\|	M2nvO\|I6OzR6NE[y

... Click to View More Cell Line Experimental Data

Assay

Methods	Test Index	PMID
Western blot	FL-PARP / Cleaved PARP ; PubMed: 26452133 Oncotarget PARP cleavage was detected by western blotting analysis after treated with PRIMA-1(met) at different concentrations for 24 hours. p-p53; PubMed: 26452133 Oncotarget Phosphorylation of p53 level was determined after PRIMA-1(met) treatment.	26452133
Growth inhibition assay	Cell viability; PubMed: 26452133 Oncotarget A panel of CRC cell lines was treated with either DMSO control or PRIMA-1(met) at indicated dosages for 48 hours, followed by CTG assays. The percentage of cell growth inhibition was normalized with respective DMSO control.	26452133

In vivo

APR-246 showed a good safety profile in a Phase I/II clinical dose-finding study on hematological malignancies and prostate cancer and both clinical and p53-dependent biological responses were observed. In animal studies, APR-246 is well tolerated. Single treatment with APR-246 inhibits tumor growth by 21% in mice bearing the aggressively growing A2780-CP20 tumor xenografts^[1].

Protocol

Cell Research:

^[1]

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Cell lines: OVCAR-3 cells
Concentrations: 40 μM
Incubation Time: 20 h
Method:
OVCAR-3 cells were plated at a density of 75 000 cells per well in 3 ml of medium in 12-well plates. Next day, 2.5 ml medium was removed and cells were treated with cisplatin or APR-246 or in combination for 20 h. Next day, cells were harvested by trypsinization, washed twice and cells were stained with Annexin V and propidium iodine (PI). After staining, the samples were analyzed by LSRII flow cytometer.

(Only for Reference)

Animal Research:

^[1]

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Animal Models: CD-1 Nu/Nu mice
Formulation: PBS
Dosages: 400 mg/kg/day
Administration: i.v.
(Only for Reference)

References

Solubility (25°C)

In vitro	DMSO	40 mg/mL (200.75 mM)
	Water	40 mg/mL (200.75 mM)
	Ethanol	40 mg/mL (200.75 mM)

* 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 APR-246 (PRIMA-1MET) SDF

Molecular Weight	199.25
Formula	C₁₀H₁₇NO₃
CAS No.	5291-32-7
Storage	3 years -20°C powder
Storage	2 years -80°C in solvent
Synonyms	N/A
Smiles	COCC1(CO)N2CCC(CC2)C1=O

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Clinical Trial Information (data from https://clinicaltrials.gov, updated on 2019-10-14)

NCT Number	Recruitment	interventions	Conditions	Sponsor/Collaborators	Start Date	Phases
NCT03745716	Recruiting	Drug: APR-246 + azacitidine\|Drug: Azacitidine	MDS	Aprea Therapeutics AB	January 11 2019	Phase 3
NCT03391050	Terminated	Drug: APR-246\|Drug: Dabrafenib	Melanoma	Aprea Therapeutics AB\|Jules Bordet Institute	January 18 2018	Phase 1\|Phase 2
NCT02999893	Suspended	Drug: APR-246	Oesophageal Carcinoma	Peter MacCallum Cancer Centre Australia	April 11 2017	Phase 1\|Phase 2
NCT00900614	Completed	Drug: APR-246	Hematologic Neoplasms\|Prostatic Neoplasms	Aprea Therapeutics AB	May 2009	Phase 1

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