Your search keyword '"Kyle, R"' showing total 44 results

1. Utility of serum free light chain measurements in multiple myeloma patients not achieving complete response to therapy.

Author

Alhaj Moustafa, M, Rajkumar, S V, Dispenzieri, A, Gertz, M A, Lacy, M Q, Buadi, F K, Hwa, Y L, Dingli, D, Kapoor, P, Hayman, S R, Lust, J A, Kyle, R A, and Kumar, S K

Subjects

ANTINEOPLASTIC agents, CANCER relapse, IMMUNOGLOBULINS, LONGITUDINAL method, MULTIPLE myeloma, PROGNOSIS, RESEARCH funding, SURVIVAL, TUMOR classification, DISEASE remission, RETROSPECTIVE studies

Abstract

Normalization of the serum-free light-chain ratio (FLCr) with the absence of bone marrow monoclonal plasma cells following achievement of a complete response (CR) to therapy denotes a stringent CR in multiple myeloma (MM), and is associated with improved overall survival (OS). However, its value in patients achieving

Published

2015

2. Racial disparities in the prevalence of monoclonal gammopathies: a population-based study of 12,482 persons from the National Health and Nutritional Examination Survey.

Author

Landgren, O, Graubard, B I, Katzmann, J A, Kyle, R A, Ahmadizadeh, I, Clark, R, Kumar, S K, Dispenzieri, A, Greenberg, A J, Therneau, T M, Melton 3rd, L J, Caporaso, N, Korde, N, Roschewski, M, Costello, R, McQuillan, G M, Rajkumar, S V, and Melton, L J 3rd

Abstract

Multiple myeloma (MM) incidence is markedly higher in blacks compared with whites, which may be related to a higher prevalence of monoclonal gammopathy of undetermined significance (MGUS). Our objective was to define the prevalence and risk factors of MGUS in a large cohort representative of the US population. Stored serum samples from the National Health and Nutritional Examination Survey (NHANES) III or NHANES 1999-2004 were available for 12,482 individuals of age ⩾50 years (2331 'blacks', 2475 Hispanics, 7051 'whites' and 625 'others') on which agarose-gel electrophoresis, serum protein immunofixation, serum-free light-chain assay and M-protein typing were performed. MGUS was identified in 365 participants (2.4%). Adjusted prevalence of MGUS was significantly higher (P<0.001) in blacks (3.7%) compared with whites (2.3%) (P=0.001) or Hispanics (1.8%), as were characteristics that posed a greater risk of progression to MM. The adjusted prevalence of MGUS was 3.1% and 2.1% for the North/Midwest versus South/West regions of the United States, respectively (P=0.052). MGUS is significantly more common in blacks, and more often has features associated with higher risk of progression to MM. A strong geographic disparity in the prevalence of MGUS between the North/Midwest versus the South/West regions of the United States was found, which has etiologic implications. [ABSTRACT FROM AUTHOR]

Published

2014

3. Racial disparities in the prevalence of monoclonal gammopathies: a population-based study of 12 482 persons from the National Health and Nutritional Examination Survey.

Author

Landgren, O, Graubard, B I, Katzmann, J A, Kyle, R A, Ahmadizadeh, I, Clark, R, Kumar, S K, Dispenzieri, A, Greenberg, A J, Therneau, T M, Melton, L J, Caporaso, N, Korde, N, Roschewski, M, Costello, R, McQuillan, G M, and Rajkumar, S V

Subjects

MONOCLONAL gammopathies, MULTIPLE myeloma, HEALTH surveys, POPULATION

Abstract

Multiple myeloma (MM) incidence is markedly higher in blacks compared with whites, which may be related to a higher prevalence of monoclonal gammopathy of undetermined significance (MGUS). Our objective was to define the prevalence and risk factors of MGUS in a large cohort representative of the US population. Stored serum samples from the National Health and Nutritional Examination Survey (NHANES) III or NHANES 1999-2004 were available for 12 482 individuals of age ⩾50 years (2331 'blacks', 2475 Hispanics, 7051 'whites' and 625 'others') on which agarose-gel electrophoresis, serum protein immunofixation, serum-free light-chain assay and M-protein typing were performed. MGUS was identified in 365 participants (2.4%). Adjusted prevalence of MGUS was significantly higher (P<0.001) in blacks (3.7%) compared with whites (2.3%) (P=0.001) or Hispanics (1.8%), as were characteristics that posed a greater risk of progression to MM. The adjusted prevalence of MGUS was 3.1% and 2.1% for the North/Midwest versus South/West regions of the United States, respectively (P=0.052). MGUS is significantly more common in blacks, and more often has features associated with higher risk of progression to MM. A strong geographic disparity in the prevalence of MGUS between the North/Midwest versus the South/West regions of the United States was found, which has etiologic implications. [ABSTRACT FROM AUTHOR]

Published

2014

4. Continued improvement in survival in multiple myeloma: changes in early mortality and outcomes in older patients.

Author

Kumar, S K, Dispenzieri, A, Lacy, M Q, Gertz, M A, Buadi, F K, Pandey, S, Kapoor, P, Dingli, D, Hayman, S R, Leung, N, Lust, J, McCurdy, A, Russell, S J, Zeldenrust, S R, Kyle, R A, and Rajkumar, S V

Subjects

ACUTE myeloid leukemia, MORTALITY, HEALTH of older people, COHORT analysis, B cell lymphoma

Abstract

Therapy for multiple myeloma (MM) has markedly changed in the past decade with the introduction of new drugs, but it is not clear whether the improvements have been sustained. We studied 1038 patients diagnosed between 2001 and 2010, grouping patients into two 5-year periods by diagnosis, 2001-2005 and 2006-2010. The median estimated follow-up for the cohort was 5.9 years with 47% alive at the last follow-up. The median overall survival (OS) for the entire cohort was 5.2 years: 4.6 years for patients in the 2001-2005 group compared with 6.1 years for the 2006-2010 cohort (P=0.002). The improvement was primarily seen among patients over 65 years, the 6-year OS improving from 31 to 56%, P<0.001. Only 10% of patients died during the first year in the latter group, compared with 16% in the earlier cohort (P<0.01), suggesting improvement in early mortality. The improved outcomes were linked closely to the use of one or more new agents in initial therapy. The current results confirm continued survival improvement in MM and highlight the impact of initial therapy with novel agents. Most importantly, we demonstrate that the improved survival is benefitting older patients and that early mortality in this disease has reduced considerably. [ABSTRACT FROM AUTHOR]

Published

2014

5. Long-term outcome with lenalidomide and dexamethasone therapy for newly diagnosed multiple myeloma.

Author

Srivastava, G, Rana, V, Lacy, M Q, Buadi, F K, Hayman, S R, Dispenzieri, A, Gertz, M A, Dingli, D, Zeldenrust, S, Russell, S, McCurdy, A, Kapoor, P, Kyle, R, Rajkumar, S V, and Kumar, S

Subjects

MULTIPLE myeloma, DEXAMETHASONE, B cell lymphoma, STEM cells, PATIENTS

Abstract

The combination of lenalidomide and dexamethasone (Len-Dex) is a commonly used initial therapy for newly diagnosed multiple myeloma (MM). Although the initial response rates and toxicity are well known, long-term outcome is not well described. We studied 286 consecutive patients with newly diagnosed MM initially treated with Len-Dex. The median (range) age at diagnosis was 63 (28-92) years, 166 (58%) patients 65 years and 175 (61%) male. The median estimated duration on Len-Dex was 5.3 months with overall response (partial response) of 72%, including 26% with very good partial response or better. The median overall survival (OS) from the diagnosis was not reached (NR) and the estimated 5-year survival was 71%. The median time to first disease progression, irrespective of transplant status, was 30.2 months. Overall, 143 (50%) patients underwent stem cell transplant. The median OS was NR for patients 70 years and 5.8 years for the older patients (P=0.01). The 5-year OS estimate for patients in International Staging System stage 1, 2 and 3 were 82, 65, and 44% respectively. There were 21 new second malignancies after MM diagnosis (6.6%). The median survival exceeding 7 years reflects the efficacy of novel agents. The risk of second malignancies doesn't appear to be excessive in this population. [ABSTRACT FROM AUTHOR]

