NOVO-CEFACLOR CAPSULE

Šalis: Kanada

kalba: anglų

Šaltinis: Health Canada

Nusipirk tai dabar

Parsisiųsti Prekės savybės (SPC)
12-10-2016

Veiklioji medžiaga:

CEFACLOR

Prieinama:

TEVA CANADA LIMITED

ATC kodas:

J01DC04

INN (Tarptautinis Pavadinimas):

CEFACLOR

Dozė:

500MG

Vaisto forma:

CAPSULE

Sudėtis:

CEFACLOR 500MG

Vartojimo būdas:

ORAL

Vienetai pakuotėje:

100

Recepto tipas:

Prescription

Gydymo sritis:

SECOND GENERATION CEPHALOSPORINS

Produkto santrauka:

Active ingredient group (AIG) number: 0113428004; AHFS:

Autorizacija statusas:

CANCELLED POST MARKET

Leidimo data:

2018-04-30

Prekės savybės

                                PRODUCT MONOGRAPH
NOVO-CEFACLOR
(cefaclor)
250 mg and 500 mg Capsules
USP
Antibiotic
Teva Canada Limited
Date of Revision: May 7, 2014
30 Novopharm Court
Toronto, Ontario
M1B 2K9
Control # 173960
PRODUCT MONOGRAPH
NOVO-CEFACLOR
(cefaclor)
250 mg and 500 mg Capsules
USP
THERAPEUTIC CLASSIFICATION
Antibiotic
ACTION
-lactam antibiotics, cefaclor owes its antibacterial activity to its
ability to bind to
and inhibit the action of certain bacterial cell wall synthetic
enzymes, the penicillin-binding
proteins.
CLINICAL PHARMACOLOGY
Cefaclor is well absorbed after oral administration to fed and fasted
subjects. Following doses
of 250 mg, 500 mg and 1 g to fasted subjects, average peak serum
levels of approximately 7, 13
and 23 mg/L respectively were obtained within 0.5 to 1.0 hour. Total
absorption is the same
whether the drug is given before or after meals. However, when it is
taken after food, the peak
concentration achieved is 50% to 75% of that observed when the drug is
administered to fasted
subjects and is delayed by 0.8 to 1 hour. Approximately 25% of
cefaclor is bound to human
plasma.
Within 8 hours 60% to 85% of the drug is excreted unchanged in the
urine, the greater portion
being excreted within the first 2 hours. During this 8-hour period,
peak urine concentrations
following the 250 mg, 500 mg and 1 g doses were approximately 600, 900
and 1,900 mg/L
respectively.
The serum half-life in normal subjects is 0.6 to 0.9 hours. In
patients with reduced renal
function, the serum half-life of cefaclor is slightly prolonged. In
those with complete absence of
renal function, the plasma half-life of the intact molecule is 2.3 to
2.8 hours. Excretion
pathways in patients with markedly impaired renal function have not
been determined.
Hemodialysis shortens the half-life by 25% to 30%.
Probenecid administered with a 500 mg dose of cefaclor
increased the peak serum concentration
only slightly, from 12.4 to 13.9 mg/L, and urine levels were
predictably diminished. The mean
half-life among five fasted volunteers with normal re
                                
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