T 0354/97 (Protein secretion/GENENTECH) 03-05-2000

Reasons for the Decision

1. The appeal is admissible.

Main and second auxiliary requests

Article 123(2) EPC; added subject-matter:

2. Claim 1 of both the main request and the second auxiliary request was objected to under Article 123(2) EPC for being directed to a process for obtaining mammalian proteins, whereas, in the application as filed, mammalian proteins were not disclosed as a category of proteins to be expressed.

3. The Board agrees that proteins characterised as being mammalian are not mentioned expressis verbis in the application as filed but, in accordance with the case law of the boards of appeal (see for example, T 187/91, OJ EPO 1994, 572), considers it necessary for reaching a decision to assess whether the category of mammalian proteins is nonetheless directly and unambiguously derivable from said application, such that a reader of the description of the application as filed could reasonably have expected that a claim could be directed to this class of proteins.

4. On page 4 of the application as filed, it is stated that "the invention is based upon the discovery that yeast organisms can be caused to express, process and secrete protein that is normally heterologous to the yeast organism." On page 5, the protein to be expressed is once more defined as heterologous to the yeast. In addition, on lines 21 to 29, categories of desirable proteins are disclosed. Said proteins are regrouped according to their function: hormones, enzymes...; their properties: immunogens... ;or their structure: glycoproteins. In some categories, examples are given where the proteins are further characterized by their origin: human, bovine, but also viral. In the Board's judgment, it is not possible to deduce from the way these proteins are classified that mammalian proteins were indeed the category of proteins to be expressed. This is true, even if the examples provided in the application as filed are of the expression of human leukocyte interferon and human growth hormone (i.e of mammalian proteins), taking into account that on page 5, these proteins are defined as belonging to the categories of interferons and hormones respectively.

5. Thus, it is apparent from the application as filed that about all proteins were considered, and selecting a particular group which is not envisaged therein amounts to a non-disclosed selection.

6. One argument presented by the Appellants in favour of the category of mammalian proteins being unambiguously, albeit implicitly, disclosed in the application as filed was that two parameters of the process namely, the secretion signals and the type of cells which naturally secrete proteins, were characterized as "mammalian" on page 16 and page 29 of the application as filed, respectively, and that, therefore, the term mammalian would have been extended by the skilled reader to the protein to be expressed . This argument does not convince the Board as it is not self evident that the characterising feature of some entities mentioned in the application as filed may necessarily be taken as a characterising feature of others. The further argument drawn in particular from document (P33) that in the prior art the term "human" or "bovine" was used interchangeably with the term mammalian is not decisive in the present case. The common general knowledge of the skilled person would, of course, have it that humans or cattle are mammalians. Yet, the possibility of using the latter word for the earlier ones obviously depends on the facts at hand. Here, the situation is that proteins from neither humans nor cattle were identified as representative of the category of mammalian proteins within the framework of the invention.

7. For these reasons, the main and second auxiliary requests are refused as the subject-matter of their claim 1 does not fulfill the requirements of Article 123(2) EPC.

First auxiliary request

Article 123(2)(3) EPC; added subject-matter, broadened scope of the claims:

8. The objection raised in relation to claim 1 of the first auxiliary request was that this claim related to a process for obtaining human proteins, whereas the category of "human proteins" was not disclosed in the application as filed.

9. The situation is, however, distinctly different from that discussed above under points 2 to 6. Many references are made throughout the application as filed to human proteins to be expressed: on page 5, lines 22 to 25: human growth hormone, human interferons, human serum albumin and human insulin are mentioned; and on pages 30 and 37 the secretion of human interferon and human growth hormone is exemplified. Accordingly, the Board considers that, in the application as filed, the term "human" appears in relation to the proteins to be expressed in such a way that the category of human proteins is clearly and unambiguously derivable from said application. The requirements of Article 123(2) EPC are fulfilled.

