Paclitaxel - Names and Identifiers
Name | Paclitaxel
|
Synonyms | taxal taxol a PACLITAXEL Paclitaxel PACLITAXOL Paclitaxelx Paclitaxel HCL PACLITAXEL, TAXUS SPECIES Paclitaxel(natural crude) PACLITAXEL, TAXUS BREVIFOLIA N-BENZYL-BETA-PHENYLISOSERINE ESTER 7,11-methano-5h-cyclodeca[3,4]benz[1,2-b]oxete benzenepropanoic acid deriv.
|
CAS | 33069-62-4
|
EINECS | 608-826-9 |
InChI | InChI=1/C47H51NO14/c1-25-31(60-43(56)36(52)35(28-16-10-7-11-17-28)48-41(54)29-18-12-8-13-19-29)23-47(57)40(61-42(55)30-20-14-9-15-21-30)38-45(6,32(51)22-33-46(38,24-58-33)62-27(3)50)39(53)37(59-26(2)49)34(25)44(47,4)5/h7-21,31-33,35-38,40,51-52,57H,22-24H2,1-6H3,(H,48,54)/t31?,32-,33+,35?,36?,37+,38?,40?,45+,46-,47+/m0/s1 |
InChIKey | RCINICONZNJXQF-MZXODVADSA-N |
Paclitaxel - Physico-chemical Properties
Molecular Formula | C47H51NO14
|
Molar Mass | 853.92 |
Density | 0.200 |
Melting Point | 213°C (dec.)(lit.) |
Boling Point | 774.66°C (rough estimate) |
Specific Rotation(α) | D20 -49° (methanol) |
Flash Point | 9℃ |
Water Solubility | 0.3mg/L(37 ºC) |
Solubility | Insoluble in water, easily soluble in chloroform, acetone and other organic solvents. |
Vapor Presure | 0mmHg at 25°C |
Appearance | White crystalline powder |
Color | white |
Maximum wavelength(λmax) | 227nm(MeOH)(lit.) |
Merck | 14,6982 |
BRN | 1420457 |
pKa | 11.90±0.20(Predicted) |
Storage Condition | 2-8°C |
Stability | Stable. Incompatible with strong oxidizing agents. Combustible. |
Refractive Index | -49 ° (C=1, MeOH) |
MDL | MFCD00869953 |
Physical and Chemical Properties | Melting Point: 213-216°C |
Use | Broad-spectrum antineoplastic plant medicine for the treatment of ovarian cancer, breast cancer and other diseases |
Paclitaxel - Risk and Safety
Hazard Symbols | Xn - Harmful
|
Risk Codes | R37/38 - Irritating to respiratory system and skin.
R41 - Risk of serious damage to eyes
R42/43 - May cause sensitization by inhalation and skin contact.
R62 - Possible risk of impaired fertility
R68 - Possible risk of irreversible effects
R40 - Limited evidence of a carcinogenic effect
R48 - Danger of serious damage to health by prolonged exposure
R20/21/22 - Harmful by inhalation, in contact with skin and if swallowed.
R68/20/21/22 -
|
Safety Description | S22 - Do not breathe dust.
S26 - In case of contact with eyes, rinse immediately with plenty of water and seek medical advice.
S36/37/39 - Wear suitable protective clothing, gloves and eye/face protection.
S45 - In case of accident or if you feel unwell, seek medical advice immediately (show the label whenever possible.)
|
UN IDs | 1544 |
WGK Germany | 3 |
RTECS | DA8340700 |
FLUKA BRAND F CODES | 10-21 |
HS Code | 29329990 |
Hazard Class | 6.1(b) |
Packing Group | III |
Toxicity | LD50 intraperitoneal in mouse: 128mg/kg |
Paclitaxel - Introduction
Open Data Unverified Data
Taxol is a monomeric diterpenoid extracted from the bark of Taxus, which is a complex secondary metabolite, it is also the only known drug that can promote the polymerization of microtubules and stabilize the polymerized microtubules. Isotopic tracing indicates that paclitaxel binds only to polymerized microtubules and does not react with unpolymerized tubulin dimers. After exposure to paclitaxel, cells accumulate a large number of microtubules in the cell. The accumulation of these microtubules interferes with the various functions of the cell, especially the cell division stops in the mitotic phase, blocks the normal division of cells. Through Ⅱ-Ⅲ clinical research, paclitaxel is mainly applied to ovarian cancer and breast cancer, and has certain curative effect on lung cancer, colorectal cancer, melanoma, head and neck cancer, lymphoma and brain tumor.
