2',3'-ジデオキシイノシン 化学特性,用途語,生産方法
外観
白色~わずかにうすい黄色
用途
核酸アナログ逆転写酵素阻害
剤です。ウィルス DNA ポリメラーゼによる
基質の取り込みを競合的に阻害し、DNA 鎖の
伸長を停止することにより、ウィルスの増殖
阻害作用を示します。
用途
核酸アナログ逆転写酵素阻害
剤です。ウイルス DNA ポリメラーゼによる
基質の取り込みを競合的に阻害し、DNA 鎖の
伸長を停止することにより、ウイルス増殖阻
害作用を示します。
効能
抗ウイルス薬, 逆転写酵素阻害薬
説明
Didanosine is an orally active purine dideoxynucleoside analog indicated for adult and
pediatric patients with advanced HIV infection who are either intolerant or significantly
deteriorated on zidovudine. It appears to increase CD4 cell counts and decrease p24
antigen levels.Major adverse effects are pancreatitis, peripheral neuropathy and
diarrhea.Unlike zidovudine, didanosine exhibits insignificant bone marrow
suppression.
化学的特性
White Powder
使用
2?,3?-Dideoxyinosine is a potent anti-retroviral agent. It is most effective in combination therapy for the treatment of HIV and related lymphoma.
適応症
Didanosine (ddI, Videx) is an adenosine analogue with
activity against HIV-1, HIV-2, and HTLV-I. It is approved
as part of a multidrug regimen for the therapy of
HIV infection and is also used as postexposure HIV
prophylaxis
定義
ChEBI: A purine 2',3'-dideoxyribonucleoside that is inosine in which the hydroxy groups at both the 2' and the 3' positions on the sugar moiety have been replaced by hydrogen.
抗菌性
Didanosine is active against HIV-1, HIV-2 and HTLV-1.
獲得抵抗性
Codon changes at positions 65 or 74 in HIV reverse transcriptase
are associated with reduced susceptibility.
一般的な説明
Didanosine (Videx, ddI) is 2',3'-dideoxyinosine (ddI), a synthetic purine nucleoside analog that is bioactivatedto 2',3'-dideoxy-ATP (ddATP) by host cellularenzymes.The metabolite, ddATP, accumulates intracellularly,where it inhibits RT and is incorporated intoviral DNA to cause chain termination in HIVinfectedcells. The potency of didanosine is 10-to 100-foldless than that of AZT with respect to antiviral activity andcytotoxicity, but the drug causes less myelosuppressionthan AZT causes.
Didanosine is recommended for the treatment of patientswith advanced HIV infection who have received prolongedtreatment with AZT but have become intolerant to, or experiencedimmunosuppression from, the drug. AZT and ddIact synergistically to inhibit HIV replication in vitro, andddI is effective against some AZT-resistant strains of HIV.Painful peripheral neuropathy (tingling, numbness, and painin the hands and feet) and pancreatitis (nausea, abdominalpain, elevated amylase) are the major dose-limiting toxicitiesof didanosine. Didanosine is given orally in the form ofbuffered chewable tablets or as a solution prepared from thepowder. Both oral dosage forms are buffered to preventacidic decomposition of ddI to hypoxanthine in the stomach.
空気と水の反応
Water soluble.
健康ハザード
SYMPTOMS: Symptoms of exposure to a related compound include cutaneous eruptions, fever, mouth sores, thrombocytopenia, neutropenia, reversible peripheral neuropathy, gastrointestinal distress, headache, nausea and vomiting.
火災危険
Flash point data for Dideoxyinosine are not available; however, Dideoxyinosine is probably combustible.
応用例(製薬)
An analog of deoxyadenosine, formulated for oral
administration.
作用機序
Didanosine (ddl) is a purine dideoxynucleoside, which is an analogue of inosine. Chemically, it is
2′,3′-dideoxyinosine, and it differs from inosine by having hydrogen atoms in place of the 2′- and
3′-hydroxyl groups on the ribose ring. Didanosine is a pro-drug that is bioactivated by metabolism to
dideoxyadenosine triphosphate, which is a competitive inhibitor of viral RT and is incorporated into the
developing viral DNA in place of deoxyladenosine triphosphate. As such, this agent causes chain
termination because of the absence of a 3′-hydroxyl group. Didanosine inhibits HIV RT and exerts a
virustatic effect on the retroviruses. Combined with ZDV, antiretroviral activity of ddI is increased.
