## Correct Answer: D. CSF PCR for viral DNA CSF PCR for viral DNA is the gold standard for diagnosing HSV encephalitis because it offers superior sensitivity (>95%) and specificity (>99%) compared to all other methods. HSV-1 and HSV-2 are DNA viruses, and real-time PCR (qPCR) directly amplifies viral DNA from cerebrospinal fluid, providing rapid confirmation within hours. This is critical in acute encephalitis where early diagnosis guides immediate acyclovir therapy—delaying treatment even by 24–48 hours significantly worsens neurological outcomes and mortality. PCR is non-invasive (requires only CSF obtained via lumbar puncture), does not require viral culture infrastructure, and remains positive even when viral load is low. In Indian clinical practice, CSF PCR for HSV is now the standard of care per AIIMS and NIMHANS protocols for suspected viral encephalitis. The test is performed on fresh CSF and results are typically available within 4–6 hours in well-equipped centers, making it ideal for emergency decision-making in acute meningitis/encephalitis. ## Why the other options are wrong **A. IgM in CSF** — While IgM antibodies in CSF indicate intrathecal HSV-specific antibody production and suggest HSV infection, they appear only 5–7 days after symptom onset. In acute encephalitis presenting within 48–72 hours, IgM may be negative, leading to false-negative results and delayed diagnosis. IgM is also less specific than PCR and cannot differentiate between HSV-1 and HSV-2. This is an NBE trap: students confuse serology (useful for retrospective diagnosis) with direct viral detection (needed for acute management). **B. Tzanck smear of CSF** — Tzanck smear detects multinucleated giant cells and is useful for HSV skin lesions (vesicles), not for CSF. HSV encephalitis does not produce characteristic cytopathic changes visible on Tzanck smear in CSF. This test has very low sensitivity in meningitis/encephalitis and is not a standard diagnostic method for CNS HSV infection. The question stem describes systemic encephalitis, not mucocutaneous disease, making this option anatomically and clinically inappropriate. **C. CSF culture on chick embryo lines** — Although HSV can be cultured on chick embryo fibroblasts and other cell lines, viral culture from CSF is slow (takes 3–7 days), insensitive in encephalitis (many samples are culture-negative despite PCR positivity), and requires specialized virology laboratory infrastructure rarely available in Indian hospitals. In acute encephalitis, waiting a week for culture results is clinically unacceptable—acyclovir must be started empirically within hours. Culture is now obsolete for HSV encephalitis diagnosis in modern practice. ## High-Yield Facts - **CSF PCR for HSV** is the gold standard for HSV encephalitis diagnosis with >95% sensitivity and >99% specificity. - **HSV-1 accounts for ~90%** of HSV encephalitis cases in India; HSV-2 causes neonatal and primary infection encephalitis. - **IgM appears 5–7 days** after symptom onset, making it unreliable in acute presentation (<72 hours). - **Acyclovir must be started empirically** within 24–48 hours of symptom onset; PCR results guide continuation vs. discontinuation. - **CSF findings in HSV encephalitis**: pleocytosis (100–500 cells/μL, lymphocytic), elevated protein (50–100 mg/dL), normal/low glucose, negative bacterial culture. - **Temporal lobe involvement** on MRI (T2/FLAIR hyperintensity) is characteristic of HSV-1 encephalitis and supports clinical suspicion pending PCR. ## Mnemonics **PCR = Prompt, Certain, Rapid** For acute viral encephalitis, remember PCR gives you Prompt results (hours), Certainty (>95% sensitivity), and Rapid turnaround—essential for starting acyclovir immediately. Culture and serology are too slow for acute CNS infection. **HSV Encephalitis Diagnosis: FAST** F = Fever + focal seizures; A = Altered sensorium; S = Start acyclovir empirically; T = Test with CSF PCR (not culture, not serology). This memory hook emphasizes that PCR is the test of choice in acute presentation. ## NBE Trap NBE pairs IgM serology with acute viral encephalitis to trap students who confuse retrospective serological diagnosis (useful after 1–2 weeks) with acute direct viral detection (needed within 24–48 hours). The question's emphasis on "high fever, altered sensorium, seizures" signals acute presentation, where PCR—not antibodies—is the answer. ## Clinical Pearl In Indian emergency departments, empiric acyclovir is started on clinical suspicion of HSV encephalitis (fever + altered sensorium + seizures) before any test result. CSF PCR confirms the diagnosis and justifies continuation; negative PCR at 48–72 hours allows safe discontinuation, reducing unnecessary antibiotic/antiviral exposure and cost—critical in resource-limited Indian settings. _Reference: Jawetz, Melnick & Adelberg's Medical Microbiology Ch. 37 (Herpesviruses); Harrison's Principles of Internal Medicine Ch. 173 (Viral Meningitis and Encephalitis)_
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