# Anti-GQ1b Antibody Syndrome: A Clinician-Oriented Perspective on Diagnostics, Therapy, and Atypical Phenotypes—With an Illustrative 16-Case Institutional Series

**Authors:** Taro Bannai, Minako Yamada, Tomonari Seki, Yasushi Shiio, Tatsuya Yamasoba

PMC · DOI: 10.3390/jcm15020801 · 2026-01-19

## TL;DR

This paper provides a clinical guide for diagnosing and treating Anti-GQ1b antibody syndrome, emphasizing early immunotherapy and specific diagnostic tests.

## Contribution

The paper introduces a clinician-oriented approach to AGABS with insights from a 16-case series and highlights diagnostic and therapeutic strategies.

## Key findings

- Early immunotherapy improves outcomes in AGABS patients.
- Targeted electrophysiology and neuro-otologic exams help avoid misdiagnosis.
- Most patients showed co-reactivity with GT1a antibodies and had antecedent infections.

## Abstract

Anti-GQ1b antibody syndrome (AGABS) unifies triad-defined Miller Fisher syndrome (MFS), Bickerstaff brainstem encephalitis (BBE), and the ophthalmoplegic variant of Guillain–Barré syndrome (GBS-O) under a post-infectious immune mechanism centered on IgG to disialosyl gangliosides. The spectrum also encompasses triad-minus phenotypes—acute ophthalmoparesis without ataxia, acute vestibular syndrome, optic involvement, and acute sensory-ataxic neuropathy. A molecular-mimicry model with complement-mediated nodal/paranodal dysfunction explains severe early deficits despite bland limb nerve conduction studies (NCSs), the cranial/proprioceptive predilection, and generally favorable treatment responsiveness to immunotherapy. In practice, a serology-first strategy, complemented by targeted electrophysiology—blink and H-reflex testing, and, where feasible, paired SEP–ABR showing a literature-supported dissociation (normal ABR with impaired median-nerve cortical SEPs), which, in our series, was documented in one illustrative BBE case—and by structured neuro-otologic examination, mitigates the “normal-NCS trap” and enables timely treatment. Intravenous immunoglobulin (IVIg) is first-line; plasma exchange (PLEX) is an alternative in severe or IVIg-ineligible cases; and intravenous methylprednisolone (IVMP) may be added selectively for central/optic-weighted phenotypes without routine oral taper. We consolidate actionable diagnostic and therapeutic steps and examine them in an institutional series of 16 consecutive seropositive patients (2015–2025): all were anti-GQ1b-positive with frequent GT1a co-reactivity; most reported an antecedent infection—typically upper respiratory, less often gastrointestinal—within the two weeks before onset; limb NCSs were often nondiagnostic whereas reflex/evoked-potential studies were informative; two required intubation in addition to IVIg; outcomes were generally favorable with early immunotherapy. The practical message: order anti-GQ1b at first contact, pair targeted electrophysiology with neuro-otology, and treat early to exploit reversible nodal/paranodal dysfunction.

## Linked entities

- **Diseases:** Miller Fisher syndrome (MONDO:0005851), Bickerstaff brainstem encephalitis (MONDO:0019208), Guillain–Barré syndrome (MONDO:0016218), acute sensory-ataxic neuropathy (MONDO:0016500)

## Full-text entities

- **Diseases:** BBE (MESH:D004660), nodal (MESH:D013611), ophthalmoparesis (MESH:D009886), GBS-O (MESH:D020275), infection (MESH:D007239), acute vestibular syndrome (MESH:D020338), MFS (MESH:D019846), paranodal dysfunction (MESH:D006331), optic involvement (MESH:D009901), sensory-ataxic neuropathy (MESH:C537583), ataxia (MESH:D001259)
- **Chemicals:** IVMP (-), methylprednisolone (MESH:D008775)
- **Species:** Homo sapiens (human, species) [taxon 9606]

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Source: https://tomesphere.com/paper/PMC12841706