In pharmaceutical sciences, drug interactions occur when a drug's mechanism of action is affected by the concomitant administration of substances such as foods, beverages, or other drugs. A popular example of drug-food interaction is the effect of grapefruit in the metabolism of drugs. Interactions may occur by simultaneous targeting of receptors, directly or indirectly. For example, both Zolpidem and alcohol affect GABAA receptors, and their simultaneous consumption results in the overstimulation of the receptor, which can lead to loss of consciousness. When two drugs affect each other, it receives the name of a drug-drug interaction. The risk of a drug-drug interaction (DDI) increases with the number of drugs used. A large share of elderly people regularly use five or more medications or supplements, with a significant risk of side-effects from drug-drug interactions. Drug interactions can be of three kinds: additive (the result is what you expect when you add together the effect of each drug taken independently), synergistic (combining the drugs leads to a larger effect than expected), or antagonistic (combining the drugs leads to a smaller effect than expected). It may be difficult to distinguish between synergistic or additive interactions, as individual effects of drugs may vary. Direct interactions between drugs are also possible and may occur when two drugs are mixed before intravenous injection. For example, mixing thiopentone and suxamethonium can lead to the precipitation of thiopentone.

1. DRUG DRUG
INTERACTIONS
Dr. Jeenal Mistry
Senior resident,
Dept. of Pharmacology,
GMERS Medical College, Navsari.
Date: 27th January 2024

2. OUTLINES
Definitions
01
Epidemiology &
Risk factors
02
Classifications
03
Types
04
Outcome
05
Clinical
Applications
06
Drug & Herb
07
NDD
08
2

3. Drug interaction
can be defined as the
modifications of the
effect of one drug by
the prior or concomitant
administration of
another drug / food/
exogenous substance.
3

4. ▪ About 7% of hospitalizations are due to drug interactions.
▪ As the number of medications a patient takes increases,
the potential for drug interactions increases.
▪ It causes increased duration of stay, cost and mortality.
Epidemiology of Drug Interactions
4

5. ▪ Poly pharmacy Eg. Chronic disease
▪ Complex Pharmacokinetic of drug Eg. Enzyme inducer or inhibitor
▪ Low therapeutic index Eg. Lithium
▪ Diseases Eg. CCF, Renal Or Liver disease
▪ Elderly patient : Beers Criteria
Risk factors for drug interaction
5

6. Drug interaction can be classified by following ways-
▪ Nature of drug interaction
▪ Depending on the interacting substance
▪ Outcome of drug interaction
Classification of Drug Interaction
6

7. Pharmaceutical interaction Minor
Pharmacokinetic (PK) interaction Major
Pharmacodynamic (PD) interaction Major
Types of drug interaction based on nature
of interaction
7

8. ▪ Drug – Drug Interaction
▪ Drug – Food Interaction
▪ Drug – Chemical Interaction
▪ Drug – Laboratory Interaction
▪ Drug-Disease Interaction
Types of drug interaction based on
interacting substance
8

9. Harmful
Decreased
therapeutic effect
Increased toxic
effect
Beneficial
Increased
therapeutic effect
Decreased toxic
effect
Types of drug interaction based on
outcome
9

10. Also called as incompatibility.
It is a physicochemical interaction that occurs when drugs are
mixed in i.v. Infusions causing precipitation or inactivation of
active principles.
Pharmaceutical Interaction
Diazepam + Infusion fluids ====➔ Precipitation
Phenytoin + Infusion fluids ====➔ Precipitation
Heparin + Hydrocortisone ====➔ Inactivation of heparin
Kanamycin + Hydrocortisone ====➔ Inactivation of kanamycin
Carbenicillin + Gentamicin ====➔ Inactivation of Gentamicin
10

11. Pharmacokinetic Interaction
These interactions are those in which ADME properties of the object drug is
altered by the precipitant and hence such interactions are also called as
ADME interactions
The resultant effect is altered plasma concentration of the object drug.
Absorption Interaction
01
03 Metabolism Interaction
04
Excretion Interaction
02
Distribution Interaction
11

