ライフサイエンスコーパス: MTLE

1 MTLE has been well characterised and can usually be iden

2 MTLE mice with GABAergic iNs show a significant reductio

3 MTLE was associated with a regional reduction in fibre d

4 cordings, SPECT studies, and MR images of 32 MTLE patients and of a subgroup of 11 patients with path

5 Using a MTLE mouse model, we show that retrovirus-driven express

6 e epilepsy (MTLE) without MRI abnormalities (MTLE-NMRI) represent a challenge for diagnosis of the un

7 etwork excitability dynamics in epilepsy and MTLE.

8 as present in the neocortex of both NTLE and MTLE patients in similar concentrations.

9 dies, we tested the hypothesis that NTLE and MTLE subtypes of human epilepsy might differ in regards

10 ined with western blots and compared between MTLE-HS patients who were showing (n = 06) or not showin

11 nd synaptic reorganization that characterize MTLE are not seen.

12 the interneurons in a mouse model of chronic MTLE resulted in consistent mesiotemporal seizure suppre

13 At the Clinic, MTLE had been recognized to be familial in 2 patients on

14 Historically, we have considered MTLE a single disorder, but it may be time to view it as

15 Compared to 8,718 controls, MTLE cases carried a higher burden of ultrarare missense

16 pocampal neuronal loss and gliosis), defines MTLE.

17 ng patients with newly intractable disabling MTLE, resective surgery plus AED treatment resulted in a

18 12 years) had mesial temporal lobe epilepsy (MTLE) and disabling seizues for no more than 2 consecuti

19 patients with mesial temporal lobe epilepsy (MTLE) and hippocampal sclerosis.

20 ouse model of mesial temporal lobe epilepsy (MTLE) as well as in hippocampal tissue resected from ind

21 rug-resistant mesial temporal lobe epilepsy (MTLE) following anterior temporal lobe (TL) resection.

22 Mesial temporal lobe epilepsy (MTLE) is a chronic neurological disorder affecting almos

23 Mesial temporal lobe epilepsy (MTLE) is a common medically refractory neurological dise

24 Mesial temporal lobe epilepsy (MTLE) is a syndromic disorder presenting with seizures a

25 Medial temporal lobe epilepsy (MTLE) is associated with limbic atrophy involving the hi

26 knowledge of mesial-temporal-lobe epilepsy (MTLE) is extensive, yet still insufficient to draw final

27 The cause of mesial temporal lobe epilepsy (MTLE) is often unknown.

28 s of LITT for mesial temporal lobe epilepsy (MTLE) is relevant to clinicians and patients.

29 Mesial temporal lobe epilepsy (MTLE) is the most common focal epilepsy.

30 Mesial temporal lobe epilepsy (MTLE) is the most common form of focal, pharmacoresistan

31 nal damage in medial temporal lobe epilepsy (MTLE) may lead to the development of aberrant connection

32 s in acquired mesial temporal lobe epilepsy (MTLE) remains unknown.

33 patients with mesial temporal lobe epilepsy (MTLE) show abnormalities in tissue concentrations of met

34 rast to prior mesial temporal lobe epilepsy (MTLE) studies, seizure-free intervals between the initia

35 izures in the mesial temporal lobe epilepsy (MTLE) syndrome.

36 patients with mesial temporal lobe epilepsy (MTLE) using the technique of composite subtraction ictal

37 progresses to mesial-temporal lobe epilepsy (MTLE) with dual pathology.

38 Patients with mesial temporal lobe epilepsy (MTLE) without MRI abnormalities (MTLE-NMRI) represent a

39 imal model of mesial temporal lobe epilepsy (MTLE), a disease accompanied with cognitive impairment.

40 patients with mesial temporal lobe epilepsy (MTLE), but recently pHFOs have also been recorded with c

41 c seizures in mesial temporal lobe epilepsy (MTLE), but the underlying mechanism remains unclear.

42 iagnosed with mesial temporal lobe epilepsy (MTLE), e.g., in hippocampal (HPC) pathology.

43 sections from mesial temporal lobe epilepsy (MTLE), plus neural stem-cell cultures and multi-electrod

44 apy-resistant mesial temporal lobe epilepsy (MTLE), which is associated with hippocampal seizures and

45 f surgery for mesial temporal lobe epilepsy (MTLE).

46 ouse model of mesial temporal lobe epilepsy (MTLE).

47 patients with mesial temporal lobe epilepsy (MTLE).

48 y intractable mesial temporal lobe epilepsy (MTLE).

49 patients with mesial temporal lobe epilepsy (MTLE).

50 patients with mesial temporal lobe epilepsy (MTLE; n = 64), those with extratemporal lobe (XTLE; n =

51 ver, immature astroglia are present in every MTLE case and their location and activity are dependent

52 onlesional MTLE actually represents familial MTLE (FMTLE).