Last Update:2022-01-01 08:50:50
Paclitaxel - Indication
Open Data Unverified Data
The treatment of ovarian cancer and platinum-resistant ovarian cancer, breast cancer has a good effect on the treatment of prostate cancer, head and neck cancer, esophageal cancer, germ cell tumors, endometrial cancer, lymphoma, bladder cancer, upper gastrointestinal cancer, small cell and non-small cell lung cancer have good prospects.
Last Update:2022-01-01 08:50:51
Paclitaxel - Nature
Open Data Verified Data
The appearance was white crystalline or amorphous powder. It was first isolated from Taxus brevis by American chemist Wall et al. In1967. It can bind to tubulin and promote tubulin polymerization to assemble into microtubule dimer, thus inhibiting cell microtubule depolymerization and preventing cell rapid reproduction. Clinical trials have shown that paclitaxel has a significant effect in the treatment of metastatic ovarian cancer and breast cancer, and also has a certain effect in the treatment of small cell and non-small cell lung cancer, cervical cancer, anti-chemotherapy leukemia and so on. Taxol only exists in the genus Taxus, a total of 11 species, China has 4 species and 1 variety, they are TAXUS yunnanensis, Tibet TAXUS (also known as Himalaya), taxus chinensis, taxus chinensis var. Mairei (also known as Taxus chinensis). In addition to Taxol, these plants also contain a variety of other taxane diterpenes.
Last Update:2024-01-02 23:10:35
Paclitaxel - Preparation Method
Open Data Verified Data
There are three methods for producing paclitaxel. The first is a synthetic method, the second is a bacterial culture method, and the third is a direct separation from Taxus. Although the first two methods have achieved significant research results, they have not achieved industrialization. At present, the separation from natural or cultivated Taxus is still the main way to produce Taxol. The separation process is generally methanol or ethanol leaching (or ultra-off boundary extraction) a hexane de-esterification of dichloromethane or chloroform extraction of crude extract a multiple silica gel column chromatography preparative HPLC, TLC, HSCCC was purified and recrystallized to give the product. Since it is difficult to separate paclitaxel from another derivative Cephal omanmne by silica gel column chromatography and the product yield is low, Kingston et al. used 03 to selectively oxidize Olefinic Bonds in Cepha-lomannine molecules, and then purified paclitaxel by silica gel column chromatography. In recent years, great progress has been made in the decolorization and separation of crude extracts of Taxus chinensis by using polymer resin, which overcomes the problems of low yield, small yield, high cost and long growth cycle of the original separation methods.
Last Update:2022-01-01 11:15:24
Paclitaxel - Introduction
Pharmacological effects: Paclitaxel is mainly suitable for ovarian cancer and breast cancer. It also has a certain effect on lung cancer, colorectal cancer, melanoma, head and neck cancer, lymphoma, and brain tumor.
Last Update:2022-10-16 17:24:39
Paclitaxel - Small History
Open Data Unverified Data
- American chemists M.C. Wani and Monre E. Wall) for the first time from a large forest in the western United States called Pacific Yew (Pacific Yew) in the bark and wood isolated from the crude extract of paclitaxel. In the screening experiment of Taxus chinensis, Wani and Wall found that the crude extract of paclitaxel had high activity on rat tumor cells cultured in vitro, and began to isolate this active ingredient. Because of the extremely low content of the active ingredient in plants, it was not until 1971 that they shared with the professor of chemistry at Duke University, amkfall (andrt. Et al. The chemical structure of the active ingredient, a tetracyclic diterpene compound, was determined by x-ray analysis and named taxol.
- paclitaxel was found in Taxus chinensis in 1971, and its anticancer mechanism was found to be unique.
- in 1992, the US government transferred the patent to Bristol-Myers Squibb, and paclitaxel was launched.
- The World Anti-Cancer Drug Sales of paclitaxel in 1994.
- Paclitaxel sales hit 10 billion in 2000 (after no further increase in the supply of raw materials)
- in 2002, the central government issued a document prohibiting the felling of wild Taxus species and encouraging artificial cultivation.
- Bristol-Myers Squibb patent expired in 2004, and more pharmaceutical factories around the world involved in the production of paclitaxel.
