Introduction to pharmacovigilance and Malaysian Adverse Drug Reaction System (Dr [Auto-saved]_compressed.pdf

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PPPP 2232 Pharmacoepidemiology & Pharmacoeconomics
Introduction to
Pharmacovigilance /
Malaysian Adverse Drug
Reaction
ASST. PROF. DR. ZOHRA BHATTI
PhD (Clinical Pharmacy)
Department of Pharmacy Practice,
Kulliyyah of Pharmacy,
International Islamic University Malaysia,
Kuantan Campus,
Jalan Sultan Ahmad Shah, Bandar Indera Mahkota,
25200 Kuantan, Pahang
 Drug Effects

Positive
Effects
No
Drugs
response
Negative
3
Post Marketing Surveillances
(PMS)
After marketing of a drug, close monitoring for
unexpected adverse drug reactions (ADRs)
remains necessary due to the limited size of
premarketing trials, the selection of the
patients involved and the limited duration of
the trials

Post-marketing surveillance aims at a
timely detection of either new ADRs or
an increase of the frequency of ADRs
which are already known to be
associated with the drugs involved. 4
 INTRODUCTION TO
PHARMACOVIGILANCE
Before a product is No matter how extensive the
marketed, experience of its pre-clinical work in animals
safety and efficacy are limited and the clinical trials in
to its use in clinical trials. patients, certain adverse
The conditions under which effects may not be detected
patients are studied pre- until a very large number of
marketing do not necessarily people have used the
reflect the way the product will medicinal product.
be used in hospitals or in
general practice once it is
marketed.

5
DEFINITION OF PHARMACOVIGILANCE
(PV)

Pharmacovigilance (PV) is defined as “the science and activities
relating to the detection, assessment, understanding, and
prevention of adverse effects or any other drug-related
problem”.
World Health Organization. (2002). Safety of medicines: a guide to detecting and reporting
adverse drug reactions. Geneva: World Health Organization, 20.
6
In line with this definition, the
objectives of pharmacovigilance are:

To identify To prevent To assess To promote

previously harm from the risks and the safe and
unrecognized adverse reactions benefits of effective use of
adverse reactions arising from the use products in order medicinal
or changes in the of medicinal to determine what products, through
patterns of adverse products actions, if any, are providing timely
effects necessary to information about
improve their safe the safety of
use medicinal products
to patients,
healthcare
professionals and
the public

7
 DEFINITION OF ADVERSE DRUG
REACTIONS (ADRs)
ADR is defined as “a
response to a drug which
is noxious and unintended,
and which occurs at
doses normally used in
man for the prophylaxis,
diagnosis or therapy of
disease, or for
modifications of
physiological function”
World Health Organization. (1972). International drug monitoring: the role of national centres,
report of a WHO meeting [held in Geneva from 20 to 25 September 1971]. World Health
Organization.8
 DEFINITION OF ADVERSE DRUG
EVENTS (ADEs)

An injury resulting from the use of a drug
Can occur irrespective of whether or not the drug is suspected to
be the cause

Nebeker, J. R., Barach, P., & Samore, M. H. (2004). Clarifying adverse drug events: a
clinician's guide to terminology, documentation, and reporting. Annals of internal
medicine, 140(10), 795-801.9
 ADRs vs ADEs
The main difference whereas ADE is harm
between these terms is associated with any dose
that ADR is a harm of a drug, whether or not
usually suspected to be the dose is “normally used
related to the drug and in man” or due to other
may occur despite the confounders that arise
appropriate prescribing during treatment but are
and dosing. not necessarily caused by
the pharmacology of the
drug itself
AlAzmi, A., Ahmed, O., Alhamdan, H., AlGarni, H., Elzain, R. M., AlThubaiti, R. S.,... & Al Shaikh, A. (2019). Epidemiology of Preventable Drug-Related
Problems (DRPs) Among Hospitalized Children at KAMC-Jeddah: a Single-Institution Observation Study. Drug, Healthcare and Patient Safety, 11, 95.
10
Development of Pharmacovigilance as
a Discipline
Origins: Pharmacovigilance traces its roots back to the
mid-20th century when researchers began recognizing
the need for systematic monitoring of adverse drug
reactions (ADRs).

