Epilepsy and Mitochondrial Dysfunction: A Single Center’s Experience

Saneto, Russell P.

doi:10.1177/2326409817733012

Russell P. Saneto Corresponding Author:Russell P. Saneto, DO, PhD, Division of Pediatric Neurology, Department ofNeurology, University of Washington, 4800 Sand Point Way NE, Seattle, WA98195, USA.Email: russ.saneto@seattlechildrens.org

Division of Pediatric Neurology, Department of Neurology, University of Washington, Seattle, WA, USA

Corresponding Author:Russell P. Saneto, DO, PhD, Division of Pediatric Neurology, Department ofNeurology, University of Washington, 4800 Sand Point Way NE, Seattle, WA98195, USA.Email: russ.saneto@seattlechildrens.org

Declaration of Conflicting Interests

The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Figures (2)
Tables (4)

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Figure 1
A, The electroencephalogram (EEG) pattern in panel A shows interictal epileptiform discharges over the left and right hemispheres with background slowing (multifocal spike discharges [MISD]). This EEG epoch is taken from a patient who had infantile spasms at 4 months of age. This EEG epoch represents the findings at age 12 years. Panel B: This EEG epoch is from the same patient at age 12 years showing a generalized tonic seizure. At the onset of the seizure, the background becomes attenuated with the evolution of low amplitude theta frequencies after several seconds. The total time of the tonic seizure was 25 seconds (not shown). During the seizure, the patient stiffened all limbs. Panel C: An epoch taken from a patient who developed infantile spasms at the same age of the patient whose EEG is shown in Panel A. The EEG epoch was from a video EEG study at 14 years of age and demonstrating a focal motor seizure that begins over the left frontocentral region with the seizure increasing the distribution to the left lateral hemisphere. The seizure remained focal throughout the course of the seizure. The patient developed right upper extremity stiffening with a head turn to the left. Prior to the seizure, the EEG demonstrated a similar background of MISD as the patient shown in A (data not shown).

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Figure 2
A, This picture shows a drawing by patient before being placed on topiramate monotherapy. At the time of this drawing, she was having dyscognitive seizures (atypical absence episodes with postictal changes). B, This picture shows a drawing by the same patient several months after starting topiramate monotherapy. Her seizures were well controlled at the time of the drawing. At the time of this drawing, the mother had noted that her daughter was cognitively slower and had difficulty in word finding.

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Table 1
Demographics, Age of Seizure Onset, Seizure Semiology, Electron Transport Chain (ETC), and Molecular Abnormalities, and the Electroencephalograph Findings.^a a After the age of 2 years, age of onset was rounded to the nearest year.

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Table 2
Mitochondrial Patients With Infantile Spasms: Hypsarrythmia on EEG, Epileptic Spasms, and Developmental Delay.^a a The demographic of sex, age of infantile spasms onset, electron transport chain or genetic defect, medications used and age of death (if occurred) are given. ,^b b Patients 8 and 10 presented with an EEG pattern of suppression-bursts before evolving into hypsarrhythmia. ,^c c Patient 3 became seizure free on monotherapy of ketogenic diet (4:1 ratio) but had to discontinue due to parental concerns.

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Table 3
Patients With Mitochondrial DNA- and Nuclear DNA-Encoded Mutations and Epilepsy.^a a After the age of 24 months, the age of onset was rounded up/down to reflect years.

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Table 4
Seizure Medications Used for Seizure Control.^a a This table indicates the individual seizure medications that each patient used during the course of this study. ,^b b The range of seizure medications listed does not include those medications used to control status epilepticus or experimental medications used in clinical trials.

