REGGIE B. WALTON, United States District Judge
The plaintiff, Veloxis Pharmaceuticals, Inc., filed this civil suit against the defendants — the United States Food and Drug Administration ("FDA"); Margaret Hamburg, the Commissioner of the FDA; the United States Department of Health and Human Services ("DHHS"); and Sylvia Burwell, the Secretary of the DHHS — seeking declaratory and injunctive relief to redress the FDA's decision to delay complete and final approval of Envarsus XR, which is the plaintiff's anti-rejection medication for kidney transplant recipients. Complaint for Declaratory and Injunctive Relief ("Compl.") ¶ 1. Without such approval from the FDA, the plaintiff cannot market Envarsus XR until July 2016. Id. ¶ 7. The plaintiff alleges that the FDA's decision violates the Administrative Procedure Act ("APA"), 5 U.S.C. § 706(2) (2012). Id. ¶¶ 114-28. The plaintiff initially filed a motion for a preliminary injunction, but the parties subsequently agreed to "advance the trial on the merits and consolidate it with the hearing [on the plaintiff's motion for a preliminary injunction]."
The Food, Drug, and Cosmetic Act ("FDCA") governs the pharmaceutical drug approval process for both new and generic drugs. See 21 U.S.C. § 355(a) (2012) ("No person shall introduce or deliver for introduction into interstate commerce any new drug, unless an approval of an application filed pursuant to ... this section is effective with respect to such drug."). The FDCA was later amended by the Drug Price Competition and Patent Term Restoration Act of 1984 ("Hatch-Waxman Amendments"), Pub.L. No. 98-417, 98 Stat. 1585. "The significance of the Hatch-Waxman Amendments to [the FDCA] cannot be understated." Allergan, Inc. v. Crawford, 398 F.Supp.2d 13, 17 (D.D.C.2005). "Prior to 1984, all [sponsors] seeking to market pioneer drugs ... had to file [a new drug application] containing, inter alia, extensive scientific data demonstrating the safety and effectiveness of the drug. As a result, few generic ... drugs were approved by FDA." Id. The Hatch-Waxman Amendments sought to strike a "balance [between] two competing interests in the pharmaceutical industry: (1) inducing pioneering research and development of new drugs and (2) enabling competitors to bring low-cost, generic copies of those drugs to market." Takeda Pharms., U.S.A., Inc. v. Burwell, 78 F.Supp.3d 65, 68, 2015 WL 252806, at *1 (D.D.C.2015) (internal quotation marks omitted). "[The] Hatch-Waxman Amendments created an abbreviated approval process for generic ... drugs, while retaining incentives for [sponsors of] pioneer drugs, such as marketing exclusivity...." Allergan, 398 F.Supp.2d at 17 (citations omitted); see also AstraZeneca Pharms.
The length of a pioneer drug's marketing exclusivity varies. See Allergan, 398 F.Supp.2d at 17 ("Because Congress still wanted to provide incentives for new drug development, alongside the [Abbreviated New Drug Application] process that eased the marketing of generic drugs, [the] Hatch-Waxman [Amendments] entitle[d] [a New Drug Application] applicant to a period of market exclusivity ([three] or [five] years, depending on the degree of innovation reflected in the NDA)."). For example, certain provisions in the Hatch-Waxman Amendments provide three years of marketing exclusivity ("three-year exclusivity"). See 21 U.S.C. § 355(c)(3)(E)(iii), (j)(5)(F)(iii)-(iv) (providing three-year exclusivities).
Under the Hatch-Waxman Amendments, sponsors seeking to market new or generic drugs can obtain FDA approval for their drug products through one of three pathways: (1) a full New Drug Application ("NDA"), see 21 U.S.C. § 355(b)(1)
Takeda Pharms., 78 F.Supp.3d at 71-72, 2015 WL 252806, at *4 (alteration, citations, footnote, and internal quotation marks omitted).