12. Pharmacokinetic Absorption Interaction
01
Altered pH
05
Altered GIT
motility
03
Formation of
drug chelates
or complexes
06
Malabsorption
syndrome
02
Altered
bacterial flora
04
Drug induced
mucosal
damage
(1) Altered GIT absorption 12

13. A) Altered pH
The non-ionized form of a drug is more lipid soluble and more readily
absorbed from GIT than the ionized form.
Eg Antacids
Decrease efficacy of PPI
Eg H2 antagonists
↑pH
Therefore, these drugs must be separated by at least 2h.
↑pH
13

14. B) Altered intestinal bacterial flora
Eg: In patients receiving digoxin
↓
40% or more of the administered dose is metabolized by the
intestinal flora
↓
Antibiotics kill a large number of the normal
flora of the intestine
↓
Increase digoxin conc.
and increase its toxicity
14

15. C) Complexation or chelation
✓Tetracycline interacts with iron preparations
✓Sucralfate interferes with bioavailability of phenytoin
✓Cholestyramine binds with warfarin decreased absorption
✓ Antacid (aluminum or magnesium) hydroxide
Decrease absorption of
ciprofloxacin by 85%
due to chelation
15

16. D) Drug-induced mucosal damage
Antineoplastic agents e.g., Cyclophosphamide
Vincristine
Procarbazine
Inhibit absorption
of several drugs
eg., digoxin
16

17. E) Altered motility
➢Narcotics, atropine, antacids ↓ motility
➢Domperidone, metoclopramide, cisapride, ↑motility
Erythromycin
➢Methadone with didanosine →
↓GI motility→↑disintegration→↓bioavailability
➢Metoclopramide and digoxin
17

18. 2) Plasma protein binding
Acidic drug BasicDrug
Albumin ᾳ1 Acid Glycoprotein
Competitive protein binding by another drug
Increase concentration of free drug
more drug response
18
Phenytoin (90%), Tolbutamide (96%), and warfarin (99%) is highly bound to plasma
protein→ Drugs that displace these agents are: Aspirin, Sulfonamides, Phenylbutazone

19. 3) drug transporters
Transporters play key role in Drug Absorption and Excretion
Most important drug transporters
P-glycoproteins (PgP)
Interaction usually result in
Inhibit function of transporters
Inhibit drug excretion
Ultimately drug concentration increases in body
19

20. 4) Altered metabolism
Liver → Major site of drug metabolism
Other organs → WBC, skin, lung and GIT.
Altered phase I metabolism
CYP450 induction
CYP450 inhibition
Altered phase II metabolism
➢ Induction of phase II enzyme
UDP-glucuronyl transferases (UGTs)
➢ Inhibition of phase II enzyme
Competitive use of conjugate molecules
20

21. Renal excretion
A. Alkaline urine:
Na HCO3  urine pH,
 renal excretion of (weak acid) salicylates & NSAIDs
Acetazolamide, excrete bicarbonate,  urine pH,
 quinidine (weak base) excretion &  its toxicity
B. Acidic urine:
Salicylates  urine pH,
 methotraxate (weak acid) excretion &  its toxicity
21

22. Renal excretion (Cont.)
c. Competition for active secretion:
a. Weak acids
Probenecid  methotraxate excretion,  its toxicity
Probenecid  penicillin secretion,  its duration of action
b. Weak bases
Cimetidine  excretion of procainamide,  its toxicity
d. Excretion related to electrolyte balance:
Low Na+ intake causes lithium retention &  toxicity
Diuretics (thiazides), excrete more Na+, retain lithium,
 its toxicity
22

23. Pharmacodynamic Interaction
Are those in which the activity of the object drug at its site of
action is altered by the precipitant. Such interactions may be
direct or indirect.
These are of two types:
1.Direct pharmacodynamic interactions
2.Indirect pharmacodynamic interaction
23

24. Direct Pharmacodynamic Interaction
In which drugs having similar or opposing pharmacological effects are
used concurrently
The three consequences of direct interactions are:
1. Antagonism
2. Addition or summation
3. Synergism or potentiation
24

