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Statutory Instruments

2019 No. 744

Exiting The European Union

Medicines

The Medicines for Human Use (Clinical Trials) (Amendment) (EU Exit) Regulations 2019

Made

29th March 2019

Coming into force in accordance with regulation 1

The Secretary of State makes these Regulations in exercise of the powers conferred by section 8(1) of, and paragraph 21 of Schedule 7 to, the European Union (Withdrawal) Act 2018 M1.

In accordance with paragraph 1(1) of Schedule 7 to that Act, a draft of these Regulations has been laid before and approved by a resolution of each House of Parliament.

Marginal Citations

Citation and commencementU.K.

1.  These Regulations may be cited as the Medicines for Human Use (Clinical Trials) (Amendment) (EU Exit) Regulations 2019 and come into force on exit day.

Commencement Information

I1Reg. 1 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of the Medicines for Human Use (Clinical Trials) Regulations 2004U.K.

2.  The Medicines for Human Use (Clinical Trials) Regulations 2004 M2 are amended as follows.

Commencement Information

I2Reg. 2 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

Amendment of regulation 2 (interpretation)U.K.

3.—(1) Regulation 2(1) M3 is amended as follows.

(2) For the definition of “Commission Directive 2003/94/EC” substitute—

[F1“Commission Directive 2003/94/EC”, other than in Parts 2 and 3 of Schedule 7, means—

(a) in the case of an investigational medicinal product manufactured or assembled in, or imported into, Great Britain—

(i)Commission Directive 2003/94/EC laying down the principles and guidelines of good manufacturing practice for medicinal products for human use and for investigational medicinal products for human use, as modified by Schedule 2A to the 2012 Regulations, or

(ii)if Regulations have been made under the powers in regulation B17(1) of the 2012 Regulations, and have come into force, those Regulations;

(b) in the case of an investigational medicinal product manufactured or assembled in, or imported into, Northern Ireland, Commission Directive 2003/94/EC laying down the principles and guidelines of good manufacturing practice for medicinal products for human use and for investigational medicinal products for human use; ].

(3) After the definition of “container” insert—

country” means a country or territory;.

(4) In the definition of “export”, for “a third country from an EEA State” substitute “ another country from the United Kingdom ”.

(5) Omit the definition of “the GCP Directive”.

(6) For the definition of “import” substitute—

[F2“import”, except in regulation 13 and Schedule 13, means import, or attempt to import—

(a)

into Great Britain other than from Northern Ireland, or

(b)

into Northern Ireland from a country other than an EEA State,

whether by land, sea or air and “imported” is to be construed accordingly;;].

F3(7) . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

(8) For the definition of “marketing authorization”, substitute—

[F4“marketing authorization” means—

(a) a UK marketing authorization,

(b) an EU marketing authorisation (as defined in the 2012 Regulations), or

(c)an authorization granted by a regulatory body responsible for licensing medicinal products in a country that is included in the list referred to in regulation 2A(1);].

F5(9) . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

(10) Omit the definition of “third country”.

(11) After the definition of “trial site” insert—

[F6“UK marketing authorization”—

(a)has the same meaning as “UK marketing authorisation” in the 2012 Regulations (and references to “UKMA(UK)”, “UKMA(GB)” and “UKMA(NI)” in these Regulations should be construed in accordance with that definition); and

(b)includes a product licence granted by the licensing authority for the purposes of section 7 of the Medicines Act 1968;].

(12) In the definition of “unexpected adverse reaction”, in paragraph (a), after “summary of product characteristics” insert “ , or equivalent document, ”.

Textual Amendments

F1Words in reg. 3(2) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(a)

F2Words in reg. 3(6) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(b)

F3Reg. 3(7) omitted (31.12.2020 immediately before IP completion day) by virtue of The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(c)

F4Words in reg. 3(8) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(d)

F5Reg. 3(9) omitted (31.12.2020 immediately before IP completion day) by virtue of The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(e)

F6Words in reg. 3(11) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 1(f)

Commencement Information

I3Reg. 3 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M3Regulation 2(1) was amended by S.I. 2004/3224, 2005/2759, 2006/562 and 1928, 2007/3101, 2008/941, 2011/2581, 2012/1479, 1641 and 1916, 2013/235 and 2016/696 and S.R. 2008/192.

