BESCHWERDEKAMMERN BOARDS OF APPEAL OF CHAMBRES DE RECOURS DES EUROPÄISCHEN THE EUROPEAN PATENT DE L'OFFICE EUROPEEN PATENTAMTS DES BREVETS Internal distribution code: (A) [ ] Publication in OJ (B) [X] To Chairmen and Members (C) [ ] To Chairmen D E C I S I O N of 28 October 1998 Case Number: Application Number: Publication Number: Language of the proceedings: EN Title of invention: A method of treating anxiety-related disorders using sertraline Applicant: Pfizer Inc. Opponent: - Headword: Obsessive-compulsive-disorder/PFIZER Relevant legal provisions: EPC Art. 54(1) Keyword: "Novelty (yes): no possibility of deriving the claimed therapeutic application from the information available that clinical trials are in progress" Decisions cited: - Catchword: The information in a citation that a medicament is undergoing a clinical phase evaluation for a specific therapeutic application is not prejudicial to the novelty of a claim
directed to the same therapeutic application of the samemedicament if such information is plausibly contradicted by thecircumstances and if the content of said citation does notallow any conclusion to be drawn with regard to the actualexistence of a therapeutic effect or any pharmacological effectwhich directly and unambiguously underlies the claimedtherapeutic application. Europäisches European Office européen Patentamt Patent Office des brevets Case Number: T 0158/96 - 3.2.2 D E C I S I O N of the Technical Board of Appeal 3.2.2 of 28 October 1998 Appellant:
Pfizer Inc. 235 East 42nd StreetNew York, N.Y. 10017 (US)
Representative:
Ruddock, Keith StephenPfizer LimitedEuropean Patent DepartmentRamsgate RoadSandwichKent CT13 9NJ (GB)
Decision under appeal: Decision of the Examining Division of the European Patent Office posted 25 August 1995 refusing European patent application No. 90 311 797.6 pursuant to Article 97(1) EPC. Composition of the Board: Chairman: Members: Summary of Facts and Submissions
European patent application No. 90 311 797.6
(publication No. 0 429 189) was refused by the
examining division under Article 97(1) EPC on the
ground of lack of novelty of the subject-matter of
claim 1. The decision was taken on the basis of
claims 1 and 2 filed with a letter dated 26 July 1994
The use of the compound (1S-cis)-4-(3,4-dichlorophenyl)-1,2,3,4-tetrahydro-N-methyl-1-naphthalenamine or a pharmaceutically acceptable saltthereof for the manufacture of a medicament to treat orprevent obsessive-compulsive disorder.Use as claimed in claim 1 where the compound orsalt thereof is administered in a dose of from 50 to
The following documents cited during the examination
procedure are relevant for the present decision:
The Journal of Neuropsychiatry and Clinical
Neurosciences, Vol. 1, No. 3, Summer 1989,
Psychiatric Developments, 1, (1989) pages 1 to 18.
It was the examining division's judgment that the use
of the compound at issue (commonly named "sertraline")
for the treatment of obsessive-convulsive disorder
The examining division specifically relied on table 4
of document (5), which showed that in 1989 sertraline
was undergoing clinical phase II trials for obsessive-
The examining division argued that clinical phase II
tests represented a stage of drug experimentation
preceded by various proofs of activity in vitro as well
as on animals. Therefore the information conveyed by
(5) was that sertraline had already been submitted to
the complete pre-clinical experimentation necessary to
start clinical testing and had already proved useful
The examining division emphasised that it was common
practice to accept any pharmacological test, even at
its earlier stage, as the disclosure of a medical use,
as long as this test was commonly accepted as an
indication of a potential therapeutic utility. In its
view, this was the type of data that necessarily
The appellant lodged an appeal against this decision,
requesting a refund of the appeal fee because of a
procedural violation of Rule 68(2) EPC and oral
proceedings. Oral proceedings were held on 28 October
The appellant argued that, before phase II clinical
trials, drug efficacy in treating a disease was not yet
established and that, in the United States, the showing
of efficacy in humans was not a prerequisite for
conducting phase II clinical studies on a particular
drug. Declarations by Montgomery, Hollander and Grant
N. Ko, were produced. The clinical efficacy testing
was, on the contrary, conducted in phase II and III
studies. Therefore, even at the end of the phase II
stage, the efficacy of sertraline in treating OCD had
not been finally established and no conclusions could
be drawn. In fact, a large proportion of drugs entering
phase I and phase II studies did not proceed to phase
For this reason, the efficacy of sertraline in the
treatment of OCD remained an undisclosed effect hidden
within the teaching in (5), and as such it could not be
regarded as made available to the public.
