Anaplastic large cell lymphoma, ALK positive: Difference between revisions

Template:DiseaseDisorder infobox Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Alberto Plate [2]

Synonyms and keywords: ALCL-ALK(+)

Overview

The Anaplastic large cell lymphoma ALK-positive (Anaplastic Llymphoma Kinase) consist of CD30-positive T-cells with abundant cytoplasm, a pleomorphic nucleus (horseshoe-shaped nucleus) and a eosinophilic paranuclear region^[1]. This ALK-positive lymphoma has a translocation in the ALK gene [T(2;5)(p23;q35)], which will in turn, express the ALK protein^[2].

Historical Perspective

Classification

Morphologic Classification^[3]

Classical Variants

• Common pattern ALK positive anaplastic large cell lymphoma

Atypical Variants

• Small cell ALK positive anaplastic large cell lymphoma
• Lymphohistiocytic ALK positive anaplastic large cell lymphoma
• Giant cell ALK positive anaplastic large cell lymphoma
• Hodgkin's like ALK positive anaplastic large cell lymphoma

Rare Variants

• Sarcomatoid ALK positive anaplastic large cell lymphoma

Pathophysiology

ALCL morphologic features are variable, which allowed to classify this entity into five morphologic patterns^[2]:

• "Common" pattern: Its the most common morphologic variant (75%)^[4]. Cytoplasm may be basophilic or eosinophilic and the cell might have many nuclei with dispersed or clumped chromatin. In large cells, nucleoli tends to be more prominent. Given that the lymphomatous cells grow in the lymph node's sinuses, it may resemble a metastatic tumor.
• Lymphohistiocytic pattern (10%): histiocytes with acidophilic cytoplasm and a perinuclear clear area, which represents the Golgi apparatus. This cells have eccentric nuclei with condensed chromatin^[5]. Lymphomatous cells tend tu cluster around the perivascular area, evidenced by immunostaining with CD30 and ALK antibodies^[2].
• Hodgkin's like pattern (3.3%): Morphological characteristics reassemble Hodgkin's lymphoma, variant nodular sclerosis^[6]. Predominates in female patients over male patients.
  • Immunophenotype^[6]
    • Positive: CD30, ALK, epithelial membrane antigen (EMA), CD43 (only 66% of the times) and perforin.
    • Negative: CD15, CD20, Pax5/BSAP and EBV.
• Small cell pattern (8.3%): Present nuclear irregularity and perivascular/intravascular distribution^[7]. Occasionally, this lymphomatous cells have pale cytoplasm with a central nucleus ("fried egg cell")^[2].
• Giant cell pattern (3.3%)

One single patient may present more than one morphologic pattern in the same or progressive biopsies^[1].

Causes

The ALK positive Anaplastic large cell lymphoma has a rearrangement in the Anaplastic Lymphoma Kinase (ALK) gene. The most frequent gene translocation is T(2;5)(p23;q35)^[8]. This translocation produces a chimeric protein between the nucleolar phosphoprotein (NPM) gene (5q35) a ALK gene (2p23), which has structural similarity to the insulin growth factor receptor.^[9] Normal T-cells require IL-2 as a growth factor, while T-cells of patients with ALK positive Anaplastic large cell lymphoma, have a constitutive activating IL-2 receptor, caused by the new NMP-ALK chimeric protein.^[10]

Other genetic gene mutations include^[11]:

• T(1;2), encoding a tropomyosin3 (TPM3)/ALK fusion protein (10 to 20 percent of cases)
• T(2;3), encoding a TRK fusion gene (TFP)/ALK fusion protein (2 to 5 percent of cases)
• Inv(2), encoding a ATIC (Pur H gene)/ALK fusion protein (2 to 5 percent of cases)
• T(2;17), encoding a clathrin heavy (CLTC)/ALK fusion protein (2 to 5 percent of cases)
• T(2;17), encoding a ALO17/ALK fusion protein (2 to 5 percent of cases)
• T(2;19), encoding a tropomyosin 4 (TPM4)/ALK fusion protein (<1 percent of cases)
• T(2;22), encoding a non-muscle myosin (MYH9)/ALK fusion protein (<1 percent of cases)

Differential Diagnosis

• ALCL ALK negative
• Primary cutaneous ALCL
• DLBCL, anaplastic type
• DLBCL, plasmablastic type
• Hodgkin lymphoma

Epidemiology and Demographics

This entity affects primarily young, male patients^[12] and accounts for 3% of all NHL, 40% of all large cell lymphomas^[13] and 10%-20% of childhood lymphomas, although it is particularly incident in patients between 10 and 29 years^[14].

A more recent study evaluated 1,320 cases of peripheral T-cell lymphomas and NK cell lymphomas between 1990 and 2002 in 22 different centers, concluding that the ALK-Positive ALCL is the fifth most incident (6.6% of total patients)^[15], although in the United states, it's the most frequent type of peripheral T-cell lymphoma.

Risk Factors

Natural History, Complications and Prognosis

Prognosis

To establish the prognosis, we use the International Prognostic Iindex (IPI)^[16]. The IPI accounts 5 variables:

• Patient's age (>60 years)
• Serum lactate dehydrogenase (LDH) above normal
• Eastern Cooperative Oncology Group (ECOG) performance status
• Ann Arbor clinical stage III or IV
• Number of involved extra nodal sites > 1

If any of this criteria is met, one point is awarded for the IPI, which allows to classify patients prognosis into the following categories:

• 0 to 1: Low risk
• 2: Low-intermediate risk
• 3: High-intermediate risk
• 4 to 5: High risk

The International Peripheral T cell Lymphoma Project estimated the probability of a 5-years survival for each of the IPI stages^[17]:

• Low risk (IPI 0-1): 90%
• Low-intermediate risk (IPI 2): 68%
• High-intermediate risk (IPI 3): 23%
• High risk (IPI 4-5): 33%

Diagnosis

History and Symptoms

Most adult patients present with painless lymphadenopathy. Although retroperitoneal and peripheral^[18] lymphadenopathy is very common, other possible locations include the gastrointestinal tract, breast^[19], spleen^[20], liver^[21], bone^[21], heart^[22] and respiratory tract^[23].

Common symptoms include typical B symptoms^[24](Fever, weight loss and night sweats).

Laboratory Findings^[25]

• Anemia
• Thrombocytopenia
• Elevated lactate dehydrogenase (LDH) levels

Treatment

CHOP-E Regimen

It includes:

• Cyclophosphamide
• Doxorubicin
• Vincristine
• Prednisone
• Etoposide

References