Literature DB >> 34535632

Myeloma research on the move.

Heinz Ludwig¹.

Abstract

Entities: Chemical

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Year: 2021 PMID： 34535632 PMCID： PMC8448885 DOI： 10.1038/s41408-021-00550-z

Source DB: PubMed Journal: Blood Cancer J ISSN： 2044-5385 Impact factor: 11.037

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In the last years, remarkable progress has been achieved in our understanding of the biology and management of multiple myeloma (MM). Some of these advancements and possible future directions are addressed below and summarized in Table 1.

Table 1

Advances in multiple myeloma research with clinical implications.

	New findings	Possible consequences
Genomic data	Whole-genome sequencing revealed two types of MGUS: 1. with myeloma-defining events already present at diagnosis, with high risk for progression 2. A stable myeloma precursor condition with low risk of progression	Genomic definition of multiple myeloma
		Possible scenarios:
		1. Stable myeloma precursor condition
		2. Multiple myeloma-CRAB^neg
		3. Multiple Myeloma-CRAB^pos
Treatment of HR SMM/early MM	Genome sequencing defined two types of multiple myeloma as indicated above	Biology-based definition will select patients who benefit most from early treatment initiation (not necessarily HR/SMM patients defined by present algorithms)
Mass spectrometry	Higher sensitivity for detection of monoclonal proteins (MP)	Mass spectrometry (MS) will become the preferred technology for the detection and quantification of MPs. The higher sensitivity will reveal a higher prevalence of MGUS MS may be used in addition to NGS or NGF, or a sole method for MRD assessment
Diffusion weighted whole-body MRI	Higher sensitivity for detection of focal lesions, diffuse infiltration, and extramedullary disease compared to PET/CT	Likely to become the preferred imaging technology, but published standards for acquisition and reporting of WB MRI must be adhered to
ASCT	Improves PFS in all patients, in high-risk patients, OS is prolonged as well	Will remain standard, particularly in cytogenetic high-risk patients until the introduction of more effective therapies
Daratumumab (and likely other anti CD38 antibodies)	Two studies in NTE patients show already an OS benefit when combined with chemotherapy backbones for first-line therapy, in TE patients daratumumab combinations resulted in deeper responses, higher MRD^neg rates, and longer PFS. For OS longer FU is required. In later treatment lines, daratumumab combinations resulted in significant benefit, as well as daratumumab single-agent therapy	Anti-CD38 antibody combinations have become standard for first-line therapy
MRD status	The predictive value of MRDneg has been documented in an extensive meta-analysis. NGS (FDA approved) and NGF have a sensitivity of 10^-6, MRD^neg is associated with a survival advantage	MRD assessment is already standard in clinical trials, and likely will be approved as a proxy for OS Sustained MRD^neg ultimate goal of therapy
Maintenance therapy	Addition of anti-CD-38 antibodies or proteasome inhibitors to lenalidomide maintenance improves outcome	Drug combinations will be used for maintenance therapy but long term follow up data are required for further recommendations
Antibody conjugates, BiTEs, and other antibodies	Belantamab mafodotin showed significant single-agent activity in RRMM, several BiTEs showed high response rates in heavily pretreated patients	This drug class will be eagerly taken up in clinical practice, because of the substantial activity and easy access as drugs may be available on- the-shelf. Caveats are the toxicity and limited PFS. Will be combined with various drugs and moved to earlier lines of therapy
CAR-T cells	The CARTITUDE trial showed 97% ORR and 77% PFS rate after one year, similar slightly less impressive results were reported in KarMMa trial	Aside from anti-CD 38 antibodies the second most important game-changer. Will be evaluated for first-line therapy. Modifications of the CAR-T cells will further increase efficacy. Modified allogeneic CAR-T cells will become on-the-shelf products

Advances in multiple myeloma research with clinical implications. Mass spectrometry (MS) will become the preferred technology for the detection and quantification of MPs. The higher sensitivity will reveal a higher prevalence of MGUS MS may be used in addition to NGS or NGF, or a sole method for MRD assessment The predictive value of MRDneg has been documented in an extensive meta-analysis. NGS (FDA approved) and NGF have a sensitivity of 10-6, MRDneg is associated with a survival advantage MRD assessment is already standard in clinical trials, and likely will be approved as a proxy for OS Sustained MRDneg ultimate goal of therapy

Genomic data suggest rethinking the definition of myeloma

Whole-genome sequencing revealed two types of MGUS: A progressive myeloma precursor condition defined as a clonal entity in which myeloma-defining genomic events have already been acquired at the time of diagnosis and which is associated with a high risk of progression to MM; and an MGUS with a stable myeloma precursor condition, in which myeloma-defining genomic events are rare and which follows an indolent clinical course with a low risk of progression [1]. In those patients, branching evolution may still lead to progressive disease, but this seems to be rare and usually takes longer. These findings may inaugurate a new era of a genomic definition of monoclonal gammopathies, abandoning the arbitrarily defined categories MGUS, SMM, and MM, which depend on the disease burden but not on the underlying biology. This may be replaced by a genetic definition that may distinguish between three types: A. stable precursor condition of multiple myeloma, B. multiple myeloma—CRABneg, and C. multiple myeloma—CRABpos.