The rapporteur issued a preliminary communication in
which he emphasised that the decisive point was not
whether the efficacy in humans of sertraline had
already been conclusively established in all its
clinical aspects when it was undergoing clinical phase
II trials, but whether during any of the earlier
phases, ie the preclinical studies and the clinical
phase I trials, the novel therapeutic activity, or any
other effect able to point directly to this therapeutic
activity, had already been identified, whether or not
its observed efficacy would have been sufficient to
In reply to the official communication and during the
oral proceedings, the appellant submitted affidavits by
Rasmussen and Brumfield. Attached to the latter, the
"Information for Sponsor-Investigators Submitting
Investigational New Drug Application (IND's)"
issued by the Centre for Drug Evaluation and
Research of the US Food and Drug Administration
(FDA) and including a heading entitled "Draft
Summarisation", relating to Title 21, part 312 of
The official text of Section 312.21 of Title 21 of
the Code of Federal Regulations. Section 312.21 of
Title 21 provides definitions of clinical phases
I, II and III of an investigation of a new drug.
At the oral proceedings, the appellant further
explained that no animal model suitable for evaluating
the efficacy of a substance in treating OCD was
available by 1989, and, for these reasons, the pre-
clinical studies of sertraline were simply aimed at
evaluating the different aspects of toxicity and
Moreover, while it was exceptionally possible in
certain disease areas that some data relating to the
efficacy of a new drug under investigation could be
obtained during clinical phase I, this was certainly
not the case of sertraline in the treatment of OCD.
The appellant requested that the decision of the
examining division be set aside and the patent be
granted on the basis of claims 1 and 2 filed with the
letter dated 26 July 1994, pages 1 to 4 of the
description also filed with the letter dated 26 July
1994 and pages 5 and 6 of the description as originally
The appellant also requested reimbursement of the
Reasons for the Decision
Amended claims 1 and 2 are disclosed in claim 10 and on
page 3, lines 18 to 21 of the original application
respectively. Therefore they meet the requirements of
Claim 1 is directed to the second or subsequent
therapeutic application of sertraline, or a
pharmaceutically acceptable salt thereof, said
therapeutic application being the treatment or
prevention of obsessive-compulsive disorder.
This claim belongs to the family of use claims
protecting the use of a given substance for the
manufacture of a medicament for obtaining a therapeutic
effect in the treatment of a disease.
Therefore, the present claim 1 is to be construed as
implicitly including the functional technical feature
that sertraline, when formulated into a medicament and
administered to patients, achieves a therapeutic effect
or any pharmacological effect which directly and
unambiguously underlies the claimed therapeutic
For the purpose of assessing novelty, it thus has to be
examined whether or not the same therapeutic effect has
been shown in the prior art documents.
The sole point addressed by the examining division in
the decision under appeal is the novelty of the claimed
subject-matter in relation to the prior document (5).
This piece of literature describes the clinical utility
of pharmacological agents that act on serotonin
receptors. The part relevant to the present case is the
section entitled "Serotonin-Uptake Blockers" (pages 258
to 260), in which attention is focused on a series of
selective 5-HT (ie serotonin) uptake blockers including
sertraline. As illustrated in Table 4 on page 259,
these compounds were, by 1989, at varying stages of
clinical evaluation. The table reports that sertraline
(Pfizer) was undergoing clinical phase III trials for
depression and clinical phase II trials for obsessive-
As explained in the first paragraph under the heading
"Serotonin-Uptake Blockers" (page 258), drugs that
block the transport back of the released serotonin
(5-HT) into the presynaptic terminals potentiate the
action of 5-HT and, as reported, alleviate a variety of
clinical disorders such as depression, panic attacks,
obsessive-compulsive disorders and obesity. Following
this introductory paragraph, the document reports three
sections specifically addressed to depression, panic
disorder and OCD (pages 258 to 260). Sertraline is
cited in the first section, in relation to depression,
as being the most potent inhibitor of the 5-HT uptake
relative to norepinephrine in rat brain, and as being
as effective in treating major depressive disorders as
standard tricyclics. However, no reference at all to
sertraline is to be found in the section addressed to
obsessive-compulsive disorder or in any other part of
the document. Thus, the skilled reader of document (5)
could not find any textual support, explanation or
confirmation of the information conveyed by table 4 in
