Your search keyword '"Murray, David L."' showing total 11 results

1. Implications of detecting serum monoclonal protein by MASS‐fix following stem cell transplantation in multiple myeloma.

Author

Abeykoon, Jithma P., Murray, David L., Murray, Isaiah, Jevremovic, Dragan, Otteson, Gregory E., Dispenzieri, Angela, Arendt, Bonnie K., Dasari, Surendra, Gertz, Morie, Gonsalves, Wilson I., Kourelis, Taxiarchis V., Muchtar, Eli, Dingli, David, Warsame, Rahma, Go, Ronald S., Lacy, Martha Q., Leung, Nelson, Buadi, Francis, Lin, Yi, and Kyle, Robert A.

Subjects

*STEM cell transplantation, *MULTIPLE myeloma, *BLOOD proteins, *DESORPTION ionization mass spectrometry

Abstract

Summary: Measurable residual disease (MRD) assessment by marrow‐based next‐generation flow cytometry (NGF) following autologous stem cell transplantation (ASCT) may lead to false‐negative results due to patchy marrow involvement and extramedullary disease in patients with multiple myeloma. We assessed the value of simultaneous MRD evaluation with NGF and serum matrix‐assisted laser desorption ionization time‐of‐flight mass spectrometry (MASS‐FIX). Of all 61 complete responders who were NGF‐negative for MRD, around day‐100 post ASCT, 59% were MASS‐FIX‐positive. At median follow‐up of 26 months, 69% of MASS‐FIX(+)/NGF(−) patients were alive and progression‐free versus 96% of MASS‐FIX(‐)/NGF(−) patients, P = 0·02. MASS‐FIX, a simple peripheral blood‐based assay complements marrow‐based NGF to accurately prognosticate patients with myeloma. [ABSTRACT FROM AUTHOR]

Published

2021

2. In from the cold: M‐protein light chain glycosylation is positively associated with cold agglutinin titer levels.

Author

Juskewitch, Justin E., Murray, Josiah D., Norgan, Andrew P., Moldenhauer, Sheila K., Tauscher, Craig D., Jacob, Eapen K., and Murray, David L.

Subjects

GLYCOSYLATION, TITERS, COOMBS' test, MONOCLONAL antibodies, CARDIAC amyloidosis, DIAGNOSIS, CA 19-9 test

Abstract

Background: Primary cold agglutinin disease (CAD) is a monoclonal antibody (M‐protein) and complement‐mediated chronic hemolytic disease process. Antibody glycosylation can play a role in both antibody half‐life and complement fixation. Recently, M‐protein light chain (LC) glycosylation has been shown to be associated with AL amyloidosis. We hypothesized that M‐protein LC glycosylation is also associated with cold agglutinin (CA) titers and CA‐mediated hemolysis. Study Design and Methods: A cross‐sectional study of patients undergoing CA titer evaluation underwent mass spectrometric analysis for M‐proteins and M‐protein LC glycosylation. A subset of serum samples also underwent evaluation for the ability to trigger cold hemolysis in vitro. M‐protein and M‐protein LC glycosylation rates were compared across CA titer groups, clinical diagnosis, direct antiglobulin testing (DAT) results, and cold in vitro hemolysis rates. Results: Both M‐protein and M‐protein LC glycosylation rates significantly differed across CA titer groups with the highest rates in those with elevated CA titers. M‐protein LC glycosylation occurred almost exclusively on IgM kappa M‐proteins and was significantly associated with positive DAT results and a clinical diagnosis of CAD. Cold in vitro hemolysis was demonstrated in two patients who both had a CA titer of more than 512 but there was no significant association with CA titer group or M‐protein LC glycosylation status. Conclusion: M‐protein LC glycosylation is significantly associated with higher CA titer levels. Given the role that antibody glycosylation can play in antibody half‐life and complement fixation, further studies are needed to clarify the effects of LC glycosylation within the context of CAD. [ABSTRACT FROM AUTHOR]

Published

2021

3. Glycosylation of immunoglobulin light chains is highly prevalent in cold agglutinin disease.

Author

Sidana, Surbhi, Murray, David L., Dasari, Surendra, Go, Ronald S., Muchtar, Eli, Willrich, Maria A., Snyder, Melissa, Kohlhagen, Mindy, Lust, John A., Kourelis, Taxiarchis V., Kumar, Shaji K., Dispenzieri, Angela, and Gertz, Morie A.

Published

2020

4. Systemic AL amyloidosis with an undetectable plasma cell dyscrasia: A zebra without stripes.

Author

Staron, Andrew, Kataria, Yachana, Murray, David L., Sloan, J. Mark, and Sanchorawala, Vaishali

Published

2020

5. Clinical features, laboratory characteristics and outcomes of patients with renal versus cardiac light chain amyloidosis.

