Management of multiple myeloma in older people

SummaryMultiple myeloma is a neoplastic proliferation of a plasma cell clone that produces a monoclonal immunoglobulin. It is one of the most common haematological malignancies and the incidence increases with age, with a median age at diagnosis of 65–70 years. The diagnosis of multiple myeloma requires the presence of ≥10% plasma cells in the bone marrow and an M-protein in serum and/or urine. Cytogenetic status, serum β2-microglobulin and response to therapy are the key prognostic factors. Treatment is necessary for the patient diagnosed with symptomatic multiple myeloma, with organ damage. Patients older than 65 years are ineligible for autologous transplantation. The introduction of novel agents, such as thalidomide, bortezomib and lenalidomide, have changed the management of myeloma and extended overall survival. However, in older patients the results are not as satisfactory and treatment strategies have to be individualized to improve tolerability and optimize efficacy.

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A Rare Pulmonary Manisfestation of Kahler's disease

Journal of Medical Research and Innovation ◽

10.15419/jmri.115 ◽

2018 ◽

pp. e000115

Author(s):

Gaurav Baheti ◽

Ankur Jain

Keyword(s):

Multiple Myeloma ◽

Plasma Cells ◽

Organ Damage ◽

M Protein ◽

Light Chains ◽

Primary Malignancy ◽

Myeloma Cells ◽

Abnormal Growth ◽

Excess Amount ◽

Monoclonal Immunoglobulins

Kahler's disease also known as Multiple Myeloma (MM) is one of the most dangerous primary malignancy of the bone marrow which is significant for its plasma cells proliferation and abnormal growth of monoclonal immunoglobulins (including M protein and light chain proteins: κ and λ). Excess amount of M protein is a potential blood thickener due to its effects on viscosity, while an excess amount of light chains could lead to an end-organ damage. MM presenting as Interstital Lung Disease (ILD) has been documented in very rare occasions till date and hence, we are presenting forward a letter showing the importance of considering MM as a differential when a patient presents with ILD features by presenting one such case of a patient who was diagnosed with MM and developed ILD secondary due to infiltration of Myeloma cells in the parenchyma of the lungs.

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Smoldering Multiple Myeloma

BioMed Research International ◽

10.1155/2015/623254 ◽

2015 ◽

Vol 2015 ◽

pp. 1-7

Author(s):

Minjie Gao ◽

Guang Yang ◽

Yuanyuan Kong ◽

Xiaosong Wu ◽

Jumei Shi

Keyword(s):

Multiple Myeloma ◽

Early Treatment ◽

Plasma Cells ◽

Intermediate Stage ◽

Organ Damage ◽

M Protein ◽

Smoldering Multiple Myeloma ◽

Risk Of Progression ◽

Bone Marrow Plasma ◽

Peripheral Blood Plasma

Smoldering multiple myeloma (SMM) is an asymptomatic precursor stage of multiple myeloma (MM) characterized by clonal bone marrow plasma cells (BMPC) ≥ 10% and/or M protein level ≥ 30 g/L in the absence of end organ damage. It represents an intermediate stage between monoclonal gammopathy of undetermined significance (MGUS) and symptomatic MM. The risk of progression to symptomatic MM is not uniform, and several parameters have been reported to predict the risk of progression. These include the level of M protein and the percentage of BMPC, the proportion of immunophenotypically aberrant plasma cells, and the presence of immunoparesis, free light-chain (FLC) ratio, peripheral blood plasma cells (PBPC), pattern of serum M protein evolution, abnormal magnetic resonance imaging (MRI), cytogenetic abnormalities, IgA isotype, and Bence Jones proteinuria. So far treatment is still not recommended for SMM, because several trials suggested that patients with SMM do not benefit from early treatment. However, the Mateos et al. trial showed a survival benefit after early treatment with lenalidomide plus dexamethasone in patients with high-risk SMM. This trial has prompted a reevaluation of early treatment in an asymptomatic patient population.