relation to sertraline for the indication obsessive-
compulsive disorder. Under these circumstances, the
novelty-destroying effect of this document, alleged by
the examining division, is confined and limited to the
teaching explicitly or implicitly derivable from
The only explicit teaching derivable from table 4 is
that sertraline, by 1989, was being submitted to phase
II trials for the indication obsessive-compulsive
disorder. Neither the table nor any other part of the
document reports the results of any such phase II
The description of clinical phase I, II and III
investigations, the targets and the models to be used
are given in Section 312.21 of Title 21 of the Code of
Federal Regulations released by the US FDA, relative to
Investigational New Drug Applications (IND's). The text
of this part of the Code of Federal Regulations was
According to the aforementioned Section 312.21,
phase II includes controlled clinical studies conducted
in patients with the disease or condition under study
for the purpose of evaluating the effectiveness of the
Although one of the targets of phase II is indeed that
of evaluating the effectiveness of the drug, thus
whether or nor the drug exhibits the alleged
therapeutic activity in patients, the answer to this
question could not be predicted by the skilled reader,
as document (5) lacks any anticipation of a preliminary
positive or negative outcome of phase II trials. Only
the successful approval of the drug in the subsequent
phase evaluation, namely phase III, would imply an
For this reason the skilled person, reading in table 4
that sertraline was undergoing phase II trials for OCD,
had no means of concluding from this information,
reliably and beyond mere speculation, that the drug
finally proved, during this phase, any therapeutic
effect potentially useful in the treatment of OCD. In
fact, as the appellant reiterated, and as a matter of
common general knowledge, many candidate drugs
submitted to phase I and II evaluation do not proceed
Table 4 also imparts an implicit teaching to the
skilled reader. In fact, in order to be approved for
clinical phase II trials, the tested substance must
have complied with all the requirements of the previous
clinical phase I and pre-clinical investigation.
Therefore, the therapeutic efficacy of sertraline in
the treatment of OCD or any other effect indicating
therapeutic efficacy may have been observed already
For this reason, if the person skilled in the field of
psychiatry, faced with the information that sertraline
was undergoing phase II trials for OCD as disclosed in
table 4 of document (5), was in a position to conclude
with the required certainty that the anti-OCD activity
of sertraline, or any other pharmacological effect, ie
indisputably underlying such a therapeutic application,
had already been shown or proven during phase I trials
or during the pre-clinical experimentation, then the
teaching of document (5) would have to be regarded as
prejudicial to the novelty of the claimed subject-
According to Section 312.21 of Title 21 of the Code of
Federal Regulations, clinical phase I studies are
designed to determine the metabolism, the structure-
activity relationship, the pharmacokinetic and
pharmacological effects of the drug in humans, the side
effects associated with increasing doses and, only if
possible, to gain early evidence of effectiveness.
Thus, proving the existence of therapeutic
effectiveness in the treatment of OCD was not a
mandatory requirement of the phase I investigation
which had to be met before submitting sertraline to the
subsequent phase study. This is also confirmed by the
fact that, according to the Code of Federal
Regulations, phase I is not necessarily conducted on
patients, but may be conducted on normal volunteers.
Therefore, the reader of (5) could not conclude that a
therapeutic effect had already been proven or observed
Although the direct evidence of a therapeutic effect
was not to be expected from the phase I trials in the
present case, the skilled reader knew that such
evidence could possibly also be derived from the
results of previous investigations, such as those
concerning the pharmacokinetic and the pharmacological
properties of a substance. It is indeed not exceptional
that a pharmacological effect observed in an early
investigation may directly and unambiguously reflect a
therapeutic effect, thus underlying a therapeutic
application. For this reason, it is not unusual for an
early shown pharmacological effect to be accepted, for
the purpose of patent protection, as sufficient proof
of a therapeutic application. Yet this is not a general
At the priority date of the European application,
sertraline was known to be a selective serotonin re-
uptake inhibitor. By blocking the transport back of
serotonin into the presynaptic terminals, sertraline
potentiates the action of serotonin [see (5), page 258
"Serotonin-uptake blockers"]. As is well-known to those
skilled in the art, serotonin is a neurotransmitter
exhibiting a multiplicity of physiological activities.
