Term
How much water should be used to flush medications? |
|
Definition
15 mL water before and after |
|
|
Term
Should you replace an occluded NG tube in an alert and oriented patient with a larger bore size NG tube to prevent further occlusions? |
|
Definition
No because the discomfort associated with it makes it a poor choice for short-term feeds |
|
|
Term
What causes physical drug-nutrient interaction? What are the results? |
|
Definition
Physical interactions are caused by drug and formulation pH, chemical reactions, protein complexity, time, temperature, duration of exposure.
Physical interactions result in precipitation in PN or EN, disruption of emulsions for IVFE or EN, altered viscosity, change in consistency, clumping, or curdling of EN formulation. |
|
|
Term
What is a pharmaceutical drug-nutrient interaction? What is the result? |
|
Definition
Pharmaceutical interaction caused by alteration of a specialized dosage form or administration by a different route than what was intended.
Results in loss of drug activity or toxicity |
|
|
Term
What is a pharmacokinetic drug-nutrient interaction? What is the result? |
|
Definition
Pharmacokinetic interactiion occurs before the drug reaches the site of action and can be caused by altered absorption, presystemic metabolism, hepatic metabolism.
Results in loss of drug activity, toxicity |
|
|
Term
What is a pharmacodynamic drug-nutrient interaction? What are the results? |
|
Definition
A pharmacodynamic interaction occurs at the site of action. Binding sites or receptors are usually involved.
It results in loss of drug activity or toxicity. |
|
|
Term
What is a pharmacological drug-nutrient interaction? What are the results? |
|
Definition
A pharmacological drug-nutrient interaction is an extension of the drug's normal pharmacological actions.
It can result in the inability to provide PN or EN due to adverse effects. |
|
|
Term
What is a common outcome of a physical DNI in relation to EN? |
|
Definition
|
|
Term
Which type of DNI typically occurs before the drug or nutrients reach the patient? |
|
Definition
|
|
Term
Which vitamin quickly degrades when added to PN? Why? |
|
Definition
Thiamin due to hydrolysis, photodegradation, and other forms of chemical degradation |
|
|
Term
How does pH of a drug affect compatibility with PN? |
|
Definition
Drugs that are a very high or very low pH are typically incompatible with PN |
|
|
Term
How can calcium precipitate in a VAD be treated? |
|
Definition
A 0.1 N hydrochloric acid can be instilled in the occluded lumen to dissolve the precipitate, or the VAD can be replaced. |
|
|
Term
How does EN protein type influence the risk of physical drug interaction with EN? |
|
Definition
The presence of a complex protein (not hydrolyzed or free AA) increases risk of physical DNI |
|
|
Term
What components of EN have been shown to NOT affect risk of drug-nutrient interaction? |
|
Definition
Fiber content, nitrogen content, dilution of formulation
|
|
|
Term
How does protein type affect risk of physical drug interaction in EN? |
|
Definition
Protein source (caseinates, soy, whey) may have some effect on interactions. Casein seems to be more reactive than whey because it is less acid-stable. |
|
|
Term
How do the base components of a drug affect its risk of physical interaction with EN? |
|
Definition
Base components (whether the drug is water-based, alcohol-based, or alcohol-based) affects the compatibility of the drug with EN more than the drug itself in most cases |
|
|
Term
Which drug has been shown to be incompatible with fiber-containing EN formulas and compatible with fiber-free ones (it is an exception)? |
|
Definition
|
|
Term
What is the best way to prevent physical drug nutrient interactions? |
|
Definition
The best way to prevent physical DNIs is by not allowing the drugs to mix with either EN or PN formulations |
|
|
Term
How should EN or PN be handled when administering a drug through the same device as the EN or PN infusion?? |
|
Definition
The EN or PN should be stopped, and the access device should be flushed with fluids that are compatible with the EN/PN formulation as well as the drug. |
|
|
Term
How should EN/PN access devices be flushed when administering medications? |
|
Definition
The access device should be flushed before and after drug administration and between administrations if more than one drug is administered. |