Insertion of regulation 2A (list of countries for the purpose of the definition of “marketing authorization”)U.K.

4.  After regulation 2, insert—

List of countries for the purpose of the definition of “marketing authorization”

2A.(1) The licensing authority must publish a list of countries for the purpose of the definition of “marketing authorization”.

(2) In order to determine whether a country should be included in the list referred to in paragraph (1), the licensing authority may, in particular, take into account the regulatory equivalence of that country to the United Kingdom in assessing the safety, quality and efficacy of medicinal products.

(3) The licensing authority must—

(a)review the countries it has included in the list referred to in paragraph (1) to determine if it is still satisfied that the country should remain on that list, and if it is not so satisfied, remove that country from the list; and

(b)undertake such a review at least every three years beginning with the date on which that country is included in that list..

Commencement Information

I4Reg. 4 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 3 (sponsor of a clinical trial)U.K.

5.—(1) Regulation 3 M4 is amended as follows.

(2) In paragraph (11)(a), for “an EEA State”, substitute “ the United Kingdom or a country that is included in the list referred to in paragraph (11A) ”.

(3) After paragraph (11), insert—

(11A) The licensing authority must publish a list of countries where a sponsor of a clinical trial, or their legal representative, may be established for the purpose of paragraph (11).

(11B) In order to determine whether a country should be included in the list referred to in paragraph (11A), the licensing authority may, in particular, take into account—

(a)the mechanisms that the country has in place to assist the licensing authority in contacting, or obtaining information in respect of, a sponsor or legal representative that is established there; and

(b)the country's ability to assist the licensing authority in any action it may need to take in respect of a sponsor or legal representative that is established there.

(11C) The licensing authority must—

(a)review the countries it has included in the list referred to in paragraph (11A) to determine if it is still satisfied that the country should remain on that list, and if it is not so satisfied, remove that country from the list; and

(b)undertake such a review at least every three years beginning on the date on which that country is included in that list..

Commencement Information

I5Reg. 5 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M4Regulation 3 was amended by S.I. 2006/1928.

Omission of regulation 4 (responsibility for functions under the Directive)U.K.

6.  Omit regulation 4 M5.

Commencement Information

I6Reg. 6 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M5Regulation 4 was amended by S.I. 2006/1928 and 2012/1916.

Amendment of regulation 13 (supply of investigational medicinal products for the purpose of clinical trials)U.K.

7.—(1) Regulation 13 is amended as follows.

(2) For paragraph (2)(b) M6, substitute—

[F7(b) in the case of—

(i)an investigational medicinal product manufactured or assembled in the United Kingdom, the product has been manufactured or assembled—

(aa)in accordance with the terms of a manufacturing authorisation, or

(bb)in the case of assembly only, under the exemption in regulation 37;

(ii)an investigational medicinal product imported into Northern Ireland from an EEA State—

(aa)the product has been manufactured, assembled or imported into an EEA State in accordance with the terms of an authorisation referred to in Article 13 of the Directive granted by a competent authority of an EEA State, and

(bb)the production batch of investigational medicinal products of which the product is a part has been checked and certified by a qualified person pursuant to Article 13(3) and (4) of the Directive;

(iii)an investigational medicinal product imported into Northern Ireland from a country other than an EEA State, the product has been imported into Northern Ireland in accordance with the terms of a manufacturing authorisation;

(iv)an investigational medicinal product imported into Great Britain other than from Northern Ireland, the product has been imported in accordance with the terms of a manufacturing authorisation.].

