Primary gastrointestinal lymphoma

Gastrointestinal lymphomas are a diverse group of extranodal non-Hodgkin lymphomas that most commonly affect the stomach, small intestine, and colon. Diagnosis is challenging because these tumors often manifest with nonspecific symptoms such as abdominal pain, weight loss, and/or GI bleeding. Histological subtypes vary; mucosa-associated lymphoid tissue (MALT) lymphoma and diffuse large B-cell lymphoma are the most common. Diagnostic studies include endoscopy with biopsy and cross-sectional imaging. Management depends on the subtype, and may consists of chemotherapy, immunotherapy, and occasionally surgery.

MALT lymphoma is discussed in a separate article.

Epidemiology ^[1][2]

• Diffuse large B-cell lymphoma of the GI tract (DLBCL) accounts for 70% of all gastric lymphomas. ^[1]
• Peak incidence: 50 years ^[2]
• ♂ > ♀

Etiology ^[1][2]

• DLBCL may manifest as:
  • De novo tumor
  • Transformation of a low-grade B-cell lymphoma, most commonly MALT lymphoma
• May occur in patients with immunocompromise (e.g., due to HIV infection, posttransplant)

Clinical features ^[1]

• Features are nonspecific and may include:
  • Abdominal pain
  • Dyspepsia
  • Nausea and vomiting
  • Diarrhea
  • Palpable abdominal mass

Diagnosis

Endoscopic assessment with biopsy and histopathology analysis is required for diagnostic confirmation.

Endoscopy ^[1]

Findings are nonspecific and may include:

• Erythematous mucosa
• Mucosal ulceration or erosions
• Enlarged and thickened gastric folds

Biopsy ^[1][2]

• Histopathology
  • Diffuse cell proliferation infiltrating the gastric glands and the lamina propria
  • Neoplastic cells are medium to large, with markedly enlarged nuclei and scant pale or eosinophilic cytoplasm.
• Immunohistochemistry ^[2]
  • Positive: CD20, CD79a, PAX-5
  • Variable expression: BCL-2, BCL-6, MUM-1, CD-43, c-MYC ^[2]

Differential diagnoses ^[1]

• Nonneoplastic conditions
  • Reactive gastropathy and gastritis
  • Reactive germinal centers within MALT lymphoma
• Malignancies
  • Gastric adenocarcinoma
  • Other gastrointestinal lymphomas (e.g., MALT lymphoma, mantle cell lymphoma, follicular lymphoma)

Management

• Management depends on tumor stage.
• First-line therapy consists of chemoimmunotherapy (i.e., R-CHOP and dose–adjusted EPOCH-R).
• Second-line therapy
  • Autologous stem cell transplant
  • Anti-CD19 CAR T cell therapy

Classification of Burkitt lymphoma ^[1][2][3]

Burkitt lymphoma is classified into three variants, each with different epidemiological and clinical characteristics.

• Sporadic variant
  • Affects all age groups
  • Variant in which GI tract involvement is most common.
  • May be associated with EBV infection, especially in older adults
• Endemic variant
  • Mostly affects children and adolescents
  • 95–100% of patients have EBV infection; infection with Plasmodium spp. is also common. ^[3]
• Immunodeficiency-associated variant
  • Mostly affects adults
  • Commonly associated with HIV infection, may be associated with EBV infection

Epidemiology ^[1][2][3]

• Burkitt lymphoma accounts for ∼ 5% of all primary non-Hodgkin lymphomas of the GI tract. ^[1]
• The sporadic and endemic variants most commonly affect children and adolescents; the immunodeficiency-associated variant typically affects adults.
• The endemic variant occurs in equatorial Africa and Papua New Guinea. ^[3]

Etiology ^[1][2]

• Derived from germinal center B cells
• t(8;14) leads to overactivation of the C-MYC gene and transcription.

Clinical features ^[1][2][3]

Presentation is typically dramatic, with a rapidly growing mass that spreads systemically.

