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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 >> Actavis & Ors v Eli Lilly And Company [2016] EWHC 1955 (Pat) (10 August 2016) URL: http://www.bailii.org/ew/cases/EWHC/Patents/2016/1955.html Cite as: [2016] EWHC 1955 (Pat) |
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Case No: HP-2015-000012 Case No: HP-2015-000048 Case No: HP-2015-000062 |
CHANCERY DIVISION
PATENTS COURT
7 Rolls Building Fetter Lane London EC4A 1NL |
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B e f o r e :
____________________
ACTAVIS GROUP PTC EHF (A company incorporated under the laws of the state of Iceland) |
Claimant in HP-2014-000040 |
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- and - |
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ACTAVIS UK LTD |
Fourth Party in HP-2014-000040 |
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ACTELION PHARMACEUTICALS LTD (a company incorporated under the laws of the state of Switzerland) |
Claimant in HP-2015-000012 |
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- and - |
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ACTELION PHARMACEUTICALS UK LIMITED |
Fourth Party in HP-2015-000012 |
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(1) TEVA UK LIMITED (2) TEVA PHARMACEUTICAL INDUSTRIES LIMITED (a company incorporated under the laws of Israel) |
Claimants in HP-2015-000048 |
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- and - |
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GENERICS (UK) LIMITED (TRADING AS MYLAN) |
Claimant in HP-2015-000062 |
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ICOS CORPORATION (a company incorporated under the laws of the state of Washington, USA) |
Defendant |
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- and - |
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ELI LILLY AND COMPANY (a company incorporated under the laws of Indiana, USA) |
Third Party |
____________________
Andrew Waugh QC, Thomas Hinchliffe QC, Katherine Moggridge (instructed Simmons & Simmons LLP) appeared for the Defendant and Third Party.
Thomas Mitcheson QC also appeared for the Defendant and Third Party
Hearing dates: 15th - 17th, 20th - 24th, 29th, 30th June and 1st July
____________________
Crown Copyright ©
Mr Justice Birss
Topic | Paragraph |
Introduction | 1 |
The issues | 5 |
The witnesses | 32 |
Technical Background | 53 |
The 181 Patent | 72 |
The skilled person and the common general knowledge – 181 | 72 |
The 181 patent specification | 99 |
Claim construction - 181 | 117 |
Priority -181 | 138 |
The priority document | 143 |
Is the Named Compound tadalafil? | 160 |
What are compounds 1 to 5? | 192 |
Ranges | 211 |
Priority overall | 228 |
Added matter - 181 | 235 |
Novelty - 181 | 238 |
Obviousness – 181 | 257 |
Obviousness – the facts | 287 |
Insufficiency - 181 | 343 |
Infringement - 181 | 346 |
The 092 Patent | 357 |
The skilled person and the common general knowledge – 092 | 357 |
The 092 patent specification | 377 |
Claim construction - 092 | 385 |
Priority -092 | 392 |
Added matter - 092 | 395 |
Novelty - 092 | 400 |
Obviousness – 092 | 410 |
Insufficiency - 092 | 459 |
Claims limited by pharmacokinetic properties | 460 |
Claim 12 | 468 |
Claims 1 to7 – particle size distribution | 469 |
Infringement - 092 | 490 |
Conclusion | 491 |
Annex 1 – relevant claims of the 181 patent | Annex 1 |
Annex 2 – relevant claims of the 092 patent | Annex 2 |
Introduction
The issues
A pharmaceutical unit dosage composition comprising 1 to 5 mg of a compound having the structural formula:
said unit dosage form suitable for oral administration up to a maximum total dose of 5 mg per day.
A free drug particulate form of a compound having a formula
and pharmaceutically acceptable salts and solvates thereof in which the compound is present as solid particles not intimately embedded in a polymeric co-precipitate, wherein at least 90% of the particles have a particle size of less than about 40 microns.
i) Lilly accepts claims 16, 17 and 18 lose priority. They are Swiss form use claims dependent on claims 8 and 9. They stand or fall with claims 8 and 9.
ii) The two notional claims encompassed by claim 19 are distinct. Insofar as claim 19 is dependent on claims 13-15 then, if priority is lost, Lilly accepts that notional claim lacks novelty. Insofar as claim 19 is dependent on claims 16-18 then, by virtue of the dependencies of those claims, claim 19 will include the features in claims 8-9 (for which the issue is the inevitability of the pharmacokinetics). That notional claim is not entitled to priority and it stands or falls with claims 8-9. If one of the two notional claims encompassed by claim 19 is valid and the other invalid, an amendment to the claim dependencies will be needed under s63.
