ライフサイエンスコーパス: mitochondrial membrane

1 aedalus (Daed), that is located on the outer mitochondrial membrane.

2 ondria and binds to cardiolipin in the inner mitochondrial membrane.

3 ase that regulates mPTP opening in the inner mitochondrial membrane.

4 elease of a proton gradient across the inner mitochondrial membrane.

5 enables colocalization with HK1 on the outer mitochondrial membrane.

6 d the correct distribution of cristae on the mitochondrial membrane.

7 C) is a major transport protein of the inner mitochondrial membrane.

8 tion of subunits of the translocase of outer mitochondrial membrane.

9 nd is consistently associated with the inner mitochondrial membrane.

10 bind either to the plasma membrane or to the mitochondrial membrane.

11 otenoid cleavage enzyme located in the inner mitochondrial membrane.

12 ize precursor translocation across the inner mitochondrial membrane.

13 n of mislocalized TA proteins from the outer mitochondrial membrane.

14 synthesis during erythropoiesis at the outer mitochondrial membrane.

15 energize precursor passage across the inner mitochondrial membrane.

16 in 1) and its receptor proteins on the outer mitochondrial membrane.

17 As, and other signaling enzymes to the outer mitochondrial membrane.

18 that we found was associated with the inner mitochondrial membrane.

19 th the phospholipid cardiolipin in the inner mitochondrial membrane.

20 cies by modulating the fluidity of the inner mitochondrial membrane.

21 latory mechanisms on both sides of the inner mitochondrial membrane.

22 a Ca(2+)-selective ion channel in the inner mitochondrial membrane.

23 dria by ubiquitinating proteins on the outer mitochondrial membrane.

24 f the elongating mitoribosome onto the inner-mitochondrial membrane.

25 ssociated with protein crowding in the inner mitochondrial membrane.

26 duced further hyperpolarization of the inner mitochondrial membrane.

27 l-1 and Bok predominantly takes place at the mitochondrial membrane.

28 ce quinone, while pumping protons across the mitochondrial membrane.

29 reduction of O(2) by complex IV in the inner mitochondrial membrane.

30 tion modulates the biophysical properties of mitochondrial membranes.

31 olipin (CL) is the signature phospholipid of mitochondrial membranes.

32 r systems that mimic the major components of mitochondrial membranes.

33 an altered lipid composition of both MAM and mitochondrial membranes.

34 erize and heterooligomerize in bacterial and mitochondrial membranes.

35 rate of ADP or ATP translocation across the mitochondrial membranes.

36 s of dynamic interactions between the ER and mitochondrial membranes.

37 inases I and II and creatine kinase bound to mitochondrial membranes.

38 compound SS-31 (elamipretide) with model and mitochondrial membranes.

39 the surface electrostatics of both model and mitochondrial membranes.

40 SPO), an activated glial marker expressed on mitochondrial membranes.

41 correcting for variable permeabilization of mitochondrial membranes.

42 Translocase of outer mitochondrial membrane 34 (TOMM34) orchestrates heat sho

43 stem 60-kD subunit, the translocase of outer mitochondrial membrane 40-kD subunit (TOM40), the TOM20s

44 ctional receptors in MAMs vs. the rest of ER/mitochondrial membranes, a parameter called the channel

45 t an atomic model of a substrate-bound inner mitochondrial membrane AAA+ quality control protease in

46 near the mitochondrial surface, and involves mitochondrial membrane-anchored factors.

47 ial Rho (Miro) GTPases localize to the outer mitochondrial membrane and are essential machinery for t

48 icantly prevents maspin binding to the inner mitochondrial membrane and decreases cytochrome c releas

49 In addition, CO-EtOAc depolarizes the mitochondrial membrane and decreases the mitochondrial o

50 annelrhodopsin-2 fusion protein to the inner mitochondrial membrane and formation of functional catio

51 pin (CL), binds to transporters of the inner mitochondrial membrane and plays a central role in forma

52 is dependent upon MAO anchoring to the outer mitochondrial membrane and shuttling electrons through t

53 KA) and other signaling enzymes at the outer mitochondrial membrane and thereby controls mitochondria

54 the mitochondria by clustering on the outer mitochondrial membrane and thereby permeabilizing it.

