Chemotherapeutic Agents

Lecture 17 by Dr.Alaa Fadhil Alwan
            Chemotherapeutic Agents

Antineoplastic drugs are classified according to their mode of action and the 
phase of the cell cycle in which the drug is active. This classification is not 
absolute; it is likely that more than one mechanism is involved. Multiple 
intracellular sites might be implicated and not confined to specific cycle 
events. However, it is always the rapidly dividing cells that are most sensitive 
to these drugs. Chemotherapeutic drugs that are most effective during a 
particular phase of the cycle are known as cell cycle–specific drugs.
CELL CYCLE–SPECIFIC AGENTS: ANTIMETABOLITES, VINCA 
ALKALOIDS, EPIPODOPHYLLOTOXINS, TAXANES
1. Antimetabolites
Antimetabolites are synthetically formulated to mimic the naturally produced
Metabolites, purines, pyrimidines, or folates essential for the synthesis of 
nucleic acids and DNA. This results in cell death. They exert their effects 
during the S phase of the cell life cycle and are most effective against tumors 
that have a high growth fraction. Example of chemotherapy with major side 
effect

Cytosine arabinoside: 

Myelosuppression, neurotoxicity (at higher doses and in older 

patients’ severe cerebellar syndrome, other neurologic disturbances

Deoxycoformycin: 

Myelosuppression, infection, nausea, hepatic and renal toxicity, rash

6-Mercaptopurine

: Nausea, myelosuppression, liver toxicity (cholestasis), fever, skin rash

Methotrexate

: Myelosuppression, severe mucositis (dose dependent), skin rash, acute          

encephalopathy, arachnoiditis with intrathecal administration

Fludarabine: Myelosuppression

, neurotoxicity (encephalopathy at high doses), protracted 

immunosuppression, fatigue, and somnolence

Thioguanine

: Myelosuppression, some nausea, diarrhea, cholestasis

2. Mitotic Inhibitors
Mitotic inhibitors interfere with the formation of the mitotic spindle, causing
Metaphase arrest. They are primarily known as M-phase active. These drugs 
are the vinca alkaloids, and the epipodophyllotoxins.
asters.
3. VINCA ALKALOIDS                       EPIPODOPHYLLOTOXINS         
Vinblastine  

neurotoxicity

                      Etoposide  

Bone marrow depression

Vincristine                                          Teniposide                       
Vindesine
Vinorelbine

CELL CYCLE–NONSPECIFIC AGENTS: ALKYLATING AGENTS,
NITROSOUREAS, ANTITUMOR ANTIBIOTICS, HORMONES, HORMONE
ANTAGONISTS
Antineoplastic agents that are effective through all phases of the cell cycle 
and are not limited to a specific phase are called cell cycle–nonspecific drugs. 
These drugs directly affect the DNA molecule and display no specificity for 
cells that are dividing. They are considered more toxic than their cell cycle–

specific counterparts because their destructive action does not differentiate 
between normal and malignant cycling cells. Their toxicities are felt 
throughout the cell cycle. Non-specific agents are given in bolus doses 
because they cause death independently of the proliferative state of the cell. 
These agents also reduce the number of cells that make up a tumor, which is 
known as the tumor burden.

1. Alkylating Agents
Alkylating agents alter DNA structure through the poorly understood process 
of alkylation (H

+ 

ion alkyl substitution), which results in cross-linking and 

strand breaking of DNA and destruction of its template. Destruction of the 
DNA genetic template terminates replication of the information needed for 
cellular division and leads to cell lysis. The alkylating agents are described as 
radiomimetic because they mimic the actions of radiation therapy on the cells. 
The alkylating agents are as follows:

Busulfan: 

Severe pancytopenia, skin hyperpigmentation

Carboplatin: 

BM suppression

Melphalan: 

stem cell injury

Chlorambucil: 

Leukopenia

Cisplatin: Severe

 nausea/vomiting

Cyclophosphamide and Ifosfamide 

: hemorrhagic cystitis

Dacarbazine:

 Severe nausea/vomiting

2. Nitrosoureas
Nitrosoureas are alkylating agents that also destroy DNA so that synthesis 
can no longer occur, but they are unique in that they are lipid-soluble and 
cross the blood–brain barrier into the central nervous system. The 
nitrosoureas are:
Carmustine and Lomustine:

