Ex Parte Buelow

Patent Trial and Appeal Board

Nov 7, 2013

12130818 (P.T.A.B. Nov. 7, 2013)

UNITED STATES PATENT AND TRADEMARK OFFICE
____________

BEFORE THE PATENT TRIAL AND APPEAL BOARD
____________

Ex parte ROLAND BUELOW
____________

Appeal 2012-008014
Application 12/130,818
Technology Center 1600
____________

Before LORA M. GREEN, MELANIE L. McCOLLUM and
ANNETTE R. REIMERS, Administrative Patent Judges.

REIMERS, Administrative Patent Judge.
DECISION ON APPEAL

Appeal 2012-008014
Application 12/130,818

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STATEMENT OF THE CASE1
Roland Buelow (Appellant)2 appeals under 35 U.S.C. § 134(a) from
the Examiner’s decision to reject claims 14-22 and 35-39. We have
jurisdiction over this appeal under 35 U.S.C. § 6(b). We REVERSE.

CLAIMED SUBJECT MATTER
Appellant’s invention “relates to transgenic animals having one or
more inactivated endogenous immunoglobulin loci” (Spec. 1, para. [002]).
Claim 14 is representative and reads as follows:
14. A viable rodent germ cell having at least one
endogenous immunoglobulin (Ig) gene inactivated
by the action of at least one meganuclease.

THE EVIDENCE
The Examiner relies on the following references in rejecting the
appealed claims:
Kucherlapati (‘205) US 5,574,205 Nov. 12, 1996
Kucherlapati (‘598) US 5,939,598 Aug. 17, 1999
Kucherlapati (‘181) US 6,075,181 Jun. 13, 2000
Kucherlapati (‘598*) US 6,114,598 Sep. 5, 2000
Kucherlapati (‘835) US 6,139,835 Oct. 31, 2000
Kucherlapati (‘584) US 6,150,584 Nov. 21, 2000
Kucherlapati (‘963) US 6,162,963 Dec. 19, 2000
Buelow (‘534) US 2003/0017534 A1 Jan. 23, 2003
Kucherlapati (‘752) US 6,514,752 B1 Feb. 4, 2003

1 Claims 1-13, 23-34, 40 and 41 have been canceled.
2 The real party in interest is OMT, Inc.
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Kucherlapati (‘103) US 6,657,103 B1 Dec. 2, 2003
Kucherlapati (‘986) US 6,673,986 B1 Jan. 6, 2004
Kucherlapati (‘610) US 6,713,610 B1 Mar. 30, 2004
Buelow (‘880) US 2004/0158880 A1 Aug. 12, 2004
Buelow (‘392) US 2005/0153392 A1 Jul. 14, 2005
Buelow (‘263) US 2005/0229263 A1 Oct. 13, 2005
Buelow (‘696) US 2006/0026696 A1 Feb. 2, 2006
Buelow (‘398) US 2006/ 0117398 A1 Jun. 1, 2006
Jakobovits (‘244) US 7,064,244 B2 Jun. 20, 2006
Arnould (‘826) US 2006/0153826 A1 Jul. 13, 2006
Arnould (‘949) US 2006/0206949 A1 Sep. 14, 2006
Buelow (‘084) US 7,129,084 B2 Oct. 31, 2006
Buelow (‘668) US 7,585,668 B2 Sep. 8, 2009
Jakobovits (‘893) WO 98/24893 Jun. 11, 1998
Schooten WO 02/12437 A2 Feb. 14, 2002
Buelow (‘001) WO 2005/038001 A2 Apr. 28, 2005

M. H. Porteus and D. Carroll, Gene targeting using zinc fingernucleases, 23
NATURE BIOTECHNOLOGY 967-973 (2005).

Vasquez et al., Manipulating the mammalian genome by homologous
recombination, 98 PNAS 8403-8410 (2001).

Donoho et al., Analysis of Gene Targeting and Intrachromosomal
Homologous Recombination Stimulated by Genomic Double-Strand
Breaks in Mouse Embryonic Stem Cells, 18 MOLECULAR AND
CELLULAR BIOLOGY 4070-4078 (1998).

Cohen-Tannoudji et al., I-SceI-Induced Gene Replacement at a Natural
Locus in Embryonic Stem Cells, 18 MOLECULAR AND CELLULAR
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BIOLOGY 1444-1448 (1998).

Pabo et al., DESIGN AND SELECTION OF NOVEL CYS2HIS2
ZINC FINGER PROTEINS, 70 ANNU. REV. BIOCHEM. 313-340 (2001).

M. Isalan and Y. Choo, Rapid, High-Throughput Engineering of
Sequence-Specific Zinc Finger DNA-Binding Proteins, 340 METHODS IN
ENZYMOLOGY 593-609 (2001).

Definition of the word “germ cell” (Online Free Medical Dictionary
definition of “germ cell”, 2010).

Appellant presents additional evidence in the Declarations filed under
37 C.F.R. § 1.132 of Dr. Ina Dobrinski,3 Dr. Andrew M. Scharenberg,4 and
Dr. Eckhard Wolf,5 all of which were filed November 15, 2011.

