Multiple myeloma is a cancer of plasma cells that results in overproduction of abnormal antibodies in the bone marrow. It commonly causes bone pain, fractures, anemia, and kidney problems. Risk factors include age over 60 and exposure to chemicals like pesticides, radiation, or certain industrial chemicals. Treatment may include chemotherapy, steroids, stem cell transplantation, radiation, surgery, and newer drugs like thalidomide, lenalidomide, and bortezomib to improve outcomes. Despite recent advances, multiple myeloma remains incurable and patients often relapse, highlighting the need for additional therapeutic options.
2. 2
Cancer of plasma cells.
Malignanat B cell lymphoproliferative disorder of the
marrow with plasma cell predominating.
Most common primary malignancy of bone.
Plasma cells come from B lymphocytes, and produce
antibodies (immunoglobulins).
Myeloma cells produce abnormal immunoglobulins.
– Overproduce monoclonal protein or paraprotein.
– Ineffective immunoglobulins.
– Leads to decreased bone marrow function.
– Destruction of bone tissue.
3. Incidence
• Increases with age
– Ages from 5th to 7th
decade
• Males > Females (2:1)
• Any pt > 40 yrs with new bone tumor should include in d/d of
MM and metastatic carcinoma,
• Accounts for about
– 1% of all malignancies in whites
– 13% of all hematologic cancers in whites
4. RISK FACTORS
• Age >60.
• Exposure to pesticides ( DDT ).
• Radiation
• Wood,leather,sheet metal & nuclear industry
worker
• Exposure to ptroleum products (Benzene)
• Kaposi’s sarcoma Herpes Virus(Presence of IL-
6 and HHV8 )
5. MULTIPLE MYELOMA: Pathophysiology
The pathological and clinical features of
myeloma are due to:
• 1. Tissue infiltration
• 2. Production of large amount of paraprotein
• 3. Impairment of immunity.
11. • May be symptomatic or asymptomatic.
• Symptomatic myeloma characterized by presence of ROTI
and CRAB.
• Myeloma Related Organ or Tissue Impairment.
• Calcium levels increased
• Renal failure
• Anemia
• Bone lesion
12. • FBC- normal or low.
• ESR, CRP-almost always raised.
• Blood film- Rouleaux formation, macrocytosis.
• U&Es, Cr-renal failure
• Serum B2 microglobulin >2.5mg/L.
• Raised LDH
• Serum calcium- normal or raised.
• Serum ALP-normal
• Total protein-normal or raised.
• Serum albumin- normal or low.
• SPE- monoclonal band.
• Serum free light chain assay
• Uric acid-normal or raised
• 24-hour urine electrophoresis and immunofixation is used for
assessment of light-chain excretion.
• Bone marrow aspirate or trephine shows characteristic infiltration by
plasma cells .Amyloid may be found.
13. 1) Xrayz
- Multiple punched out sharply demarcated
purely lytic lesion without any srrounding
rective sclerosis.
- Lack of reactive bone formation
2) Immunochistochemistry
- +ve for CD 56
3)Monocolnal gammopathy
14. • In Monoclonal gammopathies &
Myeloma the single clone of plasma
cells produce a homogeneous
monoclonal immunoglobulin ( M
protein) characterized by the presence
of a sharp, well-defined band with a
single heavy chain and a similar band
with a kappa or lambda light chain
• The M protein is identified as a narrow
peak or "spike" in the g, ß or a 2 regions
19. Stage
International Staging System
Criteria
I β2-microglobulin < 3.5; albumin ≥ 3.5
II Neither stage I nor stage III values
III β2-microglobulin > 5.5
Staging:
Durie-Salmon system: widely used since
1975
Stage based on M-protein levels, bone
lesions, Hb values, serum calcium—many
variables
International Staging System
Simplified staging based on serum β2-
microglobulin
20. Staging
• Salmon-Durie staging system for multiple myeloma
• Stage I
– Hemoglobin level greater than 10 g/dL
– Calcium level less than 12 mg/dL
– Radiograph showing normal bones or solitary plasmacytoma
– Low M protein values (ie, IgG <5 g/dL, IgA <3 g/dL, urine <4 g/24 h)
• Stage II
– Findings that fit neither stage I nor stage III criteria
• Stage III
– Hemoglobin level less than 8.5 g/dL
– Calcium level greater than 12 mg/dL
– Radiograph showing advanced lytic bone disease
– High M protein value (ie, IgG >7 g/dL, IgA >5 g/dL, urine >12 g/24 h)
• Subclassification A involves a creatinine level less than 2 g/dL.
• Subclassification B involves a creatinine level greater than 2 g/dL.
