S.I. No. 598/2007 - European Communities (Human Tissues and Cells Traceability Requirements, Notification of Serious Adverse Reactions and Events and Certain Technical Requirements) Regulations 2007


Notice of the making of this Statutory Instrument was published in

“Iris Oifigiúil” of 4th September, 2007.

I, MARY HARNEY, Minister for Health and Children, in exercise of the powers conferred on me by section 3 of the European Communities Act 1972 (No. 27 of 1972) and for the purpose of giving effect to Directive 2006/86/EC of the European Commission implementing Directive 2004/23/EC of the European Parliament and of the Council as regards traceability requirements, notification of serious adverse reactions and events and certain technical requirements for the coding, processing, preservation, storage and distribution of human tissues and cells, do hereby make the following Regulations:

1. These Regulations may be cited as the European Communities (Human Tissues and Cells Traceability Requirements, Notification of Serious Adverse Reactions and Events and Certain Technical Requirements) Regulations 2007.

2. (1) These Regulations, other than Regulation 22, shall come into operation on 1 September 2007.

(2) Regulation 22 shall come into operation on 1 September 2008.

Interpretation

3. (1) In these Regulations—

“critical” means potentially having an effect on the quality and/or safety of or having contact with the cells and tissues;

“human application” means the use of tissues or cells on or in a human recipient and extracorporal applications;

“organisations responsible for human application” means a health care establishment or a unit of a hospital or another body which carries out human application of human tissues and cells;

“partner donation” means the donation of reproductive cells between a man and a woman who declare that they have an intimate physical relationship;

“procurement organisation” means a health care establishment or a unit of a hospital or another body that undertakes the procurement of human tissues and cells and that may not be accredited, designated, authorised or licensed as a tissue establishment;

“quality management” means the coordinated activities to direct and control an organisation with regard to quality;

“quality system” means the organisational structure, defined responsibilities, procedures, processes, and resources for implementing quality management and includes all activities which contribute to quality, directly or indirectly;

“reproductive cells” means all tissues and cells intended to be used for the purpose of assisted reproduction;

“Responsible Person” in relation to a tissue establishment, means the person who has been designated pursuant to Regulation 8 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ) as the responsible person for that tissue establishment.

“serious adverse event” means any untoward occurrence associated with the procurement testing, processing, storage or distribution of tissues and cells—

(a) that might lead to the transmission of a communicable disease, to death or life-threatening, disabling or incapacitating conditions for patients, or

(b) which might result in, or prolong, hospitalisation or morbidity;

“serious adverse reaction” means an unintended response, including a communicable disease, in the donor or in the recipient associated with procurement or human application of tissues and cells—

(a) that is fatal, life-threatening, disabling or incapacitating, or

(b) which results in, or prolongs, hospitalisation or morbidity;

“Standard Operating Procedures” (SOPs) means written instructions describing the steps in a specific process, including the materials and methods to be used and the expected end product;

“tissue establishment” means a tissue bank or a unit of a hospital or another body where activities of donation, procurement, testing, processing, preservation, storage or distribution of human tissues and cells are undertaken;

“traceability” means the ability to locate and identify the tissue/cell during any step from procurement, through processing, testing and storage, to distribution to the recipient or disposal, which also implies the ability to identify the donor and the tissue establishment or the manufacturing facility receiving, processing or storing the tissue/cells, and the ability to identify the recipient(s) at the medical facility/facilities applying the tissue/cells to the recipient(s); traceability also covers the ability to locate and identify all relevant data relating to products and materials coming into contact with those tissues/cells;

“validation” (or “qualification” in the case of equipment or environments) means establishing documented evidence that provides a high degree of assurance that a specific process, piece of equipment or environment will consistently produce a product meeting its predetermined specifications and quality attributes; a process is validated to evaluate the performance of a system with regard to its effectiveness based on intended use;

(2) A word or expression that is used in these Regulations and is also used in the Commission Directive 2006/86/EC of 24 October 2006 has, unless the contrary intention appears, the same meaning in these Regulations as it has in that Directive.

