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Characteristics
Of Different Types Of Chemotherapy
Source
VI. Anticancer Chemotherapy
K. Antitumor Agents
1. Agents which alter DNA
PHCL 765
CHEMOTHERAPY
Chapter 7 in Mosby
Chemotherapy
is the science of selective toxicity. The goal of chemotherapeutic
treatment is to selectively attenuate or destroy pathogenic
micro-organisms or cells with minimal side effects to the host.
These targeted cells or organisms may be bacteria, viruses,
protozoans, fungi, helminths, or tumor cells. In order to achieve
selective toxicity, the target for chemotherapeutic agents may be
unique to the target population, may be structurally different in
the target population from the form in the host population, or may
be more essential in the target population than in the host
population. We will explore the targets and the mechanisms of action
of various classes of chemotherapeutic drugs, and will relate both
the therapeutic effects and the adverse effects of these drugs to
those targets and mechanisms.
The first
task in learning this material is to recognize the drug names and to
assign them to a class, based on target cell or organism, or
mechanism of action, or both. For some classes of drugs, such as the
penicillins and the cephalosporins, this will be a simple task. For
other groups the memorization is more challenging. Once assigned to
a class, one should recall the general characteristics of that
class: pharmacokinetics (i.e. absorption, distribution,
metabolism, excretion), pharmacodynamics (i.e. mechanism of
action, spectrum of activity, resistance), and adverse effects.
Often a single drug will be described as the prototype for a class.
You should learn everything about the prototype drug and then learn
how each member differs from the prototype. Please note that the
designation "prototype" simply denotes a model drug with
characteristics typical for the group. This does not imply relative
clinical importance.
I.
General Principles of Chemotherapy
-
Note: Although these chapters address antimicrobial chemotherapy,
many of the same basic principles apply to antiparasitic and
anticancer chemotherapy as well.
-
Understand the concept of selective toxicity — what it is and how
it may be achieved
-
Recognize
and understand the different types of targets for chemotherapeutic
drugs, and how these mechanisms relate to selective toxicity
-
Know the
definitions of chemotherapeutic spectrum and chemotherapeutic
index and how they relate to selective toxicity
-
Understand the role of the host in chemotherapy
-
Be aware
of both general and specific pharmacokinetic barriers to effective
chemotherapy
-
Understand the difference between bacteriostatic and bactericidal,
and how this relates to drug choice and dosage intervals
-
Know
general mechanisms for resistance to chemotherapeutic drugs, and
appreciate how the use of these drugs selects for resistant
populations
-
Know the
indications for combination chemotherapy
-
Know the
rationale behind chemoprophylaxis
-
Understand the appropriate and inappropriate uses of
chemotherapeutic drugs
II.
Antibacterial Chemotherapy:
A.
Inhibitors of cell wall synthesis (ICWS)
1.
Penicillins
-
Structure-function relationships-- the beta-lactam ring
-
Role of
penicillin binding proteins (PBP) and murein hydrolases
-
Chemotherapeutic spectrum of penicillins
-
Mechanisms of resistance — beta-lactamases
-
Cross-resistance
-
Acid-
and beta-lactamase-resistant penicillins
-
Adverse
reactions — hypersensitivity
2.
Cephalosporins
-
Similarities to and differences from penicillins
-
Changes
in pharmacokinetics and chemotherapeutic spectrum of first-,
second-, and third-generation cephalosporins
3. Other
beta-lactams
a.
Aztreonam
b. Imipenam
c. Clavulanic acid
4. Other
ICWS
a.
Vancomycin
b. Bacitracin
c. Isoniazid (only for M. tuberculosis)
B.
Membrane-active agents
-
Understand the mechanism of action of polymyxins and gramicidin,
and how this differs from ICWS
-
Know the
clinical uses of these agents
C.
Inhibitors of protein synthesis (IPS)
1.Aminoglycosides
-
Know
mechanisms of action for aminoglycosides
-
Know
spectrum of activity and clinical uses
-
Know
pharmacokinetics — routes of administration, excretion
-
Know
the classic adverse effects of aminoglycosides
-
Understand the dependency of therapeutic and toxic effects on
pharmacokinetics
-
Understand development of resistance to aminoglycosides
-
Role in
combination chemotherapy
2.
Tetracyclines, erythromycins, chloramphenicol, clindamycin,
spectinomycin
-
Know
mechanisms of action for these IPS
-
Know
spectrum of activity and clinical uses
-
Understand the dependency of therapeutic and toxic effects on
pharmacokinetics
-
Understand why the use of these IPS is relatively limited (i.e.
specific indications for use)
D.
