Ex Parte GillisDownload PDFPatent Trial and Appeal BoardMay 28, 201311542221 (P.T.A.B. May. 28, 2013) Copy Citation UNITED STATES PATENT AND TRADEMARK OFFICE UNITED STATES DEPARTMENT OF COMMERCE United States Patent and Trademark Office Address: COMMISSIONER FOR PATENTS P.O. Box 1450 Alexandria, Virginia 22313-1450 www.uspto.gov APPLICATION NO. FILING DATE FIRST NAMED INVENTOR ATTORNEY DOCKET NO. CONFIRMATION NO. 11/542,221 10/04/2006 John R. Gillis 6777 4025 6858 7590 05/28/2013 BREINER & BREINER, L.L.C. 115 NORTH HENRY STREET ALEXANDRIA, VA 22314 EXAMINER SHAHNAN SHAH, KHATOL S ART UNIT PAPER NUMBER 1645 MAIL DATE DELIVERY MODE 05/28/2013 PAPER Please find below and/or attached an Office communication concerning this application or proceeding. The time period for reply, if any, is set in the attached communication. PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE __________ BEFORE THE PATENT TRIAL AND APPEAL BOARD __________ Ex parte JOHN R. GILLIS __________ Appeal 2012-002780 Application 11/542,221 Technology Center 1600 __________ Before MELANIE L. McCOLLUM, JEFFREY N. FREDMAN, and ULRIKE W. JENKS, Administrative Patent Judges. FREDMAN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal 1 under 35 U.S.C. § 134 involving claims to a process for automated evaluation of sterility test indicators. The Examiner rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. 1 Appellant identifies the Real Party in Interest as SGM Biotech, Inc. (App. Br. 2). Appeal 2012-002780 Application 11/542,221 2 Statement of the Case Background “This invention relates to automated procedures for monitoring sterility test-indicators individually for results following intended exposure of a test-ampoule to a selected microbial-biocidal treatment cycle” (Spec. 1 ¶ 0002). The Claims Claims 1-9, 17, and 18 are on appeal. Claim 1 is representative and reads as follows: 1. Process for automated-evaluation and authenticated documentation of effectiveness, or absence thereof, of selected individual microbial-biocidal treatment-cycles, comprising A) providing a housing-structure, presenting (i) individual test-cell receptacles, each for receiving an individual biological indication (B-I) Test-Ampoule, for (ii) evaluating, subsequent to intended exposure to a designated microbial-biocidal treatment-cycle, (iii) biocidal effectiveness, or absence thereof, of such treatment-cycle on a B-I Test-Ampoule within an individual housing-structure test-cell; B) correlating (i) size and configuration of an individual B-I Test-Ampoule, with respect to (ii) size and configuration of such an individual receptacle, (iii) inserting such Test-Ampoule into such correlated size and configuration receptacle, for purposes of C) biologically evaluating effectiveness following completion of such selected microbial-biocidal treatment-cycle, by (i) automatically-controlling: (a) heating within such housing-structure for establishing incubation conditions, Appeal 2012-002780 Application 11/542,221 3 (b) establishing a selected incubation temperature within such B-I Test-Ampoule, and (ii) recording time of establishment of incubation temperature, within (iii) such correlated size and configuration B-1 Test Ampoule, for (a) evaluating intended microbial-biocidal results within such Test-Indicator; or, alternatively - (b) evaluating microbial-activity, (iv) within such Test-Ampoule; and (v) wherein each B-I Test-Ampoule in each test-cell is evaluated by a separate source of radiant energy and a photo-detector for said radiant energy. The issues A. The Examiner rejected claims 1-9, 17, and 18 under 35 U.S.C. § 103(a) as obvious over Bolea 2 and Gillis 3 (Ans. 4-5). B. The Examiner rejected claims 1-9, 17, and 18 under 35 U.S.C. § 112, first paragraph as failing to comply with the written description requirement by incorporating new matter (Ans. 5-6). A. 35 U.S.C. § 103(a) over Bolea and Gillis The Examiner finds that Bolea et al. teach a process and apparatus for automated- evaluation and authenticated documentation of effectiveness, or absence thereof, of selected individual microbial-biocidal treatment-cycles, comprising providing a housing-structure, presenting individual test-cell receptacles, each for receiving an individual biological-indication (B-1) test-Ampoule. (See abstract and claims). Bolea et al. teach visible means such as fluorescence in response to biological 2 Bolea et al., US 6,025,189, issued Feb. 15, 2000. 