Features:
- Contiguous spread, bimodal (30s, 50s), more curable
Investigations:
- Excisional biopsy: Reed-Sternberg cells
- PET/CT: Staging
Treatment:
- Stage IIA↓: Radiation
- Stage IIB↑: ABVD chemotherapy ± radiation (bulky disease)

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Non-Hodgkin Lymphoma (NHL)

Features:
- Haematogenous spread, less B symptoms
- Extranodal involvement: GI, mediastinal, skin, Waldeyer’s ring
Subtypes:
- MALT lymphoma (H. pylori-related), Burkitt’s lymphoma
Investigations:
- Excisional biopsy (not FNA)
- PET/CT: Staging
Treatment:
- Stage IIA↓: Radiation
- Stage IIB↑: R-CHOP chemo
- H. pylori eradication for early MALT lymphoma

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Complications

Lymphoma

Risk Factors

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Pathophysiology

Malignant proliferation of lymphocytes (B, T, or NK cells)
In Hodgkin Lymphoma (HL), EBV can drive B-cell dysregulation with Reed-Sternberg cells
Non-Hodgkin Lymphoma (NHL) often involves more diverse genetic/epigenetic mutations leading to abnormal lymphocyte proliferation

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Presentation

Lymphadenopathy
- HL: Often painless, contiguous spread, commonly cervical or mediastinal nodes
- NHL: Widespread nodal involvement, can be peripheral or central, often non-contiguous spread
B Symptoms (fever >38°C, night sweats, weight loss >10% in 6 months)
- More common in classical HL but can occur in high-grade NHL
- Important for Ann Arbor staging classification
Extranodal Disease
- NHL commonly affects GI tract (e.g. MALT lymphoma), skin, bone marrow, CNS
Mediastinal Mass
- May cause cough, chest discomfort, SVC syndrome (facial swelling, venous engorgement)
Other Signs
- Fatigue, pruritus, recurrent infections (immune dysfunction), or organ-specific symptoms if infiltration (e.g. hepatic, splenic)

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HODGKIN LYMPHOMA (HL)

Features

Often affects younger adults (bimodal peaks: 30s and 50s)
Characterised by Reed-Sternberg cells (large, binucleate B cells) on excisional biopsy
Typically spreads contiguously from one lymph node region to adjacent areas
Generally higher cure rates compared to most NHL subtypes

Investigations

Excisional Lymph Node Biopsy: To identify Reed-Sternberg cells and classify HL subtype (e.g. nodular sclerosis, mixed cellularity)
Baseline Staging
- PET/CT scan for both staging and assessment of metabolic activity
- FBC, ESR, LDH, albumin, LFTs, renal function, HIV status
- Bone marrow biopsy if indicated by PET findings or advanced disease

Treatment

Early Stage (I–II)
- Often combined modality: ABVD (Adriamycin, Bleomycin, Vinblastine, Dacarbazine) for 2–4 cycles plus involved-site radiotherapy (especially bulky disease)
- Stage IIA disease might receive fewer chemo cycles plus radiation
Advanced Stage (IIB–IV)
- ABVD for more cycles or escalated BEACOPP in high-risk disease
- Radiotherapy to bulky sites if needed
Prognosis
- Generally excellent long-term survival in early stage
- Late toxicity includes secondary malignancies (breast, lung), cardiac or pulmonary complications

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NON-HODGKIN LYMPHOMA (NHL)

Features

Diverse group with various histologies: Indolent (follicular, MALT) vs Aggressive (diffuse large B-cell lymphoma [DLBCL], Burkitt’s)
More common than HL, typically non-contiguous spread
B symptoms less consistent but present in aggressive subtypes
Extranodal involvement (GI tract, skin, CNS, Waldeyer’s ring, bone marrow)

Subtypes

MALT Lymphoma
- Often gastric, associated with H. pylori infection
- Early stage may resolve with H. pylori eradication
Burkitt’s Lymphoma
- Highly aggressive, c-myc translocation
- Associated with EBV in endemic (African) form
Diffuse Large B-Cell Lymphoma (DLBCL)
- Most common aggressive NHL in adults
- Presents with rapidly enlarging mass, can involve extranodal sites

Investigations

Excisional Biopsy (preferred) or core biopsy for histological diagnosis
PET/CT for staging and treatment response
Bone Marrow Biopsy if suspicion of marrow involvement
Lab Tests: FBC, LDH (prognostic marker), LFTs, renal function, HIV, hepatitis B/C screening

Treatment

Early Stage (I–II)
- Involved-field or involved-site radiotherapy ± short-course chemo (e.g. R-CHOP for DLBCL)
- Indolent lymphoma (e.g. follicular) can be treated with radiotherapy alone in localised disease
Advanced Stage (≥IIB)
- R-CHOP (Rituximab, Cyclophosphamide, Doxorubicin, Vincristine, Prednisolone) mainstay for B-cell lymphomas
- Intensive regimens (e.g. Hyper-CVAD, CODOX-M/IVAC) for high-grade subtypes (Burkitt’s)
- Consider autologous stem cell transplant in refractory or relapsed disease
H. pylori-Positive MALT
- Eradication therapy (PPI + clarithromycin + amoxicillin/metronidazole) may induce remission in early gastric MALT

Complications

Tumour Lysis Syndrome
- High cell turnover (especially Burkitt’s, DLBCL)
- Prophylaxis with IV fluids, allopurinol or rasburicase
SVC Syndrome
- Mediastinal mass compresses the superior vena cava → facial swelling, distended neck veins
- Urgent treatment with steroids or radiotherapy to relieve obstruction
Infections
- Immunosuppression from disease or therapy (e.g. neutropenia, hypogammaglobulinaemia)
- Prophylactic antimicrobials or IVIG in select cases
Bone Marrow Failure
- Anaemia, neutropenia, thrombocytopenia
- May require transfusions, growth factors, or dose adjustments
CNS Involvement
- More common in aggressive subtypes (DLBCL, Burkitt’s)
- Prophylactic intrathecal chemo if high risk (testicular involvement, high IPI score)

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Follow-Up and Survivorship

Response Evaluation
- Repeat PET/CT after therapy to assess remission or persistent disease
- Physical exams and blood tests at regular intervals (every 3–6 months initially)
Long-Term Monitoring
- Look out for late relapses, secondary malignancies, cardiac/pulmonary toxicity (anthracyclines, bleomycin)
- Encourage vaccination (influenza yearly, pneumococcal, avoid live vaccines if immunosuppressed)
- Lifestyle advice (no smoking, manage CV risk factors)
Fertility
- Consider fertility preservation prior to chemo (sperm/egg freezing)
Palliative Care
- For refractory or relapsed disease, symptom control and quality of life remain priorities

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Notes:

Suspect lymphoma in patients with unexplained lymphadenopathy (especially >2 cm, persistent >4 weeks), B symptoms, or mediastinal masses
Excisional lymph node biopsy is crucial for histological classification (FNA not sufficient)
Prompt referral to haematology/oncology for staging and management if suspicion is high
Monitor for acute complications (TLS, SVC syndrome) and coordinate supportive care
Emphasise adherence to follow-up: cure rates can be high in some subtypes (HL, DLBCL) but vigilant post-treatment surveillance is essential

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