Impact of Minimal Residual Negativity Using Next Generation Flow Cytometry on Outcomes in Light Chain Amyloidosis

Overview

Journal Am J Hematol

Specialty Hematology

Date 2020 Feb 4

PMID 32010993

Citations 19

Authors

Surbhi Sidana

Eli Muchtar

M Hasib Sidiqi

Dragan Jevremovic

Angela Dispenzieri

Wilson Gonsalves

Francis Buadi

Martha Q Lacy

Suzanne R Hayman

Taxiarchis Kourelis

Prashant Kapoor

Ronald S Go

Rahma Warsame

Nelson Leung

S Vincent Rajkumar

Robert A Kyle

Morie A Gertz

Shaji K Kumar

Affiliations

Soon will be listed here.

Abstract

We evaluated bone marrow minimal residual disease (MRD) negativity in 44 patients with light chain (AL) amyloidosis using next generation flow cytometry (sensitivity ≥1 × 10 ; median events analyzed: 8.7 million, range: 4.8 to 9.7 million). All patients underwent MRD testing in 2 years from start of therapy (median: 7 months). The overall MRD negative rate was 64% (n = 28). The MRD-negative rate after one-line of therapy was 71% (20/28). And, MRD negative rates were higher with stem-cell transplant as first-line therapy (86%, 18/21) vs chemotherapy alone as first-line treatment (29%, 2/7), P = .005. The MRD negative rate amongst patients in complete response was 75% (15/20), and in very good partial response, 50% (11/22). There were two patients in partial response/rising light chains (with renal dysfunction) who were MRD negative. There were no differences in baseline characteristics of MRD negative vs MRD positive patients, except younger age amongst MRD-negative patients. Patients with MRD negativity were more likely to have achieved cardiac response at the time of MRD assessment, 67% (8/12) vs 22% (2/7), P = .04. Renal response rates were similar in both groups. Progression free survival was assessed in the 42 patients achieving CR or VGPR. After median follow-up of 14 months, the estimated 1-year progression free survival in MRD negative vs MRD positive patients was 100% (26 patients, 0 events) vs 64% (16 patients, five events), P = .006, respectively. MRD assessment should be explored as a surrogate endpoint in clinical trials and MRD risk-adapted trials may help optimize treatment in AL amyloidosis.

Citing Articles

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Early minimal residual disease eradication in light chain amyloidosis generates deeper and faster cardiac response.

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