TETRACYCLINE ANTIBIOTICS
Outline
Copyright, Purdue Research Foundation, 1996
| BMS 445 Intro |
| Drug Groups |
| Slides / Graphics |
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Overview
- Broad spectrum including some protozoans
- Relatively safe
- Major differences are pharmacokinetic
- Cross resistance frequent
Members
- Group 1
- Tetracycline
- Oxytetracycline
- Group 2
- Demeclocycline
- Methacycline
- Group 3
Structure and chemical characteristics
- [pic]
Four fused 6-membered rings
- Source: Streptomyces spp
- Amphoteric, but usually formulated as chlorides
- Groups time of introduction & pharmacokinetics
- Group 1
- Older
- Dose intervals shorter
- More use in veterinary medicine
- Group 2
- Group 3
- Newer derivatives
- Dose intervals longer
- Some uses in veterinary medicine
Mechanism of action
- Inhibit protein synthesis
- bind reversibly to 30S ribosomal subunit
- decrease aa-tRNA to "acceptor" site
- Static
- Higher concentrations affect mammalian ribosomes
Resistance
- Significant resistance, but still useful
- Cross-resistance significant
- Plasmid-borne transporter pumps drug out
Pharmacokinetics
Absorption/administration
- IM -- only oxytetracycline and tetracycline
- Others -- sterile abscesses!
- IV -- SLOW to avoid cardiovascular collapse
- oxytetracycline
- tetracycline
- doxycycline
- Primarily PO
- F varies widely with drug & effect of food
- F = 90 to 100%
- F=58 to 77%
- Others
- Food decreases
- Insoluble chelates -- Ca++, Al+++, Mg++
- MILK?, Antacids?
- Some laxatives have Mg++
Distribution
- Doxycycline
- Rx in eye
- Rx in genitourinary tract
- All
- most body fluids
- CNS rel. poor, not ideal (10-25% of plasma)
- Intracelluar
- Rate: Ziv and Sulman (1974) with Cattle
- Time to reach given ratio milk:serum
Time to reach stated ratio
| Drug | Time | Ratio reached |
|---|
| Doxycycline & Minocycline | 20 min | >1.5 |
|---|
| Tetracycline | 60 min | 1.25 |
|---|
| Oxytetracycline | 60 min | 0.5 |
|---|
- Volumes of distribution --
- Bind to intracellular nucleic acids
- Bind to Ca++ bones & teeth
- Volumes of distribution -- comparative
Species Differences in Vd
| Drug | Species | Vd (L/Kg) |
|---|
| Doxycycline | Humans | 0.7 |
|---|
| Minocycline | Dogs | 1.9 |
|---|
| Humans | 0.4 |
|---|
| Oxytetracycline | Horses | 1.4 |
|---|
| Cattle | 0.8 |
|---|
| Dogs | 2.1 |
|---|
| Cats | 2.1 |
|---|
| Humans | 1.9 |
|---|
Elimination
- Both renal & biliary
- Significant enterohepatic circulation
- Doxycycline & minocycline -- primarily bile
- Others -- primarily urine
Most active form
- Elimination half-lives
- 6-11 hr -- tetracycline & oxytetracycline
Anuria -- incr. to 57 to 108 hr
- 11-23 hr -- doxycycline & minocycline
anuria little change
- Horses & cattle -- similar to humans
BUT: horses & donkeys may be longer --
see significant toxicity in these species [Bowersock 1995]
- Dogs / humans -- comparison
- 6 / 9.5 hr -- oxytetracycline
- 6 / 10.6 hr -- tetracycline
- 6 / 17.5 hr -- minocycline
- Drug interaction
- Doxycycline half-life may be decreased >50% by
phenytoin and barbiturates induce hepatic enz
Adverse effects
- Considered relatively non-toxic
Allergies
Biological adverse effects
- Important!
- Superinfection
- Especially if poor F adm PO
- Nearly always alter the intestinal flora
- Effect w/in 24-48 h
- Yeasts / other pathogens
- Horses!
- Signs of altered flora
- Diarrhea
- Indigestion
- ruminants
- horses
- rabbits, etc.
