PHARMACOVIGILANCE TRAINING Is Crucial To Your Business. Learn Why!

Pharmacovigilance Training is Crucial to Business.

Yes! You have read it right.

Pharmacovigilance training is crucial for your business better than any other PV activity. Training is one of the crucial components for running the business however, it gets neglected many times. Pharmaceutical companies or Contract Research Organizations (CRO) are set up pharmacovigilance training departments and develop some training modules for their employees and give self consolation that they have set up PV training as per recommendation from the Good Pharmacovigilance Practice modules (GVP).

GVP Module I – Pharmacovigilance systems and their quality systems emphasize the importance of PV training by mentioning a few of the following recommendations-

1. A sufficient number of competent and appropriately qualified and trained personnel shall be available for the performance of pharmacovigilance activities [IR Art 10(1), Art 14(1)].
2. The organization should ensure that adequate resources are available and that training is provided.
3. All personnel involved in the performance of pharmacovigilance activities shall receive initial and continued training [IR Art 10(3), Art 14(2)].
4. For marketing authorization holders, this training shall relate to the roles and responsibilities of the personnel [IR Art 10(3)].
5. Training plans should be based on training needs assessment and should be subject to monitoring.
6. The organization shall keep training plans and records for documenting, maintaining, and developing the competencies of personnel [IR Art 10(3), Art 14(2)].
7. Training plans and records shall be kept and made available for audit and inspection [IR Art 10(3), Art 14(2)].
8. The applicant or marketing authorization holder should provide the QPPV with training in relation to its pharmacovigilance system, which is appropriate for the role prior to the QPPV taking up the position and which is appropriately documented
9. Where the QPPV has not completed basic medical training in accordance with Article 24 of Directive 2005/36/EC, the marketing authorization holder shall ensure that the QPPV is assisted by a medically trained person (i.e. in accordance with Article 24 of Directive 2005/36/EC) and this assistance shall be duly documented [IR Art 10(1)].
10. Adequate training should also be considered by the organization for those staff members to whom no specific pharmacovigilance tasks and responsibilities. 

In the majority of the organizations, the skeleton structure of training are as follow- 

• Induction Training - Self-explanatory- Given at the time of induction
• Ongoing Training - Issue of new controlled documents (i.e. SOP, Work Instruction (WI), Job-Aid) or Revision of existing controlled documents
• Refresher Training - Periodic Training for controlled documents
• Adhoc Training - As an when it is needed. Publication of new regulatory guidelines or training imparted as a part of a regulatory inspection or findings from audit or inspection.

Provision of pharmacovigilance activity is one of the mandatory requirements to obtain marketing authorization in certain countries. After getting marketing authorization, an organization should continue to monitor the benefit-risk profile of the molecule. Trained pharmacovigilance professionals are required to carry out PV activity.

According to GVP, training shall relate to the roles and responsibilities of the personnel. However, many organizations failed to identify training requirements according to job-role which might lead to delay or failure in PV deliverables in terms of quality and quantity. 

Let understand this with the ICSR example- 

Let us assume if any organization processed 220 Individual Case Safety Report (ICSR)/cases per month by 3 persons (Data Entry, Quality Review, and Medical Review). We can say that 10 cases are processed per day with 48 mins of average processing time (considering 480mins per day work and 22 working days). 

If we identify training gaps and planed targeted training and can able to reduce 20% (9.6 mins) of single case processing time. Then we can have 38.4 mins of average processing time and the same team can contribute 12.5 cases per day (instead of the previous 10 cases). That means we now have revised productivity of 275 cases per month i.e. ~ 25% rise compared to the previous month. 

If the same example we go for higher processing time then productivity falls significantly.

If we extrapolate this with the large numbers then it significantly impacts our work efficiency and that leads to business. 

This can be applied to the quality part also...In a general sense, data entry performed by a trained data entry person has a low or minimal error which leads to completion of quality review and medical review in a shorter time and ultimately productivity boost up and business also.

The training concept can be applied to other pharmacovigilance functions like literature review, aggregate reports, signal detection activities, etc. 

Once the system improves, then we can have no or minor findings in audits and inspections. Ultimately, It is a WIN-WIN situation for any organization by strengthening training culture and periodic assessment of the effectiveness of training. 

Signing Off. 

Thank you.😊

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Service Level Agreement (SLA) in Pharmacovigilance perspective

Service Level Agreement (SLA) is generally mutual commitment between service provider and a client. In pharmacovigilance industry, pharmacovigilance service provider and pharmaceutical company (client) come together in agreement for various PV activities. This could be single PV activity or End to End PV activities on behalf of client.

Pharmacovigilance SLA is not differ from another domain like IT industry where it prevails since long. It contains following common components of any SLA like –

·         Nature and scope of work

o   Region specific (USA, EU or ROW) or Worldwide

o   Single PV activity (ICSR processing  or literature review, etc.) or End to End PV Activity (ICSR processing, Literature Review, Aggregate Reports (PSUR/ADCO/PADER), Risk Management Plan (RMP), Signal Detection, etc.)  

o   ICSR Processing - All type of ICSR processing (Regulatory, Literature, Spontaneous) or specialized ICSR processing i.e. clinical trial or litigation, processing and case submission timelines

o   Literature Review – Literature review from global databases like Embase, PubMed or local journal review or both local and global review, preparation and maintenance of search strings

o   Aggregate Reports – Aggregate Report schedule preparation and maintenance, Ad-hoc reports, Nature of report format (PSUR, PBRER or regional specific like ANVISA, CDSCO, COFEPRIS, etc.), timeline related to finalization of draft and submission

o   Risk Management Plan (RMP) – New RMP or Maintenance of RMP, preparation and management of additional risk minimization measures (ARMM) or additional pharmacovigilance activities like non-clinical studies, clinical trials or non-interventional studies.