10. The requirements of Article 123(3) EPC are also fulfilled as the category of human proteins is narrower than that of mammalian proteins.

Article 83 EPC: sufficiency of disclosure

11. Claim 1 is directed to the production of human proteins in any yeast strain using any heterologous secretion signal sequence. Its scope of protection is, thus, very wide. Yet, in accordance with the case law of the EPO with regard to sufficiency of disclosure (see for example, T 19/90, OJ EPO 1990, 476), this mere fact is not in itself a ground for considering the patent as not complying with the requirements of Article 83 EPC. To reach a decision on this issue, it is necessary to assess whether the invention may be performed over the whole area claimed without undue burden or application of inventive skill.

12. The teaching in the description of the patent in suit is that, in order to carry out the claimed process, it is necessary in a first instance to isolate the DNA encoding the desired protein and to clone it into a plasmid vector suited for expression in yeast, in functional combination with the DNA encoding a secretion signal peptide heterologous to the yeast, then to transform the construct into the yeast cells wherein the protein is expressed, processed and secreted. The relevant disclosure on how to accomplish the basic task of constructing the relevant plasmids is provided on page 5, lines 16 to 18 and page 7, lines 47 to 48 by reference to specific documents of the state of the art. A protocol for the transformation of S.cerevisiae is described on pages 4 and 5. The secretion in S.cerevisiae of human interferon and human growth hormone is exemplified. In the Board's judgment, the skilled person wanting to secrete proteins in the yeast culture medium would have been able to follow the provided information as a matter of routine experimentation. And, indeed, evidence that human proteins can be secreted by the claimed process is readily found in post-published documents (P60) to (P62), (P65), (P66), (P72) and (A11) which describe the secretion from yeast of interleukin 1, pancreatic secretory trypsin inhibitor, lyzozyme, salivary alpha-amylase, vascular permeability factor, antithrombin and insulin, respectively.

13. The Respondents I and II pointed out to documents (P74), (P26) and (P41), where HSA, tpA and HGH are reported to be secreted in the periplasmic space of S.cerevisiae rather than in the culture medium using their natural secretion signals (HSA and tpA) or an artificial signal sequence (HGH), as well as to document (P42), which discloses the failure of producing human alpha-antitrypsin, as evidence that the claimed process could not be carried out over the whole scope of the claim.

14. The Board cannot consider document (P41) as evidence that HGH is not secreted in the culture medium by the claimed process, since the patent in suit teaches on pages 36 to 38 that it is secreted in the culture medium when a signal sequence derived from the interferon genes is used. As for HSA and tpA, documents (P73), (A18) and document (A10) show that they are secreted in the culture medium by using other secretion signals than their own and/or different yeast strains such as P.pastoris and K.lactis. This implies that, if secretion in the culture medium is not obtained directly, it may nonetheless be achieved by changing the above mentioned parameters. The question is, thus, whether the patent in suit contains sufficient information for the skilled reader to be able to do so without undue burden and application of inventive skills.

15. On page 3, lines 34 to 37 of the patent in suit, it is stated: ""Heterologous signal polypeptide" refers to such polypeptides not normally produced or employed by a yeast system and may be selected from the signal polypeptide native to the heterologous protein under consideration, or other heterologous (signal) polypeptide functionally linked to the heterologous protein under consideration". On page 5, lines 31 and 32, it is stated: "Various yeast strains can be employed--see Lodder et al., The Yeasts, a Taxonomic Study, North Holland Publ.Co., Amsterdam." Thus, the patent in suit draws the skilled person's attention to the possibility of using yeast strains and signal sequences different from those specifically disclosed in the patent specification.

16. As already stated under point 12 supra, the Board does not consider that, at the filing date, undue burden was involved in carrying out the necessary experimental steps leading to secretion, including vector construction and yeast protoplast transformation. The Appellants argued in relation to transformation that improved protocols were used when expressing tpA in K.lactis (document (A10)) and HSA in P.pastoris (document (A16)). Yet, there is no evidence on file that the results obtained according to these documents would not have been obtained when using the usual transformation method. In this context, it is noted that document (A16), page 493 discloses that P.pastoris can be transformed by the spheroplast method first described in 1978.

