Piperazine ( ) is an organic compound that consists of a six-membered ring containing two nitrogen atoms at opposite positions in the ring. Piperazine exists as small alkaline deliquescent crystals with a saline taste.
The piperazines are a broad class of chemical compounds , many with important pharmacological properties, which contain a core piperazine functional group .
Origin and naming [ edit ]
Piperazines were originally named because of their chemical similarity with piperidine , part of the structure of piperine in the black pepper plant (Piper nigrum ). It is important to note, however, that piperazines are not derived from plants in the Piper genus .
Chemistry [ edit ]
Piperazine is freely soluble in water and ethylene glycol , but insoluble in diethyl ether . It is a weak base with two pKb s of 5.35 and 9.73 at 25 °C.; the pH of a 10% aqueous solution of piperazine is 10.8-11.8. Piperazine readily absorbs water and carbon dioxide from the air. Although many piperazine derivatives occur naturally, piperazine itself can be synthesized by reacting alcoholic ammonia with 1,2-dichloroethane , by the action of sodium and ethylene glycol on ethylene diamine hydrochloride , or by reduction of pyrazine with sodium in ethanol .
A form in which piperazine is commonly available industrially is as the hexahydrate , C4 H10 N2 . 6H2 O, which melts at 44 °C and boils at 125-130 °C.[2]
Two common salts in the form of which piperazine is usually prepared for pharmaceutical or veterinary purposes are the citrate, 3C4 H10 N2 .2C6 H8 O7 (i.e. containing 3 molecules of piperazine to 2 molecules of citric acid ), and the adipate, C4 H10 N2 .C6 H10 O4 (containing 1 molecule each of piperazine and adipic acid ).[2]
Industrial production [ edit ]
Piperazine is formed as a co-product in the ammoniation of 1,2-dichloroethane or ethanolamine . These are the only routes to the chemical used commercially.[3] The piperazine is separated from the product stream, which contains ethylenediamine , diethylenetriamine , and other related linear and cyclic chemicals of this type.
As an anti-helmintic [ edit ]
Piperazine was first introduced as an anthelmintic in 1953[citation needed ] . A large number of piperazine compounds have anthelmintic action. Their mode of action is generally by paralysing parasites , which allows the host body to easily remove or expel the invading organism. The neuromuscular effects are thought to be caused by blocking acetylcholine at the myoneural junction. This action is mediated by its agonist effects upon the inhibitory GABA (γ-aminobutyric acid) receptor . Its selectivity for helminths is because vertebrates only use GABA in the CNS and the helminths' GABA receptor is a different isoform to the vertebrates' one.[4]
Piperazine hydrate , piperazine adipate and piperazine citrate (used to treat ascariasis and enterobiasis [5] ) are the most common anthelmintic piperazine compounds. These drugs are often referred to simply as "piperazine" which may cause confusion between the specific anthelmintic drugs, the entire class of piperazine-containing compounds, and the compound itself.
Diethylcarbamazine , a derivative of piperazine, is used to treat some types of filariasis .
Other uses [ edit ]
Piperazines are also used in the manufacture of plastics, resins, pesticides, brake fluid and other industrial materials. Piperazines, especially BZP and TFMPP were extremely common adulterants in the club and rave scene, often being passed off as MDMA , although they do not share many similarities in their effects.
Piperazine is also a fluid used for CO2 and H2 S scrubbing in association with methyl diethanolamine (MDEA).
Carbon Capture and Storage [ edit ]
Simplified absorption column. Typical operating range: 35-50
o C and 5-205 atm of absolute pressure
Amine blends that are activated by concentrated piperazine are used extensively in commercial CO2 removal for carbon capture and storage (CCS) because piperazine advantageously allows for protection from significant thermal and oxidative degradation at typical coal flue gas conditions. The thermal degradation rates for methyl diethanolamine (MDEA) and piperazine (PZ) are negligible, and PZ, unlike other metals, protect MDEA from oxidative degradation.[6] This increased stability of the MDEA/PZ solvent blend over MDEA and other amine solvents provides for greater capacity for and requires less work to capture a given amount of CO2 .
