Fla. Admin. Code R. 59A-1.005
(1) Organizational Requirements.
(a) Institutional Identity.
1. The purpose of the OPO, eye bank, or tissue bank shall be clearly established and documented.
2. Documentation of institutional identity shall include whether the OPO, eye bank, or tissue bank is independent or part of another institution.
3.The OPO, eye bank, or tissue bank shall have a functional identity with a professional staff and a commitment to maintain and preserve records and operating procedures for future reference and historical continuity.
4. Policies and procedures shall be maintained for personnel and other activities.
(c) OPO, Eye Bank, or Tissue Bank Director. Each OPO, eye bank, or tissue bank shall have a director qualified by training and experience for the scope of activities being pursued.
1. The director shall be responsible for:
a. Development, implementation and maintenance of all procedures and policies,
b. All administrative operations including compliance with these standards,
c. The daily operation of the OPO, eye bank, or tissue bank,
d. Specifying technically acceptable means for retrieving, processing, quality control, storage, and distribution, as applies to the scope of activities being pursued,
e. Providing all staff members with adequate information to perform their duties safely and competently,
f. Appointing technical staff with capabilities and training appropriate to their function and ensuring that competency is maintained by participation in training courses and technical meetings or other educational programs. Such training shall be recorded in the employee’s personnel file,
g. Establishing quality control and quality assurance programs. These programs shall include ongoing monitoring and evaluation of activities, identification of problems, and development of plans for corrective action. These procedures and records shall be reviewed at least annually; and,
h. Maintaining a working relationship with medical examiner offices in the OPO, eye bank, or tissue bank’s service area.
2. If the director appointed does not have medical licensure, the OPO, eye bank, or tissue bank shall have at least one physician, employed or under contract, to ensure compliance with all medical aspects and with all requirements for specialist knowledge of the particular organs and tissues processed.
3. The director is authorized to delegate his or her responsibilities to trained and competent staff. If responsibilities are delegated, the director remains responsible for ensuring that all duties are properly performed.
(e) Policies and Procedures. Each OPO, eye bank or tissue bank shall maintain detailed and unambiguous policies and procedures which detail all aspects of retrieval, processing, testing, storage, and distribution practices; as applicable.
1. Each of these procedures shall be reviewed and affirmed in writing annually by the director or designee.
2. Modifications of standard procedures and development of new procedures shall be approved by the director or designee prior to implementation.
3. Obsolete revised procedures shall be retained separately to maintain a historical sequence.
4. Copies of policies and procedures shall be available to the staff at all times. Technical staff shall be required to state in writing that they have read and understand the policies and procedures applicable to his or her specific responsibilities.
5. Copies of policies and procedures shall be available to surveyors for inspection upon request.
(g) Records.
1. Donor and recipient records shall be accurate, complete, and confidential as required by Section 456.057, F.S. Donor record confidentiality shall not preclude access by surveyors for the Agency when conducting an inspection or investigation pursuant to paragraphs 59A-1.009(1)(a), (b), (c), F.A.C., and the medical examiner for cases which fall within the medical examiner’s jurisdiction, as established under Section 406.05, F.S. Donor medical records and final results of all laboratory tests shall be reviewed and affirmed by the medical director, designees, or medical contractee to ensure suitability of the donated organ(s) or tissue(s) for the intended application.
2. Documentation shall be concurrent with the performance of each activity in the retrieval, preparation, testing, storage, and distribution of organs and tissues in such a manner that all activities can be clearly traced. All records shall be legible and indelible and shall identify the person performing the procedures/tasks. The record shall include dates of entries and test results. The expiration period assigned to specific categories of processed tissues is to be recorded in the policies and procedures.
3. Records shall be as detailed as necessary for a clear understanding of each activity and shall be available for inspection by surveyors when conducting an inspection or investigation pursuant to paragraphs 59A-1.009(1)(a), (b), (c), F.A.C., upon request and within the bounds of medical-legal confidentiality, pursuant to Section 456.057, F.S.
4. Each organ donor, tissue and any components derived from tissue shall be assigned, in addition to generic designation, a unique identification number to identify the material from retrieval through distribution and utilization.
