The Federal Food, Drug, and Cosmetic Act of 1938, as amended in
1962, establishes a system of pre-marketing clearance for drugs and
prohibits in § 505(a) the introduction into commerce of any
"new drug" unless a new drug application (NDA) filed with the Food
and Drug Administration (FDA) was
effective with respect
to such drug. Under the Act, procedures were established for filing
"new drug" applications not only for the
safety of drugs
but for their
efficacy as well. Standards were provided
under which, after notice and hearing, FDA could refuse to allow an
NDA to become effective, or could suspend an NDA in effect on the
basis of new evidence that the drug was not effective. FDA is
directed to refuse approval of an NDA and to withdraw prior
approval if "substantial evidence" (§ 505(d)) that the drug is
effective for its intended use is lacking. All NDA's "effective"
prior to 1962 were deemed "approved," and manufacturers were given
two years to develop substantial evidence of effectiveness during
which previously approved NDA's could not be withdrawn by FDA for
the drug's lack of effectiveness. The 1962 Act also contained a
"grandfather" clause exempting from the effectiveness requirements
any drug which, on the day preceding enactment, (1) was
commercially used or sold in the United States, (2) was not a "new
drug" as defined in the 1938 Act, and (3) "was not covered by an
effective application" for a new drug under the 1938 Act. FDA had
permitted more than 9,000 NDA's to become effective between 1938
and 1962, of which some 4,000 were still on the market.
Additionally, manufacturers have marketed thousands of "me-too"
drugs without applying for clearance, drugs similar or identical to
drugs with effective NDA's, marketed in reliance on
Page 412 U. S. 610
the "pioneer" drug application approved by FDA. To aid it in
fulfilling the statutory mandate to review all marketed drugs,
whether or not previously approved, for their efficacy, FDA
retained the National Academy of Sciences-National Research Council
(NAS-NRC) to create expert panels to review by class the efficacy
of each approved drug. Holders of NDA's were invited to furnish the
panels with the best available data to establish efficacy and FDA
announced that it would apply NASNRC efficacy findings to all
drugs, including the "me-too" drugs. Respondent in No. 72-394
(Hynson) had filed an application for a drug called Lutrexin under
the 1938 Act. FDA informed Hynson that the studies submitted with
the application were not sufficiently well controlled to justify
the claims of effectiveness, but allowed the application to become
effective, since the 1938 Act permitted evaluation of a new drug
solely on the basis of its safety. When the 1962 amendments became
effective, Hynson submitted evidence of the efficacy of the drug,
but the NAS-NRC panel reported that Hynson had not satisfied the
requirements. Notice of an intention to withdraw approval of the
NDA's covering the drug was given by the Commissioner of Food and
Drugs. Before the hearing, Hynson brought suit in the District
Court for a declaratory judgment that the drug was exempt from the
efficacy review provisions of the 1962 Act, or that there
was no lack of substantial evidence of the drug's efficacy.
Petitioners' motion to dismiss was granted. While the District
Court litigation was pending, the Commissioner denied Hynson's
request for a hearing based on claims of "substantial evidence" of
Lutrexin's effectiveness, and withdrew the NDA for the drug, ruling
that it was not exempt from the 1962 amendments and that Hynson had
not submitted adequate evidence that the drug was not a new drug or
was effective. The Court of Appeals reversed, holding that, while
the drug was not exempt, Hynson was entitled to a hearing on the
substantial evidence issue. No. 72-414 is a cross-petition by
Hynson from the judgment of the Court of Appeals, which suggested
that only a district court has authority to determine whether
Lutrexin is a "new drug." While Hynson agrees that the Commissioner
has authority to determine new drug status in proceedings to
withdraw approval of the product's NDA, some manufacturers, parties
to other suits in this group of cases, advance the contrary
view.
Held:
1. The 1962 amendments and the regulations issued thereunder,
which express well established principles of scientific
investigation,
Page 412 U. S. 611
in their reduction of the "substantial evidence" standard to
detailed guidelines for the protection of the public, make FDA's
so-called administrative summary judgment procedure appropriate.
Pp.
412 U. S.
617-619.
2. FDA's procedure, whereby it will not provide a formal hearing
when it is apparent at the threshold that the applicant has not
tendered
any evidence which,
on its face, meets
the statutory standards as particularized by the regulations, is
valid.
United States v. Storer Broadcasting Co.,
351 U. S. 192;
FPC v. Texaco, 377 U. S. 33. Pp.
412 U. S.
620-622.
3. In No. 72-394, the Court of Appeals' holding that Hynson was
entitled to a hearing on whether its submission of evidence
satisfied its threshold burden of providing "substantial evidence"
is affirmed. Pp.
412 U. S.
622-623.
4. The heart of the statutory procedure is the grant of primary
jurisdiction to FDA, subject to judicial review when administrative
remedies are exhausted. Pp.
412 U. S.
623-627.
5. Although a drug can be "generally recognized" by experts as
effective for intended use within the meaning of the Act only when
that expert consensus is founded upon "substantial evidence," any
ruling on Lutrexin's "new drug" status is premature, and must await
the outcome of the hearing on whether Hynson submitted "substantial
evidence," as held in No. 72-394 (item 3,
supra). Pp.
412 U. S.
628-632.
6. Lutrexin is not exempt under the "grandfather" provisions of
the 1962 Act, as held by FDA and the Court of Appeals, and their
construction accords with the legislative history, which suggests
that the exemption is afforded only for drugs that never had been
subject to new drug regulation. Pp.
412 U. S.
632-634.
461 F.2d 215, affirmed as modified.
DOUGLAS, J., delivered the opinion of the Court, in which
BURGER, C. .J., and WHITE, MARSHALL, BLACKMUN, and REHNQUIST, JJ.,
joined. POWELL, J., filed an opinion concurring in the result as to
Part I and joining in Part II of the Court's opinion,
post, p.
412 U. S. 637.
BRENNAN, J., took no part in the consideration or decision of the
cases. STEWART, J., took no part in the decision of the cases.
Page 412 U. S. 612
MR. JUSTICE DOUGLAS delivered the opinion of the Court.
These cases, together with
Weinberger v. Bentex
Pharmaceuticals, Inc., post, p.
412 U. S. 645,
CIBA Corp. v. Weinberger, post, p.
412 U. S. 640, and
USV Pharmaceutical Corp. v. Weinberger, post, p.