(3) A word or expression that is used in these Regulations and is also used in the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ) has, unless the contrary intention appears, the same meaning in these Regulations as it has in those Regulations.

Application

4. (1) These Regulations shall apply to the coding, processing, preservation, storage and distribution of:

(a) human tissues and cells intended for human applications; and

(b) manufactured products derived from human tissues and cells intended for human applications where those products are not covered by other Regulations.

(2) The provisions of Regulations 7 to 21 concerning traceability and the reporting of serious adverse reactions and events shall also apply to the donation, procurement and testing of human tissues and cells.

Requirements for the accreditation, designation, authorisation or licensing of tissue establishments

5. A tissue establishment shall comply with the requirements set out in Schedule 1.

Requirements for the accreditation, designation, authorisation, licensing of tissue and cell preparation processes

6. Preparation processes at all tissue establishments shall comply with the requirements set out in Schedule 2.

Notification of serious adverse reactions

7. (a) Each procurement organisation shall have procedures in place to retain the records of tissues and cells procured and to notify tissue establishments without delay of any serious adverse reactions in the living donor which may influence the quality and safety of tissues and cells;

(b) Organisations responsible for human application of tissues and cells shall have procedures in place to retain the records of tissues and cells applied and to notify tissue establishments without delay of any serious adverse reactions observed during and after clinical application which may be linked to quality and safety of tissues and cells;

(c) Each tissue establishment that distributes tissues and cells for human application shall provide information to the organisation responsible for human application of tissues and cells about how that organisation should report serious adverse reactions as referred to in (b).

8. Each tissue establishment shall:

(a) have procedures in place to communicate to the Irish Medicines Board without delay all relevant available information about suspected serious adverse reactions as referred to in Regulation 7(a) and (b);

(b) have procedures in place to communicate to the Irish Medicines Board without delay the conclusion of the investigation to analyse the cause and the ensuing outcome.

9. The responsible person designated for each tissue establishment shall notify the Irish Medicines Board of the information included in the notification set out in Part A of Schedule 3.

10. Each tissue establishment shall:

(a) notify the Irish Medicines Board of the actions taken with respect to other implicated tissues and cells that have been distributed for human applications;

(b) notify the Irish Medicines Board of the conclusion of the investigation, supplying at least the information set out in Part B of Schedule 3.

Notification of serious adverse events

11. (a) Each procurement organisation and tissue establishment shall have procedures in place to retain the records and to notify tissue establishments without delay of any serious adverse events that occur during procurement which may influence the quality and/or safety of human tissues and cells;

(b) Each organisation responsible for human application of tissues and cells shall have procedures in place to notify tissue establishments without delay of any serious adverse events that may influence the quality and safety of the tissues and cells;

(c) Each tissue establishment shall provide to the organisation responsible for human application information about how that organisation should report serious adverse events to them that may influence the quality and safety of the tissues and cells.

12. In the case of assisted reproduction, any type of gamete or embryo misidentification or mix-up shall be considered to be a serious adverse event. All persons or procurement organisations or organisations responsible for human application performing assisted reproduction shall report such events to the supplying tissue establishments for investigation and notification to the Irish Medicines Board.

13. Each tissue establishment shall:

(a) have procedures in place to communicate to the Irish Medicines Board without delay all relevant available information about suspected serious adverse events as referred to in paragraph 11(a) and (b);

(b) have procedures in place to communicate to the Irish Medicines Board without delay the conclusion of the investigation to analyse the cause and the ensuing outcome.

14. The responsible person designated for each tissue establishment shall notify the Irish Medicines Board of the information included in the notification set out in Part A of Schedule 4.

15. Each tissue establishment shall:

(a) evaluate serious adverse events to identify preventable causes within the process;

(b) notify the Irish Medicines Board of the conclusion of the investigation, supplying at least the information set out in Part B of Schedule 4.

