1/2015
vol. 40
Invasive pulmonary Successful treatment of Epstein-Barr virus-related post-transplant lymphoproliferative disease with central nervous system involvement following allogeneic haematopoietic stem cell transplantation –a case study
(Centr Eur J Immunol 2015; 40 (1): 122-125)
Online publish date: 2015/04/22
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Introduction
Post-transplant lymphoproliferative disease (PTLD) is a rare but severe complication that develops in patients after haematopoietic stem cell transplantation (HSCT) or solid organ transplantation (SOT) [1]. It is a heterogeneous group of lymphoproliferations with spectrum ranging from benign hyperplasia to aggressive lymphomas. The majority of cases are of B-cell origin, T-cell PTLD is reported in 10-15% of cases [2]. More than half (60-70%) of cases of PTLD are associated with Epstein-Barr virus, and these are usually early cases, within the first year after transplantation. Epstein-Barr virus-negative PTLD usually occurs late after transplantation, and more often after SOT than HSCT [3]. According to the World Health Organisation (WHO) classification, PTLD may have one of four major histological forms: early benign lesions, polymorphic PTLD, monomorphic PTLD, or the least common form of classical Hodgkin lymphoma [4].
The underlying mechanism of EBV-positive PTLD is based on the inability of the immune system to control latent EBV infection [5]. The most significant risk factors for the development of EBV-related PTLD in patients after HSCT are transplantation from an unrelated or HLA-mismatched donor, including haploidentical or cord blood transplantation, donor-recipient serological mismatch regarding EBV, and T-cell depletion in transplanted material or use of antithymocyte globulin (ATG) [1, 6]. The disease is usually diagnosed as B-cell lymphoma but with a highly heterogeneous clinical picture. The diagnosis is likely when significant lymphadenopathy or other organ involvement is observed along with high blood EBV-DNAemia and in the absence of other disease. To establish a proven diagnosis EBV must be detected in material from a biopsy of an involved organ [7]. Post-transplant lymphoproliferative disease with central nervous system (CNS) involvement, which is difficult to confirm, is considered a high risk disease [8].
Case report
The patient, a 29-year-old woman, was diagnosed with T-cell lymphoblastic lymphoma stage IIB in 2012. She received chemotherapy according to Polish Adult Leukaemia Group protocol ALL – 2007, with complete remission (CR). Because of early relapse, therapy with fludarabine, cytarabine, and mitoxantrone (FLAM regimen) was administered, and after the second CR was achieved the patient was qualified for allogeneic HSCT. The transplantation procedure was performed on 28th August 2013. The patient was conditioned with ablative therapy based on total body irradiation and cyclophosphamide and transplanted with peripheral blood stem cells from an unrelated donor: a 45-year-old male with one HLA mismatch. Both donor and recipient were serologically EBV-positive and CMV-negative prior to the transplantation. Graft-versus-host disease (GvHD) prophylaxis consisted of standard doses of cyclosporine A and methotrexate, as well as ATG-Fresenius in a dose of 40 mg/kg. The post-transplant period was uncomplicated. Neutrophil recovery (absolute neutrophil count > 0.5 × 106/l) occurred on day +16. The patient was discharged from the hospital on day +28 in good general condition. She was under careful clinical monitoring every 7 to 10 days in an outpatient clinic, with no adverse symptoms and no GvHD. Assays for EBV and CMV reactivation performed with PCR method to detect viral DNA remained negative for 60 days after transplantation.