THE REJECTION
The following rejection is before us for review:
Claims 14-22 and 35-39 stand rejected under 35 U.S.C. § 103(a) as
unpatentable over Kucherlapati (‘205), Kucherlapati (‘598), Kucherlapati
(‘181), Kucherlapati (‘598*), Kucherlapati (‘835), Kucherlapati (‘584),
Kucherlapati (‘963), Kucherlapati (‘752), Kucherlapati (‘103), Kucherlapati
(‘986), Kucherlapati (‘610), Jakobovits (‘244), Jakobovits (‘893), Schooton,
Buelow (‘534), Buelow (‘880), Buelow (‘392), Buelow (‘263), Buelow
(‘001), Buelow (‘696), Buelow (‘398), Buelow (‘084), Buelow (‘668), or
Arnould (‘826), Arnould (‘949), Porteus, Vasquez, Donoho, or Cohen-
Tannoudji, Pabo, Isalan and the definition of “germ cell”.

3 Hereafter the “Dobrinski Declaration”.
4 Hereafter the “Scharenberg Declaration”.
5 Hereafter the “Wolf Declaration”.
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ANALYSIS
Independent claim 14 recites “[a] viable rodent germ cell having at
least one endogenous immunoglobulin (Ig) gene inactivated by the action of
at least one meganuclease” (App. Br., Clms. App’x.). In rejecting the
claims, the Examiner offers two different theories as to why the cited
references render the claimed germ cell obvious.
Under the first theory, the Examiner finds that Kucherlapati,
Jakobovits, Schooten, Buelow and Arnould (‘826) (i.e., the first 24
references cited)
taught methods of inactivating endogenous V
(variable), J (joining) and C (constant) Ig
(immunoglobulin) genes of mice and humanizing
the immunoglobulin gene to make human V, J and
C IG gene products. The mice whose genomes
have an inactivated IgG gene implicitly comprise
egg and sperm having an inactivated IgG gene
further comprising the human immunoglobulin
gene as indicated by reproduction of the mice and
germline transmission of the inactivated,
humanized Ig gene

(Ans. 7). Further, according to the Examiner,

[t]he first 24 references are not limited to ES cells
with an inactivated Ig gene inactivated because
they also taught transgenic mice whose genomes
have an inactivated IgG gene which inherently
comprise egg and sperm having an inactivated IgG
gene further comprising the human
immunoglobulin gene as evidenced by germline
transmission of the inactivated, humanized Ig gene
to [the] offspring
(Ans. 16).

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In the second theory, the Examiner takes the position that

ES [Embryonic Stem] cells are “germ cells”
because the term “germ cell” is defined as an
ovum or sperm cell or one of their developmental
precursors (see definition of “germ cell” provided,
Free Online Medical Dictionary, 2010), because
the term in the [S]pecification includes germ cells
and “precursors thereof” (pg 20, paragraph 140),
. . . Since ES cells become entire mice including
egg/sperm, they are “precursors” of egg/sperm.
Accordingly, the broadest reasonable interpretation
of “germ cell” encompasses ES cells because they
are germ line cells capable of becoming egg or
sperm

(Ans. 17-18). As such, the Examiner finds that “the ES cells with the
inactivated Ig genes used to make the transgenic mice taught in the first 24
references are also considered ‘germ cells’ as claimed” (Ans. 8).
In reference to either the first or second theory, the Examiner finds
that “[t]he first 24 references cited in the paragraph above did not teach the
endogenous V, J and C Ig genes were inactivated in germ cells by
meganuclease” (Ans. 8). The Examiner further finds that “using
meganuclease to inactivate genes in ES cells was well known in the art at the
time of filing” as described by Donoho, Cohen-Tannoudji, Porteus and
Vasquez (Ans. 8). The Examiner concludes that
it would have been obvious to those of ordinary
skill in the art at the time the invention was made
to inactivate an endogenous Ig gene in an ES cell
as described by the first 24 references cited using
meganuclease as described by Arnould, Porteus,
Vasquez, Donoho, or Cohen-Tannoudji. The
advantages of using meganuclease are discussed
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on pg 1447, Fig. 4 and col. 2, lines 10-22, of
Cohen-Tannoudji and throughout the secondary
references, i.e. increased targeting
(Ans. 9).
In response to the Examiner’s second theory, Appellant contends that
interpreting the definition of “germ cell” provided
by the cited Free Online Medical Dictionary as
encompassing an embryonic stem cell is clearly
erroneous because such characterization can only
occur if the Office (1) inappropriately dismisses
unrefuted fact evidence that the customary
meaning of “germ cell” given by those of ordinary
skill in the art does not encompass an embryonic
stem cell and (2) also improperly disregards the
fact that the proposed interpretation is inconsistent
with Appellant’s use of the term in the
[S]pecification
(App. Br. 11).
Appellant’s arguments are persuasive. Appellant’s Specification does
not expressly define the term “germ cell” or otherwise indicate that this term
is used in a manner other than its ordinary and customary meaning. The
Specification does describe that “[i]n one embodiment, the method involves
transfecting germ cells, which may include precursors thereof such as
spermatagonial stem cells” (Spec. 20, para. [00140]). We agree with
Appellant that an ordinary and customary meaning of the term “germ cell”6
is “a sexual reproduction cell” (see App. Br. 11), which is consistent with
Appellant’s use of this term in the Specification. We further agree with
Appellant that a skilled artisan would recognize that “precursors of germ

