`Petition for Inter Partes Review
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`UNITED STATES PATENT AND TRADEMARK OFFICE
`_____________________
`
`BEFORE THE PATENT TRIAL AND APPEAL BOARD
`_____________________
`
`Fresenius Kabi USA LLC,
`Petitioner
`
`v.
`
`ASTRAZENECA AB,
`Patent Owner
`_____________________
`
`Case IPR2017-01913
`Patent No. 8,329,680
`
`PETITION FOR INTER PARTES REVIEW OF
`U.S. PATENT NO. 8,329,680
`UNDER 35 U.S.C. §§ 311-319 AND 37 C.F.R. § 42.100 ET SEQ.
`
`Mail Stop: Patent Board
`Patent Trial and Appeal Board
`United States Patent and Trademark Office
`P.O. Box 1450
`Alexandria, VA 22313-1450
`
`
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`III.
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`IV.
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`V.
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`IPR2017-01913
`Petition for Inter Partes Review
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`I.
`II.
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`TABLE OF CONTENTS
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`INTRODUCTION ........................................................................................ 1
`NOTICES, STATEMENTS AND PAYMENT OF FEES ........................... 4
`A.
`Real Party In Interest Under 37 C.F.R. § 42.8(b)(1) .......................... 4
`B.
`Related Matters Under 37 C.F.R. § 42.8(b)(2) .................................. 4
`C.
`Lead and Back-Up Counsel Under 37 C.F.R. § 42.8(b)(3) ............... 6
`D.
`Service Information Under 37 C.F.R. § 42.8(b)(4) ............................ 7
`E.
`Grounds for Standing Under 37 C.F.R. § 42.104(a) .......................... 7
`F.
`Fees Under 37 C.F.R. § 42.103 .......................................................... 7
`IDENTIFICATION OF CHALLENGE UNDER 37 C.F.R. §
`42.104(B) ...................................................................................................... 7
`FRESENIUS KABI’S GROUNDS OF UNPATENTABILITY ARE
`DISTINCT FROM THOSE PRESENTED BY MYLAN ............................ 9
`OVERVIEW OF THE ‘680 PATENT AND PROSECUTION
`HISTORY ................................................................................................... 12
`A.
`The ‘680 Patent ................................................................................ 12
`B.
`The Prosecution History of the ‘680 Patent ..................................... 14
`LEVEL OF ORDINARY SKILL IN THE ART ........................................ 17
`VI.
`VII. CLAIM CONSTRUCTION ....................................................................... 18
`A.
`“Achieves”........................................................................................ 18
`B.
`“Therapeutically Significant” ........................................................... 18
`C.
`“Wherein the method achieves a therapeutically significant
`blood plasma fulvestrant concentration of at least 2.5 ngml-1 /
`[8.5 ngml-1] for at least four weeks” ................................................ 19
`VIII. SCOPE AND CONTENT OF THE PRIOR ART...................................... 19
`A.
`The Prior Art Discloses All Limitations of the Challenged
`Claims ............................................................................................... 19
`1.
`Howell Closely Matches the Claimed Invention ................... 19
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`IX.
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`2.
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`3.
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`b.
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`c.
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`2. McLeskey Discloses the Claimed Formulation and Was
`Not a “Treatment Failure” ..................................................... 22
`O’Regan Confirms the Route of Administration ................... 27
`3.
`DeFriend Discloses Dose-Dependent Pharmacokinetics ...... 27
`4.
`B. AstraZeneca’s Attempts to Detract From These Prior Art
`Teachings Fail .................................................................................. 27
`1.
`AstraZeneca’s Purported “Lead Compound” Analysis is
`Inapplicable ............................................................................ 28
`AstraZeneca’s Efficacy Arguments Are Contrary to
`Law ......................................................................................... 30
`AstraZeneca’s Claims of Unpredictability Are Specious ...... 30
`a.
`The Pharmacokinetic Limitations Are Expressly
`Disclosed in the Prior Art ............................................ 31
`It Was Well-Known That Fulvestrant Was
`Administered Intramuscularly ..................................... 33
`The Claimed Combination of Excipients Were
`Neither Unexpected Nor Surprising ............................ 34
`DETAILED EXPLANATION AND SUPPORTING EVIDENCE .......... 36
`A. Ground 1: The Challenged Claims Are Obvious Over Howell ....... 37
`1.
`A POSA Would Have Been Motivated to Develop a
`Formulation to Achieve the Results Reported in Howell ...... 37
`A POSA Would Have A Reasonable Expectation of
`Success in Developing a Formulation to Achieve the
`Howell Results ....................................................................... 39
`Howell Discloses Fulvestrant Concentrations of at Least
`8.5 ng/ml at Day 28 ................................................................ 41
`All Other Limitations Are Disclosed By Howell And
`The Knowledge of a POSA ................................................... 46
`B. Ground 2: The Challenged Claims Are Obvious Over Howell
`and McLeskey .................................................................................. 48
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`2.
