Myeloma Drug Sensitivity Testing to Optimize Retreatment with Anti-CD38 Monoclonal Antibodies in Daratumumab-Refractory Patients

de, Olivia Perez; Walker, Z.; Forsberg, Peter; Mark, Tomer M.; Sherbenou, Daniel W.

doi:10.1182/blood-2020-137819

Cited by 5 publications

(3 citation statements)

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“…To further increase the suspension time for achieving better printing stabilities, Ficoll, a biocompatibility polysaccharide widely used in density-gradient centrifugation ( 34 ), was introduced as an additive to the support bath. For enhanced visualization, GelMA was conjugated with N -hydroxysuccinimide-fluorescein (green).…”

Section: Resultsmentioning

confidence: 99%

Liquid-embedded (bio)printing of alginate-free, standalone, ultrafine, and ultrathin-walled cannular structures

Tang

Luo

Lian

et al. 2023

Proc. Natl. Acad. Sci. U.S.A.

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While there has been considerable success in the three-dimensional bioprinting of relatively large standalone filamentous tissues, the fabrication of solid fibers with ultrafine diameters or those cannular featuring ultrathin walls remains a particular challenge. Here, an enabling strategy for (bio)printing of solid and hollow fibers whose size ranges could be facilely adjusted across a broad spectrum, is reported, using an aqueous two-phase embedded (bio)printing approach combined with specially designed cross-linking and extrusion methods. The generation of standalone, alginate-free aqueous architectures using this aqueous two-phase strategy allowed freeform patterning of aqueous bioinks, such as those composed of gelatin methacryloyl, within the immiscible aqueous support bath of poly(ethylene oxide). Our (bio)printing strategy revealed the fabrication of standalone solid or cannular structures with diameters as small as approximately 3 or 40 μ m, respectively, and wall thicknesses of hollow conduits down to as thin as <5 μ m. With cellular functions also demonstrated, we anticipate the methodology to serve as a platform that may satisfy the needs for the different types of potential biomedical and other applications in the future, especially those pertaining to cannular tissues of ultrasmall diameters and ultrathin walls used toward regenerative medicine and tissue model engineering.

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Section: Resultsmentioning

confidence: 99%

Liquid-embedded (bio)printing of alginate-free, standalone, ultrafine, and ultrathin-walled cannular structures

Tang

Luo

Lian

et al. 2023

Proc. Natl. Acad. Sci. U.S.A.

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“…(iii) The question of retreating patients with anti-CD38 mAbs (i.e., sequencing of anti-CD38) is still unanswered, and possibly the new generations of anti-CD38 mAbs will integrate MM treatments only if they display a higher efficacy than daratumumab/isatuximab or if they allow patients to be retreated with the same class. Trials are expected to further explore this hypothesis 14 , 15 .…”

Section: Immune-based Treatments: the Present And The Future Of Multi...mentioning

confidence: 99%

Recent advances in the treatment of multiple myeloma: a brief review

Bobin¹,

Leleu²

2022

Fac Rev

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The recent history of multiple myeloma has been marked by tremendous advances in the treatments available, which have ultimately improved the patients’ survival. Immune-based therapies, starting with the emergence of anti-CD38 monoclonal antibodies, whose impact is seen across all groups of patients, are probably the greatest evolution in the field of myeloma so far. Building on the efficacy of immunotherapy, “modern” immunological treatments such as CAR-T cells or bispecific antibodies are being developed. There clearly are lots of expectations for these novel immunotherapies, and, though first developed in relapsed myeloma, they will surely challenge the current strategies in early lines of treatment. Immunotherapy, since the development of anti-CD38, is a milestone in the treatment of myeloma and has already led to many paradigm shifts. Nevertheless, myeloma remains an incurable disease and diversified options are still required, notably for heavily pretreated patients. Non-immune-based treatments, which were responsible for most successes previously, are not to be completely abandoned. Novel pathophysiological mechanisms have been unraveled in the past few years, and thus, new targets have been identified, leading to the development of new drugs and new drug classes, such as XPO1 inhibitors and anti-BCL-2. Overall, the future of multiple myeloma is full of possibilities and considerable changes are still expected in the sequencing of treatments in the years to come.

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“… 50 Moreover, recent data support the possibility of treating patients refractory to daratumumab with isatuximab, due to MM cells “re-sensitization” after withdrawal daratumumab. 51 However, the multicenter retrospective MAMMOTH study 52 demonstrated that patients who become refractory to CD38 and those “penta-refractory” (refractory to CD38 mAb, two PIs and two IMiDs) had median OS of 8.6 and 5.6 months, respectively, so this poor outcome requires development and introduction in clinical practice of innovative therapeutic options.…”

Section: “Old” Generation Immunotherapiesmentioning

confidence: 99%

Novel Experimental Drugs for Treatment of Multiple Myeloma

Offidani

Corvatta²,

Morè

et al. 2021

JEP

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Multiple myeloma (MM) is the second most frequent hematological malignancy characterized by bone marrow aberrant plasma cells proliferation leading to a genetic complex and heterogeneous disease, with a median survival ranging from two to more than 10 years. By using new drugs such as proteasome inhibitors (PIs), immunomodulatory drugs (IMiDs), monoclonal antibodies (mAbs) in different combinations and high-dose therapy followed by auto-transplantation, there has been an amazing improvement in the outcome of this disease in recent years. Despite this, MM is still considered an incurable disease, characterized by remission periods alternated with relapse/progression episodes finally leading to resistant disease. In particular, patients who become refractory to PIs, IMiDs and mAbs have a very poor outcome. Moreover, to overcome resistant residual disease, a large combination of drugs will be increasingly used in early lines of therapy; this further reduces the therapeutic options at each relapse. This natural history means that MM always needs new drugs/strategies to overcome the incoming resistance. New combinations of naked mAbs are becoming the therapy of choice for patients refractory to lenalidomide and/or PI; conjugated mAbs will be useful in triple- and more-refractory patients; CAR-T cells and bispecific mAbs have shown relevant results in very advanced stages of disease. In this review, we reported the results of these new therapies and explored their potential applications. Personalized and precision medicine seem to be the new frontier of cancer treatment. Although no single or few factors have been identified as disease drivers in MM, recurrent gene mutations were recognized and specific compounds targeting these alterations were developed and studied. Therefore, we reviewed these targeted drugs to try to understand what the best therapeutic strategy in MM is.

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Myeloma Drug Sensitivity Testing to Optimize Retreatment with Anti-CD38 Monoclonal Antibodies in Daratumumab-Refractory Patients

Cited by 5 publications

References 0 publications

Liquid-embedded (bio)printing of alginate-free, standalone, ultrafine, and ultrathin-walled cannular structures

Liquid-embedded (bio)printing of alginate-free, standalone, ultrafine, and ultrathin-walled cannular structures

Recent advances in the treatment of multiple myeloma: a brief review

Novel Experimental Drugs for Treatment of Multiple Myeloma

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