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Reduction In Proliferative Rate of Myeloma Plasma Cells Measured by the Plasma Cell Labeling Index Predicts Improved Survival In Multiple Myeloma

Blood ◽

10.1182/blood.v116.21.4048.4048 ◽

2010 ◽

Vol 116 (21) ◽

pp. 4048-4048

Author(s):

Jeremy T Larsen ◽

Cheng E. Chee ◽

John Lust ◽

Philip R. Greipp ◽

S. Vincent Rajkumar

Keyword(s):

Multiple Myeloma ◽

Overall Survival ◽

Mayo Clinic ◽

Plasma Cells ◽

Initial Therapy ◽

Response To Therapy ◽

Cell Labeling ◽

M Protein ◽

Response Criteria ◽

Proliferative Rate

Abstract Abstract 4048 Background: The plasma cell labeling index (PCLI) is measured as the percentage of bone marrow plasma cells (PC) in the S phase of the cell cycle and provides an estimate of the proliferative capacity of malignant PC in multiple myeloma (MM). The International Myeloma Working Group (IMWG) uniform response criteria measure the monoclonal (M) protein and serum free light chain (FLC) assay to evaluate clinical response. An elevated PCLI is an established adverse prognostic risk factor for survival, however it is unknown if the PCLI response to therapy offers further prognostic value. Methods: Data from 176 newly diagnosed MM patients from 1985 to 2005 were collected from the Mayo Clinic dysproteinemia database. Inclusion criteria for the study required a minimum initial PCLI of 0.5% and a subsequent PCLI 4 months after initiation of therapy. Baseline and subsequent serum M-protein, progression date, and overall survival were recorded. Clinical responses were assessed by the IMWG uniform response criteria. The association of PCLI response and treatment response (CR, VGPR, or PR) was assessed univariately. Overall survival based on PCLI response, M-spike reduction, and treatment response by IMWG criteria was estimated using the Kaplan-Meier method. Results: The median overall survival (OS) was 47 months (range: 4 – 165). Ninety-four patients (53%) demonstrated a ≥60% reduction in PCLI after initial therapy (responders) and this conferred a significant OS advantage of 51 months vs. 34 months (P<0.01; Figure 1) compared to those who achieved <60% PCLI reduction (non-responders) after initial therapy. The median PCLI percent difference following 4 months of therapy was -67% (+/− 137%; range: -100 to 953%). When patients were stratified into high (PCLI of ≥3%), intermediate (PCLI ≥1%) and low (PCLI <1%) risk groups, OS was significantly improved in the high and intermediate PCLI groups if they achieved ≥60% reduction in PCLI after initial therapy, 31 vs. 7 months (P<0.0022; Figure 2) and 63 vs. 25 months (P<0.0005; Figure 3), respectively. As observed in prior studies, patients with PCLI of ≥3% at diagnosis had shorter overall survival (17 months) when compared to patients with an initial PCLI of <1% (61 months; P < 0.0001). Of the 94 responders, 39% (n=37) did not achieve a response to therapy as measured by M-protein. Thirteen patients (14%) had no measurable serum M-protein at baseline. Conversely, 35% (n=31) of patients that responded by M-protein criteria did not achieve a PCLI response. In patients who achieved CR/PR after 4 months of therapy, the median PCLI reduction was 83.7% vs. 22.5% (P <0.0004) compared to patients with stable disease (not meeting criteria for CR or PR) or progressive disease (as specified by IMWG response criteria). This reflects a significant reduction in disease burden and as expected, median OS was better in the CR/PR group (53 vs. 31 months, P <0.0016). Conclusion: Our study demonstrates that the degree of PCLI reduction after therapy is important in predicting overall survival and response to therapy. This is an important finding in the current setting of effective MM treatment options, whereby patients who do not achieve an adequate response as defined as ≥60% reduction in PCLI in our study, may require change in therapy. Our data confirm that reduction of M-protein is an important surrogate endpoint, as patients who achieved PR and CR lived significantly longer. A significant portion of individuals 39% had a measurable response by PCLI that was not detected by M-protein. Further studies are needed to evaluate the predictive value of the addition a criterion that looks at reduction in proliferative rate as measured by PCLI or other methods such as flow cytometry. Disclosures: Greipp: Mayo Clinic: Patents & Royalties.