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`3.
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`4.
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`IPR2017-01913
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`b.
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`1.
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`2.
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`3.
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`A POSA Would Have Been Motivated to Combine
`Howell and McLeskey ........................................................... 48
`a.
`The Target Fulvestrant Concentration in Howell
`Would Have Led a Skilled Formulator to
`McLeskey .................................................................... 48
`The Record Confirms the Motivation to Combine
`Howell and McLeskey ................................................. 51
`A POSA Would Have A Reasonable Expectation of
`Success in Administering the McLeskey Formulation
`Intramuscularly to Achieve the Results Reported in
`Howell .................................................................................... 55
`Every Limitation Is Disclosed By Howell and
`McLeskey ............................................................................... 60
`C. Ground 3: The Challenged Claims Are Obvious Over Howell,
`McLeskey, and O’Regan .................................................................. 62
`1.
`A POSA Would Have Been Motivated to Combine
`Howell, McLeskey, and O’Regan .......................................... 62
`A POSA Would Have A Reasonable Expectation of
`Success in Combining Howell, McLeskey, and
`O’Regan ................................................................................. 63
`Every Limitation Is Disclosed By Howell, McLeskey,
`and O’Regan .......................................................................... 64
`D. Ground 4: Claims 2 and 6 Are Obvious Over Howell,
`McLeskey, O’Regan, and DeFriend ................................................. 66
`1.
`A POSA Would Have Been Motivated to Combine
`Howell, McLeskey, O’Regan, and DeFriend ........................ 66
`A POSA Would Have A Reasonable Expectation of
`Success in Combining Howell, McLeskey, O’Regan,
`and DeFriend .......................................................................... 68
`Every Limitation Of Claims 2 and 6 Is Disclosed By
`Howell, McLeskey, DeFriend, and O’Regan ........................ 69
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`2.
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`3.
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`2.
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`3.
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`X.
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`XI.
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`SECONDARY CONSIDERATIONS FAIL TO OVERCOME THE
`EVIDENCE OF OBVIOUSNESS ............................................................. 70
`A.
`There Is No Nexus to the Claimed Invention .................................. 70
`B. AstraZeneca’s Secondary Considerations Arguments Fail .............. 71
`1.
`AstraZeneca Cannot Show Long-Felt Need .......................... 71
`2.
`The Results Were Not Unexpected ........................................ 72
`a.
`Dr. Robertson’s Arguments Are Contradicted By
`His Own Work ............................................................. 72
`The Release Profile and Effect of Benzyl
`Benzoate Were Expected ............................................. 73
`CONCLUSION .......................................................................................... 73
`
`b.
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`TABLE OF AUTHORITIES
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`Page(s)
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`FEDERAL CASES
`Alcon Research, Ltd. v. Apotex Inc.,
`687 F.3d 1362 (Fed. Cir. 2012) ............................................................................ 54
`
`Allergan, Inc. v. Apotex Inc.,
`754 F.3d 952 (Fed. Cir. 2014) .............................................................................. 71
`
`Allergan, Inc. v. Sandoz Inc.,
`726 F.3d 1286 (Fed. Cir. 2013) ............................................................................ 33
`
`Alza Corp. v. Mylan Labs., Inc.,
`464 F.3d 1286 (Fed. Cir. 2006) ............................................................................ 30
`
`AstraZeneca LP v. Breath Ltd.,
`603 F. App’x 999 (Fed. Cir. 2015) ...................................................................... 71
`
`AstraZeneca Pharms. LP, et al. v. Agila Specialties, Inc., et al.,
`No. 1:15-cv-06039-RMB-KMW (D.N.J.) ............................................................. 4
`
`AstraZeneca Pharms. LP, et al. v. Glenmark Pharms. Inc., USA,
`No. 1:15-cv-615 (D.N.J.) ....................................................................................... 5
`
`AstraZeneca Pharms. LP, et al. v. InnoPharma Licensing LLC,
`No. 1:16-cv-1962-RMB-KMW (D.N.J.) ............................................................... 5
`
