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United States Court of Appeals
for the Federal Circuit
______________________
DANA-FARBER CANCER INSTITUTE, INC.,
Plaintiff-Appellee
v.
ONO PHARMACEUTICAL CO., LTD., TASUKU
HONJO, E.R. SQUIBB & SONS, L.L.C., BRISTOL-
MYERS SQUIBB COMPANY,
Defendants-Appellants
______________________
2019-2050
______________________
Appeal from the United States District Court for the
District of Massachusetts in No. 1:15-cv-13443-PBS,
United States District Judge Patti B. Saris.
______________________
Decided: July 14, 2020
______________________
DONALD ROSS WARE, Foley Hoag LLP, Boston, MA, ar-
gued for plaintiff-appellee. Also represented by SARAH S.
BURG, BARBARA A. FIACCO.
SETH P. WAXMAN, Wilmer Cutler Pickering Hale and
Dorr LLP, Washington, DC, argued for defendants-appel-
lants. Also represented by STEVEN JARED HORN, THOMAS
SAUNDERS; MATTHEW TYMANN, Los Angeles, CA; DIANNE B.
ELDERKIN, STEVEN D. MASLOWSKI, MATTHEW A. PEARSON,
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Akin, Gump, Strauss, Hauer & Feld, LLP, Philadelphia,
PA.
______________________
Before NEWMAN, LOURIE, and STOLL, Circuit Judges.
LOURIE, Circuit Judge.
Ono Pharmaceutical Co. Ltd., Tasuku Honjo, E.R.
Squibb & Sons, L.L.C., and Bristol-Myers Squibb Co. (col-
lectively, “Ono”) appeal from the judgment of the United
States District Court for the District of Massachusetts af-
ter a bench trial ordering that Dr. Gordon Freeman and Dr.
Clive Wood be added to U.S. Patents 7,595,048 (“the ’048
patent”), 8,168,179 (“the ’179 patent”), 8,728,474 (“the ’474
patent”), 9,067,999 (“the ’999 patent”), 9,073,994 (“the ’994
patent”), and 9,402,899 (“the ’899 patent”) as co-inventors.
Dana-Farber Cancer Inst., Inc. v. Ono Pharm. Co., 379 F.
Supp. 3d 53 (D. Mass. 2019) (“Decision”). Because we con-
clude that the district court did not err in its inventorship
determination, we affirm.
BACKGROUND
This appeal presents an inventorship dispute over
groundbreaking work in the field of cancer treatment.
Each patent at issue claims a method of treating cancer by
administering antibodies targeting specific receptor-ligand
interactions on T cells.
The human immune system comprises many different
cell types, but two types of those cells are relevant here:
dendritic cells and T cells. Dendritic cells detect pathogens
and present antigens—proteins from a pathogen or tu-
mor—to T cells. T cells have a variety of functions but, as
relevant here, are responsible for processing information to
develop an immune response in the body using receptors
on their surfaces. The primary receptor on a T cell, the T
cell receptor, can bind to antigens to activate an immune
response. But a signal sent to a T cell receptor will not
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activate the T cell unless a ligand binds to one of its co-
stimulatory receptors, such as CD28. CD28 has two lig-
ands, B7-1 and B7-2, which are expressed in dendritic cells
that have detected infection or cancer. For a T cell to acti-
vate an immune response, two things must happen: (1) an
antigen on a dendritic cell must bind to the T cell receptor,
and (2) a B7 ligand on the dendritic cell must bind to the
CD28 receptor on the T cell. In the absence of an infection
or cancer, dendritic cells do not express B7 ligands on their
surface thus blocking an immune response. B7 ligands also
bind to an inhibitory receptor called CTLA-4, which is only
expressed in highly activated T cells. B7 ligands bind more
tightly to CTLA-4 than to CD28, so if both receptors are
being expressed, CTLA-4 prevents the B7 ligands from ac-
tivating the T cell through the CD28 receptor.
