A pilot study of pembrolizumab in smoldering myeloma: report of the clinical, immune, and genomic analysis

Author:

Manasanch Elisabet E.1ORCID,Han Guangchun2,Mathur Rohit1,Qing Yun3,Zhang Zheng1,Lee Hans1ORCID,Weber Donna M.1,Amini Behrang4ORCID,Berkova Zuzana1ORCID,Eterovic Karina5,Zhang Shaojun2ORCID,Zhang Jianhua2,Song Xingzhi2,Mao Xizeng2,Morgan Margaret5,Feng Lei3,Baladandayuthapani Veera3,Futreal Andrew2,Wang Linghua2ORCID,Neelapu Sattva S.1ORCID,Orlowski Robert Z.16

Affiliation:

1. Department of Lymphoma/Myeloma,

2. Department of Genomic Medicine,

3. Department of Biostatistics,

4. Department of Diagnostic Radiology, Division of Diagnostic Imaging,

5. Genomics Platform, and

6. Department of Experimental Therapeutics, The University of Texas MD Anderson Cancer Center, Houston, TX

Abstract

Abstract Multiple myeloma is, in most patients, an incurable cancer. Its precursors can be identified with routine tests setting the stage for early intervention to prevent active myeloma. We investigated the efficacy and safety of pembrolizumab, an antiprogrammed cell death 1 antibody, in smoldering myeloma patients with intermediate/high risk of progression to symptomatic myeloma. Thirteen patients were treated with a median number of 8 cycles. One patient achieved a stringent complete response with bone marrow next-generation sequencing negativity at 10−4 that is ongoing at 27 months (8%); 11 had stable disease (85%), and 1 progressed (8%). Three patients discontinued therapy due to immune-related adverse events: 2 with transaminitis and 1 due to tubulointerstitial nephritis. Immune profiling of bone marrow samples at baseline showed markers associated with a preexisting immune response in the responder compared with nonresponders and features of increased T-cell exhaustion in nonresponders. Consistent with this, transcriptome sequencing of bone marrow samples at baseline revealed an increased interferon-γ signature in the responder compared with the nonresponders. In summary, our results suggest that smoldering myeloma may be immunogenic in a subset of patients, and therapies that enhance antitumor T-cell responses may be effective in preventing its progression. This trial was registered at www.clinicaltrials.gov as #NCT02603887.

Publisher

American Society of Hematology

Subject

Hematology

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