Post-transplant lymphoproliferative disorder

Post-transplant lymphoproliferative disorder
Post-transplant lymphoproliferative disorder
Other names	PTLD
Specialty	Immunology

Post-transplant lymphoproliferative disorder (PTLD) is the name given to a B cell proliferation due to therapeutic immunosuppression after organ transplantation. These patients may develop infectious mononucleosis-like lesions or polyclonal polymorphic B-cell hyperplasia. Some of these B cells may undergo mutations which will render them malignant, giving rise to a lymphoma.^{[citation needed]}

In some patients, the malignant cell clone can become the dominant proliferating cell type, leading to frank lymphoma, a group of B cell

organ transplant

.

Signs and symptoms

Symptoms of PTLD are highly variable and nonspecific, and may include fever, weight loss, night sweats, and fatigue. Symptoms may be similar to those seen in infectious mononucleosis (caused by EBV). Pain or discomfort may result from lymphadenopathy or mass effect from growing tumors. Dysfunction may occur in organs affected by PTLD. Lung or heart involvement may result in shortness of breath.^{[citation needed]}

Laboratory findings may show abnormally low white blood cell, red cell counts, and platelet counts. In addition, serum uric acid and lactate dehydrogenase levels may be elevated, while serum calcium levels may be decreased. All of these findings together can suggest tumor lysis syndrome.^{[citation needed]}

Causes

The disease is an uncontrolled proliferation of B cell

interleukin-10, an endogenous, pro-regulatory cytokine, has also been implicated.^{[citation needed}

]

In immunocompetent patients, Epstein-Barr virus can cause

T-cell immunosurveillance can lead to the proliferation of these EBV-infected B-lymphocytes.^{[citation needed}

]

However, calcineurin inhibitors (tacrolimus and ciclosporin), used as immunosuppressants in organ transplantation inhibit T cell function, and can prevent the control of the B cell proliferation.^{[citation needed]}

Depletion of T cells by use of anti-T cell

OKT3 (muromonab-CD3).^{[citation needed}

]

Polyclonal PTLD may form tumor masses and present with symptoms due to a mass effect, e.g. symptoms of bowel obstruction. Monoclonal forms of PTLD tend to form a disseminated malignant lymphoma.

Diagnosis

Definitive diagnosis is achieved by biopsying the involved tissue, which will reveal lymphoproliferative neoplasia. Most lesions will show malignant B cells, whereas a minority will show T cell neoplasia. CT imaging may show enlarged lymph nodes or a focal mass. PET scan may be helpful in the evaluation, which may show an increase in metabolic activity (PET avid) lesion, potentially guiding decisions on where to direct biopsies.

Neurologic symptoms, such as confusion or focal weakness, which may suggest involvement of the nervous system. This may be evaluated with an MRI of the brain with gadolinium based contrast and lumbar spinal tap with testing of the cerebral spinal fluid for EBV viral levels.

The presence of respiratory symptoms, such as cough or shortness of breath, in the setting of immunosuppression may suggest infection. Opportunistic infections may present in a similar fashion to PTLD. Evaluation with sputum culture for bacteria, Pneumocystis carinii, and acid fast bacilli, and fungal infections are often helpful.

Treatment

PTLD may spontaneously regress on reduction or cessation of

non-Hodgkin's lymphoma and may be fatal. A phase 2 study of adoptively transferred EBV-specific T cells demonstrated high efficacy with minimal toxicity.^[4]

Epidemiology

PTLD is the second most common malignancy that occurs as a complication following solid organ transplantation (skin cancer is the most common). Less commonly, PTLD occurs after hematopoietic stem cell transplantation. The incidence varies by the type of transplantation: the lowest rates are seen with bone marrow transplants and liver transplants. The highest rates of PTLD are seen with lung and heart transplants, which is primarily due to the need for higher levels of immunosuppression. The incidence of PTLD is highest in the first year after transplantation; roughly 80 percent of cases after transplant occur in the first year. Transplantation of unmatched or mismatched HLA bone marrow also increase the risk of PTLD. ^[citation needed]

The main risk factors for PTLD are the degree of immune suppression and the presence of Epstein-Barr virus. Specifically, higher levels of T cell immunosuppression increase the risk PTLD. Individuals who have never been infected by the Epstein-Barr virus (EBV negative) who receive an organ from a donor with prior EBV infection are 24 times more likely to develop PTLD. Similarly, CMV mismatching (with a CMV negative recipient from a CMV positive donor) increases the risk of PTLD.^{[citation needed]}

References

PMID 15660500
.

PMID 21521464
.

^ "Hematopathology". webpath.med.utah.edu.

PMID 17468341
.

