Route of Drug Administration
Route of Drug Administration
Route of Drug Administration
be able to describe various routes of drug administration including the concentration versus time profile that
might expected from their administration
be able to describe the biopharmaceutically relevant advantages and disadvantages of various routes of drug
administration
One method of classifying routes of administration is ENTERAL and PARENTERAL. Enteral means to do with the
GI tract and includes oral, buccal, and rectal. Parenteral means not through the alimentary canal and commonly
refers to injections such as IV, IM, and SC; but could also include topical and inhalation. We can also distinguish
IV from the rest, as with all others at least one membrane must be crossed, thus an absorption process is involved in
the administration and the pharmacokinetic model.
References
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Advantages:
Cheap - no need to sterilize (but must be hygienic of course), compact, multi-dose bottles, automated machines
produce tablets in large quantities.
Variety of dosage forms available - fast release tablets, capsules, enteric coated, layered tablets, slow release,
suspensions, mixtures
Disadvantages:
Sometimes inefficient - high dose or low solubility drugs may suffer poor availability, only part of the dose may be
absorbed. Griseofulvin was reformulated about 1970 to include the drug as a micronized powder. The
recommended dose at that time was decreased by a factor of two because of the improved bioavailability.
First-pass effect - drugs absorbed orally are transported to the general circulation via the liver. Thus drugs which are
extensively metabolized will be metabolized in the liver during absorption.
e.g. the propranolol oral dose is somewhat higher than the IV, the same is true for morphine. Both these drugs and
many others are extensively metabolized in the liver.
Food - Food and G-I motility can effect drug absorption. Often patient instructions include a direction to take with
food or take on an empty stomach. Absorption is slower with food for tetracyclines and penicillins, etc. However,
for propranolol bioavailability is higher after food, and for griseofulvin absorption is higher after a fatty meal.
Local effect - Antibiotics may kill normal gut flora and allow overgrowth of fungal varieties. Thus, antifungal agent
may be included with an antibiotic.
Unconscious patient - Patient must be able to swallow solid dosage forms. Liquids may be given by tube.
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Figure 7.2.1 Typical Plot of Cp versus Time after Oral Administration Fast and Slow Release Dosage Forms
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Advantages:
First pass - The liver is by-passed thus there is no loss of drug by first pass effect for buccal or sublingual
administration. Bioavailability is higher.
Rapid absorption - Because of the good blood supply to the area of absorption is usually quite rapid, especially for
drugs with good lipid solubility.
Drug stability - pH in mouth relatively neutral (cf. stomach - acidic). Thus a drug may be more stable.
Disadvantages:
Holding the dose in the mouth is inconvenient. If any part of the dose is swallowed that portion must be treated as
an oral dose and subject to first pass metabolism.
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Advantages:
By-pass liver - Some (but not all) of the veins draining the rectum lead directly to the general circulation thus by-
passing the liver. Therefore there may be a reduced first-pass effect.
Useful - This route may be most useful for patients unable to take drugs orally or with younger children.
Disadvantages:
Erratic absorption - Drug absorption from a supppository is often incomplete and erratic. However for some drugs it
is quite useful. There is research being conducted to look at methods of improving the extent and variability of
rectal administration. Absorption from solutions used as an enema may be more reliable.
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Advantages:
Rapid - A quick response is possible. Plasma concentration can be precisely controlled using IV infusion
administration.
Total dose - The whole dose is delivered to the blood stream. That is the bioavailability is generally considered to
100% after IV administration. Larger doses may be given by IV infusion over an extended time. Poorly soluble
drugs may be given in a larger volume over an extended time period.
Veins relatively insensitive - to irritation by irritant drugs at higher concentration in dosage forms.
Disadvantages:
Suitable vein - It may be difficult to find a suitable vein. There may be some tissue damage at the site of injection.
Maybe toxic - Because of the rapid response, toxicity can be a problem with rapid drug administrations. For drugs
where this is a particular problem the dose should be given as an infusion, monitoring for toxicity.
Requires trained personnel - Trained personnel are required to give intravenous injections.
Expensive - Sterility, pyrogen testing and larger volume of solvent means greater cost for preparation, transport and
storage.
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Advantages:
Absorption can be fast from aqueous solution but slower with depot formulations. Absorption is usually complete.
Improved by massage or heat. Vasoconstrictor may be added to reduce the absorption of a local anesthetic agent,
thereby prolonging its effect at the site of interest.
Disadvantages:
Can be painful. Finding suitable sites for repeat injection can be a problem.
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Larger volume than SC can be given by IM. They may be easier to administer than IV injections.
A depot or sustained release effect is possible with IM injections, e.g. procaine penicillin.
Disadvantages:
Trained personnel required for injections. The site of injection will influence the absorption, generally the deltoid
muscle provides faster and more complete absorption.
Absorption can be rapid from aqueous solution. Absorption is sometimes erratic, especially for poorly soluble
drugs, e.g. diazepam, phenytoin. The solvent maybe absorbed faster than the drug causing precipitation of the drug
at the site of injection.
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Absorption of gases is relatively efficient, however solids and liquids are excluded if larger than 20 micron and
even then only 10 % of the dose may be absorbed. Cromolyn is taken as a powder with 50 % of the particles within
the range of 2 to 6 micron. Larger than 20 micron and the particles impact in the mouth and throat. Smaller than 0.5
micron and they aren't retained. Some portion of the dose may be swallowed.
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Generally absorption is quite slow. Absorption through the skin especially via cuts and abrasions or from sites were
the skin is quite thin can be quite marked. This can be a real problem in handling toxic materials in the laboratory
or pharmacy. This can also be a serious problem with garden chemicals.
There may be some skin irritation. Drug absorption will vary by site of administration, skin condition, age and
gender.
Systemic absorption (transdermal) is better with low dose, low MWt, lipid soluble drugs.
Examples of drugs delivered by the transdermal route include estradiol, fentanyl, nicotine (various forms),
nifedipine and nitroglycerin.
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