17. It is important that secretion was achieved every time the skilled person, faced with an initial failure, chose to make use of other secretion signals and/or yeast strains (see point 14, supra). Consequently, the failure observed with human alpha-antitrypsin (document (P42)) is no convincing proof that the claimed process is not reproducible with this protein, because no efforts were made to correct said failure. The authors of document (P42) explain on page 6598 that the observed failure could "result from strain variation or from intrinsic properties of the molecules". These possible causes for failure are those which can be alleviated by the remedies mentioned above in relation to tpA and HSA.

18. Document (P45) discusses why the mechanisms involved in secretion may be complex. Yet, it is not relevant to enablement since the person skilled in the art had the disclosure of the patent in suit for guidance.

19. In the course of their pleadings, both the Appellants and the Respondents I and II made reference to numerous decisions of the boards of appeal concerning sufficiency of disclosure: more specifically to T 409/91, T 435/91, T 612/92, T 292/85, T 694/92, T 931/91 (see points IV and V supra) and T 14/83 (OJ 1984, 105; also cited in T 931/91).

20. In the cases T 409/91 and T 435/91, it was readily apparent from the teachings provided in the specification of the patents in question that the invention as claimed would not be reworkable over its whole scope. In T 612/92, there existed factual evidence in the post-published prior art that the invention could not be carried out over a large area of the claims. The facts upon which these decisions are based are thus obviously different from those in the present case in view of the findings under points 12, 15. and 16, supra.

21. Other cited decisions address the question of what should be the technical contribution by the claimed invention for sufficiency of disclosure to be acknowledged, taking at the same time into account the essence of said invention and the manner in which it was claimed. Thus, in T 292/85, the essence of the invention was found to be a new technique and the board held that the description of one way of carrying out this technique enabled the skilled person to perform the invention without undue burden over a broad range as long as there were suitable variants known to the skilled person which would provide the same effect for the invention. In T 694/92 the board held that more than one example might be necessary in order to support claims of a broad scope, in cases where the gist of the claimed invention consisted of the achievement of a given technical effect by known techniques in different areas of application. In the Board's judgment, the subject-matter of the patent in suit is different from that in both these cases because it is neither a new technique in the sense given to the term in T 292/85, as the technical effect of secreting heterologous proteins in the culture medium of yeast cells was already known from 1981 (see document (P45), page 2), nor is there only one example disclosed to support the broad claim.

22. There is factual evidence in the present case that the claimed process is workable although, in few cases, success was not reached at first try. Thus, the situation is rather analogous to that encountered in the case T 14/83 (see supra) where it is stated under point 6 of the decision,: "However, occasional lack of success of a claimed process does not impair its feasibility in the sense of Article 83 EPC if, e.g., some experimentation is still to be done to transform the failure into success, provided that such experimentation is not undue and does not require inventive activity."

23. For these reasons, the Board concludes that the requirements of Article 83 EPC are fulfilled.

Article 54 EPC: novelty:

24. Document (P37) is relevant to novelty under Article 54(3)(4) EPC. It is concerned with the expression of the gene encoding HSA in E.coli and yeasts. It discloses that the translated region of said gene contains, in addition to the open-reading frame for mature HSA, a signal peptide which is cleaved when the protein is secreted (page 2, line 16 to page 3, line 15). In Example 7, the expression of the HSA gene in yeast cells is contemplated but not disclosed expressis verbis. Constructs were made, whereby the main body of the HSA gene is inserted into yeast expression vectors. Information on how to obtain expression is given by way of reference to the state of the art (lines 31 to 32). In the Board's judgment, this teaching provides a technical disclosure at the same technical level as that provided by the patent in suit with regard to the cloning in yeast cells of mammalian DNA sequences in general for the purpose of secretion. They are, thus, considered enabling (see also point 12, supra).