Treatment of high-risk smoldering multiple myeloma or of early myeloma?

As indicated above, the presently applied parameters of high-risk SMM do not reflect the genomic structure of individual patients and thus preclude optimal patient selection for early treatment. Further studies will path the way for a biology-based definition or a combination of these factors with conventional parameters of those patients that have already acquired the genetic machinery for malignant progression and thus would benefit most from early treatment initiation. As many experts consider myeloma still as being incurable, the question of optimal patient selection and timing for treatment initiation is highly pertinent. In the future, this question will become less relevant, because of the better differentiation between risk groups and further improvements in treatment outcome.

Mass spectrometry will replace conventional methods for M-protein assessment

Mass spectrometry (MS) shows higher sensitivity for the detection of monoclonal proteins (MP) compared to the conventional electrophoretic techniques [2] and will become the preferred technology for the detection and quantification of monoclonal proteins with profound implications. More individuals with a tiny MP will be detected, thus increasing the global prevalence of MGUS. Sequential studies will confirm that MGUS can be transient like other lymphoproliferative diseases such as alpha heavy chain disease [3], and this phenomenon may be more frequent in individuals with small MPs. The Spanish PETHEMA group [4] found a significant concordance between patients defined as MRDneg either by NGF or MS, and a similar prognostic accuracy of both techniques for PFS. In addition, they identified a small group of either MSneg−MRDpos, and MSpos−MRDneg patients. Whether MS will be used in addition to MRD testing, or whether MS may even replace conventional MRD testing needs to be explored. In case of similar sensitivity and predictability, MS could even become the preferred MRD test because it enables frequent serial testing, which may inform on both reaching and sustaining MSneg, as well as losing MSneg status as an early indication of relapse.

Whole-body MRI may become the preferred imaging technology

Present imaging guidelines in MM recommend low dose CT, PET/CT, and whole-body MRI (WB MRI) irrespective of their individual advantages and limitations. This may change if results of a recent prospective randomized study [5] showing higher sensitivity of diffusion-weighted WB MRI for detection of myeloma bone and extramedullary disease compared to PET/CT will be confirmed, and if diffusion-weighted WB MRI findings inform equally well or even better about imaging assessed myeloma response and its correlation with progression-free survival as PET/CT. An important requirement for achieving optimal MRI results is the standardization of acquisition and reporting of diffusion-weighted WB MRI. Further analysis showed a fivefold higher sensitivity of diffusion-weighted WB MRI (81.7% vs 16.7%) for detection of diffuse bone marrow infiltrations compared to PET-CT. All patients with high-risk cytogenetics had diffuse marrow infiltrations and most of them were missed by PET/CT. This study might become practice-changing recommending diffusion-weighted WB MRI for detection of myeloma bone and extramedullary lesions. This would also impact on the selection of the imaging technique for exclusion of residual disease in NGS or NGF-defined MRDneg patients.

Autologous stem cell transplantation, particularly in high-risk disease, will remain standard for the near future

Autologous stem cell transplantation (ASCT) has greatly improved treatment outcome before the introduction of new agents and continues to be a valuable choice in the era of novel agents. ASCT during induction therapy improved PFS over conventional chemotherapy in practically all trials, but OS was found to be similar in most studies [6]. Discussion is ongoing whether ASCT can be replaced by novel treatments in standard-risk patients. Several trials have established its benefit in patients with high-risk (HR) cytogenetics with the improvement of both PFS and OS [7]. The most recent confirmation of the efficacy of ASCT comes from the Italian FORTE study [8]. This trial showed superiority of KRd over KCd for induction therapy and most importantly, a significant improvement of the depth of response and PFS with eight cycles of KRd plus ASCT compared to 12 cycles of KRd. The advantage of ASCT was seen in patients with standard-risk cytogenetics, in those with one, and with two or more cytogenetic high-risk abnormalities. Hence, ASCT will remain standard of care, particularly in cytogenetic HR patients until further improvements in first-line therapy.

