ライフサイエンスコーパス: brain inflammation

1 didate for the treatment of HIV-1-associated brain inflammation.

2 CNS glial cell type, also can contribute to brain inflammation.

3 opic effects of type 1 interferons in taming brain inflammation.

4 analysis in real time after triggering focal brain inflammation.

5 's disease (AD) is associated with prominent brain inflammation.

6 ion and in aging-associated microgliosis and brain inflammation.

7 ls including systemic inflammation and local brain inflammation.

8 of Plasmodium falciparum infection caused by brain inflammation.

9 ells lacking TCF1 and LEF1 fails to suppress brain inflammation.

10 pagation of tau in humans is associated with brain inflammation.

11 y gene expression and experimentally induced brain inflammation.

12 ferroptosis-induced cell death, and reduces brain inflammation.

13 lucidate the mechanisms of ChP regulation of brain inflammation.

14 glia-astrocyte positive feedback loop during brain inflammation.

15 nic (Tg4510) mouse model exhibiting elevated brain inflammation.

16 lar miRNA and TLR7 sensing in sepsis-induced brain inflammation.

17 egnancy on offspring behavioral outcomes and brain inflammation.

18 plasma EVs may be involved in posttraumatic brain inflammation.

19 e that neuronal STAT3 may directly influence brain inflammation.

20 ic seizures, which is preceded by persistent brain inflammation.

21 Q311X(A) mice with slow progression and mild brain inflammation.

22 trocyte-mediated microglia activation during brain inflammation.

23 rocytes and microglia play critical roles in brain inflammation.

24 ibit elevated expression of immune genes and brain inflammation.

25 e is temporally correlated with the onset of brain inflammation.

26 prevented PTB, neonatal mortality, and fetal brain inflammation.

27 el object recognition test, but not signs of brain inflammation.

28 ed the reparative capacity of NSCs following brain inflammation.

29 toxic amyloid-beta as well as regulation of brain inflammation.

30 on cognition, depressive-like behavior, and brain inflammation.

31 oimmune encephalomyelitis onset and enhanced brain inflammation.

32 (-/-) mice, which was accompanied by reduced brain inflammation.

33 ctively contributes to neuronal death during brain inflammation.

34 laques in APP/PS1 mice, as well as increased brain inflammation.

35 ight induce cerebral blood flow responses to brain inflammation.

36 insight into new therapeutic strategies for brain inflammation.

37 id MVs as a marker and therapeutic target of brain inflammation.

38 ers and is stable for months without causing brain inflammation.

39 f PGE2 EP4 receptor signaling in suppressing brain inflammation.

40 ir characteristic amoeboid morphology during brain inflammation.

41 We report here detection of active brain inflammation 3 months after successful inhibition

42 Such focal brain inflammation aggravates secondary brain injury by

43 We examined these samples for systemic and brain inflammation; amyloid-beta peptide (Abeta) and Ser

44 ry gene expression in a mouse model of acute brain inflammation and a mouse model of Alzheimer's dise

45 SPO PET as a potential biomarker to evaluate brain inflammation and anti-inflammatory therapies, a be

46 brain demyelination significantly attenuates brain inflammation and astrocyte reactivity.

47 , the activation of mast cell contributes to brain inflammation and brain injury.

48 of inflammatory cells, which can exacerbate brain inflammation and contribute to poor outcome.

49 (WNV) is a vectorborne pathogen that induces brain inflammation and death.

50 sensitive systems for detection of mammalian brain inflammation and disease.

51 Sustained brain inflammation and hyperactivation of inflammasome c

52 s a critical role for CD73 as a modulator of brain inflammation and immune function.

53 oited to develop therapies that can mitigate brain inflammation and improve the outcome after TBI.

54 widely recognized to play critical roles in brain inflammation and injury, although the responsible

55 ality and morbidity that are associated with brain inflammation and injury, but currently the only ef

56 a trigger astrocyte reactivity, resulting in brain inflammation and massive amyloid and tau pathologi

57 ficient naive CD4(+) T cells failed to cause brain inflammation and neurobehavioral disorders in Rag1

58 eferentially into the brain, contributing to brain inflammation and neurobehavioral disorders, thereb

59 their sensor Toll-like receptor 7 (TLR7) in brain inflammation and neurological dysfunction.

60 peripheral inflammation can exacerbate local brain inflammation and neuronal death.

61 copy (MRS) can be used to monitor changes in brain inflammation and neuronal integrity associated wit

62 HypoMg-induced brain inflammation and oxidative stress were suppressed

63 -LOX mice was associated with an increase in brain inflammation and parasite burden.

64 caspase-1/11 deficient mice show deficits in brain inflammation and parasite control.

65 ain, as potential gatekeepers for modulating brain inflammation and pathology after stroke.