`AstraZeneca Pharms. LP, et al. v. InnoPharma, Inc.,
`No. 1:16-cv-894-RMB-KMW (D.N.J.) ................................................................. 5
`
`AstraZeneca Pharms. LP, et al. v. Mylan Institutional LLC,
`No. 1:16-cv-4612-RMB-KMW (D.N.J.) ............................................................... 5
`
`AstraZeneca Pharms. LP, et al. v. Mylan Pharms. Inc. et al.,
`No. 1:15-cv-7009-RMB-KMW (D.N.J.) ............................................................... 5
`
`AstraZeneca Pharms. LP, et al. v. Sagent Pharms., Inc. et al.,
`No. 1:14-cv-05539-RMB-KMW (D.N.J.) ............................................................. 5
`
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`AstraZeneca Pharms. LP, et al. v. Sandoz Inc.,
`No. 1:14-cv-03547-RMB-KMW (D.N.J.) ............................................................. 5
`
`AstraZeneca Pharms. LP, et al. v. Teva Pharms. USA, Inc. et al.,
`No. 1:15-cv-7889-RMB-KMW (D.N.J.) ............................................................... 5
`
`Aventis Pharma S.A. v. Hospira, Inc.,
`743 F. Supp. 2d 305 (D. Del. 2010), aff’d, 675 F.3d 1324 (Fed. Cir. 2012) ... 35
`
`Cubist Pharms., Inc. v. Hospira, Inc.,
`805 F.3d 1112 (Fed. Cir. 2015) ............................................................................ 59
`
`Duramed Pharms., Inc. v. Watson Labs., Inc.,
`413 F. App’x 289 (Fed. Cir. 2011) ...................................................................... 55
`
`Galderma Labs., L.P. v. Tolmar, Inc.,
`737 F.3d 731 (Fed. Cir. 2013) ................................................................. 29, 32, 67
`
`Hewlett-Packard Co. v. Mustek Sys., Inc.,
`340 F.3d 1314 (Fed. Cir. 2003) ............................................................................ 43
`
`Hoffmann-La Roche Inc. v. Apotex Inc.,
`748 F.3d 1326 (Fed. Cir. 2014) ....................................................................... 4, 30
`
`In re Applied Materials, Inc.,
`692 F.3d 1289 (Fed. Cir. 2012) ............................................................................ 40
`
`In re Ethicon, Inc.,
`844 F.3d 1344 (Fed. Cir. 2017) ..................................................................... 52, 53
`
`In re Huai-Hung Kao,
`639 F.3d 1057 (Fed. Cir. 2011) ............................................................................ 70
`
`In re ICON Health & Fitness,
`496 F.3d 1374 (Fed. Cir. 2007) ............................................................................ 37
`
`Iron Grip Barbell Co. v. USA Sports, Inc.,
`392 F.3d 1317 (Fed. Cir. 2004) ............................................................................ 40
`
`KSR Int’l Co. v. Teleflex Inc.,
`550 U.S. 398 (2007) ............................................................................................. 51
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`Merck & Cie v. Gnosis S.P.A.,
`808 F.3d 829 (Fed. Cir. 2015) .............................................................................. 32
`
`Merck & Co. v. Biocraft Labs., Inc.,
`874 F.2d 804 (Fed. Cir. 1989) .............................................................................. 28
`
`Merck & Co. v. Teva Pharms. USA, Inc.,
`395 F.3d 1364 (Fed. Cir. 2005) ............................................................................ 70
`
`Metso Minerals, Inc. v. Powerscreen Int’l Distrib., Ltd.,
`526 F. App’x 988 (Fed. Cir. 2013) ...................................................................... 32
`
`Pfizer, Inc. v. Apotex, Inc.,
`480 F.3d 1348 (Fed. Cir. 2007) ............................................................... 41, 71, 72
`
`PharmaStem Therapeutics, Inc. v. ViaCell, Inc.,
`491 F.3d 1342 (Fed. Cir. 2007) ............................................................................ 34
`
`Purdue Pharma Prods. L.P. v. Par Pharm., Inc.,
`377 F. App’x 978 (Fed. Cir. 2010) ...................................................................... 28
`
`Randall Mfg. v. Rea,
`733 F.3d 1355 (Fed. Cir. 2013) ............................................................................ 38
`
`Santarus, Inc. v. Par Pharm., Inc.,
`694 F.3d 1344 (Fed. Cir. 2012) ............................................................................ 59
`
`Smith & Nephew, Inc. v. Rea,
`721 F.3d 1371 (Fed. Cir. 2013) ............................................................................ 31
`
`Unigene Laboratories, Inc. v. Apotex, Inc.,
`655 F.3d 1352 (Fed. Cir. 2011) ............................................................................ 29
`
`FEDERAL STATUTES
`
`35 U.S.C. § 102(b) ..................................................................................................... 7
`
`35 U.S.C. § 103 .......................................................................................................... 7
`
`35 U.S.C. § 325(d) ..................................................................................................... 9
`
`35 U.S.C. §§ 311-319 ................................................................................................ 1
`
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`PETITIONER’S EXHIBIT LIST
`
`Exhibit No.
