| Identification | Back Directory | [Name]
Reserpine | [CAS]
50-55-5 | [Synonyms]
H 520
R-e-s
reserp
Kitine
Raugal
Raulen
Raucap
Rausan
Resine
rezide
Serfin
Serpen
T-Serp
Anguil
serpoid
serpone
Sertabs
Sertina
serpine
Serpate
Sedserp
Riserpa
rivased
Rivasin
rolserp
Sandril
Restran
Rau-sed
Raupoid
Raurine
Neoserp
recipin
rauwita
Rawilid
Rautrin
Rauvlid
Alkarau
Alserin
Apoplon
Apsical
Banasil
banisil
Benazyl
carpacil
Carrserp
Eberpine
gilucard
Hiserpia
ent50146
Eserpine
Eskaserp
Hypersil
Idsoserp
Rauwilid
Rauwipur
Raupasil
resaltex
Resedrex
resedril
rese-lar
reser-ar
Reserbal
Resercen
reserfia
Reserjen
Reserlor
regroton
renese-r
Reserpex
reserpal
Quiescin
Rausedan
Rausedil
Rausedyl
Lemiserp
Loweserp
rezerpin
residine
Respital
resocalm
resomine
resperin
Reserpil
reserpur
salupres
Roxinoid
seominal
serfolia
Serolfia
Serp-AFD
serpalan
serpazil
serpazol
serpedin
Serpasil
serpasol
Serpipur
Serpicon
serplexk
serpogen
serpyrit
Triserpin
usafcb-27
serpresan
Serpiloid
serpivite
serpatone
serpazide
Serpaloid
Serpanray
ser-a-gen
serathide
resersana
reserutin
resiatric
reserpene
Reserpoid
resperine
Interpina
Neoserfin
Raudiford
Raudixoid
Rauloydin
Raumorine
Raunervil
Raunorine
Rauwoleaf
Resercaps
Rauserpol
Rausingle
Hypersine
hiposepil
hydropine
hydroserp
esidrix#2
Escaspere
diurese-r
ENT 50146
Eberspine
Elserpine
Deserpine
Carditivo
RESERPINE
Bioserpine
Broserpine
Austrapine
diupres250
diupres500
Enipresser
Hiposerpil
hydromox-r
Rauserpine
Rauwasedin
Reserpamed
reserpanca
Purserpine
NCI-C50157
klimanosid
mallopress
Maviserpin
Mayserpine
salutensin
Sedaraupin
Serpentina
Vio-Serpine
Mephaserpin
l-Carpserp
Key-serpine
reserpidefe
hydrosine25
hydropres25
hydropres50
Helfoserpin
diutensen-r
Eskaserpine
Ascoserpina
l-Carpserp
metatensin#2
metatensin#4
Temposerpine
Reserpine bp
salazide-demi
Reserpine,98%
Reserpine,99%
RESERPINE,USP
RESERPINE(RG)
Rauserpin-Alk
Crystoserpine
demi-regroton
gamma-Serpine
hydroserpalan
hydroserpine#1
chloroserp-250
chloroserp-500
Neo-antitensol
trichlortensin
serpasilpremix
Serpasil premix
salutensin-demi
ReserpinePuriss
hydrochloride#1
hydrochloride#2
hydroserpineplus
chloroserpin-250
METHYL RESERPATE
RESERPINE BP/USP
tri-hydroserpine
RESERPINE,REAGENT
chloroserpine-500
hydro-reserpine-25
hydro-reserpine-50
hydro-fluserpine#1
Reserpine (200 mg)
RESERPINE extrapure
ReserpineC33H40N209
serpasil-apresoline
rcrawastenumberu200
component of Regroton
component of Renese R
reserpine crystalline
(3β,16β,17α,18β,20α)-
RESERPINE, CRYSTALLIZED
serpine(pharmaceutical)
Serpine (pharmaceutical)
Reserpine, froM Rauvolfia
component of Butiserpazide
YohiMban-16-carboxylic acid
Reserpine Standard for LC-MS
3,20-YohiMban-16-carboxylic acid
Reserpine Vetec(TM) reagent grade
3,4,5-TRIMETHOXYBENZOYL METHYL RESERPATE
Reserpine (base and/or unspecified salts)
methylreserpate3,4,5-trimethoxybenzoicacid
oxy-methylester3,4,5-trimethoxybenzoate(ester)
Methyl reserpate 3,4,5-trimethyloxybenzoic acid
(3beta,16beta,17alpha,18beta,20alpha)-methyleste
,methylester,(3beta,16beta,17alpha,18beta,20alpha)-
METHYL RESERPATE 3,4,5-TRIMETHOXYBENZOIC ACID ESTER
imethoxy-,methylester,3,4,5-trimethoxybenzoate(ester)
11,17-dimethoxy-18-((3,4,5-trimethoxybenzoyl)oxy)-yohimban-16-carboxylicaci
11,17-dimethoxy-18-[(3,4,5-trimethoxybenzoyl)oxy]-yohimban-16-carboxylicaci