- Yeast overgrowth -- Sore mouth and perineal itching
Direct toxicity
Irritation
- Gastric mucosa -- cramps / burning
- Nausea / vomiting
- Can add food if minocycline & doxycycline
- IM/SC injections
- Usually prohibited
- Pain on injection
- Sterile abscesses
Deposition in calcified tissues
- Borwn discoloration of teeth
- Teeth fluoresce under UV
- Deformatin of bone
Dizziness/light headedness
- Minocycline -- caused CDC to recommend avoiding if non-essential
- Due to vestibular or CNS toxicity
Antianabolic effect
- Decreased protein synthesis
- If decreased renal funcitn, increased Serum Urea Nitrogen (SUN)
Photosensitivity
- All
- Especialy demeclocycline
- Avoid sunlight
Clinical application
- Long list -- Consult current therapy
- Wide range of organisms including bacterial & protozoans
- Gram-negative and Gram-positive bacteria
- Examples include Brucella,
Francisella, Pseudomonas pseudomallei,
Neisseria gonorrhoea, and Treponema pallidum.
- Many Pasteurellae and Borrelia hurgdorferi (Lyme disease)
- Common in Vet Med
- combination with sulfas (e.g., sulfadimethoxine [Albon] with which they are synergistic.
Used to treat most Strept, Staph, Pasteurella infections in cattle
[Bowersock 1995].
- Rickettsial infections
- eg., Q fever and Rocky Mountain Spotted Fever,
- Mycoplasmas and Chlamydia
- Often pneumonia and genitourinary tract infections
- Psittacosis --Chlamydia psittaci
- Malaria and ameobiasis in combo with other drugs
- Demeclocycline --
- SIADH -- syndrome of inappropriate (excess) antidiuretic hormone
- Non-infectious
- Inhibits ADH-induced water reabsorption
References
- Ziv & Sulman, Am. J. Vet. Res. 35:1197, 1974.
- USPDI, 11th edition, 1991
- USPDI, 15th edition, 1995
- BM6th88, Huber, W.G., Tetracyclines, in Veterinary Pharmacology
and Therapeutics, 6th edition, eds. Booth, N.H. and McDonald,
L.E., Iowa State University Press, 1988.
- Rang, H.P. and M.M. Dale. Pharmacology, Churchill
Livingstone, New York 1987, Chapter 30.
- Bowersock, T., 1995. Personal communication.
Study Questions
- What is the major basis for selecting one drug from among
the tetracycline group? Assuming you answered pharmacokinetic
properties, how could this be reconciled with the fact that specific
tetracyclines are often recommended for specific infectious processes?
- Minocycline used to be the recommended treatment for meningococcal
carriers, but CDC in Atlanta no longer recommends this? What specific
toxicity is associated with minocycline? What does the change
in this recommendation imply about cost-benefit ratios for some
uses of drugs?
- In what way are the tetracyclines (and sulfonamides to be
studied later) different from other antibacterials in their action
on protozoans? Be able to name two protozoan diseases for which
the tetracyclines are reasonable parts of the therapy.
- Why do you suppose a group of drugs is generally regarded
as non-toxic when they produce so many adverse effects?
- You should be able to recognize and discuss the basis of
each of the tetracycline adverse effects, e.g., superinfections,
diarrhea, and increased SUN. You should be able to list and discuss
at least two representative effects from each of the two important
(for the tetracyclines) categories of adverse effects.
- How does the cross resistance of bacteria to tetracyclines
compare to that of the beta-lactams and aminoglycosides?
- What special precautions must be taken with the tetracyclines
when used P.O.? Which two are apparently not affected by this
problem?
- Why are many of the tetracyclines never used IM or SC?
- Why is intravenous administration of tetracyclines dangerous,
despite the fact that it is one of the important means of use?
Note that some persons believe calcium chelation is the cause
of this hypotension, but that is not necessarily true. Addition
of calcium salts to infusions is not considered good practice.
Slow administration is!
- Explain how the apparent Vd of some tetracyclines can be
greater than the total body water?
- What is the effect of poor renal or hepatic function on the
elimination rate of the tetracyclines. Name one that is primarily
eliminated via the kidney and one that is primarily eliminated
via the bile.
- How could the concomitant administration of phenytoin or
phenobarbital result in drug failure with doxycycline?
| Drug Groups |
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Gordon L. Coppoc, DVM, PhD
Professor of Veterinary Pharmacology
Head, Department of Basic Medical Sciences
School of Veterinary Medicine
Purdue University
West Lafayette, IN 47907-1246
Tel: 317-494-8633Fax: 317-494-0781
Email: coppoc@vet.purdue.edu
Last modified
1:10 PM on 4/17/96
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