Elevated Serum Free Light Chains Research Articles

SAT0286 Serum Immunoglobulin Free Light Chain Assessment in Psoriatic Arthritis

BackgroundElevation of free light chains (FLC) represents B cell activation and has been detected in the autoantibodies positive rheumatologic disorders such as rheumatoid arthritis (RA) and Sjögren syndrome. Psoriatic arthritis...

Immunoglobulin heavy chain/light chain pair measurement is associated with survival in diffuse large B-cell lymphoma

Elevated serum free light chains (FLCs) have been associated with an unfavorable prognosis in diffuse large B-cell lymphoma (DLBCL). The aim of this study was to determine the clinical relevance of a quantitative assessment of intact circulating immunoglobulin (Ig), using serum Ig heavy chain/light chain pair (HLC) measurements in patients with DLBCL. FLC and HLC were measured in 409 serum samples of patients with DLBCL included in the LNH03-B clinical trial program of the Groupe d’Etudes des Lymphomes de l’Adulte (GELA). Patients with an abnormal IgMκ/IgMλ ratio or an abnormal FLC ratio more frequently displayed adverse clinical characteristics. Patients with abnormal IgMκ/IgMλ ratios had inferior progression-free survival (PFS) and overall survival (OS) as compared to patients with a normal ratio in the overall cohort (5-year PFS 44.9% vs. 69.3%, p = 0.0003 and 5-year OS 50.8% vs. 78.1%, p = 0.0003) and in the R-CHOP (rituximab, cyclophosphamide, doxorubicin, vincristine, prednisone) cohort (5-year OS 43.5% vs. 70.3%, p = 0.003). In multivariate analysis, including elevated FLC/HLC and International Prognostic Index (IPI), an abnormal IgMκ/IgMλ ratio (hazard ratio [HR] = 1.54, 95% confidence interval [CI] 1.03–2.3, p = 0.03) remained predictive of shorter progression-free survival. Gene expression profile experiments and immunohistochemistry indicate that this measurement is at least partially related to tumor cell secretion. Both elevated serum FLCs and an abnormal IgMκ/IgMλ ratio are associated with unfavorable outcomes in patients with DLBCL treated by R-CHOP.

Serum free light chain ratio as a biomarker for high-risk smoldering multiple myeloma

A markedly elevated serum free light chain (FLC) ratio may serve as a biomarker for malignant transformation in high-risk smoldering multiple myeloma (SMM) and identify patients who are at imminent risk of progression. We retrospectively studied the predictive value of the serum (FLC) assay in 586 patients with SMM diagnosed between 1970 to 2010. A serum involved/uninvolved FLC ratio ≥ 100 was used to define high-risk SMM, which included 15% (n=90) of the total cohort. Receiver operating characteristics analysis determined the optimal FLC ratio cut-point to predict progression to symptomatic multiple myeloma (MM) within 2 years of diagnosis, which resulted in a specificity of 97% and sensitivity of 16%. Fifty-six percent of patients developed progressive disease during median follow-up of 52 months, but this increased to 98% in the subgroup of patients with FLC ratio ≥ 100. The median time to progression in the FLC ratio ≥ 100 group was 15 months versus 55 months in the FLC <100 group (P<0.0001). The risk of progression to MM within the first 2 years in patients with an FLC ratio ≥ 100 was 72%; the risk of progression to MM or light chain amyloidosis in 2 years was 79%. We conclude that a high FLC ratio ≥ 100 is a predictor of imminent progression in SMM, and such patients may be considered candidates for early treatment intervention.

Autologous stem cell transplant for light chain deposition disease: Incorporating bortezomib to the induction therapy

Autologous stem cell transplant for light chain deposition disease: Incorporating bortezomib to the induction therapy

Elevated serum free light chains are associated with inferior event free and overall survival in Hodgkin lymphoma

The serum free light chain (FLC) assay quantitates free immunoglobulin kappa and lambda light chains, which has prognostic value in plasma cell dyscrasias. However, there is limited data on serum FLC in lymphoid malignancies. We analyzed the association of pretreatment FLC with event-free survival (EFS) and overall survival (OS) in 100 patients with Hodgkin lymphoma (HL). Elevated polyclonal FLC were present in 30% of patients; these patients had an inferior EFS (HR = 4.84; 95% CI: 1.84-12.7) and OS (HR = 8.87; 95% CI: 2.35-33.52) compared to patients with normal FLC. Further studies of FLC in HL are warranted.