The Food and Drug Administration Modernization Act of 1997 ("FDAMA"), Pub.L. No. 105-115, 111 Stat. 2296, further amended the FDCA. ViroPharma, Inc. v. Hamburg, 898 F.Supp.2d 1, 6 (D.D.C. 2012). Leading up to the passage of the FDMA,
Id. at 6-8 (alteration and citations omitted); see also 21 U.S.C. § 355(v)(1)(A)-(B) (three-year exclusivity to old antibiotics, so long as Section 505(b) NDA submitted after October 8, 2008).
When a kidney is transplanted from a donor to a recipient, the immune system of the recipient will try to reject the kidney. A.R. at FDA 00006. At the time the kidney is transplanted, the recipient is generally referred to as a "de novo patient." Id.
To prevent rejection, the de novo patient must take "drugs that suppress the immune system ... at the time the [kidney] is transplanted...." Id. An immunosuppressive drug regimen usually contains a combination of three or four drugs. Id. at FDA 00007. The recipient must be on the regimen from the time the kidney is transplanted, and continue to be on it as long as the kidney is "viable." Id. at FDA 00006. The "intensive level of immunosuppression administered" to a de novo patient, which lasts "until early after the [transplant] surgery," is called "induction." Id. at FDA 00006-7. After the transplant surgery, "the [recipient]'s regimen of ... immunosuppressants is carefully and frequently monitored ... and may be adjusted to minimize the development of adverse reactions while keeping the [recipient]'s immune system from rejecting the kidney." Id. at FDA 00007. "The goal is to customize the regimen to find the optimum balance between the efficacy and the toxicity of the immunosuppressive regimen." Id. Once the de novo patient achieves the optimum balance, the recipient is referred to as a "maintenance patient." Id. Thereafter, one of the three to four immunosuppressive drugs the patient had been receiving can be discontinued and replaced with another drug. Id. at FDA 00008. This replacement process is called "conversion." Id.
Tacrolimus is an immunosuppressant approved for use in preventing organ rejection. Id. at FDA 00009. Astellas Pharma US, Inc. ("Astellas") submitted, and the FDA approved, a Section 505(b)(1) NDA for a tacrolimus formulation in 1994, under the trade name Prograf ("Prograf NDA"). Id. Prograf is a twice-daily, immediate release capsule that is used for the "prophylaxis of organ rejection in patients receiving," among other organ transplants, "kidney ... transplants." Id.
Tacrolimus is also considered an antibiotic drug by statute. See id. (citing 21 U.S.C. § 321(jj)). And because it was the subject of a NDA before the FDAMA was enacted in 1997, it is considered an "old antibiotic." Id. at FDA 00010; see also Allergan, 398 F.Supp.2d at 18 (explaining old antibiotics).
In 2005, Astellas submitted a Section 505(b)(1) NDA for a different tacrolimus formulation under the trade name Astagraf XL ("Astagraf XL NDA"). A.R. at FDA 00010. For this formulation, it sought approval for a once-daily, extended release capsule for the "prophylaxis of organ rejection following," again among other organ transplantations, a "kidney transplantation." Id. at FDA 00010. In 2009, Astellas withdrew the Astagraf XL NDA after the FDA identified some deficiencies in the NDA. See id. at FDA 00011-12; id. at FDA 00874. Astellas submitted a new
The plaintiff submitted a Section 505(b)(2) NDA for a tacrolimus formulation, under the trade name Envarsus XR in December 2013 ("Envarsus XR NDA"). Id. at FDA 00016. Envarsus XR is a once daily, extended-release tablet, used for the "prophylaxis of organ rejection in both de novo and conversion kidney transplant patients." Id. at FDA 00018. The Envarsus XR NDA relies on its own independent clinical studies, as well as clinical studies relied upon for the approval of the Prograf NDA. Id. at FDA 00016. The FDA tentatively approved Envarsus XR in October 2014. Id. at FDA 00018. That same month, however, the FDA determined that Astagraf XL's three-year exclusivity prevented the FDA from fully approving Envarsus XR in all respects. Id. at FDA 00019. Specifically,
Id. Because the FDA withheld final approval of Envarsus XR for the prophylaxis of organ rejection in de novo kidney transplant patients, the plaintiff cannot market Envarsus XR for this use. See id.
