Angioimmunoblastic T-cell lymphoma
 

 

Uploaded: 2008-01-01, Updated: 2008-01-01

The Key Features

  • Diffuse paracortical infiltrate of polymorphous neoplastic T cells

  • Prominent proliferation of high endothelial venules

  • Proliferation of follicular dendritic cells

CASE STUDY

 

Case 1: Axillary lymph node

 

CLINICAL FEATURES

  • A peripheral T-cell lymphoma with a polymorphous infiltrate in lymph node, a prominent proliferation of high endothelial venules and follicular dendritic cells;

  • Age: middle to elderly; Gender: M=F;

  • 15-20% of peripheral T-cell lymphoma, 1-2% of non-Hodgkin lymphoma;

  • Clinical presentations: often generalized peripheral lymphadenopathy, hepatosplenomegaly, frequent skin rash, and commonly bone marrow involvement upon biopsy.

MICROSCOPIC FINDINGS

  • Loss of normal lymph node architecture

    • Diffuse paracortical infiltrate of polymorphous neoplastic T cells

    • Lymph node architecture is partially or totally effaced

    • Lymphoid follicles, hyperplastic, depleted or regressed, with irregular borders and lack of mantle zones

  • Neoplastic T cells

    • Small to medium-sized but occasionally large cells, usually show minimal cytologic atypia

    • Abundant clear to pale cytoplasm, distinct cell membranes and irregular nuclear contour

    • Often in clusters around high endothelial venules

    • Often obscured by reactive lymphocytes, immunoblasts, plasma cells, histiocytes, and eosinophils

  • Prominent proliferation high endothelial venules

    • Prominent arborizing high endothelial venules with PAS positive amorphous perivascular material

    • The nuclei of endothelial cells are round to oval with regular nuclear contour and a small central nucleolus

  • Prominent proliferation of follicular dendritic cells

    • Follicular dendritic cell proliferation outside germinal centers/around high endothelial venules

    • Highlighted by CD21 staining

  • B cell proliferation

    • >70% are EBV positive

    • May be polymorphic or monomorphic, immunoblastic or plasmacytic

    • Immunoglobulin gene rearrangement detected in 10% cases

    • May produce a Hodgkin-like proliferation with Reed-Sternberg-like cells

SUBTYPES

 

DIFFERENTIAL DIAGNOSES

  • Reactive lymphadenopathies

  • Multicentric Castleman's disease

  • Diffuse large B-cell lymphoma

  • Classical Hodgkin's Disease

IMMUNOHISTOCHEMISTRY AND SPECIAL STAINS

  • Neoplastic cells are mature T-cells with CD3+, CD4+

  • In most cases, the neoplastic T-cells show aberrant expression of CD10

  • Loss of T-cell antigen such as CD7 can occur in some cases

  • EBV positive in >75% cases, mostly in B-cells, not T-cells

  • Follicular dendritic cells CD21+

CYTOGENETICS

  • TCR gene rearrangement in 75% cases

  • 90% have cytogenetic alterations: trisomy 3, trisomy 5 and gain of chromosome X

TREATMENT AND PROGNOSIS

  • Aggressive, median survival <3 years

REFERENCES

  • Jaffe ES, Harris NL, Stein H, Vardiman JW, editors. Pathology and genetics of tumours of haematopoietic and lymphoid tissues. World Health Organization classification of tumours. Lyon (France): IARC Press; 2001.

  • Practical Diagnosis of Hematologic Disorders, Fourth Edition. By Carl R. Kjeldsberg, 2006.