5. Records shall identify the donor, document the pathological and microbiological evaluation of the donor, verify the conditions under which the organ or tissue is retrieved, processed and stored, if applicable, and indicate disposition of the transplanted organ or tissue. Maintenance of these records shall be the responsibility of the director or designee. All records concerning donor history and processing information shall be made available to the transplant surgeon upon request, except those infringing upon donor confidentiality.
6. All records and communication between the OPO, eye bank or tissue bank and its donors, persons identified by Section 765.512(3), F.S., and patient recipients shall be regarded as confidential and privileged. Surveyors shall have access to records and communication at the time of the inspection as specified in Rule 59A-1.009, F.A.C.
7. Maintenance and certification records, if applicable, on facilities, instruments, and equipment, including their monitors, shall be maintained. These records shall indicate dates of inspection, name of facility, and performance evaluations. Each OPO, eye bank or tissue bank shall include in its procedures manual, the monitoring, inspection and cleaning procedures and schedules for each piece of equipment. Documented cleaning schedules for laboratory equipment shall be maintained. Records of function checks requiring interpretation of findings must include the interpretation. Records must include:
a. Temperature of incubators when in use,
b. Spore lot number and expiration date used for autoclave function check; and,
c. Control and test results.
8. Each OPO, eye bank, or tissue bank shall document all aspects of its quality assurance program.
9. An adverse reactions file shall be maintained pursuant to Rule 59A-1.011, F.A.C.
10. All of these records shall be retained for seven years for OPOs and ten years for tissue banks and eye banks and be available for Agency inspection.
(2) Safety and environmental control. Written procedures for the operation shall be established and approved by the director. Instructions for action in case of emergency or exposure to communicable disease, chemical and biological hazard precautions shall be included.
(c) All organs or tissues found positive for human immunodeficiency virus shall be rendered noncommunicable or shall be destroyed, unless specifically labeled to identify the human immunodeficiency virus and:
1. Is used for research purposes, or
2. Is used to save the life of another and is transferred with the recipient’s informed consent.
(3) Facilities and equipment.
(4) Ethical Standards.
(6) Acquisition of Organs and Tissues.
(a) General.
1. OPO, eye bank, or tissue bank personnel shall have written procedures to ensure that consent for donation is obtained in compliance with Chapter 765, F.S.
2. OPO, eye bank, or tissue bank personnel shall be trained regarding obtaining and documenting consent for donation.
3. Consent shall be obtained from the donor, next of kin, or other designated legal entity in order of priority and availability according to Section 765.512, F.S.
4. A copy of the signed consent form shall remain a part of the patient’s hospital medical record if signed at the hospital.
5. The original signed consent form or record of telephone consent shall be retained in the OPO, eye bank, or tissue bank’s donor record.
(b) Informed Consent.
1. Permission to procure organs and tissues from donors which is obtained by informed consent shall be as defined in Rule 59A-1.003, F.A.C., and shall be documented in writing. The consent form shall include the organs and tissues for which permission is granted (e.g., bone from the upper or lower extremities or bone from below the waist). Information provided shall be written or spoken in language understandable to the donor or the donor’s next of kin.
2. Permission to retrieve organs and tissues from non-living donors shall be sought from next of kin in order of legal precedence as required by Section 765.512, F.S.
3. In any cases falling under the provisions of Chapters 406 and 765, F.S., the permission of the medical examiner or appropriate designee shall be obtained prior to the procurement of any organ(s) and tissue(s). The donor records shall indicate the name of the contact person in the medical examiner’s office, date and time of contact, and limitations, if any, imposed by those giving permission (e.g., DO NOT TOUCH CHEST).
(10) Donor Selection. Each OPO,tissue bank or eye bank engaged in the retrieval or recovery of organs or tisssues, shall have written procedures regarding donor selection.
(16) Data Collection. Each OPO, tissue bank, and eye bank shall collect, maintain, and report the following data annually to the Agency:
(20) Each OPO shall employ or have under contract a physician medical director who:
(22) Financial Policies and Procedures.
(a) The OPO shall have accounting and other fiscal procedures necessary to ensure the fiscal stability of the organization, including procedures to obtain payment for kidneys and non-renal organs provided to transplant centers.
1. There shall be an annual budget approved by the board of directors or advisory board.
2. Unless otherwise provided by law, there shall be an annual audit conducted by an independent public accountant. In the case of hospital OPOs, the hospital must undergo an annual financial audit.
