| Obligatory | 1. Eyes:
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| Discretionary | 1. Eyes:
d) If the potential donor has been cured of a carcinoma in situ (CIS) and discharged from follow-up, accept. Donors who have been returned to routine screening following treatment for cervical CIS can be accepted. If the potential donor has had a diagnosis of melanoma in situ (including Lentigo Maligna), refer to Designated Clinical Support Officer to confirm they have not had an invasive melanoma (eg Lentigo Maligna Melanoma). e) Potential donors with a high risk of cancer due to family history or following genetic tests, even if had or having prophylactic surgery or on prophylactic medication (e.g. Tamoxifen), or on routine follow up, accept. f) Primary turmours of the central nervous system with a low risk of distant metastasis are acceptable for all tissues except for sclera: See additional information section for information.
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| See if Relevant | Basal Cell Carcinoma |
| Additional Information | Many malignancies spread through the blood stream and by invading surrounding tissues. Viruses that can be spread by blood and tissue donation can also cause some malignancies. For these reasons it is considered safer not to accept blood from people who have had a malignancy. Basal cell carcinoma (rodent ulcer) does not spread through the blood, therefore people who have had successful treatment may donate. The term carcinoma in situ (CIS) refers to a group of abnormal cells which have not invaded deeper tissue or spread to another part of the body. Donors who have been cured and discharged from follow up may donate. For cervical CIS, donors can be accepted if treatment is complete and any follow up smear, if performed, did not show abnormal cells. Regular screening smears are not defined as follow up. Premalignant conditions are very common, particularly in older donors. Regular monitoring should prevent donors with invasive malignancy from being accepted. However donors with a haematological clonal pre-malignant condition e.g. smouldering myeloma should not be accepted for tissue donation. Monoclonal gammopathy of uncertain significance (MGUS) with IgG paraproteins (rather than IgA or IgM) at <15 g/l and normal serum free light chain ratio has a 1% risk of progression to multiple myeloma over 25 years. MGUS must be distinguished from smouldering myeloma, which is diagnosed when paraprotein levels are above 30 g/l and bone marrow plasma cells are >10% total nucleated cells. Donors with smouldering myeloma must not be accepted for tissue donation Melanoma in situ which has been cured by excision is not associated with a risk of metastasis. Patients with a confirmed diagnosis of melanoma in situ (i.e. Breslow thickness of 0 and no regression) do not require ongoing follow up beyond the initial post-operative appointment.
(b) Refer to SaBTO document “Transplantation of organs from deceased donors with cancer or a history of cancer” for generic advice: https://www.gov.uk/government/publications/transplantation-of-organs-from-donors-with-a-history-of-cancer, Eyes - only corneas are accepted under discretionary (1) above as these are avascular and therefore are not likely to be involved in distant metastasis. The vascular parts of the eye are excluded. The predominant mode of progression of primary tumours of the CNS is by invasion and infiltration. Due to the anatomical proximity of the CNS and orbit, these donors should be deferred from sclera donation. |
| Reason for Change | Advice has been added for basal cell carcinoma treated systemically. |
| Donor Information |
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This entry was last updated in
TDSG-DD Edition 203, Release 35