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`Application No. 15/121,623
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`- 23 -
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`GEUIJEN et al.
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`The Office next ascribes an overly broad interpretation to the phrase "ligand-induced
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`receptor function" in support of its claim that it cannot be predicted what "epitope-specific effects"
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`an antibody will have on the antigen to which it binds. Again here, the Office ignores the disclosure
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`in the specification which discloses actual bispecific antibodies and binding arms that inhibit
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`receptor function, in favor of hypothesizing that the disclosure should be summarily discounted
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`because antibodies may have epitope-specific effects — a claim that is not supported by any direct
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`evidence as to the claimed invention. Rather, the Office uses a number of references, none of which
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`discloses bispecific antibodies that bind ErbB-2 and ErbB-3, to attempt to bolster its rejection.
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`Teachings related to an anti-CD23 antibody on binding of IgE to its receptor (as in the Bettler et al.
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`reference), or the ability of an anti-CD47 antibody to induce apoptosis of Jurkat T cells or PBMCs
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`(as in Pettersen et al.) is not relevant here.
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`Moreover, Applicant respectfully reminds the Office that the claimed antibodies must bind
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`to specific regions of ErbB-2 and ErbB-3. Therefore, even if there were "epitope-specific effects,"
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`arguendo, the claimed genus of antibodies recites domains to which the binding arms are required
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`to bind. The Office attempts to support its erroneous position by citing to Fu et al. (Office Action,,
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`p. 24). However, Fu discloses antibodies that bind to domain III and not domain I of ErbB-2.
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`Therefore, any relevance of Fu would be to antibodies that bind an entirely different domain of
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`ErbB-2 than the claimed invention.
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`In attempting to support its position that the claims are not adequately described in the
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`specification, the Office points to evidence that actually supports a showing of adequate description.
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`The Office points to Table 6 of the specification and states that "while antibodies 'PG2916' and
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`'PG2971' [which bind domain I of ErbB-2] are both capable of inhibiting proliferation of SKBR-3
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`cells, the latter is less than half as effective as the former." Applicant respectfully asserts that the
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`Atty. Dkt. No. 4096.0100002/DAS/PAC/E-H
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