Annual reports

16. The Irish Medicines Board shall submit to the European Commission an annual report by 30th June of the following year, on the notification of serious adverse reactions and events received by it.

17. The Irish Medicine Board shall make available to tissue establishments the report it receives from the European Commission summarising the report the Commission received from competent authorities of Member States.

18. Data transmission shall comply with the data exchange format specifications as set out in Part A and B of Schedule 5 and shall provide all the information necessary to identify the sender and maintain its reference data.

Communication of information between competent authorities and to the Commission

19. The Irish Medicines Board shall communicate to the competent authorities of other Member States and to the Commission such information as is appropriate with regard to serious adverse reactions and events, in order to guarantee that adequate actions are taken.

Traceability

20. Each tissue establishment shall have effective and accurate systems to uniquely identify and label cells/tissues received and distributed.

21. Each tissue establishment and each organisation responsible for human application shall retain the data set out in the Schedule 6 for at least 30 years, in an appropriate and readable storage medium.

European coding system

22. (a) Each tissue establishment shall allocate a single European identifying code to all donated material, to ensure proper identification of the donor and the traceability of all donated material and to provide information on the main characteristics and properties of tissues and cells. The code shall incorporate at least the information set out in Schedule 7.

(b) Paragraph (a) shall not apply to partner donation of reproductive cells.

SCHEDULE 1 Requirements for accreditation, designation, authorisation or licensing of tissue establishments as referred to in Regulation 5

A. ORGANISATION AND MANAGEMENT

1. A Responsible Person must be appointed having the qualifications and responsibilities provided for in Regulation 8 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ).

2. A tissue establishment must have an organisational structure and operational procedures appropriate to the activities for which accreditation / designation / authorisation / licensing is sought; there must be an organisational chart which clearly defines accountability and reporting relationships.

3. Every tissue establishment must have access to a nominated medical registered practitioner to advise on and oversee the establishment’s medical activities such as donor selection, review of clinical outcomes of applied tissues and cells or interaction as appropriate with clinical users.

4. There must be a documented quality management system applied to the activities for which accreditation / designation / authorisation or licensing is sought, in accordance with the standards laid down in these Regulations.

5. It must be ensured that the risks inherent in the use and handling of biological material are identified and minimised, consistent with maintaining adequate quality and safety for the intended purpose of the tissues and cells. The risks include those relating in particular to the procedures, environment, staff health status specific to the tissue establishment.

6. Agreements between tissue establishments and third parties must comply with Regulation 16 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ). Third party agreements must specify the terms of the relationship and responsibilities as well as the protocols to be followed to meet the required performance specification.

7. There must be a documented system in place, supervised by the responsible person, for ratifying that tissues and/or cells meet appropriate specifications for safety and quality for release and for their distribution.

8. In the event of termination of activities the agreements concluded and the procedures adopted in accordance with Regulation 12(9) of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ) shall include traceability data and material concerning the quality and safety of cells and tissues.

9. There must be a documented system in place that ensures the identification of every unit of tissue or cells at all stages of the activities for which accreditation/ designation / authorisation / licensing is sought.

B. PERSONNEL

1. The personnel in tissue establishments must be available in sufficient number and be qualified for the tasks they perform. The competency of the personnel must be evaluated at appropriate intervals specified in the quality system.

2. All personnel should have clear, documented and up-to-date job descriptions. Their tasks, responsibilities and accountability must be clearly documented and understood.

3. Personnel must be provided with initial / basic training, updated training as required when procedures change or scientific knowledge develops and adequate opportunities for relevant professional development. The training programme must ensure and document that each individual:

(a) has demonstrated competence in the performance of their designated tasks;

(b) has an adequate knowledge and understanding of the scientific / technical processes and principles relevant to their designated tasks;

(c) understands the organisational framework, quality system and health and safety rules of the establishment in which they work, and

(d) is adequately informed of the broader ethical, legal and regulatory context of their work.

