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England and Wales High Court (Patents Court) Decisions |
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You are here: BAILII >> Databases >> England and Wales High Court (Patents Court) Decisions >> Dr Reddy's Laboratories (UK) Ltd & Anor v Warner-Lambert Company LLC [2012] EWHC 3715 (Pat) (20 December 2012) URL: http://www.bailii.org/ew/cases/EWHC/Patents/2012/3715.html Cite as: [2013] RPC 31, [2013] WLR(D) 8, (2013) 130 BMLR 97, [2013] Bus LR 612, [2012] EWHC 3715 (Pat) |
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CHANCERY DIVISION
PATENTS COURT
Strand, London, WC2A 2LL |
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B e f o r e :
____________________
(1) DR REDDY'S LABORATORIES (UK) LTD (2) DR REDDY'S LABORATORIES LTD |
Claimants |
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- and - |
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WARNER-LAMBERT COMPANY LLC |
Defendant |
____________________
Ms Kelyn Bacon and Mr Max Schaefer (instructed by Arnold & Porter (UK) LLP)
for the Defendant
Hearing dates: 20, 21 and 22 November 2012
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Crown Copyright ©
Mr Justice Roth :
INTRODUCTION
THE LEGISLATIVE REGIME
Marketing Authorisation
Supplementary Protection Certificate (SPC)
"…the period that elapses between the filing of an application for a patent for a new medicinal product and authorisation to place the medicinal product on the market makes the period of effective protection under the patent insufficient to cover the investment to put into the research."
Since medicines, in particular those requiring lengthy and expensive research, will not be developed unless they have sufficient patent protection, there was also a concern that lack of extended protection would lead to the relocation of pharmaceutical research away to countries that offered better protection. As a result, some Member States introduced their own system of national SPCs and the EU regime was therefore also designed to introduce uniform protection across all Member States.
Paediatric extension
"The Paediatric Regulation was to encourage specific research – and dissemination of knowledge about its results - into already known medicines as to their applicability for children. Prior to the Regulation there was no specific incentive for such research. If you discovered a new medicine you could patent it. You could then get an SPC if there was delay in getting an MA. And that was that. There was no particular requirement or incentive for going on to investigate whether the medicine was suitable (or unsuitable) for children or had particular application for children. The Paediatric Regulation provides an incentive – an extra six months of protection - for having conducted such research."
"(1) Before a medicinal product for human use is placed on the market in one or more Member States, it generally has to have undergone extensive studies, including pre-clinical tests and clinical trials, to ensure that it is safe, of high quality and effective for use in the target population.
(2) Such studies may not have been undertaken for use in the paediatric population and many of the medicinal products currently used to treat the paediatric population have not been studied or authorised for such use. Market forces alone have proven insufficient to stimulate adequate research into, and the development and authorisation of, medicinal products for the paediatric population.
(3) Problems resulting from the absence of suitably adapted medicinal products for the paediatric population include inadequate dosage information which leads to increased risks of adverse reactions including death, ineffective treatment through under-dosage, non-availability to the paediatric population of therapeutic advances, suitable formulations and routes of administration, as well as use of magistral or officinal formulations to treat the paediatric population which may be of poor quality.
(4) This Regulation aims to facilitate the development and accessibility of medicinal products for use in the paediatric population, to ensure that medicinal products used to treat the paediatric population are subject to ethical research of high quality and are appropriately authorised for use in the paediatric population, and to improve the information available on the use of medicinal products in the various paediatric populations. These objectives should be achieved without subjecting the paediatric population to unnecessary clinical trials and without delaying the authorisation of medicinal products for other age populations.
…
(6) The establishment of a system of both obligations and rewards and incentives has proved necessary to achieve these objectives. …"
"'paediatric investigation plan' means a research and development programme aimed at ensuring that the necessary data are generated determining the conditions in which a medicinal product may be authorised to treat the paediatric population"
The scheme of the Paediatric Regulation
(i) The applicant draws up a draft PIP and submits it to the EMA (through the PDCO) for agreement: Article 15. Article 15(2) provides:"The paediatric investigation plan shall specify the timing and the measures proposed to assess the quality, safety and efficacy of the medicinal product in all subsets of the paediatric population that may be concerned. In addition, it shall describe any measures to adapt the formulation of the medicinal product so as to make its use more acceptable, easier, safer or more effective for different subsets of the paediatric population."(ii) The proposed PIP is assessed by the PDCO, which may request modifications to the plan. The PDCO then adopts an opinion, pursuant to Article 17(1):
"…as to whether or not the proposed studies will ensure the generation of the necessary data determining the conditions in which the medicinal product may be used to treat the paediatric population or subsets thereof, and as to whether or not the expected therapeutic benefits justify the studies proposed. When adopting its opinion, the Committee shall consider whether or not the measures proposed to adapt the formulation of the medicinal product for use in different subsets of the paediatric population are appropriate."(iii) The PDCO opinion is sent to the EMA which, subject to a procedure that entitles the applicant to have the opinion re-examined, adopts a decision annexing the PDCO opinion: Articles 18 and 25.