In November 2014, the plaintiff met with the FDA and expressed its belief that the FDA had erred for several reasons in delaying complete and final approval of Envarsus XR on the basis of Astagraf XL's three-year exclusivity. Id. at FDA 00019-20; see also id. at FDA 0158890, 1592-1622, 1623-25, 1626-43. Thereafter, in December 2014, the plaintiff provided additional arguments to the FDA as to why its delay of complete and final approval was erroroneous. Id. at FDA 01739-42. Upon review of the plaintiff's submissions to the FDA, the FDA proposed a compromise: "it could [fully] approve Envarsus
In cases involving review of final administrative actions, the summary judgment standard of review set forth in Federal Rule of Civil Procedure 56 does not apply.
"The scope of review under the `arbitrary and capricious' standard is narrow and a court is not to substitute its judgment for that of the agency." Motor Vehicle Mfrs. Ass'n of U.S., Inc. v. State Farm Mut. Auto. Ins. Co., 463 U.S. 29, 43, 103 S.Ct. 2856, 77 L.Ed.2d 443 (1983). The agency must show that it "examine[d] the relevant data and articulate[d] a satisfactory explanation for its action including a rational connection between the facts found and the choice made." Id. (internal quotation marks omitted). "Under the APA, it is the role of the agency to resolve factual issues to arrive at a decision that is supported by the administrative record, whereas the function of the district court is to determine whether or not as a matter of law the evidence in the administrative record permitted the agency to make the decision it did." Hi-Tech Pharmacal Co. v. FDA, 587 F.Supp.2d 13, 18 (D.D.C.2008) (internal quotation marks and citation omitted). "[T]here is a presumption in favor of the validity of the administrative
All of the plaintiff's arguments are premised on the allegation that the FDA incorrectly interpreted and applied various portions of the FDCA, as amended. See, e.g., Compl. ¶¶ 7-9. The Court must review the FDA's interpretations of the FDCA under the two-step framework outlined in Chevron, U.S.A., Inc. v. Natural Res. Def. Council, Inc., 467 U.S. 837, 104 S.Ct. 2778, 81 L.Ed.2d 694 (1984). This is
Takeda, 2015 WL 252806, at *22 (quoting Chevron, 467 U.S. at 842-43, 104 S.Ct. 2778); see also Pharm. Research & Mfrs. of Am. v. Thompson, 251 F.3d 219, 224 (D.C.Cir.2001) (explaining that under the first step of Chevron, the Court must exhaust the "traditional tools of statutory construction," such as analyses of the "text, structure, purpose, and legislative history" of the statute"). "Chevron deference is frequently given to the FDA's interpretation of the FDCA, as well as its own regulations." Teva Pharms., Indus., 355 F.Supp.2d at 116 (internal quotation marks omitted).
The plaintiff contends that the FDA should not have granted three-year exclusivity to Astagraf XL because the Astagraf XL NDA was submitted and pending before October 2008, and the QI Act conferred three-year exclusivity on an old antibiotic only if the NDA was submitted after October 2008. See Pl.'s Summ. J. Mem. at 40-43. Although the FDA concedes that the Astagraf XL NDA was submitted and pending before October 2008, it nevertheless maintains that Astagraf XL was properly awarded three-year exclusivity because the Astagraf XL NDA was withdrawn in 2009, and then a new Astagraf XL NDA was submitted in 2012. See Defs.' Summ. J. Mem. at 22-23; see also A.R. at FDA 00031-33.