Published

2013

6. Impact of primary molecular cytogenetic abnormalities and risk of progression in smoldering multiple myeloma.

Author

Rajkumar, S V, Gupta, V, Fonseca, R, Dispenzieri, A, Gonsalves, W I, Larson, D, Ketterling, R P, Lust, J A, Kyle, R A, and Kumar, S K

Subjects

MULTIPLE myeloma, CYTOGENETICS, IMMUNOGLOBULINS, CHROMOSOMAL translocation, CHROMOSOME abnormalities

Abstract

We studied 351 patients with smoldering multiple myeloma (SMM) in whom the underlying primary molecular cytogenetic subtype could be determined based on cytoplasmic immunoglobulin fluorescent in situ hybridization studies. Hundred and fifty-four patients (43.9%) had trisomies, 127 (36.2%) had immunoglobulin heavy chain (IgH) translocations, 14 (4%) both trisomies and IgH translocations, 53 (15.1%) no abnormalities detected and 3 (0.9%) had monosomy13/del(13q) in the absence of any other abnormality. Among 127 patients with IgH translocations, 57 were t(11;14), 36 t(4;14), 11 musculoaponeurotic fibrosarcoma (MAF) translocations, and 23 other or unknown IgH translocation partner. Time to progression (TTP) to symptomatic multiple myeloma was significantly shorter in patients with the t(4;14) compared with patients with t(11;14), median 28 versus 55 months, respectively, P=0.025. The median TTP was 28 months with t(4;14) (high-risk), 34 months with trisomies alone (intermediate-risk), 55 months with t(11;14), MAF translocations, other/unknown IgH translocations, monosomy13/del(13q) without other abnormalities, and those with both trisomies and IgH translocations (standard-risk), and not reached in patients with no detectable abnormalities (low-risk), P=0.001. There was a trend to shorter TTP with deletion 17p (median TTP, 24 months). Overall survival from diagnosis of SMM was significantly inferior with t(4;14) compared with t(11;14), median 105 versus 147 months, respectively, P=0.036. [ABSTRACT FROM AUTHOR]

Published

2013

7. Plasma cell leukemia: consensus statement on diagnostic requirements, response criteria and treatment recommendations by the International Myeloma Working Group.

Author

Fernández de Larrea, C, Kyle, R A, Durie, B G M, Ludwig, H, Usmani, S, Vesole, D H, Hajek, R, San Miguel, J F, Sezer, O, Sonneveld, P, Kumar, S K, Mahindra, A, Comenzo, R, Palumbo, A, Mazumber, A, Anderson, K C, Richardson, P G, Badros, A Z, Caers, J, and Cavo, M

Subjects

*LEUKEMIA treatment, *LEUKEMIA diagnosis, *MULTIPLE myeloma diagnosis, *MULTIPLE myeloma, *RESEARCH funding, *DISEASE progression

Abstract

Plasma cell leukemia (PCL) is a rare and aggressive variant of myeloma characterized by the presence of circulating plasma cells. It is classified as either primary PCL occurring at diagnosis or as secondary PCL in patients with relapsed/refractory myeloma. Primary PCL is a distinct clinic-pathological entity with different cytogenetic and molecular findings. The clinical course is aggressive with short remissions and survival duration. The diagnosis is based upon the percentage (≥ 20%) and absolute number (≥ 2 × 10(9)/l) of plasma cells in the peripheral blood. It is proposed that the thresholds for diagnosis be re-examined and consensus recommendations are made for diagnosis, as well as, response and progression criteria. Induction therapy needs to begin promptly and have high clinical activity leading to rapid disease control in an effort to minimize the risk of early death. Intensive chemotherapy regimens and bortezomib-based regimens are recommended followed by high-dose therapy with autologous stem cell transplantation if feasible. Allogeneic transplantation can be considered in younger patients. Prospective multicenter studies are required to provide revised definitions and better understanding of the pathogenesis of PCL. [ABSTRACT FROM AUTHOR]

Published

2013

8. Treatment patterns and outcomes in elderly patients with multiple myeloma.

Author

Bang, S-M, Kyle, R A, Rajkumar, S V, and Kumar, S

Subjects

*MULTIPLE myeloma, *DISEASES in older people, *PREDNISONE, *THALIDOMIDE

Abstract

This article discusses a study which examined treatment patterns and outcomes among elderly patients with multiple myeloma (MM) who were seen at the Mayo Clinic in Rochester, Minnesota between January 1999 and December 2008. The study findings showed that MM has a more malignant biology in elderly patients. It is also noted that the trial showed a prolongation of survival with modest toxicity with melphalan, prednisone and thalidomide.

Published

2013

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

Author

Larsen, J T, Kumar, S K, Dispenzieri, A, Kyle, R A, Katzmann, J A, and Rajkumar, S V

Subjects

MULTIPLE myeloma, BIOMARKERS, DISEASE progression, BONE marrow, LEUKEMIA

Abstract

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. [ABSTRACT FROM AUTHOR]

Published

2013

10. High levels of peripheral blood circulating plasma cells as a specific risk factor for progression of smoldering multiple myeloma.

Author

Bianchi, G, Kyle, R A, Larson, D R, Witzig, T E, Kumar, S, Dispenzieri, A, Morice, W G, and Rajkumar, S V

Subjects

*B cell lymphoma, *MULTIPLE myeloma, *LYMPHOID tissue, *BLOOD, *PLASMA cells

Abstract

Smoldering multiple myeloma (SMM) carries a 50% risk of progression to multiple myeloma (MM) or related malignancy within the first 5 years following diagnosis. The goal of this study was to determine if high levels of circulating plasma cells (PCs) are predictive of SMM transformation within the first 2-3 years from diagnosis. Ninety-one patients diagnosed with SMM at Mayo Clinic from January 1994 through January 2007, who had testing for circulating PCs using an immunofluorescent assay and adequate follow-up to ascertain disease progression, were studied. High level of circulating PCs was defined as absolute peripheral blood PCs >5 × 106/l and/or >5% PCs per 100 cytoplasmic immunoglobulin (Ig)-positive peripheral blood mononuclear cells. Patients with high circulating PCs (14 of 91 patients, 15%) were significantly more likely to progress to active disease within 2 years compared with patients without high circulating PCs, 71% versus 24%, respectively, P=0.001. Corresponding rates for progression within 3 years were 86% versus 34%, respectively, P<0.001. Overall survival (OS) after both SMM diagnosis and MM diagnosis was also significantly different. High levels of circulating PCs identify SMM patients with an elevated risk of progression within the first 2-3 years following diagnosis. [ABSTRACT FROM AUTHOR]

Published

2013

11. Suppression of uninvolved immunoglobulins defined by heavy/light chain pair suppression is a risk factor for progression of MGUS.

Author

Katzmann, J A, Clark, R, Kyle, R A, Larson, D R, Therneau, T M, Melton, L J, Benson, J T, Colby, C L, Dispenzieri, A, Landgren, O, Kumar, S, Bradwell, A R, Cerhan, J R, and Rajkumar, S V

Subjects

IMMUNOGLOBULINS, SERUM, MULTIVARIATE analysis, DISEASE progression

Abstract

We hypothesized that the suppression of uninvolved immunoglobulin in monoclonal gammopathy of undetermined significance (MGUS) as detected by suppression of the isotype-specific heavy and light chain (HLC-pair suppression) increases the risk of progression to malignancy. This approach required quantitation of individual heavy/light chains (for example, IgGλ in IgGκ MGUS patients). Of 1384 MGUS patients from Southeastern Minnesota seen at the Mayo Clinic from 1960 to 1994, baseline serum samples obtained within 30 days of diagnosis were available in 999 persons. We identified HLC-pair suppression in 27% of MGUS patient samples compared with 11% of patients with suppression of uninvolved IgG, IgA or IgM. HLC-pair suppression was a significant risk factor for progression (hazard ratio (HR), 2.3; 95% confidence interval (CI) 1.5-3.7; P<0.001). On multivariate analysis, HLC-pair suppression was an independent risk factor for progression to malignancy in combination with serum M-spike size, heavy chain isotype and free light chain ratio (HR, 1.8; 95% CI, 1.1-3.00; P=0.018). The finding that HLC-pair suppression predicts progression in MGUS and occurs several years before malignant transformation has implications for myeloma biology. [ABSTRACT FROM AUTHOR]