Daratumumab—chemotherapy combinations have become the new standard for first-line therapies

Daratumumab is a game-changer for MM therapy, active as single-agent therapy in heavily pretreated patients, synergistic with several chemotherapy backbones in later lines of therapy, and finally a valuable combination partner for first-line treatment regimens with an already documented survival advantage in patients not eligible for transplantation (ALCYONE and MAIA) [9]. Studies in transplant-eligible patients (CASSIOPEIA) [10] showed an impressive prolongation of PFS, but for OS, longer follow-up will be required. In elderly patients and in studies with relapsed refractory myeloma (POLLUX and CASTOR) [9], daratumumab was given until progression or intolerance, while in the transplant studies, daratumumab maintenance is usually restricted to 2 years. Long follow-up is needed for documentation of a possible survival benefit.

MRD status will become a surrogate parameter for overall survival

New technologies, in particular next-generation sequencing (NGS) and next-generation flow (NGF), have successfully been adapted to enable the detection of one myeloma cell within one million nucleated bone marrow cells. Patients achieving MRDneg at a threshold level of 10−6 show prolonged survival compared to MRDpos patients [11]. Achieving MRDneg at least once is already associated with a survival advantage, but sustained MRDneg is the ultimate goal. Remarkably, patients with HR cytogenetics achieving MRDneg seem to fair equally well as MRDneg standard-risk patients. A comprehensive meta-analysis has confirmed the close association between MRDneg and survival in practically all treatment scenarios, including younger and older patients, first or later lines of therapy, and different risk groups [11]. This relationship was even noted in the BELLINI study with discordant PFS and OS results [12]. Overall survival is still considered the gold standard for evaluation of the impact of any new therapy, but with an increasing survival expectancy of MM patients, meeting overall survival as primary study endpoint becomes increasingly difficult to achieve, highlighting the need for a surrogate marker, such as sustained MRDneg.

Standard lenalidomide maintenance therapy is challenged by new drugs and combinations

Lenalidomide maintenance after ASCT is still the gold standard, but trials with proteasome inhibitors and anti-CD38 antibodies, either as single-agent or in combination with lenalidomide, are ongoing. Carfilzomib added to lenalidomide resulted in improved PFS in all cytogenetic risk groups, with the exception of patients with ampl1q in the FORTE study [8], compared to single-agent lenalidomide, thus showing that carfilzomib may be a valuable combination partner for lenalidomide, but the requirement for intravenous infusion limits the treatment duration of carfilzomib. Recent results from the CASSIOPEIA trial [13] indicate significant activity of daratumumab maintenance treatment in patients without daratumumab during induction therapy, a finding which would speak against continuous exposure, but PFS2 tended to be superior in patients exposed both during induction and maintenance therapy to daratumumab. In the GRIFFIN study [9], patients randomized to daratumumab-lenalidomide maintenance showed significantly higher sCR and MRDneg rates compared to the lenalidomide arm. Presently, new drugs such as CELMoDs and BiTEs are evaluated as maintenance treatments.

BiTEs, other antibodies, and antibody toxin conjugates

Belantamab Mafodotin shows remarkable single-agent activity in RRMM patients [14], which has prompted its evaluation in combination with several backbones. Keratopathy as a side effect is an issue, but progress has been made in mitigating this complication by dose reduction, longer treatment intervals, or both. Bi-specific T cell engager (BiTEs) have two binding sites: one targeting an immune cell and the other a myeloma membrane antigen [15]. Clinical studies showed high anti-myeloma activity with response rates up to 83% in heavily pretreated patients. Treatment with BiTEs can be associated with a previously uncommon side effect profile including CIRS and neurotoxicity. The ease of administration of BiTEs and their ready availability on-the-shelf gives them an advantage over cellular therapies.

CAR-T cells and other cellular therapies

With the development of CAR-T cell therapy, an old dream of hematologists became true. Harnessing the patient’s own immune system can induce marked tumor responses in far advanced, heavily pretreated patients. A response rate of 97% with high rates of MRDneg disease and a PFS rate of 77% after one year has been reported in the CARTITUDE-1 study [16], but the persistence of CAR-T cells and long-term myeloma control is still an issue. Several developments making CAR-T cells even more efficient and better tolerable are ongoing. Bispecific CAR-T cells may reduce the risk for antigen escape, fully human CAR constructs will improve persistence, allogeneic CAR-T cells may, after adequate gene editing to remove the T cell receptor and disruption of the MHC complex, be available on-the-shelf. Importantly, trials are already ongoing comparing upfront CAR-T cell therapy with ASCT.