C. EQUIPMENT AND MATERIALS

1. All equipment and material must be designed and maintained to suit its intended purpose and must minimise any hazard to recipients and/or staff.

2. All critical equipment and technical devices must be identified and validated, regularly inspected and preventively maintained in accordance with the manufacturers' instructions. Where equipment or materials affect critical processing or storage parameters (e.g. temperature, pressure, particle counts, microbial contamination levels), they must be identified and must be the subject of appropriate monitoring, alerts, alarms and corrective action, as required, to detect malfunctions and defects and to ensure that the critical parameters are maintained within acceptable limits at all times. All equipment with a critical measuring function must be calibrated against a traceable standard if available.

3. New and repaired equipment must be tested when installed and must be validated before use. Test results must be documented.

4. Maintenance, servicing, cleaning, disinfection and sanitation of all critical equipment must be performed regularly and recorded accordingly.

5. Procedures for the operation of each piece of critical equipment, detailing the action to be taken in the event of malfunctions or failure, must be available.

6. The procedures for the activities for which accreditation / designation / authorisation / licensing is sought, must detail the specifications for all critical materials and reagents. In particular, specifications for additives (e.g. solutions) and packaging materials must be defined. Critical reagents and materials must meet documented requirements and specifications and when applicable the requirements of Council Directive 93/42/EEC of 14 June 1993 concerning medical devices1 and Directive 98/79/EC of the European Parliament and of the Council of 27 October 1998 on in vitro diagnostic medical devices2 .

1 OJ L 169, 12.7.1993, p. 1. Directive as last amended by Regulation (EC) No 1882/2003 of the European Parliament and of the Council (OJ L 284, 31.10.2003, p. 1).

2 OJ L 331, 7.12.1998, p. 1. Directive as amended by Regulation (EC) No. 1882/2003.

D. FACILITIES / PREMISES

1. A tissue establishment must have suitable facilities to carry out the activities for which accreditation / designation / authorisation or licensing is sought, in accordance with the standards laid down in these Regulations.

2. When these activities include processing of tissues and cells while exposed to the environment, this must take place in an environment with specified air quality and cleanliness in order to minimise the risk of contamination, including cross-contamination between donations. The effectiveness of these measures must be validated and monitored.

3. Unless otherwise specified in paragraph 4, where tissues or cells are exposed to the environment during processing, without a subsequent microbial inactivation process, an air quality with particle counts and microbial colony counts equivalent to those of Grade A as defined in the current European Guide to Good Manufacturing Practice (GMP), Annex 1 and Directive 2003/94/EC is required with a background environment appropriate for the processing of the tissue / cell concerned but at least equivalent to GMP Grade D in terms of particles and microbial counts.

4. A less stringent environment than specified in paragraph 3 may be acceptable where:

(a) a validated microbial inactivation or validated terminal sterilisation process is applied;

(b) or, where it is demonstrated that exposure in a Grade A environment has a detrimental effect on the required properties of the tissue or cell concerned;

(c) or, where it is demonstrated that the mode and route of application of the tissue or cell to the recipient implies a significantly lower risk of transmitting bacterial or fungal infection to the recipient than with cell and issue transplantation;

(d) or, where it is not technically possible to carry out the required process in a Grade A environment (for example, due to requirements for specific equipment in the processing area that is not fully compatible with Grade A).

5. Where a less stringent environment than that specified in paragraph 3 operates pursuant to paragraphs 4(a), (b), (c) and (d), then that environment must be specified. It must be demonstrated and documented that the chosen environment achieves the quality and safety required, at least taking into account the intended purpose, mode of application and immune status of the recipient. Appropriate garments and equipment for personal protection and hygiene must be provided in each relevant department of the tissue establishment along with written hygiene and gowning instructions.

