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Vincristin

Several of the naturally occurring indoles also have clinical importance. The dimeric vinca alkaloid vincristine and closely related compounds were among the first of the anti-mitotic class of chemotherapeutic agents for cancer[14]. The mitomycins[15] and derivatives of ellipticine[16] are other examples of compounds having anti-tumour activity. Reserpine, while not now a major drug, was one of the first compounds to show beneficial effects in treatment of mental disorders[17]... [Pg.2]

Until separation techniques such as chromatography (28,29) and counter-current extraction had advanced sufficientiy to be of widespread use, the principal alkaloids were isolated from plant extracts and the minor constituents were either discarded or remained uninvestigated. With the advent of, first, column, then preparative thin layer, and now high pressure Hquid chromatography, even very low concentrations of materials of physiological significance can be obtained in commercial quantities. The alkaloid leurocristine (vincristine, 22, R = CHO), one of the more than 90 alkaloids found in Catharanthus roseus G. Don, from which it is isolated and then used in chemotherapy, occurs in concentrations of about 2 mg/100 kg of plant material. [Pg.533]

The influences of herbicides on cell division fall into two classes, ie, dismption of the mitotic sequence and inhibition of mitotic entry from interphase (G, S, G2). If ceU-cycle analyses indicate increases in abnormal mitotic figures, combined with decreases in one or more of the normal mitotic stages, the effect is upon mitosis. Mitotic effects usually involve the microtubules of the spindle apparatus in the form of spindle depolymerization, blocked tubulin synthesis, or inhibited microtubule polymerization (163). Alkaloids such as colchicine [64-86-8J,viahla.stiae [865-21-4] and vincristine [57-22-7] dismpt microtubule function (164). Colchicine prevents microtubule formation and promotes disassembly of those already present. Vinblastine and vincristine also bind to free tubulin molecules, precipitating crystalline tubulin in the cytoplasm. The capacities of these dmgs to interfere with mitotic spindles, blocking cell division, makes them useful in cancer treatment. [Pg.46]

Chemotherapeutic agents are grouped by cytotoxic mechanism. The alkylating agents, such as cyclophosphamide [50-18-0] and melphalan [148-82-3] interfere with normal cellular activity by alkylation deoxyribonucleic acid (DNA). Antimetabohtes, interfering with complex metaboHc pathways in the cell, include methotrexate [59-05-2] 5-fluorouracil [51-21-8] and cytosine arabinoside hydrochloride [69-74-9]. Antibiotics such as bleomycin [11056-06-7] and doxombicin [23214-92-8] h.a.ve been used, as have the plant alkaloids vincristine [57-22-7] and vinblastine [865-21-4]. [Pg.406]

Dactinomycin is useful against several tumors especially Wilms tumor of the kidney and rhabdomyosarcoma. Wilms tumor normally requires a combination of surgery, x-ray irradiation, and dactinomycin plus vincristine [57-22-7] or other antitumor agents. Resistance of the multidmg... [Pg.157]

Cumulative organ toxicity also presents a significant obstacle for effective chemotherapy. In many cases, the severity of the toxicity impedes the broader use of an agent. Other specific toxicities are associated with specific agents, for example cardiotoxicity with adriamycin (32), renal toxicity with i7j -platinum (28), and neurotoxicity with vincristine (49). [Pg.444]

The alkaloid mixture from the extraction of Vinca rosea plants (as in vinblastine extraction) was chromatographed to give vincristine which was then converted to the sulfate, according to U.S. Patent 3,205,220. [Pg.1584]

Vincristine may also be prepared in a semisynthetic process starting from vinblastine. Vinblastine or a salt thereof, preferably the sulfate, is oxidized with chromic acid or with one of its salts at a low temperature, the reaction mixture is neutralized or rendered alkaline and the product is separated therefrom by extraction, the extract is evaporated to dryness, the dry residue is optionally formylated, vincristine, and optionally N-demethylvinblastine also, are Isolated from the product, and the product(s) are optionally converted into their salts preferably into the sulfates, according to U.S. Patent 3,899,493. [Pg.1584]

Phentermine HCI Vinblastine sulfate Vincristine sulfate Benzene sulfonyl chloride Glybuzole Glymidine Tranilast... [Pg.1615]

