Initial Spontaneous Remission Of Posttransplantation Epstein Barr Virus-related B-cell Lymphoproliferative Disorder Of The Skin In A Renal Transplant Recipient: Case Report And Review Of The Literature On Cutaneous B-cell Posttransplantation Lymphoproliferative Disease
Blokx, W. A., Andriessen, M. P., van Hamersvelt, H. W., & van Krieken, J. H. (2002). Initial spontaneous remission of posttransplantation Epstein Barr virus-related B-cell lymphoproliferative disorder of the skin in a renal transplant recipient: case report and review of the literature on cutaneous B-cell posttransplantation lymphoproliferative disease. The American Journal of dermatopathology, 24(5), 414–422. https://doi.org/10.1097/00000372-200210000-00008
View Original Source →Abstract
Primary cutaneous posttransplantation B-cell lymphoproliferative disorder is rare. The few previously reported patients were all treated with surgery, radiotherapy, or lowering of immunosuppression. We describe a 65-year-old woman presenting with an intermammary skin ulcer 21 years after renal transplantation, proving on biopsy to be an Epstein Barr virus (EBV)-related posttransplantation B-cell lymphoproliferative disorder. A few weeks later, the skin ulcer showed complete clinical regression. Hematologic staging evaluation showed no evidence of extracutaneous involvement. Despite continuation of immunosuppression, the patient stayed free of disease until 18 months after initial diagnosis, when she developed a progressive hemiparesis and died of acute myocardial infarction. At autopsy, a recurrent B-cell posttransplantation lymphoproliferative disorder in the left side of the thalamus region (measuring 1 x 0.8 cm) was established. The long interval between the primary cutaneous lesion and the localized brain recurrence supports primary skin posttransplantation lymphoproliferative disorder, especially because the patient was not treated for her posttransplantation lymphoproliferative disorder. Review of the literature on primary cutaneous posttransplantation B-cell lymphoproliferative disorder and this case gives the impression that cutaneous posttransplantation B-cell lymphoproliferative disorders of B-cell lineage behave in a more benign manner than identical lesions arising extracutaneously. Because of the rare occurrence of posttransplantation B-cell lymphoproliferative disorder primarily involving the skin, extracutaneous origin should be excluded. If B-cell lineage can be established, EBV is present, alterations in oncogenes or tumor suppressor genes associated with malignant lymphoma are absent, and bcl-6 gene mutation associated with progression is absent, initially aggressive treatment might be avoided. However, long-term clinical follow-up with prolonged maintenance therapy (reduction of immunosuppression or antiviral therapy) for prevention of recurrent posttransplantation lymphoproliferative disorder seems indicated, as is demonstrated by the case reported in the current study.
Case Details
Disease Location
Skin ulcer thalamus
Personal Characteristics
65 -year-old female may 2000 renal transplantation in 1979, likely due to chronic pyelonephritis, never had a period of rejection osteoporosis of lumbar spine
Clinical Characteristics
Skin ulcer 21 years after renal transplantation with ebv-related primary cutaneous posttransplantation b-cell lymphoproliferative disorder (b-cell ptld) skin ulcer was a 1 x 1 cm intermammary ulcer with a slightly raised border. No other regional lymphadenopathy biopsy of ulcer was conducted to check for basal cell carcinoma suspicion histologic exam showed partial epidermal ulceration with thrombi in superficial capillaries of the underlying superficial dermis. Next to this ulceration, the epithelium showed slight hyperkeratosis and acanthosis. A mild exocytosis of nontypical lymphocytes with spongiosis was present without pautrier abscesses. In the dermis and subcutis there were nodular infiltrates of large atypical lymphocytes, partially situated around blood vessels and adnexa. Atypical lymphocytes had large, pleomorphic, oval to round, sometimes indented nuclei and pale cytoplasm. Nucleoli was prominent. These large cells were intermingled with a small number of lymphocytes of normal size and mature plasma cells. No necrosis was present immunohistochemical stains revealed that large atypical lymphocytes were strong positive for CD20, 30, and ebv-latent membrane protein. Immunoglobulin light and heavy chain staining was unreliable, and light chain restriction could not be demonstrated. Results were negative for alk-1 and bcl-6. Ebv in situ hybridization with the eber probe showed strong nuclear positivity, thus the ebv-related diagnosis serologic signs of active ebv infection were current 3 years before the current episode of lymphoproliferative disease, at that time ebv serologic status was determined because of slight, temporary elevation of serum alanine aminotransferase (60u/l) witho hematologic or clinical signs of ebv infection. At time of ptld, there were high immunoglobulin g titers against viral capsid antigen and early antigen, positive immunoglobulin m against vca and low or undetectable immunoglobulin g titer against nuclear antigen. Likely ebv infection triggered the development of the lymphoproliferative disease 18 months later, right-sided hemiparesis and dysphagia developed. CT showed bleeding around a hypodense lesion in the left side of thalamic region which was suspect for recurrent cerebral posttransplantation lymphoma. Died of myocardial infarction 18 months after initial diagnosis and autopsy established a recurrent b-cell ptld in the left side of the thalamus region (1 x 0.8cm) and area showed extensive necrosis; within margins of necrosis atypical perivascular infiltrates of small lymphocytes admixed with large pleomorphic centroblast-like lymphocytes were present. Ptld immunohistochemical analysis confirmed positivity of the lymphocyte tumor cells for b-cell markers, CD30, cutaneous ebv-latent membrane protein, and positive ebv eber in situ hybridization autopsy also revealed generalized atherosclerosis and coronary sclerosis with occlusive thrombosis of the right-side coronary artery and acute posterior myocardial infarction.
Remission Characteristics
A few weeks later after biopsy, witho further clinical intervention, the ulcer showed complete clinical regression CT scans of thorax, abdomen, and x-thorax showed neither enlarged lymph nodes nor abnormalities in organs including the transplant kidney bone marrow biopsy were normal stay disease free for 18 months after initial diagnosis then developed a progressive hemiparesis and died of acute myocardial infarction
Treatment & Mechanisms
Proposed Remission Mechanisms
Antiviral treatment and reduction/discontinuation of immunosuppression cutaneous b-cell ptld has been treated with surgery or radiotherapy
Clinical Treatment
Immunosuppressive treatment of azathioprine and prednisolone since time of transplantation and when ulcer appeared palliative care for thalamic lesion: diadreson f to prevent corticosteroid withdrawal
Non-Clinical Treatment
None reported