3. There shall be adequately trained staff or qualified contractors to ensure the establishment and maintenance of internal controls and general accounting functions. The general accounting functions shall include management of accounts receivable, management of accounts payable and other disbursements, and the handling of cash. An OPO shall maintain the ability to generate periodic statements of the status of the assets, liabilities and fund balance, and statements of its periodic revenues and expenses. Hospital OPOs shall be exempt from this requirement to the extent that these functions are performed by hospital staff.
(e) The accounting records of the OPO shall permit the expensing of indirect costs, (e.g., office rent, utilities, administrative salaries and salary related costs) so that they may be allocated in compliance with Medicare rules and guidelines.
1. The OPO’s costs shall be charged as expenses and allocated in accordance with the appropriate guidance provided by the Medicare program or by the appropriate hospital authority for hospital OPOs and by established agreements with other agencies, companies, providers or vendors.
2. The costs paid by the OPO for services used in the procurement of organs (for example, surgeon’s fees, donor evaluation fees, laboratory, transportation, etc.) shall be based on reasonable and customary fees within the service area as determined by the OPO. The OPO may refer to limitations on the reimbursement of such costs as specified by the Medicare program.
(24) An OPO’s policies and procedures for the evaluation and management of a potential organ donor shall be in writing. Evaluation and management of donors is mandatory for organs which may be allocated to and received by the Organ Procurement and Transplantation Network (OPTN)-approved transplant programs to ensure that all organ donors meet the minimum standards and the requirements established by the OPTN policies, effective April 6, 2017, incorporated herein by reference and available at HYPERLINK "http://www.flrules.org/Gateway/reference.asp?No=Ref-09009" http://www.flrules.org/Gateway/reference.asp?No=Ref-09009.
(c) The evaluation of the donor shall include:
1. An attempt to acquire a social history which may be obtained from individuals not limited to the person giving consent;
2. A physical examination of the donor;
3. Documentation of the donor’s ABO group, donor’s weight and height;
4. A review of the donor’s current inpatient medical record; and,
5. Documentation of significant events in the donor’s clinical course.
(f) The OPO shall evaluate the infectious disease status of the potential donor. All serological testing shall be noted to be either pre- or post-transfusion. Such evaluation shall include:
1. Hepatitis testing according to OPTN policies and procedures;
2. Appropriate FDA-licensed HIV-1/HIV-2 screens;
3. Serologic test for syphilis (STS);
4. Blood and urine cultures;
5. Cytomegalovirus (CMV); and,
6. Complete blood count (CBC).
(25) Allocation of Donated Organs.
(26) Procurement Procedures. The OPO shall have written policies and procedures to facilitate and coordinate the recovery of donated organs by trained and qualified personnel.
(c) The OPO is responsible for coordinating anesthesia support for the organ procurement process. The OPO shall provide protocols to the anesthesia support service for the intra-operative procedure which address:
1. Maintaining an adequate blood pressure, fluid volume, organ perfusion and function;
2. Adequate oxygenation and oxygen transport to the organs being procured;
3. Replacement of excessive volume loss; and,
4. Administration of required and desirable medications to facilitate organ procurement and function.
(f) In all organ donors, the OPO is responsible for distributing the following documentation to each transplant center receiving an organ from an individual donor:
(VII) OPO identification number.
c. The OPO shall document the following information for purposes of follow-up:
(VI) Copy of declaration of death note.
d. Documentation of donor history. The OPO shall obtain a medical and social history of each potential donor in an attempt to determine whether the potential donor is at increased risk as described in “PHS Guideline for Reducing Human Immunodeficiency Virus, Hepatitis B Virus, and Hepatitis C Virus Transmission Through Organ Transplantation”, as published in Public Health Reports/July-August 2013/Volume 128, incorporated herein by reference and available online at: HYPERLINK "http://www.flrules.org/Gateway/reference.asp?No=Ref-09010" http://www.flrules.org/Gateway/reference.asp?No=Ref-09010. That history shall be communicated to the physician responsible for the care of the recipient.
e. The documented past medical history shall, when available, include significant episodes of the following:
(V) History of disease specific to transplantable organs and treatment of same.
f. The current hospital history is the most vital and shall include:
(IV) Record of blood transfusions – type and amount.
