Overview Pharmacological effects Clinical evaluation Adverse reactions Chemical properties Application
ChemicalBook > CAS DataBase List > Vinorelbine tartrate

Vinorelbine tartrate

Overview Pharmacological effects Clinical evaluation Adverse reactions Chemical properties Application
Vinorelbine tartrate Structure
Vinorelbine tartrate
  • CAS No.125317-39-7
  • Chemical Name:Vinorelbine tartrate
  • CBNumber:CB8761554
  • Molecular Formula:C53H66N4O20
  • Formula Weight:1079.11
  • MOL File:125317-39-7.mol
Vinorelbine tartrate Property
Safety
  • Hazard Codes  :Xi
  • Risk Statements  :43
  • Safety Statements  :26-36
  • RIDADR  :UN 1544PSN1 6.1 / PGII
  • WGK Germany  :3
  • HS Code  :29339900
  • NFPA 704:
    0
    2 0
Hazard and Precautionary Statements (GHS)
  • Symbol(GHS)
  • Signal wordWarning
  • Hazard statements H317
  • Precautionary statements P280
Vinorelbine tartrate Price More Price(2)
  • Brand: Sigma-Aldrich(India)
  • Product number: V2264
  • Product name : Vinorelbine ditartrate salt hydrate
  • Purity: ≥98% (HPLC), powder
  • Packaging: 5MG
  • Price: ₹11268.83
  • Updated: 2022/06/14
  • Buy: Buy
  • Brand: Sigma-Aldrich(India)
  • Product number: PHR3160
  • Product name : Vinorelbine Tartrate
  • Purity: pharmaceutical secondary standard, certified reference material
  • Packaging: 500MG
  • Price: ₹86307.73
  • Updated: 2022/06/14
  • Buy: Buy