4.1 Elevated Serum Free Light Chains Independently Identify a Poor Risk Group of Stage A CLL Patients

4.1 Elevated Serum Free Light Chains Independently Identify a Poor Risk Group of Stage A CLL Patients

Case 29-2011

Cardiac and renal failure developed in a 66-year-old woman. Echocardiography suggested infiltrative cardiomyopathy, lytic bone lesions were seen on imaging, and elevated serum free light chains were detected. A diagnostic procedure was performed.

AL Amyloidosis and Concomitant Myeloma: Time to Reconsider Assumptions

AbstractAbstract 4044 Background:Conventionally, multiple myeloma is believed to coexist in approximately 10% of AL amyloidosis patients. However, it is unclear whether this figure is too low based on current World Health Organization criteria. These criteria, mainly created to differentiate myeloma from monoclonal gammopathy of undetermined significance, include the presence of ≥ 10% plasma cells on a bone marrow biopsy or aspirate as being diagnostic of myeloma. Aims:To define the frequency and relevance of a concomitant diagnosis of myeloma in patients with AL amyloidosis. Methods:Records from consecutive patients with biopsy-proven AL amyloidosis treated at the Stanford University Amyloid Center were reviewed. Plasma cell percentages were determined by manual counts from bone marrow aspirate smears and by CD138 immunohistochemistry (IHC) performed on bone marrow core biopsies. Results:A total of 41 patients (median age 61 years, 32% female) were evaluated. The median number of organs involved with amyloidosis was 2 (range 1–4), with 28 patients (68%) having cardiac involvement, 22 patients (54%) having renal involvement, 15 patients (37%) having gastrointestinal involvement, 12 patients (29%) having soft tissue involvement, and 10 patients (24%) having nervous system involvement. All patients had bone marrow biopsies and aspirates performed at the time of amyloid diagnosis, with most undergoing both manual counts of plasma cells from aspirates and IHC from core biopsies. Based on conventional criteria, manual aspirate counts defined 15/28 (54%) patients as having myeloma, and IHC defined 26/31 (84%) patients as having myeloma (p=0.01). Only nine patients had a detectable serum paraprotein on immunofixation (median 1.1 g/dl, range 0.4–2.6). 81% of patients had an elevated serum free light chain (85% lambda), with a median level of 37.3 mg/dl (range 8.6–256 mg/dl). Compared to the frequency of elevated plasma cells, the prevalence of anemia (29%), hypercalcemia (14%), impaired kidney function (21%), and lytic lesions (7%) was low. After a median follow-up of 13 months (range 1–127 months), the one-year overall survival (74% vs. 58%) and three-year overall survival (50% vs. 50%) was not significantly different between patients with ≥10% plasma cells and patients with <10% plasma cells (p=NS). Discussion:As defined by bone marrow plasma cell involvement, a strikingly high percentage (84%) of AL amyloidosis patients would be considered to have concurrent myeloma. This figure is much higher than has been traditionally quoted in the literature, likely due to the utilization of newer methods of counting plasma cells. There was a low prevalence of myeloma-associated end-organ effects (hypercalcemia, anemia, renal insufficiency, lytic bone lesions), and a myeloma diagnosis had no impact on survival. Conclusion:In this cohort of AL amyloid patients, concomitant myeloma was present in the vast majority of patients using modern diagnostic techniques. The significance of this diagnosis appears to be minimal – calling into question whether the diagnostic criteria for myeloma should be redefined in this population. Disclosures:Witteles:Celgene: Research Funding. Liedtke:Celgene: Lecture fee, Research Funding. Schrier:Celgene: Research Funding.

Elevated Pre-Treatment Serum Immunoglobulin Free Light Chains (FLC) Are Associated with Poor Event-Free and Overall Survival in Diffuse Large B-Cell Lymphoma (DLBCL).