• Median survival is as follows:
– Stage I, >60 months
– Stage II, 41 months
– Stage III, 23 months
21. Diagnosis
• The classic triad of myeloma
– Marrow plasmacytosis (>10%)
– Lytic bone lesions
– Serum and/or urine M component
• The diagnosis may be made in the absence of bone
lesions if the plasmacytosis is associated with a
progressive increase in the M component over time
or if extramedullary mass lesions develop
22. Confirmation of 1 major and 1 minor criterion
or 3 minor criteria in symptomatic patients
Major Diagnostic Criteria Minor Diagnostic Criteria
Biopsy-proven
plasmacytoma
Bone marrow sample =
10% to 30% plasma cells
Bone marrow sample =
30% plasma cells
Minor monoclonal
immunoglobulin levels in
blood or urine (< 3 g/dL)
Elevated monoclonal
immunoglobulin levels in
blood or urine
Osteopenia/lytic bone
lesions (confirmed through
imaging studies)
Abnormally low antibody
levels (not associated with
malignant cells) in the blood
23. Slowly evolving cancer
• MGUS
Monoclonal Gammopathy of Unknown
Significance
• Asymptomatic myeloma
• Symptomatic myeloma
24. Myeloma classification
Monoclonal Gammopathy of Undetermined Significance
Serum M-protein < 3 g/dL
Bone marrow plasma cells < 10%
Absence of anemia, renal failure, hypercalcemia, lytic bone lesions
Asymptomatic Multiple Myeloma
Smoldering Multiple Myeloma Indolent Multiple Myeloma
Serum M-protein > 3 g/dL and/or
bone marrow plasma cells ≥ 10%
Bone marrow plasmacytosis
No anemia, renal failure,
hypercalcemia, lytic
bone lesions
Mild anemia or few small lytic bone
lesions
Stable serum/urine M-protein
No symptoms
Presence of serum/urine M-protein
Symptomatic Multiple Myeloma
Bone marrow plasmacytosis (> 10%)
Anemia, renal failure, hypercalcemia, or lytic bone lesions
26. Bad prognosis if…
• Raised B2-microglobulin >4.
• Low serum albumin <3g/dl.
• Cytogenetics –ch13 deletion, hypodiploidy,
T(4:14)
• Raised LDH, CRP, Cr.
• Low platelet <150 and Hb<100.
• Bone marrow plasma cell percentage ≥ 50%
• Age >70.
27. Goals of MM Therapy
Goals of treatment
Address pain relief & other disease
symptoms
Control disease activity
prevent further organ damage
Debulk tumor and use internal fixation
augmented with methacrylate
Joint arthoplasty
Prolong overall survival
Preserve normal performance
29. • Radiotherapy
• Surgery
• Bone care – bisphosphonates
• Transfusions
• Growth factors
• Treatment and prevention of infections
• Monitoring, management and prevention of
s/e
Other treatment / Supportive care
30. Management of Complications
• UREMIA: rehydratation, diuretics,steroids,antibiotics if renal
infection is suspected, hemodialysis if these measures fail.
• HYPERCALCEMIA: rehydratation, steroids, bisphosphonates,
diuretics.
• PARAPLEGIA: decompressive laminectomy, radiotherapy,
chemotherapy.
• BONE LESIONS: if painful and localised, chemo or local radio-
therapy, analgetics, biphosphonates.
• SEVERE ANEMIA: transfusions, erytropoetin
• HYPERVISCOSITY SYNDROME: plasmapheresis, correction of
hypercalcemia.
• BLEEDING: platelet concentrates, fresh frozen plasma
31. Current Frontline Options
•Examples of current Novel agent combinations:
•Thalidomide based : TD, CTD, MPT
•Bortezomib (Velcade) based: Vdex, VMP, CVD,
PAD, VRD
•Lenalidomide (Revlimid) based: LenDex, Lendex
33. 33
Recent Clinical Data: VISTA
VMP (Velcade+Melphalan+Prednisolone) significantly prolongs
survival in the largest MP-based phase III study
Consistency of treatment effect
Rapid and durable responses with very high Complete
Response rate (similar to transplantation)
Prolonged Time To Progression
VMP consistently superior across all prognostic subgroups
including patients with poor prognostic characteristics
VMP well tolerated
Results establish VMP as a new standard of care for MM patients not
eligible for HDT-ASCT, based on the highest level of evidence1
1. Anderson et al. Leukemia 2008;22:231-9.
34. Multiple Myeloma: Current Status
Relapsed Disease
• Transient Response to Therapy
• Survival 1-3 years
Diagnosis
• Survival 3-5 yrs
• Survival <12mo without therapy
Relapsed and
Refractory
• Resistant to all therapy
• Universally fatal
• Survival 6-9 months
First-Line:
• VAD
• MP
• Transplant (depending on age)
5-year Mortality: 75%; 10-year Mortality: 95-98%
Second Line:
• VAD
• Dexamethasone
• Thalidomide
• Transplant
• Investigational Therapy
Refractory:
• Supportive or palliative care
• Investigational Therapy
• Deaths 12,000/yr.
50 - 75% Response Rate
All patients relapse
Unmet Medical Need
Choice of therapy at relapse dependent on
duration of response & previous therapies.
Response rate & duration reduced with each
sequential regimen
35. Hope
New drugs on the horizon
• Carfilzomib
• Pomalidomide
• Panobinostat
• Vorinostat
• Elotuzumab
Old drugs with new use
• Bendamustine
Notas do Editor
(Only 2 to 3 percent of cases are reported in patients &lt; 30 years)