(3) After paragraph (2), insert—

(2A) The condition specified in paragraph (2)(b) does not apply to an investigational medicinal product that has been manufactured or assembled in accordance with the terms of a F8... marketing authorization [F9or marketing authorisation issued by the competent authority of an EEA State in accordance with Directive 2001/83/EC] relating to that product..

(4) Omit paragraph (3).

[F10(5) For paragraph (4) substitute—

(4) The restriction in paragraph (1) shall not apply to—

(a)the sale or supply of a medicinal product in Great Britain in accordance with the terms of a UKMA(GB) or UKMA(UK), and

(b)the sale or supply of a medicinal product in Northern Ireland in accordance with—

(i)the terms of a UKMA(NI) or UKMA(UK), or

(ii)an EU marketing authorisation (as defined in the 2012 Regulations)..]

Textual Amendments

F7Words in reg. 7(2) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 2(a)

F8Word in reg. 7(3) omitted (31.12.2020 immediately before IP completion day) by virtue of The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 2(b)(i)

F9Words in reg. 7(3) inserted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 2(b)(ii)

F10Reg. 7(5) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 2(c)

Commencement Information

I7Reg. 7 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M6Paragraph (2)(b) was amended by S.I. 2006/1928.

Amendment of regulation 15 (ethics committee opinion)U.K.

8.  In regulation 15(5)(e) M7, after “summary of product characteristics” insert “ , or equivalent document, ”.

Commencement Information

I8Reg. 8 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M7Paragraph (5) was amended by S.I. 2006/1928.

Amendment of regulation 20 (authorisation procedure for clinical trials involving medicinal products with special characteristics)U.K.

9.  In regulation 20(1)(a), for paragraph (i) substitute—

(i)which do not have a marketing authorization and are developed by means of one of the following biotechnological processes—

(aa)recombinant DNA technology,

(bb)controlled expression of genes coding for biologically active proteins in prokaryotes and eukaryotes including transformed mammalian cells,

(cc)hybridoma and monoclonal antibody methods, or.

Commencement Information

I9Reg. 9 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 21 (clinical trials conducted in third countries)U.K.

10.—(1) Regulation 21 is amended as follows.

(2) In the heading, for “third countries” substitute “ countries other than the United Kingdom ”.

(3) In paragraph (1), for “a third” substitute “ another ”.

Commencement Information

I10Reg. 10 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Insertion of regulation 27B (publication of information)U.K.

11.  After regulation 27A (information sharing) M8, insert—

Publication of information

27B.(1) Subject to paragraph (3), the licensing authority may make accessible to the public information contained in the items listed in paragraph (2) insofar as it relates to a clinical trial carried out, or being carried out, under these Regulations.

(2) The items listed in this paragraph are—

(a)the request for authorisation made under regulation 17;

(b)any amended request for authorisation made under regulation 18, 19 or 20;

(c)any amendment to the protocol made under regulation 23, 24 or 25;

(d)the favourable opinion of the ethics committee given in accordance with regulation 15 or the favourable opinion given by an appeal panel in accordance with paragraph 4 of Schedule 4;

(e)the notification of the end of the clinical trial made under regulation 27.

(3) Prior to making information available to the public under paragraph (1), the licensing authority must, after consulting such persons as the licensing authority considers appropriate, publish a list of the information which may be made accessible to the public under paragraph (1)..

Commencement Information

I11Reg. 11 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M8Regulation 27A was inserted by S.I. 2006/1928.

Amendment of regulation 31 (suspension or termination of clinical trial)U.K.

12.  In regulation 31(4), omit sub-paragraphs (b), (d) and (e).

Commencement Information

I12Reg. 12 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 31A (trial master file and archiving)U.K.

13.  In regulation 31A(4)(b) M9

(a)for “applicable”, substitute “ relevant ”; and

(b)for the words “Directive 2001/83/EC” to the end, substitute “ these Regulations ”.

Commencement Information

I13Reg. 13 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M9Regulation 31A was inserted by S.I. 2006/1928.