13 in total

1. Bortezomib, thalidomide, and dexamethasone with or without daratumumab before and after autologous stem-cell transplantation for newly diagnosed multiple myeloma (CASSIOPEIA): a randomised, open-label, phase 3 study.

Authors: Philippe Moreau; Michel Attal; Cyrille Hulin; Bertrand Arnulf; Karim Belhadj; Lotfi Benboubker; Marie C Béné; Annemiek Broijl; Hélène Caillon; Denis Caillot; Jill Corre; Michel Delforge; Thomas Dejoie; Chantal Doyen; Thierry Facon; Cécile Sonntag; Jean Fontan; Laurent Garderet; Kon-Siong Jie; Lionel Karlin; Frédérique Kuhnowski; Jérôme Lambert; Xavier Leleu; Pascal Lenain; Margaret Macro; Claire Mathiot; Frédérique Orsini-Piocelle; Aurore Perrot; Anne-Marie Stoppa; Niels Wcj van de Donk; Soraya Wuilleme; Sonja Zweegman; Brigitte Kolb; Cyrille Touzeau; Murielle Roussel; Mourad Tiab; Jean-Pierre Marolleau; Nathalie Meuleman; Marie-Christiane Vekemans; Matthijs Westerman; Saskia K Klein; Mark-David Levin; Jean Paul Fermand; Martine Escoffre-Barbe; Jean-Richard Eveillard; Reda Garidi; Tahamtan Ahmadi; Sen Zhuang; Christopher Chiu; Lixia Pei; Carla de Boer; Elena Smith; William Deraedt; Tobias Kampfenkel; Jordan Schecter; Jessica Vermeulen; Hervé Avet-Loiseau; Pieter Sonneveld
Journal: Lancet Date: 2019-06-03 Impact factor: 79.321

2. A large meta-analysis establishes the role of MRD negativity in long-term survival outcomes in patients with multiple myeloma.

Authors: Nikhil C Munshi; Herve Avet-Loiseau; Kenneth C Anderson; Paola Neri; Bruno Paiva; Mehmet Samur; Meletios Dimopoulos; Margarita Kulakova; Annette Lam; Mahmoud Hashim; Jianming He; Bart Heeg; Jon Ukropec; Jessica Vermeulen; Sarah Cote; Nizar Bahlis
Journal: Blood Adv Date: 2020-12-08

3. Autologous haematopoietic stem-cell transplantation versus bortezomib-melphalan-prednisone, with or without bortezomib-lenalidomide-dexamethasone consolidation therapy, and lenalidomide maintenance for newly diagnosed multiple myeloma (EMN02/HO95): a multicentre, randomised, open-label, phase 3 study.

Authors: Michele Cavo; Francesca Gay; Meral Beksac; Lucia Pantani; Maria Teresa Petrucci; Meletios A Dimopoulos; Luca Dozza; Bronno van der Holt; Sonja Zweegman; Stefania Oliva; Vincent H J van der Velden; Elena Zamagni; Giuseppe A Palumbo; Francesca Patriarca; Vittorio Montefusco; Monica Galli; Vladimir Maisnar; Barbara Gamberi; Markus Hansson; Angelo Belotti; Ludek Pour; Paula Ypma; Mariella Grasso; Alexsandra Croockewit; Stelvio Ballanti; Massimo Offidani; Iolanda D Vincelli; Renato Zambello; Anna Marina Liberati; Niels Frost Andersen; Annemiek Broijl; Rossella Troia; Anna Pascarella; Giulia Benevolo; Mark-David Levin; Gerard Bos; Heinz Ludwig; Sara Aquino; Anna Maria Morelli; Ka Lung Wu; Rinske Boersma; Roman Hajek; Marc Durian; Peter A von dem Borne; Tommaso Caravita di Toritto; Thilo Zander; Giorgina Specchia; Anders Waage; Peter Gimsing; Ulf-Henrik Mellqvist; Marinus van Marwijk Kooy; Monique Minnema; Caroline Mandigers; Anna Maria Cafro; Angelo Palmas; Susanna Carvalho; Andrew Spencer; Mario Boccadoro; Pieter Sonneveld
Journal: Lancet Haematol Date: 2020-04-30 Impact factor: 18.959

Review 4. Heavy chain diseases.

Authors: Dietlind L Wahner-Roedler; Robert A Kyle
Journal: Best Pract Res Clin Haematol Date: 2005 Impact factor: 3.020

5. Ciltacabtagene autoleucel, a B-cell maturation antigen-directed chimeric antigen receptor T-cell therapy in patients with relapsed or refractory multiple myeloma (CARTITUDE-1): a phase 1b/2 open-label study.