412 U. S. 655, all
here on certiorari, raise a series of questions under the 1962
amendments [
Footnote 1] to the
Federal Food, Drug, and Cosmetic Act of 1938. 52 Stat. 1040. The
1938 Act, which established a system of pre-marketing clearance for
drugs, prohibited the introduction into commerce of any "new drug"
unless a new drug application (NDA) filed with the Food and Drug
Administration (FDA) [
Footnote
2] was effective with respect to that drug. § 505(a), 52
Stat. 1052. Under the 1938 Act, a "new drug"
Page 412 U. S. 613
was one not generally recognized by qualified experts as safe
for its intended use. § 201(p)(1). The Government could sue to
enjoin violations, prosecute criminally, and seize and condemn the
articles. §§ 301(d), 302(a), 303, 304. The Act
established procedures for filing NDA's, § 505(b), and
provided standards under which, after notice and hearing, FDA could
refuse to allow an NDA to become effective, §§ 505(c) and
(d), or could suspend an NDA in effect on the basis of new evidence
that the drug was unsafe. § 505(e). Orders denying or
suspending an NDA could be reviewed in a district court on the
administrative record. § 505(h).
The 1962 Act amended § 201(p)(1) of the 1938 Act to define
a "new drug" as a drug not generally recognized among experts as
effective, as well as safe, for its intended use. 21
U.S.C. § 321(p)(1). A new drug, as now defined, still may not
be marketed unless an NDA is in effect. FDA is now directed to
refuse approval of an NDA and to withdraw any prior approval if
"substantial evidence" [
Footnote
3] that the drug is effective for its intended use is lacking.
21 U.S.C. §§ 355(d) and (e). Thus, the basic clearance
system, requiring FDA approval of an NDA before a "new drug" may be
lawfully marketed, was continued, except that FDA now either must
approve or disapprove an application within 180 days. 21 U.S.C.
§ 355(c). (Under the 1938 Act an application automatically
became effective if it was not disapproved.) Judicial review was
transferred to the courts of appeals. 21 U.S.C. § 355(h).
Page 412 U. S. 614
Since the Act, as amended, requires affirmative agency approval,
all NDA's "effective" prior to 1962 were deemed "approved" under
the new definition, and manufacturers were given two years to
develop substantial evidence of effectiveness, during which
previously approved NDA's could not be withdrawn by FDA for a
drug's lack of effectiveness. [
Footnote 4] The 1962 amendments also contain a
"grandfather" clause exempting from the effectiveness requirements
any drug which, on the day preceding enactment, (1) was
commercially used or sold in the United States, (2) was not a "new
drug" as defined in the 1938 Act (it being generally recognized as
safe), and (3) "was not covered by an effective application" for a
new drug under the 1938 Act. [
Footnote 5]
Between 1938 and 1962, FDA had permitted 9,457 NDA's to become
effective. Of these, some 4,000 were still on the market. In
addition, there were thousands of drugs which manufacturers had
marketed without applying to FDA for clearance. These drugs, known
as "me-toos," are similar to or identical with drugs with effective
NDA's, and are marketed in reliance on the "pioneer" drug
application approved by FDA. In some cases, a manufacturer obtained
an advisory opinion letter from FDA that its product was generally
recognized among experts as safe.
To aid in its task of fulfilling the statutory mandate to review
all marketed drugs for their therapeutic efficacy, whether or not
previously approved, FDA retained the National Academy of
Sciences-National Research Council (NAS-NRC) to create expert
panels to review by class the efficacy of each approved drug.
Holders of NDA's were invited to furnish the panels with
Page 412 U. S. 615
the best available data to establish the effectiveness of their
drugs. [
Footnote 6] The panels
reported to FDA; and on January 23, 1968, FDA announced its policy
of applying the NAS-NRC efficacy findings to all drugs, including
the related "me-too" drugs. [
Footnote 7]
I
Respondent in No. 72-394, Hynson, Westcott & Dunning, Inc.,
had filed an application under the 1938 Act for a drug called
Lutrexin, recommended by Hynson for use in the treatment of
premature labor, threatened and habitual abortion, and
dysmenorrhea. FDA informed Hynson that Hynson's studies submitted
with the application were not sufficiently well controlled to
justify the claims of effectiveness, and urged Hynson not to
represent the drug as useful for threatened and habitual abortion.
But FDA allowed the application to become effective, since the 1938
Act permitted evaluation of a new drug solely on the grounds of its
safety. Before the 1962 amendments, Hynson filed an
application for a related drug which FDA, again on the basis of the
test of safety, allowed to become effective. When the 1962
amendments became effective and NAS-NRC undertook to appraise the
efficacy of drugs theretofore approved as safe, Hynson submitted a
list of literature references, a copy of an unpublished study, and
a representative sample testimonial letter on behalf of Lutrexin.
The panel of NAS-NRC
Page 412 U. S. 616
working in the relevant field reported to FDA that Hynson's
claims for effectiveness of the drug were either inappropriate or
unwarranted in the absence of submission of further appropriate
documentation. At the invitation of the Commissioner of Food and
Drugs, Hynson submitted additional data. But the Commissioner
concluded that this additional information was inadequate, and
published notice of his intention to withdraw approval of the NDA's
covering the drug, offering Hynson the opportunity for a
pre-withdrawal hearing. Before the hearing could take place, Hynson
brought suit in the District Court for a declaratory judgment that
the drugs in question were exempt from the
efficacy review
provisions of the 1962 amendments or, alternatively, that there was
no lack of substantial evidence of the drug's
efficacy.
The Government's motion to dismiss was granted, the District Court
ruling that FDA had primary jurisdiction and that Hynson had failed
to exhaust its administrative remedies.
While the District Court litigation was pending, FDA promulgated
new regulations establishing minimal standards for "adequate and
well controlled investigations" and limiting the right to a hearing
to those applicants who could proffer at least some evidence
meeting those standards. [
Footnote
8] Although Hynson maintained that it was not subject to the
new regulations because its initial request for a hearing predated
their issuance, it renewed its request and submitted the material
which it claimed constituted "substantial evidence" of Lutrexin's
effectiveness. The Commissioner denied the request for a hearing
and withdrew the NDA for Lutrexin. He ruled that Lutrexin is not
exempt from the 1962 amendments and that Hynson had not submitted
adequate evidence that Lutrexin is not a new drug or is effective.
The Court
Page 412 U. S. 617
of Appeals reversed, 461 F.2d 215, holding that, while the drug
in question was not exempt, Hynson was entitled to a hearing on the
substantial evidence question.
Section 505(e) [
Footnote 9]
directs FDA to withdraw approval of an NDA if the manufacturer
fails to carry the burden of showing there is "substantial
evidence" [
Footnote 10]
respecting the
efficacy of the drug. As the Court of
Appeals says, "substantial evidence" was substituted for
"preponderance" of the evidence. 461 F.2d at 220. The Act and the
Regulations, in their reduction of that standard to detailed
guidelines, [
Footnote 11]
make FDA's so-called administrative summary judgment procedure
appropriate.
The general contours of "substantial evidence" are defined by
§ 505(d) of the Act to include
"evidence consisting of adequate and well controlled
investigations, including clinical investigations, by experts
qualified by scientific training and experience to evaluate the
effectiveness of the drug involved, on the basis of which it could
fairly and responsibly be concluded by such experts that the drug
will have the effect it purports or is represented to have under
the conditions of use prescribed, recommended, or suggested in the
labeling or proposed labeling thereof."