25. By carrying out the expression of the HSA gene in yeasts in the manner contemplated in document (P37), secretion of HSA in the culture medium will necessarily follow. Thus, document (P37) is damaging to the novelty of claim 1, as it provides a process for the secretion of a human protein in the yeast culture medium.

26. Auxiliary request 1 is, thus, rejected for failing to fulfill the requirements of Article 54 EPC.

Auxiliary request 3

27. Claim 1 relates to a process for obtaining specific proteins which are listed as desirable to obtain on page 5 lines, 22 to 28 of the application as filed. The requirements of Article 123(2) EPC are fulfilled. Those of Article 123(3) EPC are also fulfilled as the scope of the claim is narrower than that of the granted claim 1 which related to mammalian proteins in general. Furthermore, claim 1 also meets the requirements of Article 84 EPC.

28. Claim 1 comprises the production of human serum albumin with which document (P37) is specifically concerned. Thus, the findings under points 24 and 25 supra of lack of novelty of the subject-matter of claim 1 of auxiliary request 1 over document (P37) apply mutatis mutandis to the subject-matter of this claim 1.

29. Auxiliary request 3 is, thus, rejected for lack of novelty.

Auxiliary request 4

Article 123(2)(3) EPC; added subject-matter, enlargement of the scope of the granted claims:

30. Claim 1 of auxiliary request 4 differs from claim 1 of auxiliary request 1, which was found allowable under Article 123(2)(3) EPC (cf. points 8 to 10 supra), by the addition of the process feature "...and further comprising the step of recovering said human protein from the medium of the culture". A process comprising this feature is disclosed in the application as filed, for example, on page 4, lines 18 to 24. The requirements of Article 123(2) EPC are, thus, fulfilled.

31. The requirements of Article 123(3) EPC are also fulfilled as the scope of claim 1 is narrower than that of the corresponding granted claim 10, which related to the recovery from the culture medium of mammalian proteins in general.

Article 83 EPC; sufficiency of disclosure:

32. The findings of sufficiency of disclosure in relation to the claims of auxiliary request 1 (see points 11 to 23, above) apply mutatis mutandis to the claims of auxiliary request 4. In the Board's judgment, the additional step of recovering the human protein from the medium is within the skilled person's ability as it is a process which is carried out every time a protein is produced. No arguments have been presented to the contrary.

Article 54 EPC; novelty:

33. As already stated (see point 24, supra), document (P37) does not disclose expressis verbis a process whereby HSA is secreted in the culture medium of yeast cells. This necessarily implies that there is no disclosure in this document of HSA being recovered from said medium. The Respondents I and II drew the Board's attention to the passage on page 11, lines 7 to 9 where it is stated that "The purification of human serum albumin can be accomplished by using procedures well known in the art". However, in the Board's judgment, this sentence, which is written in the context of producing HSA in E.coli as well as in yeasts, does not necessarily imply that HSA is recovered from the culture medium before purification, there being the other possibility that it may be recovered from the host cells themselves. Accordingly, document (P37) does not destroy the novelty of claim 1 of auxiliary request 4. No further novelty objections were raised against any of the claims of auxiliary request 4. The Board is convinced that no other documents on file are damaging to the novelty of the claims of this auxiliary request.

34. The requirements of Article 54 EPC are, thus, fulfilled.

35. The conclusions reached in terms of formal requirements (points 30 and 31, supra), sufficiency of disclosure (point 32, supra) and novelty (point 33, supra) equally apply to the auxiliary request 4 for the Contracting State AT.

Article 56 EPC; inventive step:

36. The Opposition Division has not yet decided the issue of inventive step. The Board does not consider it appropriate to carry out the examination of inventive step itself at this stage of the proceedings, but decides to use its discretionary power under Article 111(1) EPC to remit the case to the Opposition Division for further prosecution.