Amendment of regulation 33 (notification of suspected unexpected serious adverse reactions)U.K.

14.—(1) Regulation 33 is amended as follows.

(2) Omit paragraph (1)(b)(ii).

(3) Omit paragraph (3)(b).

(4) Omit paragraph (4).

(5) Omit paragraph (6)(b), and the “and” immediately preceding it.

Commencement Information

I14Reg. 14 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 34 (clinical trials conducted in third countries)U.K.

15.—(1) In the heading of regulation 34, for “third countries” substitute “ countries other than the United Kingdom ”.

(2) In regulation 34—

(a)for “a third country” substitute “ another country ”; and

(b)for the words “entered into” to the end, substitute—

reported as soon as possible to the licensing authority, and in any event—

(a)in the case of a reaction that is fatal or life-threatening, within 7 days beginning with the day after the sponsor was first aware of the reaction; or

(b)in any other case, within 15 days beginning with the day after the sponsor is first aware of the reaction..

Commencement Information

I15Reg. 15 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 35 (annual list of suspected serious adverse reactions and safety report)U.K.

16.—(1) Regulation 35 is amended as follows.

(2) In paragraph (2)(b), for “EEA State” substitute “ any country ”.

(3) In paragraph (3)—

(a)for “an EEA State” substitute “ a country ”; and

(b)for sub-paragraphs (a) and (b), substitute—

(a)the date on which the trial was authorised by a regulatory body responsible for authorising clinical trials in that country; or

(b)where the clinical trial was conducted in a country without a formal authorisation process, a date designated by the sponsor that is linked to the commencement of the first clinical trial..

Commencement Information

I16Reg. 16 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 36 (requirement for authorisation to manufacture or import investigational medicinal products)U.K.

[F1117.  In regulation 36(2), after “marketing authorization” insert “or marketing authorisation issued by the competent authority of an EEA State in accordance with Directive 2001/83/EC”.]

Textual Amendments

F11Reg. 17 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 3

Commencement Information

I17Reg. 17 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 43 (qualified persons)U.K.

[F1218.  In regulation 43—

(a)for paragraphs (1) and (2) substitute—

(1) Subject to paragraphs (4) and (5), the holder of a manufacturing authorisation must have at his disposal the services of at least one qualified person—

(a)where the manufacturing authorisation relates wholly to the import of an investigational medicinal product into Great Britain from an approved country for import, who must operate and be ordinarily resident in either the United Kingdom or an approved country for import, or

(b)in any other case, who must operate and be ordinarily resident in the United Kingdom, and

who is responsible for carrying out the duties referred to in paragraph 2.

(2) Subject to paragraphs (2A) and (2C), the qualified person is responsible for ensuring that—

(a)in the case of an investigational medicinal product manufactured in Northern Ireland, each production batch has been manufactured and checked in compliance with—

(i)the requirements of these Regulations;

(ii)the principles and guidelines of good manufacturing practice;

(iii)the product specification, as defined in Part 1 of Schedule 7; and

(iv)the request, particulars and documents submitted to the licensing authority under regulation 17 in respect of the clinical trial in which the product is to be used;

(b)in the case of an investigational medicinal product manufactured in Great Britain, each production batch has been manufactured and checked in compliance with—

(i)the requirements of these Regulations;

(ii)the principles and guidelines of good manufacturing practice, as modified by Schedule 2A to the 2012 Regulations or any regulations made under the power in regulation B17(1) of those Regulations;

(iii)the product specification, as defined in Part 1 of Schedule 7; and

(iv)the request, particulars and documents submitted to the licensing authority under regulation 17 in respect of the clinical trial in which the product is to be used;

(c)in the case of an investigational medicinal product imported into Northern Ireland from a country other than an EEA State, each production batch has been manufactured and checked in compliance with—

(i)standards of good manufacturing practice at least equivalent to the principles and guidelines of good manufacturing practice;