• GI tract involvement (most common in the sporadic form)
  • Rapidly growing large masses, commonly in the ileocecal region
  • Bowel obstruction
• Other organs may be affected, e.g.:
  • Peritoneum
  • Thyroid
  • Breasts
  • Kidney
  • Ovaries, testicles
  • CNS (most common in the immunodeficiency-associated variant)
• Tumor lysis syndrome

Differential diagnoses

• Diffuse large B-cell lymphoma
• Other high-grade B-cell lymphomas with MYC translocations, e.g.:
  • Mantle cell lymphoma
  • Precursor B-cell lymphoblastic lymphoma

Diagnosis

General principles ^[3]

• Obtain initial laboratory studies (e.g., CBC, LDH, viral serologies).
• Staging of non-Hodgkin lymphomas is required for all patients.
• Diagnosis is confirmed with histopathological studies.
• See "Diagnosis of non-Hodgkin lymphoma" for more information.

Histopathology ^{[3] [1][2]}

A large-bore core needle or surgical biopsy is required; findings are similar across the three variants of Burkitt lymphoma.

• Diffuse infiltrate of monomorphic, medium-sized B cells
  • Round nuclei with vesicular chromatin and multiple basophilic nucleoli
  • Basophilic cytoplasm
• Ki-67 index ∼ 100% ^[1][3]
• Multiple tingible body macrophages ("starry sky" pattern)

Immunohistochemistry ^[1][2][3]

• Positive markers
  • B-cell markers (e.g., CD20)
  • Germinal center B-cell markers: CD19, CD10, BCL-6, PAX5
• Negative markers
  • BCL-2
  • CD5
  • CD23

Cytogenetics

• MYC t (8;14) in ∼ 75% of tumors ^[1][3]
• May not be detected with standard fluorescence in situ hybridization

Management ^[3]

Emergency management is required to avoid complications.

• Systemic chemoimmunotherapy: combination regimens (e.g., cyclophosphamide, rituximab, methotrexate), based on patient risk
• CNS prophylaxis: in patients with features of high-risk tumors (e.g., patients with ECOG PS ≥ 2, ↑ LDH, tumor size ≥ 7 cm)
• See also "Treatment of non-Hodgkin lymphoma."

Burkitt lymphoma can be cured in ∼ 90% of children and adolescents. ^[3]

Complications ^[2]

• Hemorrhage
• Necrosis
• Tumor lysis syndrome
• Intestinal perforation

Epidemiology ^[4]

• Prevalence is highest in Europe (∼ 9%) and among individuals of northern European descent. ^[4]
• Peak incidence: 60–70 years ^[4]
• ♂ ≈ ♀

Etiology ^[4]

• EATL occurs in the context of celiac disease (patients may be undiagnosed).
• HLA-DQA1*0501, HLA-DQB*0201 may be present.
• Patients with refractory celiac disease are at the highest risk for EATL.
  • De novo tumor: in patients without complicated celiac disease
  • Secondary to refractory celiac disease

Clinical features ^[1][4]

• Symptoms are nonspecific and may mimic celiac disease, e.g.:
  • Constitutional symptoms
  • Abdominal pain
  • Diarrhea
  • Clinical features of bowel obstruction (e.g., vomiting)
  • GI bleeding
  • Intestinal perforation (in 25–50% of patients) ^[4]
• Refractory celiac disease features may be present.
• Hemophagocytic syndrome (in 16–40% of patients) ^[4]
• Involvement of extraintestinal organs (e.g., bone marrow, lung, skin)

Diagnosis ^[1][4]

Endoscopy with biopsy, and histopathology and immunohistochemistry analysis are required for diagnosis.

• Histopathology
  • Diffuse proliferation of pleomorphic, medium to large atypical lymphocytes
  • Cells have a round or irregular nucleus, with abundant eosinophilic or pale cytoplasm
  • Concomitant polymorphic inflammatory infiltrate (e.g., eosinophils, neutrophils, plasma cells)
  • Vascular invasion and extensive necrosis are common.
  • Adjacent mucosa may show features of celiac disease (e.g., villous atrophy, crypt hyperplasia).
• Immunohistochemistry
  • Positive markers
    • CD3
    • CD7
    • CD103
    • Cytotoxic granule proteins (TIA-1, granzyme B, and perforin)
  • Negative markers
    • CD4
    • CD56
    • ALK
  • Variable: CD30, CD8 (infrequent)

