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1 ls that promoted optimal GC polarization and cholesterol biosynthesis.
2 enzyme A that can be used for fatty acid and cholesterol biosynthesis.
3 4 methyl groups in one of the later steps of cholesterol biosynthesis.
4 EBP-2, a master transcriptional activator of cholesterol biosynthesis.
5 but can be modulated by agents that disrupt cholesterol biosynthesis.
6 including unexpected upregulation of retinal cholesterol biosynthesis.
7 l absorption, cholesterol precursors reflect cholesterol biosynthesis.
8 sion as well as the more commonly considered cholesterol biosynthesis.
9 olesterol to cholesterol in the last step of cholesterol biosynthesis.
10 P-1c and SREBP-2 and genes of fatty acid and cholesterol biosynthesis.
11 li-Opitz syndrome (SLOS) caused by defective cholesterol biosynthesis.
12 agonist and compactin, a statin inhibitor of cholesterol biosynthesis.
13 ns, are essential for feedback inhibition of cholesterol biosynthesis.
14 ed to lower cholesterol levels by inhibiting cholesterol biosynthesis.
15 plays an important role in the regulation of cholesterol biosynthesis.
16 E caused a pronounced inhibition of de novo cholesterol biosynthesis.
17 -CoA reductase that are potent regulators of cholesterol biosynthesis.
18 e CE but an approximately 3-fold decrease in cholesterol biosynthesis.
19 lesterol, indicative of a marked decrease in cholesterol biosynthesis.
20 glutaryl CoA reductase, leading to decreased cholesterol biosynthesis.
21 own-regulates lipid metabolism, particularly cholesterol biosynthesis.
22 cytoskeleton regulation, and fatty acid and cholesterol biosynthesis.
23 omplementing the statin drugs, which inhibit cholesterol biosynthesis.
24 e encodes a sterol dehydrogenase involved in cholesterol biosynthesis.
25 CR7), an enzyme catalyzing the final step of cholesterol biosynthesis.
26 assumed to stem from their ability to reduce cholesterol biosynthesis.
27 on of mevalonate, a rate-controlling step in cholesterol biosynthesis.
28 ase (HMGCoAR) is required for isoprenoid and cholesterol biosynthesis.
29 s having high cholesterol absorption and low cholesterol biosynthesis.
30 represents the first committed step in human cholesterol biosynthesis.
31 CoA) reductase, the rate-limiting enzyme for cholesterol biosynthesis.
32 osphatidylcholine that influences macrophage cholesterol biosynthesis.
33 ve inhibitors of the rate-limiting enzyme in cholesterol biosynthesis.
34 of cholesterol because of the inhibition of cholesterol biosynthesis.
35 rred with a similar potency as inhibition of cholesterol biosynthesis.
36 al of two C-4 methyl groups in post-squalene cholesterol biosynthesis.
37 mes caused by defects in the final stages of cholesterol biosynthesis.
38 , which catalyzes a rate-controlling step in cholesterol biosynthesis.
39 unable to suppress LDL receptor activity and cholesterol biosynthesis.
40 e reactions are the first committed steps in cholesterol biosynthesis.
41 ctase (HMGR) catalyzes the committed step in cholesterol biosynthesis.
42 ents, including peroxisomes, are involved in cholesterol biosynthesis.
43 plays an essential role in the regulation of cholesterol biosynthesis.
44 that functions in one of the later steps of cholesterol biosynthesis.
45 ffected Bpa mice support a role for Nsdhl in cholesterol biosynthesis.
46 described end-product feedback regulation of cholesterol biosynthesis.
47 ple malformation syndrome due to a defect in cholesterol biosynthesis.
48 olesterol could be slowed by inhibiting late cholesterol biosynthesis.
49 nonsteroidal inhibitors of MDR also inhibit cholesterol biosynthesis.
50 1.14.99.7) is a key rate-limiting enzyme in cholesterol biosynthesis.
51 ts novel components for modules, such as for cholesterol biosynthesis.
52 n of PD-L1, and enrichment for signatures of cholesterol biosynthesis.
53 alene to 2,3(S)-oxidosqualene, a key step in cholesterol biosynthesis.
54 p < 0.05 for each), which suggests increased cholesterol biosynthesis.
55 tumor suppressor gene through inhibition of cholesterol biosynthesis.
56 ion (but not lipofuscin) via upregulation of cholesterol biosynthesis.
