NU-AZATHIOPRINE TABLET
국가: 캐나다
언어: 영어
출처: Health Canada
제품 특성 요약
(SPC)
11-02-2004
이 제품에 대한 일부 문서는 현재 사용할 수 없습니다. 고객 서비스에 요청을 보내면 가능한 빨리 알려 드리겠습니다.
요청을 보내십시오.
요청을 보내십시오.
유효 성분:
AZATHIOPRINE
제공처:
NU-PHARM INC
ATC 코드:
L04AX01
INN (International Name):
AZATHIOPRINE
복용량:
50MG
약제 형태:
TABLET
구성:
AZATHIOPRINE 50MG
관리 경로:
ORAL
패키지 단위:
100
처방전 유형:
Prescription
치료 영역:
IMMUNOSUPPRESSIVE AGENTS
제품 요약:
Active ingredient group (AIG) number: 0101830001; AHFS:
승인 상태:
CANCELLED (UNRETURNED ANNUAL)
승인 날짜:
2018-03-28
제품 특성 요약
1
PRODUCT MONOGRAPH
NU-AZATHIOPRINE
AZATHIOPRINE TABLETS USP
50 MG
IMMUNOSUPPRESSIVE AGENT
NU-PHARM INC.
DATE OF PREPARATION:
50 MURAL STREET UNITS 1 & 2
January 12, 2004
RICHMOND HILL, ONTARIO
L4B 1E4
_Control #: 089003_
2
PRODUCT MONOGRAPH
NU-AZATHIOPRINE
Azathioprine Tablets USP
50 mg
THERAPEUTIC CLASSIFICATION
Immunosuppressive Agent
ACTIONS AND CLINICAL PHARMACOLOGY
METABOLISM
Azathioprine is well absorbed following oral administration. Maximum
serum radioactivity
occurs at one to two hours after oral
35
S-azathioprine and decays with a half-life of five hours.
This is not an estimate of the half-life of azathioprine itself but is
the decay rate for all
35
S-
containing metabolites of the drug. Because of extensive metabolism,
only a fraction of the
radioactivity is present as azathioprine. Usual doses produce blood
levels of azathioprine, and
of mercaptopurine derived from it, which are low (<1
:
g/mL). Blood levels are of little predictive
value for therapy since the magnitude and duration of clinical effects
correlate with thiopurine
nucleotide levels in tissues rather than with plasma drug levels.
Azathioprine and
mercaptopurine are moderately bound to serum proteins (30%) and are
partially dialyzable.
Azathioprine is cleaved _in vivo_ to mercaptopurine. Both compounds
are rapidly eliminated from
blood and are oxidized or methylated in erythrocytes and liver; no
azathioprine or
mercaptopurine is detectable in urine after eight hours. Conversion to
inactive 6-thiouric acid by
xanthine oxidase is an important degradative pathway, and the
inhibition of this pathway in
patients receiving Zyloprim® (allopurinol) is the basis for the
azathioprine dosage reduction
required in these patients (see Drug Interactions under PRECAUTIONS).
Proportions of
metabolites are different in individual patients, and this presumably
accounts for variable
magnitude and duration of drug effects. Renal clearance is probably
not important in predicting
biological effectiveness or toxicities, although dose reduction is
practised in
전체 문서 읽기
