Setty M. Magaña scite author profile

Background: Plasma exchange (PLEX) is a beneficial rescue therapy for acute, steroid-refractory central nervous system inflammatory demyelinating disease (CNS-IDD). Despite the approximately 45% PLEX response rate reported among patients with CNS-IDD, determinants of interindividual differences in PLEX response are not well characterized.Objective: To perform an exploratory analysis of clinical, radiographic, and serological features associated with beneficial PLEX response.

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Posterior reversible encephalopathy syndrome in neuromyelitis optica spectrum disorders

Magaña¹,

Matiello²,

Pittock³

et al. 2009

Neurology

188

117

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Brain lesions in some patients with neuromyelitis optica spectrum disorder (NMOSD) may be accompanied by vasogenic edema and manifest as posterior reversible encephalopathy syndrome (PRES). Water flux impairment due to aquaporin-4 autoimmunity may predispose to PRES in patients with NMOSD who experience blood pressure fluctuations or who are treated with therapies that can cause rapid fluid shifts.

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Neuromyelitis optica IgG stimulates an immunological response in rat astrocyte cultures

Howe

Kaptzan

Magaña

et al. 2014

Glia

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Neuromyelitis optica (NMO) is a primary astrocyte disease associated with CNS inflammation, demyelination, and tissue injury. Brain lesions are frequently observed in regions enriched in expression of the aquaporin-4 (AQP4) water channel, an antigenic target of the NMO IgG serologic marker. Based on observations of disease reversibility and careful characterization of NMO lesion development, we propose that the NMO IgG may induce a dynamic immunological response in astrocytes. Using primary rat astrocyte-enriched cultures and treatment with NMO patient-derived serum or purified IgG, we observed a robust pattern of gene expression changes consistent with the induction of a reactive and inflammatory phenotype in astrocytes. The reactive astrocyte factor lipocalin-2 and a broad spectrum of chemokines, cytokines, and stress response factors were induced by either NMO patient serum or purified IgG. Treatment with IgG from healthy controls had no effect. The effect is disease-specific, as serum from patients with relapsing-remitting multiple sclerosis, Sjögren’s, or systemic lupus erythematosus did not induce a response in the cultures. We hypothesize that binding of the NMO IgG to AQP4 induces a cellular response that results in transcriptional and translational events within the astrocyte that are consistent with a reactive and inflammatory phenotype. Strategies aimed at reducing the inflammatory response of astrocytes may short circuit an amplification loop associated with NMO lesion development.

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Neuromyelitis Optica IgG Serostatus in Fulminant Central Nervous System Inflammatory Demyelinating Disease

Magaña¹,

Pittock²,

Lennon³

et al. 2009

Arch Neurol

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MPAPASS software enables stitched multiplex, multidimensional EV repertoire analysis and a standard framework for reporting bead-based assays

Welsh

Killingsworth

Kepley

et al. 2022

Cell Reports Methods

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Setty M. Magaña

Beneficial Plasma Exchange Response in Central Nervous System Inflammatory Demyelination

Posterior reversible encephalopathy syndrome in neuromyelitis optica spectrum disorders

Neuromyelitis optica IgG stimulates an immunological response in rat astrocyte cultures

Neuromyelitis Optica IgG Serostatus in Fulminant Central Nervous System Inflammatory Demyelinating Disease

MPAPASS software enables stitched multiplex, multidimensional EV repertoire analysis and a standard framework for reporting bead-based assays

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