g. Documentation of donor hemodynamics.
h. Documentation of blood pressures shall include:
(VI) Swan Ganz and central venous pressure readings and which shall be correlated with blood pressure, when available.
i. Transfused donor. All potential donors are to be tested for HIV-1/HIV-2 antibodies in accordance with the following rule administered by the Department of Health: Rule 64D-2.005, F.A.C. If the donor’s pre-transfusion test is antibody negative and subsequent transfusions are pre-tested, retesting for HIV-1/HIV-2 antibodies is not necessary. If no pre-transfusion blood sample is available, the donor institution must provide, along with the screening test results, a complete history of all transfusions received by the donor during the ten (10) day period immediately prior to removal of the organs. Except as provided in Section 59A-1.005(2)(c), F.A.C., organs from donors with repeatedly reactive screening tests for HIV-1/HIV-2 antibodies are not suitable for transplantation unless subsequent confirmation testing unequivocally indicates that the original test result was unconfirmed. If additional tests related to HIV-1/HIV-2 antibodies are performed, the results of all tests must be communicated immediately to the recipient’s institution.
1. Verification of donor ABO type;
2. Copy of death determination from the donor’s medical record;
3. Copy of consent for organ procurement from the donor’s medical record; and,
4. Copy of the following OPO donor information:
a. The OPO shall be responsible for documentation of demographic information relative to the donor so that pertinent information is available for centers considering organs for transplant. The OPO shall document information that will enable follow-up with the next of kin and donor hospital personnel.
b. The OPO shall have a standardized method of recording the following information on each donor:
(27) Documentation of Organ-Specific Test Results. Requirements for organ specific testing shall be in writing. The OPO shall provide the transplanting physician with certain test results for the evaluation of organ function. These results shall be documented in a standardized manner.
(a) The OPO shall, at minimum, document the following available lab results for ALL donors:
1. CBC;
2. Electrolytes;
3. ABO typing;
4. Blood and urine cultures;
5. Serological testing in accordance with OPTN policies, effective April 6, 2017;
6. Appropriate FDA-licensed HIV-1/HIV-2 screens. If blood products have been given, a pre-transfused sample shall be obtained. If unavailable, explanation shall be documented in the donor’s medical record;
7. Cultures, including blood, and urine, which allow for interpretation of laboratory results. Each OPO must define procedures for the type, source and indication for obtaining these cultures;
8. CMV antibody.
(b) Kidney evaluation:
1. Urinalysis;
2. Creatinine; and,
3. Blood urea nitrogen (BUN).
(c) Liver evaluation:
1. Liver enzymes;
2. Total bilirubin;
3. Direct bilirubin; and,
4. Prothrombin time/partial thromboplastin time (PT/PTT).
(d) Heart evaluation:
1. 12 lead EKG;
2. Cardiology consult;
3. Chest X-ray;
4. Blood gases;
5. Echocardiogram or cardiac cath (optional); and,
6. Creatine phosphokinase including MB fraction.
(e) Pancreas evaluation:
1. Serum amylase;
2. Serum lipase; and,
3. Glucose.
(f) Lung evaluation:
1. Blood gases;
2. Chest X-ray; and,
3. Sputum gram stain and culture.
(28) The OPO shall document detailed information on volume intake and urine output in order to assess and maintain donor stability.
(29) Documentation of Organ Retrieval Procedure.
(b) Documentation shall include:
1. Blood pressures, urine output, and fluids administered;
2. Medications administered;
3. Blood products administered;
4. Type and amount of perfusion solution and flush characteristics;
5. Type of storage solution;
6. Type of procurement procedure (i.e., enbloc, in-situ perfusion);
7. Aortic cross-clamp time and date;
8. Description of typing material available;
9. Warm ischemia time;
10. Anatomical description:
a. Kidneys – include number of vessels and approximate length and diameter of each;
b. Extra renal – include description and any injuries or abnormalities; and,
11. Organs recovered and not utilized. If the organs are not used for transplantation or research, a written note regarding disposition shall be documented in the OPO’s donor records.
(30) Documentation of Organ Recipient Information.
(b) The following information shall be documented on each recipient:
1. Name;
2. A recipient identification number;
3. Recipient center; and,
4. Age, sex, and race.
(33) Tissue Bank Organizational Staff Requirements.