21 U.S.C. § 355(d). Acting pursuant
Page 412 U. S. 618
to his "authority to promulgate regulations for the efficient
enforcement" of the Act, § 701(a), 21 U.S.C. § 371(a),
the Commissioner has detailed the
"principles . . . recognized by the scientific community as the
essentials of adequate and well controlled clinical investigations.
They provide the basis for the determination whether there is
'substantial evidence' to support the claims of effectiveness for
'new drugs.' . . ."
21 CFR § 130.12(a)(5)(ii). They include a "plan or
protocol" setting forth the objective of the study and an adequate
method for selecting appropriate subjects, [
Footnote 12] explaining the methods of
observation and steps taken to minimize bias, providing a
comparison by one of four "recognized" methods of the results of
treatment or diagnosis with a control, and summarizing the methods
of analysis, including any appropriate statistical methods.
Id., § 130.12(a)(5)(ii)(a). No investigation will be
considered "adequate for approval of a new drug" unless the test
drug is "standardized as to identity, strength, quality, purity,
and dosage form to give significance to the results of the
investigation."
Id. § 130.12(a)(5)(ii)(b). Finally,
the regulation provides that
"[u]ncontrolled studies or partially controlled studies are not
acceptable as the sole basis for the approval of claims of
effectiveness. Such studies, carefully conducted and documented,
may provide corroborative support. . . . Isolated case reports,
random experience, and reports lacking the details which permit
scientific evaluation will not be considered."
Id., § 130.12(a)(5)(ii)(c). Lower courts have
upheld the validity of these regulations, [
Footnote 13]
Page 412 U. S. 619
and it is not disputed here that they express well established
principles of scientific investigation. Moreover, their strict and
demanding standards, barring anecdotal evidence indicating that
doctors "believe" in the efficacy of a drug, are amply justified by
the legislative history. The hearings underlying the 1962 Act show
a marked concern that impressions or beliefs of physicians, no
matter how fervently held, are treacherous. [
Footnote 14] Congress in its definition of
"substantial evidence" in § 505(d), wrote the requirement of
"evidence consisting of adequate and well controlled
investigations." The Senate Report makes clear that an abrupt
departure was being taken from old norms for marketing drugs. There
had been mounting concern over
efficacy of drugs as well
as their
safety. [
Footnote 15] The Report stated: [
Footnote 16]
"[A] claim could be rejected if it were found (a) that the
investigations were not 'adequate;' (b) that they were not 'well
controlled;' (c) that they had been conducted by experts not
qualified to evaluate the effectiveness of the drug for which the
application is made; or (d) that the conclusions
Page 412 U. S. 620
drawn by such experts could not fairly and responsibly be
derived from their investigations."
To be sure, the Act requires FDA to give "due notice and
opportunity for hearing to the applicant" before it can withdraw
its approval of an NDA. § 505(e), 21 U.S.C. § 355(e).
FDA, however, by regulation, requires any applicant who desires a
hearing to submit reasons
"why the application . . . should not be withdrawn, together
with a well-organized and full factual analysis of the clinical and
other investigational data he is prepared to prove in support of
his opposition to the notice of opportunity for a hearing. . . .
When it clearly appears from the data in the application and from
the reasons and factual analysis in the request for the hearing
that there is no genuine and substantial issue of fact . . .
e.g., no adequate and well controlled clinical
investigations to support the claims of effectiveness,"
the Commissioner may deny a hearing and enter an order
withdrawing the application based solely on these data. 21 CFR
130.14(b). What the agency has said, then, is that it will not
provide a formal hearing where it is apparent at the threshold that
the applicant has not tendered any evidence which, on its face,
meets the statutory standards as particularized by the
regulations.
The propriety of such a procedure was decided in
United
States v. Storer Broadcasting Co., 351 U.
S. 192,
351 U. S. 205,
and
FPC v. Texaco, 377 U. S. 33,
377 U. S. 39. We
said in
Texaco:
"[T]he statutory requirement for a hearing under § 7 [of
the Natural Gas Act] does not preclude the Commission from
particularizing statutory standards through the rulemaking process
and barring at the threshold those who neither measure up to them
nor show reasons why in the public interest the rule should be
waived."
Ibid.
Page 412 U. S. 621
There can be no question that, to prevail at a hearing, an
applicant must furnish evidence stemming from "adequate and well
controlled investigations." We cannot impute to Congress the design
of requiring, nor does due process demand, a hearing when it
appears conclusively from the applicant's "pleadings" that the
application cannot succeed. [
Footnote 17]
The NAS-NRC panels evaluated approximately 16,500 claims made on
behalf of the 4,000 drugs marketed pursuant to effective NDA's in
1962. Seventy percent of these claims were found not to be
supported by substantial evidence of effectiveness, and only 434
drugs were found effective for all their claimed uses. If FDA were
required automatically to hold a hearing for each product whose
efficacy was questioned by the NAS-NRC study, even though many
hearings would be an exercise in futility, we have no doubt that it
could not fulfill its statutory mandate to remove from the market
all those drugs which do not meet the effectiveness requirements of
the Act.
Page 412 U. S. 622
If this were a case involving trial by jury as provided in the
Seventh Amendment, there would be sharper limitations on the use of
summary judgment, [
Footnote
18] as our decisions reveal.
See, e.g., Adickes v. Kress
& Co., 398 U. S. 144,
398 U. S.
153-161;
White Motor Co. v. United States,
372 U. S. 253. But
Congress surely has great leeway in setting standards for releasing
on the public, drugs which may well be miracles or, on the other
hand, merely easy money-making schemes through use of fraudulent
articles labeled in mysterious scientific dress. The standard of
"well controlled investigations" particularized by the regulations
is a protective measure designed to ferret out those drugs for
which there is no affirmative, reliable evidence of effectiveness.
The drug manufacturers have full and precise notice of the evidence
they must present to sustain their NDA's, and, under these
circumstances, we find FDA hearing regulations unexceptionable on
any statutory or constitutional ground.
Our conclusion that the summary judgment procedure of FDA is
valid does not end the matter, for Hynson argues that its
submission to FDA satisfied its threshold burden. In reviewing an
order of the Commissioner denying a hearing, a court of appeals
must determine whether the Commissioner's findings accurately
reflect the study in question, and, if they do, whether the
deficiencies he finds conclusively render the study inadequate or
uncontrolled in light of the pertinent regulations. [
Footnote 19]
Page 412 U. S. 623
There is a contrariety of opinion within the Court concerning
the adequacy of Hynson's submission. Since a majority are of the
view that the submission as sufficient to warrant a hearing, we
affirm the Court of Appeals on that phase of the case.