Under the FDCA, as amended by the QI Act, the Court agrees with the
To the extent that Congress did not address the precise conflict presented here, i.e., the FDCA is silent as to the withdrawal and "resubmission" of an old antibiotic NDA that was pending on or before October 2008,
Once an old antibiotic, such as tacrolimus, is eligible for marketing exclusivities, the FDCA entitles those antibiotics to limited marketing exclusivities. In pertinent part, the FDCA states:
21 U.S.C. § 355(c)(3)(E)(iii). According to the plaintiff, this provision does not bar the FDA from granting final approval of Envarsus XR for the prophylaxis of organ rejection in de novo kidney transplant patients because: (1) the Envarsus XR NDA "did not rely upon any of the studies or data supporting approval of Astagraf XL or upon [the] FDA's prior findings that Astagraf XL is safe and effective"; (2) Envarsus XR and Astagraf XL are significantly different drugs; and (3) the plaintiff
The parties' conflicting interpretations of the term "relied upon" in 21 U.S.C. § 355(c)(3)(E)(iii) stand in stark contrast to one another. On the one hand, the plaintiff argues that the term "relied upon" "unambiguously requires" that the three-year exclusivity of a first-in-time 505(b) drug, i.e., the drug that is the subject of a first-in-time 505(b) NDA, can block a second-in-time 505(b)(2) drug from market entry, i.e., the drug that is the subject of a second-in-time 505(b)(2) NDA, only if the second-in-time 505(b)(2) NDA has "relied upon" the first-in-time 505(b) NDA.
The term "relied upon" is not defined in the FDCA. Nevertheless, the statutory provision is clear as to how three-year exclusivity operates and can be unambiguously parsed into essentially two components: entitlement to exclusivity and scope of that exclusivity. See, e.g., Goldstein v. SEC, 451 F.3d 873, 878 (D.C.Cir.2006) ("The lack of a statutory definition of a word does not necessarily render the meaning of a word ambiguous...."). Under the plain language of this provision, entitlement to three-year exclusivity requires: (1) submission of a 505(b) NDA
Once exclusivity is appropriately granted to the drug that is the subject of the first-in-time 505(b) NDA, the FDA
21 U.S.C. § 355(c)(3)(E)(iii) (emphasis added). In other words, the FDA may not approve a second-in-time NDA that shares "conditions of approval" with the first-in-time 505(b) drug. Id. Moreover, the FDA is prohibited only from approving a second-in-time NDA that is a 505(b)(2) NDA, as this provision does not speak to a second-in-time 505(b)(1) NDA. Compare id. § 355(b)(2) ("An application submitted under paragraph (1) for a drug for which the investigations described in clause (A) of such paragraph and relied upon by the applicant for approval of the application were not conducted by or for the applicant and for which the applicant has not obtained a right of reference or use from the person by or for whom the investigations were conducted...." (emphasis added)), with id. § 355(c)(3)(E)(iii) (no approval of second-in-time application where "the investigations described in clause (A) of subsection (b)(1) of this section and relied upon by the applicant for approval of the application were not conducted by or for the applicant and if the applicant has not obtained a right of reference or use from the person by or for whom the investigations were conducted" (emphasis added)); see also Vill. of Barrington, Ill. v. Surface Transp. Bd., 636 F.3d 650, 664 (D.C.Cir. 2011) ("The normal rule of statutory construction is that identical words used in different parts of the same act are intended to have the same meaning." (alterations and internal quotation marks omitted)). Exclusivity under 21 U.S.C. § 355(c)(3)(E)(iii) is triggered by an overlap in the conditions of approval between the first-in-time 505(b) drug and the second-in-time 505(b)(2) NDA and not an overlap between the "new clinical investigations" supporting the first-in-time 505(b) NDA and second-in-time 505(b)(2) NDA. Indeed, it would frustrate Congress's intent to incentivize new drug development through, among other means, marketing exclusivities, if a second-in-time 505(b)(2) NDA could escape the reach of the three-year exclusivity by simply relying on a 505(b) NDA different than the first-in-time 505(b) NDA. That result would reduce the incentive of the sponsor of the first-in-time 505(b) NDA to research and develop new drugs.