55 may be responsible for release of cyt c from mitochondrial membranes and ensuing inactivation of its

56 ovel cAMP/PKA signalling domain localised at mitochondrial membranes and regulated by PDE2A2.

57 to ensure the concerted transport of the two mitochondrial membranes and the correct distribution of

58 TcAPx-CcP was found closely associated with mitochondrial membranes and, most interestingly, with th

59 ependent on the proton gradient of the inner mitochondrial membrane, and it inhibits the activity of

60 we show that MDR-1 is present in the oocyte mitochondrial membrane, and it protects the female gamet

61 zed tail-anchored (TA) proteins of the outer mitochondrial membrane are cleared by a newly identified

62 Vesicles originate from the outer mitochondrial membrane as observed by tracking Tom20 loc

63 ences in cardiolipin content between the two mitochondrial membranes, as well as dynamic fluctuations

64 Whereas outer mitochondrial membrane-associated degradation is typical

65 and proteomic analysis, we showed that human mitochondrial membrane ATP synthase subunit O is an intr

66 AKAP1-PKA "signaling islands" from the outer mitochondrial membrane augments progression toward metas

67 ondrial disorders and are believed to target mitochondrial membranes because they are enriched in the

68 At the onset of this process, the inner mitochondrial membrane becomes depolarized and permeable

69 diolipin on the concave surface of the inner mitochondrial membrane, before oxidizing the lipid and i

70 The mitochondrial membrane-bound AAA protein Bcs1 translocat

71 Mitochondrial membrane-bound Bax intensity significantly

72 subunits of succinate dehydrogenase (SDH), a mitochondrial membrane-bound enzyme complex that is invo

73 of the Golgi complex, peroxisomes, and outer mitochondrial membrane, but only detect very low steady-

74 trafficked normally to plasma, nuclear, and mitochondrial membranes, but caused reduced neurite outg

75 these proteins via its BH3 domain and to the mitochondrial membrane by a carboxyl-terminal sequence (

76 drive proton translocation across the inner mitochondrial membrane by an unresolved mechanism.

77 chain, translocates protons across the inner mitochondrial membrane by harnessing the free energy gen

78 We show that overloading of mitochondrial membrane carrier, but not matrix proteins,

79 t sites was modulated by the outer and inner mitochondrial membrane channels, voltage-dependent anion

80 hat the Mcl-1 TMD forms homooligomers in the mitochondrial membrane, competes with full-length Mcl-1

81 In turn, this change in mitochondrial membrane composition interferes with the p

82 ely, supported by direct visualization of LD-mitochondrial membrane contact sites.

83 ysosomes precedes membrane permeabilisation, mitochondrial membrane depolarisation and caspase indepe

84 o safeguard mechanisms, induced by transient mitochondrial membrane depolarization and activation of

85 ibited mitochondrial respiration and induced mitochondrial membrane depolarization and apoptosis in a

86 LL-rearranged leukemia cells did not undergo mitochondrial membrane depolarization or apoptosis despi

87 affected mitochondrial respiration, elicited mitochondrial membrane depolarization, and disrupted mit

88 n tumor cell killing, caspase activation, or mitochondrial membrane dissipation by DOX, in human canc

89 Mitochondrial membrane dynamics is a cellular rheostat t

90 PINK1 that fails to accumulate at the outer mitochondrial membrane, either by mutagenesis of this ne

91 Cardiolipin is a phospholipid of the inner mitochondrial membrane essential for the function of num

92 interacts with phospholipids, reducing inner mitochondrial membrane fluidity and the mobility of free

93 e we record AAC currents directly from inner mitochondrial membranes from various mouse tissues and i

94 es mitofusin 2, a membrane-bound mediator of mitochondrial membrane fusion and inter-organelle commun

95 tochondrial functions, including metabolism, mitochondrial membrane fusion and/or fission dynamics, a

96 lates Mitofusin, which is required for outer mitochondrial membrane fusion.

