Anti–Interleukin-6 and Janus Kinase Inhibitors for Severe Neurologic Toxicity of Checkpoint Inhibitors

Pïcca, Alberto; Valyraki, Nefeli; Birzu, Cristina; Kramkimel, N.; Hermine, Olivier; Zahr, Noël; Berzero, Giulia; Psimaras, Dimitri

doi:10.1212/nxi.0000000000001073

Cited by 19 publications

(18 citation statements)

References 7 publications

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“…We have applied and validated the nSMOL assay for more than 40 mAbs including 2 Fc fusion proteins 8,9,21,[46][47][48] . The exquisite specificity of mAbs and availability of 6 CDR legions (3 from each heavy and light chains) enables robust selection of the signature peptide as we and others have demonstrated 30 .…”

Section: Discussionmentioning

confidence: 99%

“…This feature curtails errors introduced through sample dilution and during the process of extrapolation of mAb concentration from the standard curve, while such errors are difficult to mitigate in ELISA (e.g., a linear standard curve is typically accompanied by narrower dynamic range whereas wider dynamic range ends up with a sigmoidal standard curve). Although others successfully measured mAbs using the nSMOL assay 47,52,53 and we demonstrated the minimal inter-operator variabilities in measuring bevacizumab with the nSMOL assay 49 , we have built and validated a prototype for an automated nSMOL platform using an automated liquid handler in our effort to further address inter-operator variabilities (manuscript in preparation). We also showed reasonable inter-instrument/platform variabilities from the LC-MS when conducting the nSMOL assays.…”

Section: Discussionmentioning

confidence: 99%

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A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

Iwamoto

Koguchi

Yokoyama

et al. 2022

Preprint

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Accurate quantitation of antibody is critical for development of monoclonal antibody therapeutics (mAbs). Therapeutic drug monitoring has been applied to measure levels of mAbs in clinics for dose adjustment for autoimmune disease. Trough levels of mAbs can be a biomarker for cancer immunotherapy. Thus, the deployment of a rapid and universal platform for mAb monitoring may benefit processes ranging from drug development to clinical practice for a wide spectrum of diseases. However, mAb monitoring often requires development and conduct of an individual ligand binding assay such as ELISA, which is impractical to scale. We streamlined quantitation of antibody therapeutics by a nano-surface and molecular-orientation limited (nSMOL) proteolysis assay using LC-MS with a universal reference antibody (refmAb-Q), for accurate multiplexed quantitation of unique signature peptides derived from mAbs. This innovative refmAb-Q nSMOL platform may provide a practical solution for quantitating an ever-increasing number of mAbs from developmental to clinical use settings.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

Iwamoto

Koguchi

Yokoyama

et al. 2022

Preprint

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show abstract

“…Major advantages of the refmAb-Q nSMOL assay stem from its backbone, the nSMOL assay. We have applied and validated the nSMOL assay for more than 40 mAbs including 2 Fc fusion proteins 8,9,21,[47][48][49] . The exquisite specificity of mAbs and availability of 6 CDR legions (3 from each heavy and light chains)…”

Section: Discussionmentioning

confidence: 99%

“…This feature curtails errors introduced through sample dilution and during the process of extrapolation of mAb concentration from the standard curve, while such errors are difficult to mitigate in ELISA (e.g., a linear standard curve is typically accompanied by narrower dynamic range whereas wider dynamic range ends up with a sigmoidal standard curve). Although others successfully measured mAbs using the nSMOL assay 48,53,54 and we demonstrated the minimal inter-operator variabilities in measuring bevacizumab with the nSMOL assay 50 , we have built and validated a prototype for an automated nSMOL platform using an automated liquid handler in our effort to further address inter-operator variabilities (manuscript in preparation).…”

Section: Discussionmentioning

confidence: 99%

A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

Iwamoto

Koguchi

Yokoyama

et al. 2022

Analyst

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“…1 (3)) suppresses pro-inflammatory cascades and has shown to ameliorate neurologic symptoms and relapse rates in patients with NMOSD refractory to multiple immunosuppressive therapies [ 135 – 137 ]. Tocilizumab has improved neurological symptoms in a patient with ICI-related steroid-refractory transverse myelitis with high levels of IL-6 in the CSF [ 138 ] and demonstrated efficacy in patients with ICI-mediated cerebritis [ 139 ]. Satralizumab is a modified anti-IL-6R antibody with a pH-dependent antibody-antigen binding which prolongs the elimination half-life of the drug and has been recently FDA-approved for the treatment of NMOSD [ 140 ].…”

Section: Potential Future Biologics Therapiesmentioning

confidence: 99%

Paraneoplastic Autoimmune Neurological Syndromes and the Role of Immune Checkpoint Inhibitors

Duong

Prüss

2022

Neurotherapeutics

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The introduction of immune checkpoint inhibitors (ICIs) in oncologic therapies has led to a paradigm shift in cancer treatment. ICIs have increased the overall survival in patients with malignant melanoma, small-cell lung cancer, and many other tumor entities. Despite their clinical benefits, these novel cancer immunotherapies can induce neurological immune-related adverse events (irAEs). Such immune-mediated complications can manifest within the spectrum of paraneoplastic neurological syndromes (PNSs). PNSs are rare immune-mediated complications of systemic cancers that can involve every aspect of the nervous system. The emergence of PNSs with ICI treatment opens further pathways to study the complex immunopathological interplay of cancer immunity, cross-reactive neurological autoimmune phenomena, and effects of ICIs on the immune system. ICI-induced PNSs comprise a diverse antibody repertoire and phenotypic spectrum with severe and life-threatening disease progression in some cases. Timely diagnosis and urgent interventions are pivotal for a favorable neurologic and oncologic outcome. This review focuses on the pathogenesis of cancer immunotherapy and the disruption of immune tolerance in PNSs and provides an overview of the most pertinent clinical manifestations and principles of diagnostic and therapeutic managements in light of the expected increase in PNSs due to the widespread use of ICIs in clinical practice. This review further discusses potential and evolving concepts of therapeutic monoclonal antibodies for the treatment of PNSs.

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Anti–Interleukin-6 and Janus Kinase Inhibitors for Severe Neurologic Toxicity of Checkpoint Inhibitors

Cited by 19 publications

References 7 publications

A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

A rapid and universal liquid chromatograph-mass spectrometry-based platform, refmAb-Q nSMOL, for monitoring monoclonal antibody therapeutics

Paraneoplastic Autoimmune Neurological Syndromes and the Role of Immune Checkpoint Inhibitors

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