- in 2004, Huayuan began to operate the Taxus project and set up a Taxol refining and processing plant directly under the plan, with the target of being the largest TAXUS base in China and even Asia.
- in 2005, the central government issued a new document, the national census of TAXUS resources, encourage planting.
- in 2005, this project accepted investment from individual investors.
Last Update:2022-01-01 08:50:52
Paclitaxel - Use
Open Data Verified Data
can be used for the treatment of metastatic ovarian cancer and breast cancer; Also for the treatment of small cell and non-cell lung cancer, cervical cancer, anti-chemotherapy leukemia and so on.
Last Update:2022-01-01 11:15:25
Paclitaxel - Efficient separation and purification of Taxol
Open Data Unverified Data
- This includes: a. Extraction to obtain an extract containing Taxol using TAXUS as a raw material; B. Removal of colloid to remove colloid impurities in the extract; And c. Separation and purification.
- the production process of paclitaxel is as follows: the bark of Taxus chinensis is crushed (the finer the better),85% ~ 95% alcohol (what is the ratio of material to liquid?) 35-55 ° C hot reflux extraction three times (how much time is needed each time?), 50-70 ℃ vacuum decompression concentration to heat specific gravity 1.1~1.2g/ml, chloroform extraction, extract concentration into paste, paclitaxel content 1% chloroform paste, the paclitaxel content of 1% chloroform paste and chloroform dissolved completely, and silica gel stirred evenly, cool dry, sieved, filled into the column, chloroform-methanol gradient elution, TLC detection, segment combined concentration, the semi-finished product with paclitaxel content of 5-8% was prepared. The semi-finished product with paclitaxel content of 5-8% was completely dissolved by adding acetone, mixed with silica gel, dried, sieved, and filled into the chromatography column, acetone-petroleum ether gradient elution, TLC detection, combined and concentrated, paclitaxel content of 20 ~ 25% semi-finished products, with acetone-petroleum ether system crystallization 3~4 times, Suction filtration, 50 ℃ vacuum drying under reduced pressure, the semi-finished product with paclitaxel content of 75-80% was obtained, and the product with paclitaxel content ≥ 99.5% was obtained by 16Mpa pressure chromatography, TLC detection, fractional merging and concentration, acetone-petroleum ether crystallization of target concentrate, Suction filtration and drying;
- the process of removing the colloid is as follows: the colloid is removed by high-pressure silica gel column chromatography, and the taxane compound is separated into paclitaxel, cephalomannine and 7-taxol.
Last Update:2022-01-01 08:50:52
Paclitaxel - Docetaxel
Open Data Unverified Data
docetaxel is a potent inhibitor of bone marrow activity derived from the yew tree. Blood cell and platelet counts are monitored during treatment. The mechanism of action of the drug is similar to that of paclitaxel, which inhibits the depolymerization of microtubules and inhibits cell division. Treatment of advanced or metastatic breast cancer and non-small cell lung cancer by intravenous infusion.
Last Update:2022-01-01 08:50:53
Paclitaxel - International Market Analysis
Open Data Unverified Data
- so far, there are only two kinds of paclitaxel raw materials on the international market: one is from the bark of various Taxus species; the other is to extract the "10-berry red alkali" from the branches of European ornamental Taxus, and then semi-synthesized, that is, docetaxel (docetaxel), its structure is very similar to the natural extraction of paclitaxel. These two kinds of raw materials are the best-selling raw material products in the international pharmaceutical market, and have been in short supply for a long time. According to the estimation of relevant departments, the sales volume ratio of paclitaxel and docetaxel is about 10:1.
- in the United States, Paclitaxel Injection (trade name: Paclitaxel) is mainly exclusively produced by Bristol-Myers Squibb, and there are about two or three pharmaceutical companies producing Paclitaxel raw materials and preparations, however, the market is basically a monopoly of Bristol-Myers Squibb, and the total sales of paclitaxel preparations produced by several other companies are only a fraction of Bristol-Myers Squibb. While the docetaxel drug substance and preparation are mainly produced by the French Planck Company and several companies such as the United Kingdom, Italy and so on, Planck has the largest output.
- paclitaxel is the preferred anti-tumor drug in hospitals all over the world. In recent years, the world's tumor Incidence Rate than 10 years ago has nearly doubled, lung cancer, breast cancer and ovarian cancer and other malignant tumors also showed a multiple trend, these cancer patients are the main users of paclitaxel. Overall, sales of paclitaxel will only rise, not decline, until no new plant-based anti-cancer drug can take its place.