Vinorelbine tartrate Chemical Properties,Usage,Production

  • Overview Vinorelbine belongs to vinblastine derivatives, its action is similar to vincristine. It is first marketed in 1989 in France. The main role is to combine tubulin, consequently, it causes microtubule formation disorder during cells mitosis.
    Vinorelbine belongs to cycle specific drugs, it is used clinically in the treatment of non-small cell lung cancer (NSCLC) and breast cancer, ovarian cancer, head and neck squamous cell carcinoma, leukemia. In addition,it also has a strong inhibitory effect on small cell lung cancer, colon cancer, brain tumors, malignant melanoma.
  • Pharmacological effects Vinorelbine tartrate is the tartrate form of vinorelbine ,it is a semi-synthetic  vincristine compound, it belongs to M phase specific drugs, mechanism of action is similar to vincristine . Mainly it , by selectively blocking mitotic cell tubulin polymerization to form microtubule and  inducing tubulin depolymerization , impedes spindle microtubules,and it makes cell division stop  in the middle, and it has few effect on the synthetic tubulin in the shaft of nerve cells. Since NVB affinity for axonal microtubules is poor, only when there is a high concentration of it ,it has effect on axonal , so it has the lower neurotoxicity than other vincristine drugs,and it  has a greater therapeutic index. Human pharmacokinetics of vinorelbine show that after intravenous administration there is a three-compartment model, the volume  of distribution is large , PPB is up to 50% to 80%, plasma clearance rate is high, the terminal elimination phase T1/2 is 40 h, it has a rapid tissue distribution, concentration in tissues is significantly higher than vincristine (VCR), vindesine (VDS). Plasma clearance is 0.8 L/(kg • h),it is mainly through biliary secretion, and it is excreted with the feces, urine excretion accounts for 10% to 15%.It has a higher efficacy and less adverse reactions of the nervous system.
  • Clinical evaluation Numerous clinical studies have shown that vinorelbine is one of the most effective drugs for the treatment of non-small cell lung cancer and breast cancer, single agent response rate is 14% to 35% and 30% to 60% respectively. And DDP combination chemotherapy in NSCLC and with doxorubicin combination therapy of breast cancer, efficiency is up to 30% to 50% and 50% to 77%, respectively. It has a good effect on ovarian cancer, malignant lymphoma, head and neck cancer, esophageal cancer.
  • Adverse reactions
    • Vinorelbine hematologic toxicity is dose-limiting , mainly it is neutropenia, which mostly restore  within 7d, it has a certain influence on red blood cells , thrombocytopenia and anemia incidence is less than 2%.
    • Neurotoxicity mainly performs as tendon reflexes (about 25%), occasional paresthesia, few patients may have gastrointestinal autonomic nerve paralysis induced constipation (17%~41%),  paralytic ileus is rare  , 2% 6% of the patients suffer finger (toe) numb, but the incidence is much lower than the VCR and VDS.
    • Incidence of gastrointestinal side effects is less than 10%. Occasionally, nausea, vomiting, dyspnea, and bronchospasm, often occur in a few minutes or several hours after treatment . Alopecia incidence is less than 10%.
    • Vinorelbine drug extravasation into the surrounding tissue can cause burning, injection site phlebitis, local tissue necrosis, ulceration, cellulitis.
    • Myelosuppression is dose-limiting toxicity. 3 to 5 days after the medication, transient myelosuppression can occur, usually it can recover within 10 days, attention should be paid to prevent infection. Neurotoxicity is visible.
  • Chemical properties White or almost white powder or crystalline powder, odorless.
  • Application Antineoplastic agents
  • Chemical Properties Pale Yellow Powder
  • Uses Vinorelbine Bitartrate is an antineoplastic.
  • Definition ChEBI: The L-(+)-tartrate salt of vinorelbine.
  • brand name Navelbine (Pierre).
  • General Description Vinorelbine ditartrate is available in 1- and 5-mL vials at aconcentration of 10 mg/mL for IV use. It is FDA approvedfor the treatment of NSCLC. The agent has also been usedin treating metastatic breast cancer, cervical cancer, uterinecancer, and lung cancer especially in older patients or thosewith physical difficulties. Vinorelbine is the most lipophilicof the vinca alkaloids because of modifications of thecatharanthine ring system and dehydration of the piperidinering. This allows the agent to be quickly taken up into cellsincluding lung tissue where concentrations are 300-foldhigher than plasma concentrations. This is 3 to 13 timeshigher than the lung concentrations seen with vincristine.The agent is highly protein bound (80%–91%) and metabolizedby CYP3A. The major metabolite seen is the 4-Odesacetylderivative, which is equally active with the parentbut only formed in small quantities. The agent is eliminatedprimarily (33%–88%) in the bile with some appearing inthe urine (16%–30%). The elimination half-life is 27 to43 hours. The toxicities seen for vinorelbine includemyelosuppression, which is dose limiting but ceases upondiscontinuation of drug. This is most commonly seen as aneutropenia, and patient’s neutrophil count should be monitoredprior to and during therapy to decrease the chanceof infection. Additional toxicities include nausea/vomiting,elevation of liver function tests, alopecia, generalized fatigue,and inappropriate secretion of antidiuretic hormone.Neurotoxicity is seen with vinorelbine but occurs to a lesserdegree compared with other vinca alkaloids because of itsdecreased affinity for axonal microtubules.
  • Biological Activity Selective mitotic microtubule antagonist that exhibits > 20 fold selectivity over axonal microtubules. Inhibits proliferation of multiple human tumor cell lines (IC 50 = 1.25 nM in HeLa cells) and blocks metaphase/anaphase transition by suppression of microtubule dynamics (IC 50 = 3.8 nM). Reduces spindle length by 29% and inhibits microtubule polymerization at micromolar concentrations.
  • Biochem/physiol Actions Vinorelbine is a potent anti-mitotic, anti-tumor agent. Vinorelbine inhibits microtubule assembly. Low neurotoxicity is related to its higher affinity for mitotic microtubules than for axonal microtubules.
Vinorelbine tartrate Preparation Products And Raw materials
Raw materials
Preparation Products
Vinorelbine tartrate Suppliers
Global(544)Suppliers
  • Supplier:
    career henan chemical co
  • Tel:+86-0371-86658258<br/>+8613203830695
  • Email:sales@coreychem.com
  • Country:China
  • ProdList:29859
  • Advantage:58
Vinorelbine tartrate Spectrum
125317-39-7, Vinorelbine tartrateRelated Search:
  • VINORELBINE TARTRATE
  • APIs
  • Anti-cancer & immunity
  • Inhibitors
  • Antineoplastic
  • standardized herbal extract
  • reference standards from Chinese medicinal herbs (TCM).
  • phytochemical
  • pharmaceutical intermediate
  • chemical reagent
  • Pharmaceuticals
  • Intermediates & Fine Chemicals
  • 生物碱类
  • 抑制剂
  • 药靶配体
  • 原料
  • 试剂
  • 化学试剂
  • 原料药
  • 医药原料
  • 有机中间体
  • 标准品 -中药标准品
  • 分析试剂-对照品
  • 标准品-中药标准品
  • 医用原料
  • 优势产品
  • 分析试剂标准品
  • 医药原料
  • 细胞生物学试剂
  • 小分子抑制剂,天然产物
  • 对照品,标准品
  • 标准品
  • 中药对照品
  • 细胞生物学
  • 生物活性小分子
  • 医药中间体
  • 植物提取物
  • TABINES他宾类产品(Anti-cancer)
  • 抗肿瘤药
  • 细胞信号和神经生物学
  • 医药原料药
  • Cytoskeleton and Extracellular Matrix
  • Microtobule Inhibitors
  • BioChemical
  • Cell Signaling and Neuroscience
  • Cell Biology
  • C45H54N4O82C4H6O6
  • C45H54N4O8H2O
  • C45H54N4O82C4H6O8
  • C53H66N4O20
  • C45H54N4O82C4H6O6C53H66N4O20
  • C45H54N4O82C4H6O6C
  • C49H60N4O14
  • 酒石酸长春瑞滨,10 MM DMSO 溶液
  • VINORELBINE TARTRATE (NAVELBINE),MITOTIC MICROTUBULE拮抗剂
  • 酒石酸长春瑞滨/生物碱
  • 酒石酸长春瑞滨/D1A
  • (3AR,3A1R,4R,5S,5AR,10BR)-4-乙酰氧基-3A-乙基-9-((8R)-4-乙基-8-(甲氧基羰基)-1,3,6,7,8,9-六氢-2,6-METHANOAZECINO[4,3-B]吲哚-8-基)-5-羟基-8-甲氧基-6-甲基-3A,3A1,4,5,5A,6,11,12-八氢-1H-吲哚嗪并[8,1-CD]咔唑-5-甲酸甲酯 双((2R,3R)-2,3-二羟基琥珀酸盐)

Home

My