薬物動態学
Oral absorption: c. 40%
C
max 400 mg once daily: 0.93 mg/L
Plasma half-life: c. 1.4 h
Volume of distribution: c. 1 L/kg
Plasma protein binding: <5%
Absorption
Bioavailability is reduced by about half when taken with food and the drug should be given at least 30 min before a meal. The peak plasma concentration achieved by enteric-coated tablets is less than half that of buffered tablets.
Distribution
Central nervous system (CNS) penetration is relatively poor. Median concentrations in semen (455 ng/mL; range < 50–2190 ng/mL) are greater than those in blood (<50 ng/mL; range <50–860 ng/mL). It is secreted in breast milk.
Metabolism
Based upon animal studies it is presumed that metabolism occurs by the pathways responsible for the elimination of endogenous purines by xanthine oxidase. Metabolism may be altered in patients with severe hepatic impairment; however, no specific dose adjustment is recommended.
Excretion
Renal clearance by glomerular filtration and active tubular secretion accounts for 50% of total body clearance. Urinary recovery accounts for about 20% of the oral dose in adults. The half-life increases three-fold in patients requiring dialysis. Patients with a creatinine clearance <60 mL/min may be at greater risk of toxicity.
臨床応用
Treatment of HIV infection (in combination with other antiretroviral drugs)
副作用
Most serious are pancreatitis (fatal and non-fatal), lactic
acidosis
and severe hepatomegaly with steatosis (fatal and nonfatal),
retinopathy, optic neuritis and dose-related peripheral
neuropathy. Patients with low body weight may require dose
modification. A strong association with non-cirrhotic
portal
hypertension has been described.
The combination with stavudine should be avoided in
pregnant women as fatal cases of lactic acidosis have been
reported. Caution should also be exercised in patients
with known risk factors for liver disease. Therapy should
be stopped in patients who develop clinical or laboratory
evidence of lactic acidosis or hepatotoxicity. Monitoring
lactate levels prospectively is not recommended as mild
hyperlactatemia occurs in asymptomatic patients and has a
poor positive predictive value for the development of lactic
acidosis.
Caution should be exercised in co-administering other
drugs with known neurotoxicity and in patients with a history
of neuropathy. Treatment should stop if symptoms and
signs of neuropathy are observed, but the condition is usually
reversible and patients with resolved neuropathy may be
retreated at a reduced dosage. Retinal depigmentation has
been observed in children and twice-yearly dilated retinal
examination is recommended.
代謝
Didanosine is less toxic than ZDV. The CSF fluid/plasma
ratio of ddI is 0.2. Didanosine is ultimately converted to hypoxanthine, xanthine, and uric acid through the
usual metabolic pathway for purines. The latter is a nontoxic metabolic product.
Didanosine is given in advanced HIV infection, ZDV intolerance, or significant clinical/immunologic
deterioration.
予防処置
Buffering agents that are compounded with didanosineto counteract its degradation by gastric acid mayinterfere with the absorption of other drugs that requireacidity (e.g., indinavir, delavirdine, ketoconazole, fluoroquinolones,tetracyclines, dapsone). An enteric-coatedformulation (Videx EC) that dissolves in the basic pH ofthe small intestine is not susceptible to these interactions.Ganciclovir and valganciclovir can increase bloodlevels of didanosine.The use of zalcitabine with didanosineis not recommended because that combination carriesan additive risk of peripheral neuropathy.The combinationof didanosine with stavudine increases the riskof pancreatitis, hepatotoxicity, and peripheral neuropa-thy. Stavudine should not be given with didanosine topregnant women because of the increased risk of metabolicacidosis.
2',3'-ジデオキシイノシン 上流と下流の製品情報
原材料
準備製品