Inhibitors of folate-dependent pathways
1.
Sulfonamides
-
Know
the mechanism of action of sulfonamides
-
Understand the concept of "antimetabolite"
-
Appreciate the role of pharmacokinetics in the action and uses
of sulfonamides
-
Know
the pharmacokinetic and pharmacodynamic differences among
various sulfonamides
-
Know
the adverse effects of sulfonamides
2.
Trimethoprim
-
Know
the mechanism of action of trimethoprim
-
Understand the rationale of combined sulfonamide-trimethoprim
chemotherapy
-
Know
the clinical uses and adverse effects associated with
trimethoprim
E. DNA
gyrase inhibitors
-
Understand the function of DNA gyrases, and the effects of their
inhibition
-
Know the
clinical uses of quinolones and fluoroquinolones
-
Know the
adverse effects and potential drug-drug interaction for quinolones
F. Urinary
tract antiseptics
Understand the role of pharmacokinetics in the treatment of
urinary tract infections
G.
Antimycobacterial agents
-
Appreciate the consequences of the mycobacterial life cycle in
regard to chemotherapy
-
Know
mechanisms of action for antimycobacterial drugs
-
Know the
distinction between "first-line" and "second-line" anti-TB drugs,
and why this distinction is disappearing
-
Know the
pharmacogenetics of isoniazid metabolism
-
Know the
appropriate use of drug combinations in antimycobacterial
chemotherapy
III.
Antifungal Chemotherapy
-
Understand why selective toxicity against fungal pathogens is more
difficult to achieve than is antibacterial selectivity
-
Know the
mechanisms of action, pharmacokinetics, and clinical uses of the
antifungal drugs
-
Know the
adverse effects of antifungal drugs
A.
Antifungal azoles
B.
Membrane-active agents
C.
Antimetabolites
D.
Griseofulvin
IV.Antiparasitic
Chemotherapy:
A.Basic
Principles of Antiparasitic Chemotherapy
B.Antiprotozoal Chemotherapy
1.
Antimalarials
2. Other
antiprotozoal drugs
C.
Anthelminthic Agents
-
Know
mechanisms of action against intestinal and extra-intestinal
parasites
-
Know
drugs used clinically in North America (limit to infections by
Ascaris, pinworm, hookworm, tapeworm)
V.
Antiviral Chemotherapy and Chemoprophylaxis
-
Understand the viral life cycle and its' implications for
chemotherapy
-
Know the
mechanisms of action for major antiviral drugs
-
Know
saqunavir is a protease inhibitor
VI.
Anticancer Chemotherapy
-
Know
mechanisms of action for classes of anticancer drugs
-
Understand the role of pharmacokinetics in anticancer chemotherapy
-
Know the
adverse effects of anticancer drugs, both the common effects and
the "signature" toxicities of specific agents
-
Understand the basis for selective toxicity of anticancer drugs,
and how this relates directly to both therapeutic and adverse
effects
-
Understand the need for total kill of target cells
-
Understand resistance and multi-drug resistance in anticancer
chemotherapy
-
Appreciate the importance of multi-drug and multi-modality therapy
VII.
Drug List for the Chemotherapy Unit
A. Cell
Wall Synthesis Inhibitors
1.
Penicillins
|
BENZYL PENICILLIN (PENICILLIN G)
BENZATHINE PENICILLIN G
PHENOXYMETHYL PENICILLIN (PENICILLIN V)
NAFCILLIN
OXACILLIN
CLOXACILLIN
DICLOXACILLIN
AMPICILLIN
AMOXACILLIN
CARBENICILLIN
TICARCILLIN
MEZLOCILLIN
PIPERACILLIN |
2.
Cephalosporins
|
1st generation |
2nd generation |
3rd generation |
4th generation |
|
CEFADROXIL
CEPHALOTIN
CEPHALEXIN
CEFAZOLIN
CEPHAPIRIN
CEPHRADINE |
CEFOXITIN
CEFACLOR
CEFAMANDOLE
CEFUROXIME
LORCARBEF
CEFONICID
CEFOTETAN |
CEFTRIAXONE
CEFTAZIMIDE
MOXALACTAM
CEFOTAXIME
CEFPODOXIME
CEFTIZOXIME
CEFOPERAZONE |
CEFEPIME |
3. Other
beta-lactams
|
AZTREONAM
IMIPENEM/CILASTATIN
CLAVULANIC ACID |
4. Other
cell wall synthesis inhibitors
|
VANCOMYCIN
BACITRACIN
CYCLOSERINE |
B. Agents
Which Affect Cell Membranes
1.