11,17-DIMETHOXY-18-[(3,4,5-TRIMETHOXYBENZOYL)OXY]YOHIMBAN-16-CARBOXYLIC ACID METHYL ESTER
(3β,16β,17α,18β,20α)-11,17-Dimethoxy-18-[(3,4,5-trimethoxybenzoyl)oxy]yohimban-16-carboxylicacidmethylester
YohiMban-16-carboxylicacid, 11,17-diMethoxy-18-[(3,4,5-triMethoxybenzoyl)oxy]-, Methyl ester, (3b,16b,17a,18b,20a)-
3beta,20alpha-Yohimban-16beta-carboxylic acid, 18beta-hydroxy-11,17alpha-dimethoxy-methyl ester 3,4,5-trimethoxybenzoate (ester)
Yohimban-16-carboxylic acid, 11,17-dimethoxy-18-[(3,4,5-trimethoxybenzoyl)oxy]-, methyl ester, (3beta,16beta,17alpha,18beta,20alpha)-
Yohimban-16-carboxylic acid, 11,17-dimethoxy-18-(3,4,5-trimethoxybenzoyl)oxy-, methyl ester, (3.beta.,16.beta.,17.alpha.,18.beta.,20.alpha.)- | [EINECS(EC#)]
200-047-9 | [Molecular Formula]
C33H40N2O9 | [MDL Number]
MFCD00005091 | [MOL File]
50-55-5.mol | [Molecular Weight]
608.68 |
| Chemical Properties | Back Directory | [Appearance]
Reserpine is a white to pale buff to slightly
yellow crystalline substance that darkens on exposure to
light. | [Melting point ]
~265 °C (dec.)
| [alpha ]
D23 -118° (CHCl3); D26 -164° (c = 0.96 in pyridine); D26 -168° (c = 0.624 in DMF) | [Boiling point ]
655.12°C (rough estimate) | [density ]
1.2336 (rough estimate) | [refractive index ]
177 ° (C=1, DMF) | [Fp ]
22℃ | [storage temp. ]
2-8°C | [solubility ]
Practically insoluble in water, very slightly soluble in ethanol (96 per cent). | [form ]
neat | [pka]
6.6(at 25℃) | [color ]
Off-white | [Stability:]
Stable, but darkens slowly in light. Combustible. Incompatible with strong acids, reducing agents, oxidizing agents. | [optical activity]
[α]20/D 123±3°, c = 1% in chloroform | [Water Solubility ]
Soluble in water. | [Merck ]
14,8145 | [BRN ]
102014 | [InChIKey]
QEVHRUUCFGRFIF-MDEJGZGSSA-N | [LogP]
4.050 (est) | [CAS DataBase Reference]
50-55-5 | [IARC]
3 (Vol. 24, Sup 7) 1987 | [NIST Chemistry Reference]
Reserpine(50-55-5) | [EPA Substance Registry System]
Yohimban-16-carboxylic acid, 11,17-dimethoxy-18-[(3,4,5-trimethoxybenzoyl)oxy]-, methyl ester, (3.beta.,16.beta.,17.alpha., 18.beta.,20.alpha.)-(50-55-5) |
| Hazard Information | Back Directory | [Chemical Properties]
off-white crystalline powder | [Usage]
An indole alkaloid found in Rauwolfia serpentina. Inhibits vesicular uptake of catecholamines and serotonin. Reserpine is reasonably anticipated to be a human carcinogen. Antihypertensive. | [Uses]
An indole alkaloid found in Rauwolfia serpentina. Inhibits vesicular uptake of catecholamines and serotonin. Reserpine is reasonably anticipated to be a human carcinogen. Antihypertensive. | [Uses]
An inhibitor of transport of biogenic amines into adrenal chromaffin granules | [Definition]
ChEBI: An alkaloid found in the roots of Rauwolfia serpentina and R. vomitoria. | [Brand name]
Rau-Sed (Bristol-Myers Squibb); Sandril
(Lilly); Serpasil (Novartis). | [General Description]
White or cream to slightly yellow crystals or crystalline powder. Odorless with a bitter taste. | [Air & Water Reactions]
Insoluble in water. Reacts slowly with air and water. Darkens slowly on exposure to light. | [Reactivity Profile]
Reserpine is a weak base and can form salts with strong acids. Incompatible with oxidizing agents and reducing agents. | [Fire Hazard]
Flash point data for Reserpine are not available; however, Reserpine is probably combustible. | [Hazard]
Questionable carcinogen.
