2-amino-1-phenylethanol

Phenylethanolamine (sometimes abbreviated PEOH), or β-hydroxyphenethylamine, is a trace amine with a structure similar to those of other trace phenethylamines as well as the catecholamine neurotransmitters dopamine, norepinephrine, and epinephrine. As an organic compound, phenylethanolamine is a β-hydroxylated phenethylamine that is also structurally related to a number of synthetic drugs in the substituted phenethylamine class. In common with these compounds, phenylethanolamine has strong cardiovascular activity and, under the name ''Apophedrin'', has been used as a drug to produce topical vasoconstriction.''The Merck Index, 10th Ed.'' (1983), p. 1051, Merck & Co., Rahway.

In appearance, phenylethanolamine is a white solid.

Phenylethanolamine is perhaps best known in the field of bioscience as part of the enzyme name "phenylethanolamine N-methyl transferase", referring to an enzyme which is responsible for the conversion of norepinephrine into epinephrine, as well as other related transformations.

Occurrence

Phenylethanolamine has been found to occur naturally in several animal species, including humans.

Chemistry

Synthesis

An early synthesis of phenylethanolamine was by the reduction of 2-nitro-1-phenyl-ethanol.G. A. Alles (1927). "The comparative physiological action of phenylethanolamine." ''J. Pharmacol. Exp. Ther.'' 32 121–133. Other early syntheses are summarized in a paper by Hartung and Munch.

A more recent synthesis, providing a better yield, is by the reduction of benzoyl cyanide using LiAlH₄.

Properties

Chemically, phenyethanolamine is an aromatic compound, an amine, and an alcohol. The amino-group makes this compound a weak base, capable of reacting with acids to form salts.

Two common salts of phenylethanolamine are the hydrochloride, C₈H₁₁NO.HCl, m.p. 212 °C, and the sulfate, (C₈H₁₁NO)₂.H₂SO₄, m.p. 239–240 °C.M. L. Tainter (1929). "Pharmacological actions of phenylethanolamine." ''J. Pharmacol. Exp. Ther.'' 36 29–54.

The pK_a of phenylethanolamine hydrochloride, at 25 °C and at a concentration of 10mM, has been recorded as 8.90.

The presence of the hydroxy-group on the benzylic carbon of the phenylethanolamine molecule creates a chiral center, so the compound exists in the form of two enantiomers, d- and l-phenylethanolamine, or as the racemic mixture, d,l-phenylethanolamine. The dextrorotatory isomer corresponds to the S-configuration, and the levorotatory isomer to the R-configurationM. F. Rafferty , D. S. Wilson , J. A. Monn , P. Krass , R. T. Borchardt , and G. L. Grunewald (1982). "Importance of the aromatic ring in adrenergic amines. 7. Comparison of the stereoselectivity of norepinephrine N-methyltransferase for aromatics. Nonaromatic substrates and inhibitors." ''J. Med. Chem.'' 25 1198–1204. The data given at right is for the racemate.

The synthesis of (''S'')-(+)-phenylethanolamine, from (+)- mandelic acid, via (+)- mandelamide, has been described. The physical constants reported in this paper are as follows: m.p. 55–57 °C; �= + 47.9° (c 2.4, in ethanol).

Pharmacology

Early, classical pharmacological studies of phenylethanolamine were carried out by Tainter, who observed its effects after administering it to rabbits, cats and dogs. The drug produced a rapid rise in blood pressure when administered intravenously, but had little or no effect when given by any other route: doses as high as 200 mg given subcutaneously to rabbits did not alter blood pressure, nor were there any effects when the drug was intubated into the stomach.

In man, a total oral dose of 1 g also produced no effects.

Doses of 1–5 mg/kg, intravenously, caused no definite changes in respiration in cats or rabbits, and additional experiments showed that phenylethanolamine had no broncho-dilatory properties in animals. There was a similar lack of effect when the drug was given subcutaneously to man.

''In vivo'' and ''in vitro'' experiments involving cat and rabbit intestinal smooth muscle showed that the drug produced relaxation and inhibition.

A detailed examination of the mydriatic effect of phenylethanolamine led Tainter to conclude that this drug acted by direct stimulation of the radial dilator muscle in the eye.