(iv) In its application for a marketing authorisation (whether a new authorisation or an authorisation of new indications) the applicant includes the decision of the EMA agreeing to the PIP and "results of all studies performed and details of all information collected in compliance with" the agreed PIP: Articles 7 and 8.
(v) The PDCO may be asked for its opinion as to "whether studies conducted by the applicant are in compliance with" the agreed PIP. That request may be made by the applicant prior to submitting its application for a marketing authorisation (ie stage (iv) above) or by the competent authority which has received the application: Article 23(2). The competent authority has to "take account" of the PDCO's opinion but is not bound by it: Article 23(3).
(vi) The competent authority which has received the application must verify that the PIP has been complied with: Article 23(1). This process is referred to as the "compliance check". However, although stage (v) above is optional, the parties agree that in practice the national competent authorities carry out the compliance check on the basis of an opinion to that effect from the PDCO.
(vii) If the compliance check is satisfied and a marketing authorisation (or extension to an existing authorisation) is granted, the results of all studies conducted in compliance with the PIP will be included in the summary of product characteristics ("SmPC"): Article 28(1); and the competent authority includes within the authorisation a statement indicating compliance with the PIP: Article 28(3).
(viii) If the application includes the results of all studies conducted in compliance with the PIP, the applicant receives a six-month extension to the SPC, but there is no such extension if the competent authority concludes that the studies do not conform with the PIP: Articles 36(1) and 24.
(ix) "Where there is a particular cause for concern", the competent authority as a condition for granting the marketing authorisation shall require that a risk management system be set up or that specific post-marketing studies be performed and submitted for review: Article 34(2). This provision continues:
"The risk management system shall comprise a set of pharmacovigilance activities and interventions designed to identify, characterise, prevent or minimise risks relating to medicinal products, including the assessment of the effectiveness of those interventions"
(a) Even where completion of the PIP does not lead to the authorisation of a paediatric indication, if the results of the studies made in compliance with the PIP are included in the SmPC and, if appropriate, the product information leaflet, that will entitle the applicant to the reward of a paediatric extension: Article 36(1), second para. This is explained in recital (28):"Because the reward is for conducting studies in the paediatric population and not for demonstrating that a product is safe and effective in the paediatric population, the reward should be granted even when a paediatric indication is not authorised. However, to improve the information available on the use of medicinal products in the paediatric population, relevant information on use in paediatric populations should be included in authorised product information."(b) The requirement to comply with a PIP can be waived by the EMA (on the advice of the PDCO) if it concludes that the product is likely to be ineffective or unsafe in all or part of the paediatric population, or that the disease or condition which the product is intended occurs only among adults, or that the product does not represent a significant therapeutic benefit over existing treatments for children. The applicant may apply for such a waiver or the PDCO may of its own motion advise that a waiver should be granted. The latter may be an important safeguard since the patentee would receive the significant benefit of a paediatric extension for seeking to establish whether the product can be used on children when it may be ascertainable at the outset that this would be inappropriate or unnecessary. See Articles 11-13.
(c) Provision is made for deferral of the initiation or completion of some or all of the studies in the PIP. Such a deferral may be requested by the applicant when submitting the proposed PIP or by the PDCO of its own motion. The conditions for a deferral are addressed below in the discussion of Dr Reddy's grounds of appeal.
THE PAEDIATRIC EXTENSION FOR ATORVASTATIN
Study Number |
Area | Subarea | Description |
1 | Clinical | Bioequivalence | Bioequivalence study of the final age-appropriate oral atorvastatin formulation to the existing atorvastatin formulation in healthy adult volunteers |
2 | Clinical | Pharmacokinetic, safety |
Steady-state, eight week pharmacokinetic study of atorvastatin in children and adolescents (aged 6 years to less than 18 years) with heterozygous familial hypercholesterolaemia using sparse PK sampling methodology and including flow-mediated artery dilatation assessments |
3 | Clinical | Safety | A 3-year study of the safety and follow-up study of efficacy of atorvastatin treatment of children and adolescents (aged 6 years to less than 18 years) with heterozygous familial hypercholesterolaemia |
"To provide data on the long-term follow-up of safety and efficacy in children and adolescents treated with Atorvastatin."