On day +63 the patient was urgently admitted to the transplant centre with severe headache. There were no focal neurological signs on admission; however, enlarged cervical and inguinal lymph nodes were found. Since the lymph nodes were only about 2 cm in diameter and painful, the biopsy was postponed. Blood count and biochemistry were normal. Other laboratory tests revealed blood EBV – DNAemia at the level of 1.03 × 107 copies per ml and plasma monoclonal IgG at the level of 18.8 g/l. The assays for blood CMV – DNA, HHV6 – DNA and Adenovirus – DNA were negative. Bone marrow aspiration followed by immunophenotyping revealed no abnormalities. Chest X-ray was normal, but abdominal sonography revealed mild hepatosplenomegaly. Magnetic resonance imaging (MRI) of the central nervous system revealed segmental, asymmetrical thickening of the meninges as well as subtle vasogenic changes with no brain focal lesions (Fig. 1). Lumbar punction (LP) was performed, and on the cerebrospinal fluid (CSF) examination there were 40 leukocytes per µl, identified in 100% of cases as monoclonal B-lymphocytes with flow-cytometry. Cerebrospinal fluid culture was negative.
Based on the above findings and the clinical picture, diagnosis of probable EBV-driven systemic PTLD with CNS involvement was made. Because the patient was still on low doses of Cyclosporine A, immunosuppression was withdrawn. The patient immediately received intravenous rituximab (375 mg/m2) with the intention to continue injections every 7 days. Additionally, intrathecal chemotherapy with methotrexate and dexamethason was administered. Previously enlarged lymph nodes became impalpable after the first dose of rituximab. Despite the immediate introduction of therapy, the patient’s neurological status deteriorated and she became unconscious. On the 12th day after admission the patient unexpectedly experienced a sudden cardiac arrest in the form of asystole. After successful resuscitation the treatment with rituximab and intrathecal chemotherapy was continued at the Intensive Care Unit with a gradual decrease of blood EBV – DNA load. Cerebrospinal fluid assessment revealed 48 leukocytes per µl with monoclonal B-lymphocytes comprising < 1% of the cells; however, EBV – DNA load in the CSF was 6.90 × 104 copies per ml. After the second dose of intrathecal chemotherapy, an oedema of the lumbosacral region was noticed, presumably resulting from CSF extravasation. At this time, probably due to the mentioned complication, transient flaccid tetraparesis occurred. Intrathecal treatment was therefore discontinued, but therapy with intravenous rituximab was continued. After the third dose of intravenous rituximab, the patient’s condition significantly improved. As the sedation was gradually withdrawn, she remained in good logical contact. Serum EBV – DNAemia reached undetectable level on the 27th day after admission. No monoclonal plasma protein was present.
At eight months after transplantation there were no symptoms of PTLD, and blood EBV – DNA assay remained negative. There was no evidence of monoclonal plasma protein. The picture of bone marrow remained free from abnormalities. The control MRI revealed only discreet sustained vasogenic changes, and the previously seen oedema and meningeal thickening were absent. The patient regained motor skills with only slight debilitation of left lower limb. Limited GvHD with skin involvement developed five months after transplantation.
Discussion
Post-transplant lymphoproliferative disease is a rare condition, but its incidence is increasing because of the growing number of transplantation procedures and longer survival of patients thereafter [8]. After SOT, PTLD occurs in 1-16% of patients, depending on the transplanted organ [9]. After HSCT the general incidence of PTLD is 3.2% [7]. Central nervous system involvement occurs in 10-15% of PTLD cases after SOT [2]. There is no exact data on CNS involvement in PTLD following HSCT, but it is said that CNS presentation occurs more frequently when compared to the general population of aggressive lymphoma patients. Both after SOT or HSCT procedures, CNS-PTLD is associated with significantly inferior survival in comparison to non-CNS-PTLD.
The spectrum of clinical pictures of CNS-PTLD has not been fully characterised yet. According to the analysis of reported events [10, 11], it usually manifests as parenchymal lesions (multifocal in 61% of cases) or as meningeal involvement, seen in about 40% of cases. Isolated leptomeningeal and ependymal localisation is rare (10%). Histopathologically CNS-PTLD is usually of monomorphic form with diffuse large B-cell lymphoma (DLBCL) or Burkitt lymphoma as the most commonly recognised [8].