25. Indirect Pharmacodynamic Interaction
In which both the object and the precipitant drugs have unrelated
effects but the latter in some way alerts the effects of the former.
Example: salicylates decrease the ability of the platelets to
aggregate thus impairing the Homeostasis if warfarin induced
bleeding occurs
25

26. Food drug interaction
❑Pharmaceutical Phase
Drug Dissolution and Disintegration
Eg. High levels of Ascorbic acid (vitamin C) ie ↓ pH
↓
↓ Efficacy of saquinavir
Foods that raise gastric pH
↓
Prevent dissolution of isoniazid
↓
↓ Efficacy
26

27. Grapefruit juice and Drug Interactions
•Calcium channel blockers
•Amlodipine
•Fenoldopam
•Nifedipine
•Nimodipine
27

28. Other Clinically Significant Herb- Drug Interactions
Object Drug Interacting Drug Outcome
Anticonvulsants Wormwood  seizure threshold
Anticonvulsants Gingko biloba  seizure threshold
Digoxin Hawthorne  digoxin activity
Saquinavir Garlic  saquinavir levels
Warfarin Feverfew  risk of bleeding
Warfarin Garlic  risk of bleeding
Warfarin Ginger  risk of bleeding
Warfarin Ginkgo  risk of bleeding
Warfarin Ginseng  anticoagulant
.
28

29. Drug-Disease Interactions
Drug Disease
○ Anticholinergics BPH, constipation, dementia
○ Antiarrhythmics (Type 1A) CHF (systolic dysfunction)
○ CCB 1st generation CHF (systolic dysfunction)
○ Amphetamines HTN, insomnia
○ Benzodiazepines COPD, Dementia
○ Beta-blockers COPD, DM
○ Digoxin Heart block
○ Tricyclic antidepressants Arrhythmias, BPH, constipation
dementia, falls, heart block
postural hypotension
○ Metoclopramide Parkinson’s disease
○ Nitrofurantoin Chronic renal failure
○ Non-aspirin NSAIDs CRF, CHF, HTN
○ Opioid analgesics BPH, constipation, dementia
29

30. 30

31. Drug Laboratory Interaction
A. Nalidixic acid, salicylate and vitamin
C → provide a false positive test of
urine sugar with benedict’s solution
B. Oestrogens exhibit false positive rise
in the values of serum thyroxine (as
they cause hyperproteinaemia)
31

32. 1. National Prescribing Service, 2009.
2. Bailey, David G.; Dresser, George; Arnold, J.
Malcolm O. (2012)
3. Emergency Hospitalizations for Adverse Drug
Events in Older Americans" Daniel S. Budnitz,
M.D., M.P.H., Maribeth C. Lovegrove, M.P.H.,
Nadine Shehab, Pharm.D., M.P.H., and Chesley L.
Richards, M.D., M.P.H. N Engl J Med
2011;365:2002-12. Copyright © 2011
Massachusetts Medical Society.
4. Hilary Hamilton, MB, MRCPI; Paul Gallagher, PhD,
MRCPI; Cristin Ryan, PhD, MPSI; Stephen Byrne,
PhD, MPSI; Denis O’Mahony, MD, FRCPI.
Potentially Inappropriate Medications Defined by
STOPP Criteria and the Risk of Adverse Drug
Events in Older Hospitalized Patients. Arch Intern
Med. 2011;171(11):1013-1019.
References
32

33. Free Online Drug Interaction Checking
https://www.drugs.com/drug_interactions.php (Drugs.com)
http://reference.medscape.com/drug-interactionchecker (Medscape)
http://www.webmd.com/interaction-checker/ (Web MD)
http://ukhealthcare.uky.edu/Library/DrugReference/Druginteractionchecke r/
(UK Healthcare Drug Interaction Checker)
http://desktopindia.com/Drug-inter.aspx (Doctor's Desktop: Medical Practice Software - Indian)
Alternative resources
33

34. Thank You ☺