The plaintiff goes to great lengths to avoid the plain meaning of 21 U.S.C. § 355(c)(3)(E)(iii). First, the plaintiff
Second, the plaintiff insists that the "importance of reliance" is confirmed by the "FDA's implementing regulation, which provides that a [second-in-time] 505(b)(2) [NDA] will be blocked by three-year exclusivity [only] to the extent that it `relies on the information supporting the conditions of approval of an original new drug application.'" Pl.'s Summ. J. Mem. at 18-19 (quoting 21 C.F.R. § 314.108(b)(4)(iv) (2012)). But the plaintiff has misread the regulation, which in fact supports the FDA's position. The regulation states that:
21 C.F.R. § 314.108(b)(4)(i)-(iv). Thus, the regulation identifies three, second-in-time drug applications, that cannot receive final FDA approval during the exclusivity period of the first-in-time 505(b) drug — one being "a 505(b)(2) [NDA] ... for the conditions of approval of the [first-in-time 505(b) NDA]." Id. § 314.108(b)(4)(iv). The element of "reliance" is relevant only where "an [ANDA is] submitted pursuant to an approved petition under section 505(j)(2)(C) of the [FDCA]...." Id.
Third, the plaintiff implores the Court to examine other provisions of the FDCA because "[h]ad Congress simply intended to describe a 505(b)(2) application [in 21
Fourth, the plaintiff asserts that the FDA's decision to delay complete and final approval of Envarsus XR for the prophylaxis of organ rejection in de novo kidney transplant patients "upends the balance sought to be achieved by Congress" under the Hatch-Waxman Amendments. Pl.'s Summ. J. Mem. at 22. Specifically, the Hatch-Waxman Amendments were enacted to, among other objectives, incentivize pharmaceutical companies and reward them for researching and developing innovative drugs. See id. at 20-23. But here, according to the plaintiff, it is "reap[ing] no reward for its own innovation and investment, while Astagraf XL is inappropriately shielded from competition against an innovative product...." Id. at 23. The Court is not persuaded.
The parties agree that the scope of Astagraf XL's marketing exclusivity is limited to the "conditions of approval" based upon the "new clinical investigations" that were conducted in support of the Astagraf XL NDA. Pl.'s Summ. J. Mem. at 29, 35; Def.'s Summ. J. Mem. at 2425. They also agree that Envarsus XR should be excluded from the marketplace only to the extent that Astagraf XL and Envarsus XR "share `conditions of approval.'" Pl.'s Summ. J. Mem. at 35 (citing 21 U.S.C. § 355(c)(3)(E)(iii)); see also Defs.' Summ. J. Mem. at 24-25. Where they differ is whether the FDA identified the relevant conditions of approval shared between Astagraf XL and Envarsus XR — once-daily, extended release formulation of tacrolimus — despite there being a "myriad [of] differences" between the two drugs. Pl.'s Summ. J. Reply at 19; see also Defs.' Summ. J. Mem. at 27-28; A.R. at FDA 000024-28, 36-37.
Because the parties agree that the term "conditions of approval" is undefined in the FDCA and that no FDA implementing regulation clarifies the meaning of that term, Pl.'s Summ. J. Mem. at 35; Defs.' Reply at 18, the parties essentially concede that the term is ambiguous, and the Court thus proceeds to step two of the Chevron test to assess whether the FDA's interpretation of the FDCA is reasonable and entitled to deference, which the Court concludes it is. The FDCA sets up a "logical
There is no dispute that the new clinical investigations that were essential to the FDA's approval of Astagraf XL and that led to three-year exclusivity for Astagraf XL were Study 158 and Study 12-03. E.g., Pl.'s Summ. J. Mem. at 30; Defs.' Summ. J. Mem. at 30. There is also no dispute that Study 158 examined "Astagraf XL in de novo kidney transplant patients with induction" and Study 12-03 investigated "Astagraf XL in de novo kidney transplant patients without induction." Pl.'s Summ. J. Mem. at 30 (citing A.R. at FDA 00035); see also A.R. at FDA 00034-35 (FDA finding that both studies demonstrated the safety and efficacy of Astagraf XL for the prophylaxis of organ rejection in de novo kidney transplant patients). In light of the results adduced from these new clinical investigations, the FDA concluded that Astagraf XL was entitled to three-year exclusivity for those innovations that distinguished it from Prograf — a once-daily, extended release tacrolimus formulation for prophylaxis of organ rejection in de novo kidney transplant patients. See AstraZeneca Pharms., 872 F.Supp.2d at 80, 83, 85. It follows that because Astagraf XL and Envarsus XR share these conditions of approval, complete and final approval of the Envarsus XR NDA must be delayed until the expiry of Astagraf XL's three-year exclusivity.