57 y secondary to inappropriate derepression of cholesterol biosynthesis.
58 l proliferation, leukocyte extravasation and cholesterol biosynthesis.
59 nol; and (iii) weak cerebellar regulation of cholesterol biosynthesis.
60 rol efflux, but also simultaneously inhibits cholesterol biosynthesis.
61 y regulated by sterol molecules derived from cholesterol biosynthesis.
62 hway in WD-fed rats was the 'Superpathway of cholesterol biosynthesis' (10/29 genes regulated, p = 1.
63 ing region of the rate controlling enzyme of cholesterol biosynthesis, 3-hydroxy-3-methylglutaryl coe
65 egulated genes, 19 genes are associated with cholesterol biosynthesis and 5 genes specify aspects of
66 signatures of cholesterol suggest increased cholesterol biosynthesis and accumulation in the materna
67 affects the expression of genes involved in cholesterol biosynthesis and alters the cholesterol leve
68 nhibitors that are known to inhibit cellular cholesterol biosynthesis and are clinically prescribed t
69 lular cholesterol accumulation by inhibiting cholesterol biosynthesis and by promoting cholesterol ex
70 causes both repression of genes controlling cholesterol biosynthesis and cellular uptake and inducti
71 esults demonstrate that MDV hijacks cellular cholesterol biosynthesis and cholesterol trafficking to
72 pression of many genes involved in lipid and cholesterol biosynthesis and decreased levels of cholest
73 pension derivatives highlighted switching in cholesterol biosynthesis and expression of five key gene
74 c mechanism of EBP-mediated isomerization in cholesterol biosynthesis and how this protein may act as
75 The mechanism by which genes involved in cholesterol biosynthesis and import are preferentially u
76 PR-Cas9-based genetic screens and identified cholesterol biosynthesis and iron uptake as essential me
77 e (SM) is the second rate-limiting enzyme in cholesterol biosynthesis and is regulated both transcrip
79 with wild-type) include lipid, steroid, and cholesterol biosynthesis and metabolism; nucleosome and
81 argeting HMGCR activity primarily influences cholesterol biosynthesis and prenylation of signaling pr
82 ieved in humans by simultaneously inhibiting cholesterol biosynthesis and promoting ABCG5/ABCG8-media
83 rization indicate deregulated fatty acid and cholesterol biosynthesis and reduced liver X receptor ac
84 inhibits the expression of genes involved in cholesterol biosynthesis and reduces plasma cholesterol
85 t StARD3 overexpression results in increased cholesterol biosynthesis and Src kinase activity in brea
86 and dampens the activity of a key enzyme in cholesterol biosynthesis and that a receptor deficiency
87 esterification does not cause inhibition of cholesterol biosynthesis and that inhibition of choleste
88 ce of environmental compounds that interrupt cholesterol biosynthesis and that methodologically hiPSC
89 ctase domain of LBR plays a critical role in cholesterol biosynthesis and that this process is essent
90 ata reveal a reciprocal relationship between cholesterol biosynthesis and the clearance of mutant neu
91 mevalonate (MEV) cascade is responsible for cholesterol biosynthesis and the formation of the interm
92 terone-sensitive pathway is involved in both cholesterol biosynthesis and the processing of LDL-deriv
93 enzymatic function in steroid biosynthesis, cholesterol biosynthesis and thyroid hormone metabolic p
95 replication and mevalonic acid, sterol, and cholesterol biosynthesis and trafficking/redistribution.
96 Our data also demonstrate that changes in cholesterol biosynthesis and uptake are only observed in
97 vestigated the effects of HIV-1 infection on cholesterol biosynthesis and uptake using microarrays.
100 ojection neurons in vivo essentially require cholesterol biosynthesis and which cell types support ne
101 ering fatty acid composition and restricting cholesterol biosynthesis and, thus, ligand availability
102 e growth, protein transport, RNA processing, cholesterol biosynthesis, and apoptosis via death domain
103 that genes associated with lipid metabolism, cholesterol biosynthesis, and circadian rhythm were most
104 relationships between membrane microdomains, cholesterol biosynthesis, and endothelial function will
106 tion at early times, and lipid biosynthesis, cholesterol biosynthesis, and mediators of immune respon
107 ) inhibits cellular proliferation, decreases cholesterol biosynthesis, and triggers apoptosis, at lea
108 parable to those previously shown to inhibit cholesterol biosynthesis, and, can be derived from chole
109 ges in terms related to P450s, transporters, cholesterol biosynthesis, and, unexpectedly, antigen pre
113 because they have a compensatory increase in cholesterol biosynthesis as a result of increased choles
114 ene epoxidase, an oxygen-requiring enzyme in cholesterol biosynthesis, as a driver of dysregulated me
115 ns and was concomitant with reduced UPR- and cholesterol biosynthesis-associated gene expression.