The discovery behind the present patents was the ex-
istence of an inhibitory receptor on T cells, PD-1, and that,
when PD-1 binds to one of its ligands, either PD-L1 or PD-
L2, the T cell is inhibited and does not attack the cell ex-
pressing the ligand. Expression of the PD-1 ligands in
healthy cells generally shields them from attack, but some
tumor cells can also express the ligands, allowing them to
circumvent an immune response. The patents in this case
capitalize on the discovery of the PD-1 receptor-ligand in-
teraction. Each claim recites uses of antibodies that target
either the PD-1 receptor or its PD-L1 ligand, blocking the
receptor-ligand interaction. By blocking the interaction,
the use of the inventions in effect stimulates the immune
response against tumor cells that would otherwise have
been hidden by their expression of the PD-L1/L2 ligands.
The appeal raises the question whether Drs. Freeman
and Wood should be deemed inventors of the subject matter
of the ’048, ’179, ’474, ’999, ’994, and ’899 patents alongside
Dr. Tasuku Honjo. Essential to this determination is a re-
counting of each researcher’s work and the nature of their
collaboration.
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Dr. Honjo, a professor at Kyoto University’s medical
school, discovered the PD-1 receptor in the early 1990s. He
isolated its DNA sequence and began working with the pro-
tein in mouse models with Dr. Nagahiro Minato, a col-
league studying tumor immunology. Using knockout mice
(wherein the PD-1 gene is not expressed), they discovered
that mice without PD-1 showed symptoms typical of auto-
immune disease, suggesting that the receptor was involved
in immune-system inhibition. Based on its structure,
Dr. Honjo believed at that time that PD-1 was in the same
family of proteins as the inhibitory receptor CTLA-4.
Drs. Honjo and Minato submitted their research for publi-
cation, and their work was published in Immunity in Au-
gust 1999.
In mid-1998, Dr. Honjo enlisted a graduate student,
Dr. Yoshiko Iwai, to conduct studies on PD-1 with knockout
mice and human tumor cell lines. Dr. Iwai found binding
of the PD-1 protein in a variety of cells, including in tumor
cells, but she did not identify the molecule that was binding
to the receptor. She also recognized that her experiments
may have yielded false positives because she used a specific
fusion protein. Her work did not continue at that time be-
cause she took a leave of absence because of illness.
In September 1998, Dr. Honjo met with representa-
tives from Ono, now an assignee of Dr. Honjo’s rights in the
instant patents, and the Genetics Institute, who connected
him to Dr. Wood, a researcher at Genetics Institute. They
discussed Dr. Honjo’s work with PD-1, and Dr. Wood
agreed to collaborate with Dr. Honjo to find the PD-1 lig-
and. Dr. Wood believed that the PD-1 receptor could be a
candidate for antibody therapy development, and accord-
ingly Dr. Honjo shared with him PD-1 reagents and a con-
fidential draft of the Immunity article.
In July 1998, Dr. Freeman, a researcher at Dana-Far-
ber, was studying novel B7 ligands. He ran a search in the
BLAST database for a sequence of 208 amino acids that
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forms part of the binding portion of the B7-1 molecule. The
search yielded 12 results—two of which were from human
ovarian tumors—and Dr. Freeman began to investigate the
sequence further, titling it “292” after its label in the data-
base.
At this point, the timelines converge. Drs. Wood, Free-
man, and Honjo began sharing information directly.
Drs. Wood and Freeman began working together to deter-
mine whether PD-1 binds to 292, and Dr. Wood informed
Dr. Honjo that it does. The three dubbed 292 “PD-L1” and
ran further experiments. Dr. Wood sent Dr. Honjo plans
for a journal article, and Dr. Honjo sent Dr. Wood anti-
PD-1 antibodies for further experimentation. Dr. Freeman
emailed Dr. Honjo for the first time at this point, discussing
the possibility of a research collaboration on the
PD-1/PD-L1 pathway.