53 zures) was 1645 (95% CI = 1448,1830) and for MTLE subjects (774 seizures) was 1500 (95% CI = 1324,163

54 t randomised trial of surgical treatment for MTLE, questions remain about the neurological consequenc

55 ation (DBS) of grey matter has been used for MTLE with limited success.

56 The chronological similarity between human MTLE and PLS rat epilepsy suggests that limbic seizure o

57 le for mGluR5 as therapeutic target in human MTLE.

58 subject as follows: epilepsy, specifying if MTLE; manifestations suspicious for epilepsy; or unaffec

59 In MTLE, NE concentrations in the CA1 subfield of the Pyram

60 The enzyme activity was lower by 38% in MTLE vs non-MTLE (mean 0.0060 [SD 0.0031] vs 0.0097 [0.0

61 tulate that the loss of perivascular AQP4 in MTLE is likely to result in a perturbed flux of water th

62 d in vivo whole-brain mGluR5 availability in MTLE patients using positron emission tomography (PET) a

63 a promising approach for seizure control in MTLE.

64 campal neurogenesis dramatically declines in MTLE patients with increased disease duration.

65 efined pattern of hippocampal deformation in MTLE patients compared with matched controls.

66 chanism which results in glutamate excess in MTLE remains unknown.

67 hanism affecting the network excitability in MTLE.

68 PET provides a focal biomarker for the EZ in MTLE with higher spatial accuracy compared to [(18) F]FD

69 Taken together with previous findings in MTLE-HS patients with IF who were evaluated by stereotac

70 in normal artificial cerebrospinal fluid in MTLE granule cells cannot be solely explained by a decre

71 (P<0.01)] and NE occurred more frequently in MTLE in Granular Cells of DG and Pyramidal Layer [P=0.05

72 amate accumulation and seizure generation in MTLE.

73 NE concentrations were higher in MTLE vs. NTLE in each subparcellation [P=0.012, 0.067 an

74 lain the perturbed glutamate homoeostasis in MTLE.

75 a new focus for therapeutic interventions in MTLE.

76 showed an overall increase in AQP4 levels in MTLE compared with non-MTLE hippocampi, quantitative Imm

77 nthetase in the hippocampus was 40% lower in MTLE than in non-MTLE samples (median 44 [IQR 30-58] vs

78 tate specific shift in metabolic networks in MTLE may improve the understanding of epileptogenesis an

79 Further, immature neurons in MTLE are mostly inactive, and are not observed in cases

80 ynaptic and cellular alterations observed in MTLE induce aberrant temporal coding in the hippocampus,

81 emporal lobe is the focus of the seizures in MTLE, and surgical resection of this structure, includin

82 explore the role of glutamine synthetase in MTLE we created a novel animal model of hippocampal glut

83 Among 242 subjects interviewed, MTLE was diagnosed in 9 of 121 relatives versus 0 of 121

84 Seventeen patients had left MTLE and 15 patients had right MTLE.

85 ateral TLH was significantly greater in left MTLE patients (p < 0.001), whereas right MTLE patients h

86 In left MTLE patients, greater extent of resection of ipsilatera

87 were set at 6 of 17 (P = 0.042) for the left MTLE group, 6 of 15 (P = 0.022) for the right MTLE group

88 networks in patients with right versus left MTLE, and can guide preoperative counseling and surgical

89 SCOM studies in patients with well-localized MTLE most commonly show a region of hyperperfusion in th

90 In the largest prospective multicenter MTLE LITT cohort, LITT was found to be well tolerated wi

91 ve NTLE patients but in only one of the nine MTLE patients (chi-square P<0.05).

92 In non-MTLE hippocampus, dystrophin was preferentially localize

93 ippocampus was 40% lower in MTLE than in non-MTLE samples (median 44 [IQR 30-58] vs 69 [56-87]% of ma

94 yme activity was lower by 38% in MTLE vs non-MTLE (mean 0.0060 [SD 0.0031] vs 0.0097 [0.0042] U/mg pr

95 s reduced by 44% in area CA1 of MTLE vs. non-MTLE hippocampi.

96 ase in AQP4 levels in MTLE compared with non-MTLE hippocampi, quantitative ImmunoGold electron micros

97 d to what extent newly diagnosed nonlesional MTLE actually represents familial MTLE (FMTLE).

98 ost one-fifth of newly diagnosed nonlesional MTLE, and it is largely unrecognized without direct ques

99 n contributes to the genetic architecture of MTLE, but does not appear to have a major role in failur

100 astrocytes was reduced by 44% in area CA1 of MTLE vs. non-MTLE hippocampi.

101 These results corroborate the concept of MTLE as a network disease, and may contribute to the und

102 that were suspicious, but not diagnostic, of MTLE occurred in 6 additional relatives versus none of t

103 ot appear to have a major role in failure of MTLE surgery.

104 cell dispersion, a pathological hallmark of MTLE.

105 patterns depending on the lateralization of MTLE may represent distinct epileptic networks in patien

106 ic rats obtained by the pilocarpine model of MTLE.

107 with seizure generation in a mouse model of MTLE.