(34) Tissue Donor Selection.
(d) Tissues with evidence of infectious diseases are conditions which shall preclude distribution for transplantation. The following is a list of examples of commonly encountered conditions which preclude donation of tissues:
1. Infectious diseases such as:
a. Septicemia (demonstrable) at time of death;
b. Systemic mycoses;
c. Meningitis or encephalitis;
d. Active systemic viral disease or past history of chronic viral disease;
e. Active tuberculosis;
f. Active or chronic hepatitis of viral or unknown etiology; and,
g. Active syphilis or anatomically demonstrable syphilitic lesions.
2. Bacterial infections such as:
a. Pyelonephritis associated with sepsis or systemic infection;
b. Gross Peritonitis or abdominal abcess (not only microscopic inflammation);
c. Pneumonia associated with sepsis or systemic infection;
d. Bacterial endocarditis;
e. Osteomyelitis; and,
f. Other potentially transmittable bacterial diseases.
3. Malignancies. Individuals with malignancies arising anywhere in the body shall be excluded from the donor pool. Any exceptions shall be approved by the medical director.
4. Collagen and immune complex diseases determined by the Medical Director to impact the specific tissues to be distributed such as:
a. Rheumatoid arthritis;
b. Systemic lupus erythematosus;
c. Polyarteritis nodsa;
d. Sarcoidosis;
e. Myasthenia gravis; and,
f. Acute rheumatic fever.
5. Transfused Donor. Tissues from a donor who has been transfused shall comply with the FDA Guidance for Industry “Eligibility Determination for Donors of Human Cells, Tissues and Cellular and Tissue-based Products (HCT/Ps),” August 2007, incorporated herein by reference and available at HYPERLINK "http://www.flrules.org/Gateway/reference.asp?No=Ref-09016" http://www.flrules.org/Gateway/reference.asp?No=Ref-09016.
6. Recipients of organ transplants. Recipients of organ transplants shall not be automatically eliminated because of the transplant.
7. Other. Toxic exposure sufficient to affect tissue procured and an unknown but suspicious medical history shall constitute a reason for rejecting a donor.
(35) Required studies of the tissue donor in addition to FDA requirements specified in Rule 59A-1.005, F.A.C.
(a) Serologies:
1. HBcAb;
2. FDA-licensed HTLV test for viable, leukocyte rich cells or tissues only;
3. Serologic test for syphilis (STS) – confirmed. Tissues from donors with positive (confirmed) tests shall not be used for transplantation; and,
4. Rh determination shall be provided cautioning about the possibility of sensitization.
(37) Tissue Bank Records.
(41) Tissue Retrieval and Processing Procedures.
(b) Tissue banks employing ethylene oxide (ETO) for sterilization of tissues, chambers of freeze-dryers, instruments or equipment must monitor occupational exposure to ethylene oxide. Semi-annual reports of ETO monitoring must be kept for 30 years. Specifically the following requirements must be met and documented:
1. Air change rate – minimum rate for rooms where ethylene oxide is used is 10 air changes per hour.
2. Review of gas circuits. The following must be checked for leaks:
a. Gas tank valves;
b. Gas tank manifolds including filter cartridges;
c. Sterilizer and other equipment door seals;
d. Pressure relief valves;
e. Gas-steam mixing chambers;
f. All elbows, compression fittings, gauges, valves, etc. along the gas circuit;
g. Gas inlet into chamber; and,
h. Chamber air intake filter.
3. ETO alarm must be installed near equipment where ETO spill may be possible.
4. Automatic aeration after sterilization without having to open sterilizer door must be provided.
5. Periodic personnel exposure monitoring must be conducted.
6. A canister type respirator (NIOSH approved and rated for 5,000 ppm ETO) and gloves must be kept in the gas sterilization area in case of an emergency.
7. Safety data sheets must be kept in the tissue bank and the location of these sheets and content must be known to the employee.
8. An emergency evacuation plan must be posted for all employees to see.
9. Personnel must be trained regarding the safe use of ETO and records retained in the file.
10. All exhaust systems must be non-circulating.
(42) Tissue Labeling.