i) Claims 8, 9, and 16 – 19 are too broad because they are limited by pharmacokinetics and not by particle size. There was also a squeeze on inevitable result.
ii) The therapeutic indication claims 12 - 19 gave rise to two points but by closing only one was live. There had been a squeeze on disclosure/enablement as between Oren and 092 but this was dropped after Lilly accepted that the 092 claims (save for those dependent on claims 8-9) would lack novelty over Oren if they lose priority. The live argument is about claim 12. The claimants say it is either too broad or so ambiguous so as to be insufficient.
iii) The particle size feature in claim 1-7 raises an ambiguity insufficiency. The issue is about characterising particle size by volume or by number. Lilly contends the claim means volume. The claimants contend the claim covers either volume or number or both and if so is truly ambiguous.
The witnesses
Technical background
Erectile dysfunction
The role of phosphodiesterases in erectile dysfunction
Potency and selectivity
Measurement of Erectile Function
IIEF Q3 When you attempted intercourse, how often were you able to penetrate (enter) your partner?
IIEF Q4 During sexual intercourse, how often were you able to maintain your erection after you had penetrated (entered) your partner?
0 – Did not attempt intercourse
1 – Almost never or never
2 – A few times (less than half the time)
3 – Sometimes (about half the time)
4 – Most times (more than half the time)
5 – Almost always or always
Formulation
Bioavailability
The 181 patent
The skilled person and the common general knowledge – 181
i) The phases of clinical research
ii) Minimal effective dose
iii) Sildenafil
iv) Second in class
v) Chronic dosing
The phases of clinical research
Minimum effective dose
Sildenafil
Second in class
Chronic dosing
Stereochemistry
The 181 patent specification
"[0009] Significantly, applicants' clinical studies also reveal that an effective product having a reduced tendency to cause flushing in susceptible individuals can be provided. Most unexpectedly, the product also can be administered with clinically insignificant side effects associated with the combined effects of a PDE5 inhibitor and an organic nitrate. Thus, the contraindication once believed necessary for a product containing a PDE5 inhibitor is unnecessary when Compound (I) is administered as a unit dose of about 1 to about 20 mg, as disclosed herein. Thus, the present invention discloses an effective therapy for sexual dysfunction in individuals who previously were untreatable or suffered from unacceptable side effects, including individuals having cardiovascular disease, such as in individuals requiring nitrate therapy, having suffered a myocardial infarction more than three months before the onset of sexual dysfunction therapy, and suffering from class 1 congestive heart failure, or individuals suffering from vision abnormalities.
[0010] The present invention relates to Compound (I) in a unit dosage form. That is, the present invention relates to a pharmaceutical unit dosage form suitable for oral administration comprising about 1 to about 5mg Compound (I)."
Claim construction - 181
Up to a maximum total dose of 5 mg per day
"1. As regards the significance of the Warner-Lambert (pregabalin) case, the facts in that case were that the infringing directions were left out (ie carved out) of the label and the alleged infringing use for pain was 'off-label'. (ie the patented use pregabalin for pain was excluded from the label).
2. In the current case, the on-label use infringes where the direction on the 2.5mg and 5mg tablet Patient Information Leaflets is to use of the 2.5mg and 5 mg tablets up to a maximum daily dose of 5mg.
3. The use of the 2.5mg and 5mg tablets at higher doses (greater than 5mg) for daily use is not indicated on the PILs nor is their use at lower doses (5mg or less) for on demand use though even if the latter were used, this would still take advantage of the fact that at the doses of 5mg and lower there is efficacy to treat but with minimal side effects akin to placebo."
(numbering added)
Priority -181
(a) to read and understand, through the eyes of the skilled person, the disclosure of the priority document as a whole;
(b) to determine the subject matter of the relevant claim;
(c) to decide whether, as a matter of substance not of form, the subject matter of the relevant claim can be derived directly and unambiguously from the disclosure of the priority document.
The priority document
"The package insert also provides instructions to administer one or more 1 to 20 mg dosage forms as needed up to a total dose of 20 mg per day. Preferably, the dose administered is 5 to 20 mg/day; more preferably 5 to 15 mg; and most preferably a 10 mg dose form administered once per day, as needed."
"One such inhibitor, (6R-trans) -6- (1, 3-benzodioxol-5-yl) - 2, 3, 4, 7, 12, 12a - hexahydro-2-methyl-pyrazino [1',2':1,6]-pyrido [3,4-b] indole-1,4-dione, was demonstrated in human clinical studies to have minimal impact on systolic blood pressure when administered in conjunction with nitrates. By contrast sildenafil demonstrates a 4 fold greater decrease in systolic blood pressure over placebo, which leads to the contraindications and warnings in certain patients."
