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Dr Saranjit Singh National Institute of Pharmaceutical Education and Research
SAS Nagar 160 062 India
Setting Impurity Standards for APIs and Dosage Forms: An IP Perspective
Indian Pharmacopoeia
Available Edition: 1996Supplements: 2000, 2002 and 2005
Control of Impurities in IP 1996 and Supplements
Tests for Related Substances
Specific Tests for the Named Impurities
General Tests for Unnamed Impurities
Total Impurity limits
Test Design and Expression of Limits for Known and Unknown Impurities
IP 1996
Total number of monographs 1253Monographs with HPLC assay methods
139
Monographs with Test for Related Substances
448
TLC methods 391 HPLC methods 57
A Typical Example - TLC Method
Established: 9 December 2004
Indian Pharmacopoeia Commission
IPC
To bring new editions and supplements of Indian Pharmacopoeia at regular intervals
To accelerate the process of preparation, certification and distribution of IP reference substances
To develop understanding with International Pharmacopoeial agencies
Mandate of IPC
‘To promote the highest standards for drugs for use in humans and animals within practical limits of the technologies available for manufacture and analysis’
Vision Statement of IPC (Adopted 8 July 2006)
……..practical limits of technologies available for manufacture and analysis?
Why mention of:
Indian industry is fragmented into:
Indian multinationals Large Companies Medium sized Small scale
In total 5500 enterprises, with differences in technological capability for manufacture and analysis
Regulatory laboratory set-up is also fragmented:
Central Laboratories State Laboratories Approved Private Test Laboratories
Presently differ in technological capability for analysis, though Central/State Laboratories are being upgraded with same brands of state-of-art sophisticated analytical instruments under Capacity Building Project
Other local compulsions
Large population of the country ~1.2 billion
Very low gross national income ~$620 (US $41,400)
390 million live on less than $1 a day
Population below poverty line: 25-29%
80% of the health care payments borne by individuals
So important for the Government to ensure continued supply of medicines at an affordable cost
Drug Name Price in India
Price in Pakistan
Price in Indonesia
Price in US
Ciprofoxacin 500 mg (10s)
29.00 423.86 393.00 2352.35
Norfloxacin 400mg (10s)
20.70 168.71 130.63 1843.66
Diclofenac 50 mg (10s)
3.50 84.71 59.75 674.77
Source: OPPI website, 45 INR = 1$
Price comparison of some well known drugs in INR
In this scenario
The drug quality standards need to be rational, practical and simple
The products sold in the country presently comply to standards laid down in Indian Pharmacopoeia 1996, the monographs of which meet the above requirements
The perspectives of IPCon impurities in
pharmaceuticals in future editions of compendia
‘To give special attention to the methods of manufacture used by the indigenous industry in selecting the pharmacopoeial tests for monitoring the toxic impurities of the concerned drug.’
An objective of IPC (Adopted 8 July 2006)
Basic decisions of IPC on Impurities
Minimum change in existing monographs
For new monographs, impurity control directed to be a part of Related Substances test
Both TLC and HPLC methods acceptable
Stringent limit, if an impurity is toxic and/or named impurity is to be controlled (e.g., N,N-dimethylalinine in cloxacillin sodium, <20ppm)
Cont.…
IPC to take care that Related Substances test in new monographs received from industry has no barrier element
In all situations, the test must be possible in Government and Private Laboratories
Other perspectives of IPC on Impurities
“The use of chromatographic methods has been greatly extended to cope with the need for more specificity in assays and in particular, in assessing the nature and extent of impurities in ingredients and products”
IP 2007: INTRODUCTION
IP 1996 versus 2007
1996 2007Total number of monographs
1253 1253 -13 +257
= 1497
Monographs with HPLC assay methods
139 139+……
Monographs with test of Related Substances
448 448+~100
TLC methods 391 ~390
HPLC methods 57 57+~100
IP 2007 General Chapter on Impurities
5.5 Impurities This chapter provides guidance on the control of impurities in drug substances and formulated preparations. It applies mainly to totally synthetic organic medicinal substances and those substances obtained by synthetic modification of a naturally-produced precursor; it is not necessarily relevant to other organic substances e.g. those of plant or animal origin, biological and biotechnological products, inorganic substances and pharmaceutical excipients. It provides an approach to the setting of limits for impurities in articles for which the individual monographs do not provide either a test or specific limits.
An impurity is defined as any component of a drug substance for pharmaceutical use or of a drug product that is not the chemical entity that defines the substance, or in the case of a drug product, not an excipient in the product. It includes among other things, degradation products of the drug substance that may develop on storage and in the case of dosage forms, those that may also be formed during manufacture and storage.
Acceptance criteria for impurities in drug substances:
Each identified specified impurity
Not more than 0.5 per cent
Each unidentified impurity Not more than 0.3 per cent
Total impurities Not more than 1.0 per cent
Provided it has been determined that the impurities are not toxic. Higher limits may be set if scientifically justified.