The collaboration culminated in a meeting in Cam-
bridge, Massachusetts in October 1999. At the meeting,
Dr. Wood disclosed that PD-1 and CTLA-4 had similar
structures and that PD-L1 antibodies inhibited the
PD-1/PD-L1 interaction. Dr. Freeman disclosed that 292
was from a human ovarian tumor and that PD-L1 shares
20% of its amino acid sequence with B7-1 and B7-2 but does
not bind to either CD28 or CTLA-4. Dr. Honjo disclosed his
unpublished knockout mouse data indicating that PD-1 in-
hibits the immune response.
After the meeting, the three began exchanging rea-
gents. Dr. Honjo ran in vitro experiments on the pathway
indicating that it inhibited the immune response, using
knockout mouse cells as a control. Drs. Freeman and Wood
filed a provisional patent application disclosing modulation
of the immune response via activating or blocking the PD-
1/PD-L1 pathway, but did not list Dr. Honjo as an inventor.
In the fall of 1999, Dr. Freeman conducted a second
BLAST search and identified another B7-like molecule
that shares 38% of its protein structure with PD-L1. Over
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the next year, Dr. Freeman conducted a number of experi-
ments on this ligand, which he labeled PD-L2.
In January 2000, Dr. Freeman asked Dr. David Dorf-
man, a pathologist at the Brigham and Women's Hospital,
and Dr. Julia Brown, a new postdoctoral researcher, to test
both normal and tumor tissues and determine whether PD-
L1 was expressed by them. Dr. Dorfman studied numerous
cell lines and found high PD-L1 expression in tumors, in-
cluding squamous cell carcinoma of the tongue, breast lob-
ular carcinoma, lung and colon adenocarcinoma, and
anaplastic large cell lymphoma. These immunohistochem-
istry results were not published until 2003.
In March 2000, Dr. Freeman emailed Dr. Honjo to tell
him about PD-L2 and to send its sequence. Drs. Honjo,
Freeman, and Wood then worked on a journal article docu-
menting their discoveries concerning PD-L1, and, in a final
round of edits in April 2000, Dr. Freeman added a sentence
to the paper stating that PD-L1 was also expressed in can-
cers and that some tumors may use PD-L1 to inhibit an
antitumor immune response. This article was published in
the Journal of Experimental Medicine on October 2, 2000.
Drs. Wood, Freeman, and Minato all separately devel-
oped antibody candidates. In March 2000, Drs. Wood and
Honjo presented results of their PD-1/PD-L1 collaborative
research at a conference. Dr. Iwai also resumed her knock-
out mice studies. By May 2000, Drs. Wood, Freeman, and
Honjo were discussing their development of anti-PD-L1 an-
tibodies and the possible use of those antibodies in treating
cancer.
In June 2000, Dr. Honjo learned of the 1999 provisional
application filed by Drs. Wood and Freeman, and chal-
lenged his exclusion as an inventor. By September, the
three had met again in Cambridge and Drs. Wood and
Freeman presented the results of their research on PD-L2.
Dr. Honjo presented some new data from Dr. Iwai’s knock-
out mice.
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In October, Dr. Iwai had generated data suggesting
that mouse melanoma tumors expressing PD-L1 grow
faster than tumors without PD-L1 expression. Ono identi-
fies October 2000 as the date Drs. Honjo, Iwai, and Minato
conceived the claimed inventions. As more data were gen-
erated by the Iwai experiments, Dr. Honjo stopped sharing
results with Drs. Freeman and Wood. The three met one
final time in April 2001.
Meanwhile, Dr. Honjo’s attorneys were pursuing his in-
ventorship claim, but Genetics Institute, the assignee of
Drs. Freeman and Wood’s patents, and its attorneys de-
clined to voluntarily add him to their patents. Genetics In-
stitute stated that Dr. Honjo could pursue his inventorship
claim at the PTO. Inventorship of those patents is not at
issue here.
In 2002, Dr. Honjo then filed his own patent applica-
tion in Japan, disclosing results from Drs. Honjo, Iwai, and
Minato’s experiments. Each patent at issue in this case
claims priority from Dr. Honjo’s Japanese patent applica-
tion; none include Drs. Freeman and Wood as inventors.
Because Dr. Freeman is an employee of Dana-Farber,
Dana-Farber is presumably the assignee of any rights he
has as an alleged inventor of any of the patents in suit.