Piperazine's solubility is low, so it is often used in relatively small amounts to supplement another amine solvent. One or more of piperazine's performance advantages are often compromised in practice due to its low concentration; nonetheless, the CO2 absorption rate, heat of absorption, and solvent capacity are increased through the addition of piperazine to amine gas treating solvents, the most common of which is MDEA due to its unmatched high rate and capacity efficiency. For example, a 5 m PZ/5 m MDEA blend yields an 11% larger difference in CO2 concentration than 8 m PZ between the lean (inlet absorbent) and rich (outlet absorbent) amine solvent streams, or in other words, more CO2 is removed from the sour (flue) gas stream per unit mass of solvent, and an almost 100% larger concentration difference than 7 m MEA .[7]
Given that typical amine-based absorption processes run at temperatures from 45 °C to 55 °C, the capabilities of piperazine are well within the bounds of and thus favored for carbon capture. Piperazine can be thermally regenerated through multi-stage flash distillation and other methods after being used in operating temperatures up to 150 °C and recycled back into the absorption process, providing for higher overall energy performance in amine gas treating processes.[8]
The advantages to using concentrated piperazine (CPZ) as an additive had been confirmed through, for example, three pilot plants in Australia that are operated by CSIRO . This program was launched to explore remedies to the high costs of post-combustion carbon capture, and the results were positive. Using CPZ, which is more reactive and thermally stable than standard MEA solutions, capital and compression (energy) costs were lowered through size reductions in absorber columns and solvent regeneration at higher temperatures.[9]
Chemistry [ edit ]
The amine groups on piperazine react readily with carbon dioxide to produce PZ carbamate at a low loading (mol CO2 /equiv PZ) range and PZ bicarbamate at an operating range of 0.31-0.41 mol CO2 /equiv PZ, enhancing the rate of overall CO2 absorbed under operating conditions (refer to Figure 1 below). Due to these reactions, there is limited free piperazine present in the solvent, resulting in its low volatility and rates of precipitation as PZ-6H2 O.[8]
Piperazine (PZ) reacts with carbon dioxide to produce PZ carbamate and PZ bicarbamate at low loading and operating range, respectively.
Piperazine derivatives as drugs [ edit ]
Many currently notable drugs contain a piperazine ring as part of their molecular structure. Examples include:
Antianginals
Antidepressants
Antihistamines
Antiserotonergics
Antipsychotics
Recreational Drugs
Urologicals
Others
Most of these agents can be classified as either phenylpiperazines , benzylpiperazines , diphenylmethylpiperazines (benzhydrylpiperazines), pyridinylpiperazines , pyrimidinylpiperazines , or tricyclics (with the piperazine ring attached to the heterocyclic moiety via a side chain ).
See also [ edit ]
References [ edit ]
^ a b c d e Merck Index , 11th Edition, 7431
^ a b The Merck index, 10th Ed. (1983), p. 1076, Rahway:Merck & Co.
^ Ashford’s Dictionary of Industrial Chemicals , 3rd edition, 7332
^ Martin RJ (31 July 1997). "Modes of action of anthelmintic drugs" . The Veterinary Journal . 154 (1): 11–34. doi :10.1016/S1090-0233(05)80005-X .
^ "Helminths: Intestinal nematode infection: Piperazine" . WHO Model Prescribing Information: Drugs Used in Parasitic Diseases - Second Edition . WHO . 1995. Retrieved 2015-08-29 .
^ Closmann, Fred; Nguyen, Thu; Rochelle, Gary T. (February 2009). "MDEA/Piperazine as a solvent for CO2 capture" . Energy Procedia . 1 (1): 1351–1357. doi :10.1016/j.egypro.2009.01.177 . Retrieved 15 April 2016 .