116 l enhanced expression of the GTPase RAC1 and cholesterol-biosynthesis-associated genes together with
117 nuclidine series previously known to inhibit cholesterol biosynthesis at the squalene synthase step,
118 asmic reticulum membrane protein involved in cholesterol biosynthesis, autophagy, oligodendrocyte for
119 cell metabolism, particularly glycolysis and cholesterol biosynthesis before the preovulatory surge o
120 oenzyme A reductase, statins not only reduce cholesterol biosynthesis but also decrease the formation
121 known for catalysing a rate-limiting step in cholesterol biosynthesis, but it also participates in th
122 he enzymatic role of DHCR7 as a reductase in cholesterol biosynthesis, but may also involve defects i
125 liver X receptor alpha (LXRalpha), regulates cholesterol biosynthesis by directly silencing the expre
126 r, we demonstrate that progesterone inhibits cholesterol biosynthesis by interfering with MDR activit
127 At 20 micromol/l, troglitazone inhibited cholesterol biosynthesis by more than 80%, resulting in
128 port prevents cholesterol esterification and cholesterol biosynthesis by preventing sterol substrates
129 indicates that oocytes regulate cumulus cell cholesterol biosynthesis by promoting the expression of
130 r supports the conclusion that inhibition of cholesterol biosynthesis by troglitazone is unlikely to
131 r, which encodes the rate-limiting enzyme of cholesterol biosynthesis called 3-hydroxy-3-methyl-gluta
132 ent-binding protein 2, a master regulator in cholesterol biosynthesis, can be activated in a noncanon
135 t, we demonstrate that progesterone inhibits cholesterol biosynthesis, causing the accumulation of a
137 -Opitz syndrome (SLOS) is an inborn error of cholesterol biosynthesis characterized by diminished cho
138 arch that demonstrate chemical inhibition of cholesterol biosynthesis compromises neurodevelopment.
139 oupled with oral and selective inhibition of cholesterol biosynthesis derived from OSC inhibition (ra
140 lesterol biosynthesis and that inhibition of cholesterol biosynthesis does not cause inhibition of ch
141 ive reactions such as fatty acid elongation, cholesterol biosynthesis, drug metabolism, and methemogl
142 sociated with CDP, including peroxisomal and cholesterol biosynthesis dysfunction and other inborn er
143 ologically or genetically induced defects in cholesterol biosynthesis, embryonic cholesterol transpor
144 27-hydroxycholesterol, known suppressors of cholesterol biosynthesis, enhance SF-1-dependent transcr
145 ions involved in de novo lipogenesis, TG and cholesterol biosynthesis, FA elongation and oxidation, l
147 e best inhibition (following oral dosing) of cholesterol biosynthesis from mevalonate (ED50 = 2.7 mg/
150 In that context, Tcf7l2 directly activates cholesterol biosynthesis genes and cholesterol supplemen
151 not rapamycin, significantly down-regulates cholesterol biosynthesis genes in a 4E-BP1-dependent man
152 ing revealed a coordinated downregulation of cholesterol biosynthesis genes in LG2KO mice that was as
153 tis is associated with altered expression of cholesterol biosynthesis genes in synovial biopsies of p
156 nregulated genes specifically predicted that cholesterol biosynthesis genes would be affected by miR-
158 rogram, dominating SREBP2 via its binding to cholesterol-biosynthesis genes and its facilitation of t
159 d stress responses, as well as downregulated cholesterol biosynthesis, glycolysis, and interleukin IL
160 n of cholesterol precursors due to defective cholesterol biosynthesis has been reported to result in
161 rs involving enzyme defects in post-squalene cholesterol biosynthesis have been identified-desmostero
162 Veratrum alkaloids and distal inhibitors of cholesterol biosynthesis have been studied for more than
164 showed a much stronger inhibition of overall cholesterol biosynthesis (IC(50) 2.3 nM) than BM 15.766
165 ng vesicle trafficking, DNA modification and cholesterol biosynthesis, identifying these as potential
168 n of the unfolded protein response (UPR) and cholesterol biosynthesis in adult rat sensory neurons.