The data in Table 1 indicate that a compound of Formula (I), wherein R1 is hydrogen or C1-6 alkyl, R2 is
and R3 is hydrogen; is especially preferred. Preferably A is
Is the Named Compound tadalafil?
"Fused rings. In simple cases the relative stereochemistry of substituted fused-ring systems can be designated by the methods used for monocycles. For the absolute stereochemistry of optically active and racemic compounds the sequence-rule procedure can be used in all cases (see Rule E-4.9 and Appendix 2); for relative configurations."
"E-3.1. Steric relations at saturated bridgeheads common to two rings are denoted by cis or trans. followed by a hyphen and placed before the name of the ring system, according to the relative positions of the exocyclic atoms or groups attached to the bridgeheads. Such rings are said to be cis-fused or trans-fused."
What are Compounds 1 to 5?
Ranges
i) Page 3 ln 6-7 which mentions dosage forms at dosages between 1 and 20 mg/dosage form;
ii) The passage bridging pages 6 and 7 which I have quoted already but will repeat:
"The package insert also provides instructions to administer one or more 1 to 20 mg dosage forms as needed up to a total dose of 20 mg per day. Preferably, the dose administered is 5 to 20 mg/day; more preferably 5 to 15 mg; and most preferably a 10 mg dose form administered once per day, as needed."
iii) Example 4 in which the Study drug (tadalafil) was given to healthy volunteers at 10mg per day;and
iv) Example 5 which describes Compound 5 (which might or might not be tadalafil) with 5 to 20 mg doses and 10 to 100 mg doses in which 10 mg being preferred.
"123. Where a priority document discloses a numerical range from which the patent claims a sub-range, the appropriate forensic question is whether the sub-range is a novel one. If it is not, then it merely forms part of the disclosure of the priority document, and the claim to the sub-range is entitled to priority."
"8.4 If the invention claimed in a later European patent application constitutes a so-called selection invention– i.e. typically, the choice of individual entities from larger groups or of sub-ranges from broader ranges of the numerical values - in respect of the subject matter disclosed in the first application this priority is claimed, the criteria applied by the EPO with a view to assessing novelty of selection inventions over the prior art must also be considered carefully when assessing whether the claim in the European patent application is in respect of the same invention as the priority application within the meaning of Article 87(1) EPC. Otherwise, patent protection for selection inventions, in particular in the field of chemistry, could be seriously prejudiced if these criteria were not thoroughly complied with when assessing priority claims in respect of selection inventions. Hence, such priority claims should not be acknowledged if the selection inventions in question are considered "novel" according to these criteria."
(Lilly's emphasis)
Priority – overall
"The principle applicable to purpose limited medical use claims must be that the material relied on to establish plausibility must be both sufficiently specific, and have a sufficient breadth of application, to fairly support the claim both in terms of the nature of the agent claimed to have an effect, and in terms of the effect claimed."
Added matter - 181
Novelty - 181
Obviousness – 181
"31. Accordingly on the basis of Eisai alone we would hold that Swiss form claims are allowable where the novelty is conferred by a new dosage regime or other form of administration of a substance.
32. So holding is far from saying that in general just specifying a new dosage regime in a Swiss form claim can give rise to a valid patent. On the contrary nearly always such dosage regimes will be obvious – it is standard practice to investigate appropriate dosage regimes. Only in an unusual case such as the present (where, see below, treatment for the condition with the substance had ceased to be worth investigating with any dosage regime) could specifying a dosage regime as part of the therapeutic use confer validity on an otherwise invalid claim."
"… the motive for defending these patents is straightforward. It is to recover in respect of and provide the incentive for the expensive and uncertain research programmes that are entailed in getting a drug to market for the benefit of patients. There is, … far, far more involved in getting a safe and efficacious drug to the patient than just finding the molecule. And in that lengthy and costly process there is every reason to reward the results of that research and development programme."
"When Mr Thorley was asked what policy reason there should be for on the one hand allowing Swiss form second medical treatment claims for different diseases but not allowing them for the same disease, the only answer he could devise was that the treatment might cost more. Why, he said, should you have to pay more for a 1mg pill than for an out of patent 5mg pill? The reason is obvious – the 1mg pill has only come about because of expensive unpredictable research. Patented things often cost more. And the reason is because the monopoly has been given as result of the research which led to it. Research into new and better dosage regimes is clearly desirable – and there is simply no policy reason why, if a novel non-obvious regime is invented, there should not be an appropriate patent reward. Such a reward cannot extend to covering the actual treatment but a Swiss form claim which specifies the new, inventive, regime is entirely in accordance with policy."
