Therapeutic drug monitoring

1. THERAPEUTIC DRUG
MONITORING
 BY:
GROUP06
Presentedto:
Ms.SUMBULYOUSAF

2. TherapeuticDrug
Monitoring
Presented To:
Mam Sumbul
Presented By:
Mahnoor Pervaiz
Roll No:
19021560-025C
Course Code: Bch-453
Course Title:
Toxicology
Group No:
O6
Department
Of Biochemistry
University
Of Gujrat

3. Presentationlayout:
 Introduction
 TDM: definition, goals & objectives
 Criteria for TDM
 Indications
 Factors affecting TDM
 TDM process
 Analytical methods
 Samples & timing
 Clinical interpretation
 Common drugs requiring TDM
 Clinical usefulness
 Problems
 Limitations
 Conclusion

4. Whatis
TDM?
(Therapeutic
drugmonitoring)
“TDM is the measurement of drug concentrations usually in
blood/ plasma that facilitates adjustment of dosage to produce a
desired response”

5. Whytdm?
 Therapeutic drug monitoring
can guide the clinician to
provide effective & safe drug
therapy in the individual
patient using serum drug
concentration.

6. Whyshoulddrug
levelbemonitored?
 Narrow therapeutic range
 Upper limit: drug toxic
 Lower limit: drug ineffective
 Same response to similar
doses

7. Isdruggivento
patientworking?

8. Monitoringofdrug
therapy:
 Monitoring of drug therapy can be done by
Therapeutic outcome using clinical end points
Pharmacodynamic measures using surrogates markers
Pharmacokinetic measures using TDM

9. Monitoringofdrug
therapy:
Therapeutic outcome:
• Therapeutic events
• Anti-convulsant-seizure
frequency
• Angina pectoris-attacks
Pharmacodynamic
measures:
• Surrogate markers
• Arterial BP-
hypertension
• Blood glucose-
diabetes
• INR-oral
anticoagulants
Pharmacokinetic
measures:
• TDM

10. TDM:Definition
“The clinical laboratory
measurement of chemical
parameter that, with
appropriate medical
interpretation, will directly
influence drug prescribing
procedures by combining
knowledge of pharmaceutics,
pharmacokinetics, &
pharmacodynamics”

11. GOALSOFTDM:
Ensure that given drug dosage produces
 Max. therapeutic benefit
Min. toxic adverse effects
Drug-appropriate conc.-site of action-produces benefits

12. TDM:Objectives
 Appropriate dosing of drug
 Chances of drug toxicity
 Economic convenience
 Reduce patient variability
 Accumulation of drug in body
 Dose-response relationship

13. Sourcesofvariability
indrugresponse:
 Pharmacokinetic variability- variation in dose & plasma conc.
 Pharmacodynamic variability- variation in drug conc. at receptor
level & response
• Bioavailability
• Plasma protein binding
• Volume of distribution
• Clearance
Pharmacokinetic
variables
• Genetic polymorphism
• Enzyme inhibitors
• Enzyme inducers
• Drug interactions
• Drug tolerance
Pharmacodynamic
variables

14. Therapeutic
range/window:
“Conc. range of drug in plasma where drug has been shown to be
efficacious without causing toxic effects in most people”
Min. Effective Conc. (MEC)
Max. Therapeutic Conc./ Minimum Toxic Conc. (MTC)

16. Criteria & Indications
forTDM
BY:
:LAIBATANZEEM
19021560-027

17. Normal vs
Therapeutic
Drug
Monitoring:

18. Therapeutic
Drug
Monitoring
forAll
Diseases???
 PlasmaconcentrationBestmonitoring
methodology
 Notusedforalldiseases……why?
Reasons:
1. Checkplasmaconc.needbloodsample
2. Instrumentationexpensive (HPLC,
Spectrophotometry)
3. Needexpertstooperate
4. Notavailableeverywhere

19. Criteria for
Therapeutic
Drug
Monitoring:
1. Effectof drugcannotbe
monitored
Not used for:
 Anti-HTN
 Anti diabetic
 Anti coagulant

20. Criteria for
Therapeutic
Drug
Monitoring:
2-NarrowTherapeuticIndex
Margin of safety
Can administer only 10-20mg
Response
starts
Shows
toxicity

21. Criteria for
Therapeutic
Drug
Monitoring:
4-Non-LinearDose-Responserelationship:
5-LinearActivemetabolite-Responserelation:
Dose
AC
Response
Response

