TY - JOUR
T1 - The clinical diversity and role of chemotherapy in lymphoproliferafive disorder in liver transplant recipients
AU - McCarthy, Michelle
AU - Ramage, John
AU - McNair, Alistair
AU - Gane, Edward
AU - Portmann, Bernard
AU - Pagliuca, Anthony
AU - Rela, Mohamed
AU - Heaton, Nigel
AU - Mufti, Ghulam J.
AU - Williams, Roger
PY - 1997/12
Y1 - 1997/12
N2 - Background/Aims: Post-transplant lymphoproliferative disorder is a well- documented complication with an incidence ranging from 2 to 10%, depending on the organ transplanted. Yet despite our increased understanding of the pathophysiology of this disease and the various treatments available, the mortality remains high at 60-80%. We present the clinical and histological features of ten adult liver transplant recipients with post-transplant lymphoproliferative disorder presenting over a 15-year period and review the therapeutic options. Methods: CD20/CD45RO immunostaining was used for T/B- cell markers; polymerase chain reaction and in-situ hybridisation for Epstein-Barr virus genome detection; κ/λ immunostaining and gene rearrangement analysis for clonality. Results: There were six females and four males (age range 24-56) with onset of post-transplant lymphoproliferative disorder-symptoms ranging from 3 to 72 months post transplant. Sites of post-transplant lymphoproliferative disorder included liver (n=4), lymph nodes (n=5), bone marrow (n=2), lungs (n= 2), kidneys (n=2), brain, ovaries, : and pancreas (n= 1). All lesions were classified as high-grade lymphoma, of B-cell lineage (9 tested); Epstein-Barr virus genome was detected in 7/10 cases. Three tumours were monoclonal; four were polyclonal and three undetermined. Treatment included immunosuppression reduction, antiviral therapy with acyclovir and/or chemotherapy (CHOP or VAPEC-B). Survival times for those patients not treated with chemotherapy were from 9 days to 30 months, whereas those receiving chemotherapy had remission times of 4 to 48 months. Conclusions: Longer-term remissions can be achieved in patients treated with systemic chemotherapy, although not without morbidity. Clonality assessment is important but treatment decisions should be based primarily on clinical features of progression, as polyclonal tumours can behave as aggressively as monoclonal tumours.
AB - Background/Aims: Post-transplant lymphoproliferative disorder is a well- documented complication with an incidence ranging from 2 to 10%, depending on the organ transplanted. Yet despite our increased understanding of the pathophysiology of this disease and the various treatments available, the mortality remains high at 60-80%. We present the clinical and histological features of ten adult liver transplant recipients with post-transplant lymphoproliferative disorder presenting over a 15-year period and review the therapeutic options. Methods: CD20/CD45RO immunostaining was used for T/B- cell markers; polymerase chain reaction and in-situ hybridisation for Epstein-Barr virus genome detection; κ/λ immunostaining and gene rearrangement analysis for clonality. Results: There were six females and four males (age range 24-56) with onset of post-transplant lymphoproliferative disorder-symptoms ranging from 3 to 72 months post transplant. Sites of post-transplant lymphoproliferative disorder included liver (n=4), lymph nodes (n=5), bone marrow (n=2), lungs (n= 2), kidneys (n=2), brain, ovaries, : and pancreas (n= 1). All lesions were classified as high-grade lymphoma, of B-cell lineage (9 tested); Epstein-Barr virus genome was detected in 7/10 cases. Three tumours were monoclonal; four were polyclonal and three undetermined. Treatment included immunosuppression reduction, antiviral therapy with acyclovir and/or chemotherapy (CHOP or VAPEC-B). Survival times for those patients not treated with chemotherapy were from 9 days to 30 months, whereas those receiving chemotherapy had remission times of 4 to 48 months. Conclusions: Longer-term remissions can be achieved in patients treated with systemic chemotherapy, although not without morbidity. Clonality assessment is important but treatment decisions should be based primarily on clinical features of progression, as polyclonal tumours can behave as aggressively as monoclonal tumours.
KW - Chemotherapy
KW - EB virus
KW - Liver transplantation
KW - Lymphoproliferative disorder
UR - http://www.scopus.com/inward/record.url?scp=0030729889&partnerID=8YFLogxK
U2 - 10.1016/S0168-8278(97)80145-6
DO - 10.1016/S0168-8278(97)80145-6
M3 - Article
C2 - 9453427
AN - SCOPUS:0030729889
SN - 0168-8278
VL - 27
SP - 1015
EP - 1021
JO - Journal of Hepatology
JF - Journal of Hepatology
IS - 6
ER -