FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2912242734> ?p ?o ?g. }

• W2912242734 endingPage "463" @default.
• W2912242734 startingPage "452" @default.
• W2912242734 abstract "Summary Objective Seizures develop in 80% of patients with anti– N ‐methyl‐ d ‐aspartate receptor (NMDAR) encephalitis, and these represent a major cause of morbidity and mortality. Anti‐NMDAR antibodies have been linked to memory loss in encephalitis; however, their role in seizures has not been established. We determined whether anti‐NMDAR antibodies from autoimmune encephalitis patients are pathogenic for seizures. Methods We performed continuous intracerebroventricular infusion of cerebrospinal fluid (CSF) or purified immunoglobulin (IgG) from the CSF of patients with anti‐NMDAR encephalitis or polyclonal rabbit anti‐NMDAR IgG, in male C57BL/6 mice. Seizure status during a 2‐week treatment was assessed with video‐electroencephalography. We assessed memory, anxiety‐related behavior, and motor function at the end of treatment and assessed the extent of neuronal damage and gliosis in the CA1 region of hippocampus. We also performed whole‐cell patch recordings from the CA1 pyramidal neurons in hippocampal slices of mice with seizures. Results Prolonged exposure to rabbit anti‐NMDAR IgG, patient CSF, or human IgG purified from the CSF of patients with encephalitis induced seizures in 33 of 36 mice. The median number of seizures recorded in 2 weeks was 13, 39, and 35 per mouse in these groups, respectively. We observed only 18 brief nonconvulsive seizures in 11 of 29 control mice (median seizure count of 0) infused with vehicle (n = 4), normal CSF obtained from patients with noninflammatory central nervous system (CNS) conditions (n = 12), polyclonal rabbit IgG (n = 7), albumin (n = 3), and normal human IgG (n = 3). We did not observe memory deficits, anxiety‐related behavior, or motor impairment measured at 2 weeks in animals treated with CSF from affected patients or rabbit IgG. Furthermore, there was no evidence of hippocampal cell loss or astrocyte proliferation in the same mice. Significance Our findings indicate that autoantibodies can induce seizures in anti‐NMDAR encephalitis and offer a model for testing novel therapies for refractory autoimmune seizures." @default.
• W2912242734 created "2019-02-21" @default.
• W2912242734 creator A5017626526 @default.
• W2912242734 creator A5028503045 @default.
• W2912242734 creator A5028610293 @default.
• W2912242734 creator A5030346561 @default.
• W2912242734 creator A5037860429 @default.
• W2912242734 creator A5041248710 @default.
• W2912242734 creator A5061418721 @default.
• W2912242734 creator A5076173662 @default.
• W2912242734 creator A5088136783 @default.
• W2912242734 date "2019-02-11" @default.
• W2912242734 modified "2023-10-16" @default.
• W2912242734 title "A mouse model of seizures in anti– <i>N</i> ‐methyl‐ <scp>d</scp> ‐aspartate receptor encephalitis" @default.
• W2912242734 cites W1087196417 @default.
• W2912242734 cites W1510634986 @default.
• W2912242734 cites W1603573791 @default.
• W2912242734 cites W1856181205 @default.
• W2912242734 cites W1887067355 @default.
• W2912242734 cites W1965907445 @default.
• W2912242734 cites W1971501807 @default.
• W2912242734 cites W1978480793 @default.
• W2912242734 cites W1979824001 @default.
• W2912242734 cites W1996752921 @default.
• W2912242734 cites W1999011928 @default.
• W2912242734 cites W2016180469 @default.
• W2912242734 cites W2033164930 @default.
• W2912242734 cites W2044019190 @default.
• W2912242734 cites W2044794002 @default.
• W2912242734 cites W2051552021 @default.
• W2912242734 cites W2053785929 @default.
• W2912242734 cites W2057216398 @default.
• W2912242734 cites W2061056490 @default.
• W2912242734 cites W2064703428 @default.
• W2912242734 cites W2074183373 @default.
• W2912242734 cites W2075313898 @default.
• W2912242734 cites W2083974405 @default.
• W2912242734 cites W2085682222 @default.
• W2912242734 cites W2095804141 @default.
• W2912242734 cites W2097556759 @default.
• W2912242734 cites W2098001563 @default.
• W2912242734 cites W2102092558 @default.
• W2912242734 cites W2105127406 @default.
• W2912242734 cites W2114398221 @default.
• W2912242734 cites W2117603434 @default.
• W2912242734 cites W2125513893 @default.
• W2912242734 cites W2129684937 @default.
• W2912242734 cites W2144003555 @default.
• W2912242734 cites W2146199022 @default.
• W2912242734 cites W2163022996 @default.
• W2912242734 cites W2171138396 @default.
• W2912242734 cites W2206429434 @default.
• W2912242734 cites W2206986585 @default.
• W2912242734 cites W2225011328 @default.
• W2912242734 cites W2280783985 @default.
• W2912242734 cites W2303462305 @default.
• W2912242734 cites W2343055661 @default.
• W2912242734 cites W2440417904 @default.
• W2912242734 cites W2493627768 @default.
• W2912242734 cites W2511028312 @default.
• W2912242734 cites W2560667011 @default.
• W2912242734 cites W2560726081 @default.
• W2912242734 cites W2619242177 @default.
• W2912242734 cites W2766822273 @default.
• W2912242734 doi "https://doi.org/10.1111/epi.14662" @default.
• W2912242734 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6684284" @default.
• W2912242734 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30740690" @default.
• W2912242734 hasPublicationYear "2019" @default.
• W2912242734 type Work @default.
• W2912242734 sameAs 2912242734 @default.
• W2912242734 citedByCount "41" @default.
• W2912242734 countsByYear W29122427342019 @default.
• W2912242734 countsByYear W29122427342020 @default.
• W2912242734 countsByYear W29122427342021 @default.
• W2912242734 countsByYear W29122427342022 @default.
• W2912242734 countsByYear W29122427342023 @default.
• W2912242734 crossrefType "journal-article" @default.
• W2912242734 hasAuthorship W2912242734A5017626526 @default.
• W2912242734 hasAuthorship W2912242734A5028503045 @default.
• W2912242734 hasAuthorship W2912242734A5028610293 @default.
• W2912242734 hasAuthorship W2912242734A5030346561 @default.
• W2912242734 hasAuthorship W2912242734A5037860429 @default.
• W2912242734 hasAuthorship W2912242734A5041248710 @default.
• W2912242734 hasAuthorship W2912242734A5061418721 @default.
• W2912242734 hasAuthorship W2912242734A5076173662 @default.
• W2912242734 hasAuthorship W2912242734A5088136783 @default.
• W2912242734 hasBestOaLocation W29122427342 @default.
• W2912242734 hasConcept C118552586 @default.
• W2912242734 hasConcept C126322002 @default.
• W2912242734 hasConcept C134018914 @default.
• W2912242734 hasConcept C142724271 @default.
• W2912242734 hasConcept C148762608 @default.
• W2912242734 hasConcept C159654299 @default.
• W2912242734 hasConcept C170493617 @default.
• W2912242734 hasConcept C203014093 @default.
• W2912242734 hasConcept C2522874641 @default.
• W2912242734 hasConcept C2777682930 @default.
• W2912242734 hasConcept C2778186239 @default.

• next