LOURIE, Circuit Judge.
Baxter International, Inc. (Baxter) appeals from the February 28, 1991, decision of the United States Patent and Trademark Office Board of Patent Appeals and Interferences, Appeal No. 90-2204. The Board affirmed the rejection of claims 1, 3-12,14-16, 20-23, and 29-37, in a reexamination of U.S. Patent 4,222,379 (the Smith patent) as anticipated under 35 U.S.C. § 102(b). The Board also affirmed the rejection of claims 1-24 as obvious under 35 U.S.C. § 103. Claims 25-28 were allowed by the examiner and are not in issue. We affirm.
BACKGROUND
The Smith invention relates to a multiple blood bag system for collecting, processing and storing the therapeutic components of whole blood (red blood cells, plasma, and platelets).
The system includes a first (donor) bag for collection and storage of the red blood cells and at least one second (transfer) bag
for collection and storage of another blood component. According to the Smith invention, the donor bag contains a hemolysis-suppressing, blood-leachable plasticizer, di-2-ethylhexyl phthalate (DEHP), whereas the second bag is made of a different plastic polymer, free of blood leachable plasticizer. Prior to the time of the Smith invention, the industry used DEHP as a plasticizer in blood storage bags, but desired to eliminate DEHP due to concern about its possible deleterious effects. It was discovered by another Baxter employee that DEHP had the apparently unexpected effect of suppressing hemolysis in red blood cells, thus making it desirable to store red blood cells in bags containing
DEHP. The Smith patent claimed this discovery as a multiple bag system.
On October 16, 1987, Baxter filed a request for reexamination of the Smith patent. With the request, Baxter submitted a copy of a document entitled “Contract PH 43-67-1403; Final Technical Progress Report; Development of Containers for Preservation of Frozen Blood Components” (Becker document). This document, describing a new blood bag system, was authored by Mr. Becker, a Baxter employee, in October 1969 and was discovered during preparation for an earlier interference proceeding. Mr. Becker’s testimony, taken during the earlier proceeding, was also submitted. In reexamination, the examiner rejected most of the patent claims over the Becker reference and the Board affirmed. Baxter then appealed to this court.
DISCUSSION
A. Anticipation
Anticipation is a question of fact. Therefore, we will not reverse the Board’s finding of anticipation unless it is clearly erroneous.
In re Bond,
910 F.2d 831, 833, 15 USPQ2d 1566, 1567 (Fed.Cir.1990).
The Board found that the Becker document taught both two- and three-blood bag systems in which the primary or donor bag was made of polyvinyl chloride (PYC) and a secondary or satellite bag was made of unplasticized Teflon®. The Board also found that one skilled in the art would have known that the primary bag was plasticized with DEHP, thereby anticipating the Smith invention. We agree.
In describing its blood bag system, the Becker document makes two references to then-available commercial blood bag systems. The most significant reference is on page 49, where Becker describes his double blood pack system design as “very similar to [Baxter] Travenol’s commercial, two bag blood container. The exception is that the secondary transfer pack was a 350 ml Teflon container_” The Board was correct in characterizing the dispositive question regarding anticipation as whether one skilled in the art would reasonably understand or infer from the Becker document’s teaching that Becker’s primary bag was plasticized with DEHP. As Baxter notes, there is no express reference to DEHP in the Becker document.
Testimony from those skilled in the art, through depositions and declarations, and Baxter’s own admissions, established that Baxter’s commercial systems during this time period all contained a primary bag plasticized with DEHP. Therefore, since Becker referred to Baxter’s commercial system and Baxter’s commercial systems utilized a DEHP-plasticized primary bag, it is clear that one skilled in the art would have known that Becker was referring to a DEHP-plasticized primary bag. That fact, coupled with Becker’s disclosure that the second bag was made of Teflon®, leads to the unmistakable conclusion that the claims at issue were anticipated.