General Chapter
Acceptance criteria for degradation products in drug products:
Each identified degradation product
Not more than 1.0 per cent
Each unidentified degradation products
Not more than 0.5 per cent
Total degradation products Not more than 2.0 per cent
Provided it has been determined that the impurities are not toxic. Higher limits may be set if scientifically justified.
General Chapter (cont…)
‘Although a primary objective of the Pharmacopoeia is to guarantee the identity, strength, purity and quality of official articles, it is not possible to include in each monograph a test for every impurity or contaminant or even an adulterant that might be present’
Viewpoints in the General Chapter
“The exclusion of a limit for impurities in a monograph does not absolve the manufacturer of providing assurance to the user on the safety of a drug.
It is incumbent on the manufacturer to follow good manufacturing practices (GMP) and to ensure the limitation of impurities based on knowledge of the properties of the chemical entity and the likelihood of related substances being associated with the end product during production and subsequent storage.”
Viewpoints in the General Chapter (cont..)
“Material found to contain an impurity not detectable by the prescribed tests of a monograph may be deemed to be not of pharmacopoeial quality particularly if the nature of the impurity(ies) found is not compatible with GMP.
In any case, the specifications should in course of time be refined to include tighter and more specific limits in the light of experience with production batches and a better understanding of the manufacturing process.”
Viewpoints in the General Chapter (cont..)
So, an overall perspective of IPC
CONTROL OF IMPURITIES is more stronger regulatory and GMP issue, than compendial
So only reasonable control in IP, except for those related substances that are known or even doubted to adversely influence safety of the product
What IPC aspires for
Information on impurities associated with side effects or toxic reactions, including genotoxicity, so that specific named tests can be added in existing or new monographs of Indian Pharmacopoeia
Simple tests for these impurities
Current Dynamics of
Indian Pharmaceutical
Industry
Top Indian Companies – Way Ahead
Export oriented Indian companies, which have world class facilities, completely comply to stringent International regulatory expectations on impurities
Some of the Indian companies have more than 600 HPLC systems, change 100 columns per day, and are equipped with most sophisticated instruments, like LC-MS, LC-NMR, etc., which are being used for impurity profiling and structure characterization
An Example of Maturity of Indian Industry
FDAnews Drug Daily BulletinNov. 16, 2007 | Vol. 4 No. 226
Generic Firm Commences Gabapentin Recall Due to Excessive Impurities
Ranbaxy Pharmaceuticals initiated a voluntary Class III recall of 73 million gabapentin tablets because the allowed level of impurities in the tablets exceeded their specification limits,
according to FDA documents.
Gabapentin is the active ingredient in Pfizer’s antiseizure drug Neurontin, which is off patent. The affected dosage strengths include the 600- and 800-mg tablets. Ranbaxy’s abbreviated new drug application (ANDA) for the tablet formulation is for those two strengths and the firm holds
approval for a capsule formulation as well.
The company could not comment on whether the recall will create a shortage of its tablets.
A Few Distinct Advantages
The drive of export-oriented Indian Pharma companies, to meet stringent quality and impurity control expectations of International agencies, has lead not only to creation of excellent facilities and trained manpower, it has been indirectly responsible for improvement of quality of pharmaceuticals sold within the country, as the same companies hold 70% share in the local market
This is happening without intervention of local pharmacopoeial and regulatory agencies
The Benefit of Indian System as a Whole
The Indian system encourages the big players, but it also protects medium and small scale enterprises, which are very much needed in the chain of supply of drugs to large population of the country with marked differences in paying capacities
Summing up…
For a country with >1.2 billion people
The priority is
AVAILABILITY of
GOOD QUALITY DRUGS at
AN AFFORDABLE COST
Our belief is…
GOOD QUALITY of drugs and products can be well
assured by recently adopted approach of IPC on impurities
Somehow…
We at IPC are not fully convinced
on the trend in USP, EP, BP, etc. on searching impurities in each and every
product, even old and well established, at ICH thresholds, which we consider is
guided more by protectionist approach of big players in Pharmaceutical industry
A glimpse of emerging standards….
European Pharmacopoeia 5.0, 2005
EP 5.0 (2005)(Ph Eur monograph 0906)
Due to tropical environmental conditions in India, it may not be reasonable to expect Industry to control individual degradation products in formulations at 0.1 or 0.15%
Moreover, a moot point….
If there is no emphasis on impurities in kilogram(s) and liters of food taken by an individual in a day
Then how come it is a so serious issue for few milligrams of drug(s) consumed in a tiny pill daily?
So overall,
1. There is a need to ponder whether the forensic analysis of pharmaceuticals is all that necessary
2. Something, which is real toxic and difficult for our bodies to handle, must be controlled but not every type of minutiae
3. The compendia require innovative thinking, wherein impurities are classified drug-wise as ‘toxic’ and ‘safe’, with emphasis only on those that might be harmful
4. Compendia must pursue policy of exclusion rather than inclusion, unlike the trend being pursued currently
Thanks so much