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Multiple myeloma and related conditions

10.1093/med/9780199568741.003.0290 ◽

2018 ◽

Author(s):

Graham Collins ◽

Chris Bunch

Keyword(s):

Multiple Myeloma ◽

Bone Marrow ◽

Monoclonal Gammopathy ◽

Plasma Cells ◽

Cell Clone ◽

Bone Marrow Failure ◽

Organ Damage ◽

End Organ Damage ◽

Clonal Proliferation ◽

Uncertain Significance

Multiple myeloma is a cancerous disorder of the bone marrow and arises from a clonal proliferation of plasma cells, resulting in end-organ damage (e.g. renal failure, hypercalcaemia, bone disease, and bone marrow failure). When a plasma cell clone is only detected in one site (either bony or soft tissue), it is termed a plasmacytoma. Monoclonal gammopathy of uncertain significance is also a clonal proliferation of plasma cells but, by definition, does not result in end-organ damage. This chapter addresses the diagnosis and management of multiple myeloma.

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Single Arm, Prospective, Open-Label Phase II Trial to Evaluate the Efficacy of Isatuximab in Patients with Monoclonal Gammopathy of Renal Significance

Blood ◽

10.1182/blood-2019-123496 ◽

2019 ◽

Vol 134 (Supplement_1) ◽

pp. 3161-3161 ◽

Cited By ~ 1

Author(s):

Vikram Premkumar ◽

Suzanne Lentzsch ◽

Divaya Bhutani

Keyword(s):

Multiple Myeloma ◽

B Cell ◽

Plasma Cell ◽

Monoclonal Gammopathy ◽

Plasma Cells ◽

Cell Clone ◽

Advisory Committees ◽

Renal Response ◽

Hematologic Response ◽

Stable Renal Function

Background: Monoclonal gammopathy of renal significance (MGRS) is a monoclonal B cell disorder, not meeting the definition of lymphoma or myeloma, that produces monoclonal proteins which deposit in the kidneys. Permanent renal damage can occur either as a consequence of direct deposition of toxic proteins or by an induced inflammatory response. Due to the low burden of the plasma cell clone, patients do not otherwise qualify for potentially toxic anti-plasma cell treatments and treatment is generally based on consensus opinion. To date there are no clinical trials exploring treatment options. Isatuximab is a chimeric mouse/human IgG1k monoclonal antibody which targets CD38 on both malignant and normal plasma cells and exhibits it antitumor effects primarily by antibody-dependent cellular toxicity. Isatuximab has recently been shown to be an active drug in the treatment of multiple myeloma, with improvements seen in hematologic and renal markers, and has been shown to have manageable toxicity. Given the efficacy of isatuximab in multiple myeloma, we propose a trial evaluating isatuximab monotherapy to treat the small plasma cell clone in MGRS with the hopes of maximizing response and minimizing toxicity. Study Design and Methods: The primary objective of this study is to evaluate efficacy of isatuximab monotherapy in patients with MGRS in order to establish a standard of care treatment for patients with this disease. Adult patients with proteinuria of at least 1 gram in 24 hours and a histopathological diagnosis of MGRS on renal biopsy in the last 24 months will be eligible for the trial. Patients will be excluded if their estimated GFR is below 30 mL/min, they have multiple myeloma, high risk smoldering myeloma, other B cell neoplasm meeting criteria for treatment, concurrent diabetic nephropathy, or require dialysis. Patients will be screened for B cell disorders with bone marrow biopsy and aspirate, serum protein electrophoresis (SPEP) with immunofixation (IFE), 24-hour urine protein electrophoresis (UPEP), free light chain (FLC) testing and screening PET/CT at time of enrollment. Enrolled patients will be administered isatuximab 20 mg/kg IV weekly for 4 weeks and then will receive the same dose every 2 weeks thereafter for a total of 6 months. Patients may be continued on treatment following completion of the 6 months at the discretion of the provider. To reduce the risk of infusion related reactions, patients will receive premedications with corticosteroids, diphenhydramine, H2 blockade and acetaminophen at least 60 minutes prior to infusion. Patients will have repeat SPEP + IFE, 24-hour UPEP + IFE and FLC testing every 4 weeks. There will be an optional repeat kidney biopsy 9-12 months following treatment initiation to assess pathologic response in the kidneys. Statistical Methods: The study will be comprised of 20 patients being treated with isatuximab over a span of 24-30 months. Ten patients will be initiated on the therapy for a period of 6 months. Interim analysis will be done after these patients have completed all the treatment cycles. If 4 out of 10 patients show response in form of improved/stable renal function, the study will proceed to include next 10 patients. If >50% of the first group of 10 patients show doubling of creatinine while on therapy, that would be considered as an indication to discontinue the therapy and the study due to drug toxicity. Endpoints: The primary endpoint will be efficacy as measured by renal response and hematologic response. Renal response will be measured by assessing the amount of proteinuria in a 24 hour urine sample. A sustained reduction in proteinuria by 30% from the patient's baseline amount of proteinuria with stable renal function (serum eGFR within 20% of baseline) will be considered a positive renal response. Hematologic response will be quantified per the 2016 International Myeloma Working Group (IMWG) uniform response criteria for multiple myeloma. An important secondary endpoint will be safety and will be analyzed from all patients who receive any study drug. Adverse events will be characterized and graded according to the National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE) version 5.0. Other endpoints include time to dialysis and rate of minimal residual disease (MRD) negativity. Disclosures Lentzsch: Caelum Biosciences: Equity Ownership, Membership on an entity's Board of Directors or advisory committees; Bayer: Consultancy; Janssen: Consultancy; Takeda: Consultancy; BMS: Consultancy; Proclara: Consultancy; Abbvie: Consultancy; Clinical Care Options: Speakers Bureau; Sanofi: Consultancy, Research Funding; Multiple Myeloma Research Foundation: Honoraria; International Myeloma Foundation: Honoraria; Karyopharm: Research Funding; Columbia University: Patents & Royalties: 11-1F4mAb as anti-amyloid strategy. Bhutani:Sanofi: Membership on an entity's Board of Directors or advisory committees. OffLabel Disclosure: Our trial will be evaluating the efficacy of targeting CD38 on plasma cells with isatuximab in patients with monoclonal gammopathy of renal significance (MGRS). We will evaluate the effects of this drug on 24 hour proteinuria and hematologic response.