Thalidomide Tragedy: The thalidomide disaster of the
1950s and 1960s, where the drug caused severe birth
defects, served as a wake-up call for the necessity of
pharmacovigilance. This incident highlighted the
importance of post-marketing surveillance to detect rare
but serious ADRs.
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Development of Pharmacovigilance as a
Discipline:
Regulatory Responses: In response to the thalidomide
tragedy, regulatory agencies worldwide started implementing
pharmacovigilance systems to monitor drug safety more
effectively. This led to the establishment of formal
pharmacovigilance programs in many countries

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Milestones in Pharmacovigilance History
WHO Program: The World Health Organization (WHO) initiated its
Programme for International Drug Monitoring in 1968. This
program aimed to facilitate the exchange of information on ADRs
among member countries and promote collaboration in
pharmacovigilance activities.
Pharmacovigilance Guidelines: Various international bodies, such
as the International Conference on Harmonisation (ICH) and the
Council for International Organizations of Medical Sciences
(CIOMS), developed guidelines and standards for
pharmacovigilance practices. These guidelines provide a
framework for the systematic monitoring and reporting of ADRs.
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Rawlins and Thompson classification
of adverse drug reactions
Since the 1970s, ADRs have traditionally been classified into two broad
categories: Types A and B.
The usual characteristics of these different types of reactions are
contrasted, followed by some examples:
Type A (Augmented) reactions:
Dose‐related; Predictable from drug pharmacology; Common;
Reversible; Manageable with dose adjustment.
Classic examples of Type A reactions are
Bleeding (warfarin), hypoglycaemia(anti‐diabetic agents) & headache
(nitrates)
14
 TYPES of adverse drug
reactions
Type B (Bizzare) reactions:
Not dose‐related; Unpredictable; Uncommon; Serious irreversible;
Indicative that the drug needs to be stopped.
Classic examples of Type B reactions are
Anaphylaxis (penicillins), hepatitis (halothane) & agranulocytosis
(clozapine)
Additional categories of ADRs
Type C (Chronic), e.g. adrenal suppression with corticosteroids.
Type D (Delayed), e.g. tardive dyskinesia with neuroleptics.
Type E (End of use), e.g. withdrawal reactions with benzodiazepines
15
 DoTS Classification
In 2003, a system of
classification was proposed by
Aronson and Ferner based on
dose‐relatedness, time course and
susceptibility;
DOSE TIME SUSCEPTIBLITY
Toxic Independent Age
Collateral Dependent Gender
Hyper susceptibility rapid administration Ethnic origin
First dose Genetic disease
Delayed
Withdrawal
Early, intermediate,
late
16
DoTS
Classification
 DoTS classification is more
The classification system categorizes complete as it allows the
ADRs into five types, each representing a evaluation of ADRs
different aspect of the relationship between according to the dose used of
the drug and the adverse event: the suspect drug, the time
between ADR occurrence and
Type I (Dose-Related) the drug administration
(consumption), for reactions
Type II (Time-Related) that are time-dependent, and
Type III (Susceptibility-Related) the relationship with different
Type IV (Withdrawal-Related) susceptibility factors that
determine an increased risk of
Type V (Unexpected Failure of Therapy). adverse reactions.
17
 DoTS Classification Example
Osteoporosis due to corticosteroids:
this reaction occurs at therapeutic doses, usually after some
months of treatment. Females and older people are at the
greatest risk. Hence, it would be classified as:
Dose: collateral effect
Time: late
Susceptibility: age, sex
Significance of DOTS approach
The DOTS approach is useful because it addresses the limitations
of the Type A/B scheme into which many ADRs do not clearly fit.

18
 ADR REPORTING SYSTEM

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 MADRAC, DCA &
NPRA
Malaysia set up its national
pharmacovigilance system with the
establishment of the Malaysian
Adverse Drug Reactions Advisory
Committee (MADRAC) in 1987.
MADRAC acts as an advisory body to
the Drug Control Authority (DCA)
on local and international drug safety
issues.
The National Adverse Drug Reaction
Monitoring Centre, located within the
National Pharmaceutical
Regulatory Agency (NPRA) serves
as the secretariat to MADRAC, and
has been a member of the WHO
Programme for International Drug
Safety Monitoring since 1990.
What MADRAC do?

Promote ADR reporting in Malaysia

Provide information and advice to the DCA in order that regulatory action can be taken

based on the ADRs received (local & foreign).

Provide information to doctors, pharmacist and other health care professionals on ADRs.

Participate in the WHO ADR monitoring programs.

21
Pharmacovigilance
System

One of the pharmacovigilance
requirements for pharmaceutical
companies is the establishment of a
pharmacovigilance system within their
organizations.
Pharmaceutical companies need to
ensure their pharmacovigilance
systems are up to standards as any
deficiencies may impact patient safety.
23
Pharmacovigilance Evaluating
Methods
Spontaneous ADR Reporting.
Prescription Event Monitoring (PEM).
Case–Control and Case–Crossover Studies.
Cohort Studies.
Randomized Controlled Trials.