The plaintiff has devoted substantial effort to explain why the FDA erroneously identified Study 158 as a "new clinical investigation" pursuant to 21 U.S.C. § 355(c)(3)(E)(iii). E.g., Pl.'s Summ. J. Mem. at 30-33. This argument was neither brought to the FDA's attention prior to this lawsuit nor even alluded to in the plaintiff's complaint.
"Simple fairness to those who are engaged in the tasks of administration, and to litigants, requires as a general rule that courts should not topple over administrative decisions unless the administrative body not only has erred but has erred against objection made at the time appropriate under its practice." United States v. L.A. Tucker Truck Lines, Inc., 344 U.S. 33, 37, 73 S.Ct. 67, 97 L.Ed. 54 (1952). The District of Columbia Circuit has consistently held that courts "are bound to adhere to the `hard and fast rule of administrative law, rooted in simple fairness, that issues not raised before an agency are waived and will not be considered by a court on review.'" Coburn v. McHugh, 679 F.3d 924, 929 (D.C.Cir. 2012) (quoting Nuclear Energy Inst. v. EPA, 373 F.3d 1251, 1297 (D.C.Cir.2004) (per curiam)); see also CSX Transp., Inc. v. Surface Transp. Bd., 584 F.3d 1076,
On November 17, 2014, the FDA sent the plaintiff the "FDA Exclusivity Summary for Astagraf XL." Plaintiff's Motion for Preliminary Injunction ("Prelim.Inj.Mot."), Exhibit ("Ex.") 4 (Declaration of Jennifer L. Bragg ("Bragg.Decl")) ¶ 6; see also A.R. at FDA 0108289. The FDA Exclusivity Summary for Astagraf XL ("Astagraf XL Summary") identified Study 158 as a "new clinical investigation" that was essential to the approval of Astagraf XL and that supported the three-year exclusivity for the drug.
The plaintiff seeks to supplement the administrative record with "the FDA's own Statistical Review and Evaluation from the [Prograf] supplemental New Drug Application" ("Prograf Review and Evaluation") and the "FDA's minutes of a June 17, 1997 meeting between FDA and the sponsor of Duoneb" ("Douneb Meeting Minutes").
Supplementation of the administrative record is only appropriate in exceptional or "unusual" circumstances. City of Dania Beach v. FAA, 628 F.3d 581, 590 (D.C.Cir.2010) ("[W]e do not allow parties to supplement the record `unless they can demonstrate unusual circumstances justifying a departure from this general rule.'" (quoting Tex. Rural Legal Aid v. Legal Servs. Corp., 940 F.2d 685, 698 (D.C.Cir. 1991))); see also Cape Hatteras Access Pres. Alliance v. U.S. Dep't of Interior, 667 F.Supp.2d 111, 112 (D.D.C.2009) ("A court that orders an administrative agency to supplement the record of its decision is a rare bird."). This is because "[t]here is a strong presumption that the agency properly compiled the administrative record." Ivy Sports Med., LLC v. Sebelius, No. 11-cv-1006(RLW), 2012 WL 5248176, at *1 (D.D.C. Oct. 24, 2012). Thus, "[s]upplementation of the administrative record is the exception, not the rule." Id. (internal quotation marks omitted).