"113. Where, therefore, the evidence reveals that to arrive at the invention, the skilled person has to embark on an experiment or series of experiments where there was no fair expectation of success, the conclusion will generally be that the invention was not obvious. Mr Thorley submitted that one had to distinguish between experiments which were conducted in order to make an informed decision as to what to do, and experiments which are conducted only because it is believed that they will produce the desired end result. The former type could be obvious experiments to do, notwithstanding that they were performed without any prior knowledge of the result, or whether the result would predict a successful outcome of the whole project. There was an independent motive for driving the project forward, namely to find out whether a solution to the problem was possible.
114. I think that the guiding principle must be that one has to look at each putative step which the skilled person is required to take and decide whether it was obvious. Even then one has to step back and ask an overall question as to whether the step by step analysis, performed after the event, may not in fact prove to be unrealistic or driven by hindsight. Thus to return for a moment to the facts of this case, both sides are agreed that there is nothing per se inventive in embarking on in vitro pre-formulation testing to determine the physico-chemical characteristics of the API. Such tests would be performed in ignorance of the results of the testing and in ignorance of whether any particular formulation strategy would have a fair expectation of success. But they would nevertheless be an obvious thing to do. They are obvious because the evidence shows that the skilled person would do them anyway, as part of his routine work.
115. How one would proceed after purely routine steps have been performed may involve more in the way of a value judgment. The mere fact that further steps can be characterised as being performed in order to make an informed decision cannot prevent those steps from contributing to a finding of inventiveness."
"The question of obviousness must be considered on the facts of each case. The court must consider the weight to be attached to any particular factor in the light of all the relevant circumstances. These may include such matters as the motive to find a solution to the problem the patent addresses, the number and extent of the possible avenues of research, the effort involved in pursuing them and the expectation of success."
Obviousness – the facts
i) The phase I studies would show that the maximum tolerated doses for tadalafil would be 500mg in a single dose and 100mg daily dosing.
ii) The routine testing so far would have shown that tadalafil has a higher IC50 against PDE6 than sildenafil. That is an indication to the skilled team that tadalafil may have fewer visual disturbance side effects than sildenafil.
iii) Although the potency (IC50) for tadalafil against PDE5 is reported in Daugan as 2 nM, the skilled team would measure it themselves. They might get a value of between about 2 to 2.5 nM (2.5 nM is the value reported in the 181 patent).
iv) The routine testing would include pharmacokinetics and this would have revealed that tadalafil has a half-life of 17.5 hours, which is much longer than sildenafil (4 hrs). The claimants say this would indicate that chronic daily dosing should be tried. I will consider that below.
v) Another pharmacokinetic parameter which would be identified is the mean accumulation ratio which would be between 1.59 and 1.96 with the higher ratio at lower doses (10mg).
vi) The molecular weight of tadalafil would be known (not by testing). The claimants submit that this would demonstrate that the molecular weights of tadalafil and sildenafil have a ratio of about 5:4. The ratio is not in dispute but this point is relevant to a free standing issue about the obviousness of a 5mg dose which I will consider below.
"Taking [the pharmacokinetic data] into account, the skilled clinician would have counselled the skilled team that a 50mg dose would be the best targeted starting dose to assess safety, tolerability and efficacy. The skilled clinician would discount the 100mg, due to its unfavourable side effect profile (100% occurrences of musculoskeletal pain and myalgia are not clinically acceptable). The skilled clinician would not select a dose as low as 10 mg because as compared to the 10 mg doses the 50mg dose demonstrated significantly higher drug concentrations, making efficacy more likely. Also, based on this study, the 50mg dose appears to have an equivalent (and in some cases more favourable) side effect profile than the 10mg dose."
"So a paper exercise, that is absolutely fine and dandy, but that is not how it goes in real life."
[T5/640/25-641/3]
"Q. And so what I am suggesting to you, these three factors that the skilled person would positively know about would lead the skilled person to know that there may be other factors that could go one way or the other, but as a starting point on your approach a skilled person without any efficacy data at all would believe that rough and ready the 25 mg of sildenafil should equate to about a 5 mg of tadalafil.
A. Using these criteria only as a paper exercise, yes.
Q. One thing we can say for sure is that he would certainly predict doses below 20 mg would be efficacious. Yes?
A. Yes."
Daily dosing rather than on demand dosing?