No evidence is on record showing that, before the
priority date of the European application, a clear and
accepted relationship between these physiological
activities and the many psychiatric disorders and
diseases (ranging from depression to anxiety) allegedly
affected by the potentiation or the depression of the
serotoninergic neurotransmission had finally been
established. Thus, the skilled reader of (5) had no
means of concluding with the required certainty that
any evidence of a therapeutic effect in relation to OCD
could have been produced by the results of the
pharmacological studies carried out in clinical
As underlined in the decision under appeal, clinical
trials are generally preceded by pre-clinical studies
The examining division held that the information
conveyed by document (5) was that sertraline had
already undergone the complete pre-clinical phase
experimentation, in animals, including the pre-clinical
activity tests showing the utility of sertraline for
treating OCD. It also stressed that, for the purposes
of patent disclosure, it was common practice to accept
any pharmacological test as the disclosure of a medical
use, as long as this test was commonly accepted as an
indicator of potential therapeutic utility, and this
was the type of data that had to precede phase II
The board does not share the examining division's
conclusion in the present case. For a prior-art
document to be recognised as prejudicial to the novelty
of a claimed subject-matter, the information conveyed
by this document cannot be interpreted on the basis of
rules, which, though normally valid, do not necessarily
apply to the specific situation and therefore may lead
In fact, given the level of knowledge on OCD available
in 1989, as illustrated in the documents on record and
in the affidavits and declarations produced during the
proceedings, the person skilled in the field of
psychiatry had no reasonable ground for expecting the
pre-clinical evaluation of sertraline to include any
"activity-test showing the utility of the substance in
the treatment of OCD", and still less for expecting any
pharmacological test to exist that was "commonly
accepted" as an indicator of the potential therapeutic
As argued by the appellant (see Montgomery statutory
declaration, point 8), OCD is a complex behavioural
disorder involving both obsessions and compulsions,
which only relatively recently has been operationally
defined to allow testing of a homogeneous population.
Accordingly, it was only after December 1989 that it
was possible to develop a consensus on how to study
This picture is confirmed by document (7), which
describes the level of knowledge on obsessive-
It is reported under the heading "Treatment Effects"
(page 6) that "Until recently, psycho-pharmacologic
interventions in OCD were thought to be largely
ineffective. Little evidence was available to document
reductions in obsession, compulsion, or phobic
avoidance in response to pharmacological treatment. In
part, this reflected methodological problems adversely
affecting treatment outcome studies in OCD including
small sample size, non-standardized diagnoses, lack of
valid and reliable assessment procedures, inadequate
control groups, and the presence of intercurrent
diagnoses, particularly major depression".
As further indicated by the appellant, the evaluation
of a potential anti-OCD effect was rendered even more
difficult by the fact, also confirmed by (7), page 11,
third paragraph, that the anti-OCD effect often
appeared late, without reaching its peak until 3 to 5
The board is, therefore, convinced that the skilled
person, faced with the teaching in table 4, and
conscious of all the difficulties and problems still
found in 1989 in assessing drug-effectiveness in
treating OCD, even in human patients, would not
realistically have concluded that evidence of
sertraline effectiveness had already been produced by
the pre-clinical studies in animals.
Under these specific circumstances, the board
recognises as plausible the appellant's arguments,
though not confirmed by documents, that experimentation
in animals was not indicative of any therapeutic
effectiveness of sertraline for OCD since no animal
model for OCD actually existed, but was simply intended
to prove the lack of any form of toxicity and to gain
early knowledge about the metabolism of the substance.
In view of the foregoing, the board's judgment is that
the conclusion of the examining division that the
subject-matter of claims 1 and 2 lacks novelty over the
teaching of document (5) is not justified.
Although, by virtue of Article 111(1) EPC, the board
may exercise any power within the competence of the
department responsible for the decision appealed, in
the present case the board considers it appropriate to
remit the case to the first instance for further
prosecution of the examination. In fact, important
patentability aspects still need to be addressed by the
The board notes that the patent application includes no
example or evidence substantiating the novel
therapeutic effect of sertraline underlying the present
invention. Nor was any evidence of the alleged effect
produced during the proceedings before the examining
division or during the appeal proceedings. Whether this
situation implies a deficiency which may still be
remedied with the submission of evidence, or whether it
has inescapable substantive consequences with regard to
the clarity of the claims, the repeatability of the
invention or the inventive step involved in the claimed
subject-matter are questions that need to be discussed
in the first place before the examining division.
Reimbursement of the appeal fee was also requested by
the appellant, on the ground that no reason for the
rejection of claim 2 was stated in the decision, which
amounted, in the appellant's view, to a substantial
procedural violation of Rule 68(2) EPC.
The board emphasises that all the claims belonging to
one set of claims form an indivisible unit representing
the appellant's request. Even if only one of the claims
fails to meet the requirements of the EPC, the whole
set of claims is to be rejected, regardless of whether
the remaining claims might be patentable if claimed
separately. It is in fact the responsibility of the
appellant to formulate or to amend the claims in such a
way that the whole set of claims may be acknowledged as
patentable. In the judgment of the examining division,
the subject-matter of claim 1 did not meet the
requirements of Articles 52(1) and 54 EPC. The
examining division was therefore not obliged to examine
claim 2 and to give further reasons in relation to this
For these reasons it is decided that:
The decision under appeal is set aside.
The case is remitted to the first instance for further
The reimbursement of the appeal fee is refused.
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