3 Gillis, J., US 6,455,272 B1, issued Sep. 24, 2002. Appeal 2012-002780 Application 11/542,221 4 activity (see abstract). As to new added limitation in step(v), Bolea also teaches separate source of energy that each B-1 test Ampoule is tested (Ans. 4-5). The Examiner finds that “Bolea et al. do not teach Bromocresol purple and spectroscopic quantitative measurement” (Ans. 5). The Examiner finds that “Gillis teach Bromocresol purple, see claims specially claim 3. Gillis teach spectroscopic quantitative measurement” (Ans. 5). The Examiner finds it obvious “to combine the teachings of Bolea et al. and Gillis to obtain the instant invention because Bolea et al. teach an apparatus which reads a plurality of biological indicators to determine the efficacy of a plurality of sterilization cycles” (Ans. 5). The issue with respect to this rejection is: Does the evidence of record support the Examiner‟s conclusion that Bolea and Gillis render claim 1 obvious? Findings of Fact 1. Bolea teaches “a system for determining the efficacy of a sterilization cycle. More specifically, the present invention relates to a system for reading fluorescence from a biological sterility indicator in order to determine the efficacy of the sterilization cycle” (Bolea, col. 1, ll. 15-19). 2. Bolea teaches that An apparatus reads a plurality of biological indicators contained in a biological indicator vessel (the indicator and the vessel being collectively referred to as a BI) to determine efficacy of a plurality of sterilization cycles. Each BI exhibits fluorescence in response to biological activity indicative of bacterial growth in the vessel. A plurality of BI holders are each configured to receive one of the BIs. A Appeal 2012-002780 Application 11/542,221 5 carriage is controllably movable relative to the plurality of BI holders to positions proximate each of the BI holders. A radiation emitter is mounted on the carriage and is positioned to impinge radiation on a BI received in a selected BI holder. A fluorescence sensor is also mounted on the carriage and is positioned to sense fluorescence exhibited by the BI in the selected BI holder in response to the radiation. A controller is coupled to the fluorescence sensor to receive a fluorescence signal and to provide an output signal indicative of the fluorescence sensed. The controller is configured to control the position of the carriage to intermittently position the carriage proximate each of the BI holders then holding a BI. A memory is coupled to the controller and is configured to receive and store data indicative of the fluorescence of each BI based on the fluorescence signals received by the controller. (Bolea, col. 3, ll. 16-38.) 3. Bolea teaches that a “BI reading apparatus 10 includes housing 12, which provides a plurality of DI receiving wells 14” (Bolea, col. 4, ll. 24-26). 4. Bolea teaches that a “BI 22 is first placed in a sterilizer along with the other devices or equipment to be sterilized. Then, the sterilization cycle is performed. The sterilization cycle may typically include steam sterilization, dry heat sterilization, or chemical or radiation sterilization techniques.” (Bolea, col. 6, ll. 12-16.) 5. Bolea teaches that “[d]ifferent time frames, temperature regimes and sterilization cycles require the use of different types of BIs, as is known” (Bolea, col. 6, ll. 16-18). Appeal 2012-002780 Application 11/542,221 6 6. Bolea teaches that the operator then, in one preferred embodiment, inputs into reading apparatus 10 (preferably through operator interface 19) the particular type of BI being used as BI 22. This accomplishes a number of things. First, the particular type of BI being used indicates microprocessor 32 the correct set point for the heater 48 or 50 associated with the reading well 14 into which the BI 22 will be placed. For instance, one type of BI may require incubation at approximately 60° C. while another type may require incubation at approximately 37° C. . . . In any case, microprocessor 32 preferably controls the heaters to desired set points with closed loop control (Bolea, col. 6, ll. 20-32). 7. Bolea teaches that “based on the type of BI being used, microprocessor 32 retrieves from memory corresponding fluorescent kinetic behavior information for use in providing the efficacy output. The kinetic information is preferably indicative of the fluorescent behavior of the particular BI under circumstances in which the sterilization cycle to which it was exposed has been efficacious and non-efficacious” (Bolea, col. 6, ll. 34- 40). 