Considering the programme as a whole and obviousness overall.
i) In terms of motives to find a solution to the problem the patent addresses, the skilled team would be highly motived by Daugan and the success of sildenafil to investigate tadalafil as a treatment for erectile dysfunction.
ii) As for possible avenues of research, overall tadalafil would be obvious to investigate. In terms of doses however, 5 mg/day is a significantly lower dose than the 50 mg dose exemplified in the Daugan prior art and the marketed doses of sildenafil. It is also significantly lower than the 50 mg dose which would be chosen for the first test of efficacy at Phase IIa. It would not be chosen in the routine first dose ranging study. The team would not have anticipated daily dosing as something to be studied from the outset but once the half-life was discovered it is likely that daily dosing would be included.
iii) In terms of effort, overall the programme would involve very substantial resources of time, money and people but it would be pursued. However, by the time the idea of investigating lower doses presents itself, the team would have established safe, tolerable and effective doses of tadalafil at 25mg on demand and 10 mg for daily dosing. At that stage the impetus to investigate lower doses would be reduced but not eliminated.
iv) Expectations of success can be considered overall and in relation to particular studies. Overall the team would embark on the project with a reasonable expectation of success in establishing tadalafil as a safe, tolerable and effective treatment for tadalafil. However, the claimants failed to prove that efficacy at 5mg tadalafil was predictable or worth considering by the skilled team based on the properties of tadalafil as compared to sildenafil. The team would know that in principle there would be a minimum effective dose for tadalafil but would also know that its definition depends on a value judgment made by the team. In relation to the dose ranging studies, the team would conduct them hoping for a dose response. Following discovery of a plateau starting at 25 mg or 10mg, there would very likely be a subsequent dose ranging study which included 5 mg. The team would include a 5 mg dose in this study hoping to see a dose response but that does not mean they would have a reasonable expectation that 5mg would produce a clinically relevant effect at all nor one with minimal side effects. Assuming a 5 mg /day dose of tadalafil was tested, it would not be tested with a reasonable expectation of success.
v) Considering unexpected or surprising results, the position is as follows. The path to a 5 mg dose requires the discovery of new information such as the half life and the IC50 vs PDE6. That information would inevitably be found in any clinical programme. The path includes an important result which is unexpected even if it is not actually surprising, i.e. the plateau in the dose response from 10 to 100 mg. There is also a surprising result: the existence of a useful effect with reduced side effects. The claimed 5mg /day dose has that property.
vi) A number of value judgments would be required of a skilled team in a programme which reaches the claimed invention. One is to define the level of clinical effect to be regarded as relevant. Another is to embark on investigating daily dosing. An important value judgment is what to do when an unexpected plateau in the dose response has been identified at the same time as a marketable dose.
Insufficiency - 181
Infringement - 181
"56. The principle I derive from these authorities is that the question the court is asking in every case is whether, viewed in all the relevant circumstances, there was a sufficiently strong probability that an injunction would be required to prevent the harm to the claimant to justify bringing the proceedings. In adding the word sufficiently to the word strong I do not mean to put a gloss on the words of Chadwick LJ [in Lloyd v Symonds [1998] EWCA Civ 511], rather I am seeking to encapsulate the idea that the degree of probability required will vary from case to case depending on all the circumstances but that mere possibilities are never enough. To justify coming to court requires there to be a concrete, strong and tangible risk that an injunction is required in order to do justice in all the circumstances.
57. If a defendant really does, at the date of the proceedings, have no intention to do the act then in the majority of cases that will be conclusive of the question whether there was a sufficiently strong probability to justify proceedings. (e.g. London Borough of Islington). However it seems to me that the question is not confined to the defendant's subjective intentions. A defendant's overt acts must be capable of being relevant. To take an extreme case, if a man began taking actual preparatory steps to commit some unlawful act seriously damaging to the claimant and in infringement of the claimant's rights and did so in full view of the claimant and well aware that the claimant could see them, he could hardly complain if the claimant started proceedings and the court decided to grant a final injunction to prevent it. A statement at trial that he had never intended to go through with it would get short shrift.
58. I bear in mind that intentions are not necessarily simple. A state of mind need not merely be either one thing or another. Also in this case the defendants are corporate entities to whom an intention can only be imputed."
The 092 patent
The skilled person and the common general knowledge – 092
Common general knowledge – 092
Dosage forms
Absorption
Solubility
Dissolution
where:
dm/dt = the dissolution rate
A = available surface area of the undissolved API for dissolution
Cs = solubility of the API (equilibrium solubility)
Ct = concentration of dissolved API in the bulk of the dissolution fluid at time t
k = a constant / term relating to diffusion of dissolved API away from the dissolving material and the thickness of the stagnant layer
Biopharmaceutics Classification System
Dose number
Do = (M0 / V0) / Cs
in which:
M0 is the mass of drug administered (i.e. the dose);
V0 is the volume of dissolution medium available in which the dose may dissolve (e.g. the volume of liquid in the stomach); and
Cs is the drug compound's aqueous solubility (determined experimentally).