`
`Description
`
`Exhibit 1001 U.S. Patent No. 8,329,680 (“the ‘680 patent”)
`
`Exhibit 1002 Reserved
`
`Exhibit 1003 Reserved
`
`Exhibit 1004 Reserved
`
`Exhibit 1005 Reserved
`
`Exhibit 1006 Copy of Prosecution History for U.S. Patent No. 6,774,122
`(downloaded from PAIR)
`
`Exhibit 1007 Howell et al., Pharmacokinetics, pharmacological and anti-
`tumour effects of the specific anti-oestrogen ICI 182780 in
`women with advanced breast cancer, 74 BRIT. J. CANCER
`300–08 (1996) (“Howell”)
`
`Exhibit 1008 McLeskey et al., Tamoxifen-resistant fibroblast growth factor-
`transfected MCF-7 cells are cross-resistant in vivo to the
`antiestrogen ICI 182,780 and two aromatase inhibitors, 4 CLIN.
`CANCER RESEARCH 697–711 (1998) (“McLeskey”)
`
`Exhibit 1009 O’Regan et al., Effects of the Antiestrogens Tamoxifen,
`Toremifene, and ICI 182,780 on Endometrial Cancer Growth, 90
`J. NAT’L CANCER INST. 1552–1558 (1998) (“O’Regan”)
`
`Exhibit 1010 Order, AstraZeneca Pharms. LP v. Sandoz Inc., No. 14–03547
`(D.N.J. July 29, 2015), ECF No. 102
`
`Exhibit 1011
`
`Institution Decision in Mylan Pharms. Inc. v. AstraZeneca AB,
`Paper No. 11, IPR2016-01325 (P.T.A.B. Dec. 14, 2016)
`
`Exhibit 1012 Declaration of Diane Burgess, Ph.D. and Accompanying
`Exhibits
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`viii
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`Exhibit 1013 Declaration of Richard Bergstrom, Ph.D. and Accompanying
`Exhibits
`
`Exhibit 1014 Declaration of Dorraya El-Ashry, Ph.D. and Accompanying
`Exhibits
`
`Exhibit 1015 Declaration of Adrian Harris, M.B., Ph.D. and Accompanying
`Exhibits
`
`Exhibit 1016 U.S. Patent No. 4,659,516 (“the ‘516 patent”)
`
`Exhibit 1017 AstraZeneca’s Preliminary Response in Mylan Pharms. Inc. v.
`AstraZeneca AB, Paper No. 10, IPR2016-01325 (P.T.A.B. Oct.
`6, 2016)
`
`Exhibit 1018 DeLuca, Formulation of Small Volume Parenterals,
`PHARMACEUTICAL DOSAGE FORMS: PARENTERAL MEDICATIONS
`VOLUME 1 (Avis ed., 2d ed. 1992)
`
`Exhibit 1019 Declaration Under 37 C.F.R. § 1.132 of Ronald J. Sawchuk in
`Application No. 12/285,887
`
`Exhibit 1020 Declaration Under 37 C.F.R. § 1.132 of Paul Richard Gellert in
`Application No. 10/872,784
`
`Exhibit 1021 Faslodex® Label, available at:
`www.accessdata.fda.gov/drugsatfda_docs/label/2012/021344s01
`9s020lbl.pdf
`
`Exhibit 1022 DiPiro, Concepts in Clinical Pharmacokinetics (2010)
`
`Exhibit 1023 Qiu, Developing Solid Oral Dosage Forms: Pharmaceutical
`Theory and Practice (2009)
`
`Exhibit 1024 Tozer, Introduction to Pharmacokinetics and
`Pharmacodynamics: The Quantitative Basis of Drug Therapy
`(2006)
`
`ix
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`Petition for Inter Partes Review
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`Exhibit 1025 Caldwell, An Introduction to Drug Disposition: The Basic
`Principles of Absorption, Distribution, Metabolism, and
`Excretion, 23 Toxicologic Pathology 102 (1995)
`
`Exhibit 1026 Wills, “Basic Pharmacodynamic Concepts and Models,”
`Pharmacodynamics and Drug Development: Perspectives in
`Clinical Pharmacology (1994)
`
`Exhibit 1027 Derendorf, Handbook of Pharmacokinetic/Pharmacodynamic
`Correlation 53 (1995)
`
`Exhibit 1028 Mager, Scaling Pharmacodynamics from In Vitro and
`Preclinical Animal Studies to Humans, DRUG METAB.