8. Bolea teaches that: After the baseline reading is obtained, microprocessor 32 waits for a designated time out. The length of the time out will correspond to the particular BI type being used, and how fast spore growth activity is expected to occur . . . After the desired time out, another florescence reading is taken from the particular BI 22 . . . If microprocessor 32 determines that the second florescence reading exceeds the baseline florescence reading by a statistically significant amount, that means that a statistically significant amount of biological activity (spore growth) has occurred in BI 22 Appeal 2012-002780 Application 11/542,221 7 during the incubation cycle. Thus, the sterilization cycle has not been efficacious. Microprocessor 32 therefore provides an output to display panel 16 indicating that the sterilization cycle has not been efficacious. (Bolea, col. 8, ll. 14-42.) 9. Bolea teaches an embodiment where “a plurality of independently controllable heaters are provided so that different types of biological indicators can be incubated and read by a single system” (Bolea, col. 3, ll. 43-46). 10. Figure 1 of Bolea is reproduced below: “FIG. 1 is a perspective view of a biological indicator apparatus” (Bolea, col. 3, ll. 56-57). 11. Bolea teaches that in “one preferred embodiment, a BI presence sensor 52 is associated with each BI receiving well 14” (Bolea, col. 5, ll. 62- 63). Appeal 2012-002780 Application 11/542,221 8 12. Bolea teaches that “where the BI presence sensor is an electro- optic sensor, such as an infrared detector, the radiation source of the detector is shut off during fluorescence measurements” (Bolea, col. 16, ll. 6-9). 13. Bolea teaches that “in one preferred embodiment, as soon as system 10 or system 14 is powered up, microprocessor 32 cycles through each of the BI presence sensors to determine whether any of wells 14 are populated with BIs” (Bolea, col. 16, ll. 14-17). 14. Bolea teaches a method where “the user must independably [sic] chart the time when each BI was placed in the incubator, track the duration that each BI is incubated, and record the results of the reading step for each BI so as to chart the efficaciousness of each associated sterilization cycle” (Bolea, col. 2, ll. 56-61). 15. Gillis teaches an indicator material which is bromcresol purple (see Gillis, col. 12, l. 24). 16. Gillis teaches that “[m]ultiple early-load-release evaluations of sterilizing effectiveness for both „dry‟ and „wet‟ sterilizer loads, are made available by selective spectroscopic quantitative measurements of peak absorption of electromagnetic radiation” (Gillis, abstract). Principles of Law Claim terms are interpreted using the broadest reasonable interpretation in light of the Specification. See, e.g., In re Hyatt, 211 F.3d 1367, 1372 (Fed. Cir. 2000) (“[D]uring examination proceedings, claims are given their broadest reasonable interpretation consistent with the specification.”). Appeal 2012-002780 Application 11/542,221 9 “The combination of familiar elements according to known methods is likely to be obvious when it does no more than yield predictable results.” KSR Int’l Co. v. Teleflex Inc., 550 U.S. 398, 416 (2007). Analysis Claim interpretation is at the heart of patent examination because before a claim is properly interpreted, its scope cannot be compared to the prior art. In this case, the issue is drawn to the limitation “wherein each B-1 Test-Ampoule in each test-cell is evaluated by a separate source of radiant energy and a photo-detector for said radiant energy” in claim 1, clause (C)(v). Appellant contends that Bolea does not teach “each test-cell is evaluated by a separate source of radiant energy and a photo-detector therefor” (App. Br. 10-11). Appellant contends that “[r]ather, Bolea discloses a carriage for carrying one fluorescence signal and fluorescence sensor for evaluating the multiple B-I holders. This carriage moves to each specific B-I holder” (Reply Br. 3). Clause (C)(v) in claim 1 does not impose any limitations on the source of radiant energy or the type of photo detector. More importantly, clause (C)(v) does not link itself to clause (C)(iii) by using either “said evaluation,” “the evaluation,” or a different signal word indicating that the evaluation in clause (C)(v) has antecedent basis in the “evaluating intended microbial- biocidal results” or “evaluating microbial activity” of clause (C)(iii)(a) or (C)(iii)(b). Appellant also does not identify, and we do not find, a specific teaching in the Specification that limits the evaluation in clause (C)(v) to be related to the evaluation in either clause (C)(iii)(a) or (C)(iii)(b). Appeal 2012-002780 Application 11/542,221 10 Therefore, claim 1 may broadly encompass performance of two different evaluation steps, one step which simply requires “evaluating intended microbial-biocidal results” and another step “wherein each B-I Test-Ampoule in each test-cell is evaluated by a separate source of radiant energy and a photo-detector for said radiant energy.” Bolea teaches two different evaluation steps. As Appellant points out (see App. Br. 9), Bolea teaches one step