22. Criteria for
Therapeutic
Drug
Monitoring:
2.-Drugsusedfor LifeThreatening
disease:

23. Drugs which
don’t need
Therapeutic
Drug
Monitoring:
Drugswithwidetherapeuticrange•
Hitandrundrugs:omeprazole,MAOinhibitors
Pharmacologicaleffects canbeclinicallyquantified/monitoredby
clinicalendpoints,e.g.,BP,HR,cardiacrhythm,bloodsugar,blood
cholesterolandtriglycerides,urinevolume,bodytemperature,
inflammation,pain,headache,etc.
Drugswhoseserumconcentrationsdonotcorrelatewith
therapeuticortoxiceffects.
Drugsusedtotreatlesscomplicatedornonlifethreatening
diseases
Drugfollowinglinearkinetics(lesscomplicatedpharmacokinetics)

24. Indications for
Therapeutic
Drug
Monitoring:
 Low therapeutic index
 Poorly defined clinical end point
 Drugs with saturable metabolism
 Drugs having wide distribution in the body
 Wide variation in the metabolism of drugs
 Major organ failure
 Prevention of adverse drug effects
 Suspected toxicity
 Inadequate therapeutic response (Therapeutic failure)

25. Indications for
Therapeutic
Drug
Monitoring:
 Compliance concerns (non compliance) e.g.
in epileptics
 Dosage change
 Change in patient’s clinical state
 Change in co-medications (quinidine
decreases digoxin clearance)
 Manifestations of toxicity and disease state
are similar (Nausea & vomiting occur in both
digitalis toxicity & congestive heart failure)

26. Factorsaffectingthe
TDM
19021560-035

27. Factors
affecting the
TDM
Factors
Physiological
factors
Pathological
factors
Other
factors
Many factors are affecting TDM such as:

28. Physiological
factors
affecting the
TDM:
Factors
Age
pregnancy
gender
Emotional
mood
Habits
Body
temperature
Body size
and
composition

29. Pathological
factors
affecting the
TDM
 Diseases cause individual variation in drug response
Factors
Renal failure
Liver failure
Diarrhea
Vomiting
inflammatory
bowl disease
GIT diseases
Inflammation

30. Others
factors
affecting
theTDM
 Patient’s demographic
 Dosage regimen and duration of therapy
 Alcohol and tobacco use
 Medicine or sampling errors
 Laboratory errors
 Patient compliance
 Individual capacity to distribute, metabolize and discrete the drug
 Altered protein binding

31. Process ofTDM

33. Refrences:
 Burton, M. E. (2006). Applied pharmacokinetics &
pharmacodynamics: principles of therapeutic drug monitoring,
LippincottWilliams &Wilkins.
 Rousselot, P., et al. (2015). Personalized daily doses of imatinib by
therapeutic drug monitoring increase the rates of molecular
responses in patients with chronic myeloid leukemia. Final results
of the randomized OPTIM imatinib study, American Society of
HematologyWashington, DC.
 Soola,A. H., et al. (2022). "Evaluation of the factors affecting
triage decision-making among emergency department nurses and
emergency medical technicians in Iran: a study based on Benner’s
theory." BMC Emergency Medicine 22(1): 1-9.
 https://slideplayer.com/slide/12736698/
 https://bmcemergmed.biomedcentral.com/articles/10.1186/s1287
3-022-00729

34. Therapeutic drug monitoring
 19021560-037
CONTENT:
• Analytical
Methodology
• Sample Collection

35. ANALYTICAL
Methodology
TDM
35
The fundamental
procedures necessary
for the quantification of
the drug in the body
are:
– recovery from body
fluids, tissues, and
organs
– separation from the
biological components
– quantification.

36. Introduction
The analytical
methodology employed
should ideally:
– distinguish between
compounds of similar
structure
– unchanged drug and
metabolites
– detect small amounts –
be simple enough to use as
a routine assay
– be unaffected by other
drugs administered
simultaneously
TDM 36

37. 1. Colorimetry
2. UV-
spectrometry
3. Fluorescence
spectrometry
4. Chromatography
Gas
chromatography
Mass
spectrophotometry
HPLC
HPTLC
5. Capillary
electrophoresis
Laboratory
Measureme
nts:

38. Immunoassay
:
Immunoassay
– RIA: Radio immunoassay
– Enzyme Immunoassay
– ELISA: Enzyme linked immunoassay
– EMIT: Enzyme multiplies immunotechnique
– FPIA: Fluorescence polarization immunoassay
38

39. Free drug
monitoring:
 Development of new filtration devices:
 (equilibrium dialysis, ultrafiltration, ultracentrifugation) has
made it possible to measure free unbound drug levels in
serum.
– Advantage:
 The free concentration is independent of changes in plasma
binding and is the pharmacologically active concentration.
– Disadvantage:
It is time consuming, expensive and therapeutic ranges do not
yet exist for many drugs.
39

40. Tdm 40
Samples:
Plasma or Serum is used for drug assays:
• Whole blood:
used for drugs such as cyclosporin, tacrolimus,
sirolimus