Published

2013

12. Consensus guidelines for the conduct and reporting of clinical trials in systemic light-chain amyloidosis.

Author

Comenzo, R L, Reece, D, Palladini, G, Seldin, D, Sanchorawala, V, Landau, H, Falk, R, Wells, K, Solomon, A, Wechalekar, A, Zonder, J, Dispenzieri, A, Gertz, M, Streicher, H, Skinner, M, Kyle, R A, and Merlini, G

Subjects

AMYLOIDOSIS, CLINICAL trials, IMMUNOGLOBULINS, DRUG development, HEART failure risk factors

Abstract

This manuscript summarizes the recommendations that emerged from the first Roundtable on Clinical Research in Immunoglobulin Light-chain Amyloidosis (AL), a meeting sponsored by the Amyloidosis Foundation (Clarkston, MI, USA) to develop a consensus of experts on a modern framework for clinical trial design and drug development in AL. Recent diagnostic and technical advances in AL, and updated consensus guidelines for assessing hematologic and organ responses, enable us to define study populations, appropriate end points, and other criteria for all phases of clinical research. This manuscript provides a framework for the design and conduct of systematic collaborative clinical research in AL to encourage more rapid testing of therapies and to expedite new drug development and approval. [ABSTRACT FROM AUTHOR]

Published

2012

13. Hematopoietic cell transplantation for primary plasma cell leukemia: results from the Center for International Blood and Marrow Transplant Research.

Author

Mahindra, A, Kalaycio, M E, Vela-Ojeda, J, Vesole, D H, Zhang, M-J, Li, P, Berenson, J R, Bird, J M, Dispenzieri, A, Gajewski, J L, Gale, R P, Holmberg, L, Kumar, S, Kyle, R A, Lazarus, H M, Lonial, S, Mikhael, J, Milone, G A, Munker, R, and Nath, R

Subjects

LYMPHOID tissue, PLASMA cell diseases, DIAGNOSIS, CELL transplantation, CONFIDENCE intervals

Abstract

There are limited data on hematopoietic cell transplantation (HCT) in primary plasma cell leukemia (pPCL), an aggressive plasma cell disorder. We report outcomes of 147 patients with pPCL receiving autologous (n=97) or allogeneic (n=50) HCT within 18 months after diagnosis between 1995 and 2006. Median age was 56 years and 48 years for autologous HCT and allogeneic HCT, respectively. Progression-free survival (PFS) at 3 years was 34% (95% confidence interval (CI), 23-46%) in the autologous group and 20% (95% CI, 10-34%) in the allogeneic group. Cumulative incidence of relapse at 3 years was 61% (95% CI, 48-72%) in the autologous group and 38% (95% CI, 25-53%) in the allogeneic group. Overall survival (OS) at 3 years was 64% (95% CI, 52-75%) in the autologous group and 39% (95% CI, 26-54%) in the allogeneic group. Non-relapse mortality (NRM) at 3 years was 5% (95% CI, 1-11%) in the autologous group and 41% (95% CI, 28-56%) in the allogeneic group. The encouraging OS after autologous HCT, establishes the safety and feasibility of this consolidative treatment option after initial induction therapy for pPCL. Allogeneic HCT, although associated with a significantly lower relapse rate, carries a much higher risk of NRM and no OS benefit. [ABSTRACT FROM AUTHOR]

Published

2012

14. Melphalan and prednisone versus melphalan, prednisone and thalidomide for elderly and/or transplant ineligible patients with multiple myeloma: a meta-analysis.

Author

Kapoor, P., Rajkumar, S. V., Dispenzieri, A., Gertz, M. A., Lacy, M. Q., Dingli, D., Mikhael, J. R., Roy, V., Kyle, R. A., Greipp, P. R., Kumar, S., and Mandrekar, S. J.

Subjects

MULTIPLE myeloma, PREDNISONE, THALIDOMIDE, RANDOMIZED controlled trials, THROMBOSIS

Abstract

Trials comparing efficacy of melphalan prednisone (MP) with MP plus thalidomide in transplant ineligible, elderly patients with multiple myeloma have provided conflicting evidence. Although there is agreement regarding improved response rates (RRs) and higher toxicity with the addition of thalidomide to MP, the impact on progression free survival (PFS) and overall survival (OS) is less clear. We performed a meta-analysis comparing efficacy of melphalan, prednisone and thalidomide (MPT) and MP by pooling results on RR, PFS and OS reported in all the identified randomized controlled trials (RCTs) under a random effects model. Overall, six prospective RCTs, with data extractable from five published trials (n=1568) were identified. The pooled odds ratio of responding to therapy with MPT vs MP was 3.39 (P<0.001, 95% CI: 2.24-5.12). The pooled hazard ratios for PFS and OS were and 0.68 (P<0.001; 95% CI: 0.55-0.82) and 0.80 (P=0.07; 95% CI: 0.63-1.02), respectively, in favor of MPT. The odds ratios for high grade peripheral neuropathy and deep venous thrombosis were 6.6 and 2.4, respectively, in favour of MP. There was significant heterogeneity among the RCTs. Our meta-analysis demonstrates that in previously untreated, transplant ineligible, elderly myeloma patients, the addition of T to MP results in significantly improved RR and PFS with a trend towards improvement in OS compared with MP alone, but at a cost of significantly greater toxicity. [ABSTRACT FROM AUTHOR]

Published

2011

15. Relationship between elevated immunoglobulin free light chain and the presence of IgH translocations in multiple myeloma.

Author

Kumar, S., Zhang, L., Dispenzieri, A., Van Wier, S., Katzmann, J. A., Snyder, M., Blood, E., DeGoey, R., Henderson, K., Kyle, R. A., Bradwell, A. R., Greipp, P. R., Rajkumar, S. V., and Fonseca, R.

Subjects

IMMUNOGLOBULINS, MULTIPLE myeloma, FLUORESCENCE, PATIENTS, SERUM, ANTINEOPLASTIC agents, CHROMOSOME abnormalities, PROGNOSIS, RESEARCH funding, SURVIVAL analysis (Biometry), FLUORESCENCE in situ hybridization

Abstract

Elevated immunoglobulin free light chain (FLC) level and abnormal FLC ratio are commonly seen in multiple myeloma (MM) and have prognostic implications. We hypothesized that presence of immunoglobin heavy chain (IgH) translocations leads to unbalanced production of light chains and more extreme abnormalities of FLC, and may explain the prognostic value of FLC. We studied 314 patients with newly diagnosed MM enrolled in a phase III trial, in whom results of fluorescence in situ hybridization testing and data on serum FLC levels were available. Cytogenetic analyses and FLC estimates were performed on stored samples and results were correlated with clinical data. The median ratio (FLC ratio) and the absolute difference (FLC diff) between the involved and uninvolved FLC were higher among those with IgH translocations, especially t(14;16). In multivariate analysis, the prognostic value of FLC estimates on progression-free and overall survival were independent of high-risk IgH translocations t(4;14) and t(14;16). A combination of the risk factors; either abnormal FLC estimate and/or the presence of high-risk IgH translocation, achieved better prognostic stratification. We conclude that patients with IgH translocations have higher FLC levels and abnormal ratios, but the prognostic effect of FLC is only partially explained by translocation status. A system including both these risk factors allows better prediction of outcome. [ABSTRACT FROM AUTHOR]

Published

2010

16. Monoclonal gammopathy of undetermined significance (MGUS) and smoldering (asymptomatic) multiple myeloma: IMWG consensus perspectives risk factors for progression and guidelines for monitoring and management.

Author

Kyle, R. A., Durie, B. G. M., Rajkumar, S. V., Landgren, O., Blade, J., Merlini, G., Kröger, N., Einsele, H., Vesole, D. H., Dimopoulos, M., San Miguel, J., Avet-Loiseau, H., Hajek, R., Chen, W. M., Anderson, K. C., Ludwig, H., Sonneveld, P., Pavlovsky, S., Palumbo, A., and Richardson, P. G.

