2-(4-benzylpiperazin-1-yl)-N'-[(1E)-[2-hydroxy-3-(prop-2-en-1-yl)phenyl]methylidene]acetohydrazide

• ChemBase编号: 73221
• 分子式: C23H28N4O2
• 平均质量: 392.49402
• 单一同位素质量: 392.22122616
• SMILES: c1(CN2CCN(CC2)CC(=O)N/N=C/c2cccc(c2O)CC=C)ccccc1
• Canonical SMILES: C=CCc1cccc(c1O)/C=N/NC(=O)CN1CCN(CC1)Cc1ccccc1
• InChI: InChI=1S/C23H28N4O2/c1-2-7-20-10-6-11-21(23(20)29)16-24-25-22(28)18-27-14-12-26(13-15-27)17-19-8-4-3-5-9-19/h2-6,8-11,16,29H,1,7,12-15,17-18H2,(H,25,28)/b24-16+
• InChIKey: YQNRVGJCPCNMKT-LFVJCYFKSA-N

名称和登记号

名称

• IUPAC标准名: 2-(4-benzylpiperazin-1-yl)-N'-[(1E)-[2-hydroxy-3-(prop-2-en-1-yl)phenyl]methylidene]acetohydrazide; 2-(4-benzylpiperazin-1-yl)-N'-{[2-hydroxy-3-(prop-2-en-1-yl)phenyl]methylidene}acetohydrazide
• IUPAC传统名: 2-(4-benzylpiperazin-1-yl)-N'-[(1E)-[2-hydroxy-3-(prop-2-en-1-yl)phenyl]methylidene]acetohydrazide; 2-(4-benzylpiperazin-1-yl)-N'-{[2-hydroxy-3-(prop-2-en-1-yl)phenyl]methylidene}acetohydrazide
• 别名: Procaspase activating compound 1; PAC-1; (4-Benzylpiperazino)acetic acid (3-allyl-2-hyroxybenzylidene)hydrazide; 1-Piperazineacetic acid, 2-(phenylmethyl)-,[[2-hydroxy-3-(2-propenyl)phenyl]methylene]hyrrazide; PAC-1; 4-(Phenylmethyl)-1-piperazineacetic Acid (2E)-2-[[2-Hydroxy-3-(2-propen-1-yl)phenyl]methylene]hydrazide

登记号

• CAS号: 315183-21-2; 1044929-62-5
• MDL号: MFCD03302441
• PubChem SID: 162038141
• PubChem CID: 6851947

理论计算性质

• Acid pKa: 8.614495
• 质子受体: 5
• 质子供体: 2
• LogD (pH = 5.5): 1.2224518
• LogD (pH = 7.4): 2.8888998
• Log P: 3.10083
• 摩尔折射率: 117.9249 cm^3
• 极化性: 44.798073 Å^3
• 极化表面积: 68.17 Å^2
• 可自由旋转的化学键: 8
• 里宾斯基五规则: true

分子性质

理化性质

• 溶解度: deionized water: ≤2 mg/mL; DMSO: ≥10 mg/mL
• 外观: white solid

安全信息

• 保存条件: -20°C
• 欧盟危险性物质标志: 环境危害性(Nature polluting) (N); 有害性(Harmful) (Xn)
• 联合国危险货物编号: 3077
• 德国WGK号: 3
• 联合国危险货物等级: 9
• 联合国危险货物包装类别(PG): 3
• 危险公开号: 22-36/37/38-50/53
• 安全公开号: 26-36/37-60-61
• GHS危险品标识: GHS07; GHS09
• GHS警示词: Warning
• GHS危险声明: H302-H315-H319-H335-H400
• GHS警示性声明: P261-P273-P305 + P351 + P338
• 个人保护装置: dust mask type N95 (US), Eyeshields, Gloves
• RID/ADR: UN 3077 9/PG 3
• 保存温度: room temp

药理学性质

• 作用靶点: Caspase

产品相关信息

• 纯度: ≥98% (HPLC)
• 成盐信息: Free base
• Empirical Formula (Hill Notation): C23H28N4O2

