Vorinostat

Cat. No. M1780

All AbMole products are for research use only, cannot be used for human consumption.

Synonym:

SAHA; Zolinza; MK-0683; Suberoylanilide hydroxamic acid

Size	Price	Availability
Free Sample (0.5-1 mg)	USD 0	In stock
10mM*1mL in DMSO	USD 40 USD40	In stock
50mg	USD 24 USD24	In stock
100mg	USD 46 USD46	In stock
250mg	USD 60 USD60	In stock
500mg	USD 90 USD90	In stock
1g	USD 120 USD120	In stock

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Quality Control & Documentation

Purity: >99%
COA
MSDS
H-NMR

Product Information

Biological Activity

Vorinostat (SAHA, Zolinza, MK-0683) is a selective and potent histone deacetylase (HDAC) inhibitor with the IC50 value of 10 nM for HDAC-1.The pan-HDAC inhibitor vorinostat (SAHA,Zolinza,MK-0683) potentiates the activity of the proteasome inhibitor carfilzomib in human DLBCL cells in vitro and in vivo.Vorinostat (SAHA, Zolinza, MK-0683),which also inhibits HDAC6,could enhance the activity of the novel proteasome inhibitor CFZ in DLBCL cells, including those resistant to bortezomib alone.

Product Citations

FEBS J. 2024 Sep 09.

MOF-mediated acetylation of CDK9 promotes global transcription by modulating P-TEFb complex formation
Vorinostat purchased from AbMole
BMC Cancer. 2016 Nov 7;16(1):857.

Vorinostat enhances the cisplatin-mediated anticancer effects in small cell lung cancer cells.
Vorinostat purchased from AbMole

Customer Product Validations & Biological Datas

	Source	BMC Cancer (2016) . Figure 6. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	Antitumor activity in H209 xenografts
	Cell Lines	H209 cells line
	Concentrations	40mg/kg 4 times a week
	Incubation Time	5 weeks
	Results	As presented in Fig. 6, compared with vehicle and single-agent treatments, the combination treatment significantly inhibited tumor growth at day 5.

	Source	BMC Cancer (2016) . Figure 5. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	western blot
	Cell Lines	H209 and H146 cells line
	Concentrations	0.05, 0.1 and 0.2 μ M
	Incubation Time	24 h
	Results	As presented in Fig. 5a and b, vorinostat alone induced a dose-dependent reduction of TS protein levels in the H209 and H146 cells.

	Source	BMC Cancer (2016) . Figure 4. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	flow cytometry
	Cell Lines	H209 and H146 cells line
	Concentrations	0.1 μ M
	Incubation Time	24 h
	Results	The H146 cells treated with vorinostat demonstrated no distinct cell cycle arrest, whereas those treated with cisplatin exhibited cell cycle arrest in the S phase (Fig. 4b and d). Similarly, the combination treatment induced cell cycle arrest in the S phase in the H146 cells.

	Source	BMC Cancer (2016) . Figure 3. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	caspase-3 activity assay and Western blot
	Cell Lines	H209 and H146 cells line
	Concentrations	0, 0.05, 0.1 and 0.2 μ M
	Incubation Time	24 or 36 h
	Results	Therefore, our data indicated that the combination treatment dose dependently increased apoptosis in the proteolytic cleavage of PARP and activated caspase-3 in SCLC cells.

	Source	BMC Cancer (2016) . Figure 2. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	Cell viability assay and Western blot
	Cell Lines	H209 and H146 cells line
	Concentrations	0, 0.1 or 0.2 μ M
	Incubation Time	24 h
	Results	The combination treatments were more effective in inhibiting H209 cell viability in a dosedependent manner (Fig. 2a). Specifically, the cell viabilities observed when the cells were treated with combinations of cisplatin at 5 μM and vorinostat at 0.1 or 0.2 μM were 80.21 and 68.81 %, respectively (Fig. 2b).

	Source	BMC Cancer (2016) . Figure 1. Vorinostat (purity >99 %) was purchased from AbMole BioScience (Houston, TX, USA)
	Method	Cell viability assay and Western blot
	Cell Lines	H209 and H146 cells line
	Concentrations	0, 0.4 or 0.8 μ M
	Incubation Time	24 h
	Results	Overall, these results indicated that the triple combination treatment enhanced cytotoxic effects and promoted apoptosis in SCLC cells.

Protocol (for reference only)

Cell Experiment
Cell lines	HH, HuT78, MJ, MylA and SeAx cells
Preparation method	cell viability assay. The inhibitory effect of vorinostat on the viability of CTCL cell lines was examined through a CellTiter-Glo assay using various concentrations of vorinostat (0.01, 0.05, 0.15, 0.5, 1.25, 4, 10, 35, and 100 μM) for 72 h. All CTCL cell lines were sensitive to the investigated HDAC inhibitor. The inhibitory effect of vorinostat was reflected as a dose-dependent reduction in cell proliferation/viability. The IC50 of proliferation was determined at 0.146 μM in HH cells, at 2.062 μM in HuT78 cells, at 2.697 μM in MJ cells, at 1.375 μM in MylA and at 1.510 μM in SeAx cells.
Concentrations	0.01, 0.05, 0.15, 0.5, 1.25, 4, 10, 35, and 100 μM
Incubation time	72 h

Animal Experiment
Animal models	R6/2 mice motor impair
Formulation	solubilized in 5 molar equivalents of HOP-β-CD (ICN) in water
Dosages	0.67g/L
Administration	orally

Chemical Information

Molecular Weight	264.3
Formula	C14H20N2O3
CAS Number	149647-78-9
Solubility (25°C)	DMSO 55 mg/mL
Storage	Powder -20°C 3 years ; 4°C 2 years In solvent -80°C 6 months ; -20°C 1 month

References

[1] Saelen MG, et al. Radiat Oncol. Radiosensitization by the histone deacetylase inhibitor vorinostat under hypoxia and with capecitabine in experimental colorectal carcinoma.

[2] Kakizaki A, et al. Australas J Dermatol. Successful treatment of syringotropic CD8+ mycosis fungoides accompanied by hypohidrosis with vorinostat and retinoids.

[3] Lautz TB, et al. PLoS One. The effect of vorinostat on the development of resistance to doxorubicin in neuroblastoma.

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Vorinostat

SAHA; Zolinza; MK-0683; Suberoylanilide hydroxamic acid

Quality Control & Documentation

Biological Activity

Product Citations

Customer Product Validations & Biological Datas

Protocol (for reference only)

Chemical Information

References

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