6. When the activities for which accreditation / designation / authorisation or licensing is sought involve storage of tissues and cells, the storage conditions necessary to maintain the required tissue and cell properties, including relevant parameters such as temperature, humidity or air quality must be defined.

7. Critical parameters (e.g. temperature, humidity, air quality) must be controlled, monitored, and recorded to demonstrate compliance with the specified storage conditions.

8. Storage facilities must be provided that clearly separate and distinguish tissues and cells prior to release / in quarantine from those that are released and from those that are rejected, in order to prevent mix-up and cross-contamination between them. Physically separate areas or storage devices or secured segregation within the device must be allocated in both quarantine and released storage locations for holding certain tissue and cells collected in compliance with special criteria.

9. The tissue establishment must have written policies and procedures for controlled access, cleaning and maintenance, waste disposal and for the re-provision of services in an emergency situation.

E. DOCUMENTATION AND RECORDS

1. There must be a system in place that results in clearly defined and effective documentation, correct records and registers and authorised Standard Operating Procedures (SOPs), for the activities for which accreditation / designation / authorisation / licensing is sought. Documents must be regularly reviewed and must conform to the standards laid down in these Regulations. The system must ensure that work performed is standardised, and that all steps are traceable; i.e. coding, donor eligibility, procurement, processing, preservation, storage, transport, distribution or disposal, including aspects relating to quality control and quality assurance.

2. For every critical activity, the materials, equipment and personnel involved must be identified and documented.

3. In the tissue establishments all changes to documents must be reviewed, dated, approved, documented and implemented promptly by authorised personnel.

4. A document control procedure must be established to provide for the history of document reviews and changes and to ensure that only current versions of documents are in use.

5. Records must be shown to be reliable and a true representation of the results.

6. Records must be legible and indelible and may be handwritten or transferred to another validated system, such as a computer or microfilm.

7. Without prejudice to Regulation 21 all records, including raw data, which are critical to the safety and quality of the tissues and cells shall be kept so as to ensure access to these data for at least 10 years after expiry date, clinical use or disposal.

8. Records must meet the confidentiality requirements laid down in Regulation 18 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ).

9. Access to registers and data must be restricted to persons authorised by the responsible person, and to the competent authority for the purpose of inspection and control measures.

F. QUALITY REVIEW

1. An audit system must be in place for the activities for which accreditation/ designation / authorisation / licensing is sought. Trained and competent persons must conduct the audit in an independent way, at least every two years, in order to verify compliance with the approved protocols and the regulatory requirements. Findings and corrective actions must be documented.

2. Deviations from the required standards of quality and safety must lead to documented investigations, which include a decision on possible corrective and preventive actions. The fate of non-conforming tissues and cells must be decided in accordance with written procedures supervised by the responsible person and recorded. All affected tissues and cells must be identified and accounted for.

3. Corrective actions must be documented, initiated and completed in a timely and effective manner. Preventive and corrective actions should be assessed for effectiveness after implementation.

4. The tissue establishment should have processes in place for review of the performance of the quality management system to ensure continuous and systematic improvement.

SCHEDULE 2 Requirements for the authorisation of tissue and cell preparation processes at the tissue establishments as referred to in Regulation 6

The Irish Medicines Board shall authorise each tissue and cell preparation process after evaluation of the donor selection criteria and procurement procedures, the protocols for each step of the process, the quality management criteria, and the final quantitative and qualitative criteria for cells and tissues. This evaluation must comply at least with the requirements set out in this Schedule.

A. RECEPTION AT THE TISSUE ESTABLISHMENT

Upon reception of procured tissues and cells at the tissue establishment, the tissues and cells must comply with the requirements defined in the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ).

B. PROCESSING

When the activities for which the accreditation / designation / authorisation / licensing is sought include processing of tissues and cells, the tissue establishment procedures must comply with the following criteria:

1. The critical processing procedures must be validated and must not render the tissues or cells clinically ineffective or harmful to the recipient. This validation may be based on studies performed by the establishment itself, or on data from published studies or, for well established processing procedures, by retrospective evaluation of the clinical results for tissues supplied by the establishment.