where a “fluorescence sensor is also mounted on the carriage and is positioned to sense fluorescence exhibited by the BI in the selected BI holder in response to the radiation” (Bolea, col. 3, ll. 27-29; FF 2). However, Bolea also teaches a second evaluation step where “a BI presence sensor 52 is associated with each BI receiving well 14” (Bolea, col. 5, ll. 62-63; FF 11). Bolea teaches that “where the BI presence sensor is an electro-optic sensor, such as an infrared detector, the radiation source of the detector is shut off during fluorescence measurements” (Bolea, col. 16, ll. 6- 9; FF 12). Bolea teaches that “as soon as system 10 or system 14 is powered up, microprocessor 32 cycles through each of the BI presence sensors to determine whether any of wells 14 are populated with BIs” (Bolea, col. 16, ll. 14-17; FF 13). We agree with the Examiner that this second evaluation step reasonably satisfies the requirements of clause (C)(v) in claim 1, since the BI presence sensors, associated with each test location, are evaluated by their own infrared detector and radiation source, which must be extinguished during the first step evaluation using the fluorescence measurements (FF 11- 13). Appeal 2012-002780 Application 11/542,221 11 Appellant also contends that Bolea does not teach or suggest “an apparatus which records the time of establishment of incubation temperature within the B-I Test-Ampoule” (App. Br. 10). We are not persuaded. Bolea teaches that after a “baseline reading is obtained, microprocessor 32 waits for a designated time out. The length of the time out will correspond to the particular BI type being used, and how fast spore growth activity is expected to occur . . . . After the desired time out, another florescence reading is taken from the particular BI 22” (Bolea, col. 8, ll. 14-32; FF 8). Bolea also teaches a prior art method where “the user must independably [sic] chart the time when each BI was placed in the incubator, track the duration that each BI is incubated, and record the results of the reading step for each BI so as to chart the efficaciousness of each associated sterilization cycle” (Bolea, col. 2, ll. 56-61; FF 14). Thus, given the teachings of Bolea, we conclude that either Bolea teaches, or it would have been obvious over Bolea and Gillis, for the baseline reading to occur when the BI was placed into the test cell (FF 8), and to record the time of establishment in the microprocessor so that the microprocessor would know when completion of the time out would occur so as to be able to obtain the next fluorescence reading (FF 8). This is consistent with the operation of known processes in the prior art (FF 14). Conclusion of Law The evidence of record supports the Examiner‟s conclusion that Bolea and Gillis render claim 1 obvious. Appeal 2012-002780 Application 11/542,221 12 B. 35 U.S.C. § 112, written description The Examiner finds that at “issue is the term „separate source‟. It is the Examiner‟s opinion that the disclosure does not reasonably convey that each „Test Ampoule‟ has its own separate source of radiant energy” (Ans. 6). The issue with respect to this rejection is: Does the evidence of record support the Examiner‟s conclusion that the term “separate source” represents new matter? Findings of Fact 17. The Specification teaches that “[f]urther specific objects for significantly-decreasing expected times for B-I evaluations of individual Test-Ampoules are provided by utilizing selected radiant-energy-source means and selected electrometric indicator means, for expediting evaluation of microbial-status within a liquid nutrient-growth medium (NGM) which remains sealed within an individual B-I Test-Ampoule” (Spec. 2-3 ¶ 0008). 18. The Specification teaches that “[m]ore specifically, augmenting the rate of heating can decrease the time for evaluation of biocidal-status. Also, present evaluations can be expedited utilizing transmitted radiant- energy; radiant-energy technology teachings of the invention are described in greater detail later herein” (Spec. 12 ¶ 00038). 19. The Specification teaches that a “microprocessor for each radiant-energy analysis embodiment, is connected to measuring-components within the housing-structure for reporting, signaling and recording purposes; as well as, for radiant-energy analyses” (Spec. 17 ¶ 00049). Appeal 2012-002780 Application 11/542,221 13 20. Figure 4 of the Specification is reproduced below: “FIGURE 4 is an enlarged schematic presentation for describing interacting functional components arranged with respect to an individual-cell with Test-Ampoule in place” (Spec 4 ¶ 00014). 