Author

Sidana, Surbhi, Tandon, Nidhi, Gertz, Morie A., Dispenzieri, Angela, Ramirez‐Alvarado, Marina, Murray, David L., Kourelis, Taxiarchis V., Buadi, Francis K., Kapoor, Prashant, Gonsalves, Wilson, Warsame, Rahma, Lacy, Martha Q., Kyle, Robert A., Rajkumar, S. Vincent, Kumar, Shaji K., and Leung, Nelson

Subjects

CARDIAC amyloidosis, BONE marrow cells, AMYLOIDOSIS, REGRESSION analysis

Abstract

Summary: This study evaluated the differences in clinical features of 1077 newly diagnosed AL amyloidosis patients with renal involvement (n = 229, 21%), both cardiac and renal involvement (n = 443, 41%) and cardiac involvement (n = 405, 38%). Significant differences in dFLC (difference in involved and uninvolved light chains) were noted (renal, both, cardiac median: 83, 234 and 349 mg/l, P < 0.001). The proportion of patients with ≥ 10% bone marrow plasma cells (BMPCs) was lowest in renal only patients: 44%, 57%, 64%, respectively, P < 0.001. In a multivariate linear regression model incorporating organ involvement type and BMPCs ≥10%, organ involvement was a significant predictor of dFLC (P < 0.001). Median overall survival (OS) across the three groups was 83 vs. 19 vs. 16 months (P < 0.001) in patients not undergoing transplant and 5‐year OS in patients undergoing transplant was 90% vs. 75% vs. 64% (P = 0.007), respectively. In conclusion, renal involvement alone or renal + cardiac involvement in AL amyloidosis is associated with lower circulating light chain burden, which cannot be fully explained by BMPC burden alone. Increased sensitivity of the kidney to light chains, given significant interactions with the renal tubular system and secretion of modified light chain products may play a role in pathogenesis of renal AL amyloidosis and warrants further investigation. [ABSTRACT FROM AUTHOR]

Published

2019

6. The utility of MASS-FIX to detect and monitor monoclonal proteins in the clinic.

Author

Milani, Paolo, Murray, David L., Barnidge, David R., Kohlhagen, Mindy C., Mills, John R., Merlini, Giampaolo, Dasari, Surendra, and Dispenzieri, Angela

Published

2017

7. Assessment of renal response with urinary exosomes in patients with AL amyloidosis: A proof of concept.

Author

Ramirez-Alvarado, Marina, Barnidge, David R., Murray, David L., Dispenzieri, Angela, Marin-Argany, Marta, Dick, Christopher J., Cooper, Shawna A., Nasr, Samih H, Ward, Christopher J., Dasari, Surendra, Jiménez-Zepeda, Víctor H., and Leung, Nelson

Published

2017

8. MASS‐FIX may allow identification of patients at risk for light chain amyloidosis before the onset of symptoms.

Author

Kourelis, Taxiarchis, Murray, David L., Dasari, Surendra, Kumar, Sanjay, Barnidge, David, Madden, Benjamin, Arendt, Bonnie, Milani, Paolo, Merlini, Giampaolo, Ramirez‐Alvarado, Marina, Kyle, Robert A., and Dispenzieri, Angela

Published

2018

9. Using matrix-assisted laser desorption/ionization time-of-flight mass spectrometry to detect monoclonal immunoglobulin light chains in serum and urine.

Author

Barnidge, David R., Krick, Thomas P., Griffin, Timothy J., and Murray, David L.

Subjects

MATRIX-assisted laser desorption-ionization, TIME-of-flight mass spectrometry, URINALYSIS, MONOCLONAL antibodies, BLOOD serum analysis

Abstract

Rationale Use of matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOFMS) to monitor serum and urine samples for endogenous monoclonal immunoglobulins. MALDI-TOFMS is faster, fully automatable, and provides superior specificity compared to protein gel electrophoresis (PEL). Methods Samples were enriched for immunoglobulins in 5 min using Melon Gel™ followed by reduction with dithiothreitol for 15 min to separate immunoglobulin light chains and heavy chains. Samples were then desalted using C4 ZipTips, mixed with sinapinic acid matrix, and analyzed on a Bruker Biflex III MALDI-TOF mass spectrometer. Results Monoclonal immunoglobulin light chains were identified in serum and urine samples from patients with a known monoclonal gammopathy using MALDI-TOFMS with minimal sample preparation. Conclusions MALDI-TOFMS can identify a monoclonal immunoglobulin in serum and urine samples. The molecular mass of the monoclonal immunoglobulin light chain is obtained providing unprecedented specificity compared to PEL. In addition, the methodology can be automated, making it a practical alternative to PEL. Copyright © 2015 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2015

10. Detecting monoclonal light chains in urine: micro LC- ESI-Q- TOF mass spectrometry compared to immunofixation electrophoresis.

Author

Botz, Chad M., Barnidge, David R., Murray, David L., and Katzmann, Jerry A.

Subjects

URINE, MONOCLONAL antibodies, ELECTROPHORESIS, ELECTROSPRAY ionization mass spectrometry, SERUM, MOLECULAR weights

Abstract

The article discusses a study on detection of monoclonal light chains in urine. Topics discussed include use of urine protein electrophoresis (PEL) and immunofixation electrophoresis (IFE) for identifying a monoclonal immunoglobulin, electrospray-ionization time-of-flight mass spectrometry (microLC-ESI-Q-TOF MS) as an alternative to PEL and IFE for identifying monoclonal light chains in serum and urine, and same molecular mass of monoclonal light chain found in serum and urine.

Published

2014

11. Detecting monoclonal light chains in urine: microLC-ESI-Q-TOF mass spectrometry compared to immunofixation electrophoresis.

Author

Botz, Chad M., Barnidge, David R., Murray, David L., and Katzmann, Jerry A.

Published

2014