| Literature DB >> 26295485 |
Karen C Bloch, Carol A Glaser.
Abstract
Encephalitis is a devastating illness that commonly causes neurologic disability and has a case fatality rate >5% in the United States. An etiologic agent is identified in <50% of cases, making diagnosis challenging. The Centers for Disease Control and Prevention Emerging Infections Program (EIP) Encephalitis Project established syndromic surveillance for encephalitis in New York, California, and Tennessee, with the primary goal of increased identification of causative agents and secondary goals of improvements in treatment and outcome. The project represents the largest cohort of patients with encephalitis studied to date and has influenced case definition and diagnostic evaluation of this condition. Results of this project have provided insight into well-established causal pathogens and identified newer causes of infectious and autoimmune encephalitis. The recognition of a possible relationship between enterovirus D68 and acute flaccid paralysis with myelitis underscores the need for ongoing vigilance for emerging causes of neurologic disease.Entities:
Keywords: EIP; Emerging Infections Program; bacteria; encephalitis; surveillance; viruses
Mesh:
Year: 2015 PMID: 26295485 PMCID: PMC4550161 DOI: 10.3201/eid2109.150295
Source DB: PubMed Journal: Emerg Infect Dis ISSN: 1080-6040 Impact factor: 6.883
Case definition for encephalitis in the Emerging Infections Program Encephalitis Project, 1997–2010*
| Criteria |
|---|
| Major criterion (required): Altered mental status lasting ≥24 h |
| Plus |
| 1. Fever ≥38°C occurring ≤72 h before or after hospital admission |
| 2. Seizures |
| 3. Focal neurologic deficits not previously present on examination |
| 4. Cerebrospinal fluid pleocytosis (≥5 leukocytes/mm3) |
| 5. Abnormal electroencephalogram |
| 6. Abnormal neuroimaging (computed tomography or magnetic resonance imaging) representing an acute process |
*International Encephalitis Consortium case definition requires the presence of the major criteria plus ≥3 minor criteria for confirmed/probable; ≥2 for probable encephalitis ().
Core diagnostic testing algorithm for the Emerging Infections Program Encephalitis Project, 1997–2010*
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| NP swab | PCR | Year-round |
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| Serum | Serology | May–October |
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| CSF | PCR | Year-round |
| NP swab | PCR | Year-round | |
| Rectal swab | PCR | Year-round | |
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| CSF | PCR | Year-round |
| Serum | Serology | Year-round | |
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| CSF | PCR | Year-round |
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| CSF | PCR | Year-round |
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| NP swab | PCR | November–April |
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| NP swab | PCR | November–April |
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| Rectal swab | Antigen | November–April |
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| CSF | PCR | Year-round |
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| CSF | Serology | May–October |
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| Serum | Serology | May–October |
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| Serum | Serology | Year-round |
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| NP swab | PCR | Year-round |
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| Whole blood | PCR | May–October |
| Serum | Serology | May–October | |
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| NP swab | PCR | Year-round |
| Serum | Serology | Year-round | |
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| Serum | Serology | May–October |
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| CSF | VDRL | Year-round |
| Serum | RPR | Year-round |
*Diagnostic testing algorithm at the Tennessee site; regional differences and testing availability associated with minor variations in core testing at the California site. Additional supplementary testing was performed when indicated based on individualized epidemiologic, demographic, clinical, or radiographic features. CSF, cerebrospinal fluid; NP, nasopharyngeal; VDRL, venereal disease research laboratory test; RPR, rapid plasma reagin. †Arbovirus panel included Lacrosse virus, St. Louis encephalitis virus, Western equine encephalitis virus, and Eastern equine encephalitis virus.
Emerging Infections Program Encephalitis Project clinical profiles, 1997–2010*
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| Temporal lobe enhancement on imaging or activity on EEG | HSV accounted for approximately one third of cases |
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| Movement disorder | Measles (SSPE), autoimmune encephalitides |
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| Ataxia or gait disorder, or focal cerebellar lesion on imaging | Acute EBV infection seen in a minority of cases |
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| Neuroimaging showing diffuse brain edema | Deaths exceed 70% |
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| Seizures requiring anesthetic coma for management | Majority of case-patients: pediatric patients with prolonged hospitalization |
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| Onset with seizure and return to baseline mental status in <96 h | CSF typically bland; |
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| New onset of prominent psychiatric symptoms | Anti-NMDAR antibodies common in this syndrome |
*EEG, electroencephalogram; HSV, herpes simplex virus; SSPE, subacute sclerosing panencephalitis; EBV, Epstein-Barr virus; NMDAR, anti-N-methyl-D-asparate receptor.