97 In this study we report that MxB is an inner mitochondrial membrane GTPase that plays an important ro

98 e in mitofusin 2 (MFN2) expression, an outer mitochondrial membrane GTPase.

99 xylic acid (TCA) cycle enzymes, which led to mitochondrial membrane hyperpolarization and increased r

100 de rT1 increases cellular ATP production via mitochondrial membrane hyperpolarization.

101 The inner mitochondrial membrane (IMM), consisting of cristae and

102 mbrane potential (DeltaPsi) across the inner mitochondrial membrane (IMM).

103 equires division of both the inner and outer mitochondrial membranes (IMM and OMM, respectively).

104 Phospholipids are vital constituents of mitochondrial membranes, impacting the plethora of funct

105 Put6 and Put7 are tethered to the inner mitochondrial membrane in a large hetero-oligomeric comp

106 the disorganization of the cristae and inner mitochondrial membrane in several cancer cells and tumor

107 al claim that proteins ejected directly from mitochondrial membranes in our study are degraded, are i

108 ptic vesicle binding) and dysfunction (e.g., mitochondrial membrane interaction).

109 The internal mitochondrial membranes invagination (cristae) complexit

110 -protein complex whose assembly in the inner mitochondrial membrane is facilitated by the scaffold fa

111 embrane protein primarily found in the outer mitochondrial membrane, is evolutionarily conserved and

112 diolipin (CL), the signature phospholipid of mitochondrial membranes, is important for cardiovascular

113 nsition pore, a nonspecific channel in inner mitochondrial membranes, is triggered by an elevated tot

114 ate a large conductance channel in the inner mitochondrial membrane known as the PTP (permeability tr

115 The outer mitochondrial membrane localization of MondoA suggests t

116 rusion by cation exchangers across the inner mitochondrial membrane may define the threshold; however

117 ine to phosphatidylethanolamine in the inner mitochondrial membrane, must undergo an autocatalytic se

118 Cardiolipin is an anionic lipid found in the mitochondrial membranes of eukaryotes ranging from unice

119 to the endoplasmic reticulum (ER), the outer mitochondrial membrane (OMM) and peroxisomes.

120 we report that mitoNEET regulates the outer-mitochondrial membrane (OMM) protein voltage-dependent a

121 ER to mitochondria and clusters at the outer mitochondrial membrane (OMM).

122 ansmembrane beta-barrels of eukaryotic outer mitochondrial membranes (OMMs) are major channels of com

123 m in yeast by re-directing Psd1 to the outer mitochondrial membrane or the endomembrane system and sh

124 Indeed, mortalin depletion increased mitochondrial membrane permeability and induced cell dea

125 brogation of necrotic cell death mediated by mitochondrial membrane permeability transition, and open

126 eased production of reactive oxygen species, mitochondrial membrane permeability, and mitochondrial m

127 tor) can commit cells to apoptosis via outer mitochondrial membrane permeabilization.

128 s of phosphatidylcholine (PC), a predominant mitochondrial membrane phospholipid, suggesting that the

129 acrophages overexpressing ACE have increased mitochondrial membrane potential (24% higher), ATP produ

130 mitochondria relies on maintaining the inner mitochondrial membrane potential (also known as DeltaPsi

131 in cytosolic calcium, prevented the loss of mitochondrial membrane potential (by 70%-80%), and resul

132 or of succinate dehydrogenase, Rhes disrupts mitochondrial membrane potential (DeltaPsi (m) ) and pro

133 The mitochondrial membrane potential (DeltaPsi(m) ) is the m

134 Additionally, 1-6 disrupt mitochondrial membrane potential (DeltaPsi(m)) and induc

135 ndrial mass, and live microscopic imaging of mitochondrial membrane potential (DeltaPsi(m)) and optic

136 owed a reduction in intact cell respiration, mitochondrial membrane potential (DeltaPsi(m)), ROS prod

137 gulate mitochondrial ETC flux and adjust the mitochondrial membrane potential (DeltaPsi(m)), to minim

138 cation its distribution is also governed by mitochondrial membrane potential (DeltaPsi(m)).