66 nds provides a unique tool to assess diffuse brain inflammation and perilesional activity in progress

67 influx may be an effective therapy to reduce brain inflammation and promote myelin recovery in demyel

68 nti-inflammatory drugs (NSAIDs) could reduce brain inflammation and that NFP is an effective anti-inf

69 Evolving evidence suggests that brain inflammation and the buildup of proinflammatory cy

70 macrophages (Mi/MPhi) critically influences brain inflammation and the outcome after traumatic brain

71 These factors, in turn, promote liver and brain inflammation and the progression of liver fibrosis

72 e Sclerosis (MS), CVR may be diminished with brain inflammation and this may contribute to neurodegen

73 ere investigated on epileptiform discharges, brain inflammation, and BBB damage.

74 insulin resistance, brain oxidative stress, brain inflammation, and brain apoptosis, resulting in th

75 FB results in increased CSF cytokine levels, brain inflammation, and downregulation of the brain gluc

76 ides the most compelling evidence to date of brain inflammation, and more specifically microglial act

77 ssential in tempering microglial activation, brain inflammation, and neurodegeneration, with critical

78 breakdown of the blood-brain barrier (BBB), brain inflammation, and neurological dysfunction.

79 e to infection, prevented the development of brain inflammation, and protected mice from paralysis an

80 itment and their mechanisms of action during brain inflammation are not well understood.

81 mmation has not thus far clearly established brain inflammation as an early pathological event.

82 pendently, and significantly, attenuated the brain inflammation as indicated by the decreased density

83 hocyanidin B2 was also a potent inhibitor of brain inflammation as shown by reduction in astrocytosis

84 vivo, in a mouse model of EcoHIV-associated brain inflammation, as well as characterize its pharmaco

85 ng and attenuated lung injury and indices of brain inflammation at 10 days.

86 viated proinflammatory Mi/MPhi responses and brain inflammation burden after TBI.

87 tration of nitro-aspirin also attenuated the brain inflammation, but to a much lesser degree than NFP

88 te this issue, we established a new model of brain inflammation by injecting the Toll-like receptor 3

89 report in vivo detection of VCAM-1 in acute brain inflammation, by magnetic resonance imaging in a m

90 that systemic inflammation along with local brain inflammation can play a significant role in Alzhei

91 We hypothesize that acute brain inflammation caused by neonatal infection reduces

92 Brain inflammation, changes in nicotinic receptor expres

93 mer's disease (AD) is found to have striking brain inflammation characterized by clusters of reactive

94 , compromised neuronal integrity, and robust brain inflammation characterized by extensive gliosis an

95 Encephalitis is parenchymal brain inflammation, commonly due to herpes simplex virus

96 Brain inflammation contributes to the duration and recur

97 ink between cutaneous, systemic and possible brain inflammation could at least in part be driven by t

98 No brain inflammation, demyelination or right-turning behav

99 e subunit changes associated with persistent brain inflammation due to HIV-1; (2) determining whether

100 geted PET is a reliable tool for identifying brain inflammation during epileptogenesis.

101 liferating microglia as important drivers of brain inflammation during infection.

102 atory hypothesis is a paucity of evidence of brain inflammation during MDE.

103 ortem and in vivo imaging studies have shown brain inflammation early in these conditions, proportion

104 confirmed that the HHQK peptide reduces rat brain inflammation elicited after infusion of Abeta pept

105 Brain inflammation (encephalitis) in response to viral i

106 ts a systematic review of the data regarding brain inflammation evaluating microglia, astrocytes, cyt

107 nhibit NF-kappaB activation induced in acute brain inflammation even in the absence of MC1R.

108 er animals less sensitive to tissue loss and brain inflammation following experimental brain injury.

109 2019) reports that DAMP-induced sterile brain inflammation from stroke is associated with sympat

110 cific receptor Mrgprb2 regulates post-stroke brain inflammation from the meninges.

111 Therefore, neuronal loss during brain inflammation has always been assumed to be due to

112 tly, an intriguing link between TMEM106B and brain inflammation has been discovered, but how TMEM106B

113 hanism of this age-related susceptibility to brain inflammation has yet to be defined, but animal mod

114 BHB has been shown to modulate systemic and brain inflammation; however, its direct effects on micro

115 lates HSC lineage development to curb distal brain inflammation, implicating the bone marrow as a uni

116 We studied brain inflammation in 25 patients with early-onset amnes

117 Accurately measuring brain inflammation in Alzheimer's disease (AD) is crucia

118 Brain inflammation in animal models of these diseases is

119 Seizures initiate brain inflammation in glia and promote BBB damage that i

120 ion together with histological assessment of brain inflammation in infected animals revealed that cle

121 We applied 11C-ER176 to detect brain inflammation in mild cognitive impairment (MCI) ca

122 ainst the IL-2Ralpha chain, strongly reduces brain inflammation in multiple sclerosis patients.