To rebut the strong presumption of regularity afforded to the administrative record compiled by the agency, the party seeking supplementation must "put forth concrete evidence that the documents it seeks to `add' to the record were actually before the decisionmakers." Marcum v. Salazar, 751 F.Supp.2d 74, 78 (D.D.C. 2010). Conclusory statements will not suffice; rather, the plaintiff "must identify reasonable, non-speculative grounds for its belief that the documents were considered by the agency and not included in the record." Id. at 78 (quoting Pac. Shores Subdivision Cal. Water Dist. v. U.S. Army Corps of Eng'rs, 448 F.Supp.2d 1, 6 (D.D.C.2006)) (internal quotation marks omitted). "Therefore, absent clear evidence to the contrary, an agency is entitled to a strong presumption of regularity, that it properly designated the administrative record." Ivy Sports Med., 2012 WL 5248176, at *1 (internal quotation marks omitted).
The District of Columbia Circuit has recognized three narrow instances where supplementation of an administrative record may be appropriate: "(1) if the agency `deliberately or negligently excluded documents that may have been adverse to its decision,' (2) if background information
Here, the strong presumption of regularity has not been rebutted by the plaintiff for several reasons. First, the plaintiff relies on conclusory allegations that the FDA negligently or deliberately omitted these documents, as opposed to concrete evidence. See Pl.'s Supplemental Mot. at 5, 7. Second, the documents are not adverse to the FDA's decision to delay final approval of Envarsus XR until the expiry of Astagraf XL's three-year exclusivity. The argument that Study 158 was not a "new clinical evaluation" has been waived by the plaintiff, and thus the Prograf Review and Evaluation is irrelevant. And the Douneb Meeting Minutes are cumulative, as the FDA has already included its substance in the administrative record. Compare Pl.'s Supplemental Mot., Ex. B (June 17, 1997 Meeting Minutes ("Duoneb Meeting Minutes")) at 6 (FDA "expressed... opinion that ... [the Duoneb NDA] could not be approved pending expiration of ... exclusivity for Combivent NDA even if ... [the Duoneb NDA] does not reference the Combivent NDA and even if [the Duoneb NDA] provides data in support of the combination product from the literature...."); with A.R. at FDA 00047-48 (explaining how FDA "concluded that it likely would not be able to fully approve Duoneb's 505(b)(2) NDA ... due to Combivent's existing exclusivity," notwithstanding that the application "did not rely on Combivent"). Finally, any background information that may be useful from these documents has already been compiled in the administrative record by the FDA, and thus supplementation for that purpose is unnecessary. See A.R. at FDA 00047-48 (discussing exclusivity position with respect to Duoneb and Combivent); id. at 01082-89 (demonstrating reliance on Study 158 in approval of Astagraf XL). Accordingly, for all of these reasons, the Court concludes that it has appropriately reviewed the FDA's decision to delay complete and final approval of Envarsus XR, using a properly designated administrative record.
For the foregoing reasons, the Court concludes that the FDA's decision to delay final approval of Envarsus XR for the prophylaxis of organ rejection in de novo kidney transplant patients was neither arbitrary and capricious nor in excess of the FDA's statutory authority.
The plaintiff further argues that "[i]f Astellas had addressed the deficiencies [in its original NDA] without withdrawing and submitting a purportedly `new' NDA, there is no question that it would not be entitled to exclusivity under the QI Act." Pl.'s Reply at 24. That could be true, but that does not mean the FDA's interpretation here is unreasonable. Cf. ViroPharma, 898 F.Supp.2d at 21 ("interpretive line drawing lies at the heart of Chevron deference" (internal quotation marks omitted)). "[I]t was well within the [FDA]'s authority [and discretion] to set the bounds" of the statutory limitation prohibiting three-year exclusivity to an old antibiotic NDA submitted before October 2008. Id. Consistent with the legislative intent behind the QI Act, the FDA has permissibly chosen to interpret 21 U.S.C. § 355(v)(1)(A)-(B) in a narrow manner. In other words, it is within the FDA's authority and discretion to preclude eligibility for three-year exclusivity to only those antibiotics where the NDA was completely submitted and never withdrawn prior to October 8, 2008. See Allergan, 398 F.Supp.2d at 22 ("Policy judgments made by an agency within its area of expertise are also entitled to deference from the courts...." (citing Nat'l Rifle Ass'n v. Reno, 216 F.3d 122, 132 (D.C.Cir.2000))).