- According to the latest figures released World Health Organization (WHO), the United States has become the world's first cancer-prone country, with 1.4 million new cancer cases each year, accounting for about 14% of the global cancer patients that year. The United States is still the largest consumer of paclitaxel. With the increase in cancer Incidence Rate in the United States, paclitaxel is the main drug against advanced malignant tumors, and it is believed that its sales volume will continue to maintain a rapid upward trend. The United States and other developed countries have already summed up a set of optimal compatibility schemes for paclitaxel and other anticancer drugs in the course of clinical use for more than ten years, the medical sector has been inseparable from the "backbone" of paclitaxel, therefore, the demand for paclitaxel raw material will also be rising.
Last Update:2022-01-01 08:50:54
Paclitaxel - Domestic situation
Open Data Unverified Data
Jiangsu Red Bean Group has invested tens of millions of yuan three or four years ago to build the largest Taxus chinensis fast-growing forest base in east China, with a total area of 7400 mu, and received high praise from the relevant departments of the United Nations and the leaders of the domestic Forestry Department. It is expected that the Red Bean Group will start production of paclitaxel raw material and injection this year, and design an annual output of 6 million paclitaxel injections. The project has passed the acceptance of the National Drug Inspection Bureau and the provincial and municipal drug administration.
In addition, China's Northeast forest area and some mountainous areas in Yunnan and Guizhou provinces are also vigorously developing TAXUS fast-growing forest cultivation techniques. In the next 3 to 5 years, these places are expected to form new TAXUS forest areas, so as to provide a valuable new source of paclitaxel raw material in China. Hunan, Hubei and other southern mountainous provinces are also building TAXUS cultivation bases, as one of the measures to help local farmers out of poverty and become rich. According to this development trend, the annual production of paclitaxel in China is expected to exceed 100 in the next few years, thus becoming the world's major producer of paclitaxel raw materials and preparations.
Last Update:2022-01-01 08:50:54
Paclitaxel - Precautions for use of injection
Open Data Unverified Data
note
- hematological toxicity: as the main factor limiting the dose increase, G-CSF should be used when the white blood cell is less than 1500/mm3, and the blood component should be transfused when the platelet is less than 30,000/mm3.
- allergic reaction: in addition to pretreatment, if only mild symptoms such as facial flushing, skin reaction, heart rate slightly faster, slightly lower blood pressure, it is not necessary to stop the drug, can slow down the drop rate. However, if there are serious reactions such as low blood pressure, angioedema, Dyspnea, General measles, should be discontinued and given appropriate treatment. Patients with severe allergies should not be treated with paclitaxel again.
- nervous system: numbness of fingers and toes was the most common. Significant sensory and motor disturbances and reduced tendon reflexes occur in about 4% of patients, particularly at high doses. There have been individual reports of grand mal seizures during instillation.
- Cardiovascular: transient tachycardia and hypotension are common and generally do not require treatment. However, in the first hour of infusion should be closely observed, in addition to serious conduction block patients do not have to be observed every hour.
- joints and muscles: about half of the patients will feel the joints 2-3 days after administration and Myalgia, which is related to the dosage used. Usually within a few days of recovery. Muscle pain is aggravated in G-CSF of patients given.
- hepatobiliary system: since most of paclitaxel is excreted from bile, patients with hepatobiliary diseases should be carefully observed. In thousands of cases, about 8% of patients had elevated bilirubin, 23% had elevated alkaline phosphatase, and 18% had elevated aspartate aminotransferase. However, there is no information that paclitaxel has serious damage to liver function.
- Other: gastrointestinal reactions are common but generally not severe, a few may have Diarrhea and mucositis. Mild alopecia is also common.
adverse reactions
- allergic reaction: the incidence rate was 39%, of which the incidence rate of severe allergic reaction was 2%. The majority of type 1 allergies, manifested as bronchial spastic Dyspnea, urticaria and hypotension. Almost all reactions occurred during the first 10 minutes after dosing.
- Myelosuppression: The main dose-limiting toxicity, manifested as neutropenia, thrombocytopenia rare, generally occurred after 8 to 10 days. The incidence of severe neutrophils was 47%, and the incidence of severe thrombocytopenia was 5%. Anemia is more common.