II
No. 72-414 is a cross-petition by Hynson from the judgment of
the Court of Appeals. This cross-petition raises questions
concerning the "new drug" provisions of the 1962 amendments. The
Court of Appeals suggested that only a district court has authority
to determine whether Lutrexin is a "new drug." The Government
contends that the Commissioner has authority to determine new drug
status in proceedings to withdraw approval of the product's NDA
under § 505(e). Although Hynson agrees, some of the
manufacturers, parties to other suits in this group of cases,
advance the contrary view.
Prior to 1938, there was no machinery for the pre-marketing
approval of drugs sold in commerce. Under the 1906 Act, 34 Stat.
768, adulterated and misbranded drugs were narrowly defined, and
the Act provided only criminal sanctions and seizure by libel for
condemnation. As previously noted, the 1938 Act provided for
regulatory clearance of drugs prior to marketing and for
administrative suspension of any clearance if required in the
interests of public safety. To introduce a new drug, an application
had to be effective with respect to that drug. The application was
to become effective within a fixed period unless the agency, after
notice and opportunity for hearing, refused to permit it to become
effective, finding that
Page 412 U. S. 624
it could not determine from existing evidence or had not been
shown that it was safe. 52 Stat. 1041-1042, 1052. Any NDA could be
suspended if clinical experience or new testing showed that the
drug was not safe.
Id. at 1053. Orders denying or
suspending an NDA were reviewable on the administrative record in a
district court.
Ibid. Marketing a new drug without an
effective NDA could be enjoined or made the basis of a criminal
prosecution, or the drug could be seized in libel and condemnation
proceedings.
There was a steady stream of NDA's under that Act supported by
voluminous data. [
Footnote
20] Many new drugs claiming "me-too" status were marketed
illegally or were launched with an advisory opinion of FDA that
they were recognized as safe. It is estimated that, by 1969, there
were five identical or similar drugs for every drug with an
effective NDA. Enormous administrative problems were created. Each
NDA contained about 30 volumes, a stack 10 to 12 feet high; and
some contained as many as 400 volumes of data.
It is clear to us that FDA has power to determine whether
particular drugs require an approved NDA in order to be sold to the
public. FDA is indeed the administrative agency selected by
Congress to administer the Act, and it cannot administer the Act
intelligently and rationally unless it has authority to determine
what drugs are "new drugs" under § 201(p) and whether they are
exempt from the efficacy requirements of the 1962 amendments by the
grandfather clause of § 107(c)(4).
Regulatory agencies have by the requirements of particular
statutes usually proceeded on a case-by-case basis, giving each
person subject to regulation separate hearings.
Page 412 U. S. 625
But there is not always a constitutional reason why that must be
done.
United States v. Storer Broadcasting Co.,
351 U. S. 192, is
one example. We there upheld rules of the Federal Communications
Commission limiting the number of broadcasting stations a single
individual might own, saying that that was a proper exercise of the
agency's "rulemaking authority necessary for the orderly conduct of
its business."
Id. at
351 U. S. 202.
The comprehensive, rather than the individual, treatment may indeed
be necessary for quick effective relief.
See Permian Basin Are
Rate Cases, 390 U. S. 747. A
generic drug -- which is found to be unsafe and/or lacking in
efficacy -- may be manufactured by several persons or
manufacturers. To require separate judicial proceedings to be
brought against each, as if each were the owner of a Black Acre
being condemned, would be to create delay where, in the interests
of public health, there should be prompt action. A single
administrative proceeding in which each manufacturer may be heard
is constitutionally permissible measured by the requirements of
procedural due process.
FDA maintains that a withdrawal of any NDA approval covers all
"me-too" drugs. For the reasons stated, that procedure is a
permissible one where every manufacturer of a challenged drug has
an opportunity to be heard. FDA, under § 554 of the
Administrative Procedure Act, may issue a declaratory order
governing all drugs covered by a particular NDA. 5 U.S.C. §
554(e). That section prescribes the procedures an agency must
follow "in every case of adjudication required by statute to be
determined on the record after opportunity for an agency hearing."
§ 554(a). The industry maintains that § 554(e) is of no
avail to FDA because in a withdrawal proceeding a common issue is
whether a drug is a "new drug." That issue, it is argued, can be
resolved only in a court proceeding where there is an
adjudication
Page 412 U. S. 626
"on the record of [a] hearing." But that assumes an
individualized hearing and adjudication as is common in regulatory
proceedings. Section 554(e), however, does not place administrative
proceedings in that straitjacket. It provides that an agency "in
its sound discretion, may issue a declaratory order to terminate a
controversy or remove uncertainty." The termination of a
controversy over a "new drug" may often be of prime importance.
This is an age of ever-expanding dockets at the administrative, as
well as at the judicial, level. If the administrative controls over
drugs are to be efficient, they must be exercised with dispatch.
Only paralysis would result if case-by-case battles in the courts
were the only way to protect the public against unsafe or
ineffective drugs. Moreover, if every "me-too" drug in a particular
generic category had to be put to the test in court actions, great
inequities might well result. It might take months to eliminate one
"me-too" drug manufactured by one company from the market.
Meanwhile, competitors selling drugs in the same category would go
scot-free until the tedious and laborious procedures of litigation
reached them. We cannot believe that Congress engaged in such an
exercise in futility when it enacted the 1962 amendments. That
would, in effect, restore the enforcement provisions to the status
they enjoyed under the rather primitive 1906 Act. We hold that FDA,
by reason of § 554(e) of the Administrative Procedure Act, may
issue a declaratory order to terminate a controversy over a "new
drug" or to remove any uncertainty whether a particular drug is a
"new drug" within the meaning of § 201(p)(1) of the 1938 Act.
See Abbott Laboratories v. Gardner, 387 U.
S. 136.
It is argued, however, that the only lawful purpose of an FDA
hearing is to allow it a method for determining which lawsuits it
will file in the future. Yet that is only another version of the
tactics of delay and procrastination
Page 412 U. S. 627
which the industry offers as the way best to serve industry's
needs. The public needs are, however, opposed and paramount. We do
not accept the invitation to hold that FDA has no jurisdiction to
determine whether a particular drug is a "new drug" and to decide
whether an NDA should be withdrawn.
Its determination that a product is a "new drug" or a "me-too"
drug is, of course, reviewable. But its jurisdiction to determine
whether it has jurisdiction is as essential to its effective
operation as is a court's like power.
Cf. United States v.
Shipp, 203 U. S. 563,
203 U. S. 573.
The heart of the new procedures designed by Congress is the grant
of primary jurisdiction to FDA, the expert agency it created. FDA
does not have the final say, for review may be had not in a
district court (except in a limited group of cases we will
discuss), but in a court of appeals. FDA does not have unbridled
discretion to do what it pleases. Its procedures must satisfy the
rudiments of fair play. Judicial relief is available only after
administrative remedies have been exhausted.