Pfizer, which purchased Genetics Institute, is presumably
the assignee of any rights Dr. Wood has in the patents, but
Pfizer has transferred its potential interest in the patents
to Ono. None of these relationships is at issue here.
Dr. Freeman allegedly learned about the ’048 patent in
2010 but did not pursue litigation until 2015. Dr. Wood
may have known of the patents but did not get involved
until Dana-Farber filed this suit on behalf of Dr. Freeman.
In 2018, Dr. Honjo won the Nobel Prize in Physiology or
Medicine, and it is not without interest that in his ac-
ceptance speech he credited Dr. Freeman as a major collab-
orator in his work.
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The parties’ inventorship dispute began in the United
States District Court for the District of Massachusetts.
Dana-Farber brought suit alleging that Drs. Freeman and
Wood should be added as inventors on Dr. Honjo’s patents.
Dana-Farber presented an eight-point theory justifying
Drs. Freeman and Wood’s inventorship: (1) Dr. Freeman
found the 292 sequence; (2) Drs. Freeman and Wood jointly
disclosed PD-L1; (3) Drs. Freeman and Wood discovered
that PD-1/PD-L1 binding inhibits T cell activation; (4)
Dr. Freeman contributed the idea of treating cancer by
blocking the pathway in his April 2000 edits to the re-
searchers’ journal article; (5) Dr. Freeman provided rea-
gents that Dr. Iwai used in her mouse model; (6) Dr.
Freeman, through Dr. Dorfman, discovered that human
PD-L1 is expressed across a number of tumors; (7)
Drs. Freeman and Wood discovered PD-L2; and (8)
Drs. Freeman and Wood developed relevant antibodies.
In a 111-page opinion, the district court considered
each of Dana-Farber’s points. Ultimately, the court cred-
ited Drs. Freeman and Wood’s discovery of the PD-L1 lig-
and, Dr. Wood’s discovery that PD-1/PD-L1 binding
inhibits the immune response, Drs. Freeman and Wood’s
discovery that anti-PD-1 and anti-PD-L1 antibodies can
block the pathway’s inhibitory signal, and Dr. Freeman’s
immunohistochemistry experiments confirming PD-L1 ex-
pression in various tumors as contributions significant to
the conception of all six patents.
Ono appealed, and we have jurisdiction under 28
U.S.C. § 1295(a)(1).
DISCUSSION
District courts may order the correction of patent in-
ventorship by the U.S. Patent and Trademark Office “on
notice and hearing of all parties concerned.” 35 U.S.C.
§ 256(b). “[A] valid patent requires correct inventorship.”
In re VerHoef, 888 F.3d 1362, 1365 (Fed. Cir. 2018), as
amended (May 7, 2018). Inventorship is a question of law
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reviewed de novo, but the district court’s underlying find-
ings of fact are reviewed for clear error. Vapor Point LLC
v. Moorhead, 832 F.3d 1343, 1348 (Fed. Cir. 2016) (citing
Gen. Elec. Co. v. Wilkins, 750 F.3d 1324, 1329 (Fed. Cir.
2014) and then Trovan, Ltd. v. Sokymat SA, Irori, 299 F.3d
1292, 1301 (Fed. Cir. 2002)).
35 U.S.C. § 116(a) provides the standard for joint in-
ventorship:
When an invention is made by two or more persons
jointly, they shall apply for patent jointly and each
make the required oath, except as otherwise pro-
vided in this title. Inventors may apply for a patent
jointly even though (1) they did not physically work
together or at the same time, (2) each did not make
the same type or amount of contribution, or (3) each
did not make a contribution to the subject matter
of every claim of the patent.
Ono challenges the district court’s decision on two ba-
ses: (1) the district court’s legal analysis of conception, and
(2) the district court’s factual findings regarding inventor-
ship. We address each argument in turn.