139 Mitochondrial membrane potential (DeltaPsi), a readout o

140 Mitochondrial membrane potential (DeltaPsi), cell viabil

141 egy enables a light-dependent control of the mitochondrial membrane potential (Deltapsim) and coupled

142 chondrial assessment indicated reduced inner mitochondrial membrane potential (DeltaPsim) and metabol

143 Mitochondrial membrane potential (DeltaPsim) is a global

144 , sorafenib induces rapid dissipation of the mitochondrial membrane potential (DeltaPsim) that is acc

145 smic and mitochondrial pH, redox states, and mitochondrial membrane potential (DeltaPsiM).

146 K1 import is less dependent on Tim23 than on mitochondrial membrane potential (DeltaPsim).

147 Blue/green reduced mitochondrial membrane potential (MMP) and lowered intra

148 We show that mitochondrial membrane potential (MMP) can be used to pr

149 -cell RNA sequencing (RNA-seq), we show that mitochondrial membrane potential (MMP) distinguishes qui

150 ll MFGMs treatment significantly reduced the mitochondrial membrane potential (with an order of goat

151 In both mutant and wild-type cells mitochondrial membrane potential - but not amount - vari

152 he MB-gCs, in like manner to MB, can restore mitochondrial membrane potential after depolarization wi

153 -induced mild uncoupling is shown to protect mitochondrial membrane potential against FA-induced unco

154 hanistically, AMD1 depletion induced loss of mitochondrial membrane potential and accumulation of rea

155 chondrial structural rearrangements, loss of mitochondrial membrane potential and activation of mitop

156 mitochondrial complex I that does not alter mitochondrial membrane potential and bioenergetics.

157 ive oxygen species production, and decreased mitochondrial membrane potential and depolarization thre

158 TCA cycle metabolites, as well as decreased mitochondrial membrane potential and deranged mitochondr

159 energy deficiency, together with compromised mitochondrial membrane potential and elevated oxidative

160 hed cardiomyopathy, restored cardiac myocyte mitochondrial membrane potential and flavoprotein oxidat

161 olic activity was assessed as alterations in mitochondrial membrane potential and flavoprotein oxidat

162 etime becomes progressively shorter, and the mitochondrial membrane potential and glucose uptake beco

163 Complex I inhibition resulted in lower mitochondrial membrane potential and higher cytosolic RO

164 Mat1a KO hepatocytes had reduced mitochondrial membrane potential and higher mitochondria

165 Activation of PPAR-gamma partially restored mitochondrial membrane potential and IFN-gamma productio

166 impaired mitochondrial respiration, loss of mitochondrial membrane potential and increased productio

167 tive or oxidative stress, yet exhibited high mitochondrial membrane potential and increased superoxid

168 al ROS levels but positively correlated with mitochondrial membrane potential and motility.

169 itochondrial DNA, and a similar reduction in mitochondrial membrane potential and NDUFA9 protein abun

170 se invertebrate worms significantly improved mitochondrial membrane potential and oxidative stress, w

171 drial respiration and impaired regulation of mitochondrial membrane potential and quality.