详细说明

Selleck Chemicals - S2738

Research Area

• Description: Cancer

Biological Activity

• Description: PAC-1 is a potent procaspase-3 activator with EC50 of 0.22 μM.
• Targets: Procaspase-3
• IC50: 0.22 μM ^[1]
• In Vitro: PAC-1 activates procaspase-7 in a less efficient manner with EC50 of 4.5 μM. Elevated caspase 3 level in cancer cell lines allows PAC-1 to selectively induce apoptosis in a manner proportional to procaspase-3 concentration with IC50 of 0.35 μM for NCI-H226 cells to ~3.5 μM for UACC-62 cells. PAC-1 induces apoptosis in the primary cancerous cells with IC50 values of 3 nM to 1.41 μM, more potently than in the adjacent noncancerous cells with IC50 of 5.02 μM to 9.98 μM, which is also directly related to the distinct procaspase-3 concentration. ^[1] PAC-1 activates procaspase-3 by chelating zinc ions, thus relieving the zinc-mediated inhibition and allowing procaspase-3 to auto-activate itself to caspase-3. ^[2] PAC-1 is capable to induce cell death in Bax/Bak double-knockout cells and Bcl-2 and Bcl-xL-overexpressing cells with the same efficacy as its wild-type counterpart in a delayed manner. PAC-1 induces cytochrome c release in a caspase-3 independent manner, which subsequently triggers downstream caspase-3 activation and cell death. PAC-1 can not induce cell death and caspase-3 activation in Apaf-1 knockout cells, suggesting that apoptosome formation is essential for caspase-3 activation by PAC-1-mediated cell death. ^[3]
• In Vivo: Administration of PAC-1 at 5 mg with low and steady releasing significantly inhibits the growth of ACHN renal cancer xenograft in mice. Oral administration of PAC-1 (50 or 100 mg/kg) significantly retards tumor growth of NCI-H226 lung cancer xenograft in a dose-dependent manner, and markedly prevents the cancer cells from infiltrating the lung tissue. The in vivo anti-tumor effect of PAC-1 is ascribed to procaspase-3 activation and subsequently apoptosis induction consistent with the activity in vitro. ^[1]
• Features: PAC-1 is the first small molecule known to directly activate procaspase-3 to caspase-3

Protocol

• Protocol: Kinase Assay ^[1]
• In vitro procaspase-3 activation: Procaspase-3 is expressed and purified in Escherichia coli. Various concentrations of PAC-1 are added to 90 μL of a 50 ng/mL of procaspase-3 in caspase assay buffer in a 96-well plate, The plate is incubated for 12 hours at 37 °C. A 10 μL volume of a 2 mM solution of caspase-3 peptidic substrate acetyl Asp-Glu-Val-Asp-p-nitroanilide (Ac-DEVD-pNa) in caspase assay buffer is then added to each well. The plate is read every 2 minutes at 405 nm for 2 hours in a Spectra Max Plus 384 well plate reader. The slope of the linear portion for each well is determined, and the relative increase in activation from untreated control wells is calculated.
• Protocol: Cell Assay ^[1]
• Cell Lines: U-937, HL-60, CRL-1872, ACHN, NCI-H226, Hs888Lu, Hs578Bst, MCF-10A, SK-MEL-5, BT-20, MDA-MB-231, UACC-62, SK-N-SH, B16-F10 , Hs 578t, and PC-12
• Concentrations: Dissolved in DMSO, final concentrations ~100 μM
• Incubation Time: 72 hours
• Methods: Cells are exposed to various concentrations of PAC-1 for 72 hours. Cell death is quantified by the addition of MTS/PMS CellTiter 96 Cell Proliferation Assay reagent. The plates are incubated at 37 °C for approximately 1 hour (until the colored product formed), and the absorbance is measured at 490 nm.
• Protocol: Animal Study ^[1]
• Animal Models: Ovariectomized female athymic BALB/c (nude, nu/nu) mice injected subcutaneously with ACHN cells, male athymic BALB/c nude mice injected subcutaneously with NCI-H226 cells, and male athymic BALB/c–/– mice injected intravenously with NCI-H226 cells
• Formulation: Mixed with cholesterol and pelleted into a 3-mm-diameter 20-mg (total weight) pellet, or dissolved in a mixture of 24:1 vegetable oil/DMSO
• Doses: ~100 mg/kg
• Administration: Pellet implantation subcutaneously or oral gavage

References

• References: [1] Putt KS, et al. Nat Chem Biol, 2006, 2(10), 543-550.
• References: [2] Peterson QP, et al. J Mol Biol, 2009, 388(1), 144-158.
• References: [3] Seervi M, et al. Cell Death Dis, 2011, 2, e207.

Sigma Aldrich - P0115

Biochem/physiol Actions
PAC-1 is a caspase 3 activator. Caspase activation is a key strategy in cancer therapy. Caspase 3 is a key executioner caspase and direct effector of apoptosis. Hallmark of many cancers is the circumvention of signal in the activation of executioner caspases and loss of apoptotic response. EC50 for caspase 3 activation = 0.33 μM and caspase 7= 4.5 μM. The IC50 for apoptosis induction = 0.92 μM. Elevated caspase 3 level in cancerous cell lines and tissues allows PAC-1 to selectively induce apoptosis in tissues.

Toronto Research Chemicals - P132000

PAC-1 is a caspase 3 activator. Caspase activation is a key strategy in cancer therapy. Caspase 3 is a key executioner caspase and direct effector of apoptosis. Hallmark of many cancers is the circumvention of signal in the activation of executioner caspa

参考文献

• Putt KS, et al. Nat Chem Biol, 2006, 2(10), 543-550.
• Peterson QP, et al. J Mol Biol, 2009, 388(1), 144-158.
• Seervi M, et al. Cell Death Dis, 2011, 2, e207.
• Slee, E., et al.: J. Biol. Chem., 276, 7320 (2001)
• Pop, C., et al.: Biochemistry, 42, 12311 (2001)
• Li, L., et al.: Science, 305, 1471 (2001)
• Green, D., et al.: J. Clin. Invest., 115, 2610 (2001)
• Satoh, T., et al.: Clin. Cancer Res., 15, 3872 (2001)