(ii)the product specification, as defined in Part 1 of Schedule 7; and

(iii)the request, particulars and documents submitted to the licensing authority under regulation 17 in respect of the clinical trial in which the product is to be used;

(d)in the case of an investigational medicinal product imported into Great Britain other than from Northern Ireland, each production batch has been manufactured and checked in compliance with—

(i)standards of good manufacturing practice at least equivalent to the principles and guidelines of good manufacturing practice, as modified by Schedule 2A to the 2012 Regulations or any regulations made under the power in regulation B17(1) of those Regulations;

(ii)the product specification, as defined in Part 1 of Schedule 7; and

(iii)the request, particulars and documents submitted to the licensing authority under regulation 17 in respect of the clinical trial in which the product is to be used.

(2A) The qualified person is not responsible for carrying out the controls in paragraph (2) where—

(a)the product is imported into Great Britain from a country that is included on the list referred to in regulation 43A (“approved country for import”); and

(b)the qualified person ensures that there is appropriate evidence to confirm that each production batch has been certified as provided for in Article 13 of the Directive, or such equivalent certification procedure as applies in the approved country for import.

(2B) The licensing authority must publish guidance on the evidence that it considers to be appropriate for the purposes of paragraph (2A)(b).

(2C) The qualified person is not responsible for carrying out the controls in paragraph (2) where—

(a)an investigational medicinal product—

(i)which has a marketing authorization other than a UKMA(GB), is imported into Northern Ireland as a comparator product; or

(ii)which has a marketing authorization, or has been approved for marketing in another country, is imported into Great Britain as a comparator product; and

(b)documentation cannot be obtained certifying that each production batch has been manufactured and checked in accordance with standards of good manufacturing practice at least equivalent to those laid down in Commission Directive 2003/94/EC.

(2D) Where paragraph (2) does not apply by virtue of paragraph (2C), the qualified person is responsible for ensuring that each production batch has undergone all relevant analyses, tests or checks necessary to confirm its quality in accordance with the request, particulars and documents submitted to the licensing authority under regulation 17.

(2E) The qualified person is responsible for ensuring, in relation to an investigational medicinal product, that documentary evidence is produced that each batch of the product satisfies the provisions of paragraph (2), (2A) or (2D) (as the case may be).

(2F) The documentary evidence referred to in paragraph (2E) must be—

(a)kept up to date as operations are carried out; and

(b)available for inspection by the licensing authority for a period of at least five years beginning with the date on which the documentary evidence is produced.;

(b)for paragraph (5) substitute—

(5) For the purposes of this paragraph, but without prejudice to paragraph (6) below, the holder of the authorisation may regard a person as satisfying the provisions of the said Article 49 or 50, as respects formal qualifications if—

(a)in relation to the obligation in paragraph (1)(a), he is already named as a qualified person in respect of an authorisation issued in an approved country for import; or

(b)he produces evidence that—

(i)he is a member of—

(aa)the Institute of Biology,

(bb)the Pharmaceutical Society,

(cc)the Royal Society of Chemistry, or

(dd)such other body as may appear to the licensing authority to be an appropriate body for the purpose of this paragraph; and

(ii)he is regarded by the body of which he is a member as so satisfying those provisions..]

Textual Amendments

F12Reg. 18 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 4

Commencement Information

I18Reg. 18 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Insertion of regulation 43A (approved country for import)U.K.

19.  After regulation 43 insert—

Approved country for import

43A.(1) The licensing authority must publish a list of countries which it is satisfied have a regulatory framework applicable to investigational medicinal products exported to [F13Great Britain] that is equivalent to the regulatory framework in [F13Great Britain], in that the respective control and enforcement activities in those countries ensure an equivalent level of protection of public health.