It is argued that, though FDA is empowered to decide the
threshold question whether the drug is a "new drug," that power is
only an incident to its power to approve or withdraw approval of
NDA's. Some manufacturers, however, have no NDA's in effect, and
are not seeking approval of any drugs. Nevertheless, FDA may make a
declaratory order that a drug is a "new drug." While that order is
not reviewable in the court of appeals under § 505(h), it is
reviewable by the district court under the Administrative Procedure
Act. 5 U.S.C. §§ 701-704;
Citizens to Preserve
Overton Park v. Volpe, 401 U. S. 402,
401 U. S. 410;
Abbott Laboratories v. Gardner, supra, at
387 U. S.
139-148. By analogy, an agency order declaring a
commodity not exempt from regulation is normally a declaratory
order that is reviewable, as we held in
Frozen Food Express v.
United States, 351 U. S. 40.
Page 412 U. S. 628
The question then presented is whether FDA properly exercised
its jurisdiction in this instance. As indicated above, Hynson, in
requesting an administrative hearing, also asked FDA to decide that
Lutrexin is not a "new drug" within the meaning of § 201(p) as
amended, 21 U.S.C. § 321(p). [
Footnote 21] In addition, it asked that Lutrexin be
"grandfathered" under § 107(c)(4) of the 1962 amendments.
[
Footnote 22] The
Commissioner rejected both claims. Finding that Hynson had failed
to present any evidence of adequate and well controlled
investigations in support
Page 412 U. S. 629
of Lutrexin's effectiveness, he concluded that
"there is no data base upon which experts can fairly and
responsibly conclude that the safety and effectiveness of the drugs
has been proven and is so well established that the drugs can be
generally recognized among such experts as safe and effective for
their intended uses."
The Commissioner also held that Lutrexin is not exempt under
§ 107(c)(4) because its NDA, which had become effective in
1953, had not been withdrawn prior to the enactment of the 1962
amendments, and thus was "covered by an effective application"
within the meaning of § 107(c)(4)(C). The Court of Appeals
affirmed the Commissioner's ruling that Lutrexin is not exempt
under § 107(c)(4). It did not discuss his holding that
Lutrexin currently is a "new drug." Although we agree that the
Commissioner properly ruled that Lutrexin does not come within
§ 107(c)(4), we conclude that the Commissioner's order with
respect to Lutrexin's "new drug" status must be vacated.
The thrust of § 201(p) is both qualitative and
quantitative. The Act, however, nowhere defines what constitutes
"general recognition" among experts. Hynson contends that the "lack
of substantial evidence" is applicable only to proof of the actual
effectiveness of drugs that fall within the definition of a new
drug and not to the initial determination under § 201(p)
whether a drug is "generally recognized" as effective. It would
rely solely on the testimony of physicians and the extant
literature, evidence that has been characterized as "anecdotal." We
agree with FDA, however, that the statutory scheme and overriding
purpose of the 1962 amendments compel the conclusion that the
hurdle of "general recognition" of effectiveness requires at least
"substantial evidence" of effectiveness for approval of an NDA. In
the absence of any evidence of adequate and well controlled
investigation supporting the efficacy of Lutrexin,
a
fortiori,
Page 412 U. S. 630
Lutrexin would be a "new drug" subject to the provisions of the
Act. [
Footnote 23]
As noted, the 1962 amendments for the first time gave FDA power
to scrutinize and evaluate drugs for effectiveness as well as
safety. The Act requires the Commissioner to disapprove any
application when there is a lack of "substantial evidence" that the
applicant's drug is effective. § 505(d), 21 U.S.C. §
356(d). Similarly, he may withdraw approval for any drug if he
subsequently determines that there is a lack of such evidence.
§ 505(e), 21 U.S.C. § 355(e). Evidence may be accepted
only if it consists of "adequate and well controlled
investigations, including clinical investigations, by experts
qualified by scientific training and experience to evaluate the
effectiveness of the drug involved. . . ." § 505(d), 21 U.S.C.
§ 355(d). The legislative history of the Act indicates that
the test was to be a rigorous one. The "substantial evidence"
requirement reflects the conclusion of Congress, based upon
hearings, [
Footnote 24] that
clinical impressions of practicing physicians and poorly controlled
experiments do not constitute an adequate basis for establishing
efficacy. This policy underlies the regulations defining the
contours of "substantial evidence":
"Uncontrolled studies or partially controlled studies are not
acceptable as the sole basis for the approval of claims of
effectiveness. Such studies, carefully conducted and documented,
may provide corroborative support of well controlled studies. . . .
Isolated case reports, random experience, and reports lacking the
details which permit scientific evaluation will not be
considered."
21 CFR § 130.12(a)(5)(ii)(
c).
Page 412 U. S. 631
These efficacy requirements were not designed to be prospective
only. Clearly, after the initial two-year moratorium on existing
drugs, FDA has the power to withdraw an application which became
effective prior to the adoption of the 1962 amendments, if the
applicant has not provided "substantial evidence" of the drug's
efficacy. The Act plainly contemplates that such drugs will be
evaluated on the basis of adequate and well controlled
investigations. Hynson would have us hold that withdrawal
proceedings can be thwarted by a showing of general recognition of
effectiveness based merely on expert testimony and reports with
respect to investigations and clinical observation regardless of
the controls used. But we cannot construe § 201(p) to deprive
FDA of jurisdiction over a drug which, if subject to FDA
regulation, could not be marketed because it had not passed the
"substantial evidence" test. To do so "would be to impute to
Congress a purpose to paralyze with one hand what it sought to
promote with the other."
Clark v. Uebersee Finanz-Korp.,
332 U. S. 480,
332 U. S.
489.
Moreover, the interpretation of § 201(p) urged by Hynson is
not consistent with the statutory scheme as it operates on a purely
prospective basis. Under subsection (2), a drug cannot transcend
"new drug" status until it has been used "to a material extent or
for a material time." Yet, a drug cannot be marketed lawfully
before an NDA has been approved by the Commissioner on the basis of
"substantial evidence." As the Solicitor General argues,
"the Act is designed so that drugs on the market, unless exempt,
will have mustered the requisite scientifically reliable evidence
of effectiveness long before they are in a position to drop out of
active regulation by ceasing to be a 'new drug.'"
It is well established that our task in interpreting separate
provisions of a single Act is to give the Act "the most harmonious,
comprehensive meaning possible" in
Page 412 U. S. 632
light of the legislative policy and purpose.
Clark v.
Uebersee Finanz-Korp., supra, at
332 U. S. 488;
see United States v. Bacto-Unidisk, 394 U.
S. 784,
394 U. S. 798.
We accordingly have concluded that a drug can be "generally
recognized" by experts as effective for intended use within the
meaning of the Act only when that expert consensus is founded upon
"substantial evidence" as defined in § 505(d). We have held in
No. 72-394, however, that the Commissioner was not justified in
withdrawing Hynson's NDA without a prior hearing on whether Hynson
had submitted "substantial evidence" of Lutrexin's effectiveness.