6 An ordinary and customary meaning of the term “germ cell” is “a gamete
(as an egg or sperm cell) or one of its antecedent cells” MERRIAM
WEBSTER’S COLLEGIATE DICTIONARY (11th ed. 2005).
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cells encompass the entire germ cell lineage from primordial germ cells,
gonia, and all subsequent differentiating germ cells up to the spermatozoa
and oocytes” and “[a]n embryonic stem cell would not be considered a
primordial germ cell [by a skilled artisan] since an embryonic stem cell is
not a sexual reproductive cell” (App. Br. 12; see also Dobrinski Declaration
¶¶ 6-7). Consequently, we agree with Appellant that “the plain meaning of
the term ‘germ cell,’ in light of the [S]pecification as it would be interpreted
by one of ordinary skill in the art, would not encompass an embryonic stem
cell” (App. Br. 12). Thus, we find the Examiner’s interpretation of the term
“germ cell” to encompass an “embryonic stem cell” to be unreasonable in
light of the claim and the Specification. See In re Cortright, 165 F.3d 1353,
1358 (Fed. Cir. 1999) (“Although the PTO must give claims their broadest
reasonable interpretation, this interpretation must be consistent with the one
that those skilled in the art would reach”).
In response to the Examiner’s first theory, Appellant contends that
the “inherent” germ cell asserted as prior art
against the instant claims can only result from the
otherwise unsupported combination of different
prior art teachings to produce a theoretical
embyronic stem cell, which could develop further
into a theoretical transgenic animal, which might
then have a theoretical germ cell asserted as prior
art, and all of which ignores the considerable
scientific uncertainties widely recognized and
explicitly acknowledged by skilled artisans with
such an approach

(App. Br. 16). Appellant further contends that
the first 24 references show that germ line
transmission of an inactivated gene from an animal
cultivated from a modified embyronic stem cell
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occurs only occasionally, and further, [] Donoho,
Cohen-Tannoudji, Porteus and Vasquez do not
teach mice with genes inactivated by a
meganuclease. Accordingly, there is no basis to
support the hypothesis that meganuclease mediated
gene inactivation in an embryonic stem cell will
necessarily result in germline transmission of the
inactivation upon cultivation of the ES cell into an
animal
(App. Br. 17).
The Examiner’s first theory is premised on the finding that transgenic
mice that comprise a genome having an IgG gene inactivated by a
meganuclease, would inherently comprise egg and sperm having an
inactivated IgG gene (Ans. 16). However, the Examiner has not established
with any evidence or provided any explanation on this record that
reproduction of transgenic mice in any of the first 24 prior art references
would inevitably, or necessarily, result in germline transmission of the
inactivated, humanized Ig gene to the offspring, such that the inactivated,
humanized gene necessarily is present in the germ cells of the offspring.
“Inherency . . . may not be established by probabilities or possibilities. The
mere fact that a certain thing may result from a given set of circumstances is
not sufficient.” MEHL/Biophile Int’l. Corp. v. Milgraum, 192 F.3d 1362,
1365 (Fed. Cir. 1999). “An inherent characteristic must be inevitable, and
not merely a possibility or probability.” See In re Oelrich, 666 F.2d 578,
581 (CCPA 1981).
The Examiner has not satisfied the initial burden of presenting a prima
facie case of obviousness. Accordingly, we are constrained to reverse the
Examiner’s rejection of claims 14-22 and 35-39 under 35 U.S.C. § 103(a) as
unpatentable over Kucherlapati (‘205), Kucherlapati (‘598), Kucherlapati
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(‘181), Kucherlapati (‘598*), Kucherlapati (‘835), Kucherlapati (‘584),
Kucherlapati (‘963), Kucherlapati (‘752), Kucherlapati (‘103), Kucherlapati
(‘986), Kucherlapati (‘610), Jakobovits (‘244), Jakobovits (‘893), Schooton,
Buelow (‘534), Buelow (‘880), Buelow (‘392), Buelow (‘263), Buelow
(‘001), Buelow (‘696), Buelow (‘398), Buelow (‘084), Buelow (‘668), or
Arnould (‘826), Arnould (‘949), Porteus, Vasquez, Donoho, or Cohen-
Tannoudji, Pabo, Isalan and the definition of “germ cell”.7

DECISION
We REVERSE the decision of the Examiner to reject claims 14-22
and 35-39.

REVERSED

Klh

7 Because we have determined that the Examiner failed to establish a prima
facie case of obviousness, we do not reach the evidence of secondary
considerations of non-obviousness of the Scharenberg and Wolf
Declarations.