27
Spontaneous reporting system
(SRS)
The core data-generating system of
international Pharmacovigilance, relying on
healthcare professionals (and in some places
consumers) to identify and report any
suspected adverse drug reaction to their
national Pharmacovigilance center or to the
manufacturer.

28
 Spontaneous reporting system
(SRS)
Advantages
Early detection of signals of new , rare or serious ADRs.
Primary mechanism for generating suggestions regarding potential
ADRs, (hospital and out-patient care).
Operates for all drugs through out the whole of their lifetime.
Disadvantages
Under reporting. The term underreporting is predominantly used to
indicate that not all the adverse effects that occur are reported.
Variable qualities of reporting.
Data from the SRS, when taken alone, do not accurately quantify the risk
associated with a drug.

29
Prescription Event Monitoring (PEM)
A method used for the systematic collection and evaluation of
data on the safety and effectiveness of newly marketed drugs in
real-world clinical practice.
The primary purpose of PEM is to detect and assess adverse
reactions or events associated with newly marketed drugs that
may not have been identified during pre-marketing clinical trials.
Pharmacists or other healthcare providers collect information from
patient prescription forms or electronic records, including
demographic details, prescribing patterns, and adverse events
reported by patients or healthcare professionals.
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 Findings from PEM studies are reported to regulatory agencies, pharmaceutical
companies, healthcare professionals, and the scientific community through
publications.

Advantages:
It complements data from pre-marketing clinical trials by capturing ADRs that may
occur at lower frequencies or have delayed onset. Additionally, PEM allows for the
assessment of drug utilization patterns, adherence to prescribing guidelines, and
potential off-label use.
Disadvantages:
including potential underreporting of adverse events, biases in patient selection and
follow-up, reliance on healthcare providers for data collection, and challenges in
establishing causality between drug exposure and adverse reactions.

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ADR reporting by Case–Control and
Case–Crossover Studies
case-control and case-crossover studies are not typically used for
direct ADR reporting, they can indirectly contribute to the
understanding of ADRs by investigating the association between
exposure to a particular drug and the occurrence of adverse
events.
Instead, they contribute to the broader field of
pharmacoepidemiology by generating evidence on the safety
profile of drugs and identifying potential ADRs that require further
evaluation through systematic ADR reporting systems, such as
spontaneous reporting programs, pharmacovigilance databases,
and clinical trials.
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ADRs Reporting by COHORT
STUDIES
Cohort studies are a valuable tool for ADR reporting and
pharmacovigilance, as they provide longitudinal data on drug
exposure and adverse events in a defined population over time.

Cohort studies involve the prospective follow-up of a group of
individuals who are exposed to a particular drug or medication
regimen and a comparison group of unexposed individuals.

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ADRs reporting by Randomized Controlled

RCTs are primarily designed to assess the efficacy of
medications, they also play a crucial role in ADR reporting and
pharmacovigilance by providing valuable data on the safety
profile of drugs in controlled clinical settings.

By systematically collecting and analysing data on adverse
events, RCTs contribute to the ongoing evaluation of drug safety
and help ensure the safe and effective use of medications in
clinical practice.
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Scope of Pharmacovigilance in
Malaysia
The scope of pharmacovigilance in Malaysia
includes (but is not limited to):
2. Safety profile monitoring through
1. ADR/AEFI reporting by healthcare signal management process, as well as
professionals, consumers and PRH, preparation and evaluation of Periodic
collection of reports and monitoring by Benefit-Risk Evaluation Report
PRH and the Authority. (PBRER) and Risk Management Plan
(RMP).