172 ochthonous lung cancer mouse model had lower mitochondrial membrane potential and reduced mitochondri

173 chondrial unfolded protein response, loss of mitochondrial membrane potential and sensitivity to mito

174 show that, while loss of Ucp2 does increase mitochondrial membrane potential and the production of r

175 DCA treatment restored cardiac mitochondrial membrane potential and tissue ATP in the r

176 of intracellular reactive oxygen species and mitochondrial membrane potential as well as microscopy (

177 ithdrawal, miR-450a overexpression decreased mitochondrial membrane potential but increased glucose u

178 cal in this quality-control process: loss of mitochondrial membrane potential causes PINK1 to accumul

179 e found that ME/CFS CD8+ T cells had reduced mitochondrial membrane potential compared with those fro

180 Because mitochondrial membrane potential controls calcium homeos

181 , we demonstrate that the distance-dependent mitochondrial membrane potential gradient exists in vivo

182 chanistically, cysteine deprivation leads to mitochondrial membrane potential hyperpolarization and l

183 e or electron transfer chain (ETC) mitigated mitochondrial membrane potential hyperpolarization, lipi

184 using PET imaging of (18)F-BnTP, we profile mitochondrial membrane potential in autochthonous mouse

185 omena were accompanied by increased synaptic mitochondrial membrane potential in both wt and Tg2576 m

186 ent of mitochondrial transport and protected mitochondrial membrane potential in cultured sensory neu

187 cal regions, (2) identifying regions of high mitochondrial membrane potential in live animals, (3) mo

188 T imaging enabled us to functionally profile mitochondrial membrane potential in live tumours.

189 alyzed the mitochondrial redox state and the mitochondrial membrane potential in mice of both sexes w

190 itochondrial function revealed a decrease in mitochondrial membrane potential in mutant Hsp27 express

191 Here we measure mitochondrial membrane potential in non-small-cell lung

192 eased mitochondrial NADH levels and restored mitochondrial membrane potential in p62-deficient cells.

193 also found that PA stimulation decreased the mitochondrial membrane potential in podocytes and induce

194 While the pharmaceutical agents decreased mitochondrial membrane potential in porcine fetal fibrob

195 able to record neuronal Ca(2+) responses and mitochondrial membrane potential in these nerve tissues.

196 cellular ROS and alleviated the depletion of mitochondrial membrane potential in vitro.

197 Loss of mitochondrial membrane potential is accompanied by reduc

198 The JC-1 staining shows the mitochondrial membrane potential is decreased after the

199 on of COX6B2 attenuates OXPHOS and collapses mitochondrial membrane potential leading to cell death o

200 mPTP opening decreases the mitochondrial membrane potential leading to the activati

201 The model reveals that reduction in the mitochondrial membrane potential leads to significant de

202 andard chemotherapeutics sensitized cells to mitochondrial membrane potential loss and apoptosis.

203 asmic volume control, absence of significant mitochondrial membrane potential loss, and lack of activ

204 protein linked to endosomal trafficking and mitochondrial membrane potential maintenance.

205 ds: Cardiac uptake and response to decreased mitochondrial membrane potential of (18)F-MitoPhos and (

206 Here, we monitor mitochondrial membrane potential of single lymphocytic l

207 Under normal culture conditions, the mitochondrial membrane potential of the probands' fibrob

208 ROS scavenging assays, wound healing assays, mitochondrial membrane potential readings, corneal fluor

209 Previously, we reported that mitochondrial membrane potential regulates STING-depende

210 change in NAD(+)/NADH is caused by increased mitochondrial membrane potential that impairs mitochondr

211 Treated lymphoma cells exhibited a reduced mitochondrial membrane potential that resulted in an irr

212 Mitochondrial membrane potential was assessed with JC-1

213 ced ototoxicity by increasing ATP levels and mitochondrial membrane potential was confirmed.