Abstract 136 Background:The serum free light chain (FLC) assay quantitates free kappa and free lambda immunoglobulin light chains. This assay has prognostic value in MGUS, multiple myeloma (MM), solitary plasmacytoma, and AL amyloidoisis, and has been incorporated in response criteria for both MM and AL amyloidosis. A percentage of non-Hodgkin's lymphoma (NHL) patients also present with abnormal FLC concentrations and recent data suggest that AIDS patients with elevated serum FLC are at higher risk of developing NHL. Here we assess the impact of FLC in a cohort of patients with diffuse large B-cell lymphoma (DLBCL) enrolled on a cooperative group clinical trial. Methods:Newly diagnosed DLBCL patients were treated with epratuzumab + R-CHOP (ER-CHOP) on NCCTG clinical trial N0489. Serum FLC was quantitated prior to treatment and after cycles 2 and 6 using the Freelite FLC assay (The Binding Site, Ltd., Birmingham, UK). Patients were followed per clinical trial protocol for event-free (progression, retreatment, or death due to any cause) and overall survival (EFS and OS, respectively). Results:107 patients were enrolled on the trial. 80 patients had a pre-treatment serum draw and a central pathology confirmed diagnosis of DLBCL, of which 47 had a post-cycle 2 sample (C2) and a 54 had a post-cycle 6 sample (C6). At a medium follow-up of 25 months (range 7-39), 22 patients (28%) had an event and 17 patients died (21%). Prior to treatment 23 patients (29%) had abnormal kappa concentrations (all elevated), 16 (20%) had abnormal lambda concentrations (11 elevated, 5 decreased), and 9 (11%) had an abnormal kappa/lambda ratio. FLC concentrations were significantly reduced in patients during treatment, with a median reduction in kappa (C2: 46%, C6: 64%) and lambda (C2: 44%, C6: 49%), all p<0.0001. Elevated FLC prior to treatment was highly associated with both OS (logrank p=0.009) and EFS (logrank p=0.006); these associations remained significant after adjusting for IPI (both p = 0.01). Conclusions:A significant percentage of DLBCL patients present with abnormal FLC concentrations. Kappa and lambda are significantly reduced for most patients during treatment. Elevated pre-treatment FLC concentrations are associated with inferior EFS and OS in DLBCL and this association is independent of the IPI. A follow-up study of FLC and prognosis is currently underway in a cohort of 1500 NHL patients from the Mayo Clinic and University of Iowa SPORE.Association of Pre-treatment FLC with OutcomeN (%)OS HR (95% CI)EFS HR (95% CI)Elevated KappaUnivariate23 (29%)3.3 (1.3, 8.5)2.5 (1.1, 5.9)IPI Adjusted3.1 (1.2, 8.1)2.3 (1.0, 5.5)Elevated LambdaUnivariate11 (14%)3.1 (1.1, 8.8)4.2 (1.7, 10.4)IPI Adjusted4.4 (1.5, 13.2)5.3 (2.1, 13.5)Abnormal Kappa/Lambda RatioUnivariate9 (11%)2.8 (0.91, 8.6)1.9 (0.65, 5.7)IPI Adjusted4.3 (1.4, 14.0)2.5 (0.82, 7.8)Elevated FLC (either)Univariate26 (33%)3.4 (1.3, 8.9)3.1 (1.3, 7.2)IPI Adjusted3.3 (1.3, 8.8)2.9 (1.3, 6.8) [Display omitted] [Display omitted] Disclosures:No relevant conflicts of interest to declare.

Monoclonal Gammopathy as a Determinant of Adverse Outcomes in Patients with Chronic Kidney Disease.

Elevated serum free light chain (sFLC) concentrations are associated with glomerular and tubulointerstitial disease. We have analyzed a cohort of patients with chronic kidney disease (CKD) to determine the relationship between sFLC and clinical outcomes. 369 patients from the renal clinics at the Queen Elizabeth hospital in Birmingham were followed for a period of 8 years. We reviewed renal outcomes and all cause mortality over this period. sFLC levels were measured on baseline serum samples using a nephelometric immunoassay (The Binding Site Ltd.). The CKD patients had mean sFLC concentrations significantly higher than the normal population (kappa: 77 vs. 8.4mg/L p<0.0001; lambda: 94.7 vs. 13.4mg/L p<0.03). 65 patients (18%) had abnormal sFLC ratios suggesting clonal production of sFLC. There were 270 endpoints during follow-up (106 deaths and 164 end stage renal failures). By Kaplan Meier survival analysis an abnormal sFLC ratio is significantly associated with a worse composite outcome (p<0.02), with the dominant factor being the progression of renal impairment to end stage disease. This is the first study to assess if an abnormal sFLC ratio is predictive of outcomes in patients with CKD. These findings provide the basis for further work to evaluate whether monoclonal FLCs are prognostic of a worse outcome in patients with CKD.