108 tic variation influences seizure outcomes of MTLE surgery.

109 QP4 might be involved in the pathogenesis of MTLE.

110 ts demonstrated typical seizure semiology of MTLE.

111 In contrast to prior studies of MTLE, only 1 NTLE patient had frequent independent, cont

112 immunity-related subgroup in the syndrome of MTLE-HS.

113 enrollees undergoing LITT for drug-resistant MTLE with at least 6 months of follow-up were included.

114 cell therapy alternative for drug-resistant MTLE, which is derived from a human embryonic stem cell

115 red as a treatment option for drug-resistant MTLE.

116 nical trial (NCT05135091) for drug-resistant MTLE.

117 ts with unilateral MTLE (12 left and 8 right MTLE).

118 ents had left MTLE and 15 patients had right MTLE.

119 In right MTLE patients, CTL hypometabolism was the strongest pred

120 ocampal sclerosis (five left and seven right MTLE) and 26 healthy controls were studied.

121 TLE group, 6 of 15 (P = 0.022) for the right MTLE group, and 5 of 11 (P = 0.021) for the MTS subgroup

122 eft MTLE patients (p < 0.001), whereas right MTLE patients had significantly higher rates of contrala

123 al lobe epilepsy with hippocampal sclerosis (MTLE-HS) and to elucidate the clinical and laboratory cl

124 e epilepsy related to hippocampus sclerosis (MTLE-HS) have seizures with fear, which is called ictal

125 , those with medial temporal lobe sclerosis (MTLE), and those with extrahippocampal masses (MaTLE) wh

126 These results suggest that MTLE is associated with a state specific perfusion and p

127 These results suggest that MTLE is associated with reorganisation of the limbic sys

128 However, in the MTLE hippocampus, the perivascular dystrophin was absent

129 and activity of glutamine synthetase in the MTLE hippocampus.

130 was particularly pronounced in areas of the MTLE hippocampus with astroglial proliferation, even tho

131 f interictal spikes and fast ripples in this MTLE model.

132 ortical TLE (NTLE) and nine with mesial TLE (MTLE) were immediately placed in Ringer's lactate; stear

133 epilepticus (SE), a condition that leads to MTLE.

134 sy (LTLE; n = 8), and a rat model similar to MTLE in which rats become epileptic after electrically i

135 Thirty-one unilateral MTLE patients and 30 healthy controls underwent [(11) C]

136 ients operated for drug-resistant unilateral MTLE, of whom 196 (149 with favorable outcome and 47 wit

137 rwent surgery for drug-resistant, unilateral MTLE with normal magnetic resonance imaging (MRI) or MRI

138 graphy (VEEG) in 20 patients with unilateral MTLE (12 left and 8 right MTLE).

139 12 patients with unilateral MTLE and hippocampal sclerosis (five left and seven righ

140 he criteria for the diagnosis of NTLE versus MTLE was absence versus presence of HPC sclerosis, respe

141 5-HT concentrations were higher in NTLE vs. MTLE in the Granular Cells of DG and the Pyramidal Layer

142 While MTLE is related to static structural limbic compromise,

143 uropsychological impairments associated with MTLE.

144 the Austin Health First Seizure Clinic with MTLE and normal magnetic resonance imaging (MRI) or MRI

145 entrations were higher in NTLE compared with MTLE in each HPC subparcellation [P=0.037, 0.024 and 0.0

146 y occurred in NTLE patients as compared with MTLE patients.

147 Consecutive patients diagnosed with MTLE fulfilling the MRI criteria for HS were enrolled.

148 rolled 145 patients (73 [50.3%] female) with MTLE undergoing LITT, with 77 reaching 2-year follow-up.

149 campal tissue resected from individuals with MTLE, a major neurological disorder characterized by sei

150 ients were diagnosed with NTLE and nine with MTLE.

151 ance regenerative medicine for patients with MTLE and other cognitive disorders.

152 neocortex while eight of nine patients with MTLE had high concentrations of NE (chi-square P<0.01).

153 Relatives of patients with MTLE may experience deja vu phenomena that clinically li

154 bic structural connectivity in patients with MTLE was investigated, using diffusion tensor MRI, proba

155 ntrols (age 7-79 years) and 50 patients with MTLE with normal MRI on a 1.5-Tesla scanner.

156 eficient in the hippocampus in patients with MTLE, and we postulated that this deficiency is critical

157 receptor A in 1 patient of 111 patients with MTLE-HS and none of the control subjects.

158 a large consecutive series of patients with MTLE-HS.

159 t there might be a subgroup of patients with MTLE-NMRI in which the enlarged amygdala could be relate

160 amage similar to that found in patients with MTLE.

161 hological abnormality found in patients with MTLE.

162 perfusional limbic networks in patients with MTLE.

163 ion of spontaneous seizures in patients with MTLE.

164 pocampal microelectrodes in 10 patients with MTLE.

165 In 30 subjects with MTLE and confirmed medial temporal lobe sclerosis (MTS),