214 min treated animals maintained a more normal mitochondrial membrane potential while those isolated fr

215 n, accumulation of complex IV, and increased mitochondrial membrane potential with no change in mitoc

216 ablish a quantitative model to associate the mitochondrial membrane potential with the key pharmacoki

217 s with high concentrations of drug decreased mitochondrial membrane potential, a phenotype that was s

218 in mitochondrial respiration, impairment in mitochondrial membrane potential, aberrant mitochondrial

219 ion identified chemical probes that regulate mitochondrial membrane potential, adenosine 5'-triphosph

220 nt mitochondrial fragmentation, reduction in mitochondrial membrane potential, and a significant loss

221 ion, altered mitochondrial motility, reduced mitochondrial membrane potential, and diminished mitocho

222 essed mitochondrial gene expression, reduced mitochondrial membrane potential, and diminished oxygen

223 vities, respiratory responses, redox charge, mitochondrial membrane potential, and electron leak, we

224 Ca(2+) flux, apoptosis, mitochondrial membrane potential, and expression of surf

225 ng dysregulates iron metabolism, depolarizes mitochondrial membrane potential, and induces cell death

226 is, decreasing PI3K and Akt phosphorylation, mitochondrial membrane potential, and modulating G1-S tr

227 the increase in ROS production, decrease of mitochondrial membrane potential, and proteasome activit

228 mitochondrial variables such as respiration, mitochondrial membrane potential, buffer calcium, and su

229 ed mitochondrial defects including collapsed mitochondrial membrane potential, dissipated ATP product

230 the cell cycle at S phase, depolarization of mitochondrial membrane potential, down-regulation of Bcl

231 This rupture occurred after loss of mitochondrial membrane potential, followed by entry of b

232 ic overexpression of UQCRH in KMRC2 restored mitochondrial membrane potential, increased oxygen consu

233 hibited a lower rate of O(2) uptake, loss of mitochondrial membrane potential, increased reactive oxy

234 that is, they damage nuclear DNA, reduce the mitochondrial membrane potential, induce the epigenetic

235 take was TRPV1-dependent, dissipation of the mitochondrial membrane potential, inhibition of the mito

236 Mathematical formulations of mitochondrial membrane potential, mitochondrial Ca(2+) c

237 e oxygen species (ROS) activities, increased mitochondrial membrane potential, reduced calcium levels

238 ranslational modifications: respiration, the mitochondrial membrane potential, ROS, and apoptosis.

239 ssed produces a stable protein which impacts mitochondrial membrane potential, suggesting a potential

240 derived VCP mutant fibroblasts exhibit lower mitochondrial membrane potential, uncoupled respiration,

241 estingly, Abeta-CEL16&28 had depolarized the mitochondrial membrane potential, whereas Abeta-CEL16 ha

242 mitochondrial oxidative stress and decreased mitochondrial membrane potential, with higher mtDNA rele

243 tive imaging, bioenergetics measurements and mitochondrial membrane potential- and redox-sensitive dy

244 +) is reduced back to NADPH by activation of mitochondrial membrane potential-dependent nicotinamide

245 ondrial Ca(2+) uptake, without affecting the mitochondrial membrane potential.

246 al reactive oxygen species and protected the mitochondrial membrane potential.

247 rboxylic acid cycle (TCA), and have abnormal mitochondrial membrane potential.

248 oxidative stress and disturbances caused to mitochondrial membrane potential.

249 he parasite by decreasing ATP production and mitochondrial membrane potential.

250 led to decreased ATP synthesis and defective mitochondrial membrane potential.

251 ression and, consistent with this, decreased mitochondrial membrane potential.

252 l of energy metabolism, ultimately impacting mitochondrial membrane potential.

253 tive oxygen species or depolarization of the mitochondrial membrane potential.

254 olism, mitochondrial biogenesis and restores mitochondrial membrane potential.

255 ontributing toward the maintenance of normal mitochondrial membrane potential.

256 itosis from the single-cell time-dynamics of mitochondrial membrane potential.

257 metabolic remodeling deficits and decreased mitochondrial membrane potential; a subset had increased

258 ase, which we propose maintains intermediate mitochondrial membrane potentials under physiologic cond

259 2-fold ROS generation, and a 50% decrease in mitochondrial membrane potentials with respect to equiva

260 mice had similar respiratory activities and mitochondrial membrane potentials.