Differential diagnoses ^[4]

• Monomorphic epitheliotropic intestinal T-cell lymphoma
• Intestinal T-cell lymphoma, not otherwise specified
• Indolent T-cell lymphoproliferative disorder of the GI tract
• NK-cell enteropathy
• Inflammatory GI disorders (e.g., celiac disease, inflammatory bowel disease)

Management ^[4]

EATL has a poor response to available treatment options. ^[4]

• Chemotherapy (e.g., CHOP regimen)
• Autologous stem cell transplant postchemotherapy may improve survival rates.
• Tumor reduction surgery may reduce the risk of chemotherapy-associated complications (e.g., tumor necrosis, peritonitis, GI bleeding).

EATL is often refractory to chemotherapy; the 5-year survival rate is ∼ 10–20%. ^[4]

Epidemiology ^[1][4]

• Peak incidence: 58–62 years
• ♂ > ♀ (2:1)
• Highest incidence in Asian and Hispanic populations

Etiology ^[1][4]

• Etiology is unknown
• No association with celiac disease (formerly known as EATL type II)

Clinical features ^[1][4]

Symptoms are often nonspecific, e.g.:

• Abdominal pain
• Diarrhea
• Weight loss
• GI bleeding
• Intestinal obstruction or perforation (most commonly in the jejunum)

Diagnosis ^[1][4]

Endoscopy with biopsy and histopathology and immunohistochemistry analysis are required for diagnosis.

• Histopathology
  • Extensive infiltration of the intestinal mucosa by monomorphic small to medium-sized cells
  • Cells have clear cytoplasm, round or slightly irregular nuclei with poorly aggregated chromatin, and small nucleoli
  • Less necrosis and inflammatory cell infiltration compared to EATL
• Immunohistochemistry
  • Positive markers
    • CD3
    • CD8
    • CD56
    • CD103
  • Negative markers
    • CD5
    • CD4
  • Variable
    • CD30
    • CD20

Differential diagnoses ^[4]

• Enteropathy-associated T-cell lymphoma
• Anaplastic large cell lymphoma
• Indolent T-cell lymphoproliferative disorder of the GI tract
• NK-cell enteropathy
• Chronic active EBV infection of the GI tract
• Inflammatory disorders (e.g., celiac disease, inflammatory bowel disease)

Management ^[4]

MEITL has a very poor response to available treatment options. ^[4]

• Chemotherapy: CHOP regimen
• Autologous stem cell transplant after chemotherapy may improve survival rate.
• CNS prophylaxis may be considered. ^[4]

One third of tumors are advanced upon diagnosis; the survival rate at 5 years is ∼ 30%. ^[4]

Epidemiology ^[1][2]

• Primary GI mantle cell lymphomas (MCL) are rare.
• GI involvement in systemic MCL occurs in up to 90% of patients. ^[2]

Clinical features ^[1]

Patients may be asymptomatic or present nonspecific features, e.g.:

• Lymphadenopathy
• Constitutional symptoms
• Multiple intestinal polyposis

Diagnosis ^[1][2]

• Endoscopy: multiple intestinal polyps, ulcerations, mucosal protrusion
• Histopathology
  • Diffuse infiltration of monomorphic small-sized to medium-sized cells arranged in a nodular or mantle-zone pattern
  • Cells have irregular nuclear borders, small nucleoli, and scant cytoplasm.
• Immunohistochemistry
  • Positive markers
    • CD5
    • Cyclin D1
    • SOX11
  • Negative markers
    • CD10
    • CD23
• Cytogenetics: t(11;14)(q13;q32) is present in > 95% of patients. ^[1]

Differential diagnoses ^[1]

• Follicular lymphoma
• MALT lymphoma
• Adenomatous polyposis syndromes

Management ^[2]

Tumors are aggressive, with poor response to treatment.

• Chemotherapy (e.g., combination regimens containing cytarabine, R-CHOP).
• Autologous hematopoietic stem cell transplant and/or rituximab may be offered as consolidation therapy.