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T-cell large granular lymphocyte leukemia

T-cell large granular lymphocyte leukemia is a disease that exhibits an unexplained, chronic (> 6 months) elevation in large granular lymphocytes (LGLs) in the peripheral blood.[1]

It is also known by the following terms: Proliferation of large granular lymphocytes (LGLs), LGL leukemia, T?-lymphoproliferative disorder, T-cell chronic lymphocytic leukemia[1]

Contents


Epidemiology

T-LGL is a rare form of leukemia, comprising 2-3% of all cases of small lymphocytic leukemias.[1]

Clinical Features

Etiology

The postulated cells of origin are a transformed CD8+ T-cell with clonal rearrangements of ? chain T-cell receptor genes for the majority of cases and a CD8- T-cell with clonal rearrangements of ? chain T-cell receptor genes for a minority of cases.[1]

Clinical Presentation

This disease is known for an indolent clinical course and incidental discovery.[1] The most common physical finding is moderate splenomegaly. B symptoms are seen in a third of cases, and recurrent infections due to the associated neutropenia are seen in almost half of cases.[2][3][4][5] Rheumatoid arthritis is commonly observed in patients with T-LGL, leading to a clinical presentation similar to Felty's syndrome.[6] Signs and symptoms of anemia are commonly found, due to the association between T-LGL and erythroid hypoplasia.[7]

Laboratory Findings

The requisite lymphocytosis of this disease is typically 2-20x109/L.[7] Immunoglobulin derangements including hypergammaglobulinemia, autoantibodies, and circulating immune complexes are commonly seen.[8][9][10][5]

Sites of Involvement

The leukemic cells of T-LGL can be found in peripheral blood, bone marrow, spleen, and liver. Nodal involvement is rare.[1][2]

Morphology

Peripheral blood

The neoplastic lymphocytes seen in this disease are large in size with azurophilic granules that contains proteins involved in cell lysis such as perforin and granzyme B.[11]

Bone marrow

Bone marrow involvement in this disease is often present, but to a variable extent. The lymphocytic infiltrate is usually interstitial, but a nodular pattern rarely occurs.[1]

Molecular Findings

Immunophenotype

The neoplastic cells of this disease display a mature T-cell immunophenotype, with the majority of cases showing a CD4-/CD8+ T-cell subset immunophenotype versus other permutations of those markers.[3][4] Variable expression of CD11b, CD56, and CD57[5] are observed. Immunohistochemistry for perforin, TIA-1, and granzyme B are usually positive.[1]

Type Immunophenotype
Common type (80% of cases) CD3+, TCR??+, CD4-, CD8+
Rare variants CD3+, TCR??+, CD4+, CD8-
CD3+, TCR??+, CD4+, CD8+
CD3+, TCR??+, CD4 and CD8 variable

Genetic Findings

Clonal rearrangements of the T-cell receptor (TCR) genes are a necessary condition for the diagnosis of this disease. The gene for the ? chain of the TCR is found to be rearranged more often than the ? chain. of the TCR.[9][12]

References

pt:Leucemia linfocítica granular T





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