Risk-Adapted Intravenous Melphalan Followed by Adjuvant Dexamethasone (D) and Thalidomide (T) for Newly Diagnosed Patients with Systemic AL Amyloidosis (AL): Interim Results of a Phase II Study.

High-dose melphalan (M) with autologous stem cell transplant (ASCT) is an effective therapy for AL, but treatment-related mortality (TRM) remains high, and hematologic complete responses (CR) occur in a minority of patients. In this study, we asked whether a risk-adapted approach to IV M dosing could decrease TRM, and whether adjuvant D +/− T could improve hematologic and amyloid-involved organ response rates. Other objectives of the trial are to study prospectively the prognostic significance of the serum free light chain (FLC), troponin I, and brain natriuretic peptide (BNP) assays. Newly diagnosed untreated AL patients are risk-stratified upon enrollment. Low-risk patients (1 or 2 major organs involved, no advanced cardiac disease) receive M 100, 140, or 200 mg/m2 with ASCT based on age, presence of cardiac involvement, and renal function. High-risk patients (≥3 organs involved or advanced cardiac disease) receive 2 cycles of M 40 mg/m2 without ASCT. Patients with persistent clonal plasma cell disease at 3 months receive 9 months of adjuvant D+T or D alone (if history of deep venous thrombosis or neuropathy). Since 9/02, 38 patients (median age=57.5 (range 34–73), 68% males) have enrolled. Median time from diagnosis to enrollment is 1.5 months (range 0.5 – 7). Organ involvement includes 13 (34%) cardiac, 24 (63%) renal (12 with renal only), 13 (34%) liver/GI tract, and 10 (26%) peripheral nervous system. Thirty-two (84%) had baseline elevated serum FLC with abnormal κ:λ ratio. Thirty-four patients have been treated--3 high-risk and 31 low-risk (5 at M 100, 16 at 140 and 10 at 200 mg/m2). Treatment-related mortality is 7.4% (2/27) with an additional 7 patients alive <100 days post-treatment. Six patients, including all 3 treated high-risk patients, have died of progressive disease (PD) a median of 5.5 months (range 4–17) after M. Of the 8 patients who died, 7 had symptomatic cardiac involvement. At 3 months, 22 low-risk patients are evaluable for hematologic response. Thirteen (59%) responded (4 CR, 9 PR) and 9 had stable disease. Of the 18 patients with persistent clonal disease, 9 began T (50 to 200 mg nightly) and D (1 to 3 four-day pulses monthly), 6 began D alone, and 3 had no adjuvant therapy (refused or too ill). Five patients completed 9 months of adjuvant therapy, and 2 remain on therapy, with 2 conversions from PR→CR (T+D, D), and 1 from SD→PR (D). Reasons for discontinuation were PD (n=4), pulmonary embolus (n=1), pneumonia (n=2), and intolerance (n=2). Eleven patients are evaluable at 12 months, with 10 (91%) responses (4 CR, 6 PR) and 1 PD (9%). Seven (77%) have objective improvement in amyloid-related organ function, 2 have stable and 2 worsened AL. Preliminary analysis of serum FLC data (n=23) shows an association between a persistently abnormal κ:λ ratio 3 months after treatment and an increased risk of death (RR=1.67, 95% CI=1.10–2.52, p=0.02). Analyses of the prognostic significance of serial troponin and BNP assays are ongoing. In conclusion, risk-adapted dosing of IV M in newly diagnosed AL patients has a low TRM. Adjuvant D +/− T is feasible, with toxicity leading to discontinuation in 33% (5/15) of patients, and with a benefit to date in 20% (3/15) of patients with persistent clonal plasma cell disease 3 months post ASCT, including induction of 2 hematologic CRs.