Consequently, any ruling as to Lutrexin's "new drug" status is
premature, and must await the outcome of this hearing.
Finally, we cannot agree with Hynson that Lutrexin is exempt
from the provisions of the Act by virtue of § 107(c)(4) of the
1962 amendments. That section provides that no drug will be treated
as a "new drug" if, on the day preceding the adoption of the
amendments, the drug
"(A) was commercially used or sold in the United States, (B) was
not a new drug as defined by section 201(p) of the basic Act as
then in force, and (C) was not covered by an effective application
under section 505 of that Act. . . ."
The applicability of this section turns solely on whether
Lutrexin was "covered" by an effective NDA immediately prior to the
adoption of the 1962 amendments. Hynson argues that, when Lutrexin
became generally recognized as safe and was no longer a "new drug,"
its NDA ceased to be effective. [
Footnote 25]
Page 412 U. S. 633
That argument draws no statutory support. The 1938 Act did not
provide any mechanism other than the Commissioner's suspension
authority under § 505(e), whereby an NDA once effective could
cease to be effective. Indeed, § 505(e) leads to the
conclusion that an NDA remains effective unless it is suspended.
That section empowers FDA to withdraw approval of an NDA whenever
new evidence comes to light suggesting that the drug has become
unsafe, whether or not the drug as generally recognized as safe in
the interim.
Moreover, Hynson's argument, as the Court of Appeals recognized,
would render clause (C) superfluous. Under Hynson's reasoning, any
drug that could satisfy clause (B) --
i.e., any drug that
had become generally recognized as safe -- automatically would
satisfy clause (C). This construction, therefore, offends the well
settled rule of statutory construction that all parts of a statute,
if at all possible, are to be given effect.
See, e.g., Jarecki
v. G. D. Searle & Co., 367 U. S. 303,
367 U. S. 307;
Ginsberg & Sons v. Popkin, 285 U.
S. 204,
285 U. S. 208.
The
Page 412 U. S. 634
interpretation accorded by the Commissioner and the Court of
Appeals, on the other hand, does give clause (C) operative effect.
It would limit the exemption to drugs, generally recognized as
safe, which had not come under the blanket of an effective NDA.
This interpretation accords with the legislative history which
suggests that the exemption is afforded only for drugs that never
had been subject to new drug regulation. [
Footnote 26]
Except for the modification with respect to Lutrexin's "new
drug" status, the judgment of the Court of Appeals is
Affirmed.
MR. JUSTICE BRENNAN took no part in the consideration or
decision of these cases. MR. JUSTICE STEWART took no part in the
decision of these cases.
|
412
U.S. 609app|
APPENDIX TO OPINION OF THE COURT
Title 21 CFR § 130.12(a)(5) provides:
"(ii) The following principles have been developed over a period
of years and are recognized by the scientific community as the
essentials of adequate and well controlled clinical investigations.
They provide the basis for the determination whether there is
'substantial evidence' to support the claims of effectiveness for
'new drugs' and antibiotic drugs. "
Page 412 U. S. 635
"(
a) The plan or protocol for the study and the report
of the results of the effectiveness study must include the
following: "
"(1) A clear statement of the objectives of the study,"
"(2) A method of selection of the subjects that -- "
"(
i) Provides adequate assurance that they are suitable
for the purposes of the study, diagnostic criteria of the condition
to be treated or diagnosed, confirmatory laboratory tests where
appropriate, and, in the case of prophylactic agents, evidence of
susceptibility and exposure to the condition against which
prophylaxis is desired."
"(
ii) Assigns the subjects to test groups in such a way
as to minimize bias."
"(
iii) Assures comparability in test and control groups
of pertinent variables, such as age, sex, severity, or duration of
disease, and use of drugs other than the test drug."
"(3) Explains the methods of observation and recording of
results, including the variables measured, quantification,
assessment of any subject's response, and steps taken to minimize
bias on the part of the subject and observer."
"(4) Provides a comparison of the results of treatment or
diagnosis with a control in such a fashion as to permit
quantitative evaluation. The precise nature of the control must be
stated and an explanation given of the methods used to minimize
bias on the part of the observers and the analysts of the data.
Level and methods of 'blinding,' if used, are to be documented.
Generally, four types of comparison are recognized: "
"(
i) No treatment: Where objective measurements of
effectiveness are available and placebo effect is negligible,
comparison of the objective results in comparable groups of treated
and untreated patients."
"(
ii) Placebo control: Comparison of the results of use
of the new drug entity with an inactive preparation designed to
resemble the test drug as far as possible. "
Page 412 U. S. 636
"(
iii) Active treatment control: An effective regimen
of therapy may be used for comparison,
e.g., where the
condition treated is such that no treatment or administration of a
placebo would be contrary to the interest of the patient."
"(iv) Historical control: In certain circumstances, such as
those involving diseases with high and predictable mortality (acute
leukemia of childhood), with signs and symptoms of predictable
duration or severity (fever in certain infections), or in case of
prophylaxis, where morbidity is predictable, the results of use of
a new drug entity may be compared quantitatively with prior
experience historically derived from the adequately documented
natural history of the disease or condition in comparable patients
or populations with no treatment or with a regimen (therapeutic,
diagnostic, prophylactic) the effectiveness of which is
established."
"(5) A summary of the methods of analysis and an evaluation of
data derived from the study, including any appropriate statistical
methods."
"
Provided, however, That any of the above criteria may
be waived in whole or in part, either prior to the investigation or
in the evaluation of a completed study, by the Director of the
Bureau of Drugs with respect to a specific clinical investigation;
a petition for such a waiver may be filed by any person who would
be adversely affected by the application of the criteria to a
particular clinical investigation; the petition should show that
some or all of the criteria are not reasonably applicable to the
investigation and that alternative procedures can be, or have been,
followed, the results of which will or have yielded data that can
and should be accepted as substantial evidence of the drug's
effectiveness. A petition for a waiver shall set forth clearly and
concisely the specific provision or provisions in the criteria from
which waiver is sought, why the criteria are not reasonably
applicable to the particular
Page 412 U. S. 637
clinical investigation, what alternative procedures, if any, are
to be, or have been, employed, what results have been obtained, and
the basis on which it can be, or has been, concluded that the
clinical investigation will or has yielded substantial evidence of
effectiveness, notwithstanding nonconformance with the criteria for
which waiver is requested."
"(
b) For such an investigation to be considered
adequate for approval of a new drug, it is required that the test
drug be standardized as to identity, strength, quality, purity, and
dosage form to give significance to the results of the
investigation."
