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. 2022 Jun 2;17(6):e0263595. doi: 10.1371/journal.pone.0263595

Table 1. Frequency of neurological disease subgroups in the studies contributing IPD.

Neurological disease Studies (N = 83) n (%) Patients (N = 1979) n (%)
Encephalopathy 61 (73.5) 978 (49.4)
Encephalitis 37 (44.6) 92 (4.6)
Delirium 32 (38.6) 161 (8.1)
Coma 13 (15.7) 37 (1.9)
Encephalopathy–other 40 (48.2) 688 (34.8)
Insufficient information to define subtype 0 (0) 0 (0)
Cerebrovascular event 55 (66.3) 506 (25.6)
Ischaemic 45 (54.2) 308 (15.6)
Haemorrhagic 29 (34.9) 90 (4.5)
Vasculitis 2 (2.4) 2 (0.1)
Cerebrovascular event—other 27 (32.5) 106 (5.4)
Insufficient information to define subtype 0 (0) 0 (0)
Meningitis 9 (10.8) 15 (0.8)
Acute Disseminated Encephalomyelitis (ADEM) 12 (14.5) 14 (0.7)
Myelitis 12 (14.5) 13 (0.7)
Guillain-Barré syndrome 30 (36.1) 51 (2.6)
Radiculitis 2 (2.4) 4 (0.2)
Peripheral neuropathy 24 (28.9) 115 (5.8)
Myositis 2 (2.4) 2 (0.1)
Other neurological presentation 31 (37.3) 382 (19.3)
Smell or taste disturbance 13 (15.7) 247 (12.5)
Neuropsychiatric disorder 2 (2.4) 49 (2.5)
Myopathy 5 (6) 38 (1.9)
Autonomic dysfunction 4 (4.8) 27 (1.4)

IPD = individual patient data

1. Individual counts of studies and patients exceed the total numbers in the database, as patients with more than one diagnosis may have been counted more than once within different neurological disease categories.

2. Encephalitis and encephalopathy (including delirium and coma) are pooled together.

3. If patients have more than one neurological disease diagnosis (e.g., encephalitis and myelitis), they are described here. For some diagnoses, these patients may not be captured within the disease categories above.

4. For inclusion, neurological disease had to be acute, i.e. that reached a clinical zenith or plateau less than 28 days from the onset of first neurological symptoms, We included all clinician-defined ‘other’ neurological presentations, including smell or taste disturbance, but we excluded common systemic core complaints of COVID-19 without further qualification, e.g. fatigue, asthenia, myalgia without clinical suspicion of myopathy/myositis, or headache without clinical suspicion of meningitis/cerebrovascular event.