- neurotoxicity: the incidence of peripheral neuropathy was 62%, the most common manifestations were mild numbness and paresthesia, and the incidence of severe neurotoxicity was 6%.
- cardiovascular toxicity: there may be hypotension and asymptomatic short-term bradycardia. Muscle and joint pain: the incidence was 55%, occurred in the joints of the limbs, the incidence and severity were dose-dependent.
- gastrointestinal reaction: the incidence of Nausea, Vomit, Diarrhea and mucositis was 59%,43% and 39% respectively, generally mild and moderate.
- hepatotoxicity: ALT, elevated AST and AKP.
- alopecia: The incidence rate was 80%.
- Local reactions: inflammation in the local area of intravenous infusion of the drug and extravasation of the drug.
Last Update:2022-01-01 08:50:55
Paclitaxel - Chemical properties
Open Data Unverified Data
needle-like crystals or amorphous powders were precipitated from methanol. Melting Point 213~216 °c (decomposition). [Α] D20-49 ° (methanol). UV absorption maximum (methanol):227,273nm(& epsilon;29800,1700).
Last Update:2022-01-01 08:50:56
Paclitaxel - Production method
Open Data Unverified Data
- the content of natural products isolated and purified from the bark of yew, root of wood, leaves, shoots and seedlings was the highest in bark. TAXUS in the Chinese botanical record of the scientific name for the yew, plant classification into gymnosperm, pine, Taxus, TAXUS family, TAXUS genus. Taxaceae contains 5 genera and 23 species, and there are 4 genera and 12 species and 1 variety in China, which are Taxus wallichinanaZucc, taxus chinensis vat.Mairei) and Taxus cuspidata. Distributed in Tibet, Yunnan, Guizhou, Sichuan, Guangxi, Guangdong, Hunan, Hubei, Jiangxi, Fujian, Zhejiang, Anhui, Henan, Shanxi, Shaanxi, Gansu and Jilin mountainous areas.
- extracted from the bark or leaves of TAXUS plants. The bark or leaves of Taxus chinensis were dried in the shade, ground, and extracted with 95% ethanol. The extract was concentrated to dryness and the residue was stirred with water and dichloromethane. The organic layer was separated by standing and the aqueous layer was extracted several times with dichloromethane. The extracts and the organic layer were combined and concentrated to dryness. The residue was dissolved in ethyl acetate-methanol (3:1) and mixed with fresh celite, and the solvent was removed under reduced pressure. The remaining powder was subjected to flash column chromatography, eluting with hexane followed by dichloromethane. The latter was collected and the methylene chloride was distilled off under reduced pressure. The residue was dissolved in ethyl acetate and chromatographed on 70 sets (3-4 per set) of medium pressure flash chromatography columns filled with silica gel, eluting with hexane-acetone of different proportions. Fractions containing the product were collected and concentrated. The residue was purified by a medium pressure flash chromatography column packed with silica gel, eluting with different ratios of methanol-dichloromethane. The product-containing fractions were collected and concentrated under reduced pressure. The residue was separated by preparative high performance liquid chromatography, and the obtained product was recrystallized twice with aqueous methanol to obtain pure paclitaxel. Yield: bark 0.028%, leaves 0.0088%. Yield: bark 93.3%, leaves 88%. Melting Point: 212~214 ℃,[α] D20-49 degrees (1%, chloroform).
- the bark of Taxus chinensis was crushed, dried in the shade, and soaked with 1% citric acid aqueous solution for 24h before percolation. The permeate was extracted with dichloromethane, and the extract was dried, concentrated and vacuum-dried. Column chromatography was performed twice on silica gel, and the collected effluent contained paclitaxel and cephalomannine. Based on the difference of their side chain structure, they were dissolved in carbon tetrachloride with bromine, and only the three of the three of the bromine, and then through silica gel column chromatography, can only contain the effluent of paclitaxel, after treatment, the Taxol quality product was obtained, the content was 99.19%, the yield was 4.5 × 10-5, and the recovery was 70%.
Last Update:2022-01-01 08:50:56
Paclitaxel - Identification method
Open Data Unverified Data
a. Infrared absorption: The main absorption band in the infrared spectrum is consistent with the control.
B. HPLC identification: in the content detection, the retention time of the main peak in the chromatogram prepared by the detection is consistent with the retention time of the main peak in the standard preparation chromatogram.