Subjects

*MONOCLONAL gammopathies, *PLASMA cell diseases, *MULTIPLE myeloma, *B cell lymphoma, *LYMPHOMAS

Abstract

Monoclonal gammopathy of undetermined significance (MGUS) was identified in 3.2% of 21 463 residents of Olmsted County, Minnesota, 50 years of age or older. The risk of progression to multiple myeloma, Waldenstrom's macroglobulinemia, AL amyloidosis or a lymphoproliferative disorder is approximately 1% per year. Low-risk MGUS is characterized by having an M protein <15 g/l, IgG type and a normal free light chain (FLC) ratio. Patients should be followed with serum protein electrophoresis at six months and, if stable, can be followed every 2-3 years or when symptoms suggestive of a plasma cell malignancy arise. Patients with intermediate and high-risk MGUS should be followed in 6 months and then annually for life. The risk of smoldering (asymptomatic) multiple myeloma (SMM) progressing to multiple myeloma or a related disorder is 10% per year for the first 5 years, 3% per year for the next 5 years and 1-2% per year for the next 10 years. Testing should be done 2-3 months after the initial recognition of SMM. If the results are stable, the patient should be followed every 4-6 months for 1 year and, if stable, every 6-12 months. [ABSTRACT FROM AUTHOR]

Published

2010

17. International Myeloma Working Group guidelines for the management of multiple myeloma patients ineligible for standard high-dose chemotherapy with autologous stem cell transplantation.

Author

Palumbo, A., Sezer, O., Kyle, R., Miguel, J. S., Orlowski, R. Z., Moreau, P., Niesvizky, R., Morgan, G., Comenzo, R., Sonneveld, P., Kumar, S., Hajek, R., Giralt, S., Bringhen, S., Anderson, K. C., Richardson, P. G., Cavo, M., Davies, F., Bladé, J., and Einsele, H.

Subjects

MULTIPLE myeloma, STEM cell transplantation, B cell lymphoma, CLINICAL medicine, MEDICAL care

Abstract

In 2005, the first guidelines were published on the management of patients with multiple myeloma (MM). An expert panel reviewed the currently available literature as the basis for a set of revised and updated consensus guidelines for the diagnosis and management of patients with MM who are not eligible for autologous stem cell transplantation. Here we present recommendations on the diagnosis, treatment of newly diagnosed non-transplant-eligible patients and the management of complications occurring during induction therapy among these patients. These guidelines will aid the physician in daily clinical practice and will ensure optimal care for patients with MM. [ABSTRACT FROM AUTHOR]

Published

2009

18. International myeloma working group (IMWG) consensus statement and guidelines regarding the current status of stem cell collection and high-dose therapy for multiple myeloma and the role of plerixafor (AMD 3100).

Author

Giralt, S., Stadtmauer, E. A., Harousseau, J. L., Palumbo, A., Bensinger, W., Comenzo, R. L., Kumar, S., Munshi, N. C., Dispenzieri, A., Kyle, R., Merlini, G., Miguel, J. San, Ludwig, H., Hajek, R., Jagannath, S., Blade, J., Lonial, S., Dimopoulos, M. A., Einsele, H., and Barlogie, B.

Subjects

MULTIPLE myeloma, DRUG therapy, HEMAPHERESIS, STEM cell transplantation, THERAPEUTICS, MULTIPLE myeloma diagnosis, MULTIPLE myeloma treatment, AUTOGRAFTS, BIOTHERAPY, HEMATOPOIETIC stem cell transplantation, HETEROCYCLIC compounds, ANTI-HIV agents

Abstract

Multiple myeloma is the most common indication for high-dose chemotherapy with autologous stem cell support (ASCT) in North America today. Stem cell procurement for ASCT has most commonly been performed with stem cell mobilization using colony-stimulating factors with or without prior chemotherapy. The target CD34+ cell dose to be collected as well as the number of apheresis performed varies throughout the country, but a minimum of 2 million CD34+ cells/kg has been traditionally used for the support of one cycle of high-dose therapy. With the advent of plerixafor (AMD3100) (a novel stem cell mobilization agent), it is pertinent to review the current status of stem cell mobilization for myeloma as well as the role of autologous stem cell transplantation in this disease. On June 1, 2008, a panel of experts was convened by the International Myeloma Foundation to address issues regarding stem cell mobilization and autologous transplantation in myeloma in the context of new therapies. The panel was asked to discuss a variety of issues regarding stem cell collection and transplantation in myeloma especially with the arrival of plerixafor. Herein, is a summary of their deliberations and conclusions. [ABSTRACT FROM AUTHOR]

Published

2009

19. Genetic polymorphisms of EPHX1, Gsk3beta, TNFSF8 and myeloma cell DKK-1 expression linked to bone disease in myeloma.

Author

Durie, B. G. M., Van Ness, B., Ramos, C., Stephens, O., Haznadar, M., Hoering, A., Haessler, J., Katz, M. S., Mundy, G. R., Kyle, R. A., Morgan, G. J., Crowley, J., Barlogie, B., Shaughnessy, Jr., J., and Shaughnessy, J Jr

Subjects

GENETIC polymorphisms, BONE diseases, DNA, ONCOLOGY, MULTIVARIATE analysis, CLINICAL trials, COMPARATIVE studies, GROWTH factors, HYDROLASES, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, MULTIPLE myeloma, RESEARCH, RESEARCH funding, SURVIVAL, TRANSFERASES, TUMOR necrosis factors, EVALUATION research, GENE expression profiling, DISEASE complications

Abstract

Bone disease in myeloma occurs as a result of complex interactions between myeloma cells and the bone marrow microenvironment. A custom-built DNA single nucleotide polymorphism (SNP) chip containing 3404 SNPs was used to test genomic DNA from myeloma patients classified by the extent of bone disease. Correlations identified with a Total Therapy 2 (TT2) (Arkansas) data set were validated with Eastern Cooperative Oncology Group (ECOG) and Southwest Oncology Group (SWOG) data sets. Univariate correlates with bone disease included: EPHX1, IGF1R, IL-4 and Gsk3beta. SNP signatures were linked to the number of bone lesions, log(2) DKK-1 myeloma cell expression levels and patient survival. Using stepwise multivariate regression analysis, the following SNPs: EPHX1 (P=0.0026); log(2) DKK-1 expression (P=0.0046); serum lactic dehydrogenase (LDH) (P=0.0074); Gsk3beta (P=0.02) and TNFSF8 (P=0.04) were linked to bone disease. This assessment of genetic polymorphisms identifies SNPs with both potential biological relevance and utility in prognostic models of myeloma bone disease. [ABSTRACT FROM AUTHOR]

Published

2009

20. Is the International Staging System superior to the Durie-Salmon staging system? A comparison in multiple myeloma patients undergoing autologous transplant.

Author

Hari, P. N., Zhang, M.-J., Roy, V., Pérez, W. S., Bashey, A., To, L. B., Elfenbein, G., Freytes, C. O., Gale, R. P., Gibson, J., Kyle, R. A., Lazarus, H. M., McCarthy, P. L., Milone, G. A., Pavlovsky, S., Reece, D. E., Schiller, G., Vela-Ojeda, J., Weisdorf, D., and Vesole, D.

Subjects

MULTIPLE myeloma, TRANSPLANTATION of organs, tissues, etc., LEUKEMIA diagnosis, LEUKEMIA treatment, CANCER relapse, AUTOGRAFTS, COMPARATIVE studies, HEMATOPOIETIC stem cell transplantation, IMMUNOSUPPRESSION, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, PROGNOSIS, RESEARCH, RESEARCH funding, TUMOR classification, EVALUATION research, TREATMENT effectiveness, PREDICTIVE tests, PROPORTIONAL hazards models, RETROSPECTIVE studies, DISEASE progression, KAPLAN-Meier estimator

Abstract

The international staging system (ISS) for multiple myeloma (MM) is a validated alternative to the Durie-Salmon staging system (DSS) for predicting survival at diagnosis. We compared these staging systems for predicting outcomes after upfront autologous stem cell transplantation by analyzing the outcomes of 729 patients between 1995 and 2002. With a median follow-up of 56 months, the univariate probabilities (95% CI) of non-relapse mortality (NRM), relapse, progression-free survival (PFS) and overall survival (OS) at 5 years were 7, 68, 25 and 52%, respectively. The median OS for stages I, II, III by DSS and ISS were 82, 68, 50 and 64, 68, 45 months, respectively. The concordance between the two staging systems was only 36%. Staging systems were formally compared using Cox models fit with DSS and ISS stages. The relative risks of PFS and OS were significantly different for stages I vs II and II vs III for DSS, but only for stages II vs III for ISS. Although both systems were predictive of PFS and OS, the DSS was superior in formal statistical comparison using Brier score. However, neither system was strongly predictive of outcomes, indicating the need for newer schemes incorporating other prognostic markers. [ABSTRACT FROM AUTHOR]

Published

2009

21. International Myeloma Working Group guidelines for serum-free light chain analysis in multiple myeloma and related disorders.