In the course of aggressive lymphomas in general, CNS involvement occurs in 2-30% of cases, depending on the risk factors, and it is usually fatal with a median survival time of 2-6 months in the subgroup of patients with secondary CNS disease [12]. Current treatment options for CNS lymphoma, both primary and secondary, include CNS penetrating chemotherapy, intrathecal chemotherapy, and/or brain radiation therapy, with a low rate of durable responses. High-risk patients usually receive CNS prophylaxis with intrathecal chemotherapy [12].
Therapy of PTLD in general is targeted at reconstitution of T-cell function and reduction of proliferating B-cells, whereas antiviral treatment has no clinical significance since it is of low effectiveness against the latent form of EBV [7]. Methods aimed at T-cell reconstitution include reduction of immunosuppression (RI) and T-cell immunotherapy, which can be donor lymphocyte infusion (DLI) or use of EBV-specific cytotoxic T-lymphocytes (EBV-CTL). Since DLI, although very effective, significantly increases the risk of GvHD and EBV-CTL is a complicated and not commonly available method, RI remains the basic T-cell restoring treatment. Reduction of immunosuppression or its withdrawal allows the immune system to recover and potentially control the EBV infection. It is recommended whenever possible, but its use is limited in the presence of GvHD [13]. Methods targeted at reduction of B-cells include the use of monoclonal antibodies, chemotherapy, and/or surgery [3]. Therapy with monoclonal antibodies aimed at B-cells plays the major role in the therapy of PTLD, both probable and proven. Rituximab, a monoclonal anti-CD20 antibody that depletes the number of B-cells, has proven efficacy in the therapy of systemic PTLD and significantly improves the outcomes of patients [3, 13, 14]. Rituximab and reduction of immunosuppression remain the first-line therapeutic modalities against PTLD [3, 7, 15]. In cases of resistance to rituximab or disease progression, chemotherapy and DLI are the second-line methods [7]. Surgery has only limited use in the therapy of PTLD [15].
For cases of PTLD with CNS involvement there is no established optimal treatment, but it should probably be similar to the one used in immunocompetent lymphoma, as described above. Despite the known value of rituximab in the treatment of B-lymphomas and PTLD, in case of CNS involvement the problem of blood-brain barrier impermeability occurs as a factor limiting the effectiveness of this drug administered intravenously [16]. There are attempts to administer rituximab intrathecally [5, 17] to improve its efficacy in the CNS; however, such treatment has not been licensed so far.
In the presented case PTLD with CNS involvement was successfully treated with intravenous rituximab and reduction of immunosuppression. Because the lymph node biopsy could not be performed, we did not obtain the histological type of PTLD. We had to base our therapeutic decisions on a diagnosis of probable EBV-driven systemic PTLD with B-lymphocyte proliferation. Due to the complication of LP that occurred during the treatment, initially administered intrathecal chemotherapy had to be terminated and therapy was continued solely with intravenous rituximab. The patient recovered, so we assume that penetration of rituximab to the CNS was been improved due to the compromised permeability of the blood-brain barrier resulting from meninges being involved in the course of the lymphoproliferative process. There have been other reported cases of successful CNS PTLD treatment using intravenous rituximab [18, 19], in which disruption of the blood-brain barrier probably contributed to the favourable outcome.
Our observations suggest that it is possible to achieve a positive outcome of PTLD with CNS involvement once penetration of rituximab across the blood-brain barrier is facilitated. Otherwise this improvement might be reached with intrathecal administration of rituximab. Until now there are no recommendations regarding therapy with intrathecal rituximab in PTLD with CNS involvement. This treatment modality requires further studies because it is potentially beneficial in the treatment of life-threatening complications of HSCT.
The authors declare no conflict of interest.
References
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Copyright: © 2015 Polish Society of Experimental and Clinical Immunology This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International (CC BY-NC-SA 4.0) License ( http://creativecommons.org/licenses/by-nc-sa/4.0/), allowing third parties to copy and redistribute the material in any medium or format and to remix, transform, and build upon the material, provided the original work is properly cited and states its license.
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