41. TDM
41
Other Samples:
Saliva Urine
Nasal
Secretion
Sweat

42. Guidelines
for
sampling
time:
• Short half life drugs:
– pre dose sampling
• Long half life drugs:
– at any point in the dosing interval
• One vs Two samples
 Drugs with a short half-life: peak and trough
concentrations will be very different from one another –
both samples to be obtained
 Peak and trough concentrations will not differ
substantially for drugs whose half-life is much longer
than the dosing interval – single sample is sufficient •
42

43. Timing of
Sample
Collection:
 The timing of blood collection is an important part of
therapeutic drug monitoring
 Blood sample should be collected once the drug
concentration have attained steady state.
 Absorption is variable after oral drug administration
and blood samples should be collected in elimination
phase rather than absorption / distribution phases.
• Trough conc : – when a drug is administered by
multiple oral doses, commonly used for anti-convulsant
drugs – should be obtained just prior to the next dose at
steady-state conditions
• Peak conc. : – useful for some antibiotics given IV –
Peak should be determined after drug absorption
(generally 2-4 hours for oral administration, 0.5-1 hour
for IM, SC route)
43

44. Clinical
Interpretati
on For
therapeutic
drug
monitoring
 The information required to allow interpretation of the
result should include:-
• Patient -Age, weight, sex, height, smoker status
• Clinical – clinical status (renal -serum creatinine; cardiac
-cardiac output; liver function etc.
• Other drug therapy
• Relevant disease states
• Time of the sample collection
• Time of the last dose
• Dosage regimen
• Indication for drug monitoring e.g. .lack of effect,
routine monitoring, suspected toxicity
44

45. DRUG IN
SERUMCONC:
Lower than anticipated:
• Patient non compliance
• Error in dosage regimen
• Rapid elimination
• Timing of sample
• Steady state not reached
• Change in hepatic blood
flow
• Induction of
metabolizing enzymes
• Poor bioavailability
• Increased plasma
protein binding
• Enlarged apparent
volume of distribution
45
Higher than anticipated:
• Error in dosage regimen
• Increased bioavailability
(hepatic disease)
• Slow elimination
• Inhibition of metabolizing
enzymes
• Decreased plasma protein

46. HowCAN we
make drug
monitoring
easier…
MOST APPROPRIATE SAMPLE:
Urine is the most commonly used
specimen for drug testing because of
ease of collection.Other advantages to
using urine for drug testing are the
relatively high concentrations of many
drugs and metabolites in urine
46
FAVORABLE
ANALYTICAL METHOD:
chromatographic methods such as
liquid chromatography–tandem mass
chromatography is the ability to
simultaneously analyze multiple drugs
in a single assay and methods typically
provide higher specificity for
identification of the drug.

47. UMM E RUBAB
19021560-046

48. TDM: Clinical
Applications
 To confirm adequate serum concentrations where
clinical response is inadequate: TDM can be used
to assess the appropriateness of dosing regimen to
maintain the minimum concentration required to
exhibit efficacy
 To avoid drug toxicity: maintaining within
therapeutic range
 To individualize dosing of some drug with an
unpredictable dose-response curve.
 To assess medical compliance
 To help predict a patient dose requirements

49. TDM: Clinical
Interpretation
Patient- Age, weight, sex, height, smoker
status
Clinical Status
Other drug therapy
Time of sample collection
Time of last dose
Dosage Regimen

50. Peak
and Trough
levels

52. Steps of
clinical
analysis

53. Drugs
commonly
Monitored:
 Cardio Active Drugs: Digoxin Quinidine,
Digitoxin
 Antibiotics: Gentamycin, Tobramycin
 Antidepressants: Lithium and tricyclic
antidepressants
 Antiepileptic Drugs: Phenytoin, Phenobarbitone
 Bronchodilators: Theophylline
 Cancer chemotherapy: Methotrexate
 Immunosuppressives: Cyclosporine

54. TDM: Clinical
Usefulness
Short Hospital Stay
Better disease control
Dose adjustment
Dose guidelines
Individualized dose requirements
Avoidance of unnecessary medication

55. TDM:
Problems
Physician sometime do not understand the
principles, benefits and limitations of
TDM services
Inappropriate Sampling Time
Do not state the indication of TDM
Insufficient Patient history and other
necessity data

56. Therapeuti
c Drug
Monitoring
Aims,
Limitations
And
Conclusion
s:

57. AimsOfTGM

58. How to design
a study to
evaluate
therapeutic
drug
monitoring in
infection
disease

60. Limitations
 Interference from other drugs
 Lack of training and skills
 Cost involved
 Individual variability
 Analytical variability
 Timing of samples
 Limited availability
 Clinical expertise

61. Conclusion
 Therapeutic drug monitoring is required for a small fraction of
drugs used in pharmacotherapy,but for these drugs such
monitoring is essential in order to achieve maximum efficacy of
the drug as well as to avoid drug toxicity.

62. Thank you