Author

Dispenzieri, A., Kyle, R., Merlini, G., Miguel, J. S., Ludwig, H., Hajek, R., Palumbo, A., Jagannath, S., Blade, J., Lonial, S., Dimopoulos, M., Comenzo, R., Einsele, H., Barlogie, B., Anderson, K., Gertz, M., Harousseau, J. L., Attal, M., Tosi, P., and Sonneveld, P.

Subjects

*IMMUNOGLOBULINS, *BLOOD proteins, *PLASMA cell diseases, *IMMUNOLOGIC diseases, *AMYLOIDOSIS, *LYMPHOPROLIFERATIVE disorders, *PROTEIN metabolism disorders, BONE marrow cancer

Abstract

The serum immunoglobulin-free light chain (FLC) assay measures levels of free κ and λ immunoglobulin light chains. There are three major indications for the FLC assay in the evaluation and management of multiple myeloma and related plasma cell disorders (PCD). In the context of screening, the serum FLC assay in combination with serum protein electrophoresis (PEL) and immunofixation yields high sensitivity, and negates the need for 24-h urine studies for diagnoses other than light chain amyloidosis (AL). Second, the baseline FLC measurement is of major prognostic value in virtually every PCD. Third, the FLC assay allows for quantitative monitoring of patients with oligosecretory PCD, including AL, oligosecretory myeloma and nearly two-thirds of patients who had previously been deemed to have non-secretory myeloma. In AL patients, serial FLC measurements outperform PEL and immunofixation. In oligosecretory myeloma patients, although not formally validated, serial FLC measurements reduce the need for frequent bone marrow biopsies. In contrast, there are no data to support using FLC assay in place of 24-h urine PEL for monitoring or for serial measurements in PCD with measurable disease by serum or urine PEL. This paper provides consensus guidelines for the use of this important assay, in the diagnosis and management of clonal PCD.Leukemia (2009) 23, 215–224; doi:10.1038/leu.2008.307; published online 20 November 2008 [ABSTRACT FROM AUTHOR]

Published

2009

22. Criteria for diagnosis, staging, risk stratification and response assessment of multiple myeloma.

Author

Kyle, R A and Rajkumar, S V

Subjects

*MULTIPLE myeloma, *DIAGNOSIS, *HEALTH risk assessment, *B cell lymphoma, *PLASMACYTOMA, *MULTIPLE myeloma diagnosis, *MEDICAL protocols, *RISK assessment, *TUMOR classification, *TREATMENT effectiveness, *STANDARDS

Abstract

New systems have emerged for diagnosis, staging and response assessment in multiple myeloma (MM). The diagnostic and response criteria recommended are primarily derived from the International Myeloma Working Group, with certain updates and clarifications. The International Staging System is the current standard for staging of myeloma. A new risk stratification model is provided to specifically define high-risk patients who may benefit from novel therapeutic strategies. This paper provides the current criteria for diagnosis, staging, risk stratification and response assessment of MM. [ABSTRACT FROM AUTHOR]

Published

2009

23. Clinical and biological significance of RAS mutations in multiple myeloma.

Author

Chng, W. J., Gonzalez-Paz, N., Price-Troska, T., Jacobus, S., Rajkumar, S. V., Oken, M. M., Kyle, R. A., Henderson, K. J., Van Wier, S., Greipp, P., Van Ness, B., and Fonseca, R.

Subjects

LETTERS to the editor, MULTIPLE myeloma

Abstract

A letter to the editor in response to the article "Clinical and biological significance of RAS mutations in multiple myeloma" published online on June 5, 2008 is presented.

Published

2008

24. Prognostic value of the serum free light chain ratio in newly diagnosed myeloma: proposed incorporation into the international staging system.

Author

Snozek, C. L. H., Katzmann, J. A., Kyle, R. A., Dispenzieri, A., Larson, D. R., Therneau, T. M., Melton III, L. J., Kumar, S., Greipp, P. R., Clark, R. J., Rajkumar, S. V., and Melton, L J 3rd

Subjects

PROGNOSIS, MULTIPLE myeloma treatment, B cell lymphoma, BLOOD plasma, SERODIAGNOSIS

Abstract

To determine if the serum free light chain (FLC) ratio has prognostic value in patients with symptomatic multiple myeloma (MM), baseline serum samples from a well-characterized cohort of 790 newly diagnosed MM patients were tested with the FLC assay. FLC ratio was calculated as kappa/lambda (reference range 0.26-1.65). On the basis of the distribution of values, a cutpoint kappa/lambda FLC ratio of <0.03 or >32 was chosen for further analysis. Overall survival was significantly inferior in patients with an abnormal FLC ratio of <0.03 or >32 (n=479) compared with those with an FLC ratio between 0.03 and 32 (n=311), with median survival of 30 versus 39 months, respectively. We incorporated abnormal FLC ratio with the International Staging System (ISS) risk factors (that is, albumin <3.5 g/dl and serum beta(2)-microglobulin >or=3.5 g/l), to create a risk stratification model with improved prognostic capabilities. Patients with 0, 1, 2 or 3 adverse risk factors had significantly different overall survival, with median survival times of 51, 39, 30 and 22 months, respectively (P<0.001). These findings suggest that the serum FLC ratio at initial diagnosis is an important predictor of prognosis in myeloma, and can be incorporated into the ISS for improved risk stratification. [ABSTRACT FROM AUTHOR]

Published

2008

25. The role of vertebral augmentation in multiple myeloma: International Myeloma Working Group Consensus Statement.

Author

Hussein, M. A., Vrionis, F. D., Allison, R., Berenson, J., Berven, S., Erdem, E., Giralt, S., Jagannath, S., Kyle, R. A., LeGrand, S., Pflugmacher, R., Raie, N., Raikumar, S. V., Randall, L., Roodman, D., Siegel, D., Vescio, R., Zonder, J., and Durie, B. G. M.

Subjects

MULTIPLE myeloma, SPINE abnormalities, TREATMENT of fractures, RADIOTHERAPY, THERAPEUTICS, PATIENTS

Abstract

The article focuses on the role of vertebral augmentation in the treatment of multiple myeloma. The study shows that vertebral augmentation is most likely to benefit those myeloma patients with mechanical pain and can be used for both acute and chronic fractures. However, it is not recommended for asymptomatic fractures unless there is documented increased collapse and deformity progression. A consensus statement from the International Myeloma Working Group is also presented.

Published

2008

26. Genetic aberrations and survival in plasma cell leukemia.

Author

Tiedemann, R. E., Gonzalez-Paz, N., Kyle, R. A., Santana-Davila, R., Price-Troska, T., Van Wier, S. A., Chng, W. J., Ketterling, R. P., Gertz, M. A., Henderson, K., Greipp, P. R., Dispenzieri, A., Lacy, M. Q., Rajkumar, S. V., Bergsagel, P. L., Stewart, A. K., and Fonseca, R.

Subjects

PLASMA cell leukemia, CANCER genetics, CHROMOSOMAL translocation, MULTIPLE myeloma, LEUKEMIA, CANCER, CHROMOSOME abnormalities, COMPARATIVE studies, GENES, RESEARCH methodology, MEDICAL cooperation, MOLECULAR epidemiology, GENETIC mutation, RESEARCH, RESEARCH funding, SURVIVAL, EVALUATION research, SECONDARY primary cancer, DIAGNOSIS

Abstract

Plasma cell leukemia (PCL) is an aggressive and rare hematological malignancy that originates either as primary disease (pPCL) or as a secondary leukemic transformation (sPCL) of multiple myeloma (MM). We report here the genetic aberrations and survival of 80 patients with pPCL or sPCL and make comparisons with 439 cases of MM. pPCL presents a decade earlier than sPCL (54.7 vs 65.3 years) and is associated with longer median overall survival (11.1 vs 1.3 months; P<0.001). 14q32 (IgH) translocations are highly prevalent in both sPCL and pPCL (82-87%); in pPCL IgH translocations almost exclusively involve 11q13 (CCND1), supporting a central etiological role, while in sPCL multiple partner oncogenes are involved, including 11q13, 4p16 (FGFR3/MMSET) and 16q23 (MAF), recapitulating MM. Both show ubiquitous inactivation of TP53 (pPCL 56%; sPCL 83%) by coding mutation or 17p13 deletion; complemented by p14ARF epigenetic silencing in sPCL (29%). Both show frequent N-RAS or K-RAS mutation. Poor survival in pPCL was predicted by MYC translocation (P=0.006). Survival in sPCL was consistently short. Overall pPCL and sPCL are different disorders with distinct natural histories, genetics and survival. [ABSTRACT FROM AUTHOR]

Published

2008

27. Clinically relevant end points and new drug approvals for myeloma.

Author

Anderson, K. C., Kyle, R. A., Rajkumar, S. V., Stewart, A. K., Weber, D., and Richardson, P.

