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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 >> IVAX Pharmaceuticals (UK) Ltd v Chugai Seiyaku Kabushiki Kaisha [2006] EWHC 756 (Pat) (10 April 2006) URL: http://www.bailii.org/ew/cases/EWHC/Patents/2006/756.html Cite as: [2006] EWHC 756 (Pat) |
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CHANCERY DIVISION
PATENTS COURT
Strand, London, WC2A 2LL |
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B e f o r e :
____________________
IVAX PHARMACEUTICALS (UK) LTD |
Claimant and Part 20 Defendant |
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- and - |
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CHUGAI SEIYAKU KABUSHIKI KAISHA |
Defendant and Part 20 Claimant |
____________________
Mr H. Carr QC and Mr T. Powell (instructed by Bristows) for the Defendant and
Part 20 Claimant
Hearing dates: 14 March 2006 – 17 March 2006
____________________
Crown Copyright ©
The Honourable Mr Justice Kitchin:
Introduction
i) U.S. Patent 4,200,640 (“"640”");
ii) Japanese Patent Application 57 145 659 (“"659”")
The witnesses
Technical background
i) Fillers or diluents are used to add particular properties to a formulation such as bulk, improved compression, reduced segregation and to prevent over-granulation. Some commonly used diluents are lactose, microcrystalline cellulose and starch.
ii) Disintegrants are included to enhance or promote the break up of the tablet once taken by the patient. Some commonly used disintegrants are microcrystalline cellulose and starch.
iii) Binders are the active agents which provide the cohesive binding and deformation properties required to compress the formulation into tablet form. Binders are frequently hydrophilic polymers such as polyvinylpyrrolidone, methylcellulose and starch.
iv) Lubricants and glidants are used to ease the ejection of the tablet from the die, to prevent sticking of the tablets to the punches, and to prevent excess wear on the dies and punches. Glidants also improve the flow properties of the granules or powders during the manufacturing process.
The Patent
“"Nicorandil is also relatively stable in its crystalline form but it has been shown that if nicorandil is compressed into a tablet by routine procedures it becomes unstable and its content in the tablet is likely to experience a time-dependent decrease.”" (Page 2, lines 15-17).
“"In order to avoid this problem it is conventional practice to coat the nicorandil crystals with one or more fatty or waxy substances which are solid at ordinary temperatures before compressing the same into a tablet.”" (Page 2, lines 17-19)
“"The present invention has been accomplished on the basis of this finding and the method it proposes is entirely different from the conventional method of coating the nicorandil crystals with a normally solid fatty or waxy material.”" (page 2, lines 37-39).
and:
“"In addition to its ability to produce a stable nicorandil preparation, the method of the present invention has the advantage that it obviates the need to apply a coating on the nicorandil crystals and therefore that it does not require any coating apparatus or equipment.”" (page 2, lines 44-46).
1. A process for producing a stable nicorandil-containing pharmaceutical preparation which comprises mixing nicorandil with a saturated higher aliphatic acid or a saturated higher alcohol both of which are solid at ordinary temperatures, and formulating the mixture in a suitable dosage form.3. A process according to claim 1 or 2 wherein the saturated higher aliphatic acid is palmitic acid or stearic acid.
6. A process according to claim 1 or 2 wherein the saturated higher aliphatic acid and/or the saturated higher alcohol both of which are solid at ordinary temperatures is present in an amount of at least 0.5% of the total weight of the nicorandil-containing preparation.
The skilled addressee
Common general knowledge
“"A. …..I would use it every time if I could
Q. You would?
A: If I could use it I would use it…..
Q. So the position is that we are agreed that you would only move away from magnesium stearate if you were forced to?
A. Yes. I have not disagreed with that in my witness statement.”"
i) Changing to a different form of the active ingredient; so, for example, if the active ingredient was a base, then a salt form of the drug could be used;
ii) Changing the manufacturing process and instead of using wet granulation using a non aqueous granulating fluid, such as ethanol or using direct compaction;
iii) Drying all the excipients before use;
iv) Ensuring that all the equipment in the manufacturing process was dry before use;
v) Coating the individual drug crystals with a polymer such as ethyl cellulose;
vi) Improving the packaging of the final formulation by using foil wrappers, blister packs or adding a dessicant.
Obviousness - the unamended claims
i) Identify the inventive concept of the claim;ii) Identify the common general knowledge of the skilled team;
iii) Identify the difference(s) between the prior art under consideration and that in the inventive concept of the claim;
iv) Ask whether the difference(s) would have been obvious or required invention.