(2) In order to determine whether a country should be included in the list referred to in paragraph (1), the licensing authority may, in particular, take into account—

(a)the country's system for ensuring that each batch of an investigational medicinal product has been manufactured and checked in accordance with the requirements of its legislation and any authorisation in respect of the clinical trial in which the product is to be used;

(b)the country's rules for good manufacturing practice;

(c)the regularity of inspections to verify compliance with good manufacturing practice;

(d)the effectiveness of enforcement of good manufacturing practice;

(e)the regularity and rapidity of information provided by that country relating to non-compliant manufacturers of investigational medicinal products;

(f)any on-site review of that country's regulatory system undertaken by the licensing authority;

(g)any on-site inspection of a manufacturing site in that country observed by the licensing authority; and

(h)any other relevant documentation available to the licensing authority.

(3) The licensing authority must—

(a)review the countries it has included in the list referred to in paragraph (1) to determine if it is still satisfied that the country should remain on that list, and if it is not so satisfied, remove that country from the list; and

(b)undertake such a review at least every three years beginning with the date on which that country is included in that list..

Textual Amendments

F13Words in reg. 19 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 5

Commencement Information

I19Reg. 19 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 45 (suspension and revocation of manufacturing authorisation)U.K.

20.  In regulation 45(1)(f)(i), [F14for “or any equivalent provisions in any EEA State other than the United Kingdom” substitute “or, in the case of an investigational medicinal product manufactured or assembled in Northern Ireland, any equivalent provisions in any EEA State”.] .

Textual Amendments

F14Words in reg. 20 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 6

Commencement Information

I20Reg. 20 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of regulation 48 (infringement notices)U.K.

21.  In regulation 48(3) M10, omit—

(a)sub-paragraph (a); and

(b)sub-paragraph (c), and the “and” immediately preceding it.

Commencement Information

I21Reg. 21 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M10Regulation 48 was amended by S.I. 2006/1928 and 2012/1916.

Amendment of regulation 56 (transitional provisions)U.K.

22.  In regulation 56, for “Schedule 12” substitute “ Schedules 12 and 13 ”.

Commencement Information

I22Reg. 22 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Insertion of regulation 57 (functions in relation to good clinical practice)U.K.

23.  After regulation 56, insert—

Functions in relation to good clinical practice

57.(1) Regulations may [F15, in respect of Great Britain]

(a)amend the conditions and principles of good clinical practice to take account of technical and scientific progress;

(b)specify requirements for documentation relating to a clinical trial which constitute the master file on the trial at the time the file is archived;

(c)amend or revoke the requirements of regulation 31A relating to the content of the trial master file; and

(d)require guidance published under regulation 58 to be taken into account when interpreting any enactment or other requirement to which the guidance relates.

[F16(2) Any power to make regulations under paragraph (1)—

(a)is exercisable by the Secretary of State by statutory instrument;

(b)includes power to make—

(i)different provision for different purposes or different areas;

(ii)consequential, supplementary, incidental, transitional, transitory or saving provisions, including consequential amendments to these Regulations.

( 3) Regulations under paragraph (1) are subject to annulment in pursuance of a resolution of either House of Parliament. ]

Detailed guidance

58.  The licensing authority may publish guidance on—

(a)the application format and documentation to be submitted in an application for an ethics committee opinion, in particular regarding the information that is given to subjects, and on the appropriate safeguards for the protection of personal data;

(b)the format and contents of a request for authorisation of a clinical trial, as well as the documentation to be submitted to support that request, on the quality and manufacture of the investigational medicinal product, any toxicological and pharmacological tests, the protocol and clinical information on the investigational medicinal product including the investigator's brochure;

(c)the presentation and content of any proposed substantial amendment to the clinical trial authorisation insofar as it relates to the protocol;

(d)the declaration of the end of the clinical trial;

(e)the collection, verification and presentation of adverse event or adverse reaction reports, together with decoding procedures for unexpected serious adverse reactions;

(f)the content of essential documents forming part of the trial master file;

(g)the elements to be taken into account when evaluating investigational medicinal products for the purpose of regulation 43(2)..