Subjects

*MULTIPLE myeloma, *B cell lymphoma, *CLINICAL medicine, *MYELOMA proteins, *MEDICAL experimentation on humans, *LEUKEMIA

Abstract

This manuscript summarizes the recommendations of the American Society of Hematology/US Food and Drug Administration Workshop on Clinical Endpoints in Multiple Myeloma, which brought together clinical investigators in multiple myeloma, the United States Food and Drug Administration, pharmaceutical companies, patient advocates and other concerned scientists and physicians to provide guidance, consensus and consistency in the definition of clinically relevant end points to expedite new drug approvals for multiple myeloma in the appropriate trial design settings. This manuscript will therefore be a most valuable resource to provide the framework for the design of appropriate clinical trial strategies for more rapid new drug approval in myeloma.Leukemia (2008) 22, 231–239; doi:10.1038/sj.leu.2405016; published online 1 November 2007 [ABSTRACT FROM AUTHOR]

Published

2008

28. Prevention of thalidomide- and lenalidomide-associated thrombosis in myeloma.

Author

Palumbo, A., Rajkumar, S. V., Dimopoulos, M. A., Richardson, P. G., San Miguel, J., Barlogie, B., Harousseau, J., Zonder, J. A., Cavo, M., Zangari, M., Attal, M., Belch, A., Knop, S., Joshua, D., Sezer, O., Ludwig, H., Vesole, D., Bladé, J., Kyle, R., and Westin, J.

Subjects

THROMBOEMBOLISM, CANCER patients, PREOPERATIVE risk factors, CARDIOVASCULAR diseases, MYELOMA proteins, HEPARIN, ANTICOAGULANTS

Abstract

The incidence of venous thromboembolism (VTE) is more than 1‰ annually in the general population and increases further in cancer patients. The risk of VTE is higher in multiple myeloma (MM) patients who receive thalidomide or lenalidomide, especially in combination with dexamethasone or chemotherapy. Various VTE prophylaxis strategies, such as low-molecular-weight heparin (LMWH), warfarin or aspirin, have been investigated in small, uncontrolled clinical studies. This manuscript summarizes the available evidence and recommends a prophylaxis strategy according to a risk-assessment model. Individual risk factors for thrombosis associated with thalidomide/lenalidomide-based therapy include age, history of VTE, central venous catheter, comorbidities (infections, diabetes, cardiac disease), immobilization, surgery and inherited thrombophilia. Myeloma-related risk factors include diagnosis and hyperviscosity. VTE is very high in patients who receive high-dose dexamethasone, doxorubicin or multiagent chemotherapy in combination with thalidomide or lenalidomide, but not with bortezomib. The panel recommends aspirin for patients with 1 risk factor for VTE. LMWH (equivalent to enoxaparin 40 mg per day) is recommended for those with two or more individual/myeloma-related risk factors. LMWH is also recommended for all patients receiving concurrent high-dose dexamethasone or doxorubicin. Full-dose warfarin targeting a therapeutic INR of 2–3 is an alternative to LMWH, although there are limited data in the literature with this strategy. In the absence of clear data from randomized studies as a foundation for recommendations, many of the following proposed strategies are the results of common sense or derive from the extrapolation of data from many studies not specifically designed to answer these questions. Further investigation is needed to define the best VTE prophylaxis.Leukemia (2008) 22, 414–423; doi:10.1038/sj.leu.2405062; published online 20 December 2007 [ABSTRACT FROM AUTHOR]

Published

2008

29. A practical guide to defining high-risk myeloma for clinical trials, patient counseling and choice of therapy.

Author

Stewart, A. K., Bergsagel, P. L., Greipp, P. R., Dispenzieri, A., Gertz, M. A., Hayman, S. R., Kumar, S., Lacy, M. Q., Lust, J. A., Russell, S. J., Witzig, T. E., Zeldenrust, S. R., Dingli, D., Reeder, C. B., Roy, V., Kyle, R. A., Rajkumar, S. V., and Fonseca, R.

Subjects

MULTIPLE myeloma, CLINICAL trials, MEDICAL genetics, PLASMA cells, ANEUPLOIDY

Abstract

Clinical outcomes for multiple myeloma (MM) are highly heterogeneous and it is now clear that pivotal genetic events are the primary harbingers of such variation. These findings have broad implications for counseling, choice of therapy and the design and interpretation of clinical investigation. Indeed, as in acute leukemias and non-hodgkins lymphoma, we believe it is no longer acceptable to consider MM a single disease entity. As such, the accurate diagnosis of MM subtypes and the adoption of common criteria for the identification and stratification of MM patients has become critical. Herein, we provide a consensus high-risk definition and offer practical guidelines for the adoption of routine diagnostic testing. Although acknowledging that more refined classifications will continue to be developed, we propose that the definition of high-risk disease (any of the t(4;14), t(14;16), t(14;20), deletion 17q13, aneuploidy or deletion chromosome 13 by metaphase cytogenetics, or plasma cell labeling index >3.0) be adopted. This classification will identify most of the 25% of MM patients for whom current therapies are inadequate and for whom investigational regimens should be vigorously pursued. Conversely, the 75% of patients remaining have more favorable outcomes using existing – albeit non-curative – therapeutic options.Leukemia (2007) 21, 529–534. doi:10.1038/sj.leu.2404516; published online 18 January 2007 [ABSTRACT FROM AUTHOR]

Published

2007

30. Elevation of soluble CD307 (IRTA2/FcRH5) protein in the blood and expression on malignant cells of patients with multiple myeloma, chronic lymphocytic leukemia, and mantle cell lymphoma.

Author

Ise, T., Nagata, S., Kreitman, R. J., Wilson, W. H., Wayne, A. S., Stetler-Stevenson, M., Bishop, M. R., Scheinberg, D. A., Rassenti, L., Kipps, T. J., Kyle, R. A., Jelinek, D. F., and Pastan, I.

Subjects

MULTIPLE myeloma, CHRONIC lymphocytic leukemia, ANTIGENS, FLOW cytometry, IMMUNOTHERAPY, POLYMERASE chain reaction, B cell lymphoma, PLASMA cells

Abstract

CD307 is a differentiation antigen expressed in B-lineage cells. One soluble and two membrane-bound forms have been predicted and an enzyme-linked immunosorbent assay (ELISA) for soluble CD307 established. Our goal was to determine if CD307 is expressed on the surface of cells from patients with multiple myeloma (MM), chronic lymphocytic leukemia (CLL), mantle cell lymphoma (MCL) and other B-cell malignancies and if soluble CD307 levels are elevated in the blood of patients with these B-cell malignancies. Cells and blood were collected from patients. Expression of CD307 was measured by flow cytometry and blood levels of soluble CD307 by ELISA. High soluble CD307 levels were detected in 21/43 (49%) of patients with MM, 36/46 (78%) with CLL and 9/24 (38%) with MCL. Soluble CD307 levels correlated with plasma cell percentages in bone marrow aspirates in MM and total white blood cells in CLL. CD307 on the cell membrane was detected by flow cytometry in 8/8 MM, 23/29 CLL and 4/5 MCL samples. Because CD307 is present on malignant cells from patients with MM, CLL and MCL, CD307 may be a useful therapeutic target for the treatment of these diseases. [ABSTRACT FROM AUTHOR]

Published

2007

31. International uniform response criteria for multiple myeloma.

Author

Durie, B. G. M., Harousseau, J.-L., Miguel, J. S., Bladé, J., Barlogie, B., Anderson, K., Gertz, M., Dimopoulos, M., Westin, J., Sonneveld, P., Ludwig, H., Gahrton, G., Beksac, M., Crowley, J., Belch, A., Boccadaro, M., Turesson, I., Joshua, D., Vesole, D., and Kyle, R.