Purity: 99-100%, based on dry product without water and solvent.
Related Substances: total related substances ≤ 2.0%
Organic volatile impurities: meet the requirements of the United States Pharmacopoeia (USP) and Chinese Pharmacopoeia (CP) organic volatile impurities.
Specific rotation:[α]20 D =-49.0 ° ~ 55.0 °(10mg/mL methanol solution), based on dry product without water and solvent.
Moisture: ≤ 4.0%
Residue: ≤ 0.2%.
Last Update:2022-01-01 08:50:57
Paclitaxel - Separation method
Open Data Unverified Data
step
This includes a. Extraction to obtain an extract containing Taxol using TAXUS as a raw material; B. Removal of pectin and removal of colloid impurities in the extract; And c. Separation and purification.
Process characteristics
The bark of Taxus chinensis is crushed (the finer the better),85% ~ 95% alcohol (what is the ratio of material to liquid?) 35-55 ° C hot reflux extraction three times (how much time is needed each time?), 50-70 ℃ vacuum decompression concentration to heat specific gravity 1.1~1.2g/ml, chloroform extraction, extract concentration into paste, paclitaxel content 1% chloroform paste, the paclitaxel content of 1% chloroform paste and chloroform dissolved completely, and silica gel stirred evenly, cool dry, sieved, filled into the column, chloroform-methanol gradient elution, TLC detection, segment combined concentration, the semi-finished product with paclitaxel content of 5-8% was prepared. The semi-finished product with paclitaxel content of 5-8% was completely dissolved by adding acetone, mixed with silica gel, dried, sieved, and filled into the chromatography column, acetone-petroleum ether gradient elution, TLC detection, combined and concentrated, paclitaxel content of 20 ~ 25% semi-finished products, with acetone-petroleum ether system crystallization 3~4 times, Suction filtration, 50 ℃ vacuum drying under reduced pressure, the semi-finished product with paclitaxel content of 75-80% was obtained. The product with paclitaxel content ≥ 99.5% was obtained by 16Mpa pressure chromatography, TLC detection, fractional merging and concentration.
the process of removing colloid
The high-pressure silica gel column chromatography removes the colloid, and simultaneously, the taxane compound is separated into paclitaxel, cephalomannine, and 7-epipaclitaxel 3 fractions.
side effects of slow release chemotherapy
- Clinical studies have shown that taking malt selenium to patients while using paclitaxel can help reduce cardiovascular toxicity and gastrointestinal reactions, and some cancer cells are less sensitive to paclitaxel, at this time, malt selenium can help control the killing of such cancer cells, and on the other hand, it has been proved to improve the activity of white blood cells.
- when taking chemotherapy and chemotherapy drugs at the same time, it can effectively enhance the activity of lymphokine il-12 and so on, enhance immunity, stimulate bone marrow and restore hematopoietic function of bone marrow, in addition, it can enhance the tolerance of cells to the toxicity of chemical drugs, reduce side effects and enhance the effect of chemotherapy.
- Chinese Journal of Oncology published an article by Jiao Yulian et al. "Ginsenoside Rh2 enhances paclitaxel-induced apoptosis of Hela cells" in 2006. The article pointed out: ginsenoside Rh2 can synergistically enhance the inhibitory effect of paclitaxel on the proliferation and apoptosis of H ela cells.
Last Update:2022-01-01 08:50:58
Paclitaxel - Method for Determination of content
Open Data Unverified Data
chromatographic conditions and system suitability test using eighteen alkyl silane bonded silica gel as filler; Methanol-water-acetonitrile (23:41:36) as mobile phase, the detection wavelength was 227nm. The system applicable solution 10 & micro;l under related substances shall be injected into the liquid chromatograph, and the separation degree of paclitaxel peak from paclitaxel impurity A peak and impurity B peak shall be greater than 1.0.
standard sample of paclitaxel (manufactured by Guizhou di-da), about 12mg, precision weighing, add 100ml measuring flask, add acetonitrile to dissolve and dilute to the scale, shake, 10 & micro;l was injected into the liquid chromatograph for precise measurement, and the chromatogram was recorded. According to the external standard method to calculate the peak area, that is.