Textual Amendments

F15Words in reg. 23 inserted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 7(a)

F16Words in reg. 23 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 7(b)

Commencement Information

I23Reg. 23 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Amendment of Schedule 3 (particulars and documents that must accompany an application for an ethics committee opinion, a request for authorisation, a notice of amendment and a notification of the conclusion of a trial)U.K.

24.—(1) Schedule 3 is amended as follows.

(2) In Part 1 M11, in paragraph 3(b), after “summary of product characteristics” insert “ , or equivalent document, ”.

(3) In Part 2—

(a)in paragraph 1(b), for “an EEA State”M12, substitute “the United Kingdom or a country that is included in the list referred to in regulation 3(11A)”;

(b)in paragraph 4, for “another”, substitute “ an ”;

[F17(c)in paragraph 7, after “details of any” insert “manufacturing authorisation or any”;]

(d)in paragraph 8—

[F18(i)in sub-paragraph (1), after “in accordance with” insert “regulation 43(2) or”;]

[F19(ii)for sub-paragraph (2) substitute—

(2) If an investigational medicinal product to be used in the clinical trial has been, or is to be—

(a)imported into Great Britain from a country other than Northern Ireland or imported into Northern Ireland from a country other than an EEA State, a statement from the qualified person at the disposal of the person holding the manufacturing authorisation in relation to that importation specifying—

(i)the address of any premises outside the United Kingdom at which the product was manufactured or assembled; and

(ii)the manufacturing or assembling operations performed at those premises;

(b)imported into Northern Ireland from an EEA State, a statement from the qualified person at the disposal of the person holding the authorisation referred to in Article 13 of the Directive in relation to that importation specifying—

(i)the address of any premises outside the European Economic Area at which the product was manufactured or assembled; and

(ii)the manufacturing or assembling operations performed at those premises..]

(iii)in paragraph 11(4)(a), after “summary of product characteristics” insert “ or equivalent document ”.

(4) In Part 3, in paragraph 1(b), for “an EEA State”, substitute “ the United Kingdom or a country that is included in the list referred to in regulation 3(11A) ”.

(5) In Part 4, in paragraph 1(b), for “an EEA State”, substitute “ the United Kingdom or a country that is included in the list referred to in regulation 3(11A) ”.

Textual Amendments

F17Reg. 24(3)(c) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 8(a)

F18Reg. 24(3)(d)(i) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 8(b)

F19Reg. 24(3)(d)(ii) substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 8(c)

Commencement Information

I24Reg. 24 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Marginal Citations

M11Part 1 was amended by S.I. 2008/941.

M12The words “an EEA State” were substituted by S.I. 2006/1928.

Amendment of Schedule 7 (standard provisions for manufacturing authorisations)U.K.

[F2025.  In Part 1 of Schedule 7—

(a)for “In this Schedule,” substitute “In this Schedule—”;

(b)the definition of “product specification” becomes part of a list of definitions;

(c)before the definition of “product specification” insert—

“Commission Directive 2003/94/EC”, in relation to the holder of an authorisation means—

(a)

in the case of a holder in Great Britain—

(i)

Commission Directive 2003/94/EC laying down the principles and guidelines of good manufacturing practice for medicinal products for human use and for investigational medicinal products for human use, as modified by Schedule 2A to the 2012 Regulations, or

(ii)

if Regulations have been made under the powers in regulation B17(1) of the 2012 Regulations, and have come into force, those Regulations;

(b)

in the case of a holder in Northern Ireland, Commission Directive 2003/94/EC laying down the principles and guidelines of good manufacturing practice for medicinal products for human use and for investigational medicinal products for human use;;

(d)in the definition of “product specification”, for paragraph (a) substitute—

(a)in the case of an investigational medicinal product manufactured before a request for authorisation to conduct the clinical trial involving those products has been made—

(i)in the case of an investigational medicinal product manufactured or assembled in Great Britain, in accordance with regulation 17, or

(ii)in the case of an investigational medicinal product manufactured or assembled in Northern Ireland, in accordance with regulation 17 or any equivalent provisions in any EEA State,

the specification for that product provided by the person who is to act as the sponsor of the proposed clinical trial,.]

