TABLE 1

Patient Characteristics at Time of Seizure Diagnosis

Case	Center	Age (y)	Sex	Diagnosis	Tumor localization	Treatment	Disease status	Seizure disorder before
1 + 2^*	F	64	F	AA (1989)	Right frontal	SU, RA, CT 1989	SD, no residual tumor	Yes (motor SPS, TCS)
3	R	66	F	O (1985)	Right frontal	SU, RA, PCV 1985	SD, no residual tumor	Yes (motor SPS)
4	S	44	M	A (1991)	Left frontotemporal	SU 1991, 1996, 1997	SD, no residual tumor	Yes (TCS)
				OA (1996)		RA/BCNU 1997
				AOA (1997)
5	R	54	M	A (2014)	Left frontoparietal	SU, TMZ 2014	PD of residual tumor	Yes (motor SPS)
6	S	68	F	O (2004)	Right frontal	SU 2004	SD, residual tumor	Yes (motor SPS, TCS)
				AO (2011)		SU, RA/TMZ 05/2011
						CCNU 11/2011
7	R	51	M	GBM (2013)	Right frontal	SU 2013	ID of GBM	Yes (CPS, TCS)
8	R	29	F	A (2012)	Right frontoparietal	SU 2012, TMZ 2012–2013	PD of residual tumor	Yes (motor/sensory SPS, TCS)
				sGBM (2015)		SU + RA/TMZ 2015
9	R	45	M	AO (2012)	Right frontotemporal	SU, RA/TMZ 2012	SD, residual tumor	No
						PC 2014
						BEV/CCNU 2014–2015
10	R	76	F	Nonconvulsive SE caused by septic encephalopathy (6/2013)		Anticonvulsive treatment	No recovery	Yes (nonconvulsive SE 4/2013)

11	S	66	F	Embolic cerebral ischemia (2011)		Anticonvulsive treatment	Seizure-free after 1 d	No

↵* Patient presented with same clinical symptoms and EEG findings according to SE in 2011 and 2014. At both time points combined MRI and ¹⁸F-FET PET imaging was available.
F = Freiburg, Germany; R = Regensburg, Germany; S = Salzburg, Austria; O = oligodendroglioma WHO II; A = astrocytoma WHO II; OA = oligoastrocytoma WHO II; AA = anaplastic astrocytoma WHO III; AOA = anaplastic oligoastrocytoma WHO III; AO = anaplastic oligodendroglioma WHO III; GBM = glioblastoma WHO IV (s, secondary); SU = surgery; RA = radiotherapy; TMZ = temozolomide; BCNU = carmustine; CCNU = lomustine; PC = procarbazine + CCNU; PCV = procarbazine + CCNU + vincristine; BEV = bevacizumab; SD = stable disease; PD = progressive disease; ID = initial diagnosis.