| [Biological Activity]
Binds the vesicular monoamine transporter (VMAT2) and inhibits transport of biogenic amines into adrenal chromaffin granules and synaptic vesicles. Causes depletion of biogenic amine stores. Antihypertensive and antipsychotic. | [Potential Exposure]
Reserpine, a pharmaceutical, is a natu-
rally occurring substance that is isolated from the roots of
the plant rauwolfia serpentina. Insoluble in water.
Reserpine is used as a hypertensive for humans and ani-
mals; tranquilizer, and sedative. Permitted for use as an
additive in food for human consumption, and the feed and
drinking water of food-producing animals. | [First aid]
Skin Contact: Flood all areas of body that have
contacted the substance with water. Don’t wait to remove
contaminated clothing; do it under the water stream. Use
soap to help assure removal. Isolate contaminated cloth-
ing when removed to prevent contact by others . Eye
Contact: Remove any contact lenses at once.
Immediately flush eyes well with copious quantities of
water or normal saline for at least 20?30 minutes. Seek
medical attention. Inhalation: Leave contaminated area
immediately; breathe fresh air. Proper respiratory protec-
tion must be supplied to any rescuers. If coughing, diffi-
cult breathing, or any other symptoms develop, seek
medical attention at once, even if symptoms develop
many hours after exposure. Ingestion: Contact a physi-
cian, hospital, or poison center at once. If the victim is
unconscious or convulsing, do not induce vomiting or give anything by mouth. Assure that the patient’s airway
is open and lay him on his side with his head lower than
his body and transport immediately to a medical facility.
If conscious and not convulsing, give a glass of water to
dilute the substance. Vomiting should not be induced
without a physician’s advice. | [Shipping]
UN1544 Alkaloids, solid, n.o.s. or Alkaloid salts,
solid, Hazard Class: 6.1; Labels: 6.1-Poisonous materials,
Technical Name Required. UN3077 Environmentally haz-
ardous substances, solid, n.o.s., Hazard class: 9; Labels: 9-
Miscellaneous hazardous material, Technical Name
Required. | [Incompatibilities]
A weak acid; keep away from bases.
Incompatible with oxidizers (chlorates, nitrates, peroxides,
permanganates, perchlorates, chlorine, bromine, fluorine,
etc.); contact may cause fires or explosions. Keep away
from alkaline materials, strong bases, strong acids, oxoa-
cids, epoxides, and strong reducing agents such as hydri-
deds and active metals. Compounds of the carboxyl group
react with all bases, both inorganic and organic (i.e.,
amines) releasing substantial heat, water, and a salt that
may be harmful. Incompatible with arsenic compounds
(releases hydrogen cyanide gas), diazo compounds, dithio-
carbamates, isocyanates, mercaptans, nitrides, sulfides
(releasing heat, toxic, and possibly flammable gases),thiosulfates, and dithionites (releasing hydrogen sulfate and
oxides of sulfur). | [Description]
Reserpine causes release of norepinephrine, dopamine, and serotonin at neuronal termini.