Baxter argues that these depositions, declarations, and admissions are extrinsic evidence, which may not be considered when determining the anticipatory teaching of a reference. This is incorrect. Baxter acknowledges, as it must, that extrinsic evidence may be considered when it is used to explain, but not expand, the meaning of a reference.
Scripps Clinic & Research Foundation v. Genentech, Inc.,
927 F.2d 1565, 1576-77, 18 USPQ2d 1001, 1010 (Fed.Cir.1991). Here, the depositions and declarations of skilled workers and Baxter’s admissions were used to identify what materials Baxter’s commercial bags contained at the time of the Becker document, thereby explaining what the phrase “[Baxter] Tra-venol’s commercial, two blood bag container” would have meant to one skilled in the art. This evidence clearly shows that those skilled in the art, reading the Becker document, would have known that Becker’s primary bag was plasticized with DEHP.
Additionally, Becker testified during the earlier interference that the primary bag in “[Baxter] Travenol’s commercial, two bag blood container,” to which he referred, contained DEHP. Baxter argues that this too is improperly considered extrinsic evidence and that we must look only at what the Becker document said, not at what Becker
himself did. This, however, is precisely what the Board did in considering the testimony. Becker’s testimony merely explained what he meant when using the phrase, “[Baxter] Travenol’s commercial, two blood bag container.” Although Baxter in its briefs to us questions the propriety of using Becker’s testimony, the Board’s decision did not depend solely upon it, nor does ours.
Baxter further argues that the Becker system was experimental, not FDA approved. Therefore, one skilled in the art would not necessarily have thought that Becker’s primary bag must have been plasticized with the only FDA approved plasticizer (DEHP), since there were other nonDEHP (non-FDA approved) plasticizers available at that time. This argument is not persuasive. The fact that Becker’s system was experimental is irrelevant. Becker taught use of the primary bag from Baxter’s commercial system, which was plasticized with DEHP. Therefore, all the elements of the Smith claims were disclosed in the Becker document and that is sufficient for anticipation.
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LOURIE, Circuit Judge.
Baxter International, Inc. (Baxter) appeals from the February 28, 1991, decision of the United States Patent and Trademark Office Board of Patent Appeals and Interferences, Appeal No. 90-2204. The Board affirmed the rejection of claims 1, 3-12,14-16, 20-23, and 29-37, in a reexamination of U.S. Patent 4,222,379 (the Smith patent) as anticipated under 35 U.S.C. § 102(b). The Board also affirmed the rejection of claims 1-24 as obvious under 35 U.S.C. § 103. Claims 25-28 were allowed by the examiner and are not in issue. We affirm.
BACKGROUND
The Smith invention relates to a multiple blood bag system for collecting, processing and storing the therapeutic components of whole blood (red blood cells, plasma, and platelets).
The system includes a first (donor) bag for collection and storage of the red blood cells and at least one second (transfer) bag
for collection and storage of another blood component. According to the Smith invention, the donor bag contains a hemolysis-suppressing, blood-leachable plasticizer, di-2-ethylhexyl phthalate (DEHP), whereas the second bag is made of a different plastic polymer, free of blood leachable plasticizer. Prior to the time of the Smith invention, the industry used DEHP as a plasticizer in blood storage bags, but desired to eliminate DEHP due to concern about its possible deleterious effects. It was discovered by another Baxter employee that DEHP had the apparently unexpected effect of suppressing hemolysis in red blood cells, thus making it desirable to store red blood cells in bags containing
DEHP. The Smith patent claimed this discovery as a multiple bag system.
On October 16, 1987, Baxter filed a request for reexamination of the Smith patent. With the request, Baxter submitted a copy of a document entitled “Contract PH 43-67-1403; Final Technical Progress Report; Development of Containers for Preservation of Frozen Blood Components” (Becker document). This document, describing a new blood bag system, was authored by Mr. Becker, a Baxter employee, in October 1969 and was discovered during preparation for an earlier interference proceeding. Mr. Becker’s testimony, taken during the earlier proceeding, was also submitted. In reexamination, the examiner rejected most of the patent claims over the Becker reference and the Board affirmed. Baxter then appealed to this court.