A
Ono argues that as a matter of law the district court
erred by relying on contributions of Drs. Freeman and
Wood that were too far removed from the claimed subject
matter of the patents; it also argues that these contribu-
tions were made public and were hence in the prior art be-
fore the alleged conception. In Ono’s view, the patents
claim specific methods of treating cancer using PD-1 or PD-
L1 blocking antibodies, and Drs. Honjo and Minato dis-
cussed the possible use of PD-1 for treating cancer in Octo-
ber 2000 in conjunction with data received from Dr. Iwai’s
knockout mice experiments. Thus, Ono submits, these ex-
periments, performed independently of Drs. Freeman or
Wood, were what led directly to the conception of the
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claimed inventions, and the previous work was at most
speculative because it was not in vivo. Ono also notes that
the patents were issued over Drs. Freeman and Wood’s
1999 provisional application as evidence that the patents
claim treatments that were novel and nonobvious over Drs.
Freeman’s and Wood’s alleged contributions.
Ono also argues that Drs. Freeman’s and Wood’s al-
leged inventive contributions should be deemed irrelevant
to inventorship because their work with Dr. Honjo was
published in October 2000 in the Journal of Experimental
Medicine before conception of the patented inventions.
Ono urges us to adopt a legal rule that once a contribution
is made public, it “no longer qualifies as a significant con-
tribution to conception.” Appellants’ Br. 39.
Dana-Farber responds that Ono offers an erroneous
view of the law. According to Dana-Farber, Ono’s rule
would require each joint inventor to individually have con-
ceived the complete invention and have participated in a
particular moment of conception, which is inconsistent
with law.
We agree with Dana-Farber. Ono asks us to adopt an
unnecessarily heightened inventorship standard. “[A] joint
invention is simply the product of a collaboration between
two or more persons working together to solve the problem
addressed.” Fina Oil & Chem. Co. v. Ewen, 123 F.3d 1466,
1473 (Fed. Cir. 1997) (citing Burroughs Wellcome Co. v.
Barr Labs., Inc., 40 F.3d 1223, 1227 (Fed. Cir. 1994)). To
be a joint inventor, one must:
(1) contribute in some significant manner to the
conception or reduction to practice of the invention,
(2) make a contribution to the claimed invention
that is not insignificant in quality, when that con-
tribution is measured against the dimension of the
full invention, and (3) do more than merely explain
to the real inventors well-known concepts and/or
the current state of the art.
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Pannu v. Iolab Corp., 155 F.3d 1344, 1351 (Fed. Cir. 1998);
quoted in VerHoef, 888 F.3d at 1366. There is no “explicit
lower limit on the quantum or quality of inventive contri-
bution required for a person to qualify as a joint inventor.”
Eli Lilly & Co. v. Aradigm Corp., 376 F.3d 1352, 1358 (Fed.
Cir. 2004) (quoting Fina Oil, 123 F.3d at 1473). “People
may be joint inventors even though they do not physically
work on the invention together or at the same time, and
even though each does not make the same type or amount
of contribution.” Burroughs Wellcome, 40 F.3d at 1227 (cit-
ing 35 U.S.C. § 116).
Ono attacks the inventorship case for Drs. Freeman
and Wood on the ground that they failed to participate in
certain experiments that led to the conception of the
claimed invention, but the statute and our case law make
clear that joint inventors need not contribute to all aspects
of a conception. See, e.g., Eli Lilly, 376 F.3d at 1359–59; 35
U.S.C. § 116(a). That Drs. Freeman and Wood were not
present for or participants in all the experiments that led
to the conception of the claimed inventions does not negate
their overall contributions throughout their collaboration
with Dr. Honjo.
Ono’s argument that work from Drs. Honjo, Freeman,
and Wood’s collaboration was too speculative until the Oc-
tober 2000 knockout mice studies is likewise misguided.
Conception is the touchstone of the joint inventorship in-
quiry, Sewall v. Walters, 21 F.3d 411, 415 (Fed. Cir. 1994),
and conception is complete when an idea is definite and
permanent enough that one of skill in the art could under-
stand the invention, Burroughs Wellcome, 40 F.3d at 1228.
An inventor need not know, however, that an invention will
work for its intended purpose in order for conception to be
complete, as verification that an invention actually works
is part of its reduction to practice. Id. (citing Applegate v.