169 ue to CHO cells; progesterone also inhibited cholesterol biosynthesis in all human cell lines tested.
171 y, we examined the effect of troglitazone on cholesterol biosynthesis in cultured Chinese hamster ova
172 ctors, particularly, BMP15 and GDF9, promote cholesterol biosynthesis in cumulus cells, probably as c
173 chemical effects was conducted by assessing cholesterol biosynthesis in human induced pluripotent st
175 ces cerevisiae ergosterol biosynthesis, like cholesterol biosynthesis in mammals, is regulated at the
181 back upregulation of genes in the pathway of cholesterol biosynthesis in the lovastatin-treated G5G8(
183 t neurons, we have conditionally ablated the cholesterol biosynthesis in these neurons in mice either
184 cific effects of aging, uncovering increased cholesterol biosynthesis in type-2 pneumocytes and lipof
186 innate immunity, fatty acid biosynthesis and cholesterol biosynthesis) in separate modules identified
187 tions identified several pathways related to cholesterol biosynthesis, including cholesterol metaboli
188 in cell proliferation, immune responses, and cholesterol biosynthesis, increased infiltration of neut
189 Squalestatin (1 micromol/L), an inhibitor of cholesterol biosynthesis, increased mdr2 mRNA levels by
190 of a skin-specific regulatory mechanism for cholesterol biosynthesis, independent of cholesterol reg
191 for the most part the direct consequence of cholesterol biosynthesis inhibition and the subsequent c
192 of MG63 cells with mevinolin, a statin-type cholesterol biosynthesis inhibitor that depletes the con
195 cancer recurrence, while the use of statins, cholesterol biosynthesis inhibitors widely used for trea
197 that a steroid hormone's ability to inhibit cholesterol biosynthesis is correlated with: 1) its gene
198 In this study, we provide new evidence that cholesterol biosynthesis is important to myeloid cell gr
202 cate that PSDP, a recognized intermediate of cholesterol biosynthesis, is present in immune effector
203 p regulated pathways are involved in steroid/cholesterol biosynthesis, liver cirrhosis, and connectiv
204 to interferon or a more potent inhibitor of cholesterol biosynthesis may be required to inhibit HCV
206 ently activated T cells is necessary for the cholesterol biosynthesis metabolic gene expression progr
207 coordinated repression of genes involved in cholesterol biosynthesis, namely, HMGCR, FDFT1, SQLE, an
208 the majority, including enzymes involved in cholesterol biosynthesis, of changes were regulated in m
210 all three of these enzymes are required for cholesterol biosynthesis, only inhibition of the most up
211 EBPs, important regulators of fatty acid and cholesterol biosynthesis, operate via a post-transcripti
212 s should be considered as two key factors in cholesterol biosynthesis or metabolism disorders, where
214 ivated receptor activity, and the isoprenoid/cholesterol biosynthesis pathway additionally suggest a
215 FBXW7 knockdown induced activation of the cholesterol biosynthesis pathway and changed the prenyla
216 GCR) encodes the rate-limiting enzyme in the cholesterol biosynthesis pathway and is inhibited by sta
217 odulates RhoB activity via alteration of the cholesterol biosynthesis pathway and, consequently, of t
219 ranked the DNA replication pathway above the cholesterol biosynthesis pathway as a R273H mtp53 activa
220 results point to Th PRMT5 and its downstream cholesterol biosynthesis pathway as promising therapeuti
221 l to cholesterol is the last reaction in the cholesterol biosynthesis pathway catalyzed by the micros
222 d only intermediates, not the end product of cholesterol biosynthesis pathway for these functions.