2. It has to be demonstrated that the validated process can be carried out consistently and effectively in the tissue establishment environment by the staff.

3. The procedures must be documented in SOPs which must conform to the validated method and to the standards laid down in these Regulations, accordingly with Schedule 1, Part E, paragraphs 1 to 4.

4. It must be ensured that all processes are conducted in accordance with the approved SOPs.

5. Where a microbial inactivation procedure is applied to the tissue or cells, it must be specified, documented, and validated.

6. Before implementing any significant change in processing, the modified process must be validated and documented.

7. The processing procedures must undergo regular critical evaluation to ensure that they continue to achieve the intended results.

8. Procedures for discarding tissue and cells must prevent the contamination of other donations and products, the processing environment or personnel. These procedures must comply with national regulations.

C. STORAGE AND RELEASE OF PRODUCTS

When the activities for which the accreditation / designation / authorisation / licensing is sought include storage and release of tissues and cells, the authorised tissue establishment procedures must comply with the following criteria:

1. Maximum storage time must be specified for each type of storage condition. The selected period must reflect among others possible deterioration of the required tissue and cell properties.

2. There must be a system of inventory hold for tissues and / or cells to ensure that they cannot be released until all requirements laid down in these Regulations have been satisfied. There must be a standard operating procedure that details the circumstances, responsibilities and procedures for the release of tissues and cells for distribution.

3. A system for identification of tissues and cells throughout any phase of processing in the tissue establishment must clearly distinguish released from non-released (quarantined) and discarded products.

4. Records must demonstrate that before tissues and cells are released all appropriate specifications are met, in particular all current declaration forms, relevant medical records, processing records and test results have been verified according to a written procedure by a person authorised for this task by the responsible person as specified in Regulation 8 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ). If a computer is used to release results from the laboratory, an audit trail should indicate who was responsible for their release.

5. A documented risk assessment approved by the responsible person as defined in Regulation 8 of the European Communities (Quality and Safety of Human Tissues and Cells) Regulations 2006 ( S.I. No. 158 of 2006 ) must be undertaken to determine the fate of all stored tissues and cells following the introduction of any new donor selection or testing criterion or any significantly modified processing step that enhances safety or quality.

D. DISTRIBUTION AND RECALL

When the activities for which the accreditation / designation / authorisation / licensing is sought include distribution of tissues and cells, the authorised tissue establishment procedures must comply with the following criteria:

1. Critical transport conditions, such as temperature and time limit must be defined to maintain the required tissue and cell properties.

2. The container / package must be secure and ensure that the tissue and cells are maintained in the specified conditions. All containers and packages need to be validated as fit for purpose.

3. Where distribution is carried out by a contracted third party, a documented agreement must be in place to ensure that the required conditions are maintained.

4. There must be personnel authorised within the tissue establishment to assess the need for recall and to initiate and coordinate the necessary actions.

5. An effective recall procedure must be in place, including a description of the responsibilities and actions to be taken. This must include notification to the competent authority.

6. Actions must be taken within pre-defined periods of time and must include tracing all relevant tissues and cells and, where applicable, must include trace-back. The purpose of the investigation is to identify any donor who might have contributed to causing the reaction in the recipient and to retrieve available tissues and cells from that donor, as well as to notify consignees and recipients of tissues and cells procured from the same donor in the event that they might have been put at risk.

7. Procedures must be in place for the handling of requests for tissues and cells. The rules for allocation of tissues and cells to certain patients or health care institutions must be documented and made available to these parties upon request.

8. A documented system must be in place for the handling of returned products including criteria for their acceptance into the inventory, if applicable.