Scherer, 332 F.2d 571, 573 (CCPA 1964) and Oka v.
Youssefyeh, 849 F.2d 581, 584 n.1 (Fed. Cir. 1988)). While
Dr. Iwai’s work provided important in vivo data, in vivo
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verification is not required for a conception to be definite
and permanent. See In re Isaacs, 347 F.2d 887, 889 (CCPA
1965) (holding that in vivo testing was not required to es-
tablish utility for claims to interferon). Moreover, the rec-
ord is clear that Dr. Iwai’s work was conducted after Dr.
Freeman had shown expression of PD-L1 in human tumors
and Dr. Honjo had shown that PD-L1 expression causes tu-
mor growth, so as a factual matter, PD-L1’s potential util-
ity in treating human cancers was developed jointly with
Dr. Freeman before Dr. Iwai’s work.
Ono also argues that the Honjo patents were issued
over Drs. Freeman and Wood’s 1999 provisional patent ap-
plication, so the latter contributions were thus not signifi-
cant to the dispute over inventorship of Dr. Honjo’s
patents. As a factual matter, it is unclear that Drs. Free-
man and Wood’s contributions to the inventions are co-ex-
tensive with the disclosure of their provisional application.
Regardless, joint inventorship does not depend on whether
a claimed invention is novel or nonobvious over a particu-
lar researcher’s contribution. Collaboration and concerted
effort are what result in joint inventorship. Eli Lilly, 376
F.3d at 1359. The novelty and nonobviousness of the
claimed inventions over the provisional application are not
probative of whether the collaborative research efforts of
Drs. Honjo, Freeman, and Wood led to the inventions
claimed here or whether each researcher’s contributions
were significant to their conception.
Ono also urges us to hold categorically that research
made public before the date of conception of a total inven-
tion cannot qualify as a significant contribution to concep-
tion of the total invention. Such a rule would ignore the
realities of collaboration, especially that collaboration gen-
erally spans a period of time and may involve multiple con-
tributions. It is certainly true that simply informing
another about the state of the prior art does not make one
a joint inventor. Hess v. Advanced Cardiovascular Sys.,
Inc., 106 F.3d 976, 981 (Fed. Cir. 1997) (holding that
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explaining the state of the art and providing well-known
information found in textbooks was insufficient for joint in-
ventorship). But a collaborative enterprise is not negated
by a joint inventor disclosing ideas less than the total in-
vention to others, especially when, as here, the collabora-
tors had worked together for around one year prior to the
disclosure, and the disclosure occurred just a few weeks
prior to conception. Inventorship of a complex invention
may depend on partial contributions to conception over
time, and there is no principled reason to discount genuine
contributions made by collaborators because portions of
that work were published prior to conception for the benefit
of the public. Earlier publication of an invention is obvi-
ously a potential hazard to patentability, but publication of
a portion of a complex invention does not necessarily defeat
joint inventorship of that invention, and it does not here.
B
Next, Ono raises a series of challenges to the district
court’s factual analysis for each patent. We begin where
Ono focuses the majority of its argument, the ’474 patent.
i. ’474 patent
Claim 1 of the ’474 patent recites a “method for treat-
ment of a tumor in a patient, comprising administering to
the patient a pharmaceutically effective amount of an anti-
PD-1 monoclonal antibody.” ’474 patent col. 25 ll. 13–15.
According to Ono, Dr. Freeman’s alleged contribution to
discovering PD-L1 was locating the 292 sequence in the
BLAST database, but he played no meaningful role in the
discovery that the PD-1/PD-L1 pathway is inhibitory. Ono
also contends that Dr. Freeman’s work is not a significant
contribution to the invention of the ’474 patent because the
’474 patent claims rely on anti-PD-1 antibodies, not PD-L1
antibodies.
Ono argues that Dr. Wood likewise should not be cred-
ited as a joint inventor on the ’474 patent because his work
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on the PD-L1 pathway was not a significant contribution
to the claims. Ono submits that the district court over-
stated Dr. Wood’s contributions and that Dr. Wood’s work
merely confirmed information that Dr. Honjo had already
discovered.