^ Li, Le; Voice, Alexander K.; Li, Han; Namjoshi, Omkar; Nguyen, Thu; Du, Yang; Rochelle, Gary T. (2013). "Amine blends using concentrated piperazine" . Energy Procedia . 37 : 353–369. doi :10.1016/j.egypro.2013.05.121 . Retrieved 15 April 2016 .
^ a b Rochelle, Gary; Chen, Eric; Freeman, Stephanie; Wagener, David V.; Xu, Qing; Voice, Alexander (15 July 2011). "Aqueous piperazine as the new standard for CO2 capture technology" . Chemical Engineering Journal . 171 (3): 725–733. doi :10.1016/j.cej.2011.02.011 . Retrieved 15 April 2016 .
^ Cottrell, Aaron; Cousins, Ashleigh; Huang, Sanger; Dave, Narendra; Do, Thong; Feron, Paul H.M.; McHugh, Stephen; Sinclair, Michael (September 2013). Concentrated Piperazine based Post-Combustion Capture for Australian coal-fired power plants (Report). Australian National Low Emissions Coal Research & Development. pp. 9–31. Retrieved 3 May 2016 .
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Typical antipsychotics (e.g., chlorpromazine , loxapine )
5-HT7
Antagonists: Atypical antipsychotics (e.g., amisulpride , aripiprazole , asenapine , clorotepine , clozapine , fluperlapine , olanzapine , risperidone , sertindole , tiospirone , ziprasidone , zotepine )
Butaclamol
DR-4485
EGIS-12233
Ergolines (e.g., 2-Br-LSD (BOL-148) , amesergide , bromocriptine , cabergoline , dihydroergotamine , ergotamine , LY-53857 , LY-215840 , mesulergine , metergoline , methysergide , sergolexole )
JNJ-18038683
Ketanserin
LY-215840
Metitepine (methiothepin)
Ritanserin
SB-258719
SB-258741
SB-269970
SB-656104
SB-656104A
SB-691673
SLV-313
SLV-314
Spiperone
SSR-181507
Tetracyclic antidepressants (e.g., amoxapine , maprotiline , mianserin , mirtazapine )
Tricyclic antidepressants (e.g., amitriptyline , clomipramine , imipramine )
Typical antipsychotics (e.g., acetophenazine , chlorpromazine , chlorprothixene , fluphenazine , loxapine , pimozide )
Vortioxetine
Psychedelics
(5-HT2A
agonists)
HOT-*
25*-NB*
(excludes FLY)
Subst.
mescaline
3C-*
4C-*
FLY
Others
Piperazines
4,5-DHP-DMT
2,N,N-TMT
4-AcO-DMT
4-HO-5-MeO-DMT
4,N,N-TMT
4-Propionyloxy-DMT
5,6-diBr-DMT
5-AcO-DMT
5-Bromo-DMT
5-MeO-2,N ,N -TMT
5-MeO-4,N ,N -TMT
5-MeO-α,N,N-TMT
5-MeO-DMT
5-N ,N -TMT
7,N,N-TMT
α,N,N-TMT
(Bufotenin) 5-HO-DMT
DMT
Norbaeocystin
(Psilocin) 4-HO-DMT
(Psilocybin) 4-PO-DMT
Others
Others
Dissociatives
(NMDAR
antagonists )
Deliriants
(mAChR
antagonists )
Others
Adamantanes
Adenosine antagonists
Alkylamines
Ampakines
Arylcyclohexylamines
Benzazepines
Cholinergics
Convulsants
Eugeroics
Oxazolines
Phenethylamines
1-(4-Methylphenyl)-2-aminobutane
1-Phenyl-2-(piperidin-1-yl)pentan-3-one
1-Methylamino-1-(3,4-methylenedioxyphenyl)propane
2-Fuoroamphetamine