·         Work management procedure

o   SOP to be followed (Client SOP or Service Provider SOP)

o   Work on inhouse client database or other commercially available database i.e. ARISg, ARGUS

o   Timelines to be followed for each activity

·         Quality parameters

o   Quality scoring for ICSR, Literature Review, Aggregate Reports, RMP and Signal detection activities

·         Compliance check

o   Regulatory compliance check

§  ICSR submission

§  Aggregate report submission

o   SLA compliance check

o   SDEA compliance

·         Business Continuity Plan (BCP)

o   Business Continuity Plan (BCP) details in case of natural disaster or man-made disaster

·         Audits & Inspection

o   Internal audit and frequency

o   Audit of each other

o   Audit of business partners and affiliates

o   Inspection handling plan, if any specific condition.

·         Penalty

o   Financial penalty in case of quality and quantity deviation from SLA

·         Termination clauses

o   Terms and conditions where termination of SLA to be impose like significant non-conformity in PV process

o   Critical regulatory observation due significant defect in service provider’s procedure

One should remember that SLA is a dynamic document and can be drafted and modified based upon the business need of pharmacovigilance service provider and pharmaceutical company (aka client).

Though dynamism present in SLA, each points of SLA should be thoroughly reviewed by each party who enters in to agreement.

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Pharmacovigilance Abbreviations / Acronyms

Term	Description
ADCO	Addendum to Clinical Overview
ADRs	Adverse Drug Reactions
AE	Adverse Event
AERS	Adverse Event Reporting System
ANDA	Abbreviated New Drug Application
ATC	Anatomical Therapeutic Chemical  (in Anatomical Therapeutic  Chemical Classification System)
ATMP	Advanced Therapy Medicinal Product
CAPA	Corrective And Preventive Action
CCDS	Company Core Data Sheet
CCSI	Company Core Safety Information
CHMP	Committee for Medicinal Products for Human Use
CIOMS	Council for International Organizations of Medical Sciences
CMDh	Coordination Group for Mutual Recognition and Decentralised  Procedures - Human
CMS	Concerned Member State
CRO	Contract Research Organization
CT	Clinical Trial
CTD	Common Technical Document
DCP	Decentralised Procedure
DDD	Defined Daily Dose
DHPC	Direct healthcare professional communication
DIBD	Development international birth date
DLP	Data Lock Point
DME	Designated Medical Event
DSUR	Development safety update report
DUS	Drug Utilization Study
EMA	European Medicine Agency
EU	European Union
EURD	European Union Reference Date
EV	Eudravigilance
FDA	Food and Drug Administration
GCP	Good Clinical Practice
GMP	Good Manufacturing Practice
GVP	Good Pharmacovigilance Practice
IB	Investigator´s Brochure
IBD	International birth date
ICH	International Council for Harmonisation of Technical Requirements for  Pharmaceuticals for Human Use
ICSRs	Individual Case Safety Reports
IME	Important Medical Event
IND	Investigational New Drug
INN	International Non-proprietary Name
LBI	Late Breaking Information
MA	Marketing Authorisation
MAH	Marketing Authorisation Holder
MedDRA	Medical Dictionary for Regulatory Activities
MHRA	Medicines and Healthcare Products Regulatory Agency
MRP	Mutual Recognition Procedure
NAP	National Authorised Product
NCA	National Competent Authority
NDA	New Drug Application
PASS	Post-authorisation safety study
PBRER	Periodic Benefit-Risk Evaluation Report
PI	Product Information
PIL	Product Information Leaflet
PL	Package Leaflet
PRAC	Pharmacovigilance Risk Assessment Committee
PSMF	Pharmacovigilance system master file
PSUR	Periodic Safety Update Report
PSUSA	Periodic Safety Update Single Assessment
PT	Preferred Term
PTD	Patient Treatment Days
PTY	Patient Treatment Years
PV	Pharmacovigilance
QPPV	Qulified Person responsible for Pharmacovigilance
REMS	Risk Evaluation & Mitigation Strategies
RMM	Risk Minimisation Measure
RMP	Risk Management Plan
RMS	Reference Member State
RSI	Referenced Safety Information
SAE	Serious Adverse Event
SAR	Serious Adverse Reaction
SDEA	Safety Data Exchange Agreement
SmPC	Summary of Product Characteristics
SMQ	Standardized MedDRA Query
SOC	System Organ Class
SOP	Standard Operating Procedure
TSSS	Tabular Summary of Safety Signals
WHO	World Health Organization
XEVIMPD	Extended EudraVigilance Investigational Medicinal Product Dictionary
XEVPRM	eXtended EudraVvigilance Product Report Message

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