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Raised ?2-Microglobulin as a Surrogate Marker in Non-Secretory Multiple Myeloma

Bangladesh Journal of Medical Science ◽

10.3329/bjms.v16i1.31146 ◽

2017 ◽

Vol 16 (1) ◽

pp. 142-145

Author(s):

Bimal K Agrawal ◽

Anshul Sehgal ◽

Vikas Deswal ◽

Prem Singh ◽

Usha Agrawal

Keyword(s):

Multiple Myeloma ◽

Bone Marrow ◽

Rare Case ◽

Plasma Cells ◽

Medical Science ◽

Protein A ◽

Surrogate Marker ◽

M Protein ◽

Review Of Literature ◽

Lytic Lesions

Multiple myeloma is a neoplasm of plasma cells in the bone marrow. It is characterised by lytic lesions in the bones, marrow plasmacytosis and presence of M protein in serum and/or urine. Serum ?2 microglobulin is also raised and can be used for classification and prognostication of the disease. In the absence of M protein, the disease is known as non-secretory myeloma. It is proposed that raised ?2 microglobulin can be used for diagnosis and therapeutic guidance in the absence of M protein. A rare case of nonsecretory myeloma with neurocognitive impairment along with review of literature is being presented. The patient had multiple lytic lesions in bones with marked increase in plasma cells in bone marrow. M protein was not detectable in serum or urine but serum ?2 microglobulin was much elevated.Bangladesh Journal of Medical Science Vol.16(1) 2017 p.142-145

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Feline Lymphoplasmacytic Stomatitis Associated with Monoclonal Gammopathy and Bence-Jones Proteinuria

Journal of Veterinary Dentistry ◽

10.1177/089875649401100102 ◽

1994 ◽

Vol 11 (1) ◽

pp. 25-27 ◽

Cited By ~ 4

Author(s):

Kenneth F. Lyon

Keyword(s):