Patient (Sex)	Age of Seizure Onset	Semiology	EEG Findings	ETC Abnormalities	MolecularAbnormality
1 (m)	1 month	Myo/tonic	MISD	IV
2 (m)^b b Patients who have passed away.	1 month	Myo/myoC/SE	Sl	NA	POLG
3(f)	1 month	F-motor	MISD	I, II/III
4 (m)	1 month	ES > myo/F-motor	Hyps > MISD	III
5 (m)	1 month	ES > myo/Tonic	Hyps > MISD	I
6 (m)	2 months	F-motor	MISD	III
7 (m)	2 months	ES > myo/tonic	Hyps > MISD	IV	MTOI
8(f)	2 months	Myo/tonic/F-motor	MISD	I
9 (f)^b b Patients who have passed away.	2 months	ES > tonic	BS > MISD	NA	E3/Lipoic acid
10 (m)	2 months	Myo/tonic/clonic	MISD	NA	m.11778G>A
11 (m)	3 months	F-motor/dys	MISD	NA	m.8993T>G
12 (m)	3 months	ES > myo/tonic	Hyps > MISD	I
13(f)	3 months	ES > myo/tonic/myoC	Hyps > MISD	III
14 (f)^b b Patients who have passed away. ,^c c Patients who passed away to sudden unexplained death due to epilepsy.	4 months	ES > myo/tonic	Hyps > MISD	I
15(f)	4 months	ES > myo/tonic	Hyps > MISD	II, III, IV
16(f)	4 month	ES > myo/tonic	Hyps > MISD	I
17 (f)^b,c	4 months	ES > F-motor	Hyps > MISD	I
18 Female	4 months	Myo/tonic/F-motor	MISD	I
19(f)	4 months	ES > myo/tonic	BS > Hyps > MISD	IV
20 (f)^b b Patients who have passed away.	5 months	Myo	MISD	IV
21 (m)	5 months	ES > myo/tonic	Hyps > MISD	I, IV
22 (m)	5 months	Myo/tonic/F-motor	MISD	I
23 (m)	6 months	Myo/tonic	MISD	I
24 (m)	6 months	Myo/tonic/days	GSW	III
25 (f)	6 months	Myo/tonic/atonic	MISD	I
26 (f)	6 months	Myo/tonic	MISD	III
27 (m)	6 months	Myo/tonic	MSID	I
28 (m)^b b Patients who have passed away.	7 months	Myo/tonic/GTC/myoC/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD	NA	POLG
29 (m)	8 months	F-motor	MISD	III
30 (f)	8 months	Myo/2-GTC/F-motor	GSW	I
31 (m)	8 months	Myo/2-GTC/F-motor	GSW	IV
32 (f)^b b Patients who have passed away.	9 months	Myo/EPC/F-Clonic/MyoC	MISD	NA	POLG
33 (m)^b b Patients who have passed away.	9 months	Myo/F-clonic/myoC/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD	NA	POLG
34 (m)^b b Patients who have passed away.	11 months	F-motor	MISD	I, III
35 (m)	11 months	Myo/tonic/clonic	MISD	III, IV
36 (m)^b b Patients who have passed away.	12 months	ES/myo/tonic	Hyps > MISD	IV	TANGO 2
37 (m)	12 months	Myo/tonic	MISD	NA	m.8993T>G
38 (f)^b b Patients who have passed away.	12 months	Myo/tonic	MISD	I
39 (m)^b b Patients who have passed away.	12 months	Myo/tonic	MISD	III
40 (f)^b b Patients who have passed away.	12 months	Myo/tonic/F-motor	MISD	NA	PDHC deficiency
41 (f)	15 months	Myo/tonic/F-motor	MISD	I, II/III
42 (m)	15 months	ES/myo/tonic	Hyps > MISD	I
43 (m)	18 months	Dys	MISD	IV
44 (f)	18 months	Atonic/myo	MISD	IV
45 (m)	20 months	F-motor/dys	Focal	I
46 (m)	20 month	Myo/tonic	MISD	I
47 (m)	2 years	Dys/myo	MISD	NA	m.8363G>A
48 (f)	2 years	Myo/tonic/F-motor	MISD	NA	PDHAI
49 (f)	2 years	Myo	MISD	I, III, IV
50 (f)	2 years	Dys/atonic	GSW	II/III
51 (f)	2 years	GTC (febrile)	Sl	IV
52 (f)	2 years	Dys/atonic	GSW	I
53 (f)^b b Patients who have passed away.	2 years	ES/tonic	Hyps > MISD	I, III, IV
54(f)	2 years	Myo/tonic/F-motor	MISD	I, IV
55 (f)	2 years	Myo/tonic	MISD	I
56 (f)	2 years	Myo/tonic	MISD	I, III, IV
57(f)	2 years	EPC/myo/tonic	MISD	Normal	RARS 2
58 (f)^b b Patients who have passed away.	2 years	Myo/F-clonic/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD	NA	POLG
59(f)	3 years	F-motor	MISD	I
60 (m)	3 years	F-motor/2-GTC	GSW > MISD	I/III, II/III
61 (m)	3 years	Dys	MISD	I
62 (m)	3 years	Myo/tonic	GSW	III
63 (f)^b b Patients who have passed away.	3 years	F-motor/F-clonic/myo/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD	NA	POLG
64(f)	3 years	Myo/F-motor	MISD	IV
65 (f)	4 years	Myo/2-GTC	MISD	I
66 (f)	4 years	Tonic	MISD	I
67 (m)	4 years	Dys/F-motor	GSW	I
68 (f)^b b Patients who have passed away.	4 years	F-motor/Myo/F-clonic/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD	NA	POLG
69 (m)	4 years	F-motor/myo/2-GTC/SE	MISD	NA	m.3243A>G
70 (m)^b b Patients who have passed away.	5 years	F-motor/myo/F-clonic/EPC^c c Patients who passed away to sudden unexplained death due to epilepsy.	MISD > GSW > Sl	Normal	POLG
71 (m)	5 years	F-motor/dys	MISD	III
72 (m)	5 years	F-motor	Focal	I/III, II/III
73 (m)	5 years	Myo/tonic	MISD	III, IV
74 (f)^b b Patients who have passed away.	6 years	F-motor/myo/SE	MISD	NA	POLG
75 (f)	7 years	Dys	MISD	NA	m.3243A>G
76 (f)	8 years	Dys	MISD	III
77 (f)	9 years	Myo/F-motor	MISD	I
78 (m)^b b Patients who have passed away.	10 years	F-motor/myo	MISD	I
79 (m)	10 years	F-motor/myo	MISD	NA	m.14478T>C
80 (m)^b b Patients who have passed away.	11 years	Dys (NCS)	MISD	NA	m.14459A>G
81 (f)^b b Patients who have passed away.	14 years	F-motor/myo/EPC+	MISD	III	POLG
82 (m)	14 years	F-motor/2-GTC	MISD	NA	m.3243A>G
83 (f)	17 years	F-motor/2-GTC/myo/SE	MISD	NA	POLG
84 (f)	17 years	F-motor/myo/SE	MISD	NA	POLG
85 (f)	19 years	Myo/tonic	MISD	NA	SLCI9A3