(a) Container label. Containers shall be labeled so as to identify the following:
1. Name of the product;
2. Name and address of the tissue bank;
3. Tissue identification number; and,
4. Expiration date, if applicable.
(b) Shipping label. Packages shall be labeled so as to identify the following:
1. Identification of human tissue;
2. Name and address of tissue bank;
3. Name of facility to which tissue is being shipped;
4. Recommended storage temperature; and,
5. Special instructions indicated by the particular product, e.g., DO NOT FREEZE.
(43) Tissue Shipping.
(c) All tissues shall be accompanied by a package insert which contains instructions for proper storage and reconstituting when appropriate. Specific instructions shall be enclosed with tissues requiring special handling. Such instructions shall include:
1. Presence of known sensitizing substances;
2. Type of antibiotics present, if applicable;
3. A statement that it has undergone infectious disease testing;
4. Sterilization procedure, if utilized; and,
5. Concentration of preservative(s) and/or cryoprotectant(s) in final package solution, if applicable.
(44) Tissue Tracking.
(47) Eye Bank Organization Staff Requirements.
(b) Eye Bank technical personnel.
1. A supervisory eye bank technician shall be the individual responsible for the daily operation of the eye bank laboratory. The supervisory eye bank technician shall ensure compliance with these standards for the eye bank laboratory. Each eye bank processing laboratory must have at least one certified technician in a supervisory role.
2. An eye bank technician shall be trained in acquisition, evaluation, processing, storage and distribution of eye tissue for transplantation.
3. A procurement technician shall be proficient in screening and retrieval of the eye tissue.
(48) Training, Certification, and Continuing Education.
(49) Performance Standards.
(50) Eye Donor Selection.
(a) Eye tissue from donors with the following shall not be used for penetrating keratoplasty, lamellar keratoplasty, patch grafts, epikeratoplasty or any other type of surgery:
1. Death of unknown cause;
2. Death from central nervous system diseases of unknown etiology;
3. Creutzfeldt-Jakob disease;
4. Subacute sclerosing panencephalitis;
5. Progressive multifocal leukoencephalopathy;
6. Congenital rubella;
7. Reye’s syndrome;
8. Active viral encephalitis of unknown origin;
9. Active septicemia (bacteremia, fungemia, viremia);
10. Active bacterial or fungal endocarditis;
11. Active viral hepatitis;
12. Rabies;
13. Intrinsic eye disease:
a. Retinoblastoma;
b. Malignant tumors of the anterior ocular segment;
c. Active ocular or intraocular inflammation: conjunctivitis, scleritis, iritis, uveitis, vitreitis, choroiditis, retinitis;
d. Congenital or acquired disorders of the eye which would preclude a successful outcome for the intended use, e.g., a central donor corneal scar for an intended penetrating keratoplasty, keratoconus, and keratoglobus; and,
e. Pterygia or other superficial disorders of the conjunctiva or corneal surface involving the central optical area of the corneal button.
f. Exceptions are that tissue with local eye disease affecting the corneal endothelium may be used for epikeratoplasty, patch grafts, and scleral transplant surgery, and tissue with local eye disease affecting the corneal endothelium or previous ocular surgery that does not compromise the corneal stroma may be used for lamellar keratoplasty or patch grafts.
14. Prior intraocular or anterior segment surgery:
a. Refractive corneal procedures, e.g., radial keratotomy, lamellar inserts, etc.;
b. Laser photoablation surgery;
c. If corneas are used from donors who have had prior anterior segment surgery (e.g., cataract, intraocular lens, glaucoma filtration), the corneas shall be screened by specular microscopy and meet the eye bank’s endothelial standards as determined by the medical director; and,
d. Laser surgical procedures such as argon laser trabeculoplasty, retinal and panretinal photocoagulation do not necessarily preclude use for penetrating keratoplasty but shall be cleared by the medical director.
15. Active leukemia;
16. Active disseminated lymphomas;
17. Hepatitis B surface antigen positive donors;
18. Recipients of human pituitary-derived growth hormone (pit-hGH) during the years from 1963-1985;
19. HIV seropositive donors;
20. Acquired immunodeficiency syndrome (AIDS);
21. Children (under 13 years old) and infants of mothers with AIDS or at high risk of HIV infection;
22. High risk for HIV infection based on the FDA Guidance Concerning Application of Testing and High Risk Criteria for HIV and Hepatitis for Banked Human Tissue, incorporated herein by reference.