The 092 patent specification
"[0005] The poor solubility of many ß-carboline compounds useful as PDE5 inhibitors prompted the development of coprecipitate preparations, as disclosed in PCT publication WO 96/38131 and Butler U.S. Patent No. 5,985,326. Briefly, coprecipitates of a ß-carboline with polymeric hydroxypropylmethylcellulose phthalate, for example, were prepared, milled, mixed with excipients, and compressed into tablets for oral administration. Studies revealed, however, that difficulties arose in generating precisely reproducible lots of coprecipitate product, which makes use of coprecipitates less than ideal in pharmaceutical formulations.
[0006] Additionally, clinical studies involving administration of coprecipitate tablets preliminarily revealed that maximum blood concentration of the ß-carboline compound is achieved in 3 to 4 hours, with the average time for onset of therapeutic effect not yet precisely determined. In the treatment of sexual dysfunction, such as male erectile dysfunction or female sexual arousal disorder, however, a more rapid achievement of maximum blood concentration, along with a greater prospect for rapid onset of therapeutic effect, frequently is sought by individuals desiring more immediate and/or less prolonged effects. Accordingly, a need in the art continues to exist for orally administrable ß-carboline compounds and ß-carboline-containing pharmaceutical compositions having an ability to provide a therapeutic effect within a desirable, or at least acceptable, time frame."
"The specific dose of [tadalafil] administered according to this invention is, of course, determined by the particular circumstances surrounding the case including, for example, the route of administration, the state of being of the patient, and the pathological condition being treated. A typical daily dose contains a nontoxic dosage level from about 1 to about 20 mg/day of [tadalafil]. Preferred daily doses generally are about 1 to about 20 mg/day, particularly 5 mg, 10 mg, and 20 mg tablets, administered as needed."
(a) Example 1 is an in vitro dissolution test on various samples of tadalafil with differing particle size. 10mg of each sample was dissolved in 1L of aqueous 0.5% sodium lauryl sulfate (a surfactant) at 37°C.
(b) Example 2 shows the improvement in bioavailability provided by the invention over the co-precipitate formulation. With the co-precipitate, Tmax was not reached until 3.5 hrs. With the invention, it was reached in 2hrs.
(c) Example 3 is an in vivo study in which three tablets of tadalafil with different particle sizes are tested to determine their bioequivalence. These show that decreasing particle size increases Cmax, decreases Tmax and increases AUC(0-24) (save that decreasing particle size from 20(m to 8.4(m did not decrease Tmax ).
(d) Examples 4 & 5 are formulation examples for 10 mg (example 4) and 5 mg and 20mg (both example 5) tablets.
Claim construction - 092
Priority -092
"The specific doses of a compound administered according to this invention will, of course, be determined by the particular circumstances surrounding the case including, for example, the compound administered, the route of administration, the state of being of the patient, and the pathological condition being treated. A typical daily dose will contain a nontoxic dosage level from about 1 to 20 mg/day of a particulate compound of the present invention. Preferred daily doses generally will be from about 1 to 10 mg/day, particularly of 5mg and 10mg tablets, administered once per day."
Added matter - 092
"A typical daily dose contains a nontoxic dosage level from about 1 to 20 mg/day of compound (I). Preferred daily doses generally are about 1 to about 20 mg/day, particularly 5 mg, 10 mg, and 20 mg tablets, administered as needed."
17 Q. Now, on this, there is no mention in this document, Anderson,
18 of a maximum dose. That is right, is it not?
19 A. They talk of 1-20 mg and that the physician can ultimately
20 choose the dose.
21 Q. 1-20 are typical doses. There is no mention of a maximum
22 dose. Try and find the bit that I think you are referring to
23 is 17; is that right? The passage we looked at earlier.
24 A. Yes. I do not believe they cite a maximum dose.
(T6/825/17-24)
Novelty - 092
"But the infringement must be not merely a possible or even likely consequence of performing the invention disclosed by the prior disclosure. It must be necessarily entailed. If there is more than one possible consequence, one cannot say that performing the disclosed invention will infringe. The flag has not been planted on the patented invention, although a person performing the invention disclosed by the prior art may carry it there by accident or (if he is aware of the patented invention) by design. Indeed, it may be obvious to do so. But the prior disclosure must be construed as it would have been understood by the skilled person at the date of the disclosure and not in the light of the subsequent patent."
