24928-15-2

Basic information

• Product Name: PHORBOL 12,13-DIACETATE
• Synonyms: PHORBOL 12,13-DIACETATE;PHORBOL 12,13-DIACETATE, 4BETA;PDA;5h-cyclopropa(3,4)benz(1,2-e)azulen-5-one,1,1a-alpha,16-beta,4,4a,7a-alpha,7b,;8,9,9a-decahydro-4a-beta,7b-alpha,9-beta,9a-alpha-tetrahydroxy-3-(hydroxymethy;l)-1,1,6,8-alpha-tetramethyl-,9,9a-diacetate,(+);phorbol10,11-diacetate;phorbol11,12-diacetate
• CAS NO: 24928-15-2
• Molecular Formula: C₂₄H₃₂O₈
• Molecular Weight: 448.51
• Product Categories: Activator
• Mol File: 24928-15-2.mol
• Article Data: 3

Chemical Properties

• Boiling Point: 477.23°C (rough estimate)
• Flash Point: 195.4°C
• Appearance: white/
• Density: 1.1793 (rough estimate)
• Vapor Pressure: 3.69E-16mmHg at 25°C
• Refractive Index: 1.4480 (estimate)
• Storage Temp.: −20°C
• Solubility: H2O: soluble
• BRN: 2317312
• CAS DataBase Reference: PHORBOL 12,13-DIACETATE(CAS DataBase Reference)
• NIST Chemistry Reference: PHORBOL 12,13-DIACETATE(24928-15-2)
• EPA Substance Registry System: PHORBOL 12,13-DIACETATE(24928-15-2)

Safety Data

• Hazard Codes: T+
• Statements: 26/27/28-36/37/38
• Safety Statements: 26-27-36/37/39-45
• RIDADR: UN 2811 6.1/PG 3
• WGK Germany: 3
• RTECS: GZ0651000
• F: 8-10
• HazardClass: 6.1(a)
• PackingGroup: II
• Hazardous Substances Data: 24928-15-2(Hazardous Substances Data)

Usage

Uses

Phorbol 12,13-diacetate may be used to stimulate protein kinase C (PKC) for phosphorylation of retinal proteins.

General Description

Phorbol ester with enhanced hydrophilicity.

Biochem/physiol Actions

Phorbol 12,13-diacetate (PDA) serves as a protein kinase C (PKC). It induces arrest in translocation in rod photoreceptors. PDA facilitates PKC in regulating airway contractility by inducing transient relaxation after a sustained contraction of the human isolated bronchus. PDA improves the synaptic transmission of nociceptive parabrachioamygdaloid (PBA) input onto neurons of the capsular central amygdaloid (CeAC) nucleus via activating PKC and extracellular-regulated kinase (ERK).

InChI:InChI=1/C24H32O8/c1-11-7-17-22(29,19(11)28)9-15(10-25)8-16-18-21(5,6)24(18,32-14(4)27)20(31-13(3)26)12(2)23(16,17)30/h7-8,12,16-18,20,25,29-30H,9-10H2,1-6H3/t12-,16+,17-,18-,20-,22-,23-,24-/m1/s1

Upstream product

• 19891-05-5 phorbol 12,13,20-triacetate 
• 17673-25-5 phorbol 
• 77495-83-1 phorbol 12,13-diacetate-20-trityl 
• 82400-03-1 phorbol-20-trityl ether 
• 64-19-7 acetic acid 

Downstream Products

• 25405-84-9 20-O-<4-(2-Brom-4-nitrophenyl-azo)-benzoyl>-phorbol-12,13-diacetat 
• 25405-82-7 20-O-(4-Brom-benzoyl)-phorbol-12.13-diacetat 
• 25449-41-6 20-O-(4-Iod-benzoyl)-phorbol-12.13-diacetat 
• 25405-83-8 20-O-<4-(4-Nitrophenyl-azo)-benzoyl>-phorbol-12,13-diacetat 

Relevant articles and documents

New phorbol ester derivatives as potent anti-HIV agents

Tigliane esters show many biological activities, including anti-HIV-1 activity. Our aim in this study was to establish structure-anti-HIV activity relationships for four series of tigliane-type diterpenoids. We synthesized and evaluated 29 new phorbol ester derivatives for anti-HIV activity and for cytotoxicity against human tumor cell lines. Among them, three derivatives, two phorbol-13-monoesters (5d and 5e) and a phorbol-12,13-diester (6a), showed significant anti-HIV activity. We found that better anti-HIV activity was often associated with a shorter acyl ester at C-13. Particularly, compounds with a phenyl ring in the ester side chain exhibited excellent anti-HIV activity and had good safety indexes. Due to its significant anti-HIV potency with a high selectivity index, phorbol-12,13-dicinnamoate (6a) was chosen as the potential candidate for further preclinical trials.

Inhibition of cytopathic effect of human immunodeficiency virus type-1 by various phorbol derivatives

Forty-eight derivatives of phorbol (9) and isophorbol (14) were evaluated for their inhibition of human immunodeficiency virus (HIV)-1 induced cytopathic effects (CPE) on MT-4 cells, as well as their activation of protein kinase C (PKC), as indices of anti-HIV-1 and tumor promoting activities, respectively. Of these compounds, the most potent inhibition of CPE was observed in 12-O-tetradecanoylphorbol 13-acetate (8) and 12-O-acetylphorbol 13-decanoate (6). The former also showed the strongest PKC activation activity, while the latter showed no activity at 10 ng/ml. Both activities were generally observed in those phorbol derivatives with an A/B trans configuration, but not in the isophorbol derivatives with an A/B cis configuration. Acetylation of 20-OH in the phorbol derivatives significantly reduced the inhibition of CPE, as shown in 12-O-, 20-O-diacetylphorbol 13-decanoate (6a) (IC100=15.6 μg/ml) vs. compound 6 (IC100=0.0076 μg/ml), and 12-O-tetradecanoylphorbol 13,20-diacetate (8a) (IC100=15.6 μg/ml) vs. 12-O- tetradecanoylphorbol 13-acetate (8) (IC100=0.00048 μg/ml), except in the case of 12-O-decanoylphorbol 13-(2-methylbutyrate) (4) and phorbol 12,13-diacetate (9c). The reduction of a carbonyl group at C-3 abruptly reduced the inhibition of CPE, as observed in 3β-hydroxyphorbol 12,13,20-triacetate (9f) (IC100=500 μg/ml) vs. phorbol 12,13,20-triacetate (9d) (IC100=62.5 μg/ml). Although 8 was equipotent in the inhibition of CPE, and activation of PKC, both activities were abruptly decreased by the acetylation of 20-OH and methylation of 4-OH [as in 8a and 4-O-methyl-12-O- tetradecanoylphorbol 13,20-diacetate (8b), respectively]. On the other hand, its positional isomer (12-O-acetylphorbol 13-tetradecanoate (8c) showed neither activities. The removal of a long acyl group in 8 led to a substantial loss of both activities, as shown in phorbol 13-acetate (9b). Of the 12-O-acetyl-13-O-acylphorbol derivatives, the highest inhibition of CPE was observed in 6, which has a dodecanoyl residue at C-13. Both an increase and decrease in the number of fatty acid carbon chains resulted in significant reduction of the inhibition of CPE.