Shannon and co-workers confirmed and extended some of Tainter's studies. After administering phenylethanolamine to dogs intravenously, these investigators observed that 10–30 mg/kg of the drug increased pupil diameter, and decreased body temperature; a dose of 10 or 17.5 mg/kg decreased heart rate, but a 30 mg/kg dose caused it to increase. Other effects that were noted included profuse salivation and piloerection. Phenylethanolamine also produced behavioral effects such as stereotyped head movement, rapid eye movement, and repetitive tongue extrusion. These and other observations were suggested to be consistent with an action on α- and β-adrenergic receptors.H. E. Shannon, E. J. Cone and D. Yousefnejad (1981). "Physiologic effects and plasma kinetics of phenylethanolamine and its N-methyl homolog in the dog." ''J. Pharmacol. Exp. Ther.'' 217 379–385.

Research by Carpéné and co-workers showed that phenylethanolamine did not significantly stimulate lipolysis in cultured adipocytes ("fat cells") from guinea pig or human. Moderate stimulation ( intrinsic activities about half that of the reference standard, isoprenaline) was observed in adipocytes from rat or hamster. This lipolysis was inhibited completely by bupranolol (considered to be a non-selective β-blocker), CGP 20712A (considered to be a selective β₁-antagonist), and ICI 118,551 (considered to be a selective β₂-antagonist), but not by SR 59230A (considered to be a selective β₃-antagonist).

Using a β₂ adrenergic receptor preparation derived from transfected HEK 293 cells, Liappakis and co-workers found that in wild-type receptors, racemic phenylethanolamine had ~ 1/400 x the affinity of epinephrine, and ~ 1/7 x the affinity of norepinephrine in competition experiments with ³ CGP-12177.

The two enantiomers of phenylethanolamine were studied for their interaction with the human trace amine associated receptor ( TAAR1) by a research group at Eli Lilly. From experiments with human TAAR1 expressed in rGα_sAV12-664 cells, Wainscott and co-workers observed that R-(−)-phenylethanolamine (referred to as "R-(−)-β-hydroxy-β-phenylethylamine") had an ED₅₀ of ~1800 nM, with an E_max of ~ 110%, whereas S-(+)-phenylethanolamine (referred to as "S-(+)-β-hydroxy-β-phenylethylamine") had an ED₅₀ of ~1720 nM, with an E_max of ~ 105%. In comparison, β-phenethylamine itself had an ED₅₀ of ~106 nM, with an E_max of ~ 100%.
Table 3
In other words, phenylethanolamine is a TAAR1 agonist and trace amine.

Pharmacokinetics

The pharmacokinetics of phenylethanolamine, after intravenous administration to dogs, were studied by Shannon and co-workers, who found that the drug followed the "two-compartment model", with T_1/2(α) ≃ 6.8 mins and T_1/2(β) ≃ 34.2 mins; the "plasma half-life" of phenylethanolamine was therefore about 30 minutes.

Biochemistry

Phenylethanolamine was found to be an excellent substrate for the enzyme phenylethanolamine N-methyl transferase (PNMT), first isolated from monkey adrenal glands by Julius Axelrod, which transformed it into N-methylphenylethanolamine.J.Axelrod (1962). "Purification and properties of phenylethanolamine-N-methyl transferase." ''J. Biol. Chem.'' 237 1657–1660.

Subsequent studies by Rafferty and co-workers showed that substrate specificity of PNMT from bovine adrenal glands for the different enantiomers of phenylethanolamine was in the order R-(−)-PEOH > R,S-(racemic)-PEOH > S-(+)-PEOH.

Toxicology

The minimum lethal dose (m.l.d.) upon subcutaneous administration to guinea pigs was ~ 1000 mg/kg; the m.l.d. upon intravenous administration to rabbits was 25–30 mg/kg.; in rats, the m.l.d. after intravenous administration was 140 mg/kg.

See also

* Halostachine
* List of controlled D-methamphetamine precursors

References

{{DEFAULTSORT:Hydroxyphenethylamine, 2-
Phenylethanolamines
Phenylethanolamine
Phenylethanolamine
Norepinephrine releasing agents