`PHARMACOKINET. (2009)
`
`Exhibit 1029 Colburn, Simultaneous Pharmacokinetic/Pharmacodynamic
`Modeling, PHARMACODYNAMICS AND DRUG DEVELOPMENT:
`PERSPECTIVES IN CLINICAL PHARMACOLOGY (1994)
`
`Exhibit 1030 White, Pharmacokinetic and Pharmacodynamic Considerations
`in Antimalarial Dose Optimization, 57 ANTIMICROBIAL AGENTS
`& CHEMOTHERAPY 5802 (2013)
`
`Exhibit 1031 Wakeling et al., A Potent Specific Pure Antiestrogen with
`Clinical Potential, 51 CANCER RESEARCH 3867–3873 (1991)
`(“Wakeling 1991”)
`
`Exhibit 1032 Nicholson, R.I. et al., Responses To Pure Antiestrogens (ICI
`164384, ICI 82780) In Estrogen-Sensitive And –Resistant
`Experimental And Clinical Breast Cancer, ANNALS OF THE NEW
`YORK ACADEMY OF SCIENCES, Vol. 61:148-163 (1995)
`(“Nicholson”)
`
`Exhibit 1033 Riffkin, Castor Oil as a Vehicle for Parenteral Administration of
`Steroid Hormones, 53 J. PHARM. SCI. 891–895 (1964)
`(“Riffkin”)
`
`Exhibit 1034 Finley, New Drug Being Tested in Breast Cancer Study, SAN
`ANTONIO EXPRESS-NEWS, Sept. 20, 1997
`
`x
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`IPR2017-01913
`Petition for Inter Partes Review
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`Exhibit 1035 Uges, Plasma or Serum in Therapeutic Drug Monitoring and
`Clinical Toxicology, 10 PHARMACEUTISCH WEEKBLAD
`SCIENTIFIC EDITION 185–88 (1988) (“Uges”)
`
`Exhibit 1036 Dukes et al., Antiuterotrophic effects of a pure antioestrogen, ICI
`182,780: magnetic resonance imaging of the uterus in
`ovariectomized monkeys, 135 J. ENDOCRINOLOGY 239–247
`(1992) (“Dukes”)
`
`Exhibit 1037 WO 03/006064
`
`Exhibit 1038 DeFriend et al., Investigation of a New Pure Antiestrogen (ICI
`182780) in Women with Primary Breast Cancer, 54 CANCER
`RESEARCH 408–414 (1994) (“DeFriend”)
`
`Exhibit 1039 Osborne et al., Comparison of the Effects of a Pure Steroidal
`Antiestrogen With Those of Tamoxifen in a Model of Human
`Breast Cancer, 87 J. NAT’L CANCER INST. 746–750 (1995)
`(“Osborne 1995”)
`
`Exhibit 1040 Alan E. Wakeling & Jean Bowler, ICI 182,780: A New
`Antioestrogen with Clinical Potential, 43 J. STEROID
`BIOCHEM. MOLEC. BIOL. 173–177 (1992) (“Wakeling
`1992”)
`
`Exhibit 1041 Howell, A. et al., Clinical Studies With The Specific ‘Pure’
`Antiestrogen ICI 182780, THE BREAST, Vol. 5:192-195 (1996)
`(“Howell Breast 1996”)
`
`Exhibit 1042 Copy of Prosecution History for U.S. Patent No. 8,329,680
`(downloaded from PAIR)
`
`Exhibit 1043 Robertson, J.F.R. et al., Duration Of Remission To ICI 182,780
`Compared To Megestrol Acetate In Tamoxifen Resistant Breast
`Cancer, THE BREAST, Vol. 6:186-189 (1997) (“Robertson
`1997”)
`
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`Exhibit 1044 Robertson, Fulvestrant Versus Anastrozole for the Treatment of
`Advanced Breast Carcinoma in Postmenopausal Women: A
`Prospective Combined Analysis of Two Multicenter Trials, 98
`CANCER 229-38 (2003) (“Robertson 2003”)
`
`Exhibit 1045 Howell, Response to a Specific Antioestrogen (ICI 182780) in
`Tamoxifen-Resistant Breast Cancer, 345 LANCET 989-90 (1995)
`(“Howell 1995”)
`
`Exhibit 1046 Copy of Prosecution History for the U.S. Patent No. 7,456,160
`(downloaded from PAIR)
`
`Exhibit 1047 U.S. Patent No. 5,183,814 (“Dukes ‘814”)
`
`Exhibit 1048 Parczyk, K. et al., Progesterone Receptor Repression by
`Estrogens in Rat Uterine Epithelial Cells, 63 J. STEROID
`BIOCHEMISTRY & MOLECULAR BIOLOGY 309 (1997)
`
`Exhibit 1049 Anderson, Models of New Antioestrogen Action in Vivo: Primary
`Tumours, 5 THE BREAST 186-91 (1996)
`
`Exhibit 1050 Buzdar, Update on Endocrine Therapy for Breast Cancer, 4
`CLINICAL CANCER RESEARCH 527-34 (1998)
`
`Exhibit 1051 Howell, New Endocrine Therapies for Breast Cancer, 32A EUR.
`J. CANCER 576-88 (1996)
`
`Exhibit 1052 Howell, The Definition of the ‘No Change’ Category in Patients
`Treated with Endocrine Therapy and Chemotherapy for
`Advanced Carcinoma of the Breast, 24 EUR. J. CANCER CLIN.