23. HTLV infection except in the case of viable, leukocyte cell or tissue donors;
24. Active syphilis; and,
25. Hepatitis C seropositive donors.
(51) Eye Donor Testing.
(a) Microbiologic Culturing. Culturing of eye bank donor eyes is recommended. However, the responsibility for determining the need for culturing shall reside with the transplanting surgeon.
1. Presurgical Cultures. Eye banks may elect to perform corneal-scleral rim cultures at the time of corneal preservation in tissue culture medium. Positive culture reports shall be reported to the receiving surgeon or recipient eye bank.
2. Surgical Culturing. Each eye bank shall recommend culturing of the corneal-scleral rim for corneal transplantation, or a piece of sclera for scleral implantation at the time of surgery. Positive culture results in cases of postoperative infection shall be reported to the eye bank that processed the tissue.
(b) HIV Screening.
1. Each eye bank shall have an HIV screening program using FDA-approved tests, pursuant to Rule 64D-2.005, F.A.C., for all donors of surgically designated tissue. A negative screening test shall be documented prior to release of tissue for transplantation.
2. Eye tissue from a donor who has been transfused shall comply with the FDA Guidance for Industry “Eligibility Determination for Donors of Human Cells, Tissues and Cellular and Tissue-based Products (HCT/Ps)”, August 2007.
(52) Documentation of Eye Donor Information.
(c) Minimum information to be retained. A report form for retaining donor and recipient information shall be established for permanent record and shall be readily accessible for inspection by authorized individuals, including surveyors for the Agency. The record shall include the following minimum information:
1. Eye bank identification number unique to each tissue graft;
2. Name of eye bank;
3. Location of eye bank;
4. Phone number;
5. Type of preservation;
6. Age of donor;
7. Cause of death;
8. Death date and time;
9. Enucleation or in-situ retrieval date and time;
10. Preservation date and time;
11. Slit lamp report;
12. Specular microscopy, if performed;
13. Name of enucleator/evaluator/technician;
14. Name of surgeon receiving tissue;
15. Recipient identification;
16. Utilization of non-transplantable tissue;
17. All serological or microbiological tests performed; and,
18. Adverse reactions, when reported.
(53) Eye Bank Facilities and Equipment.
(55) Eye Bank Retrieval and Processing Procedures.
(f) Scleral Preservation.
1. If the eye bank preserves scleral tissue, the selected preservation method shall be documented in the eye bank’s own procedures manual.
2. An expiration date for use of tissue shall be indicated based on the container capability and factors documented or recommended by the eye bank.
(56) Eye Tissue Evaluation. The transplanting surgeon has ultimate responsibility for determining the suitability of the tissue for transplantation.
(57) Eye Tissue Storage.
(58) Corneal or Scleral Tissue Labeling.
(b) Each corneal or scleral tissue shall be clearly and indelibly labeled to include, at least, the following:
1. Name of source eye bank;
2. Tissue identification number;
3. Type of tissue;
4. Date and time of donor’s death;
5. Date and time of corneal-scleral preservation;
6. Expiration date for scleral tissue; and,
7. A statement shall accompany the tissue stating that:
a. The tissue is intended for single patient application only and that it is not to be considered sterile and that the FDA therefore recommends culturing or reculturing; and,
b. The tissue has undergone infectious disease testing.
(59) Eye Tissue Packaging.
(c) Package insert. A package insert form shall accompany the tissue for transplantation. This form shall include the following:
1. Recommended storage temperature with specific emphasis on Do Not Freeze;
2. That the surgeon shall check for integrity of the seal and immediately report to the eye bank any evidence of possible tampering;
3. That color change per the manufacturer’s guidelines may indicate a change in pH, in which case the tissue shall not be used and a report made immediately to the eye bank;
4. Whether pre-surgical microbiological cultures were performed by the eye bank, including the advisement that culture of the donor rim and sclera shall be performed at the time of surgery; and,
5. The form shall also advise the receiving surgeon that the tissues are delivered with no warranty as to merchantability or fitness for a particular purpose, and that the receiving surgeon is ultimately responsible for judging if the tissue is suitable for use.
Rulemaking Authority 765.541(2) FS. Law Implemented, 765.541, 765.542, 765.543, 765.545 FS. History–New 11-26-92, Amended 8-20-96, 1-17-18.