"(
c) Uncontrolled studies or partially controlled
studies are not acceptable as the sole basis for the approval of
claims of effectiveness. Such studies, carefully conducted and
documented, may provide corroborative support of well controlled
studies regarding efficacy and may yield valuable data regarding
safety of the test drug. Such studies will be considered on their
merits in the light of the principles listed here, with the
exception of the requirement for the comparison of the treated
subjects with controls. Isolated case reports, random experience,
and reports lacking the details which permit scientific evaluation
will not be considered."
* Together with No. 72-414,
Hynson, Westcott & Dunning,
Inc. v. Weinberger, Secretary of Health, Education, and
Welfare,
et al., also on certiorari to the same court.
[
Footnote 1]
Drug Amendments of 1962 (Harris-Kefauver Act), 76 Stat. 70,
amending 21 U.S.C. § 301
et seq.
[
Footnote 2]
The Act originally provided for filing applications with the
Secretary of Agriculture, but his functions were assigned to FDA.
FDA is now part of the Department of Health, Education, and Welfare
(HEW), and the Secretary of HEW has delegated his responsibilities
under the Federal Food, Drug, and Cosmetic Act to the Commissioner
of Food and Drugs. 21 CR § 2.120.
[
Footnote 3]
"Substantial evidence" was defined to mean
"evidence consisting of adequate and well controlled
investigations, including clinical investigations, by experts
qualified by scientific training and experience to evaluate the
effectiveness of the drug involved, on the basis of which it could
fairly and responsibly be concluded by such experts that the drug
will have the effect it purports or is represented to have. . .
."
21 U.S.C. § 355(d).
[
Footnote 4]
Drug Amendments of 1962, §§ 107(c)(2) and (c)(3)(b),
76 Stat. 788, note following 21 U.S.C. § 321.
[
Footnote 5]
Id. § 107(c)(4).
[
Footnote 6]
31 Fed.Reg. 9426.
[
Footnote 7]
FDA has recently adopted a regulation declaring the manner in
which Drug Efficacy Study Implementation Notices and Notices of
Opportunity for Hearing apply to identical, related, and similar
drugs. Any person with an interest in such drugs is provided an
opportunity for hearing on any proposed withdrawal of NDA approval
for the basic or pioneer drug. 37 Fed.Reg. 23185, adding §
130.40 to 21 CFR.
[
Footnote 8]
35 Fed.Reg. 7251, amending 21 CFR §§ 130.12(a)(5) and
130.14.
[
Footnote 9]
Section 505(e) as amended, 21 U.S.C. § 355(e), provides in
relevant part:
"The Secretary shall, after due notice and opportunity for
hearing to the applicant, withdraw approval of an application with
respect to any drug under this section if the Secretary finds . . .
(3) on the basis of new information before him with respect to such
drug, evaluated together with the evidence available to him when
the application was approved, that there is a lack of substantial
evidence that the drug will have the effect it purports or is
represented to have under the conditions of use prescribed,
recommended, or suggested in the labeling thereof. . . ."
[
Footnote 10]
See n 3,
supra.
[
Footnote 11]
Title 21 CFR § 130.12(a)(5) as amended, 35 Fed.Reg. 7251,
is set forth in relevant part in an
412
U.S. 609app|>Appendix to this opinion.
[
Footnote 12]
Subjects must be chosen so that they are "suitable for the
purposes of the study," assigned to test groups in such a way as to
minimize bias, and comparable in terms of "pertinent variables,
such as age, sex, severity, or duration of disease, and use of
drugs other than the test drug." 21 CFR §
130.12(a)(5)(ii)(a)(2).
[
Footnote 13]
Upjohn Co. v. Finch, 422 F.2d 944 (CA6);
Pharmaceutical Manufacturers Assn. v.
Richardson, 318 F.
Supp. 301 (Del.). FDA was enjoined from enforcing the
regulations as originally issued on September 19, 1969, 34 Fed.Reg.
14596, on the ground that FDA had not complied with the notice
requirements of the Administrative Procedure Act.
Pharmaceutical Manufacturers Assn. v.
Finch, 307 F.
Supp. 858 (Del.). The regulations were reissued in their
current form on May 8, 1970. 35 Fed.Reg. 7251.
[
Footnote 14]
See Hearings on S. 1552 before the Subcommittee on
Antitrust and Monopoly of the Senate Committee on the Judiciary,
87th Cong., 1st Sess., pt.. 1, pp. 195, 282, 411-412. Much of this
aspect of the legislative background of the 1962 Act is reviewed in
enlightening detail by Judge Latchum in
Pharmaceutical
Manufacturers Assn. v. Richardson, supra, at 306
et
seq.
[
Footnote 15]
S.Rep. No. 1744, 87th Cong., 2d Sess., pt.. 2, p. 1.
[
Footnote 16]
Id. at 6.
[
Footnote 17]
This applies, of course, only to those regulations that are
precise. For example, the plan or protocol for a study must
include
"[a] summary of the methods of analysis and an evaluation of
data derived from the study, including any appropriate statistical
methods."
21 CFR § 130.12(a)(5)(ii)(a)(5). A mere reading of the
study submitted will indicate whether the study is totally
deficient in this regard. Some of the regulations, however, are not
precise, as they call for the exercise of discretion or subjective
judgment in determining whether a study is adequate and well
controlled. For example, § 130.12(a)(5)(ii)(a)(2)(i) requires
that the plan or protocol for the study include a method of
selection of the subjects that provide "
adequate assurance
that they are suitable for the purposes of the study." (Emphasis
added.) The qualitative standards "adequate" and "suitable" do not
lend themselves to clear-cut definition, and it may not be possible
to tell from the face of a study whether the standards have been
met. Thus, it might not be proper to deny a hearing on the ground
that the study did not comply with this regulation.
[
Footnote 18]
Under the Rules of Civil Procedure, the party moving for summary
judgment has the burden of showing the absence of a genuine issue
as to any material fact.
Adickes v. Kress & Co.,
398 U. S. 144,
398 U. S.
157.
[
Footnote 19]
Under the Administrative Procedure Act, a court reviews agency
findings to determine whether they are supported by substantial
evidence only in a case subject to the hearing provisions of 5
U.S.C. §§ 556 and 557 or "otherwise reviewed on the
record of an agency hearing provided by statute. . . ." 5 U.S.C.
§ 706(2)(E). This is not such a case. The question with which
we are concerned involves the initial agency determination whether
a hearing is required by statute.
See Pfizer, Inc. v.
Richardson, 434 F.2d 536, 546-547 (CA2).
[
Footnote 20]
1939 Annual Report FDA; 1941 Annual Report FA; Annual Reports
Federal Security Agency (1931952); Annual Reports HEW
(1953-1962).