Patient (Sex)	Age Onset	ETC/Genetic Defect	Medications	Age of Death
1 (m)	2 months	C-IV; MTOI	ACTH, VGB, TPM, FBM, CLB, LEV, LTG, KD
2(m)	3 months	C-I	ACTH, VGB, LTG, TPM, LEV, GAN
3(m)	3 months	C-III	ACTH, KD, LTG, RFM, LEV
4(f)	3 months	E3/lipoic acid	VGB, Prednisone, ZNS	8 months
5 (m)	3 months	C-I	PB, ACTH, VGB, LAC, LTG, LEV, KD
6(f)	4 months	C-I	ACTH, ZNS, LTG	5 years
7 (m)	4 months	C-II, C-III, C-IV	ACTH, ZNS, LTG, RFM, LAC, VPA, CLB
8(f)	4 months	C-I	ACTH, ZNS, VGB	4 years
9(f)	4 months	C-I	ACTH, VGB, LTG, CLB, RFM, GAN
10(f)	4 months	C-IV	PB, ZNS, B6/LEV/KD	4 years
11 (m)	5 months	C-I, C-IV	ACTH, ZNS, TPM, LEV, LTG, KD
12 (m)	12 months	C-IV; TANGO 2	ACTH, ZNS, VPA, CLB, CBD	3 years
13 (m)	15 months	C-I	Prednisone, ZNS, LTG
14 (f)	23 months	C-I, C-III, C-IV	ZNS, TPM, KD	5 years