Subjects

MULTIPLE myeloma, RESPONSE rates, CLINICAL trials, EVALUATION, MYELOMA proteins, HEALTH outcome assessment

Abstract

New uniform response criteria are required to adequately assess clinical outcomes in myeloma. The European Group for Blood and Bone Marrow Transplant/International Bone Marrow Transplant Registry criteria have been expanded, clarified and updated to provide a new comprehensive evaluation system. Categories for stringent complete response and very good partial response are added. The serum free light-chain assay is included to allow evaluation of patients with oligo-secretory disease. Inconsistencies in prior criteria are clarified making confirmation of response and disease progression easier to perform. Emphasis is placed upon time to event and duration of response as critical end points. The requirements necessary to use overall survival duration as the ultimate end point are discussed. It is anticipated that the International Response Criteria for multiple myeloma will be widely used in future clinical trials of myeloma.Leukemia (2006) 20, 1467–1473. doi: 10.1038/sj.leu.2404284; published online 20 July 2006 [ABSTRACT FROM AUTHOR]

Published

2006

32. Prognostic factors for hyperdiploid-myeloma: effects of chromosome 13 deletions and IgH translocations.

Author

Chng, W. J., Santana-Dávila, R., Van Wier, S. A., Ahmann, G. J., Jalal, S. M., Bergsagel, P. L., Chesi, M., Trendle, M. C., Jacobus, S., Blood, E., Oken, M. M., Henderson, K., Kyle, R. A., Gertz, M. A., Lacy, M. Q., Dispenzieri, A., Greipp, P. R., and Fonseca, R.

Subjects

CANCER genetics, CANCER patients, CHROMOSOMES, IMMUNOGLOBULINS, CHROMOSOMAL translocation

Abstract

Chromosomal hyperdiploidy is the defining genetic signature in 40–50% of myeloma (MM) patients. We characterize hyperdiploid-MM (H-MM) in terms of its clinical and prognostic features in a cohort of 220 H-MM patients entered into clinical trials. Hyperdiploid-myeloma is associated with male sex, kappa immunoglobulin subtype, symptomatic bone disease and better survival compared to nonhyperdiploid-MM (median overall survival 48 vs 35 months, log-rank P=0.023), despite similar response to treatment. Among 108 H-MM cases with FISH studies for common genetic abnormalities, survival is negatively affected by the existence of immunoglobulin heavy chain (IgH) translocations, especially those involving unknown partners, while the presence of chromosome 13 deletion by FISH did not significantly affect survival (median overall survival 50 vs 47 months, log-rank P=0.47). Hyperdiploid-myeloma is therefore a unique genetic subtype of MM associated with improved outcome with distinct clinical features. The existence of IgH translocations but not chromosome 13 deletion by FISH negatively impacts survival and may allow further risk stratification of this population of MM patients.Leukemia (2006) 20, 807–813. doi:10.1038/sj.leu.2404172; published online 2 March 2006 [ABSTRACT FROM AUTHOR]

Published

2006

33. Thalidomide as initial therapy for early-stage myeloma.

Author

Rajkumar, S V, Gertz, M A, Lacy, M Q, Dispenzieri, A, Fonseca, R, Geyer, S M, Iturria, N, Kumar, S, Lust, J A, Kyle, R A, Greipp, P R, and Witzig, T E

Subjects

MULTIPLE myeloma, THALIDOMIDE

Abstract

Patients with early-stage myeloma are typically observed without therapy until symptomatic disease occurs. However, they are at high risk of progression to symptomatic myeloma, with a median time to progression of approximately 1-2 years. We report the final results of a phase II trial of thalidomide as initial therapy for early-stage multiple myeloma in an attempt to delay progression to symptomatic disease. In total, 31 patients with smoldering or indolent multiple myeloma were studied at the Mayo Clinic. Two patients were deemed ineligible because they were found to have received prior therapy for myeloma, and were excluded from analyses except for toxicity. Thalidomide was initiated at a starting dose of 200 mg/day. Patients were followed-up monthly for the first 6 months and every 3 months thereafter. Of the 29 eligible patients, 10 (34%) had a partial response to therapy with at least 50% or greater reduction in serum and urine monoclonal (M) protein. When minor responses (25-49% decrease in M protein) were included, the response rate was 66%. Three patients had progressive disease while on therapy. Kaplan-Meier estimates of progression-free survival are 80% at 1 year and 63% at 2 years. Major grade 3-4 toxicities included two patients with somnolence and one patient each with neuropathy, deep-vein thrombosis, hearing loss, weakness, sinus bradycardia, and edema. Thalidomide has significant activity in early-stage myeloma and has the potential to delay progression to symptomatic disease. This approach must be further tested in randomized trials. [ABSTRACT FROM AUTHOR]

Published

2003

34. Chromosome abnormalities clustering and its implications for pathogenesis and prognosis in myeloma.

Author

Debes-Marun, C S, Dewald, G W, Bryant, S, Picken, E, Santana-Dávila, R, González-Paz, N, Winkler, J M, Kyle, R A, Gertz, M A, Witzig, T E, Dispenzieri, A, Lacy, M Q, Rajkumar, S V, Lust, J A, Greipp, P R, and Fonseca, R

Subjects

CHROMOSOME abnormalities, KARYOTYPES, LEUKEMIA

Abstract

The nonrandom recurrent nature of chromosome abnormalities in myeloma suggests a role for them in disease pathogenesis. We performed a careful cytogenetic analysis of patients with abnormal karyotypes (n = 254), to discern patterns of association, search for novel abnormalities and elucidate clinical implications. Patients with karyotypic abnormalities suggestive of myelodysplasia/acute leukemia were excluded. In this study we compared survival by abnormality only between patients with abnormal karyotypes. Patients with abnormalities were more likely to have features of aggressive disease as compared to all other patients without abnormalities entered into the myeloma database (lower hemoglobin, higher β[sub 2]-microglobulin, labeling-index and plasmocytosis; all P < 0.0001). Several groups of patients could be readily identified; hypodiploid (22%), pseudodiploid (36%), hyperdiploid (31%) and near-tetraploid (11%). Clustering associations were seen among several trisomies and monosomy of chromosome 13 and 14. Several monosomies (-2, -3, -13, -14 and -19), 1p translocations/ deletions, and hypodiploidy were associated with a significantly shorter survival. Trisomy of chromosome 13 was rare (<2%). Even among patients with abnormal karyotypes, specific chromosome abnormalities can impart biologic variability in myeloma, including several monosomies, hypodiploidy and abnormalities of 1 p. [ABSTRACT FROM AUTHOR]

Published

2003

35. Contrast in cytokine expression between patients with monoclonal gammopathy of undetermined significance or multiple myeloma.

Author

Donovan, K A, Lacy, M Q, Kline, M P, Ahmann, G J, Heimbach, J K, Kyle, R A, and Lust, J A

Subjects

MULTIPLE myeloma, CYTOKINES, INTERLEUKINS, PLASMA cells, B cells, COMPARATIVE studies, FLOW cytometry, IN situ hybridization, INTERLEUKIN-1, RESEARCH methodology, MEDICAL cooperation, PARAPROTEINEMIA, POLYMERASE chain reaction, RESEARCH, RNA, EVALUATION research

Abstract

We investigated whether differences in IL-6 and IL-1beta expression could be detected in monoclonal plasma cells from patients with MGUS or MM. Expression of IL-6 and IL-1beta in bone marrow cells was determined using cell sorting to enrich for plasma cells followed by reverse transcriptase/polymerase chain reaction (RT/PCR). Nineteen patients (six MGUS, two primary amyloid (AL), 11 MM) were studied. IL-6 mRNA expression was detectable in the sorted CD38+/CD45- plasma cell populations from 0/6 MGUS, 0/2 AL and 5/11 MM patients. All five MM patients with autocrine IL-6 expression demonstrated an elevated plasma cell labeling index. IL-1beta mRNA was detectable in the sorted CD38+/CD45- plasma cell populations from 1/6 MGUS, 0/2 AL and 10/11 MM patients. In situ hybridization (ISH) confirmed that the IL-1beta producing cells were plasma cells. In conclusion, autocrine production of IL-6 parallels a high labeling index and aberrant expression of IL-1beta correlates with the diagnosis of MM. Follow-up of IL-1beta-positive MGUS patients will determine whether aberrant expression of IL-1beta will predict those MGUS patients that will eventually progress to MM. [ABSTRACT FROM AUTHOR]

Published

1998

36. Long-term response to lenalidomide in patients with newly diagnosed multiple myeloma.

Author

Kourelis, T V, Kumar, S K, Srivastava, G, Gertz, M A, Lacy, M Q, Buadi, F K, Kyle, R A, and Dispenzieri, A

Subjects

DRUG efficacy, MULTIPLE myeloma treatment

Abstract

A letter to the editor is presented which discusses the efficacy of immunomodulatory (Imid) drug Lenalidomide as treatment for patients with newly diagnosed multiple myeloma.