Polymyxins
|
POLYMYXIN B
COLISTIMETHATE |
2.
GRAMICIDIN
C. Protein
synthesis inhibitors
1.
Aminoglycosides
|
STREPTOMYCIN
KANAMYCIN
NEOMYCIN
GENTAMICIN
TOBRAMYCIN
AMIKACIN
NETILMYCIN |
2.
Tetracyclines
|
TETRACYCLINE
DEMECLOCYCLINE
DOXYCYCLINE
MINOCYCLINE |
3.
Macrolides
|
ERYTHROMYCIN BASE
ERYTHROMYCIN ESTERS
AZITHROMYCIN
CLARITHROMYCIN |
4. Other
protein synthesis inhibitors
|
SPECTINOMYCIN
CHLORAMPHENICOL
CLINDAMYCIN |
D.
Inhibitors of folate-dependent pathways
1.
Sulfonamides
|
SULFISOXAZOLE
SULFACYTINE
SULFAMETHOXAZOLE
SULFASALAZINE (SALICYLAZOSULFAPYRIDINE)
SODIUM SULFACETAMIDE
MAFENIDE
SILVER SULFADIAZINE
CO-TRIMOXAZOLE |
2.
Dihydrofolate reductase inhibitors
E. DNA
gyrase inhibitors
|
NALIDIXIC ACID
CIPROFLOXACIN
NORFLOXACIN |
F. Urinary
tract antiseptics
|
NITROFURANTOIN
SYSTEMIC AGENTS |
G.Antimycobacterial drugs
|
ISONIAZID
ETHAMBUTOL
RIFAMPIN
STREPTOMYCIN
SECOND-LINE ANTI-TB DRUGS
CYCLOSERINE
ETHIONAMIDE
PYRAZINAMIDE
CAPREOMYCIN
PARA-AMINOSALICYLIC
ACID
DAPSONE |
H.
Antifungal Agents
|
KETOCONAZOLE
MICONAZOLE
CLOTRIMAZOLE
FLUCONAZOLE
ITRACONAZOLE
AMPHOTERICIN B
NYSTATIN
FLUCYTOSINE
TOLNAFTATE
GRISEOFULVIN |
I.
Antiparasitic drugs
1.
Antimalarials
|
CHLOROQUINE
MEFLOQUINE
PRIMAQUINE
PYRIMETHAMINE-SULFADOXINE (FANSIDAR) |
2. Anti-protozoal
drugs
|
METRONIDAZOLE
TRIMETHOPRIM-SULFAMETHOXAZOLE
PYRIMETHAMINE-SULFONAMIDE
PENTAMIDINE |
3.
Anthelminthic drugs
|
PRAZIQUANTEL
THIABENDAZOLE
MEBENDAZOLE
PYRANTEL PAMOATE |
J. Antiviral
Agents
|
AMANTADINE
RIMANTADINE
VIDARABINE
ACYCLOVIR
ZIDOVUDINE (AZIDOTHYMIDINE, AZT)
GANCICLOVIR
DIDEOXYINOSINE (DDI)
RIBAVARIN
SAQUINAVIR |
K. Antitumor
Agents
1. Agents
which alter DNA
a.
alkylating agents
|
MECHLORETHAMINE
CYCLOPHOSPHAMIDE
BUSULFAN
CARMUSTINE
LOMUSTINE
STREPTOZOCIN
CIS-PLATIN
CARBOPLATIN
PROCARBAZINE
MELPHALAN
THIOTEPA
TRIETHYLENEMELAMINE |
2.
Antimetabolites
a.
folic acid antagonists
b.
purine antagonists
|
6-MERCAPTOPURINE
6-THIOGUANINE |
c.
pyrimidine antagonists
|
5-FLUOROURACIL
CYTARABINE |
3. Plant
alkaloids
a.
vinca alkaloids
b.
podophyllotoxins
|
ETOPOSIDE (VP-16)
TENIPOSIDE (VM-26) |
c.
PACLITAXEL (TAXOL)
4.
Antibiotics
|
DACTINOMYCIN
DAUNORUBICIN
DOXORUBICIN
BLEOMYCIN
MITOMYCIN C
PLICAMYCIN |
5. Hormonal
agents
a.
hormones
|
PREDNISONE
ESTROGENS
DIETHYLSTILBESTROL (DES) |
b.
modulation of hormone release and action
|
AMINOGLUTETHIMIDE
LEUPROLIDE ACETATE
TAMOXIFEN |
6.
Miscellaneous agents
|
AMSACRINE (AMSA)
HYDROXYUREA
MITOXANTRONE
AZATHIOPRINE
CYCLOSPORIN A |
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