External links

Classification
ICD-9-CM: 238.77
ICD-O: M9970/1
DiseasesDB: 34154
External resources
eMedicine: ped/2851

v
t
e
Organ transplantation
Types

Allotransplantation
ABOi

Autotransplantation

Xenotransplantation

Organs and tissues

Bone

Bone marrow

Brain

Corneal

Eye

Face

Hand

Head

Heart

Heart–lung

Intestine

Kidney

Liver

Lung

Pancreas
islet cell

Penis

Skin

Spleen

Thymus

Uterus

Vagina

Medical grafting

Bone grafting

Skin grafting

Vascular bypass

Organ donation

Non-heart-beating donation

Organ procurement

Organ trade

Complications

Graft-versus-host disease

Post-transplant lymphoproliferative disorder

Transplant rejection

Transplant networks
and government
departments

BC Transplant Society

Eurotransplant

Gift of Life Marrow Registry

Human Tissue Authority

LifeSharers

National Marrow Donor Program

NOD-Lb

National Transplant Organization

NHS Blood and Transplant

Trillium Gift of Life Network

United Network for Organ Sharing

Advocacy
organizations

Anthony Nolan

Blood Cancer UK

DKMS

Halachic Organ Donor Society

Kidney Foundation of Canada

National Kidney Foundation

ORGANIZE

Joint societies

American Society of Nephrology

American Society of Transplantation

Canadian Society of Transplantation

Countries

Organ transplantation in China

Organ donation in India
Gurgaon kidney scandal

Organ transplantation in Israel

Organ transplantation in Japan

People
Heart

Christiaan Barnard

James D. Hardy

Adrian Kantrowitz

Richard Lower

Norman Shumway

Kidney

J. Hartwell Harrison

John P. Merrill

Joseph Murray

Elizabeth Ward

Michael Woodruff

Liver

Fikri Alican

James D. Hardy

Thomas Starzl

Lung

Fikri Alican

Joel D. Cooper

Vladimir Demikhov

James D. Hardy

Pancreas

Richard C. Lillehei

Penis

André van der Merwe

Other

Alexis Carrel

Jean-Michel Dubernard

Donna Mansell

Bruce Reitz

List of organ transplant donors and recipients

Related topics

Biomedical tissue

Edmonton protocol

Eye bank

Immunosuppressive drugs

Lung allocation score

Machine perfusion

Total body irradiation

Frankenstein's monster

Leukaemias, lymphomas and related disease
B cell
(lymphoma,
leukemia)
(most CD19
CD20)
By
development/
marker
TdT+

ALL (Precursor B acute lymphoblastic leukemia/lymphoma)

CD5+

CLL/SLL
)

mantle zone (Mantle cell)

CD22+

Prolymphocytic

CD11c+ (Hairy cell leukemia
)

CD79a+

germinal center/follicular B cell (Follicular

Burkitt's

GCB DLBCL

Primary cutaneous follicle center lymphoma)

marginal zone B-cell (Splenic marginal zone

MALT

Nodal marginal zone

Primary cutaneous marginal zone lymphoma)

CD15+, CD30
+)

Classic Hodgkin lymphoma (Nodular sclerosis)

CD20+ (Nodular lymphocyte predominant Hodgkin lymphoma)

CD138
+)

see immunoproliferative immunoglobulin disorders

By infection

KSHV (Primary effusion)

EBV
Lymphomatoid granulomatosis

Post-transplant lymphoproliferative disorder

Classic Hodgkin lymphoma

Burkitt's lymphoma

HCV
Splenic marginal zone lymphoma

HIV (AIDS-related lymphoma)

Helicobacter pylori (MALT lymphoma)

Cutaneous

Diffuse large B-cell lymphoma

Intravascular large B-cell lymphoma

Primary cutaneous marginal zone lymphoma

Primary cutaneous immunocytoma

Plasmacytoma

Plasmacytosis

Primary cutaneous follicle center lymphoma

T/NK
T cell
(lymphoma,
leukemia)
(most CD3
CD4

CD8)
By
development/
marker

Precursor T acute lymphoblastic leukemia/lymphoma
)

prolymphocyte (Prolymphocytic)

CD30+ (Anaplastic large-cell lymphoma

Lymphomatoid papulosis type A)

Cutaneous
MF+variants

indolent: Mycosis fungoides

Pagetoid reticulosis

Granulomatous slack skin

aggressive: Sézary disease

Adult T-cell leukemia/lymphoma

Non-MF

CD30-: Non-mycosis fungoides CD30− cutaneous large T-cell lymphoma

Pleomorphic T-cell lymphoma

Lymphomatoid papulosis type B

CD30+ cutaneous T-cell lymphoma

Secondary cutaneous CD30+ large-cell lymphoma

Lymphomatoid papulosis type A

Other
peripheral

Hepatosplenic

Angioimmunoblastic

Enteropathy-associated T-cell lymphoma

Peripheral T-cell lymphoma not otherwise specified (Lennert lymphoma)

Subcutaneous T-cell lymphoma

By infection

HTLV-1 (Adult T-cell leukemia/lymphoma)

CD56
)

Aggressive NK-cell leukemia

Blastic NK cell lymphoma

T or NK

Angiocentric lymphoma
)

Large granular lymphocytic leukemia

Lymphoid+
myeloid

Acute biphenotypic leukaemia

Lymphocytosis

Lymphoproliferative disorders (X-linked lymphoproliferative disease

Autoimmune lymphoproliferative syndrome)

Leukemoid reaction

Diffuse infiltrative lymphocytosis syndrome

Cutaneous lymphoid hyperplasia

Cutaneous lymphoid hyperplasia
with bandlike and perivascular patterns

with nodular pattern

Jessner lymphocytic infiltrate of the skin

General

Hematological malignancy

leukemia

Leukemia cutis

Lymphoproliferative disorders

Lymphoid leukemias

Retrieved from "https://en.wikipedia.org/w/index.php?title=Post-transplant_lymphoproliferative_disorder&oldid=1116170276"

[pmid15660500-1] PMID 15660500
.

[2] PMID 21521464
.

[urlHematopathology-3] "Hematopathology". webpath.med.utah.edu.

[4] PMID 17468341
.

[4]