123 d monoclonal antibody against CD25, inhibits brain inflammation in multiple sclerosis, we observed th

124 eceptors by prostaglandin E2 (PGE2) promotes brain inflammation in neurodegenerative diseases, but th

125 Astrocytes contribute to brain inflammation in neurological disorders but the mol

126 he present study, we used an animal model of brain inflammation in order to study a possible mechanis

127 Brain inflammation in patients with HE was evaluated by

128 n Ab against the IL-2R alpha-chain, inhibits brain inflammation in patients with multiple sclerosis,

129 Finally, PET can detect widespread brain inflammation in PD.

130 ammation, we investigated the development of brain inflammation in the T cell transfer model of chron

131 ic differences in cortical tissue sparing or brain inflammation in this experiment.

132 derived macrophage infiltration and enhanced brain inflammation in vivo.

133 systemic inflammation, in addition to local brain inflammation, in Alzheimer's disease (AD) progress

134 ave shown that TNF-alpha plays a key role in brain inflammation, including recruitment of inflammator

135 We investigated whether seizures induce brain inflammation independently on extracerebral factor

136 flammatory cytokines, in experimental murine brain inflammation induced by lipopolysaccharide.

137 Using a mouse model of acute brain inflammation induced by local tumor necrosis facto

138 al cortex attenuated microglia activation in brain inflammation induced by systemic injection of lipo

139 g the CXC chemokine activity associated with brain inflammation inhibits neutrophil-mediated blood-br

140 Brain inflammation is considered a crucial etiopathogene

141 Brain inflammation is increasingly recognized as a criti

142 mented, how MIA in utero leads to persistent brain inflammation is not well understood.

143 Identifying brain inflammation is possible with the recent advance i

144 s effective at suppressing both systemic and brain inflammation, it may represent a novel therapeutic

145 The development of brain inflammation largely contributes to neonatal brain

146 illing efficiency, but also long-term active brain inflammation, loss of myelin fibers and persistent

147 ing the liver and spleen, nor does it affect brain inflammation markers.

148 results suggest that persistent and diffuse brain inflammation may contribute to cognitive impairmen

149 Global brain inflammation might continuously shape the evolving

150 hionine provides further insights into heart-brain inflammation networking.

151 thionine provides further insight into heart-brain inflammation networking.

152 ven therapeutic efficacy in animal models of brain inflammation, neurodegenerative disorders and stro

153 ts into the roles of PGN as a determinant of brain inflammation, notably in multiple sclerosis (MS) a

154 stopped, the immune response was generated, brain inflammation occurred, virus was cleared, and mice

155 on, production of viral proteins, associated brain inflammation or in certain instances, antiretrovir

156 There were no differences in the amounts of brain inflammation or peak virus replication; however, I

157 DDs directly by inducing placental and fetal brain inflammation, or indirectly through affecting mate

158 ction of monocyte chemoattractant protein 1, brain inflammation, or mortality could not be accounted

159 n mediate interaction between peripheral and brain inflammation, our findings pinpoint the choroid pl

160 celerated recovery from weight loss, reduced brain inflammation, prevention of blood-brain barrier op

161 mokine family and that it may play a role in brain inflammation processes.

162 IB/SHIP1 pathway, resulting in a decrease of brain inflammation, protection of the blood-brain-barrie

163 This hallmark of brain inflammation remains unexplained.

164 FDA-approved anti-inflammatory drugs reduced brain inflammation, restored LTP and long-term memory, a

165 mplement activation is implicated in driving brain inflammation, self-cell damage and progression of

166 Brain inflammation tended to be higher in LCR rats than

167 Wild-type (wt) MAV-1 causes less brain inflammation than an early region 3 (E3) null viru

168 astrocyte reactivity and astrocyte-mediated brain inflammation that is commonly observed in many neu

169 eonates at postnatal day 3 (P3) caused acute brain inflammation that was resolved within 72 h.

170 bservations in terms of BBB permeability and brain inflammation underline age susceptibility.

171 al cells (BECs) in fueling type I IFN-driven brain inflammation was demonstrated in brain endothelial

172 Seizure-induced brain inflammation was evaluated by quantitative immunoh

173 Brain inflammation was measured by TaqMan RT-PCR amplifi

174 Brain inflammation was modeled by intravenous lipopolysa

175 /-) mice, lethality was markedly delayed and brain inflammation was significantly reduced, as demonst

176 Brain inflammation was suggested by MRS.

177 of global lipopolysaccharide (LPS)-mediated brain inflammation was used to induce global vascular ce

178 went dynamic PK PET for conditions involving brain inflammation were studied.

179 Autoimmune encephalitis (AE) is a form of brain inflammation where pathogenic autoantibodies bind

180 ilepsy characterized pathologically by focal brain inflammation with large numbers of infiltrating T

181 Brain inflammation, with an increased density of microgl

182 governing the emergence of so-called global brain inflammation would facilitate modulation of this i