Multiple Myeloma ◽

Oral Cavity ◽

Serum Protein ◽

Monoclonal Gammopathy ◽

Alkylating Agent ◽

Protein Electrophoresis ◽

M Protein ◽

Monoclonal Immunoglobulin ◽

Urine Protein ◽

Bence Jones Proteinuria

Lymphoplasmacytic stomatitis and gingivitis was diagnosed in an 8-year old female domestic shorthair. The cat had evidence of severe generalized inflammation of the oral cavity. Biopsy samples were evaluated and displayed a lichenoid, interface stomatitis which was predominantly lymphoplasmacytic. Serum protein electrophoresis confirmed a monoclonal gammopathy. Urine protein electrophoresis confirmed Bence-Jones proteinuria. Protein electrophoresis was used to diagnose monoclonal gammopathy (the production of a monoclonal immunoglobulin, or paraprotein, which is associated with a characteristic “M” protein spike on serum electrophoresis). Diseases associated with monoclonal gammopathy are similar in the dog and cat. Alkylating agent chemotherapy is used to rapidly reduce paraprotein concentrations in multiple myeloma. Multiple myeloma is the most common disorder associated with monoclonal gammopathy. This condition is less common in the cat, compared to the dog. This report examines the diagnosis and treatment of multiple myeloma in a cat presenting with severe stomatitis.

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Clarithromycin (Biaxin®), Low Dose Thalidomide and Dexamethasone (BLT-D) in Newly Diagnosed and Previously Treated African American Patients with Multiple Myeloma: A Retrospective, Single Institution Experience.

Blood ◽

10.1182/blood.v106.11.3501.3501 ◽

2005 ◽

Vol 106 (11) ◽

pp. 3501-3501

Author(s):

Jack Jacoub ◽

Joao L. Ascensao ◽

Boyer James ◽

Thomas O’Connor ◽

Reema Batra ◽

...

Keyword(s):

Multiple Myeloma ◽

African American ◽

Partial Response ◽

Plasma Cells ◽

Progression Free Survival ◽

Staging System ◽

Stage I ◽

M Protein ◽

Duration Of Treatment ◽

Previously Treated

Abstract Introduction : African-Americans (AA) are twice as likely to develop multiple myeloma (MM) than Caucasians but are largely underrepresented in clinical trials. Thalidmode plus dexamethasone is an established therapy in MM. Biaxin® may augment the efficacy of this combination possibly via potentiating steroid activity (M. Coleman, et al. Leuk Lymphoma 2002, R. Niesvizky, et al. Blood 2003, Abs #832). Methods : We conducted a retrospective review of all AA patients (pts) with symptomatic MM treated with BLT-D from 2002-present. Treatment consisted of Thalidomide 50–200mg daily, Biaxin 500mg twice daily and dexamethasone 40mg weekly. All pts received monthly bisphosphonate therapy and aspirin 81–325mg daily. Response criteria was defined as follows: complete response (CR) = no detectable M-protein, marrow plasma cells <5%; very good partial response (VGPR) = decrease in M-protein by >90%; partial response (PR) = decrease in M-protein by >50%; stable disease (SD) = M-protein decrease by <50% without clinical progression; no response (NR)= progression with no change or increase in M-protein or response <4wks. Progression free survival (PFS) was defined from the start of BLT-D until discontinuation or change in therapy due to progressive disease as clinically indicated. Toxicity was graded according to WHO criteria. Results :15 pts received BLT-D and their characteristics were as follows: all were males; median age 66 (range 30–78); IgG=53%, IgA=20%, light chain only=27%; Durie-Salmon stage I=20%, II=33%, III=47%; International Staging System stage I=20%, II=47%, III=13%, undefined = 20%; 7 were previously treated (5 pts had 1 prior regimen, 2 pts had ≥2 prior regimens). In previously treated pts (n=7) responses were as follows: no CR, 2 VGPR (28%), 3 PR (43%), 1 SD (14%) and 1 NR (14%) for an overall response rate (ORR) of 87%. Their duration of treatment ranged from 4–32 mos and median PFS in responders (VGPR+PR+SD) was 29.5 mos (range 23–35). 3 pts had BLT-D discontinued after 12–15 months of therapy and remained in stable plateau phase off therapy for > 1 year; one was referred for ASCT after 14 mo; one continues stable at 15 mo and the third relapsed at 12 months but failed to respond again to BLT-D. Responses in treatment naive pts (n=8) were as follows: no CR, 3 VGPR (38%), 1 PR (13%) and 2 SD (25%), 2 NR (25%) for an ORR of 75%. Their duration of therapy ranged from 3–20 mos and median PFS in responding patients was 11 mos (range 7–20). The longest survivor in this group (37 mos) received an ASCT after 12 mos of therapy. 13 pts (87%) remain alive at a median follow-up of 24 mos (range 8–37). Grade 3–4 toxicity consisted of 3 DVTs + 1 PE (27%), 5 hypergycemias (33%), 2 infections (13%) and 1 peripheral neuropathy (7%). Additionally, 1 pt developed superficial thrombophlebitis; 1 QT prolongation resolving with Biaxin discontinuation; 5 others with neuropathy; and 2 others with hyperglycemia. Conclusion : BLT-D is feasible and effective therapy in African-American patients with MM and is capable of inducing durable responses. However, we encountered significant thrombotic and endocrine toxicity that appears out of proportion to what has been previously reported with thalidomide plus dexamethasone alone. Furthermore, aspirin thromboprophylaxis at daily doses of 81–325 mg appears suboptimal in preventing thromboembolic events in this group of patients when prescribed this regimen.