It weakens the intracellular uptake of biogenic amines and decreases the ability to store
them in vesicles. | [Waste Disposal]
It is inappropriate and possi-
bly dangerous to the environment to dispose of expired or
waste drugs and pharmaceuticals by flushing them down
the toilet or discarding them to the trash. Household quanti-
ties of expired or waste pharmaceuticals may be mixed
with wet cat litter or coffee grounds, double-bagged in
plastic, discard in trash. Larger quantities shall carefully
take into consideration applicable DEA, EPA, and FDA
regulations. If possible return the pharmaceutical to the
manufacturer for proper disposal being careful to properly
label and securely package the material. Alternatively, the
waste pharmaceutical shall be labeled, securely packaged
and transported by a state licensed medical waste contractor
to dispose by burial in a licensed hazardous or toxic waste
landfill or incinerator. Consult with environmental regula-
tory agencies for guidance on acceptable disposal practices.
Generators of waste containing this contaminant (≥100 kg/
mo) must conform with EPA regulations governing storage,
transportation, treatment, and waste disposal. | [Physical properties]
Appearance: crystalline powder, colorless to yellowish brown, darker in case of
light. Solubility: soluble in chloroform, slightly soluble in acetone, and almost
insoluble in water, methanol, ethanol, or ether. Melting point: 264–265 °C.
Specific optical rotation: ?117.7°. | [History]
In 1931, Indian scholar Sen discovered Indian Rauvolfia have the antihypertensive
and antipsychotic effects. The following studies in medicinal chemistry and pharmacology
found that the main active ingredient is reserpine and clarified th mechanism of lowering blood pressure. In 1952, reserpine was first isolated and won
an important status in treating hypertension and neurological and psychiatric disorders
because of its remarkable physiological attributes. The structure analysis of
reserpine peaked in 1955.The total synthesis of reserpine is completed in 1956.
There are no effective antihypertensive drugs in clinic at the initial stage in our
country, and the reserpine imported from India was scarce and expensive, which
could not meet the urgent needs of patients. In
1958, the Bureau of Drug Administration of Ministry of Health presided over the
work of identifying the total alkaloids in Rauvolfia and approved the first Chinese
antihypertensive drug commercially named “Verticil”. Large scales of studies about
Chinese Rauvolfia as well as the numerous participants promote the rapid progress
of natural medicine. It can be taken as the earliest study in plant medicine since the
founding of China, providing valuable experience to our later studies. | [Biological Functions]
Reserpine (Serpasil) is the prototypical drug interfering
with norepinephrine storage. Reserpine lowers blood
pressure by reducing norepinephrine concentrations in
the noradrenergic nerves in such a way that less norepinephrine
is released during neuron activation.
Reserpine does not interfere with the release process
per se as does guanethidine.
Reserpine also interferes with the neuronal storage
of a variety of central transmitter amines such that significant
depletion of norepinephrine, dopamine, and 5-
hydroxytryptamine (serotonin) occurs. This central
transmitter depletion is responsible for the sedation and
other CNS side effects associated with reserpine therapy.
The depletion of brain amines also may contribute
to the antihypertensive effects of reserpine. | [Health Hazard]
Reserpine produces sedative, hypotensive,
LD50 value, intraperitoneal (mice): 5 mg/kg
LD50 value, oral (mice): 200 mg/kgand tranquilizing effects. This is due to itsactions of causing depletion of monoaminesfrom presynaptic nerve terminals in central and peripheral nervous systems. Theadverse side effects are drowsiness, nightmare, depression, excessive salivation, nausea, diarrhea, increased gastric secretion,abdominal cramps, and hypotension. | [Biochem/physiol Actions]
Reserpine is used to treat hypertensive pregnancy difficulties. This drug is also considered as antipsychotic and antihypertensive, to regulate high blood pressure. | [Mechanism of action]
Reserpine acts to replace and deplete the adrenergic neurons of their stores of norepinephrine by inhibiting the active
transport Mg-ATPase responsible for sequestering norepinephrine and dopamine within the storage vesicles. The
norepinephrine and dopamine that are not sequestered in vesicles are destroyed by MAO. As a result, the storage
vesicles contain little neurotransmitter, adrenergic transmission is dramatically inhibited, and sympathetic tone is
decreased, leading to vasodilation. Reserpine has the same effect on epinephrine storage in the adrenal medulla.