DISCUSSION
A. Anticipation
Anticipation is a question of fact. Therefore, we will not reverse the Board’s finding of anticipation unless it is clearly erroneous.
In re Bond,
910 F.2d 831, 833, 15 USPQ2d 1566, 1567 (Fed.Cir.1990).
The Board found that the Becker document taught both two- and three-blood bag systems in which the primary or donor bag was made of polyvinyl chloride (PYC) and a secondary or satellite bag was made of unplasticized Teflon®. The Board also found that one skilled in the art would have known that the primary bag was plasticized with DEHP, thereby anticipating the Smith invention. We agree.
In describing its blood bag system, the Becker document makes two references to then-available commercial blood bag systems. The most significant reference is on page 49, where Becker describes his double blood pack system design as “very similar to [Baxter] Travenol’s commercial, two bag blood container. The exception is that the secondary transfer pack was a 350 ml Teflon container_” The Board was correct in characterizing the dispositive question regarding anticipation as whether one skilled in the art would reasonably understand or infer from the Becker document’s teaching that Becker’s primary bag was plasticized with DEHP. As Baxter notes, there is no express reference to DEHP in the Becker document.
Testimony from those skilled in the art, through depositions and declarations, and Baxter’s own admissions, established that Baxter’s commercial systems during this time period all contained a primary bag plasticized with DEHP. Therefore, since Becker referred to Baxter’s commercial system and Baxter’s commercial systems utilized a DEHP-plasticized primary bag, it is clear that one skilled in the art would have known that Becker was referring to a DEHP-plasticized primary bag. That fact, coupled with Becker’s disclosure that the second bag was made of Teflon®, leads to the unmistakable conclusion that the claims at issue were anticipated.
Baxter argues that these depositions, declarations, and admissions are extrinsic evidence, which may not be considered when determining the anticipatory teaching of a reference. This is incorrect. Baxter acknowledges, as it must, that extrinsic evidence may be considered when it is used to explain, but not expand, the meaning of a reference.
Scripps Clinic & Research Foundation v. Genentech, Inc.,
927 F.2d 1565, 1576-77, 18 USPQ2d 1001, 1010 (Fed.Cir.1991). Here, the depositions and declarations of skilled workers and Baxter’s admissions were used to identify what materials Baxter’s commercial bags contained at the time of the Becker document, thereby explaining what the phrase “[Baxter] Tra-venol’s commercial, two blood bag container” would have meant to one skilled in the art. This evidence clearly shows that those skilled in the art, reading the Becker document, would have known that Becker’s primary bag was plasticized with DEHP.
Additionally, Becker testified during the earlier interference that the primary bag in “[Baxter] Travenol’s commercial, two bag blood container,” to which he referred, contained DEHP. Baxter argues that this too is improperly considered extrinsic evidence and that we must look only at what the Becker document said, not at what Becker
himself did. This, however, is precisely what the Board did in considering the testimony. Becker’s testimony merely explained what he meant when using the phrase, “[Baxter] Travenol’s commercial, two blood bag container.” Although Baxter in its briefs to us questions the propriety of using Becker’s testimony, the Board’s decision did not depend solely upon it, nor does ours.
Baxter further argues that the Becker system was experimental, not FDA approved. Therefore, one skilled in the art would not necessarily have thought that Becker’s primary bag must have been plasticized with the only FDA approved plasticizer (DEHP), since there were other nonDEHP (non-FDA approved) plasticizers available at that time. This argument is not persuasive. The fact that Becker’s system was experimental is irrelevant. Becker taught use of the primary bag from Baxter’s commercial system, which was plasticized with DEHP. Therefore, all the elements of the Smith claims were disclosed in the Becker document and that is sufficient for anticipation. Neither the fact that FDA approval was not needed nor the availability of other materials affects the result, since the evidence showed that the Becker reference disclosed the claimed invention, including a donor bag plasticized with DEHP.