`ONCOL. 1567-72 (1988)
`
`Exhibit 1053 Nicholson, “Pure Antioestrogens in Breast Cancer: Experimental
`and Clinical Observations,” Sex Hormones and Antihormones in
`Endocrine Dependent Pathology: Basic and Clinical Aspects,
`Proceedings of an International Symposium, Milano 347-60
`(1994) (“Nicholson”)
`
`Exhibit 1054 Santen, Use of Aromatase Inhibitors in Breast Carcinoma, 6
`ENDOCRINE-RELATED CANCER 75-92 (1999)
`
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`Exhibit 1055 EP 0 346 014
`
`Exhibit 1056 Howell, Response to a Specific Antioestrogen (ICI 182780) in
`Tamoxifen-Resistant Breast Cancer, 345 LANCET 29-30 (1995)
`
`Exhibit 1057 Dukes, Antiuterotrophic Effects of the Pure Antioestrogen ICI
`182,780 in Adult Female Monkeys (Macaca nemestrina):
`Quantitative Magnetic Resonance Imaging, 138 J.
`ENDOCRINOLOGY 203-09 (1993)
`
`Exhibit 1058 Wakeling, The Future of New Pure Antioestrogens in Clinical
`Breast Cancer, 25 BREAST CANCER RESEARCH & TREATMENT 1-
`9 (1993) (“Wakeling”)
`
`Exhibit 1059 Selective Estrogen Receptor Modulators (SERMs),
`BREASTCANCER.ORG (last modified Nov. 5, 2015),
`http://www.breastcancer.org/treatment/hormonal/serms
`
`Exhibit 1060 Howell, Fulvestrant Revisited: Efficacy and Safety of the 500-mg
`Dose, 11 CLINICAL BREAST CANCER 204-10 (2011)
`
`Exhibit 1061 Thomas, The Effects of ICI 182,780, a Pure Anti-Oestrogen, on
`the Hypothalamic—Pituitary—Gonadal Axis and on Endometrial
`Proliferation in Pre-Menopausal Women, 9 HUMAN
`REPRODUCTION 1991-96 (1994)
`
`Exhibit 1062 Freireich, Quantitative Comparison of Toxicity of Anticancer
`Agents in Mouse, Rat, Hamster, Dog, Monkey, and Man, 50
`CANCER CHEMOTHERAPY REPORTS 219-44 (1966)
`
`Exhibit 1063 Equivalent Surface Area Dosage Conversion Factors (2007)
`
`Exhibit 1064 Clarke, Antiestrogen Resistance in Breast Cancer and the Role
`of Estrogen Receptor Signaling, 22 ONCOGENE 7316-39 (2003)
`
`Exhibit 1065 Gusterson, Do we now have a relevant animal model for breast
`cancer? 1 BREAST CANCER RESEARCH 2-4 (1999)
`
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`Exhibit 1066 Johnston, Changes in Estrogen Receptor, Progesterone
`Receptor, and pS2 Expression in Tamoxifen-Resistant Human
`Breast Cancer, 55 CANCER RESEARCH 3331-38 (1995)
`
`Exhibit 1067 Waynforth, LASA Good Practice Guidelines: Administration of
`Substances (Rat, Mouse, Guinea Pig, Rabbit) (Oct. 1998),
`www.procedureswithcare.org.uk/lasa_administration.pdf
`
`Exhibit 1068 Mackey, Tolerability of Intramuscular Injections of Testosterone
`Ester in Oil Vehicle, 10 HUMAN REPRODUCTION 862-65 (1995)
`
`Exhibit 1069 Kern, “Role of Angiogenesis in the Transition to Hormone
`Independence and Acquisition of the Metastatic Phenotype,”
`Endocrinology of Breast Cancer 169-86 (Manni ed., 1999)
`
`Exhibit 1070 Neubauer, Changes in Tumour Biological Markers during
`Primary Systemic Chemotherapy (PST), 28 ANTICANCER
`RESEARCH 1797-804 (2008)
`
`Exhibit 1071 Smith, Analysis of Oil-Based Pharmaceuticals, 49 J. AMERICAN
`OIL CHEMISTS’ SOCIETY 409-13 (1972)
`
`Exhibit 1072 Spiegel & Noseworthy, Use of Nonaqueous Solvents in
`Parenteral Products, 52 J. PHARM. SCIS. 917-27 (1963)
`(“Spiegel”)
`
`Exhibit 1073 Taucher, Sequential Steroid Hormone Receptor Measurements in
`Primary Breast Cancer with or without Intervening Primary
`Chemotherapy, 10 ENDOCRINE-RELATED CANCER 91-98 (2003)
`
`Exhibit 1074 Turner, Administration of Substances to Laboratory Animals:
`Routes of Administration and Factors to Consider, 50 J.
