The transmission of donor-derived malignant melanoma to a renal allograft recipient

:  The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant melanoma in a renal allograft transplanted from a multiorgan donor. The lung transplant recipient presented with an allograft lesion that wa...

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Published inClinical transplantation Vol. 20; no. 5; pp. 547 - 550
Main Authors Milton, C.A., Barbara, J., Cooper, J., Rao, M., Russell, C., Russ, G.
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.09.2006
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Abstract :  The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant melanoma in a renal allograft transplanted from a multiorgan donor. The lung transplant recipient presented with an allograft lesion that was proven to be melanoma and of donor‐origin based on human leukocyte antigen (HLA)‐DR typing. One renal allograft recipient was undergoing his second deceased donor renal transplant, having lost his first graft from recurrent IgA nephropathy. He was unsensitized and immunosuppression consisted of tacrolimus, mycophenolate and prednisolone. He achieved stable graft function and there were no episodes of rejection. Four and a half months post‐transplant a diagnosis of donor origin melanoma in the lung recipient was made and his immunosuppression was stopped. He presented with clinical rejection two wk later and a transplant nephrectomy was undertaken. Histology demonstrated vascular and cellular rejection and there was a 3‐mm melanoma deposit with no evidence of tumour infiltrating lymphocytes. Three years post‐transplant he remained clinically well with no evidence of melanoma and received his third deceased donor renal transplant. This was complicated by cellular rejection in the first week treated with methylprednisolone and vascular rejection at day 10 treated with anti‐thymocyte globulin. Three months post‐transplant he has achieved good allograft function and remains well with no evidence clinically or on imaging of metastatic melanoma. The other renal allograft recipient was receiving his first deceased donor transplant, having end‐stage renal failure of uncertain aetiology. His immunosuppression was not stopped until melanoma was proven in the renal allograft pair six months post‐transplant and he then presented with clinical rejection six wk later. Transplant nephrectomy was undertaken and histology did not demonstrate melanoma, but severe vascular and cellular rejection was evident. At three‐yr post‐transplant he remains disease free clinically and on imaging. At present, the cardiac allograft recipient has no evidence of transmitted melanoma. The highest risk of transmission of donor origin melanoma appears to be from donors who are older and have died from an intracerebral haemorrhage. It is likely these donors have metastatic melanoma and their intracerebral haemorrhage is not primary but has occurred in an unrecognized metastatic cerebral deposit. While the occurrence of donor‐transmitted malignancy is not common, the outcome is often fatal.
AbstractList :  The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant melanoma in a renal allograft transplanted from a multiorgan donor. The lung transplant recipient presented with an allograft lesion that was proven to be melanoma and of donor‐origin based on human leukocyte antigen (HLA)‐DR typing. One renal allograft recipient was undergoing his second deceased donor renal transplant, having lost his first graft from recurrent IgA nephropathy. He was unsensitized and immunosuppression consisted of tacrolimus, mycophenolate and prednisolone. He achieved stable graft function and there were no episodes of rejection. Four and a half months post‐transplant a diagnosis of donor origin melanoma in the lung recipient was made and his immunosuppression was stopped. He presented with clinical rejection two wk later and a transplant nephrectomy was undertaken. Histology demonstrated vascular and cellular rejection and there was a 3‐mm melanoma deposit with no evidence of tumour infiltrating lymphocytes. Three years post‐transplant he remained clinically well with no evidence of melanoma and received his third deceased donor renal transplant. This was complicated by cellular rejection in the first week treated with methylprednisolone and vascular rejection at day 10 treated with anti‐thymocyte globulin. Three months post‐transplant he has achieved good allograft function and remains well with no evidence clinically or on imaging of metastatic melanoma. The other renal allograft recipient was receiving his first deceased donor transplant, having end‐stage renal failure of uncertain aetiology. His immunosuppression was not stopped until melanoma was proven in the renal allograft pair six months post‐transplant and he then presented with clinical rejection six wk later. Transplant nephrectomy was undertaken and histology did not demonstrate melanoma, but severe vascular and cellular rejection was evident. At three‐yr post‐transplant he remains disease free clinically and on imaging. At present, the cardiac allograft recipient has no evidence of transmitted melanoma. The highest risk of transmission of donor origin melanoma appears to be from donors who are older and have died from an intracerebral haemorrhage. It is likely these donors have metastatic melanoma and their intracerebral haemorrhage is not primary but has occurred in an unrecognized metastatic cerebral deposit. While the occurrence of donor‐transmitted malignancy is not common, the outcome is often fatal.
