# Clinical course and prognosis of chronic autoimmune neuropathies requiring intensive care: a retrospective cohort study

**Authors:** Hannah Preßler, Lisa Schwarz, Simon Streit, Annette Aigner, Alicia Schleicher, Frauke Stascheit, Friederike A. Arlt, Viktoria Zinnow, Tatjana Khorassani, Harald Prüss, Wolfgang Böhmerle, Andreas Meisel, Werner Stenzel, Franziska Scheibe

PMC · DOI: 10.1007/s00415-026-13694-4 · Journal of Neurology · 2026-02-25

## TL;DR

This study examines the clinical course and outcomes of chronic autoimmune neuropathies requiring intensive care, finding high mortality but potential for recovery.

## Contribution

The study provides new insights into the prognosis and treatment of severe chronic autoimmune neuropathies requiring ICU care.

## Key findings

- 95% of ICU-treated CAN patients required mechanical ventilation and showed severe tetraparesis.
- Survivors showed significant improvement in disability scores compared to baseline.
- ICU-treated patients had worse long-term outcomes compared to non-ICU patients.

## Abstract

Data on chronic autoimmune neuropathies (CAN) requiring intensive care unit (ICU) treatment are limited. This study investigated clinical and neuropathological features, immunotherapies, and outcomes of ICU-treated CAN patients.

Retrospectively, we analyzed patients with CAN admitted to the ICU between 2007 and 2024. Outcomes, assessed by Inflammatory Neuropathy Cause and Treatment (INCAT) score and modified Rankin scale (mRS), were compared to age, sex, and diagnosis-matched non-ICU outpatients using ordinal and binary logistic regression.

Among 21 included patients (chronic inflammatory demyelinating neuropathies (CIDP): n = 15, other CAN: n = 6), 95% required mechanical ventilation and exhibited severe tetraparesis at disease nadir. Biopsies from CIDP patients revealed moderate-to-severe chronic axonal loss with variable CD8 + T-cell infiltration (9/11), and complement deposition (C5b-9) was detected in all samples (n = 8/8). All patients received first-line immunotherapy at ICU, 62% required “escalation” (rituximab: n = 13, cyclophosphamide: n = 3). Five (24%) remained refractory, receiving daratumumab (n = 3), efgartigimod (n = 1), or autologous stem cell transplantation (n = 1). Six patients (29%) died, whereas survivors showed marked improvement with median change of − 2 mRS points (95% CI − 5 to − 2) and − 6 INCAT points (95% CI − 8 to− 5) at last follow-up. However, ICU-treated patients had significantly higher odds of worse long-term outcomes than matched non-ICU patients (adjusted cumulative OR: mRS 7.1 95% CI 1.9–27.3, INCAT 6.4 95% CI 1.7–23.2).

Severe CAN requiring ICU treatment is associated with high mortality, but meaningful recovery is possible in survivors. Neuropathology confirmed combined cellular and humoral mechanisms, supporting personalized, mechanism-guided therapeutic approaches.

The online version contains supplementary material available at 10.1007/s00415-026-13694-4.