`AMERICAN ASSOCIATION FOR LABORATORY ANIMAL SCIENCE
`600-13 (2011)
`
`xiv
`
`
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`IPR2017-01913
`Petition for Inter Partes Review
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`
`
`Exhibit 1075 Robertson, J.F.R. et al., A Partially-Blind, Randomised,
`Multicentre Study Comparing the Anti-Tumor Effects of Single
`Doses (50, 125 and 250 mg) Of Long-Acting (LA) ‘Faslodex’
`(ICI 182,780) With Tamoxifen In Postmenopausal Women With
`Primary Breast Cancer Prior To Surgery, in 22ND ANNUAL SAN
`ANTONIO BREAST CANCER SYMPOSIUM, Abstract No. 28 (Dec. 8-
`11, 1999) (“Robertson 1999”)
`
`Exhibit 1076 Kohler, Plasma and Tissue Concentrations Following
`Intramuscular Administration of Etofenamat. Pharmacokinetics
`of Etofenamat and Flufenamic Acid in Plasma, Synovium, and
`Tissues of Patients with Chronic Polyarthritis after
`Administration of an Oily Solution of Etofenamat, 42
`ARZNEIMITTEL-FORSCHUNG (English Abstract) (1992)
`(“Kohler”)
`
`Exhibit 1077 Jorgensen, Pharmacokinetic Studies in Volunteers of Intravenous
`and Oral Cis (Z)-Flupentixol and Intramuscular Cis (Z)-
`Flupentixol Decanoate in Viscoleo®, 18 EUR. J. CLIN.
`PHARMACOL. 355-60 (1980) (“Jorgensen”)
`
`Exhibit 1078 Petition for Inter Partes Review in Mylan Pharms. Inc. v.
`AstraZeneca AB, Paper No. 2, IPR2016-01325 (P.T.A.B. June
`29, 2016)
`
`Exhibit 1079 Handbook of Pharmaceutical Excipients (Wade ed., 2d. ed.
`1994)
`
`Exhibit 1080 FDA’s Inactive Ingredient Database (1996) (“IIG”)
`
`Exhibit 1081 Drugs@FDA Glossary of Terms, U.S. FOOD & DRUG
`ADMINISTRATION (last updated Feb. 2, 2012),
`http://www.fda.gov/Drugs/InformationOnDrugs/ucm079436.htm
`
`Exhibit 1082 Adam, “Pharmacokinetics of Agents in Relation to Response,”
`Endocrine Management of Cancer: Biological Bases 112-24
`(1988)
`
`xv
`
`
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`IPR2017-01913
`Petition for Inter Partes Review
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`
`Exhibit 1083 Baselga, Phase II Study of Weekly Intravenous Recombinant
`Humanized Anti-p185HER2 Monoclonal Antibody in Patients with
`HER2/neu-Overexpressing Metastatic Breast Cancer, 14 J.
`CLINICAL ONCOLOGY 737-44
`
`Exhibit 1084 Fabian, Clinical Pharmacology of Tamoxifen in Patients with
`Breast Cancer: Correlation with Clinical Data, 48 CANCER 876-
`82 (1981)
`
`Exhibit 1085 Goldenberg, Trastuzumab, a Recombinant DNA-Derived
`Humanized Monoclonal Antibody, a Novel Agent for the
`Treatment of Metastatic Breast Cancer, 21 CLINICAL
`THERAPEUTICS 309-18 (1999)
`
`Exhibit 1086 Wilkinson, Tamoxifen (Nolvadex*) Therapy – Rationale for
`Loading Dose Followed by Maintenance Dose for Patients with
`Metastatic Breast Cancer, 10 CANCER CHEMOTHERAPY
`PHARMACOLOGY 33-35 (1982)
`
`Exhibit 1087 Copy of Prosecution History for the U.S. Patent No. 8,466,139
`(downloaded from PAIR)
`
`Exhibit 1088 Wunsche, Estrogenic Regulation of Clusterin mRNA in Normal
`and Malignant Endometrial Tissue, 76 INT. J. CANCER 684-88
`(1998) (“Wunsche”)
`
`Exhibit 1089 Chwalisz, Modulation of Oestrogenic Effects by Progesterone
`Antagonists in the Rat Uterus, 4 HUMAN REPRODUCTION UPDATE
`570-83 (1998) (“Chwalisz”)
`
`Exhibit 1090 Robertson, Fulvestrant (Faslodex®)—How to Make a Good Drug
`Better, 12 ONCOLOGIST 774-84 (2007)
`
`Exhibit 1091 Ansel, “Dosage Form Design: Biopharmaceutic and
`Pharmacokinetic Considerations,” Pharmaceutical Dosage
`Forms and Drug Delivery Systems 101-41 (7th ed. 1999)
`
`Exhibit 1092 Lee, Standard Deviation and Standard Error of the Mean, 68
`KOREAN J. ANESTHESIOLOGY 220-23 (2015)
`
`xvi
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`IPR2017-01913
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`Exhibit 1093 Altman, Standard Deviations and Standard Errors, 331 BMJ
`903 (2005)
`
`Exhibit 1094 Tse, Bioavailability of Parenteral Drugs I. Intravenous and
`Intramuscular Doses, 34 J. PARENTERAL DRUG ASSOCIATION
`409-21 (1980)
`
`Exhibit 1095 Licciardi, Oral Versus Intramuscular Progesterone for In Vitro
`Fertilization: A Prospective Randomized Study, 71 FERTILITY &