Reserpine readily enters the CNS, where it also depletes the stores of norepinephrine and serotonin. The CNS
neurotransmitter depletion led to the use of reserpine in treating certain mental illnesses. | [Pharmacokinetics]
Limited information is available regarding the pharmacokinetics of reserpine. Peak blood concentrations for reserpine
occur within 2 hours following oral administration, and the full effects for reserpine usually are delayed for at least 2 to
3 weeks. Both CNS and cardiovascular effects may persist for several
days to several weeks after chronic oral therapy is discontinued. Reserpine appears to be widely distributed in body
tissues, especially adipose tissue; crosses the blood-brain barrier and the placenta; and is distributed into milk. The
elimination of reserpine appears to be biphasic, with a plasma half-life averaging 4.5 hours during the first phase and
approximately 11.3 days during the second phase. Reserpine is metabolized to unidentified inactive compounds.
Unchanged reserpine and its metabolites are excreted slowly in urine and feces, with an average of 60% reserpine
recovered in feces within 96 hours after oral administration of 0.25 mg of radiolabeled reserpine. | [Pharmacology]
Reserpine causes a breakdown of norepinephrine, dopamine, and serotonin in neuron end�ings. It weakens intracellular uptake of biogenic amines and reduces the ability if storing
them in vesicles. It is possible that reserpine acts on membrane vesicles, irreversibly
inhibiting ATP-Mg2� (adenosinetriphosphate) requiring process that is responsible for the
uptake of biogenic amines in interneuronal vesicles. Breakdown of catecholamines is
expressed by a decreased number of intraneuronal serotonin and dopamine. | [Clinical Use]
Reserpine is effective orally and parenterally for thetreatment of hypertension. After a single intravenous dose,the onset of antihypertensive action usually begins in about1 hour. After intramuscular injection, the maximumeffect occurs within approximately 4 hours and lasts about10 hours. When it is given orally, the maximum effectoccurs within about 2 weeks and may persist up to 4 weeksafter the final dose. When used in conjunction with otherhypotensive drugs in the treatment of severe hypertension,the daily dose varies from 100 to 250μg. | [Clinical Use]
When reserpine is given orally, its maximum effect is seenafter a couple of weeks. A sustained effect up to severalweeks is seen after the last dose has been given. This isbecause the tight binding of reserpine to storage vesicles continuesfor a prolonged time, and recovery of sympatheticfunction requires synthesis of new vesicles over a period ofdays to weeks after discontinuation of the drug. Most adverseeffects of reserpine (log P=4.37) are caused by CNS effectsbecause it readily enters the CNS. Sedation and inability toconcentrate or perform complex tasks are the most commonadverse effects. More serious is the occasional psychoticdepression that can lead to suicide, which support monoaminetheory of pathology of depression. Agents with fewer sideeffects have largely replaced reserpine in clinical use. | [Side effects]
The most troublesome untoward effects of treatment
with reserpine involve the CNS. Sedation and depression
are the most common, although nightmares
and thoughts of suicide also occur. Reserpine treatment,
therefore, is contraindicated in patients with a history
of severe depression. The occasional report of reserpine-
induced extrapyramidal symptoms, which are
similar to those seen in patients with Parkinson’ s disease,
is believed to be a result of dopamine depletion
from neurons in the CNS.