4. Safety communication, for example
3. Risk Management System: a set of Direct Healthcare Professional
pharmacovigilance activities and Communication (DHPC) Letter,
interventions designed to identify, Package Insert (PI), websites,
characterise, prevent or minimise risks publications and Consumer Medication
relating to a medicinal product, Information Leaflet (RiMUP); to ensure
including the assessment of the product information is updated with
effectiveness of those interventions. latest safety information according to
NPRA directives and circulars.
REPORTING OF ADVERSE DRUG REACTION
(ADR) AND ADVERSE EVENT FOLLOWING
IMMUNISATION (AEFI)
Information from the spontaneous Information from all these
ADR/AEFI reporting schemes, in sources may lead to the following
combination with clinical and regulatory changes/actions:
epidemiological studies as well as a) Restriction in usage;
literature, are used to aid in the b) Refinement of dosage
decision-making on product instructions;
safety. c) Strengthening of specific
warnings;
All reports submitted to NPRA are
d) Reviewing of specific labelling
treated as confidential and requirements;
reporters are not required to e) Changes in product information
divulge the identity of the based on new findings;
patient(s) involved.
Scope of ADR Reporting
The WHO encourages reporting of
all suspected ADRs. Healthcare A reaction is suspected if the
provider, product registration holder
reporting healthcare professional,
(PRH ) and consumer are requested
to report ADRs suspected to be PRH or any person who possesses
related to all products registered with any registered product(s) believes
the Drug Control Authority (DCA), that there is a possible causal
e.g. pharmaceutical products relationship between the reaction
including biologics, over–the and the product in question. If so, all
counter (OTC) products, health available relevant clinical
supplements, and natural products, information must be provided.
even for common/minor or well-
documented reaction.
Scope of ADR Reporting
(Cont.)
All adverse reactions should Adverse events, which are not
be considered reportable suspected of being product-
according to the requirements related by the healthcare
outlined in this guideline professional attending to the
regardless of whether or not patient, should not be reported
the product was used in UNLESS the PRH feels that
accordance with the product there is a possible causal
information provided by the relationship between the
PRH. reaction and the product in
question.
Scope of ADR Reporting
(Cont.)
As for regulatory reporting ADR(s) due to OTC product(s),
purposes, if an event is health supplement(s) and natural
product(s)
spontaneously reported, even if ADR(s) related to any suspected
the relationship is unknown or forms of drug interactions e.g. drug-
unstated, it should meet the drug, drug-food interactions, etc.
definition of an adverse drug Change in frequency of a known
reaction. ADR(s).
In ADR reporting, priority should ADR(s) involving special patient
populations, e.g. pregnant,
be given in the following breastfeeding, elderly or paediatric
categories: patients.
Serious ADRs
Unexpected/unlabeled ADRs for all
new and generic products.
Scope of AEFI Reporting
An AEFI is any untoward Monitoring of AEFI is an
medical occurrence which effective way to monitor
follows immunisation and immunisation safety and
which does not necessarily contributes to the credibility of
have a causal relationship with National Immunisation
the usage of the vaccine. Programme (NIP).
The adverse event may be any
unfavourable or unintended
sign, abnormal laboratory
finding, symptom or disease.
Scope of AEFI Reporting
(Cont.)
All AEFI should be reported:
Non-serious AEFI – An AEFI that is not ‘serious’ and does not pose a
potential risk to the health of the recipient.
Serious AEFI – An event that either results in death, is life-
threatening, requires in-patient hospitalisation or prolongation of
existing hospitalisation, results in persistent or significant disability or
incapacity, or is a congenital anomaly/birth defects. Any medical event
that requires intervention to prevent one of the outcomes listed above
may also considered as serious.
5 categories of AEFIs
5 categories of AEFIs
(Cont.)
https://www.npra.gov.my/index.php/en/consumer-
medication-information-leaflets-rimup.html
https://www.pharmacy.gov.my/v2/en/documents/malaysian
-orphan-medicines-guideline-2020.html
GENERAL PRINCIPLES OF ADR/AEFI
SUBMISSION
The following are ADR/AEFI reporting forms available in Malaysia. The related forms can be
found in (Appendix 1)

1.. Online reporting form 3. Consumer Side Effect Reporting Form
Available via (ConSERF)

https://npra.gov.my/index.php/en/health- For the general public
professionals/reporting-adr.html 4. Borang Pemantauan Kesan Advers
Ringan Susulan Imunisasi

2. Report on Suspected Adverse Drug Specifically for parents or guardian or
Reactions vaccinees for minor AEFI

Prepaid reporting blue form 5. Suspect Adverse Reaction Report Form
(CIOMS Form I)
For PRHs
Example of Online reporting
form
Example of Manual Form
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6/29/2024 54
CIOMS FORM

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PCNE
Classifica
tion for
Drug-
Related
Problems
www.pcne.o
rg

10/11/2020 56
 57
PHM 3113
From ADR Report to Drug Policy
Assessment
Receive ADR Verify WHO
report/information information

Requires Discuss at
Prepare policy
regulatory MADRAC
paper for DCA
action? meeting

IMPLEMENT
POLICY

PHM 3113 58
well, to maintain within the
desired range

Verily those who say, "Our Lord
is Allah," and remain firm (on
that Path),- on them shall be no Al-
fear, nor shall they grieve. Ahqaaf
46:13
SOME OF THE
DEFINITIONS
6/29/2024 65