Overview of Lymphomas

1. Overview of Lymphomas Jessica Hals, DO June 16th 2005

3. Definition • Lymphomas are malignant transformations of normal lymphoid cells which reside predominantly in lymphoid tissues • They are divided into two major types: • Non-Hodgkin’s lymphoma (NHL) • Hodgkin’s Lymphoma

4. Some Stats1 • It is estimated that there will be 63,740 new cases of lymphoma diagnosed in 2005. • 56,390 are expected to be NHL • 19,200 of these pts are expected to die from NHL • 7,350 are expected to be Hodgkin’s Lymphoma • 1,410 of these pts are expected to die

5. How to Diagnosis NHL • The initial evaluation must establish: • The precise histologic type of NHL • The extent and sites of disease • The performance status of the patient • All of this is important to establish prognosis and treatment

6. Where to start • As always with the H&P: • Key points to obtain in your “history”: • Lymphadenopathy: more than 2/3 of pt will present with peripheral adenopathy • Ask about waxing and waning of lymph nodes • As about the duration of lymphadenopathy

7. The History Cont’d • B Symptoms: • Fever defined as T>38ºC • Weight loss defined by unexplained loss of >10% of body wt over 6 mos • Night sweats defined by drenching night sweats

8. The Physical Exam • Exam all sites of potential involvement including: • Waldeyer’s ring (tonsils, base of tongue, nasopharynx) • Std L.N. sites (cervical, inguinal, etc) • Liver and spleen • Abdominal L.N. (mesenteric, retroperitoneal) • Others: occipital, preauricular, epitrochlear, etc.

9. Unusual Sites/Presentations • 10-35% will have primary extranodal NHL and about 50% will have extranodal disease during their illness • Most common site of extranodal disease is the GI tract followed by the skin • Symptoms from extranodal disease usually assoc with aggressive NHL

10. Extranodal Sites • Testicular NHL accounts for ~1% of NHL and 2% of extranodal NHL. It is the most common malign. involving the testis in men over 60 y.o • NHL can present as solitary lesion of bone • Renal involvement occurs in 2-14% of pts • Rarer sites include: prostate, bladder, ovary, orbit, heart, breast, salivary gland, thyroid and adrenal gland • Examine skin carefully and bx any suspicious lesions • NHL can account for poorly differentiated carcinoma of unknown primary

11. Diagnostic tests • Lymph node biopsy • Preferably to have an entire intact lymph node over FNA or core bx • This allows the pathologist to accurately determine the pattern of involvement and allows for enough tissue for immunologic and molecular testing

12. Tests Cont’d • Bone marrow bx • This is to determine stage • Controversial whether bilateral or unilateral bx’s are required. • Most oncologists advocate bilateral biopsy

13. Lab tests • CBC • Serum chemistries • LDH • Uric acid

14. Imaging tests • CT chest/abd/pelvis • PET scan

15. Classification3

16. Staging3

17. Prognostic Tools3

18. The FLIPI Score • The IPI was designed for aggressive lymphomas. Few Follicular lymphomas fell into the high risk group based upon the IPI and therefore it’s application to FL was being questioned • Therefore the FLIPI has been proposed as a prognostic score for follicular lymphomas

19. FLIPI • Five factors: • Age >60 • Ann Arbor stage III or IV • Hb <12g/dL • Number of nodal areas >4 • LDH >ULN

20. FLIPI Risk Groups • Low risk: 0-1 adverse factor (5 &10yr OS=91% & 71% respectively) • Intermediate Risk: 2 adverse factors (5&10yr OS=78% & 51% respectively) • High risk: 3 or more (5&10 yr OS=52% &36% respectively)

22. Aggressive NHL3

23. Tx Aggressive NHL • Are highly curable lymphomas • If early disease present (localized, non-bulky stage I or II) may use XRT only for cure • However, most advocate combined therapy for early stage disease

24. Historical tx of aggressive NHL • In 1972 Levitt, et al reported curability of large cell NHL with combination chemo2 • In 1975 DeVita et al described curing pts using COPP (Cytoxan, adriamycin, vincristine, procarbazine and prednisone)2 • During the 70’s this regimen was simplified to the classic CHOP regimen we use today (Cytoxan, adriamycin, vincristine and prednisone)

25. TX of Early Stage • A SWOG protocol randomized pts to either 3 cycles of CHOP followed by involved field XRT vs. 8 cycles of CHOP alone3 • This showed that pts had a better 5 yr. PFS and OS with combined therapy • 76% vs. 67%, PFS respectively • 82% vs. 74%, OS respectively

26. Early Stage Cont’d • The GELA trial2: • A French group has investigated a more intensive chemo regimen. They randomized pts to either 3 cycles of CHOP with XRT vs. ACVBP (adriamycin, Cytoxan, vindesine, bleomycin, prednisone followed with consolidation with ifosfamide, VP-16 and AraC) • This new regimen did improve EFS and OS, but at significant toxicity