Peripheral nervous system side effects are the result
of a reserpine-induced reduction of sympathetic function
and unopposed parasympathetic activity; symptoms
include nasal congestion, postural hypotension, diarrhea,
bradycardia, increased gastric secretion, and
occasionally impotence. Because of the increased gastric
secretion, reserpine is contraindicated for patients with peptic ulcer. In patients with little cardiac reserve,
reserpine must be administered with caution because of
its ability to interfere with sympathetic stimulation of
the heart. | [Synthesis]
Reserpine is methyl ester 2α,11-dimethoxy-3-(3,4,5-trimethoxybenzoyloxy)-
yohimban-1-carboxylic acid (12.3.1). Reserpine is one of the alkaloids isolated from a
perennial shrub of the Rauwolfia family [67–72]. It can also be synthesized [73–76]. | [target]
Caspase | SOD | Beta Amyloid | NMDAR | [Carcinogenicity]
Reserpine is reasonably anticipated to be a human carcinogen based on sufficient evidence of carcinogenicity from studies in experimental animals. | [Environmental Fate]
Reserpine is a naturally occurring alkaloid produced by several
members of genus Rauwolfia, indigenous to India, Burma,
Malaysia, Thailand, Nepal, and Indonesia. The release of
reserpine to the environment through several waste streams is
possible due to the manufacture of reserpine and/or excretion
following therapeutic use. It has a pKb of 6.6 and is expected to
be in a partially protonated state in the environment. Reserpine
released into air at ambient temperature and pressure exists
only in the particulate phase and is removed from the atmosphere
by wet and dry deposition. Reserpine released to soil is available in oral dosage forms in combinations with hydralazine
(a vasodilator) and/or hydrochlorothiazide (a thiazide
diuretic). Occupational exposure would be expected to occur
through inhalation or dermal contact. | [storage]
Room temperature | [Purification Methods]
Crystallise reserpine from aqueous Me2CO or Et2O. [Woodward et al. Tertrahedron 2 155 1958, Beilstein 25 III/IV 1319.] | [Toxicity evaluation]
The pharmacology and toxicology of reserpine stem from the
same mechanism of action. Reserpine binds tightly and
irreversibly to the adrenergic storage vesicles, inhibits the
vesicular monoamine transporter 2 (VMAT2), and prevents
the concentration of monogenic amines norepinephrine
(NE) and dopamine (DA) in the nerve terminals. The
neurotransmitters NE and DA are metabolized by monoamine
oxidases and catechol-O-methyl transferases in the
cytoplasm, depleted from nerve terminals, and are unavailable
for release into the synapse upon nerve stimulation.
Sympatholytic activity in peripheral adrenergic neurons
leads to decrease in peripheral vascular resistance, cardiac
output, and blood pressure and in the central adrenergic
neurons, causes central nervous system (CNS) depression.
The action is long lasting because replenishing the storage
vesicles with VMAT and neurotransmitters requires new
protein synthesis and may take days to weeks after discontinuation
of reserpine. |
| Safety Data | Back Directory | [Hazard Codes ]
Xn,Xi | [Risk Statements ]
22-67-36-10 | [Safety Statements ]
22-36/37/39-26 | [RIDADR ]
3077 | [WGK Germany ]
3
| [RTECS ]
ZG0350000
| [F ]
10-23 | [TSCA ]
Yes | [PackingGroup ]
II | [HS Code ]
29399990 | [Safety Profile]
Confirmed human carcinogen producing tumors of the sh and brain. Poison by ingestion, intravenous, subcutaneous, and intraperitoneal routes. Mutation data reported. An experimental teratogen. Human and experimental reproductive effects by ingestion: sullbirth, reduced viability, and other neonatal measures or effects. In humans, 0.014 mg/kg causes psychotropic effects. A medicine with side effects. Used as an addltive permitted in the feed and drinking water of animals and/or for the treatment of food-producing animals. Also permitted in food for human consumption. A sedative. When heated to decomposition it emits toxic fumes of NOx. | [Hazardous Substances Data]
50-55-5(Hazardous Substances Data) | [Toxicity]
LD50 oral in rat: 420mg/kg |
| Questions And Answer | Back Directory | [Overview]
Reserpine is an indole alkaloid found in the roots of Rauwolfia serpentina and R. vomitoria[1]. It is an antipsychotic, and antihypertensive drug that used for the control of high blood pressure and for the relief of psychoticsymptoms[1-4]. However, its adverse effects have limited its clinical use[4]. The antihypertensive actions of reserpine results from its ability to deplete catecholamines(among other monoamine neurotransmitters) from peripheral sympathetic nerve endings[2-4]. Moreover, reserpine also has a peripheral action in many parts of the body, resulting in a preponderance of the effects of the cholinergic part of the autonomous nervous system on the GI tract, smooth muscles, blood vessels, etc[4].
