ISMN TABLET (EXTENDED-RELEASE)

Država: Kanada

Jezik: engleski

Izvor: Health Canada

Kupi sada

Preuzimanje Svojstava lijeka (SPC)
21-09-2015

Aktivni sastojci:

ISOSORBIDE-5-MONONITRATE

Dostupno od:

SIVEM PHARMACEUTICALS ULC

ATC koda:

C01DA14

INN (International ime):

ISOSORBIDE MONONITRATE

Doziranje:

60MG

Farmaceutski oblik:

TABLET (EXTENDED-RELEASE)

Sastav:

ISOSORBIDE-5-MONONITRATE 60MG

Administracija rute:

ORAL

Jedinice u paketu:

30/100

Tip recepta:

Ethical

Područje terapije:

NITRATES AND NITRITES

Proizvod sažetak:

Active ingredient group (AIG) number: 0120456002; AHFS:

Status autorizacije:

CANCELLED POST MARKET

Datum autorizacije:

2017-06-27

Svojstava lijeka

                                PRODUCT MONOGRAPH
Pr
ISMN
Isosorbide-5-mononitrate extended release tablets, BP
60 mg
Antianginal Agent
SIVEM PHARMACEUTICALS ULC
4705 Dobrin Street
Saint-Laurent, Quebec
H4R 2P7
www.sivem.ca
Date of Preparation:
September 21, 2015
Submission Control No.: 187095
Sivem
TM
is a trademark of Sivem Pharmaceuticals ULC
PRODUCT MONOGRAPH
NAME OF DRUG
ISMN
isosorbide-5-mononitrate extended release tablets, BP
60 mg
THERAPEUTIC CLASSIFICATION
Antianginal agent
ACTIONS AND CLINICAL PHARMACOLOGY
As with other organic nitrates, the principal pharmacological action
of isosorbide-5-mononitrate,
the major active metabolite of isosorbide dinitrate (ISDN), is
relaxation of vascular smooth
muscle and consequent dilation of peripheral arteries and veins,
especially the latter. Dilation of
the veins promotes peripheral pooling of blood and decreases venous
return to the heart, thereby
reducing left ventricular end-diastolic pressure and pulmonary
capillary wedge pressure (pre-
load). Arteriolar relaxation reduces systemic vascular resistance,
systolic arterial pressure, and
mean arterial pressure (after-load). Dilation of the coronary arteries
also occurs. The
hemodynamic responses to isosorbide-5-mononitrate are similar to those
produced by other
nitrates.
PHARMACODYNAMICS
Dosage regimens for most chronically used drugs are designed to
provide plasma concentrations
that are continuously greater than a minimally effective
concentration. This strategy is
inappropriate for organic nitrates. Prolonged administration of
nitrate drugs according to
traditionally recommended dosage regimens has been shown to produce
tolerance. Tolerance
results in a loss of efficacy. Several well-controlled clinical trials
have used exercise testing to
assess the antianginal efficacy of continuously delivered nitrates. In
the large majority of these
trials, nitrate effectiveness was indistinguishable from placebo after
24 hours (or less) of
continuous therapy. Attempts to overcome tolerance by dose escalation,
even to doses far in
excess of those used acu
                                
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