The inventive concept
Obviousness over 640
“"by a conventional way into a pharmaceutical composition in the form of a tablet, granule, powder, capsule, suspension, parenteral injection, suppository or the like.”" (Column 3, line 65 to column 4, line 1).
“"… the object compound may be mixed with one or more pharmaceutical carriers such as lactose, starch, mannitol, kaolin, crystalline cellulose, talc, calcium carbonate, magnesium stearate or the like.”" (Column 4, lines 2-6).
i) The skilled addressee would have known that stearic acid was not just one of a number of lubricants, it was second only to magnesium stearate as the lubricant to use in excipient compatibility tests. Without invention he could (and probably would) select it as one of the two lubricants to use in pre-formulation. The other would be magnesium stearate.
ii) If magnesium stearate failed materially so as to render it unsuitable to go forward to formulation then plainly stearic acid would be obvious.
iii) But, even if it did not fail, stearic acid would (on the premises of the Patent) not have failed. There was no technical reason why it could not have been used as a lubricant.
iv) It was therefore a matter of choice rather than invention whether the skilled man chose to go forward with stearic acid as opposed to magnesium stearate.
i) All courses of action which present themselves without the exercise of invention are obvious: Brugger v Medicaid [1996] RPC 635 at 661.
ii) Evidence as to what the skilled person could or would have done can be relevant, but, at the end of the day, the key question is whether something in the claim was technically obvious in the light of the disclosure relied upon: Hallen v Brabantia [1991] RPC 195 at pp.211-212 (CA); Pharmacia v Merck [2001] EWCA Civ 1610; [2001] RPC 41 at [122]; Asahi Medical v Macopharma [2002] EWCA Civ 466 at [26] - [27].
iii) Whether or not there is a reason for taking the step from the prior art may be an important consideration, but it is not an essential requirement of a conclusion of obviousness: Pharmacia v Merck at [124].
iv) Care must be taken in suggesting that a particular route was “"obvious to try”". All will depend upon the facts of the case. So, for example, mere possible inclusion of something in a research programme on the basis you will find out more and something might turn up is not enough: St Gobain v Fusion Provida [2005] EWCA Civ 177 at [35]. But that does not mean that in every case the decision whether a claimed invention was obvious can be determined by deciding whether there was a reasonable expectation that a person might get a good result from trying a particular avenue of research: Pfizer’'s Patent [2002] EWCA Civ 1 at [57];
v) If the claimed invention is obvious for one purpose then an added and unexpected benefit, however great, will not found a valid patent: Hallen v Brabantia at p.216.
“"Q. There would be nothing unconventional in selecting stearic acid as your second lubricant?”"
A. No; no.
Q. If any adverse reaction was seen with magnesium stearate, either in pre-formulation or in this grey area ----
A. Yes, yes.
Q. ---- of early formulation, it would be entirely rational, would it not, to carry on with the stearic acid?
A. If you did spot their incompatibility, this is a question we have also had (or was in the report) about what was the degree of that degradation. As we pointed out, there are many things that are susceptible to attack with magnesium stearate which have been successfully formulated. So putting all that aside as well, yes, what you say is correct.
Q. If no adverse reaction was seen with magnesium stearate, you would want to proceed with that one?
A. Yes.
Q. Because it is perceived to be a better lubricant?
A. Yes.
Q. And it has lower cost?
A. I do not know about the cost, to be honest.
Q. You do not worry about cost?
A. No.
Q. You are an academic, wonderful.
A. Exactly, yes.
Q. You can understand that those in industry might have an interest in cost?
A. I could not tell you what the cost is.
Q. Fine. So if no adverse reaction was seen with both magnesium stearate and stearic acid ----
A. Yes.
Q. ---- there would be no technical reason for rejecting stearic acid on the basis that it would not do the job as a lubricant?
A. It is known to be, as we have discussed, less of a lubricant, so if there was no reaction with either, I firmly believe that most formulators would have chosen magnesium stearate.
Q. That was not quite the question I asked you. Let me try again.
A. OK.
Q. What I hope I said is that there would be no technical reason for rejecting stearic acid on the basis that it would not do the job ----
A. No, there is not.
Q. ---- of a lubricant?
A. Correct. Sorry, that is correct.
Q. That is fine. If you went ahead with stearic acid, as opposed to magnesium stearate, I think we have discussed how you would go ahead regardless of whether you call it pre-formulation or formulation?
A. Yes.”"
“".. if magnesium stearate showed incompatibility for any reason or if it was not possible to produce a stable formulation using magnesium stearate, stearic acid would be the next choice of lubricant.”"