The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant melanoma in a renal allograft transplanted from a multiorgan donor. The lung transplant recipient presented with an allograft lesion that was proven to be melanoma and of donor‐origin based on human leukocyte antigen (HLA)‐DR typing. One renal allograft recipient was undergoing his second deceased donor renal transplant, having lost his first graft from recurrent IgA nephropathy. He was unsensitized and immunosuppression consisted of tacrolimus, mycophenolate and prednisolone. He achieved stable graft function and there were no episodes of rejection. Four and a half months post‐transplant a diagnosis of donor origin melanoma in the lung recipient was made and his immunosuppression was stopped. He presented with clinical rejection two wk later and a transplant nephrectomy was undertaken. Histology demonstrated vascular and cellular rejection and there was a 3‐mm melanoma deposit with no evidence of tumour infiltrating lymphocytes. Three years post‐transplant he remained clinically well with no evidence of melanoma and received his third deceased donor renal transplant. This was complicated by cellular rejection in the first week treated with methylprednisolone and vascular rejection at day 10 treated with anti‐thymocyte globulin. Three months post‐transplant he has achieved good allograft function and remains well with no evidence clinically or on imaging of metastatic melanoma. The other renal allograft recipient was receiving his first deceased donor transplant, having end‐stage renal failure of uncertain aetiology. His immunosuppression was not stopped until melanoma was proven in the renal allograft pair six months post‐transplant and he then presented with clinical rejection six wk later. Transplant nephrectomy was undertaken and histology did not demonstrate melanoma, but severe vascular and cellular rejection was evident. At three‐yr post‐transplant he remains disease free clinically and on imaging. At present, the cardiac allograft recipient has no evidence of transmitted melanoma. The highest risk of transmission of donor origin melanoma appears to be from donors who are older and have died from an intracerebral haemorrhage. It is likely these donors have metastatic melanoma and their intracerebral haemorrhage is not primary but has occurred in an unrecognized metastatic cerebral deposit. While the occurrence of donor‐transmitted malignancy is not common, the outcome is often fatal.
Author Rao, M.
Russ, G.
Milton, C.A.
Cooper, J.
Barbara, J.
Russell, C.
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10.1056/NEJM200302063480620
10.1097/00002371-199401000-00005
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Issue 5
Keywords Human
Origin
Transmission
renal allograft
Transplantation
donor-origin melanoma
Malignant tumor
Metastasis
Homotransplantation
Kidney
Medicine
Treatment
Urinary system
Donor
Surgery
metastatic melanoma
Malignant melanoma
Graft
Advanced stage
Metastatic
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PublicationTitle Clinical transplantation
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Snippet :  The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant...
The transmission to organ transplant recipients of donor origin malignancy in the allograft has been described. Here we report the transmission of malignant...
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SubjectTerms Biological and medical sciences
Dermatology
donor-origin melanoma
Fundamental and applied biological sciences. Psychology
Fundamental immunology
Graft Rejection
Humans
Immunosuppressive Agents - therapeutic use
Kidney Transplantation - adverse effects
Lung Transplantation
Male
Medical sciences
Melanoma - etiology
metastatic melanoma
Middle Aged
Mycophenolic Acid - analogs & derivatives
Mycophenolic Acid - therapeutic use
Prednisolone - therapeutic use
renal allograft
Surgery (general aspects). Transplantations, organ and tissue grafts. Graft diseases
Tacrolimus - therapeutic use
Tissue Donors
Tissue, organ and graft immunology
Transplantation, Homologous
Tumors of the skin and soft tissue. Premalignant lesions
Title The transmission of donor-derived malignant melanoma to a renal allograft recipient
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