Immunoadsorption and Plasma Exchange in Seropositive and Seronegative Immune-Mediated Neuropathies

Davies, AN; Fehmi, Janev; Şenel, Makbule; Tumani, Hayrettin; Dorst, Johannes; Rinaldi, Simon

doi:10.3390/jcm9072025

Cited by 27 publications

(30 citation statements)

References 49 publications

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“…For other indications, no systematic evaluation of efficacy was done due to low numbers of patients. Efficacy data refer to subgroups of patients with sufficient clinical data and have been published previously [5,20,22].…”

Section: Outcome Parametersmentioning

confidence: 99%

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Safety and Tolerability of Plasma Exchange and Immunoadsorption in Neuroinflammatory Diseases

Dorst

Fillies

Dreyhaupt

et al. 2020

JCM

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Plasma exchange (PE) and immunoadsorption (IA) are frequently used for treatment of various autoimmune-mediated neurological diseases, including multiple sclerosis (MS), chronic inflammatory demyelinating polyneuropathy (CIDP), and Guillain–Barré syndrome (GBS). Although both methods are generally regarded as well-tolerated treatment options, evidence for safety and tolerability is low for most indications and largely relies on small case series. In this study, we retrospectively analysed adverse events (AEs) and laboratory changes in 284 patients with various neurological indications who received either PE (n = 65, 113 cycles) or IA (n = 219, 435 cycles) between 2013 and 2020 in our Neurology department. One standard treatment cycle for PE as well as IA consisted of five treatments on five consecutive days. During every treatment, the 2.0–2.5-fold individual plasma volume (PV) was treated in IA, while in PE, the 0.7-fold individual PV was replaced by human albumin solution. Overall, both methods showed an excellent safety profile; no deaths of life-threatening adverse events were recorded. Severe AEs (corresponding to grade 3 on the Common Terminology Criteria for Adverse Events grading scale v5.0) including three patients with sepsis, one pneumonia, and one pneumothorax were present in 5/435 IA cycles (1.1%); in the PE group, no severe AEs were recorded. Furthermore, although advantageous tolerability is generally considered the main advantage of IA over PE, we found that overall frequency of AEs (including grades 1 and 2) was higher in IA (67.1% of all cycles) compared to PE (35.4%; p < 0.001). The low incidence of AEs in PE might be caused by the lower PV exchanged during each treatment (0.7-fold) compared to previous studies which predominantly exchanged the 1.0–1.5-fold PV. In order to verify this hypothesis as well as confirming the efficacy of this lower-dosed scheme, prospective studies comparing different treatment regimens are needed.

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Section: Outcome Parametersmentioning

confidence: 99%

“…A retrospective analysis of 20 patients with GBS [22] yielded response rates of 61.5% for IA and 71.4% for PE after the last treatment based on the documented neurological examinations.…”

Section: Efficacymentioning

confidence: 99%

Safety and Tolerability of Plasma Exchange and Immunoadsorption in Neuroinflammatory Diseases

Dorst

Fillies

Dreyhaupt

et al. 2020

JCM

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“…From July 2017 to May 2020, we tested serum samples from 649 patients with suspected inflammatory neuropathies for IgG antibodies directed against nodal (neurofascin-186) and paranodal (neurofascin-155, contactin-1 and contactin-associated protein, Caspr1) cell-adhesion molecules, using a live, cell-based assay. [12] A standardised request form was used to collect clinical data. This study was approved by the NHS National Research Ethics Service Committee (South Central – Oxford A, 14/SC/0280).…”

Section: Methodsmentioning

confidence: 99%

“…[6] Recently, antibodies directed against nodal/paranodal proteins have been identified in atypical forms of CIDP. [4,7–12]…”

Section: Introductionmentioning

confidence: 99%

IgG1 pan-neurofascin antibodies identify a severe yet treatable neuropathy with a high mortality

Fehmi

Davies

Walters

et al. 2021

Preprint

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Guillain-Barré syndrome and chronic inflammatory demyelinating polyneuropathy are umbrella terms for a number of pathologically distinct diseases involving disabling, immune-mediated injury to peripheral nerves. Current treatments involve non-specific immunomodulation. Prospective identification of patients with specific disease mechanisms should increasingly inform the use of more targeted disease modifying therapies and may lead to improved outcomes. In this cohort study, we tested serum for antibodies directed against nodal/paranodal protein antigens. The clinical characteristics of antibody positive and seronegative patients were then compared. Eight patients with IgG1-subclass antibodies directed against both isoforms of the nodal/paranodal cell-adhesion molecule neurofascin were identified. All developed rapidly progressive tetraplegia. Cranial nerve deficits (100% versus 26%), autonomic dysfunction (75% versus 13%) and respiratory involvement (88% versus 14%) were more common than in seronegative patients. The response to intravenous immunoglobulin, steroids and/or plasmapheresis was poor. Four patients received the B-cell-depleting therapy rituximab. After several weeks, these patients began to show progressive functional improvements, became seronegative, and were ultimately discharged home. Four patients who did not receive rituximab did not improve and died following the development of infectious complications and/or withdrawal of intensive care support. IgG1 panneurofascin antibodies define a very severe autoimmune neuropathy. We urgently recommend trials of targeted immunotherapy for this serologically-classified patient group.

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“…Although to date distinct disease-related antibodies are not detected in the majority of patients, the discovery of potential pathogenic auto-antibodies against proteins of the node of Ranvier and paranodal regions [ 12 ] have corroborated the importance of auto-antibodies in at least a subgroup of patients with immune-mediated neuropathies and therefore supported the rationale to apply treatments which target these antibodies. Alexander Davies and colleagues [ 13 ] investigated whether the existence of such antibodies may predict the response to apheresis in patients with GBS and CIDP. Interestingly, they did not find a clear correlation between the presence of known auto-antibodies and treatment response, suggesting that further, undiscovered antibodies may be present.…”

Section: Introductionmentioning

confidence: 99%

Apheresis in Neurological Disorders

Dorst

2020

JCM

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Immunoadsorption and Plasma Exchange in Seropositive and Seronegative Immune-Mediated Neuropathies

Cited by 27 publications

References 49 publications

Safety and Tolerability of Plasma Exchange and Immunoadsorption in Neuroinflammatory Diseases

Safety and Tolerability of Plasma Exchange and Immunoadsorption in Neuroinflammatory Diseases

IgG1 pan-neurofascin antibodies identify a severe yet treatable neuropathy with a high mortality

Apheresis in Neurological Disorders

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