This product is natural extraction or semi-synthetic preparation. This product is (2S,5R,7S,10R,13s)-10, 20-bis (acetyloxy)-2-benzoyloxy -1, 7-dihydroxy-9-oxo-5, 20-epoxytaxane -11-ene -13-YL (3S)-3-benzoylamino-3-phenyl-d-lactate. The content of C47H51NO14 shall be 98.0% ~ 102.0% calculated as dry product.
trait
- This product is white or off-white crystalline powder.
- This product is dissolved in methanol, ethanol or chloroform, slightly soluble in ether, almost insoluble in water.
- the specific rotation of this product is accurately weighed, dissolved in methanol and quantitatively diluted to prepare a solution containing 10mg per 1ml, which is determined according to law (Appendix VI E), the specific rotation was -49.0 ° to -55.0 °.
identification
- in the chromatogram under the content determination item, the main peak of the test solution should be consistent with the retention time of the main peak of the reference solution.
The infrared absorption spectrum of - paclitaxel should be consistent with that of the control (Spectrum set 875).
examination
- the clarity and color of the solution take this product 0.1g, add methanol 10ml to dissolve, the solution should be clear and colorless.
- Related substances take this product and add acetonitrile to make a solution containing about 0.5mg per 1ml as a test solution, add acetonitrile diluted to each 1ml containing about 2.5 & micro;g, 0.5 & micro;g of the solution, as control solution (1) and control solution (2); Take paclitaxel, paclitaxel impurity A (taxotraline) and paclitaxel impurity B(7-Table 10-deacetylpaclitaxel) control appropriate amounts, dissolved in acetonitrile and diluted to prepare paclitaxel containing about 0.5mg per 1ml, paclitaxel impurity A and paclitaxel impurity B were both 2.5 & micro;g solutions, as the system suitability solution. As determined by high performance liquid chromatography (Appendix V D), silica gel bonded with eighteen alkyl silanes is filled with
Last Update:2022-01-01 08:50:58
Paclitaxel - Pharmacological action
Open Data Unverified Data
- microtubules are a component of eukaryotic cells that are formed from microtubule dimers composed of two similar polypeptide (a and p) subunits. Under normal conditions, there is a dynamic equilibrium between microtubules and tubulin dimers. Paclitaxel can make the loss of this dynamic balance between the two, induce and promote tubulin polymerization, prevent depolymerization, and stabilize microtubules. These effects result in the inability of the cells to form spindles and spindles during mitosis, inhibit cell division and proliferation, and thereby exert an antitumor effect.
- in vitro studies have shown that paclitaxel binds reversibly to microtubules, especially to the P subunit of N-terminal tubulin, this action reduces the concentration of tubulin required for polymerization, shifts the dynamic equilibrium towards microtubule assembly, and increases the rate and yield of microtubule polymerization. The microtubules induced by paclitaxel were shorter and were about ten times more flexible than the microtubules normally formed without paclitaxel. Paclitaxel binds to microtubules in a 1:1 ratio, indicating that the drug has only one binding site on the microtubules. In addition, paclitaxel inhibits the normal dynamic regeneration of the micro-network necessary for mitosis, prevents the formation of normal mitotic spindles, causes the breakage of chromosomes, and inhibits the replication of cells. 1.5~5.(Vg/L paclitaxel was incubated with CHO and A2780 ovarian cancer cell lines for 24 h,99% of the cells died, and 57% of the cells entered the human Division phase, and extensive nuclear damage occurred. Paclitaxel alters the mitotic process of cells, increasing mitotic duration from 0-5 h to 15 h, and inhibits cytoplasmic division, resulting in the formation of multinucleated cells. These multinucleate cells continue to revert to the & phase and then attempt to undergo mitosis again, but there are no resting cells in mitosis. Micronuclei are also observed in many cells. Inhibition of spindle formation appears to be associated with this abnormal mitosis. In vitro, low concentration of paclitaxel (less than 8. 5 pg/L) blocked the transition from the middle to the late phase of the cell cycle and prevented cell proliferation without increasing the amount of microtubule polymers or forming microtubule spindles. Paclitaxel inhibits cell proliferation to a degree that parallels that of blocking metaphase of cell division. Higher concentrations of paclitaxel (greater than 8.5 fig/L) increased the amount of microtubule multimers at 282 pg/L, 500% higher than control levels, and resulted in the formation of large spindle microtubules. Leukemic cells were incubated with paclitaxel at a concentration of 85 pg/L or greater for 24 h to shrink 40% of the cells and concentrate the chromosomes.
Last Update:2022-01-01 08:50:59