Chemotherapy-Related Mutational Signatures Reveal the Origins of Therapy-Related Myeloid Neoplasms

Diamond, Benjamin; Ziccheddu, Bachisio; Boyle, Eileen M.; Maclachlan, Kylee; Ossa, Juan Arango; Taylor, J. Richard; Watts, Justin M.; Lu, Sydney X.; Yellapantula, Venkata D.; Famulare, Christopher; Chojnacka, Monika; Rajanna, Arjun Raj; Mason, Emilia; Coffey, David G.; Hoffman, James E.; Kazandjian, Dickran; Bradley, Terrence; Zhu, Meng-Lei; Bolli, Niccolò; Papaemmanuil, Elli; Bolton, Kelly L.; Scordo, Michael; Lahoud, Oscar; Stein, Eytan M.; Sauter, Craig S.; Hassoun, Hani; Mailankody, Sham; Korde, Neha; Hultcrantz, Malin; Shah, Urvi; Shah, Gunjan L.; Park, Jae H.; Landau, Heather; Ganesh, Karuna; Sekeres, Mikkael A.; Nimer, Stephen D.; Chung, David J.; Ho, Caleb; Roshal, Mikhail; Lesokhin, Alexander M.; Morgan, Gareth J.; Landgren, Ola; Maura, Francesco

doi:10.1182/blood-2021-145927

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“…Deeplevel disease quantification allows patients with high levels of cPC within graft or marrow to be offered additional cycles of induction treatment, thereby not only reducing graft contamination but also their overall tumor burden prior to AHCT. In addition, Diamond et al (43) have recently reported clonal hematopoiesis present at myeloma diagnosis to contaminate stem cell graft and after bypass of high-dose melphalan to evolve into secondary malignancies under immunocompromised conditions. This report provides additional evidence toward the emerging importance of graft immune genotyping.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, Diamond et al. ( 43 ) have recently reported clonal hematopoiesis present at myeloma diagnosis to contaminate stem cell graft and after bypass of high-dose melphalan to evolve into secondary malignancies under immunocompromised conditions. This report provides additional evidence toward the emerging importance of graft immune genotyping.…”

Section: Discussionmentioning

confidence: 99%

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Is Quantification of Measurable Clonal Plasma Cells in Stem Cell Grafts (gMRD) Clinically Meaningful?

Seval

Beksaç

2022

Front. Oncol.

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With the introduction of more effective novel therapies, the prognosis of multiple myeloma (MM) has improved significantly over the past decade, resulting with a significant proportion of patients achieving durable remissions that may reach even more than 10 years. Several studies demonstrated that the real prognostic value of complete remission (CR) relies on sustained undetectable minimal residual disease (MRD). Additionally, advances in MRD detection methods used for the detection of clonal plasma cells (cPC) inside or outside the bone marrow have also improved the value of MRD. The use of peripheral blood for MRD detection could be an effective method that overcomes the spatial heterogeneity and invasive intervention with recurrent bone marrow aspirations. During the last two decades, many groups have investigated the role of circulating plasma cells (CPCs) at diagnosis. As also presented by multiple groups during the recent ASH 2021 annual meeting, CPCs are becoming recognized as an independent prognostic factor. In addition, measurement of post-induction residual plasma cells in the stem cell graft is identified as another option for MRD assessment. Earlier studies in the era of less intensive induction regimens attempts to analyze the level of CPC contamination in the graft was shown to contribute to myeloma relapse and progression. According to these recent results, higher graft purity has been found to be in concordance with deeper responses. As expected, graft minimal residual disease (gMRD) may reflect the efficacy of induction as an additional response assessment tool. Although gMRD is a non-invasive approach, it has not gained sufficient support for routine use. In view of the hurdles related to monoclonal protein assessments, high-sensitivity cellular component measurement continues to possess its value as an end point for therapeutic efficacy. In this review, we will present a structural framework for MRD testing in peripheral blood stem cell autografts in MM and review the clinical integration into MM management.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%