Authors: Jesus G Berdeja; Deepu Madduri; Saad Z Usmani; Andrzej Jakubowiak; Mounzer Agha; Adam D Cohen; A Keith Stewart; Parameswaran Hari; Myo Htut; Alexander Lesokhin; Abhinav Deol; Nikhil C Munshi; Elizabeth O'Donnell; David Avigan; Indrajeet Singh; Enrique Zudaire; Tzu-Min Yeh; Alicia J Allred; Yunsi Olyslager; Arnob Banerjee; Carolyn C Jackson; Jenna D Goldberg; Jordan M Schecter; William Deraedt; Sen Hong Zhuang; Jeffrey Infante; Dong Geng; Xiaoling Wu; Marlene J Carrasco-Alfonso; Muhammad Akram; Farah Hossain; Syed Rizvi; Frank Fan; Yi Lin; Thomas Martin; Sundar Jagannath
Journal: Lancet Date: 2021-06-24 Impact factor: 79.321

6. Venetoclax or placebo in combination with bortezomib and dexamethasone in patients with relapsed or refractory multiple myeloma (BELLINI): a randomised, double-blind, multicentre, phase 3 trial.

Authors: Shaji K Kumar; Simon J Harrison; Michele Cavo; Javier de la Rubia; Rakesh Popat; Cristina Gasparetto; Vania Hungria; Hans Salwender; Kenshi Suzuki; Inho Kim; Elizabeth A Punnoose; Wan-Jen Hong; Kevin J Freise; Xiaoqing Yang; Anjla Sood; Muhammad Jalaluddin; Jeremy A Ross; James E Ward; Paulo C Maciag; Philippe Moreau
Journal: Lancet Oncol Date: 2020-10-29 Impact factor: 41.316

7. Whole-genome sequencing reveals progressive versus stable myeloma precursor conditions as two distinct entities.

Authors: Bénedith Oben; Guy Froyen; Kylee H Maclachlan; Daniel Leongamornlert; Federico Abascal; Binbin Zheng-Lin; Venkata Yellapantula; Andriy Derkach; Ellen Geerdens; Benjamin T Diamond; Ingrid Arijs; Brigitte Maes; Kimberly Vanhees; Malin Hultcrantz; Elisabet E Manasanch; Dickran Kazandjian; Alexander Lesokhin; Ahmet Dogan; Yanming Zhang; Aneta Mikulasova; Brian Walker; Gareth Morgan; Peter J Campbell; Ola Landgren; Jean-Luc Rummens; Niccolò Bolli; Francesco Maura
Journal: Nat Commun Date: 2021-03-25 Impact factor: 14.919

8. Single-agent belantamab mafodotin for relapsed/refractory multiple myeloma: analysis of the lyophilised presentation cohort from the pivotal DREAMM-2 study.

Authors: Paul G Richardson; Hans C Lee; Al-Ola Abdallah; Adam D Cohen; Prashant Kapoor; Peter M Voorhees; Axel Hoos; Karrie Wang; January Baron; Trisha Piontek; Julie Byrne; Scott Richmond; Roxanne C Jewell; Joanna Opalinska; Ira Gupta; Sagar Lonial
Journal: Blood Cancer J Date: 2020-10-23 Impact factor: 11.037

9. Mass spectrometry for the evaluation of monoclonal proteins in multiple myeloma and related disorders: an International Myeloma Working Group Mass Spectrometry Committee Report.

Authors: David L Murray; Noemi Puig; Sigurdur Kristinsson; Saad Z Usmani; Angela Dispenzieri; Giada Bianchi; Shaji Kumar; Wee Joo Chng; Roman Hajek; Bruno Paiva; Anders Waage; S Vincent Rajkumar; Brian Durie
Journal: Blood Cancer J Date: 2021-02-01 Impact factor: 11.037

2 in total

Review 1. What's Old is New: The Past, Present and Future Role of Thalidomide in the Modern-Day Management of Multiple Myeloma.

Authors: Bruno Almeida Costa; Tarek H Mouhieddine; Joshua Richter
Journal: Target Oncol Date: 2022-06-30 Impact factor: 4.864

2. mTORC1-Inhibition Potentiating Metabolic Block by Tyrosine Kinase Inhibitor Ponatinib in Multiple Myeloma.

Authors: Uddin Md Nazim; Kausik Bishayee; Jieun Kang; Dongkwan Yoo; Sung-Oh Huh; Ali Sadra
Journal: Cancers (Basel) Date: 2022-06-02 Impact factor: 6.575

2 in total