Textual Amendments

F20Reg. 25 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 9

Commencement Information

I25Reg. 25 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Insertion of Schedule 13 (transitional provisions in relation to EU Exit)U.K.

26.  After Schedule 12 insert—

Regulation 56

SCHEDULE 13U.K.Transitional provisions relating to EU Exit

List of countries for the purpose of the definition of “marketing authorization” on [F21IP completion day] (regulation 2A)

1.(1) For the purpose of regulation 2A, during the transitional period, the licensing authority must include each EEA State in the list referred to in paragraph (1) of that regulation.

(2) Notwithstanding regulation 2A(3), the licensing authority must not, before the end of the transitional period, remove an EEA State from the list referred to in regulation 2A(1).

(3) In this paragraph, “transitional period” is the period of two years beginning with [F21IP completion day].

List of countries where a sponsor of a clinical trial, or their legal representative, may be established on [F21IP completion day] (regulation 3(11A))

2.(1) For the purpose of regulation 3, the licensing authority must include each EEA State in the list referred to in paragraph (11A) of that regulation.

(2) Notwithstanding regulation 3(11C), the licensing authority must not, before the end of the transitional period, remove an EEA State from the list referred to in regulation 3(11A).

(3) In this paragraph, “transitional period” is the period of two years beginning with [F21IP completion day].

Import of investigational medicinal products [F22into Great Britain] from EEA States during the transitional period

3.(1) The condition in regulation 13(2)(b) and the restriction in regulation 36(1) do not apply to an investigational medicinal product that is imported [F23into Great Britain] from an EEA State before the end of the transitional period, provided that the production batch of investigational medicinal products of which the product is a part has been checked and certified by a qualified person pursuant to Article 13(3) and (4) of the Directive.

(2) In this paragraph, “transitional period” is the period of one year beginning with [F21IP completion day].

Approved country for import list on [F21IP completion day] (regulation 43A)

4.(1) For the purpose of regulation 43A, during the transitional period, the licensing authority must include each EEA State in the list referred to in paragraph (1) of that regulation.

(2) Notwithstanding regulation 43A(3), the licensing authority must not, before the end of the transitional period, remove an EEA State from the list referred to in regulation 43A(1).

(3) In this paragraph, “transitional period” is the period of two years beginning with [F21IP completion day]..

Textual Amendments

F21Words in reg. 26 substituted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 10(a)

F22Words in reg. 26 inserted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 10(b)(i)

F23Words in reg. 26 inserted (31.12.2020 immediately before IP completion day) by The Human Medicines (Amendment etc.) (EU Exit) Regulations 2020 (S.I. 2020/1488), reg. 1, Sch. 1 para. 10(b)(ii)

Commencement Information

I26Reg. 26 in force at 31.12.2020 on IP completion day (in accordance with 2020 c. 1, Sch. 5 para. 1(1)), see reg. 1

Signed by authority of the Secretary of State for Health and Social Care.

Jackie Doyle-Price

Parliamentary Under-Secretary of State,

Department of Health and Social Care

Explanatory Note

(This note is not part of the Regulations)

These Regulations are made in exercise of the powers conferred by section 8(1) of the European Union (Withdrawal) Act 2018 (c. 16) and amend the Medicines for Human Use (Clinical Trials) Regulations 2004 in order to address failures of retained EU law to operate effectively and other deficiencies (in particular under section 8(2)(a), (b), (c), (d), (f) and (g) and (6)) arising from the withdrawal of the United Kingdom from the European Union.

An impact assessment of the effect that this instrument will have on the costs of business, the voluntary sector and the public sector is available from the Medicines and Healthcare Products Regulatory Agency, 10 South Colonnade, Canary Wharf, London, E14 4PU and is published alongside this instrument at .

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