Obviousness over 659
“" … tablet making was attempted with gradually increasing amounts ranging from a few times to ten-odd times the usual amount of a lubricant, such as magnesium stearate for example, which is generally used with a view to reducing the friction between particles on compression moulding a powder, but still no improvement was observed.”" (Page 4, first paragraph)
“"What we found is that you put magnesium stearate in there, you put increasing amounts of magnesium stearate in, and we would get no improvement in the stability. So you then get the stearyl alcohol, dissolve it in chloroform, either spray it on or put it in a mixture, remove the alcohol and we get a stable compound; right? Fine. I am saying that the reason we have had to go to those lengths is because of the total different nature of the two materials that you are using.”"
The proposed amendment
“"A process for producing a stable nicorandil-containing pharmaceutical preparation which comprises mixing nicorandil with palmitic or stearic acid present in an amount of at least 3% of the total weight of the nicorandil-containing preparationa saturated higher aliphatic acid or a saturated higher alcohol both of which are solid at ordinary temperatures,and formulating the mixture in a suitable dosage form”"
“"The decision as to whether there was an extension of disclosure must be made on a comparison of the two documents read through the eyes of a skilled addressee. The task of the Court is threefold:
(a) To ascertain through the eyes of the skilled addressee what is disclosed, both explicitly and implicitly in the application.
(b) To do the same in respect of the patent as granted.
(c) To compare the two disclosures and decide whether any subject matter relevant to the invention has been added whether by deletion or addition.
The comparison is strict in the sense that subject matter will be added unless such matter is clearly and unambiguously disclosed in the application either explicitly or implicitly.”"
“"Whether or not the adding of an undisclosed feature limiting the scope of protection conferred by the patent as granted would be contrary to the purpose of Article 123(2) EPC to prevent an applicant from getting an unwarranted advantage by obtaining patent protection for something he had not properly disclosed and maybe not even invented on the date of filing of the application, depends on the circumstances. If such added feature, although limiting the scope of protection conferred by the patent, has to be considered as providing a technical contribution to the subject-matter of the claimed invention, it would, in the view of the Enlarged Board, give an unwarranted advantage to the patentee contrary to the above purpose of Article 123(2)EPC. Consequently, such feature would constitute added subject-matter within the meaning of that provision. A typical example of this seems to be the case, where the limiting feature is creating an inventive selection not disclosed in the application as filed or otherwise derivable therefrom. If, on the other hand, the feature in question merely excludes protection for part of the subject-matter of the claimed invention as covered by the application as filed, the adding of such feature cannot reasonably be considered to give any unwarranted advantage to the applicant. Nor does it adversely affect the interests of third parties (cf. paragraph 12 above). In the view of the Enlarged Board, such feature is, on a proper interpretation of Article 123(2)EPC, therefore not to be considered as subject-matter extending beyond the content of the application as filed within the meaning of that provision.”"
Saturated Higher Aliphatic Acid | Additional Organic Acid | |
Example 1 | stearic acid 8% | - |
Example 3 | palmitic acid 3% | - |
Example 4 | stearic acid 16% | - |
Example 5 | stearic acid 8% | fumaric acid 10% |
Example 7 | palmitic acid 2% | salicylic acid 5% |
Example 8 | stearic acid 4% | fumaric acid 85.5% |
“"Surprisingly enough the solution of this object has been achieved, when nicorandil was mixed witha saturated higher aliphatic acidpalmitic acid or stearic acid present in an amount of at least 3% of the total weight of the nicorandil-containing preparation or a saturated higher alcoholboth ofwhichareis solid at ordinary temperatures, and optionally with fumaric acid, oxalic acid, salicylic acid, tartaric acid and/or glutaric acid, leading to a nicorandil preparation having remarkably improved stability by compressing the mixture into tablets.”"
“"The present invention has been accomplished on the basis of this finding and the method it proposes is entirely different from the conventional method of coating the nicorandil crystals with a normally solid fatty or waxy material. In one aspect, the present invention relates to a method for producing a stable nicorandil preparation by mixing nicorandil with at least 0.5% (on the basis of the weight of the preparation) ofa saturated higher aliphatic acid ora saturated higher alcoholboth ofwhichareis solid at ordinary temperatures, and optionally with at least 0.1% (on the basis of the weight of the preparation) of fumaric acid, oxalic acid, salicylic acid, tartaric acid and/or glutaric acid.”"
Obviousness – proposed amended claim 1
Obviousness over 640
Obviousness over 659
Conclusion
i) Claims 1, 3 and 6 of the Patent as granted are invalid for obviousness, but would have been infringed.
ii) The amendments are not allowable.
iii) Claim 1 as proposed to be amended would not have been invalid for obviousness and would have been infringed.