MRP1 (ABCC1) Glucuronides and sulfate conjugates of steroid hormones and bile salts, colchicine, doxorubicin, daunorubicin, epirubicin, folate, irinotecan, methotrexate, pacitaxel, vinblastine, vincristine, and others... [Pg.7]

Nitrogen mustard is clinically used for the treatment of lymphomas and some forms of lung cancer. The major indication for mechlorethamine is Hodgkin s disease as a part of the MOPP regimen (mechlorethamine + vincristine (oncovin) + procarbazine + prednisone). The usual dose consists of 6 mg/m2 on days 1 and 8. This drug has pronounced hematological toxicity (myelo-suppression). [Pg.54]

Vinca alkaloids (vincristine, vinblastine, vindesine) are derived from the periwinkle plant (Vinca rosea), they bind to tubulin and inhibit its polymerization into microtubules and spindle formation, thus producing metaphase arrest. They are cell cycle specific and interfere also with other cellular activities that involve microtubules, such as leukocyte phagocytosis, chemotaxis, and axonal transport in neurons. Vincristine is mainly neurotoxic and mildly hematotoxic, vinblastine is myelosuppressive with veiy low neurotoxicity whereas vindesine has both, moderate myelotoxicity and neurotoxicity. [Pg.155]

Vinca alkaloids are derived from the Madagascar periwinkle plant, Catharanthus roseus. The main alkaloids are vincristine, vinblastine and vindesine. Vinca alkaloids are cell-cycle-specific agents and block cells in mitosis. This cellular activity is due to their ability to bind specifically to tubulin and to block the ability of the protein to polymerize into microtubules. This prevents spindle formation in mitosing cells and causes arrest at metaphase. Vinca alkaloids also inhibit other cellular activities that involve microtubules, such as leukocyte phagocytosis and chemotaxis as well as axonal transport in neurons. Side effects of the vinca alkaloids such as their neurotoxicity may be due to disruption of these functions. [Pg.1283]

Mitotic inhibitors (antimitotics) interfere with or stop cell division. Examples of mitotic inhibitors include paclitaxel (Taxol) and vincristine (Oncovin). [Pg.592]


See other pages where Vincristin is mentioned: [Pg.1053]    [Pg.1053]    [Pg.551]    [Pg.557]    [Pg.88]    [Pg.492]    [Pg.492]    [Pg.158]    [Pg.440]    [Pg.441]    [Pg.446]    [Pg.921]    [Pg.58]    [Pg.574]    [Pg.401]    [Pg.538]    [Pg.538]    [Pg.1584]    [Pg.1584]    [Pg.1584]    [Pg.1608]    [Pg.1687]    [Pg.1711]    [Pg.1712]    [Pg.1725]    [Pg.1729]    [Pg.1755]    [Pg.416]    [Pg.460]    [Pg.638]    [Pg.751]    [Pg.1274]    [Pg.361]    [Pg.586]   
See also in sourсe #XX -- [ Pg.16 ]




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Anticancer drugs vincristine

Aprepitant Vincristine

Asparaginase Vincristine

Atta-ur-Rahman synthesis of vincristine

Benzene Vincristine sulfate

Cancer therapy vincristine

Cancer vincristine

Catharanthine vincristine from

Catharanthus alkaloids Vincristine

Catharanthus roseus vincristine from

Choriocarcinoma vincristine for

Convulsion vincristine

Effects of Vincristine on the CNS

Effects of Vincristine on the PNS

Hodgkin s disease vincristine for

Hormonal) Vincristine

Hypotension vincristine

Isoniazid Vincristine

Kuehne s synthesis of vincristine

Kutney s synthesis of vincristine

Liposomes with vincristine

Look up the names of both individual drugs and their drug groups to access full information Vincristine

MOPP regimen vincristine

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Vincristine first synthesis

Vincristine from Catharanthus

Vincristine from Vinca rosea

Vincristine from vinblastine

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Vincristine in lung cancer

Vincristine interactions

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Vincristine methiodide

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Vincristine oxidation

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Vincristine roseus

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Vincristine structure

Vincristine sulfate

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Vincristine synthetic approaches

Vincristine toxicity

Vincristine transport mechanism

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Vincristine with dactinomycin

Vincristine with itraconazole

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Vincristine, biosynthesis

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