 Prolonged myelosuppression, cumulative lung toxicity

3. Antitumor Antibiotics
Most antitumor antibiotics are isolated from fermented broths of various 
Streptomyces bacteria. The focal point of their cytotoxicity is the DNA. These 
drugs interfere with DNA-directed RNA synthesis by intercalating between the 
base pairs of DNA and generating toxic oxygen-free radicals, causing single- 
or double-stranded DNA breaks. The antitumor antibiotics are as follows:

Dactinomycin 
Mitomycin-C
Daunorubicin

         all these cause cardiotoxicity

Mitoxantrone
Doxorubicin 
Idarubicin

Hormones and Hormone Antagonists
Hormones and hormone antagonists (antihormones) are a diverse group of 
drugs that are beneficial in cancer therapy. Some hormones alter the cellular 
environment and affect the permeability of the cell membrane in ways that will 
affect cell growth. These drugs, which are hormonal or hormone-like agents, 

inhibit tumor proliferation by blocking or antagonizing the naturally occurring 
substance that stimulates tumor growth.

Androgens: testosterone proprionate, methyltestosterone,
Antiandrogens: flutamide
Antiestrogens: tamoxifen
Aromatase inhibitors: aminoglutethimide
Estrogens: diethylstilbestrol, estradiol
Glucocorticoids: prednisone, hydrocortisone, dexamethasone
Gonadotropin inhibitors: leuprolide, goserelin
Progestins: megestrol acetate

MISCELLANEOUS AGENTS
Bleomycin

: Pulmonary toxicity

Hydroxyurea:

 mild myelosuppression; some gastrointestinal toxicity; pigmentation

L

-asparaginase:

 Hypersensitivity, fever, bronchospasm, hyperglycemia

Procarbazine

: Myelosuppression

Imatinib (Gleevec)
ROUTE OF ADMINISTRATION: Oral
DRUG CLASS: Tyrosine kinase inhibitor
MECHANISM OF ACTION: Inhibition of BCR-ABL tyrosine kinase induces apoptosis
INDICATIONS: CML, gastrointestinal stromal tumors (GIST)
SIDE EFFECTS: Nausea/vomiting/diarrhea, fluid retention, muscle cramps, hemorrhage, 
musculoskeletal pain, skin rash, headache, fatigue.

Thalidomide (Thalomid)
ROUTE OF ADMINISTRATION: Oral
DRUG CLASS: Immunomodulatory agent
MECHANISM OF ACTION: Suppress excess tumor necrosis factor-

 and vascular 

endothelial growth factor-inhibiting angiogenesis.
INDICATIONS: Multiple myeloma, myelodysplastic syndrome
SIDE EFFECTS: Somnolence, rash, headache, neutropenia
COMMENT: Because of teratogenic risk, patient must be registered in distribution 
monitoring program.

Rituximab (Rituxan)
ROUTE OF ADMINISTRATION: Intravenous injection
DRUG CLASS: Monoclonal antibody
MECHANISM OF ACTION: Antibody directed against CD20 antigen, which arrests
Cell cycle initiation, compliment dependent cytotoxicity.
INDICATIONS: Refractory B-cell lymphoma, CD20-positive NHLs
SIDE EFFECTS: Headache, chills, rigors, nausea, hypotension, rash

Tretinoin (Vesanoid, all-trans retinoic acid, ATRA)
ROUTE OF ADMINISTRATION: Oral

DRUG CLASS: Vitamin A derivative
MECHANISM OF ACTION: Inhibits clonal proliferation and/or granulocyte differentiation
INDICATIONS: APL
SIDE EFFECTS: Arrhythmia, hypotension, peripheral edema, headache, fever, rash,
Nausea/vomiting, abdominal pain, retinoic acid syndrome, myelosuppression, diaphoresis

Bortizomib (Velcade)
ROUTE OF ADMINISTRATION: Intravenous injection
DRUG CLASS: Proteasome inhibitor
MECHANISM OF ACTION: Reversibly inhibits chymotrypsin-like activity at the 26S 
proteasome leading to cell-cycle arrest and apoptosis.
INDICATIONS: Multiple myeloma patients who have received at least one prior therapy
SIDE EFFECTS:  constipation, peripheral neuropathy