Cancer Drug Classes The classes of drugs currently used in the cancer clinic are  1. DNA Binding Agents (intercalating and alkylating.

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Presentation transcript:

Cancer Drug Classes The classes of drugs currently used in the cancer clinic are  1. DNA Binding Agents (intercalating and alkylating agents) Mitotic Spindle Inhibitors (modulators of tubulin polymerisation) Antimetabolites (anti-folates, pyrimidine and purine analogues) Hormones and Hormone Antagonists Miscellaneous anticancer drugs

DNA binding agents Intercalating agents Intercalating agents are flat planar aromatic compounds that insert themselves in between the DNA basepairs.   They either inhibit RNA polymerase activity but not DNA polymerase or exert their action as cancer drugs by poison the activity of topoisomerase II. Clinically used intercalating agents include ANTHRACYCLINES , MITOXANTRONE, ACTINOMYCIN D and Bleomycin

Anthracyclines are the most commonly used anticancer drug, Doxorubicin (adriamycin) having activity against a wide range of solid tumours. (Most common drug) Daunorubicin (daunomycin) being used against acute myeloid leukemia (AML) Idarubicin is a semisynthetic anthracycline that took Daunorubicin place in AML therapy. Epirubicin doxorubicin analogue used in metastatic breast cancer and gastric cancer

Anthracyclines DNA strand scission via effects on Top II enzyme (topoisomerase poisons) High-affinity binding to DNA through intercalation, resulting in blockade of DNA and RNA synthesis. Binding to membranes and altering fluidity Generation of the free radical and oxygen radicals

Anthracyclin Their main toxicities are - Bone marrow depression - Total alopecia BUT the anthracyclines have a strange dose-limiting irreversible and lethal cardiomyopathy. This cardiotoxicity may be a result of the generation of free radicals and lipid peroxidase.   HOW TO REDUCE THIS ..............

Mitoxantrone Treats pediatric and adult acute myeloid leukemia, non-Hodgkin’s lymphomas, and breast cancer. Prostate cancer ??? poisons the activity of topoisomerase II. And ........ Myelosuppression is the main side effect. Causes cardiac toxicity . Blue discoloration of finger nails for 1 – 2 days after treatments.

Actinomycin D Actinomycin is a very potent inhibitor of RNA polymerase. Does intercalate in the minor groove of the double helix. In the cancer clinic it finds use against special tumours, particularly Wilm’s tumour which is a cancer of the kidney in children (in combination with vincristine). It is also combine with methotrexate in the treatment of gestational choriocarcinoma. Its toxicities are bone marrow and gut suppression.

Actinomycin-DNA Complex

Bleomycin bleomycin intercalates DNA, the major cytotoxicity is believed to result from iron catalyzed free radical formation and DNA strand breakage. It is useful in Hodgkin’s and non-Hodgkin’s lymphomas, testicular cancer, and several other solid tumors. Adverse Effects: Bleomycin produces very little myelosuppression. The most serious toxicities of Bleomycin are pulmonary and mucocutaneous reactions.

Alkylating Agents Nitrogen Mustards Ethylenimines Nitrosoureas Alkyl Sulfonates Cyclophosphamide Thiotepa Busulfan Carmustine CCNS

Alkylating Agents Alkylating agents bind irreversibly to DNA and function by crosslinking the two Watson-Crick strands, thereby inhibiting strand separation and preventing DNA replication.

Nitrogen mustards Cyclophosphamide (oral) Ifosfamide Melphalan (oral) Chlorambucil (oral) least toxic

Nitrogen mustards cyclophosphamide most commonly used alkylating agent used in lymphomas, leukemias, sarcomas, carcinomas of breast or ovary, as well as childhood malignancies. 2. has a special place in the maintenance therapy for breast cancer. 3. It is also a potent immunosuppressant, it is used in the management of rheumatoid disorders and autoimmune nephritis. 4. Cystitis (inflammation of the urinary bladder) may result. co-administered with N-acetylcystein or 2-mercaptoethanesulfonate (mesna). Both are thiols that neutralized acrolein

Nitrosoureas The best known clinical agents are CARMUSTINE and LOMUSTINE (oral). The nitrosoureas pass the blood-brain barrier and are active against brain tumours. These drugs appear to be non-cross-resistant with other alkylating agents. Streptozocin (minimal bone marrow toxicity) used to treat insulin-secreting islet cell carcinoma of the pancreas

Platinum analogs In the clinic, cisplatin behaves very similarly to the organic alkylating agents and finds widespread use. Cisplatin has efficacy against a wide range of neoplasms. It is particularly effective in germ cell tumours (testicular cancer and ovarian tumours) and in breast cancer. Its use in combination chemotherapy has revolutionised the treatment of testicular and ovarian tumours, frequently leading to complete cure of testicular cancers in young men.

Platinum analogs Its main toxicities are to the kidney and to the ear, produces relatively little myelosuppression but can cause severe nausea, vomiting. Carboplatin is a second generation platinum analog that has less renal toxicity and gastrointestinal toxicity. Though Carboplatin has widely replace cisplatin in chemotherapeutic regimen.

Alkylating Agents therapeutic Uses Thiotepa – ovarian cancer Busulfan (oral) – chronic myeloid leukemia is linked with pulmonary fibrosis, adrenal insuffeciency and skin pigmentation

Resistance to Alkylating agents Cells become resistant to alkylating agents by 1. REPAIR OF DNA LESIONS  Alkylating agents and platinum-based agents -resistant cells up-regulate the repair systems. 2. CHEMICAL INACTIVATION OF DRUGS  DNA alkylating and platinating agents are chemically reactive, particularly reactive towards -SH groups and, accordingly, tumour cells can become resistant by up-regulating their thiol content (glutathione).