|
|
Term
What is the typical flush fluid of choice for VADs? |
|
Definition
Normal saline is typically the fluid of choice, but D5 is sometimes used |
|
|
Term
What is the minimum recommended volume of fluid for flushing feeding tubes in adults? |
|
Definition
|
|
Term
What are alternative methods for preventing physical drug interaction with EN or PN formulation? |
|
Definition
Altering infusion time (for instance cyclic infusion for daily drugs), the nutrition formulation (for instance switching to a hydrolyzed protein formula), or the drug |
|
|
Term
What is the most common form of altering a dosage form of a drug? |
|
Definition
Crushing or dissolving a solid form to create a liquid for administration via feeding tube |
|
|
Term
How should tablets and capsules be administered via tube? |
|
Definition
Solid dosage form: crushed into very fine powder and mixed with warm water
Capsule: opened and content mixed with water to form slurry |
|
|
Term
What types of drugs should not be crushed for administration? |
|
Definition
- Sustained-release, slow-release, delayed release
- Enteric-coated meds
|
|
|
Term
What drug sweetening agents can cause GI problems? |
|
Definition
Mannitol, sucrose, and particularly sorbitol |
|
|
Term
What are methods for preventing pharmaceutical interactions? |
|
Definition
- Using immediate-release forms rather than long-acting forms
- Avoiding special dosage forms such as enteric-coated or sublingual when administering via feeding tube
|
|
|
Term
Can proper tube flushing prevent pharmaceutical interactions? Can it prevent physical interactions? |
|
Definition
Flushing does not prevent pharmaceutical interactions, but can prevent concomitant physical ones |
|
|
Term
Which type of drugs are most likely to be adsorbed by a container? |
|
Definition
Fat-soluble ones (e.g. vitamin A) |
|
|
Term
What consistency should slurries/suspensions be made into before administering via feeding tube? Why? |
|
Definition
As thin as possible to avoid adhering to the tube |
|
|
Term
How does low pH affect gastric vs small bowel motility? |
|
Definition
It decreases gastric motility and increases small bowel motility |
|
|
Term
How do products with extreme high or low osmolality affect gastric and small bowel motility? |
|
Definition
They decrease gastric motility and increase small bowel motility |
|
|
Term
How do large volumes affect gastric and small bowel motility? |
|
Definition
They decrease gastric motility and increase small bowel motility |
|
|
Term
How does drug absorption differ in the duodenum vs jejunum? |
|
Definition
Most drugs are absorbed throughout the bowel, but some have a major decrease in bioavailability when administered into the jejunum (Cipro for instance) |
|
|
Term
Is it necessary to hold continuous feeds in order to given meds that are supposed to be taken on an empty stomach? |
|
Definition
|
|
Term
What is recommended to avoid EN interaction with phenytoin? |
|
Definition
- Holding EN administration for at least 1 hour and possibly 2 hours before and after administration
- Monitoring of serum phenytoin concentrations
|
|
|
Term
What is the recommendation with administering carbamezipine? |
|
Definition
- Adequate dilution of the solution or slurry prior to administration and adequate flushing after the dose are the first choice to prevent EN-carbamezipine interactions
- When these measures fail, hold feedings before and after administration
|
|
|
Term
How does phenytoin interact with tube feeds? Can this cause an occlusion? |
|
Definition
Phenytoin can bind to the EN formula or the tube, but this is not expected to increase risk of occlusion |
|
|
Term
How do EN formulations affect fluoroquinolone antibiotics? |
|
Definition
EN formulations appear to reduce bioavailability of fluoroquinolone antibiotics |
|
|
Term
What are examples of fluoroquinolone antibiotics? |
|
Definition
Ciprofloxacin, levofloxacin, ofloxacin |
|
|
Term
What is the recommendation for administering EN with fluoroquinolone antibiotics? |
|
Definition
Hold administration of EN for at least 1 hour before and 2 hours after dosing |
|
|
Term
What are the recommendations for administering warfarin with EN? |
|
Definition
- Minimize contact of drug with feeding tube
- If the first approach fails, hold EN for 1 hour before and after warfarin dose
- Closely monitor PT/INR while increasing dose
|
|
|