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CHEMOTHERAPY (15.0 hr)
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Subcommittee:
General Comments:
1. The classification of drugs as
"prototype" and "secondary" drugs may be misleading,
particularly with certain groups of chemotherapeutic agents such as the
penicillins and cephalosporins where a number of drugs may be considered
to be prototypical for different reasons (e.g., pen G, ?-lactamase
resistant agents, broad spectrum agents). Moreover, the medical students
may confuse "prototype" with "clinically most
important". Thus, it is suggested that certain "lead-in"
drugs be termed "model drugs" that exemplify the mechanism of
action and certain aspects of the pharmacology of a class of
chemotherapeutic agents. The most important drugs from the standpoint of
current clinical use should be indicated where they are distinct from the
model compound. The term "secondary drugs" should probably be
reserved for agents not currently considered clinically important.
2. The time devoted to various
topics in chemotherapy will vary from institution to institution
depending on a number of factors including (a) the amount of time spent
in microbiology on basic mechanisms of bacterial cell wall synthesis,
mechanisms of action of antibacterial drugs, etc., (b) the coverage of
this class of drugs in clinical correlation conference sessions or in
lectures given by clinical departments, (c) the expertise of the
department, and (d) teaching time available to the department.
3. Information regarding toxicity,
antibacterial spectrum, therapeutic uses, and specific pharmacology
should be covered as part of the discussion of individual drug classes.
Alternatively, it could be done by clinical indications (e.g., TB, broad
spectrum, etc.).
4. Antimicrobial drugs should be
organized for pedagogical reasons by mechanism of action, i.e.,
inhibitors of cell wall synthesis, protein synthesis inhibitors,
metabolic inhibitors, DNA gyrase inhibitors, DNA damaging agents, etc.
a.
Chemotherapy of Microbial Diseases
1)
Introduction of chemotherapy (1 hr)
Objectives:
concept of selective toxicity, concept of drug target, e.g., DNA, key enzyme
steps, cell wall synthesis, protein synthesis, general mechanisms of drug
resistance, rationale for drug combinations, rationale for
chemoprophylaxis, appropriate and inappropriate use of antimicrobial
agents, sources of information about new chemotherapeutic agents
2)
Sulfonamides and DNA gyrase inhibitors (1 hr)
Objectives:
historical development of antibiotics . mechanism of action, mechanism of
resistance, adverse reactions, drug combinations, especially trimethoprim
and sulfamethoxazole
3) Inhibitors
of Cell Wall Synthesis (2 hr)
Objectives:
steps of cell wall synthesis and points of attack for drugs, basic
chemistry and SAR mechanisms of resistance inhibition of ?-lactamases
cross resistance . adverse reactions, especially allergic reactions
4)
Inhibitors of protein synthesis
a) Aminoglycosides (1 hr)
Objectives: mechanisms of action; differences between
drugs' mechanisms, three major types of drug toxicity: neuromuscular, vestibular
oto, renal. Increased ototoxicity and nephrotoxicity in elderly.,
pharmacokinetics: blood levels are very important for use of this class
of drugs, narrow therapeutic index, combination chemotherapy, drug
interactions
b) Chloramphenicol, macrolides, and tetracyclines. (1
hr)
Objectives: mechanisms of action, antimicrobial
spectrum. toxic effects with special note of hematologic effects of
chloramphenicol, adverse effects on newborn, discussion of appropriate
use of these agents. Their usefulness is relatively limited (except
erythromycin), and they should be used only for specific therapeutic
purposes.
5)
Antimycobacterial Drugs (0.5 hr)
Objectives:
TB as a public health problem. Atypical mycobacterial infections in AIDS
and leprosy patients, mechanisms of drug action for those not covered
elsewhere . appropriate use of drug combinations. toxicity
pharmacogenetics of isoniazid metabolism. drug resistance
6)
Antifungal Agents (1 hr)
Objectives:
.mechanisms of action . topical and systemic uses
7)
Antiviral Drugs (1 hr)
Objectives:
. mechanisms of action, rationale for new agents. new HIV/AIDS drugs
8)
Antiparasitic Drugs (2 hr)
Objectives:
mechanism of action of common drugs . target for anthelmintic treatment
is adult non-dividing organisms . role of anchorage and motility in
helminth biology and its' importance as a target for anthelmintic drugs.
Malaria: disease process, life cycle of organism, importance as a world
health problem. schistosomiasis: same as above . drugs of choice for most
common parasitic infections of North America, e.g., trichomonas,
toxoplasmosis, entamoeba, histolytica, ascaris, pinworm, hookworm,
tapeworm
9)
Anticancer Drugs (4 hr)
Objectives:
fundamentals of cancer biology, therapeutic modalities; adjuvant chemotherapy,
determinants of drug response: tumor determinants, host determinants,
leukemias/lymphomas vs. solid tumors, total cell kill concept, apoptosis,
selective toxicity: why it is so difficult to achieve cell cycle
specificity, combination chemotherapy: rationale and examples, common and
peculiar toxicities . mechanisms of drug action, pharmacokinetics, where
important: e.g., methotrexate, drug resistance
10)
immunomodulators (0.5 hr)
Immunosuppressives:
. mechanism of action azathioprine, cyclosporine A, FK506
Note:
Immunosuppressive drugs are not covered as a separate topic at
represented institutions. Comments about immunosuppressive effects of
anticancer drugs are made under individual agents.
Hematopoietic
Growth Factors: mechanism of action erythropoietin, rHuGM-CSF
(sargramostin)
Chemotherapeutic Drugs to Consider
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