Published

2014

37. Risk of acute leukemia and myelodysplastic syndromes in patients with monoclonal gammopathy of undetermined significance (MGUS): a population-based study of 17 315 patients.

Author

Roeker, L E, Larson, D R, Kyle, R A, Kumar, S, Dispenzieri, A, and Rajkumar, S V

Abstract

The purpose of this study was to determine if there is an increased risk of acute leukemia and myelodysplastic syndromes (MDS) in persons with monoclonal gammopathy of undetermined significance (MGUS). We used a large population-based cohort of individuals systematically screened for the presence or absence of MGUS. MGUS status was then linked to the diagnosis of acute myeloid leukemia (AML), acute lymphoblastic leukemia (ALL) and MDS. A total of 17 315 patients age 50 and older (605 MGUS and 16 710 controls) with a cumulative 435 021 person-years of follow-up were studied. MGUS patients had a significantly higher risk of developing MDS compared with controls, hazard ratio 2.4 (95% CI 1.08, 5.32), P=0.031. There was no statistically significant increase in the risk of AML (RR 1.36 P=0.675), and no increased risk of developing ALL. [ABSTRACT FROM AUTHOR]

Published

2013

38. Efficacy of thalidomide- or lenalidomide-based therapy in proliferative multiple myeloma.

Author

Kapoor, P., Kumar, S., Mandrekar, S. J., Laumann, K. M., Dispenzieri, A., Lacy, M. Q., Dingli, D., Gertz, M. A., Kyle, R. A., Greipp, P. R., Rajkumar, S. V., and Witzig, T. E.

Subjects

LETTERS to the editor, MULTIPLE myeloma treatment, THALIDOMIDE

Abstract

A letter to the editor is presented regarding the impact of thalidomide-dexamethasone (Thal-Dex) or lenalidomide-dexamethasone (Len-Dex) based therapy on proliferative multiple myeloma (MM).

Published

2011

39. Incidence of extramedullary disease in patients with multiple myeloma in the era of novel therapy, and the activity of pomalidomide on extramedullary myeloma.

Author

Detweiler^Short, K., Rajkumar, S. V., Larson, D., Buadi, F., Hayman, S., Dispenzieri, A., Gertz, M., Kumar, S., Mikhael, J., Roy, V., Kyle, R. A., Lacy, M. Q., and Short, K Detweiler

Subjects

MULTIPLE myeloma treatment, MULTIPLE myeloma diagnosis, TREATMENT effectiveness, DISEASE incidence, DEXAMETHASONE, CLINICAL trials, CLINICAL medicine, ANTINEOPLASTIC agents, COMPARATIVE studies, RESEARCH methodology, MEDICAL cooperation, MULTIPLE myeloma, RESEARCH, RESEARCH funding, SURVIVAL, EVALUATION research, THALIDOMIDE, PHARMACODYNAMICS, THERAPEUTICS

Abstract

We studied 174 consecutive patients with relapsed refractory multiple myeloma (MM) enrolled on a phase II clinical trial of pomalidomide plus low-dose dexamethasone at Mayo Clinic. Extramedullary disease (EMD) was present at the time of trial entry in 7.5% (13 of 174 patients). The rate of EMD in the first 3 years following diagnosis of MM was 3%. The response of EMD to pomalidomide plus low-dose dexamethasone included two complete and two partial responses among the 13 patients (response rate, 31%). Overall survival measured from trial entry was significantly shorter for patients with treatment-emergent EMD compared with those who did not have EMD, (median 16 months versus not reached, P=0.002). [ABSTRACT FROM AUTHOR]

Published

2011

40. Five decades of therapy for multiple myeloma: a paradigm for therapeutic models.

Author

Kyle, R. A.

Subjects

*PROTEINS, *IMMUNOGLOBULINS, *LEUKEMIA, *MULTIPLE myeloma, *B cell lymphoma, *BLOOD plasma

Abstract

Discusses a study conducted by researchers from the United States, which demonstrated that there were two main classes of light-chain proteins. Similarity of the Bence Jones protein to the light chains of the intact serum immunoglobulin in the multiple myeloma patient; Disadvantages of using alkylating agents in multiple myeloma; Emphasis on the risk of development of myelodysplasia or acute leukemia.

Published

2005

41. Thalidomide for previously untreated indolent or smoldering multiple myeloma.

Author

Rajkumar, S V, Dispenzieri, A, Fonseca, R, Lacy, M Q, Geyer, S, Lust, J A, Kyle, R A, Greipp, P R, Gertz, M A, and Witzig, T E

Subjects

THALIDOMIDE, MULTIPLE myeloma treatment

Abstract

We conducted a clinical trial of thalidomide as initial therapy for asymptomatic smoldering (SMM) or indolent multiple myeloma (IMM). Sixteen patients were studied. Thalidomide was given orally at a dose of 200 mg/day for 2 weeks, and then increased as tolerated by 200 mg/day every 2 weeks to a maximum dose of 800 mg/day. Bone marrow microvessel density (MVD) and angiogenesis grading were estimated using CD34 immunostaining. Six patients had a confirmed response to therapy with at least 50% or greater reduction in serum and urine monoclonal (M) protein. When minor responses (25-49%) decrease in M protein concentration) were included, 11 of 16 patients (69%) responded to therapy. Major grade 3-4 toxicities included two patients with somnolence, and one patient each with syncope and neutropenia. Pre-treatment MVD was not a significant predictor of response to therapy, median MVD 4 and 12 in responders and non-responders respectively, P = 0.09. We conclude that thalidomide has significant activity in the treatment of newly diagnosed SMM/IMM. However, we do not recommend treatment with thalidomide at this stage since some patients with SMM/IMM can be stable for several months or years without any therapy. Additional randomized trials are needed to determine if thalidomide will delay progression to active multiple myeloma. [ABSTRACT FROM AUTHOR]

Published

2001

42. Single-nucleotide polymorphism rs1052501 associated with monoclonal gammopathy of undetermined significance and multiple myeloma.

Author

Greenberg, A J, Lee, A M, Serie, D J, McDonnell, S K, Cerhan, J R, Liebow, M, Larson, D R, Colby, C L, Norman, A D, Kyle, R A, Kumar, S, Rajkumar, S V, Diasio, R B, Slager, S L, and Vachon, C M

Subjects

LETTERS to the editor, GENETIC polymorphisms, MULTIPLE myeloma

Abstract

A letter to the editor is presented regarding the association of single-nucleotide polymorphism rs1052501 with monoclonal gammopathy of undetermined significance (GMUS) and multiple myeloma (MM).

Published

2013

43. Polymorphism of the erythropoietin gene promotor and the development of myelodysplastic syndromes subsequent to multiple myeloma.

Author

Landgren, O, Ma, W, Kyle, R A, Rajkumar, S V, Korde, N, and Albitar, M

Subjects

LETTERS to the editor, ERYTHROPOIETIN receptors, MYELODYSPLASTIC syndromes, PATIENTS

Abstract

A letter to the editor is presented regarding the single-nucleotide polymorphism (SNP) of erythropoietin (EPO) promoter and its prevalence in myelodysplastic syndrome (MDS) patients.

Published

2012

44. Criteria for diagnosis, staging, risk stratification and response assessment of multiple myeloma.

Author

Kyle, R A and Rajkumar, S V

Subjects

*CREATININE, *MULTIPLE myeloma diagnosis

Abstract

A correction to the article "Criteria for diagnosis, staging, risk stratification and response assessment of multiple myeloma" that was published in the 2009 issue is presented.

Published

2014