The study population is specified as at least 250 children and adolescents, of whom at least 50% are defined in terms which I was told means that they must be children under 11.
"The PDCO adopted a positive opinion that the studies conducted by the applicant are in compliance with the agreed PIP. The agreed PIP was fully completed."
"Furthermore, CHMP takes note that the agreed [PIP] is fully completed and that the PDCO issued an Opinion on Compliance. CHMP reviewed the paediatric data subject to this plan and the result of these studies reflected in the Summary of Product Characteristics and, as appropriate, the Package Leaflet."
"Whereas…
(3) It has been verified that the application includes the results of all studies performed and details of all information collected in compliance with the agreed [PIP].
(4) Therefore the application complies with the requirements laid down in point (a) of Article 7(1) of [the Paediatric Regulation]."
THE GROUNDS OF CHALLENGE
(1) The EMA acted ultra vires it powers under the Paediatric Regulation by approving a PIP that allowed Pfizer to defer completion of the third study. The circumstances in which studies in a PIP may be started but not finished are expressly defined by the Regulation and must be covered by a deferral under Article 20. No such deferral was applied for by Pfizer or granted in this case. Accordingly, the PIP was not lawfully approved under the Paediatric Regulation and Pfizer was therefore not entitled to the extension.(2) Pursuant to Article 45(3), a paediatric extension should be granted only when significant studies contained in the PIP have been completed. Here, none of the relevant bodies made an assessment as to whether either of the two studies which had been completed was significant; and, on the facts, they were clearly not significant.
(3) Even if, contrary to ground (1), it was legitimate for the EMA to approve a PIP that required the initiation but not the completion of the third study, pursuant to Article 36 Pfizer was not entitled to a paediatric extension unless it included, within its application for a marketing authorisation, the results of the completed third study.
The jurisdiction to revoke a paediatric extension
"The extension of the duration may be revoked if it was granted contrary to the provisions of Article 36 of the [Paediatric] Regulation …"
Ground 1
"Where an application under Article 7 or 8 includes the results of all studies conducted in compliance with an agreed paediatric investigation plan, the holder of the patent or supplementary protection certificate shall be entitled to a six-month extension of the [SPC]."
The foundation of Dr Reddy's argument is that in referring there to "an agreed paediatric investigation plan", Article 36(1) must mean a lawful PIP. In other words, if the EMA and PDCO do not have the power to approve the PIP in question, then compliance with it cannot properly entitle the applicant to the substantial reward of the extension. As Mr Brealey put it: "this case is about what is a lawful PIP".
"20(1). At the same time as the paediatric investigation plan is submitted under Article 16(1), a request may be made for deferral of the initiation or completion of some or all of the measures set out in that plan. Such deferral shall be justified on scientific and technical grounds or on grounds related to public health. In any event, a deferral shall be granted when it is appropriate to conduct studies in adults prior to initiating studies in the paediatric population or when studies in the paediatric population will take longer to conduct than studies in adults.
…
21(1) At the same time as the Paediatric Committee adopts a positive opinion under Article 17(1), it shall, of its own motion or following a request submitted by the applicant under Article 20, adopt an opinion, if the conditions specified in Article 20 are met, in favour of deferring the initiation or completion of some or all of the measures in the paediatric investigation plan."
"In certain cases, the Agency should defer the initiation or completion of some or all of the measures contained in a paediatric investigation plan, with a view to ensuring that research is conducted only when safe and ethical and that the requirement for study data in the paediatric population does not block or delay the authorisation of medicinal products for other populations."
"The paediatric investigation plan shall specify the timing and the measures proposed to assess the quality, safety and efficacy of the medicinal product in all subsets of the paediatric population that may be concerned. In addition, it shall describe any measures to adapt the formulation of the medicinal product so as to make its use more acceptable, easier, safer or more effective for different subsets of the paediatric population. "
It is with regard to those requirements that the PDCO adopts an opinion in accordance with Article 17(1):
"as to whether or not the proposed studies will ensure the generation of the necessary data determining the conditions in which the medicinal product may be used to treat the paediatric population or subsets thereof, and as to whether or not the expected therapeutic benefits justify the studies proposed."
"The inclusion in a marketing authorisation of the statement referred to in Article 28(3) shall be used for the purposes of applying paragraph 1 of this Article."
Ground 3
Ground 2
"1. By 26 January 2008, any paediatric studies already completed, by the date of entry into force, in respect of products authorised in the Community shall be submitted by the marketing authorisation holder for assessment to the competent authority.