21. The Specification teaches that the “schematic arrangement of FIGURE 4 can be adapted for describing placement of colormetric radiant- energy source and detector means; plus other functioning components, which are interrelated with respect to each other, for decreasing the time required for detecting a treatment-cycle failure, within a B-1 Test-Ampoule, as held within an individual test-receptacle” (Spec. 15 ¶ 00045). 22. The Specification teaches that a “test-cell receptacle for each B- I Test-Ampoule, and its heating means, are located within the housing- structure; and, all measuring equipment is wired for functioning with each respective test-cell receptacle; and, expedited radiant energy analyses, enables decreasing the overall number of test-cells in a housing-structure embodiment” (Spec 17 ¶ 00050). Appeal 2012-002780 Application 11/542,221 14 23. The Specification teaches “FIGURE 4 is an enlarged schematic presentation for describing interacting functional components arranged with respect to an individual-cell with Test-Ampoule in place, for decreasing the time required, in accordance with the invention, for evaluating the microbial-status of such B-1 Test-Ampoule” (Spec. 4 ¶ 00014). Principles of Law “[T]he written description requirement does not demand either examples or an actual reduction to practice; a constructive reduction to practice that in a definite way identifies the claimed invention can satisfy the written description requirement” Ariad Pharmaceuticals, Inc. v. Eli Lilly and Co., 598 F.3d 1336, 1352 (Fed. Cir. 2010). “[I]t is the specification itself that must demonstrate possession. And while the description requirement does not demand any particular form of disclosure, … or that the specification recite the claimed invention in haec verba, a description that merely renders the invention obvious does not satisfy the requirement” Id. (citations omitted). Analysis As we interpreted claim 1, clause (C)(v) above, the claim requires that “each test-cell is evaluated by a separate source of radiant energy and a photo-detector for said radiant energy” (Claim 1). While the Specification discusses the use of radiant energy sources (FF 17-18) as well as measuring components (FF 19), none of the locations cited by Appellant (see App. Br. 8; FF 17-22) provide descriptive support for multiple “separate” sources of radiant energy for each distinct test cell as required by claim 1. “When no such description can be found in the specification, the only thing the PTO Appeal 2012-002780 Application 11/542,221 15 can reasonably be expected to do is to point out its nonexistence.” Hyatt v. Dudas, 492 F.3d 1365, 1370 (Fed. Cir. 2007). Appellant contends that “Figure 4 illustrates one test-cell of the multiple test-cells. In this Figure, there is shown a separate source of radiant energy 28 and a separate photo-detector 30. Accordingly, the specification clearly indicates that each test-cell includes a separate source of radiant energy and a separate photo-detector for detecting said radiant energy” (Reply Br. 2). We are not persuaded. The brief description of Figure 4 states that “FIGURE 4 is an enlarged schematic presentation for describing interacting functional components arranged with respect to an individual-cell with Test- Ampoule in place, for decreasing the time required, in accordance with the invention, for evaluating the microbial-status of such B-1 Test-Ampoule” (Spec. 4 ¶ 00014; FF 23). There is no teaching identified by Appellant that supports the position that Figure 4 illustrates one test cell of a multi-cell unit. Even if we agree with Appellants that Figure 4 illustrates a portion of a multi-cell unit, the figure and accompanying text do not indicate whether each test cell comprises its own radiant energy source and detector. While it may be obvious that each test cell of Figure 4 could include its own radiant energy source and detector, “a description that merely renders the invention obvious does not satisfy the [written description] requirement.” Ariad, 598 F.3d at 1352. Conclusion of Law The evidence of record supports the Examiner‟s conclusion that the term “separate source” represents new matter. Appeal 2012-002780 Application 11/542,221 16 SUMMARY In summary, we affirm the rejection of claim 1 under 35 U.S.C. § 103(a) as obvious over Bolea and Gillis. Pursuant to 37 C.F.R. § 41.37(c)(1)(vii)(2006), we also affirm the rejection of claims 2-9, 17, and 18 as these claims were not argued separately We affirm the rejection of claims 1-9, 17, and 18 under 35 U.S.C. § 112, first paragraph as failing to comply with the written description requirement by incorporating new matter. No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. § 1.136(a)(1)(iv). AFFIRMED lp Copy with citationCopy as parenthetical citation