"104 I can therefore turn to the case on inevitable result. As I have said, in relation to this issue experiments were performed. This has produced a very large amount of evidence. Inhale has identified every single difference between the description of the process and apparatus in [the prior art] and that used in Quadrant's experiments and argues that the latter are neither a repetition of [the prior art] nor do they prove that a product within the claims of the patent would inevitably be made. Each of the points taken by Inhale has been addressed by Quadrant. However, it is not necessary to go through each of them because, for the reasons set out in the last preceding paragraph, it has not been proved that repetition of the teaching in the document would inevitably have produced something with a Tg above 20°C . Once again, it is overwhelmingly likely that such a Tg would have been achieved, but that is not enough for the purpose of anticipation."
"85. Is that finding good enough for an inevitable result? The legal requirement is that this feature of the claim be the inevitable result of carrying out the prior teaching. Does that mean that if there is some other possibility, even a fairly remote one, that some other result would follow, I should conclude the result is not inevitable? Or am I concerned to establish what, on the balance of probabilities would in fact occur? In my judgment, it is the latter approach which is correct. The inevitable result test does not require proof of individual facts to a quasi-criminal standard. It may be impossible to establish the relevant technical facts to that standard. It is another matter if the evidence establishes that sometimes one result will follow and sometimes another, depending on what conditions are used. But there is nothing of that kind suggested here. It is simply a question of what occurs in fact."
"I consider it highly likely that the formulation accordingly to Example 1 of Oren (which contains tadalafil with a d90 particle size of 4 µm) would exhibit Cmax and AUC values with the ranges […] stated by claims 8 and 9."
Obviousness – 092
The skilled person's expectations of micronisation
"If the drug is a case 2 drug (high permeability, low solubility) then absorption from solution is faster than dissolution and sink conditions are likely to prevail in vivo. As a general rule one should maintain sink conditions in the dissolution media if possible, such that the drug dissolves in less that 20-30% of the dissolution media.
Other factors which need to be considered, especially for case 2 drugs, are particle aggregation and the effective particle size in vivo. Quite often the first approach to increasing the dissolution rate of drugs in this class is micronization. This however, also increases the surface energy and hence potential for particle aggregation. When predicting in vivo bioavailability from in vitro dissolution profiles, it is critical that the particle size used in the model reflect the in vivo particle size."
(my emphasis)
"In the case of tadalafil, which cannot form a salt in physiological conditions, the skilled formulator would first consider particle size reduction via micronisation, probably in conjunction with use of a surfactant.
T7/1076/6-22:
6 Q. Let me understand I am clear on your evidence. Your evidence
7 is that you would go for the micronised formula first, not
8 because you think it is likely to work, but because it is the
9 most simple one?
10 A. I think it is likely to work. I did not say it was not likely
11 to work. I said all of these are likely to work. But it has
12 a huge advantage in as being the most routine,
13 straightforward, robust formulation. There is an enormous
14 advantage for it.
15 Q. I need to pick you up on that one. You say you expect it to
16 work. You have spent most of this morning telling his
17 Lordship that you cannot predict whether they will work.
18 A. Maybe we should be clear on the definition of work. I expect
19 it to improve things. As I just said to you, I cannot tell
20 you in a clinical trial whether any of these formulations are
21 going to achieve, you know, the particular goal of the
22 clinical trial. That is, you know, a biological outcome. But
23 I have an expectation that all of these will be better than
24 not doing anything.
"Mere possible inclusion of something within a research programme on the basis you will find out more and something might turn up is not enough. If it were otherwise there would be few inventions which were patentable. The only research which would be worthwhile (because of the prospect of protection) would be in areas totally devoid of prospect."
i) In terms of motives to find a solution to the problem the patent addresses, the skilled team would be highly motived by Daugan and the success of sildenafil to investigate tadalafil as a treatment for erectile dysfunction.
ii) As for possible avenues of research, overall tadalafil would be obvious to investigate. With low solubility and given the high dose required relative to it (i.e. a high dose number) there are some but not many options to consider. Top of the list is micronisation. It is simple and well known. The micronised formulation would include a surfactant.
iii) In terms of effort, overall the programme would involve very substantial resources of time, money and people but it would be pursued. The impetus to look at possible formulations would be substantial. At the point the formulations were being tested, the team would not have an alternative successful avenue available to them.
iv) Overall the team would embark on the project with a reasonable expectation of success in establishing tadalafil as a safe, tolerable and effective treatment for erectile dysfunction. The team would not know for sure that tadalafil could be formulated successfully but they would not give up without testing a fairly short list of expedients, of which micronisation would be one. In relation to the test of the formulation itself the team would have a high expectation that micronisation would improve the formulation. I have rejected Prof Frijlink's views on the skilled team's expectations of success both based on timings in the gastrointestinal tract and based on inferences from Daugan.
v) In terms of unexpected or surprising results, the low solubility of tadalafil is not unexpected although it does present a problem for the team. Nevertheless it is a problem the team is familiar with in general terms. The team would not be surprised that micronisation worked.
vi) The only significant value judgment which would be required of a skilled team in a programme which reached the claimed invention would be to test a micronised formulation of tadalafil (including a surfactant). That would not be a difficult decision.