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Immunoglobulin Free Light Chains at Diagnosis: Predictors of Progression and Survival in Solitary Plasmacytoma of Bone.

Blood ◽

10.1182/blood.v106.11.5080.5080 ◽

2005 ◽

Vol 106 (11) ◽

pp. 5080-5080 ◽

Cited By ~ 1

Author(s):

David Dingli ◽

Robert A. Kyle ◽

Vincent S. Rajkumar ◽

Grzegorz S. Nowakowski ◽

Dirk R. Larson ◽

...

Keyword(s):

Multiple Myeloma ◽

Plasma Cells ◽

Univariate Analysis ◽

Prognostic Indicator ◽

M Protein ◽

Solitary Plasmacytoma ◽

Time To Progression ◽

Number Of Patients ◽

M Proteins ◽

Risk Of Progression

Abstract Background: Solitary plasmacytoma of bone (SBP) is a localized collection of monoclonal plasma cells that is potentially curable with local radiation therapy but associated with a high risk of progression to multiple myeloma. We hypothesized that an abnormal immunoglobulin free light (FLC) ratio at diagnosis may be a prognostic indicator of transformation risk. Methods: We identified a cohort of 133 patients with SBP for whom stored serum taken at the time of diagnosis was available. The diagnosis was ascertained and serum FLC determined in 126 patients. Results: From this cohort, 48 patients have progressed to myeloma and the median time to progression among those who progressed was 1.9 years. On univariate analysis, age (p<0.001), gender (p=0.035), abnormal FLC ratio at diagnosis (p=0.009) and persistence of serum or urine M-protein after therapy (p=0.0070 were all associated with a shorter overall survival (OS) and time to progression to multiple myeloma. Progression by Normal FLC(0.26–1.65) Progression by Normal FLC(0.26–1.65) On multivariate analysis, an abnormal FLC ratio retained its independence in a model that includes age at diagnosis but lost its significance when combined with persistence of the serum or urine M-protein. However, serum or urine M-proteins are not detectable in a significant number of patients with SBP and therefore not informative. Conclusion: The FLC ratio at the time of diagnosis of SBP is a powerful predictor of risk and a useful aid to management of patients with this condition.

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Metastatic Bone Survey in Monoclonal Gammopathy of Undertermined Significance: Useful or Not?