261 lity, reactive oxygen species generation and mitochondrial membrane potentials.

262 ific targeting of Arf6 to plasma membrane or mitochondrial membranes promotes recruitment and colocal

263 ndrial Ca(2+) uptake is mediated by an inner mitochondrial membrane protein called the mitochondrial

264 Succinate dehydrogenase (SDH) is an inner mitochondrial membrane protein complex that links the Kr

265 MitoNEET is an outer mitochondrial membrane protein essential for sensing and

266 The outer mitochondrial membrane protein mitochondrial Rho GTPase

267 Mitochondrial membrane protein p32 can block mtDNA synth

268 Here, we identify the inner mitochondrial membrane protein, prohibitin 2 (PHB2), as

269 ) myoblasts, and a significant enrichment of mitochondrial membrane proteins among proteins showing a

270 ctional and structural requirement of CL for mitochondrial membrane proteins has been studied in vitr

271 Mitochondrial density and the abundance of mitochondrial membrane proteins in skeletal muscle incre

272 829) describe mass spectrometry on mitochondrial membrane proteins ionized directly from th

273 teins into soluble, peripheral, and integral mitochondrial membrane proteins, and the assignment of 8

274 , succinyl-CoA was used to succinylate liver mitochondrial membrane proteins.

275 ked to Fragile-X syndrome elevates the inner mitochondrial membrane proton leak, leading to increased

276 we show that GSDME-N also permeabilizes the mitochondrial membrane, releasing cytochrome c and activ

277 cyt c autoinactivation via its release from mitochondrial membranes remain largely unknown.

278 D multisubunit channel residing in the inner mitochondrial membrane required for mitochondrial Ca(2+)

279 about how cardiolipin concentration affects mitochondrial membrane structure and dynamics.

280 The ETC is organized into inner mitochondrial membrane supercomplexes that promote subst

281 Both mitochondrial membranes surround the hydrophilic interme

282 ciated X apoptosis regulator (BAX), an outer mitochondrial membrane-targeting pro-apoptotic protein,

283 ndently of one another to sites on the inner mitochondrial membrane that are in proximity to contact

284 ghtly controlled Ca(2+) channel of the inner mitochondrial membrane that regulates cellular metabolis

285 ctivation of signaling pathways in the inner mitochondrial membrane, thereby modulating its function

286 DP prevented astrocyte loss by targeting the mitochondrial membrane to prevent the hyperoxia-induced

287 tes a hetero-oligomeric complex on the inner mitochondrial membranes to maintain crista structure.

288 how they associate with protein complexes in mitochondrial membranes to support bioenergetics and mai

289 The translocase of outer mitochondrial membrane (TOMM) complex is the entry gate

290 n particular, we identify a network of inner mitochondrial membrane transporters as a hub required fo

291 The mitochondrial membrane undergoes extreme remodeling duri

292 s targeted to protein complexes on the inner mitochondrial membrane via affinity for cardiolipin to p

293 drial morphology, and Ca(2+) permeability of mitochondrial membrane was investigated in the presence

294 l-CoA synthetase ACSL1, and localizes to the mitochondrial membrane where it likely activates long ch

295 ukaryotic AAA+ ATPase localized to the outer mitochondrial membrane, where it is thought to extract m

296 olipin (CL) is the signature phospholipid of mitochondrial membranes, where it is synthesized locally

297 ut this form also plays a structural role on mitochondrial membranes, which is independent of phospha

298 ide a 30- to 90-nm invagination of the outer mitochondrial membrane, whose necked aperture to the cyt

299 al E3 ubiquitin ligase anchored in the outer mitochondrial membrane with its RING finger domain facin

300 Mst1/2 from the cytosol to the phagosomal or mitochondrial membrane, with ROS subsequently activating