Liquid biopsies and minimal residual disease in lymphoid malignancies

Zerdan, Maroun Bou; Kassab, Joseph; Saba, Ludovic; Haroun, Elio; Zerdan, Morgan Bou; Allam, Sabine; Nasr, Lewis; Macaron, Walid; Mammadli, Mahinbanu; Moussa, Suaad; Chaulagain, Chakra P

doi:10.3389/fonc.2023.1173701

Cited by 5 publications

References 180 publications

(206 reference statements)

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Epilogue: Towards a Toolbox for a Pragmatist Approach to Conceptualization of Health and Disease

Schermer,

van der Linden,

Bolt

et al. 2024

Philosophy and Medicine

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In this Epilogue, we bring together the different strands of the volume, and reflect on the lessons learned in the international workshop. We discuss next questions to be asked and steps to be taken for the further development and application of our pragmatic approach. We end by tentatively proposing a ‘toolbox’ intended to give guidance to further inquire on the concept and conceptions of Disease, specific diseases, and health, as they function in numerous practical contexts.

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Epilogue: Towards a Toolbox for a Pragmatist Approach to Conceptualization of Health and Disease

Schermer,

van der Linden,

Bolt

et al. 2024

Philosophy and Medicine

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Full-Length Immune Repertoire Reconstruction and Profiling at the Transcriptome Level Using Long-Read Sequencing

Luo,

Zhang,

et al. 2024

Clinical Chemistry

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Background Due to the diversity of the immune repertoire (IR), reconstructing full-length IR using traditional short-read sequencing has proven challenging. Methods A full-length IR sequencing (FLIRseq) work flow was developed with linear rolling circle amplification and nanopore sequencing. Its accuracy and quantification ability were verified by plasmid mixtures and commercial B-cell receptor/T-cell receptor sequencing (BCR/TCR-seq) based on short reads. IRs in tissues and the peripheral blood from 8 patients with acute lymphoblastic leukemia, 3 patients with allergic diseases, 4 patients with psoriasis, and 5 patients with prostate cancer were analyzed using FLIRseq. Results FLIRseq reads had lower mismatch rates and gap rates, and higher identify rates than nanopore reads (all P < 2.2 × −16). The relative quantification of components by FLIRseq was consistent with the actual quantification (P > 0.05). FLIRseq had superiority over BCR/TCR-seq, providing the long complementarity-determining region 3, B-cell isotype, and the rarely used V gene sequence. FLIRseq observed an increase in clonotype diversity (P < 0.05) and a decrease in the percentage of abnormal BCRs/TCRs in patients with leukemia in remission. For patients with allergic diseases or psoriasis, FLIRseq provided direct insights into V(D)J recombination and specific immunoglobulin classes. Compared with that in prostate cancer tissues, the full-length V segment of the biased T-cell receptor β chain from lymphocytes in psoriatic tissues showed a more consistent AlphaFold2-predicted protein structure (P < 0.05). Conclusions FLIRseq enables unbiased and comprehensive analyses of direct V(D)J recombination and immunoglobulin classes, thereby contributing to characterizing pathogenic mechanisms, monitoring minimal residual disease, and customizing adoptive cell therapy.

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Measurable Residual Disease Testing in Multiple Myeloma Following T-Cell Redirecting Therapies

Shim,

Fonseca

2024

Cancers

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Several novel T-cell-based therapies have recently become available for multiple myeloma (MM). These T-cell redirecting therapies (TRTs) include chimeric antigen receptor T-cells (CAR-T) and bispecific antibodies (BiAbs). In both clinical trial and real-world data, these therapies have demonstrated high rates of deep clinical response, and some are now approved for second-line treatment for relapsed MM. The deep and sustained clinical responses these therapies are capable of inducing will require sophisticated response monitoring to provide meaningful information for patient care. Obtaining measurable residual disease (MRD) negativity has been validated as an independent positive prognostic marker for progression-free survival (PFS) and overall survival (OS) in both newly diagnosed and relapsed refractory patients with multiple myeloma. Assessment for MRD negativity was performed in all of the trials for FDA-approved TRT. Here, we summarize pertinent data for MRD assessment following TRT in MM and provide a rationale and structured framework for conducting MRD testing post TRT.

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Liquid biopsies and minimal residual disease in lymphoid malignancies

Cited by 5 publications

References 180 publications

Epilogue: Towards a Toolbox for a Pragmatist Approach to Conceptualization of Health and Disease

Epilogue: Towards a Toolbox for a Pragmatist Approach to Conceptualization of Health and Disease

Full-Length Immune Repertoire Reconstruction and Profiling at the Transcriptome Level Using Long-Read Sequencing

Measurable Residual Disease Testing in Multiple Myeloma Following T-Cell Redirecting Therapies

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