Patient (Sex)	Age Onset	Gene	Mutation	Status Epilepticus	Number Seizure Medications	Death
1 (m)	1 month	POLG	c.428C>T/c.679C>T	Yes	3	l year
2 (m)	2 months	ND5	m.ll778G>A	No	3
3 (m)	2 months	MTOI	c.176C>G/c.922A>G	No	9
4 (m)	3 months	MT-ATP6	m.8993T>G	No	4	7 years
5 (m)	7 months	POLG	c.2740A>C/c.3286C>T	Yes	4	2 years
6(f)	9 months	POLG	c.l399G>A/c.2897T>G	Yes	5
7(m)	9 months	POLG	c.l399G>A/c.33l3G>C	Yes	8	l year
8(m)	12 months	TANGO2	c.7ll-3C>G/del exon 3-9	Yes	5	4 years
9 (m)	12 months	MT-ATP6	m.8993T>G	No	4
10 (m)	24 months	MT-TK	m.8363G>A	No	4
11 (f)	24 months	RARS2	c.472_474delAAA/c.772C>A	Yes	7
12(f)	24 months	PDHAI	c.904C>A	No	2
13(f)	3 years	POLG	c.l399G>A/c.202C>T	Yes	5	3 years
14(f)	3 years	POLG	c.2242G>C/c.2554C>T	Yes	4	8 years
15(f)	4 years	POLG	c.2242G>C/c.2542G>A	Yes	6	7 years
16 (m)	4 years	MTTLI	m.3243A>G	Yes	4
17 (m)	5 years	MtDNA	7.4 kb deletion	No	3
18 (m)	5 years	POLG	c.l399G>A/c.2542G>A	Yes	5	l2 years
19(f)	6 years	POLG	c.229C>G/c.2243G>C	Yes	6	8 years
20 (f)	7 years	MTTLI	m.3243A>G	Yes	3
21 (m)	10 years	ND6	m.l4487T>C	Yes	3
22 (m)	11 years	ND6	m.l4459T>G	Yes	l	l5 years
23 (f)	14 years	POLG	c.l399G>A/c.l399G>A	Yes	6	24 years
24 (f)	17 years	POLG	c.l399G>A/c.l399G>A	Yes	5
25 (f)	17 years	POLG	c.l399G>A/c.l399G>A	Yes	6
26 (f)	19 years	SLCI9A3	c.l228A>G/c.223G>A	Yes	4

Medication	Patients
Adrenocorticotrophic hormone	11
Carbamazepine	12
Clobazam	11
Ethosuximide	10
Felbamate	3
Ketogenic diet	21
Lacosamide	8
Lamotrigine	57
Levetiracetam	53
Oxcarbazepine	9
Phenobarbital	10
Prednisone	2
Phenytoin	4
Topiramate	24
Rufinamide	7
Valproic acid	18
Vigabatrin	9
Zonisamide	30

[1] Corresponding Author:Russell P. Saneto, DO, PhD, Division of Pediatric Neurology, Department ofNeurology, University of Washington, 4800 Sand Point Way NE, Seattle, WA98195, USA.Email: russ.saneto@seattlechildrens.org

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Epilepsy and Mitochondrial Dysfunction: A Single Center’s Experience

Abstract