The competent authority may update the summary of product characteristics and package leaflet, and may vary the marketing authorisation accordingly. …
2. All existing paediatric studies, as referred to in paragraph 1, and all paediatric studies initiated prior to the entry into force of this Regulation shall be eligible to be included in a paediatric investigation plan, and shall be taken into consideration by the Paediatric Committee when assessing applications for paediatric investigation plans, waivers and deferrals and by competent authorities when assessing applications submitted pursuant to Article 7, 8 or 30.
3. Without prejudice to the previous paragraph, the rewards and incentives of Articles 36, 37 and 38 shall only be granted provided that significant studies contained in an agreed Paediatric Investigation Plan are completed after the entry into force of this Regulation.
4. In consultation with the Agency, the Commission shall draw up guidelines to establish assessment criteria for the significance of studies for the purposes of applying paragraph 3."
"For the purpose of the application of Article 45(3), this statement shall also indicate whether significant studies contained in the agreed [PIP] have been completed after the entry into force of this Regulation."
That provision concerns the statement to be made by the competent authority within the marketing authorisation.
"No paediatric studies, as referred to in paragraph 1 [ie completed before the entry into force of the Regulation], which have at the date of entry into force of this Regulation already been submitted for assessment in the third country, shall be taken into consideration for the rewards and incentives provided for in Article 36, 37 and 38."
This was explained in the Commission's Explanatory Memorandum as follows:
"Pharmaceutical companies have, in some cases, already conducted clinical trials in children. However, frequently, the results of these studies have not been submitted to Competent Authorities and have not resulted in updates to product information. To deal with this issue, it is proposed that any studies completed before this proposed legislation is adopted will not be eligible for the rewards and incentives proposed for the EU. …"
"If studies, as referred to in paragraph 1, are included in an approved paediatric investigation plan they can be taken into consideration for the rewards and incentives provided for in Articles 36, 37 and 38, including when they have already been submitted for assessment in a third country."
"Any paediatric studies, as referred to in paragraph 1, which have at the date of entry into force of this Regulation already been submitted for assessment in a third country, shall not, on their own, be sufficient to qualify for the rewards and incentives provided for in Articles 36, 37 and 38."
"This amendment would run counter to the objective, central to this Regulation, of stimulating research into medicines for children. New paediatric research into substances which may already have paediatric indications covered by a patent or supplementary protection certificate (for instance, to extend the use of the product to other paediatric subpopulations or to better adapt it to the specific needs of children) would be discouraged. Moreover, it would discourage paediatric research by third parties (different holders of patents or supplementary protection certificates). This would also be difficult to reconcile with the purpose of the [SPC Regulation] which aims at giving sufficient protection to all research, including new applications of an existing product.
However, and in line with the purpose of this amendment, it is appropriate to clarify in the Regulation that the rewards associated with a completed agreed Paediatric Investigation Plan should only be triggered by research completed after entry into force of the Regulation. In this way, it will be ensured that any extension of the supplementary protection certificate or of market exclusivity under Articles 36 and 37 of this Regulation is based on new paediatric research."
This led to the introduction of Article 44(3) in the draft with wording that became Article 45(3) of the final Regulation.
"The Council cannot agree to the first part of the amendment, which relates to patents. A basic patent (protecting the molecule) covers all medicinal uses of the substance, hence it covers also any paediatric medicinal use. A specific paediatric patent only exists in the case of a so-called 'usage patent'. The Commission proposal prolongs the basic patent; in such circumstances it would be difficult to operate the 'non-cumulative' test set out in the first part of the amendment and it would go against the objective of stimulating innovation and research. However, consistent with the spirit of the amendment, the Council considers that there is a need to clarify that the rewards and incentives which resulted from completion of an agreed paediatric investigation plan should only be available if at least some significant research was completed after the entry into force of the Regulation."
"Significant studies contained in the agreed PIP have been completed after the entry into force of [the Paediatric Regulation]."
That appears to be the formal statement envisaged by Article 28(3). This suggests that the MHRA may have considered that Article 45(3) does apply in this case or, possibly, it included that statement out of an abundance of caution. However, whatever the explanation, the approach of the MHRA cannot affect the proper construction of the legislation.
"When carrying out its tasks, the Paediatric Committee shall consider whether or not any proposed studies can be expected to be of significant therapeutic benefit to and/or fulfil a therapeutic need of the paediatric population."
I accept that the criteria applicable under those provisions are different from the criteria for significance under Article 45(3) as set out in Part 4.2 of the Commission's Guidelines. Nonetheless, I am entirely satisfied for the reasons set out above that Article 45(3) is not of general application and does not apply when all the studies included in a PIP were initiated after the Paediatric Regulation came into force. I should add that although this is a question of the proper interpretation of the Paediatric Regulation, I see no need to refer this question to the European Court of Justice for a preliminary ruling.