Anti-NMDA Receptor Encephalitis Clinical Pathway — Inpatient
Paroxysmal Sympathetic Hyperactivity (PSH)
PSH most frequently occurs soon after an acute brain injury and has been observed in children and adults with anti-NMDARE. Core clinical features of PSH include tachycardia, hypertension, tachypnea, central fever, diaphoresis, and/or increased muscle tone with possible dystonic posturing. Episodes have a rapid onset and are changes in core vital signs and clinical features that occur simultaneously for multiple days. They are most often triggered by noxious stimulation, such as acute pain, suctioning, loud noises, repositioning, urinary retention, increased tone, acute illness, but they can also occur without apparent trigger.
The term PSH was established as the standard by a consensus committee in 2014. Nomenclature to describe this constellation of cardiovascular and physical symptoms has varied over time and includes over 30 historical terms such as “dysautonomia”, “sympathetic storm”, and “autonomic storming”.
Non-pharmacologic Management
PSH can be triggered by a variety of interventions as listed above. Many of the contributing factors can be managed or avoided by prevention and treatment strategies. Some strategies include:
- Avoidance of noxious stimuli
- Clustering care when able/appropriate
- Control light and noise in the child's room
- Daily review of need for tubes/lines
- Continued evaluation of child's environment for noxious stimuli (e.g., diaper change, IV infiltrate, laying on lines or cords, irritation by clothing)
- Use of appropriate preventative strategies when triggering therapies are indicated
- Identification and appropriate treatment and/or prevention of urinary retention and constipation
- Involvement of Child Life, PT/OT
Pharmacologic Management
The below management and dosing strategies are not validated and come from one group’s experience in one tertiary medical center.
There is no standard of care for pharmacologic intervention for PSH. The choice of medications must be tailored based on child-specific vital signs, clinical status, and clinical effects. Therapies should always be evaluated for drug-disease contraindications, drug-drug interactions, and clinical effects. For ongoing management, please work with the primary service, clinical pharmacy, and PM&R.
Medications
| PSH Symptom Targeted | Baclofen | Benzodiazepines | Bromocriptine | Clonidine | Dantrolene | Dexmedetomidine* | Gabapentin | Opioids | Propranolol |
|---|---|---|---|---|---|---|---|---|---|
| Agitation | Yes | Yes | Yes | Yes | Yes | Yes | |||
| Hypertension | Yes | Yes | Yes | Yes | |||||
| Tachycardia | Yes | Yes | Yes | Yes | |||||
| Diaphoresis | Yes | Yes | |||||||
| Hyperthermia | Yes | Yes | Yes | Yes | |||||
| Hypertonia | Yes | Yes | Yes | Yes | Yes | Yes | |||
| Tachypnea | Yes | ||||||||
| Abortive Therapy of Acute Episodic Symptoms | Yes | Yes | Yes | Yes | |||||
| Maintenance/Prophylaxis | Yes | Yes | Yes | Yes | Yes | Yes | Yes | Yes | Yes |
| *Dexmedetomidine is restricted to children located in an intensive care unit (ICU) | |||||||||
Therapy De-escalation
Many of these pharmacotherapies require a wean prior to discontinuation. Please work with clinical pharmacy and/or the managing service to determine an appropriate plan for therapy de-escalation.
References
- Paroxysmal Sympathetic Hyperactivity in Severe Anti-N-Methyl-d-Aspartate Receptor Encephalitis: A Single Center Retrospective Observational Study
- Characteristics and Outcomes of Paroxysmal Sympathetic Hyperactivity in Anti-NMDAR Encephalitis
- Successful Management of Paroxysmal Sympathetic Hyperactivity in Anti-N-Methyl-D-Aspartate Receptor