| [Indications]
Reserpine is a drug used for the treatment of hypertension[4, 5,7, 8] and schizophrenia[although rarely used nowadays][4, 6]. It can also be used as an anticholinergic drug to combat excessive cholinergic activity in many parts of the body as well as parkinsonism[9]. Reserpine can be used as sedative for horses in veterinary field. It is used as a long-acting tranquilizer to subdue excitable or difficult horses and has been used illicitly for the sedation of show horses, for-sale horses, and in other circumstances where a "quieter" horse might be desired[10]. In addition, it can be used frequently as a highly useful analytic reference standard in the field of mass spectrometry owing to its availability, ease of ionization under electrospray conditions and stability in solution[11].
| [Mode of action]
Reserpine is an adrenergic blocking agent used to treat mild to moderate hypertension through disrupting the normal process norepinephrine vesicular storage. The antihypertensive actions of Reserpine are a result of its ability of depleting catecholamines from peripheral sympathetic nerve endings[12-14]. These substances are normally involved in controlling heart rate, force of cardiac contraction and peripheral resistance. Reserpine takes effect through inhibition of the ATP/Mg2+ pump responsible for the sequestering of neurotransmitters into storage vesicles located in the presynaptic neuron[13]. The neurotransmitters that are not sequestered in the storage vesicle are readily metabolized by monoamine oxidase[MAO] causing a reduction in catecholamines[12, 14].
| [Adverse reactions]
Some common adverse reactions of reserpine include dizziness, feeling sleepy, dry mouth, headache, muscle pain, stuff nose, upset stomach or throwing up, loose stools, anxiety, weight gain and nosebleed[15, 16]. More severe adverse reactions could occur as allergic reactions(such as rash, hives, itching, red, swollen, blistered with or without fever; wheezing; tightness in the chest or throat; trouble breathing, swallowing, or talking; unusual hoarseness; or swelling of the mouth, face, lips, tongue, or throat), chest pain or pressure, low mood(nervousness, suicidal mood, emotional ups and downs and anxiety), enlarged breasts, breast soreness, bad dreams, not hungry, swelling, lowered interest in sex, hearing loss, shortness of breath, trouble controlling body movements, pain when passing urine[16].
| [Warning and precautions]
Patients of the following conditions should be disabled: being allergic, depression history, a history of suicidal thought, a stomach ulcer, ulcerative colitis and who are subjecting to treatment with electroconvulsive therapy. Patients should also seek advice from the doctors if he/she has gallstones, kidney disease, or a history of stomach problems or slow digestion, plan or has already become pregnant. Since reserpine can pass into breast milk and may do harm to a nursing baby, breast-feed is not allowed during taking this drug. Reserpine is only allowed for use in people older than 18 years old[16].
| [References]
1. https://www.drugbank.ca/drugs/DB00206
2. Doyle, A. E., E. G. Mcqueen, and F. H. Smirk. "Treatment of hypertension with reserpine, with reserpine in combination with pentapyrrolidinium, and with reserpine in combination with Veratrum alkaloids." Circulation11.2(1955]:170.
3. Hughes, W. M., E. Dennis, and J. H. Moyer. "Treatment of hypertension with oral reserpine alone and in combination with hydralazine or hexamethonium. " American Journal of the Medical Sciences229.2(1955]:121-134.
4. The Columbia Encyclopedia, Sixth Edition. Copyright © 2001-05 Columbia University Press.
5. Kurland, A. A. "Comparison of chlorpromazine and reserpine in treatment of schizophrenia; a study of four hundred cases. " A.m.a.archives of Neurology & Psychiatry 75.5(1956]:510-513.
6. Braun, M. "Reserpine as a therapeutic agent in schizophrenia. " American Journal of Psychiatry 116.3(1960]:744.
7. Shamon SD, Perez MI[2009]. "Blood pressure lowering efficacy of reserpine for primary hypertension". Cochrane Database of Systematic Reviews. 4[4]: CD007655.
8. Chobanian AV, Bakris GL, Black HR, et al.[2003]. "The Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure: the JNC 7 report". JAMA. 289[19]: 2560–72.
9. Sharma, V. K., Harik, S. I., Ganapathi, M., Busto, R., & Banerjee, S. P.[1979]. Locus ceruleus lesion and chronic reserpine treatment: effect on adrenergic and cholinergic receptors in cerebral cortex and hippocampus. Experimental Neurology, 65(3], 685-690.
10. http://www.wedgewoodpetrx.com/learning-center/professional-monographs/reserpine-for-veterinary-use.html
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