Dana-Farber responds that Ono failed to argue that
the inventors’ contributions differ from patent to patent be-
fore the district court. According to Dana-Farber, “the
claimed methods are all based on conception of the same
core invention: blocking the PD-1/PD-L1 interaction so that
the tumor cannot use the pathway to evade immune sys-
tem attack.” Appellees’ Br. 41 (emphasis omitted). Dana-
Farber cites the district court’s fact finding that knowing
the structure and function of PD-L1 was essential to all the
claimed inventions.
We agree with Dana-Farber, and with the district
court, that Drs. Freeman and Wood are joint inventors of
the ’474 patent. The ’474 patent claims use of anti-PD-1
antibodies in treating cancer and does not explicitly men-
tion PD-L1. But PD-1 is just a receptor. Unless one also
knows that the PD-1 receptor binds to at least one ligand
that inhibits the immune response, such as PD-L1, there
would be no reason to use anti-PD-1 antibodies to treat tu-
mors. The ’474 patent claims need not explicitly recite PD-
L1 for research on PD-L1 to have been a significant contri-
bution to conception of the invention.
The record certainly confirms this reality. The district
court credited testimony from Dana-Farber’s expert, Dr.
Kenneth Murphy, that not all antibodies that bind to a re-
ceptor or ligand block the signal. Ono’s expert, Dr. Mark
Greene, did not contest that Dr. Honjo needed to under-
stand the receptor-ligand interaction to develop effective
therapeutic antibodies. But even apart from expert testi-
mony, Dr. Honjo’s own efforts underscore the importance
of understanding the receptor-ligand relationship to con-
ception. In 1992, Dr. Honjo discovered PD-1 and theorized
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that it played a role in inhibiting the immune response.
But despite having this knowledge, Dr. Honjo still enlisted
collaboration with the Genetics Institute to search for lig-
ands for PD-1. Even under Ono’s view of the facts,
knowledge of PD-1 was itself insufficient for Dr. Honjo to
conceive of the method claimed in the ’474 patent.
It is clear based on the record that Drs. Freeman and
Wood both contributed to conception of the ’474 patent. Dr.
Freeman connected the 292 sequence to PD-1 and directed
important immunohistochemistry experiments revealing
that several types of tumors express PD-L1. Dr. Wood pro-
vided Dr. Honjo with the first confirmation that the PD-
1/PD-L1 interaction was inhibitory, supported by experi-
mental data. Drs. Freeman and Wood’s work on PD-L1,
Dr. Wood’s discovery that the PD-1/PD-L1 interaction in-
hibits the immune response, and Dr. Freeman’s discovery
of PD-L1 expression by human tumors were significant
building blocks upon which the ’474 patent is built.
ii. The remaining patents
Each of the remaining patents recites treatment of tu-
mors, lung cancer, or melanoma by administering anti-PD-
1 or anti-PD-L1 antibodies. Ono makes arguments about
the remaining patents, but each argument depends signif-
icantly on our acceptance of its arguments regarding the
’474 patent. As we concluded above, discovery of PD-1 in a
vacuum was insufficient for conception. Drs. Freeman and
Wood’s work linking PD-1 to its ligand and expression in
tumors was a significant contribution to each of these pa-
tents’ conception.
Ultimately, the decision in this appeal rests on the ex-
tensive factual determinations made by the district court
relating to the work performed together by Drs. Wood and
Freeman, and Dr. Honjo that were not clearly erroneous,
and the court made no errors of law.
Case: 19-2050 Document: 49 Page: 16 Filed: 07/14/2020
16 DANA-FARBER CANCER INSTITUTE v. ONO PHARMACEUTICAL
CO., LTD.
CONCLUSION
We have considered the parties’ remaining arguments
but find them unpersuasive. Because we conclude that the
district court did not err in holding Drs. Freeman and Wood
should be included as joint inventors of the ’048, ’179, ’474,
’999, ’994, and ’899 patents, we affirm the district court’s
conclusions.
AFFIRMED