E. FINAL LABELLING FOR DISTRIBUTION

1. The primary tissue / cell container must provide:

(a) type of tissues and cells, identification number or code of the tissue / cells, and lot or batch number where applicable;

(b) identification of the tissue establishment;

(c) expiry date;

(d) in the case of autologous donation, this has to be specified (for autologous use only) and the donor / recipient has to be identified;

(e) in the case of directed donations — the label must identify the intended recipient;

(f) when tissues and cells are known to be positive for a relevant infectious disease marker, it must be marked as: BIOLOGICAL HAZARD.

If any of the information under paragraphs (d) and (e) above cannot be included on the primary container label, it must be provided on a separate sheet accompanying the primary container. This sheet must be packaged with the primary container in a manner that ensures that they remain together.

2. The following information must be provided either on the label or in accompanying documentation:

(a) description (definition) and, if relevant, dimensions of the tissue or cell product;

(b) morphology and functional data where relevant;

(c) date of distribution of the tissue / cells;

(d) biological determinations carried out on the donor and results;

(e) storage recommendations;

(f) instructions for opening the container, package, and any required manipulation / reconstitution;

(g) expiry dates after opening / manipulation;

(h) instructions for reporting serious adverse reactions and / or events as set out in Regulations 7 to 15;

(i) presence of potential harmful residues (e.g. antibiotics, ethylene oxide etc).

F. EXTERNAL LABELLING OF THE SHIPPING CONTAINER

For transport, the primary container must be placed in a shipping container that must be labelled with at least the following information:

(a) identification of the originating tissue establishment, including an address and phone number;

(b) identification of the organisation responsible for human application of destination, including address and phone number;

(c) a statement that the package contains human tissue / cells and HANDLE WITH CARE;

(d) where living cells are required for the function of the graft, such as stem cells gametes and embryos, the following must be added:“DO NOT IRRADIATE”;

(e) recommended transport conditions (e.g. keep cool, in upright position, etc.);

(f) safety instructions / method of cooling (when applicable).

SCHEDULE 3 NOTIFICATION OF SERIOUS ADVERSE REACTIONS

PART A

Rapid Notification for suspected serious adverse reactions

Tissue establishment

Report identification

Reporting date (year / month / day)

Individual affected (recipient or donor)

Date and place of procurement or human application (year / month / day)

Unique donation identification number

Date of suspected serious adverse reaction (year / month / day)

Type of tissues and cells involved in the suspected serious adverse reaction

Type of suspected serious adverse reaction(s)

PART B

Conclusions of serious adverse reactions investigation

Tissue establishment

Report identification

Confirmation date (year / month / day)

Date of serious adverse reaction (year / month / day)

Unique donation identification number

Confirmation of serious adverse reaction (Yes / No)

Change of type of serious adverse reaction (Yes / No)If Yes, Specify

Clinicial outcome (if known)— Complete recovery— Minor sequelae— Serious sequelae— Death

Outcome of the investigation and final conclusions

Recommendations for preventive and corrective actions

SCHEDULE 4 NOTIFICATION OF SERIOUS ADVERSE EVENTS

PART A

Rapid notification for suspected serious adverse events

Tissue establishment

Report identification

Reporting date (year / month / day)

Date of serious adverse event (year / month / day)

Specification

Serious adverse event, which may affect quality and safety of tissues and cells due to a deviation in:

Tissues and cells defect

Equipment Failure

Human Error

Other (specify)

Procurement

Testing

Transport

Processing

Storage

Distribution

Materials

Others (specify)

PART B

Conclusions of serious adverse events investigation

Tissue establishment

Report identification

Confirmation date (year / month / day)

Date of serious adverse event (year / month / day)

Root cause analysis (details)

Corrective measures taken (details)

SCHEDULE 5 ANNUAL NOTIFICATION FORMAT

PART A

Annual notification format for serious adverse reactions

Reporting Country

Reporting Date 1 January — 31 December (year)

Number of serious adverse reaction(s) per type of tissue and cell (or product in contact with tissues and cells)

Type of tissue / cell (or product in contact with tissues and cells)

Number of serious adverse reaction(s)

Total number of tissues / cells of this type distributed (if available)

1

2

3

4

...