## Full-text entities

- **Genes:** ENO2 (enolase 2) [NCBI Gene 2026] {aka HEL-S-279, NSE}, CD19 (CD19 molecule) [NCBI Gene 930] {aka B4, CVID3}, UCHL1 (ubiquitin C-terminal hydrolase L1) [NCBI Gene 7345] {aka HEL-117, HEL-S-53, NDGOA, PARK5, PGP 9.5, PGP9.5}, PMP22 (peripheral myelin protein 22) [NCBI Gene 5376] {aka CIDP, CMT1A, CMT1E, DSS, GAS-3, GAS3}, NEFL (neurofilament light chain) [NCBI Gene 4747] {aka CMT1F, CMT2E, CMTDIG, NF-L, NF68, NFL}, NPEPPS (aminopeptidase puromycin sensitive) [NCBI Gene 9520] {aka AAP-S, MP100, PSA}, MAG (myelin associated glycoprotein) [NCBI Gene 4099] {aka GMA, S-MAG, SIGLEC-4A, SIGLEC4, SIGLEC4A, SPG75}, FCGRT (Fc gamma receptor and transporter) [NCBI Gene 2217] {aka FCRN, FcgammaRn, alpha-chain}, CNTN1 (contactin 1) [NCBI Gene 1272] {aka CMYO12, CMYP12, F3, GP135, MYPCN}, TNFRSF17 (TNF receptor superfamily member 17) [NCBI Gene 608] {aka BCM, BCMA, CD269, TNFRSF13A}, CNTNAP1 (contactin associated protein 1) [NCBI Gene 8506] {aka CASPR, CHN3, CNTNAP, NRXN4, P190}, CD8A (CD8 subunit alpha) [NCBI Gene 925] {aka CD8, CD8alpha, IMD116, Leu2, p32}
- **Diseases:** tetraparesis (MESH:C565722), conduction block (MESH:D006327), motor neuropathy (MESH:D010523), chronic immune mediated neuropathy (MESH:C567355), oculomotor disorder (MESH:D015840), dventilation-associated pneumonia (MESH:D011014), myocarditis (MESH:D009205), bacterial infection (MESH:D001424), axonal degeneration (MESH:D009410), respiratory failure (MESH:D012131), bleeding (MESH:D006470), falls (MESH:C537863), CMV (MESH:D003586), aspiration (MESH:D011015), Sepsis-Related Organ Failure (MESH:D009102), Autoimmune nodopathy (MESH:D001327), nemaline myopathy (MESH:D017696), facial or bulbar palsy (MESH:D010244), CAN (MESH:D019693), Axonal damage (MESH:D001480), Disability (MESH:D009069), Staphylococcus haemolyticus (MESH:D013203), damage (MESH:D020263), DADS neuropathy (MESH:D009422), axonal loss (MESH:D012183), INCAT (MESH:D020330), infectious (MESH:D003141), sepsis (MESH:D018805), IgG4 (MESH:D000077733), Anti-MAG neuropathy (MESH:C565538), nerve (MESH:C537568), neuromuscular diseases (MESH:D009468), fever (MESH:D005334), MMN (MESH:D000080364), death (MESH:D003643), complement (MESH:D007153), rectal and bronchial carcinoma (MESH:D002283), flu-like infection (MESH:D007251), Demyelination (MESH:D003711), antibody-mediated neurological diseases (MESH:D020274), Rare Disease (MESH:D035583), ischemic MCA infarction (MESH:D020244), urothelial carcinoma (MESH:D014523), viral (MESH:D014777), Clostridium enterocolitis (MESH:D004761), nerve damage (MESH:D000080902), PLEX (MESH:D054219), aCranial nerve abnormalities (MESH:D005155), axonal neuropathy (MESH:D020269), Inflammatory (MESH:D007249), upper respiratory tract infection (MESH:D012141), trauma (MESH:D014947), Myasthenia (MESH:D020294), Chronic inflammatory axonal polyneuropathy (MESH:D020277), fiber loss (MESH:D000071075), dysphagia (MESH:D003680), critically ill (MESH:D016638), nodal (MESH:D013611), rectal carcinoma (MESH:D012004), infection (MESH:D007239)
- **Chemicals:** bortezomib (MESH:D000069286), steroid (MESH:D013256), daratumumab (MESH:C556306), methotrexate (MESH:D008727), methylene blue (MESH:D008751), Cyclophosphamide (MESH:D003520), RTX (MESH:C024353), glutaraldehyde (MESH:D005976), cyclosporine (MESH:D016572), efgartigmod (-), mycophenolate mofetil (MESH:D009173), CPM (MESH:C037534), azathioprine (MESH:D001379), Efgartigimod (MESH:C000718373), Rituximab (MESH:D000069283)
- **Species:** Homo sapiens (human, species) [taxon 9606], Rattus norvegicus (brown rat, species) [taxon 10116]

## Full text

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Source: https://tomesphere.com/paper/PMC12935830