Insufficiency - 092
i) Claims which are limited only by pharmacokinetic properties and not by particle size are insufficient as being too broad. This applies to claims 8, 9 and 16 to 19 (subject to dependency);
ii) Claim 12 is insufficient as it is ambiguous or too broad because it is not limited to sexual dysfunction and covers any disease;and
iii) Claims 1 to 7 are insufficient because the way they claim a particle size distribution is truly ambiguous.
Claims limited by pharmacokinetic properties
Claim 12
Claims 1 to 7 - particle size distribution
"… it is necessary to distinguish between claims that are difficult to construe or that have a "fuzzy boundary" (in the words of Lord Hoffmann in Kirin-Amgen Inc v Hoechst Marion Roussel Ltd [2004] UKHL 46, [2005] RPC 9 at [126]) on the one hand from claims that are truly ambiguous on the other. It is regrettably common for claims to be difficult to construe, but the court will nevertheless strive to give such claims a sensible meaning having regard to the inventor's purpose. It is also common for claims to have a fuzzy boundary, because an integer of the claim involves some question of degree or an imprecise functional limitation. It is well established that is not itself objectionable. If a claim is truly ambiguous, so that it is unclear what is the correct test to determine whether or not a product or process infringes, however, then the claim is insufficient, …."
[In this case ambiguity was rejected on the facts.]
Infringement - 092
Conclusion
i) At least claim 7 of the 181 patent is valid and infringed;
ii) All the claims of the 092 patent are invalid.
In addition to claim 1, the relevant claims of the 181 patent are:
2. The dosage form of claim 1 comprising 2.5mg of the compound in unit dosage form.
3. The dosage form of claim 1 comprising 5mg of the compound in unit dosage form.
6. The dosage form of any of claims 1 through 3 for use in treating a condition where inhibition of PDE5 is desirable.
7. The dosage form of claim 6 wherein the condition is a sexual dysfunction.
10. Use of a unit dose containing 1 to 5 mg of a compound having the structure [of tadalafil] for the manufacture of a medicament for administration up to a maximum total dose of 5 mg of said compound per day in a method of treating sexual dysfunction in a patient in need thereof.
12. The use of Claim 10 or 11, wherein the unit dose contains 2.5 mg of the compound.
13. The use of Claim 10 or 11, wherein the unit dose contains 5 mg of the compound.
2. The free drug particulate form of claim 1 wherein at least 90% of the particles have a particle size of less than about 25 microns.
3. The free drug particulate form of claim 1 wherein at least 90% of the particles have a particle size of less than about 15 microns.
4. The free drug particulate form of claim 1 wherein at least 90% of the particles have a particle size of less than about 10 microns.
8. A pharmaceutical composition comprising:
(a) a free drug form of a compound having the formula of [tadalafil] and pharmaceutically-acceptable salts and solvates thereof, in which the compound is present as solid particles not intimately embedded in a polymeric co-precipitate; and
(b) one or more pharmaceutically-acceptable carriers, diluents, or, excipients.
wherein the composition exhibits a Cmax of 180 to 280 micrograms/litre or an AUC (0-24) of 2280 to 3560 microgram hour/litre, measured using a 10 milligram dose of the compound.
9. The composition of claim 8 wherein the composition exhibits a Cmax of about 180 to about 280 micrograms/litre and an AUC (0-24) of 2280 to 3560 microgram.hour/litre.
12. A free drug particulate form according to any one of claims 1 to 4 for use in a method of treatment.
13. Use of particles of a free drug particulate form according to any one of claims 1 to 4 or a pharmaceutical composition according to any one of claims 5 to 7 for the manufacture of a medicament for the treatment of sexual dysfunction.
14. The use of claim 13 wherein the sexual dysfunction is male erectile dysfunction.
15. The use of claim 13 wherein the sexual dysfunction is female sexual arousal disorder.
16. Use of a pharmaceutical composition according to claim 8 or 9 for the manufacture of a medicament for the treatment sexual dysfunction.
17. The use of claim 16 wherein the sexual dysfunction is male erectile dysfunction,
18. The use of claim 16 wherein the sexual dysfunction is female sexual arousal disorder.
19. The use of anyone of claims 13 to 18, wherein the medicament is formulated for oral administration up to a maximum daily dose of 20 mg per day.