2-Fuoromethamphetamine
2-OH-PEA
2-Phenyl-3-aminobutane
2-Phenyl-3-methylaminobutane
2,3-MDA
3-Fuoroamphetamine
3-Fluoroethamphetamine
3-Fluoromethcathinone
3-Methoxyamphetamine
3-Methylamphetamine
3,4-DMMC
4-BMC
4-CMC
4-Ethylamphetamine
4-Fluoroamphetamine
4-Fluoromethamphetamine
4-MA
4-Methylbuphedrone
4-Methylcathinone
4-MMA
4-Methylpentedrone
4-MTA
6-FNE
AL-1095
Alfetamine
a-Ethylphenethylamine
Amfecloral
Amfepentorex
Amfepramone
Amidephrine
2-Amino-1,2-dihydronaphthalene
2-Aminoindane
5-(2-Aminopropyl)indole
2-Aminotetralin
Acridorex
Amphetamine (Dextroamphetamine , Levoamphetamine )
Amphetaminil
Arbutamine
β-Methylphenethylamine
β-Phenylmethamphetamine
Benfluorex
Benzedrone
Benzphetamine
BDB
BOH
3-Benzhydrylmorpholine
BPAP
Buphedrone
Bupropion
Butylone
Camfetamine
Cathine
Cathinone
Chlorphentermine
Cilobamine
Cinnamedrine
Clenbuterol
Clobenzorex
Cloforex
Clortermine
Cypenamine
D -Deprenyl
Denopamine
Dimethoxyamphetamine
Dimethylamphetamine
Dimethylcathinone
Dobutamine
DOPA (Dextrodopa , Levodopa )
Dopamine
Dopexamine
Droxidopa
EBDB
Ephedrine
Epinephrine
Epinine
Etafedrine
Ethcathinone
Ethylnorepinephrine
Ethylone
Etilamfetamine
Etilefrine
Famprofazone
Fencamfamin
Fencamine
Fenethylline
Fenfluramine (Dexfenfluramine , Levofenfluramine )
Fenproporex
Feprosidnine
Flephedrone
Fludorex
Formetorex
Furfenorex
Gepefrine
Hexapradol
Hexedrone
HMMA
Hordenine
4-Hydroxyamphetamine
5-Iodo-2-aminoindane
Ibopamine
IMP
Indanylamphetamine
Iofetamine
Isoetarine
Isoethcathinone
Isoprenaline
L -Deprenyl (Selegiline)
Lefetamine
Lisdexamfetamine
Lophophine
MBDB
MDA
MDBU
MDEA
MDMA
MDMPEA
MDOH
MDPR
MDPEA
Mefenorex
Mephedrone
Mephentermine
Metanephrine
Metaraminol
Mesocarb
Methamphetamine (Dextromethamphetamine , Levomethamphetamine )
Methoxamine
Methoxyphenamine
MMA
Methcathinone
Methedrone
Methoxyphenamine
Methylenedioxycathinone
Methylone
Mexedrone
MMDA
MMDMA
MMMA
Morforex
N,alpha-Diethylphenylethylamine
N-Benzyl-1-phenethylamine
N-Ethylbuphedrone
N-Ethylhexedrone
N,N-Dimethylphenethylamine
Naphthylamphetamine
Nisoxetine
Norepinephrine
Norfenefrine
Norfenfluramine
Normetanephrine
L -Norpseudoephedrine
Octopamine (drug)
Orciprenaline
Ortetamine
Oxifentorex
Oxilofrine
PBA
PCA
PCMA
PHA
Pentorex
Pentedrone
Pentylone
Phenatine
Phenpromethamine
Phentermine
Phenylalanine
Phenylephrine
Phenylpropanolamine
Pholedrine
PIA
PMA
PMEA
PMMA
PPAP
Phthalimidopropiophenone
Prenylamine
Propylamphetamine
Pseudoephedrine
Ropinirole
Salbutamol (Levosalbutamol )
Sibutramine
Synephrine
Theodrenaline
Tiflorex
Tranylcypromine
Tyramine
Tyrosine
Xylopropamine
Zylofuramine
Phenylmorpholines
Piperazines
Piperidines
Pyrrolidines
Racetams
Tropanes
Tryptamines
Others