Total

Total number of tissues / cells distributed (including type of tissue and cell for which no serious adverse reactions were reported):

Number of recipients affected (total number of recipients):

Nature of the serious adverse reactions reported

Total number of serious adverse reaction(s):

Transmitted bacterial infection

Transmitted viral infection

HBV

HCV

HIV-1/2

Other (specify)

Transmitted parasitical infection

Malaria

Other (specify)

Transmitted malignant diseases

Other disease transmissions

Other serious reactions (specify)

PART B

Annual notification format for serious adverse events

Reporting country

Reporting date 1 January — 31 December (year)

Total number of tissues and cells processed

Specification

Total number of serious adverse events, which may have affected quality and safety of tissues and cells due to a deviation in:

Tissues and cells defect (specify)

Equipment Failure (specify)

Human Error (specify)

Other (specify)

Procurement

Testing

Transport

Processing

Storage

Distribution

Materials

Others (specify)

SCHEDULE 6 INFORMATION ON THE MINIMUM DONOR / RECIPIENT DATA SET TO BE KEPT AS REQUIRED IN REGULATION 21.

A. BY TISSUE ESTABLISHMENTS

Donor identification

Donation identification that will include at least:

—Identification of the procurement organisation or Tissue establishment

—Unique Donation ID number

—Date of procurement

—Place of procurement

—Type of donation (e.g. single v multi-tissue; autologous v allogenic; living v deceased)

Product identification that will include at least:

—Identification of the tissue establishment

—Type of tissue and cell / product (basic nomenclature)

—Pool number (if applicable)

—Split number (if applicable)

—Expiry date

—Tissue / cell status (i.e. quarantined, suitable for use etc.)

—Description and origin of the products, processing steps applied, materials and additives coming into contact with tissues and cells and having an effect on their quality and / or safety.

—Identification of the facility issuing the final label

Human application identification that will include at least:

—Date of distribution / disposal

—Identification of the clinician or end user / facility

B. BY ORGANISATIONS RESPONSIBLE FOR HUMAN APPLICATION

(a) Identification of the supplier tissue establishment

(b) Identification of the clinician or end user / facility

(c) Type of tissues and cells

(d) Product identification

(e) Identification of the recipient

(f) Date of application

SCHEDULE 7

INFORMATION CONTAINED IN THE EUROPEAN CODING SYSTEM

(a) Donation identification:

—Unique ID number

—Identification of the tissue establishment

(b) Product identification:

—Product code (basic nomenclature)

—Split number (if applicable)

—Expiry date

/images/ls

GIVEN under my Official Seal,

31 August 2007

MARY HARNEY

Minister for Health and Children.

EXPLANATORY NOTE

(This note is not part of the Instrument and does not purport to be a legal interpretation)

These Regulations give effect to Commission Directive 2006/86/EC of 24th October 2006. The Regulations may be cited as the European Communities (Human Tissues and Cells Traceability Requirements, Notification of Serious Adverse Reactions and Events and Certain Technical Requirements) Regulations 2007.

The Regulations set down standards for the quality and safety of human tissues and cells during coding, processing, preservation, storage and distribution to the healthcare establishment where they will be applied to the human body. The Regulations do not extend to the human application of these tissues and cells (such as implantation surgery, perfusion, insemination or transfer of embryos). The provisions in the Regulations concerning traceability and the reporting of serious adverse reactions and events also apply to the donation, procurement and testing of human tissues and cells.

1 OJ L 169, 12.7.1993, p. 1. Directive as last amended by Regulation (EC) No 1882/2003 of the European Parliament and of the Council (OJ L 284, 31.10.2003, p. 1).

2 OJ L 331, 7.12.1998, p. 1. Directive as amended by Regulation (EC) No. 1882/2003.