[
Footnote 21]
That section provides:
"The term 'new drug' means -- "
"(1) Any drug (except a new animal drug or an animal feed
bearing or containing a new animal drug) the composition of which
is such that such drug is not generally recognized, among experts
qualified by scientific training and experience to evaluate the
safety and effectiveness of drugs, as safe and effective for use
under the conditions prescribed, recommended, or suggested in the
labeling thereof, except that such a drug not so recognized shall
not be deemed to be a 'new drug' if at any time prior to the
enactment of this chapter it was subject to the Food and Drugs Act
of June 30, 1906, as amended, and if at such time its labeling
contained the same representations concerning the conditions of its
use; or"
"(2) Any drug (except a new animal drug or an animal feed
bearing or containing a new animal drug) the composition of which
is such that such drug, as a result of investigations to determine
its safety and effectiveness for use under such conditions, has
become so recognized, but which has not, otherwise than in such
investigations, been used to a material extent or for a material
time under such conditions."
[
Footnote 22]
That section provides:
"In the case of any drug which, on the day immediately preceding
the enactment date, (A) was commercially used or sold in the United
States, (B) was not a new drug as defined by section 201(p) of the
basic Act as then in force, and (C) was not covered by an effective
application under section 505 of that Act, the amendments to
section 201(p) made by this Act shall not apply to such drug when
intended solely for use under conditions prescribed, recommended,
or suggested in labeling with respect to such drug on that
day."
[
Footnote 23]
It also follows that, if Hynson were not entitled to a hearing
under § 505(e), it would not be entitled to a hearing on its
claim that Lutrexin is not a "new drug."
[
Footnote 24]
See Hearings,
supra, n 14.
[
Footnote 25]
Hynson also argues that Lutrexin is exempt by operation of
§ 107(c)(2), which provides:
"An application filed pursuant to section 505(b) of the basic
Act which was 'effective' within the meaning of that Act on the day
immediately preceding the enactment date shall be deemed, as of the
enactment date, to be an application 'approved' by the Secretary
within the meaning of the basic Act as amended by this Act."
Hynson contends that Lutrexin, generally recognized as safe
prior to 1962, was not a "new drug" under applicable standards
before the 196 amendments. Thus, the argument goes, its NDA had
ceased to be effective and could not be deemed "approved" under
§ 107(c)(2). Consequently, there was no approval that could be
withdrawn in administrative proceedings pursuant to §
505(e).
This argument shares a common thread with the argument under
§ 107(c)(4) -- that the NDA for Lutrexin had ceased to be
effective. The argument is no more persuasive under §
107(c)(2) than § 107(c)(4). In addition, the construction
offered by Hynson would upset the carefully drawn transitionary
provisions of §§ 10(c)(2) and (c)(3). Since the
Commissioner now must affirmatively approve or disapprove all
NDA's, § 107(c)(2) was enacted to remove the administrative
burden of approving each and every NDA then effective. It also
protected the marketing authority of all manufacturers that had
effective NDA's. Without this provision, no manufacturer whose drug
had become generally recognized as safe could have continued to
market the drug if it was not also generally recognized as
effective.
[
Footnote 26]
See S.Rep. No. 1744, 87th Cong., 2d Sess., pt.. 2, p.
8; H.R.Rep. No. 2464, 87th Cong., 2d Sess., 12; H.R.Rep. No. 2526,
87th Cong., 2d Sess., 22-23. Hynson contends that the construction
afforded by FDA renders the exemption nugatory and defeats the
legislative purpose. The provision, however, does exempt drugs
that, as a generic class, were never subject to new drug
regulation. These consist primarily of over the counter drugs
which, although they were not "grandfathered" under the 1938 Act,
were not subject to new drug regulation because of universal
recognition of the safety of their old, established ingredients at
the time they came on the market.
MR. JUSTICE POWELL, concurring in part, and concurring in the
result in part.
I concur in
412 U. S.
which disposes of the issues raised by Hynson, Westcott &
Dunning, Inc., in its cross-petition (No. 72-414). As to
412 U. S.
which addresses issues raised in the petition filed by the
Commissioner of FDA (No. 72-394), I concur only in the result, and
state briefly the limited sense in which I accept the Court's
conclusion.
Insofar as the Court today sustains the holding below that
Hynson's submission to FDA raised "a genuine and
Page 412 U. S. 638
substantial issue of fact" requiring a hearing on the ultimate
issue of efficacy, 21 CFR § 130.14(b), I am in accord.
Hynson's presentation in support of the efficacy of Lutrexin
clearly justified a hearing as to whether the drug was supported by
"adequate and well controlled investigations," 21 U.S.C. §
355(d), even as that term is defined in the Commission's
regulations. 21 CFR § 130.12(a)(5). For this reason, I concur
in the result reached in this case. I cannot agree on this record,
however, with any implications or conclusions in the Court's
opinion to the effect that the regulations -- as construed and
applied by the Commissioner in this case -- are either compatible
with the statutory scheme or constitutional under the Due Process
Clause. [
Footnote 2/1] Such
questions have not been squarely presented here and, in light of
the Court's conclusion that Hynson has complied with the
regulations, their resolution is unnecessary to the Court's
decision.
Were we required to reach these issues, there might well be
serious doubt whether the Commissioner's rigorous threshold
specifications as to proof of "adequate and well controlled
investigations," coupled with his restrictive summary judgment
regulation, go beyond the statutory requirements and in effect
frustrate the congressional mandate for a pre-withdrawal
"opportunity for hearing." 21 U.S.C. § 355(e). There is also a
genuine issue of procedural due process where, as in this case, the
Commissioner construes his regulations to deny a hearing as to the
efficacy of a drug established and used by the medical profession
for two decades, and where its effectiveness
Page 412 U. S. 639
is supported by a significant volume of clinical data and the
informed opinions of experts whose qualifications are not
questioned. [
Footnote 2/2]
These important and complex questions should await decision in
future cases in which the issues are briefed fully and are
necessary to the Court's decision.
[
Footnote 2/1]
Cf. Fuentes v. Shevin, 407 U. S.
67,
407 U. S. 80
(1972), and cases cited therein. I do not question, of course, the
authority of the Commissioner to adopt reasonable regulations
consistent with the statute and which do not, as applied, deprive
persons of their property without the elementary due process of a
fair opportunity for a hearing.
[
Footnote 2/2]
There can be no doubt, both from the legislative history and the
language of the 1962 amendments to the Act, that Congress intended
to impose standards that would bar reliance upon anecdotal evidence
or mere professions of belief by doctors as determinative of a
drug's efficacy. But it is also clear that Congress intended to
protect against the arbitrary withdrawal or withholding of approval
of a drug where there is "substantial evidence" of its
effectiveness. To provide protection against such action,
especially when authority is vested in an official who acts in an
administrative, as well as judicial, capacity, the Act specifically
provides for a hearing. The public interest is twofold: (i) to
remove from the market, in accordance with due process, drugs of no
utility or effectiveness; and (ii) to retain on the market those
drugs that are efficacious. In an understandable zeal to remove the
former, an administrative agency must not overlook both the
interest of the public and the right of the proprietor in
protecting the drugs that are useful in the prevention, control, or
treatment of illness.