`STERILITY 614-18 (1999)
`
`Exhibit 1096 August 21, 2008 Applicant Amendment and Response in
`Application No. 10/872,784
`
`Exhibit 1097 Balant-Gorgia, Pharmacokinetic Optimisation of the Treatment
`of Psychosis, 25 CLIN. PHARMACOKINET. 217-36 (1993)
`
`Exhibit 1098 Chien, Solubilization of Steroids by Multiple Co-Solvent Systems,
`23 CHEM. PHARM. BULL. 1085-90 (1975)
`
`Exhibit 1099 Ford, “Parenteral Products,” Pharmaceutics: The Science of
`Dosage Form Design 359-80 (Aulton ed., 1988)
`
`Exhibit 1100 Cunliffe-Beamer, “Biomethodology and Surgical Techniques,”
`The Mouse in Biomedical Research, Volume III: Normative
`Biology, Immunology, and Husbandry 401-37 (Foster ed., 1983)
`
`Exhibit 1101 Way, “Cosolvent Use in Injectable Formulations,” Injectable
`Drug Development: Techniques to Reduce Pain and Irritation
`215-66 (Gupta ed., 1999)
`
`Exhibit 1102 Nema, Excipients and Their Use in Injectable Products, 51 PDA
`J. PHARM. SCI. & TECH. 166-71 (1997)
`
`Exhibit 1103 Ogasawara, Effects of Experimental Chemoendocrine Therapy
`with a Combination of a Pure Antiestrogen and 5-Fluorouracil
`on Human Breast Cancer Cells Implanted in Nude Mice, 29
`SURGERY TODAY 149-56 (1999)
`
`xvii
`
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`IPR2017-01913
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`
`Exhibit 1104 Oldham, “Mass Transport to Electrodes,” Chemical Kinetics 79-
`143 (Bamford ed., 1986)
`
`Exhibit 1105 Powell, Compendium of Excipients for Parenteral Formulations,
`52 PDA J. PHARM. SCI. & TECH. 238-311 (1998)
`
`Exhibit 1106 Remington’s Pharmaceutical Sciences 1538-39, 1545-50, 1686-
`88 (18th ed. 1990)
`
`Exhibit 1107 Roberts, Investigation of Cosolvent Effects on the Solvation of
`AOT Reverse Micelles in Supercritical Ethane, 102 J. PHYS.
`CHEM. B 9074-80 (1998)
`
`Exhibit 1108 Sawka, Physiological Consequences of Hypohydration: Exercise
`Performance and Thermoregulation, 24 MEDICINE & SCIENCE IN
`SPORTS & EXERCISE 657-70 (1992)
`
`Exhibit 1109 Simmons, The Laboratory Mouse: Selection and Management
`127-28 (1970)
`
`Exhibit 1110 Ting, Solubility of Naproxen in Supercritical Carbon Dioxide
`with and without Cosolvents, 32 IND. ENG. CHEM. RES. 1471-81
`(1993)
`
`Exhibit 1111 Tse, Bioavailability of Parenteral Drugs II. Parenteral Doses
`Other Than Intravenous and Intramuscular Routes, 34 J.
`PARENTERAL DRUG ASSOCIATION 484-95 (1980)
`
`Exhibit 1112 U.S. Patent No. 4,212,863
`
`Exhibit 1113 USP 23 – NF 18, The United States Pharmacopeia – The
`National Formulary 13-14 (1995)
`
`
`
`
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`TABLE OF ABBREVIATIONS
`
`7α-[9-(4,4,5,5,5-pentafluoropentylsulphinyl)nonyl]oestra-1,3,5(10)-
` triene-3,17β-diol .................................................................................. Fulvestrant
`
`Estrogen receptor .................................................................................................... ER
`
`Estrogen receptor-positive ........................................................... ER+ or ER-positive
`
`Estrogen-receptor downregulators ..................................................................... ERDs
`
`Hormone-dependent ............................................................................................... HD
`
`ICI 182,780 ................................................................................................ Fulvestrant
`
`Intramuscular .......................................................................................................... IM
`
`Percent volume in volume .................................................................................. %v/v
`
`Percent weight in volume ................................................................................... %w/v
`
`Person of ordinary skill in the art ...................................................................... POSA
`
`Selective estrogen-receptor modulators .......................................................... SERMs
`
`Subcutaneous ........................................................................................