27. Early Tx Summary • For most patients with early, non-bulky (<10cm) stage I or II, 3 cycles of CHOP followed by involved field XRT is std • The role of using rituximab in early stage is gaining evidence: • Early studies suggest a benefit to adding rituximab to chemotherapy

28. Advanced Stage Tx • CHOP is still the most commonly used regimen, and now with the addition of rituximab • Several groups are investigating more aggressive chemo regimens • Here are a few:

29. The German group2 • They divided pts into three groups: young good px, young poor px, and elderly • They then randomized pts to one of four arms: • Arm 1: CHOP 21 (traditional 21 day cycle) • Arm 2: CHOP 14 (14 day cycle of CHOP) • Arm 3: CHOEP 21 (CHOP+VP-16 q 21 days) • Arm 4: CHOEP 14 (above q 14 days)

30. The German Results • CHOEP 21 improved EFS, but CHOP 14 and CHOEP 14 improved EFS, CR and OS over std CHOP 21 • The Germans now consider CHOEP 14 preferred chemo for young good px pt • Based on the results of the MInT tx in young good px pts (CHOP-like chemo w/ Rituxan), they also will add Rituxan to their chemo • They are also using this same regimen for young poor px pts

31. The French Approach3 • Study randomized pts to 3 cycles CHOP +XRT vs. 3 cycles ACVBP followed by consolidation. • EFS (82% vs. 74%), OS (90% vs. 81%) were in favor of the chemo only arm • Ongoing study using above +Rituxan

32. The North Americans • CHOP+Rituxan considered std of care • Trials are ongoing to improve outcomes

34. Indolent NHL • Follicular lymphoma is most common type of indolent NHL • Majority of pts present w/ stage III/IV disease with multiple enlarged LN that have been present for a long time • Generally not considered curable

35. Natural Hx of Indolent NHL • Can have long symptom free intervals • Several studies show no OS advantage to early treatment vs. waiting until progression or symptoms develop. • Can go for years w/o needing tx. and obs alone is a feasible approach. Median survival for stage III/IV is 7-10 yrs

36. Tx Early Stage I/II indolent NHL • For stage I/II XRT may be reasonable sole tx

37. Tx for advanced disease • Chemotherapy remains the mainstay of treatment. • Various regimens exist • CVP, Fludarabine, FC, FCR, CVP-R • All appear to have same RR • Rituximab can be used alone or in combo w/ other regimens • Radio-labeled monoclonal antibodies are also available for refractory/relapsed disease (Bexxar and Zevalan) • Transplantation has been investigated for relapsed disease

38. Summary of Tx Indolent NHL

39. Tx summary Cont’d

40. Marginal Zone Lymphomas (MZL) • 3 main types: • Splenic • MALT lymphoma • Nodal • Can occur in GI tract, salivary glands, thyroid, orbit, conjunctiva, breast and lung • Surgery or XRT usually sufficient to treat

41. Splenic lymphoma • <5% NHL • Median age 65 • Present w/ splenomegaly, lymphocytosis • Course is indolent. Survival 70% @10yr • Tx of choice is splenectomy

42. MALT lymphomas • Extranodal lymphoma associated w/ mucosal tissue • ~5% of NHL, 50% of these are gastric • Most are stage I/II at presentation • Gastric MALTomas assoc w/ H.pylori infection. Tx w/ Abx causes regression of lymphoma in majority of cases • XRT or resection can be used for other sites of MALToma

43. Extra-nodal MZL • Are extremely rare • Usually indolent • Surgery can be used w/ or w/o XRT

44. Mantle Cell Lymphoma • Considered intermediate aggressive. Median survival is 3-4 yrs. • Median age of 63 w/ male predominance. • Usually stage IV at dx • Distinctive features include: Cyclin D1+ and t(11:14)

45. Tx Mantle Cell Lymphoma • CVP (Cytoxan, vincristine, prednisone) • Hyper-CVAD (mtx, adriamycin, Cytoxan, vincristine, dexamethasone, AraC-C) w/ and w/o rituximab has also been used. • Relapses are common even after BMT

47. AID-related lymphomas • AIDS defining malignancies: • Kaposi’s sarcoma, NHL, primary CNS lymphoma, invasive cervical carcinoma • AIDS related NHL: • Primary CNS lymphoma (PCNSL) • Systemic NHL • 1º effusion NHL

48. HIV related NHL • Usually in pts w/ CD4 count <100cell/µL • High grade NHL, (diffuse large B cell immunoblastic variant or Burkitt’s lymphoma are most common) • Indolent NHL are much less common • Most present w/o adenopathy and w/ stage IV dz.

49. TX systemic AIDS related NHL • “std” chemo considered CHOP, although there is controversy. • Rituximab is investigational but early studies suggest synergism • HAART therapy should be continued or initiated • These pts do worse than in HIV(-) pts

50. PCNSL in HIV • Usually w/ CD4 counts <50cell/µL • Present w/ focal or non-focal neurological symptoms: • confusion, lethargy, memory loss, hemiparesis, aphasia, and/or seizures that have usually been present for less than three months • DX w/ MRI/LP/EBV DNA in CSF/brain bx/rule out toxoplasmosis