The Board therefore properly concluded that one skilled in the art would have known that Becker was referring to a DEHP-plasticized primary bag and a Teflon® secondary bag, a combination within the scope of the appealed claims. Since we do not find the Board’s conclusion to be clearly erroneous, we affirm its finding that claims 1, 3-12,14-16, 20-23, and 29-37 were anticipated by the Becker document.
B. Obviousness
The Board affirmed the rejection of claims 1-24 as obvious. Since we have agreed that Becker anticipates the subject matter of claims 1, 3-12, 14-16, 20-23, and 29-37, and since anticipation is the ultimate of obviousness,
see In re Fracalossi,
681 F.2d 792, 794, 215 USPQ 569, 571 (CCPA 1982), the subject matter of these claims is necessarily obvious and we need not consider them further.
As for claims 2, 13, 17-19, and 24, which were rejected only for obviousness, Baxter has conceded that these claims stand or fall together. The Board found that in addition to the express teachings of Becker, the admitted knowledge in the prior art
established that it would have been prima facie obvious to plasticize the donor bag with DEHP and to construct the second bag from materials exhibiting different physical characteristics. We affirm on another basis.
Baxter has not argued nonobviousness with any particularity. Instead, its arguments are based on its premise that the Becker document fails to describe a system containing a DEHP primary. Although claims 2, 13, 17-19, and 24 stand rejected solely under § 103, Baxter has not argued the merits of any specific claim demonstrating nonobviousness. Rather, Baxter has rested its argument on the general premise that Becker would not have suggested to one skilled in the art that the primary bag was plasticized with DEHP, essentially the same argument advanced to rebut the anticipation rejection. It is not the function of this court to examine the claims in greater detail than argued by an appellant, looking for nonobvious distinctions over the prior art. Since we have determined that the Becker document would have taught use of a DEHP-plasti-cized donor bag, we affirm the rejection of the remaining claims as obvious.
Baxter also argues that commercial success and unexpected results rebut a prima facie finding of obviousness. Since Baxter has not effectively argued that these particular claims differ from what is disclosed
in Becker, this argument must fail. Moreover, information solely on numbers of units sold is insufficient to establish commercial success.
See Kansas Jack, Inc. v. Kuhn,
719 F.2d 1144, 1151, 219 USPQ 857, 861 (Fed.Cir.1983). The evidence of commercial success cited by Baxter includes only the percentage of
its
blood bag sales accounted for by the Smith system. No market share information was provided beyond saying that the bags were “significantly favored” by users. Baxter’s evidence that most of its commercial bags were within the scope of the patent claims is not sufficient to establish commercial success.
Finally, Baxter argues that the unexpected hemolysis-suppression quality of DEHP rebuts any prima facie showing of obviousness. However, when unexpected results are used as evidence of non-obviousness, the results must be shown to be unexpected compared with the closest prior art.
In re De Blauwe,
736 F.2d 699, 705, 222 USPQ 191, 196 (Fed.Cir.1984). Here, the closest prior art was the Becker system, utilizing a DEHP primary bag. Mere recognition of latent properties in the prior art does not render nonobvious an otherwise known invention.
In re Prindle,
297 F.2d 251, 254, 132 USPQ 282, 283-84 (CCPA 1962). Since the prior art bags plasticized with DEHP were inherently suppressing hemolysis, albeit unknown at the time of the Becker document, this he-molysis-suppressing function is not a basis for rebutting a prima facie finding of obviousness.
We have considered Baxter’s other arguments and have found them to be unpersuasive.
CONCLUSION
For the foregoing reasons, the decision of the Board is
AFFIRMED.