Blood ◽

10.1182/blood.v112.11.2728.2728 ◽

2008 ◽

Vol 112 (11) ◽

pp. 2728-2728

Author(s):

Vrushali s Dabak ◽

Esther Urbaez Duran ◽

Muath Dawod ◽

Amr Hanbali

Keyword(s):

Risk Factors ◽

Multiple Myeloma ◽

Bone Marrow ◽

Serum Calcium ◽

Plasma Cells ◽

Bone Marrow Aspiration ◽

Hemoglobin Concentration ◽

M Protein ◽

Risk Of Progression ◽

Male Sex

Abstract Introduction: Monoclonal gammopathy of undetermined significance (MGUS) is defined as the presence of a serum monoclonal protein <3g/dl, with fewer than 10% plasma cells in bone marrow and absence of lytic bone lesions, anemia, hypercalcemia and renal insufficiency. Incidence increases with age, especially over 70 and its progression to malignant disease occurs at 1% per year. However, so far there are no studies which can reliably distinguish patients who would progress from those who would remain stable. Based on available literature, it is concluded that MGUS has low risk of progression when M-protein is less than 1.5 g/dl, with no reduction in polyclonal immunoglobulins and bone marrow plasma cells less than 5%. The recommended testing with suspected MGUS is hemoglobin concentration, protein studies, serum calcium, and creatinine. Metastatic bone survey (MBS) and bone marrow aspiration are felt unnecessary if M-protein is less than 1.5 g/dl. However literature to support the use of MBS at diagnosis based on the level of M-protein is limited. Also our observation has been that due to lack of clear guidelines, most physicians obtain a baseline MBS and some follow patients with yearly or every other year MBS irrespective of the level of M-protein. Hence, we decided to review patients diagnosed with MGUS at our institution to determine the importance of MBS and if possible identify risk factors like age, race, M-protein level, hemoglobin concentration, serum calcium or creatinine level, which would identify a subgroup of patients needing a MBS. In doing so we were hoping to separate out those patients in whom we could recommend against unnecessary use of the skeletal survey below a certain defined M protein level. Study: We reviewed charts on 1906 patients at Henry Ford hospital diagnosed with MGUS between 1990 and 2007. All patients with at least one M-protein and one MBS done were included in the analysis. We excluded patients with a level of M-protein >3.0 g/dl, who never had a skeletal survey in our system, had a light chain myeloma, plasmacytoma, chronic lymphocytic lymphoma(CLL), amyloidosis or protein evaluation done for diagnosis other than MGUS. We had 620 such patients. We collected data regarding their age, sex, ethnicity, date of diagnosis, type and level of the M-protein, hemoglobin level, serum calcium and creatinine at baseline, result of the MBS, date of progression to multiple myeloma (MM) if any and the date of last follow up if they did not progress to MM. Positive MBS is defined as x ray findings consistent with myelomatous changes with bone marrow aspiration confirming diagnosis of MM. Results: Of 620 patients, 36 had a positive MBS and applying non parametric Mann Whitney test and a chi-squared test, positive results seemed to correlate with higher level of M-protein, IgG subtype, lower hemoglobin and higher creatinine. Male sex and older age were other risk factors. Using the LOES curve to graph the risk of a positive skeletal event with the level of M-protein, risk was noted to increase significantly with M-protein in the range of 1.8– 3.0 (odds ratio 8.84 compared with 1.31 if level was less than 1.8), which was highly statistically significant as shown in figure 1. Further for 97/620 who progressed to multiple myeloma, the risk of progression was significantly higher for males, younger age at diagnosis of MGUS, lower hemoglobin, higher level of M-protein, IgG subtype and a positive skeletal event. Discussion: Our study is a retrospective chart review with its own limitations. However to our knowledge this is the first study to define the level of M-protein in patients with MGUS above which obtaining a MBS may be of value. Our study identifies 1.8 as a cut off value of M-protein below which doing routine MBS without symptoms of bone pains or other laboratory features suggesting progression to multiple myeloma might be unnecessary. Other risk factors for a positive event and progression to MM like lower hemoglobin, higher creatinine, older age, male sex and IgG subtype in our study are in keeping with what has been described in the literature. Conclusion: Based on our study, obtaining baseline MBS in all patients with suspected MGUS was not beneficial. Hence, we would not recommend obtaining MBS in patients with M-protein <1.8 g/dl in absence of other risk factors for progression to multiple myeloma. Figure 1: LOES curve showing increased likelihood of positive MBS for increasing MPEV level. Figure 1:. LOES curve showing increased likelihood of positive MBS for increasing MPEV level.

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