223 risingly revealed that downregulation of the cholesterol biosynthesis pathway improves neurological p
224 n is available on the peroxisomal isoprenoid/cholesterol biosynthesis pathway in normal brain tissue
225 iets, yellow perch juveniles up-regulate the cholesterol biosynthesis pathway in order to maintain ho
226 e for one or more products of the mevalonate/cholesterol biosynthesis pathway in the progression of p
227 ndogenous role for AhR as a regulator of the cholesterol biosynthesis pathway independent of its DRE-
228 sitivity to SQLE inhibition results not from cholesterol biosynthesis pathway inhibition, but rather
230 indings suggest that the upregulation of the cholesterol biosynthesis pathway may negatively impact f
231 in vivo and highlight EBP, an enzyme in the cholesterol biosynthesis pathway that could potentially
233 clasts, inhibits a rate-limiting step in the cholesterol biosynthesis pathway, essential for osteocla
234 elta8,Delta7-isomerase), a key enzyme in the cholesterol biosynthesis pathway, which was previously i
246 g analysis showed the Complement Cascade and Cholesterol Biosynthesis Pathways as the most enriched a
247 that nuclear factor kappa B (NF-kappaB) and cholesterol biosynthesis pathways were activated, and sp
251 se proper CNS development depends on de novo cholesterol biosynthesis, peroxisomes must play a critic
253 ich mutations in enzymes catalyzing steps in cholesterol biosynthesis produce a buildup of sterol int
255 our study uncovers a master regulator of the cholesterol-biosynthesis program and an attractive targe
256 ast cancer (TNBC) exhibits a hyper-activated cholesterol-biosynthesis program that is strongly linked
257 ions as an essential activator of the entire cholesterol-biosynthesis program, dominating SREBP2 via
258 as evidenced by elevated mRNA levels of the cholesterol biosynthesis rate-limiting enzyme 3-hydroxy-
261 t, we demonstrate that progesterone inhibits cholesterol biosynthesis resulting in the accumulation o
262 ly genome lacks several enzymes required for cholesterol biosynthesis, ruling out cholesterol and cho
264 mice through repression of genes involved in cholesterol biosynthesis, such as Hmgcr, which encodes t
265 tradiol, which is a more potent inhibitor of cholesterol biosynthesis than expected based solely on h
266 or-activated receptor-alpha by precursors of cholesterol biosynthesis, that underlie common changes (
267 reases in mRNAs encoding multiple enzymes of cholesterol biosynthesis, the LDL receptor, and fatty ac
268 that SREBP-2 regulates all genes involved in cholesterol biosynthesis, the LDL receptor, and PCSK9; a
269 ucial role that lanosterol synthase plays in cholesterol biosynthesis, there is great interest in the
270 serum cholesterol through inhibiting hepatic cholesterol biosynthesis thereby upregulating the hepati
271 heterodimer partner also directly regulates cholesterol biosynthesis through inhibition of 3-hydroxy
272 d chemical probe (SH42), we inhibited distal cholesterol biosynthesis through selective inhibition of
273 ion of scavenger receptor BI, and to inhibit cholesterol biosynthesis through the direct repression o
274 d function of the PM lipid rafts: they bring cholesterol biosynthesis to completion by participating
275 novel pathway by which UV radiation acts on cholesterol biosynthesis to control Ca(2+) influx by Ora
277 a suggest that targeting beta-catenin and/or cholesterol biosynthesis, together with AKT, could have
278 xidized oxysterols are strong suppressors of cholesterol biosynthesis under specific pathological con
279 qualene epoxidase, a rate-limiting enzyme in cholesterol biosynthesis, underlies suppression in one l
281 e identify shared transcriptional changes in cholesterol biosynthesis upon loss of top-ranked genes.
283 esterol uptake, using Ldlr(-/-) cells, or of cholesterol biosynthesis, using mevastatin-treated WT ce
284 del, representing dioxin-mediated effects on cholesterol biosynthesis via the mevalonate pathway, had
287 h, triglyceride synthesis was unchanged, but cholesterol biosynthesis was reduced by 20%, and acetate
288 th defective efflux and sterol accumulation, cholesterol biosynthesis was reduced in Abcg1(-/-)/Abcg4
289 g hormone (TSH) exerts an inductor effect on cholesterol biosynthesis, we aimed to investigate the re
290 Because lathosterol is an intermediate in cholesterol biosynthesis, we conclude it is unlikely tha
291 commonly found for enzymes of post-squalene cholesterol biosynthesis, we have identified a novel ass
293 alyses revealed that the effects of ROCK2 on cholesterol biosynthesis were instead mediated via a nov
294 he variability, genes encoding regulators of cholesterol biosynthesis were reproducibly down-regulate
295 d biosynthesis of which 17 of 18 involved in cholesterol biosynthesis were significantly up regulated
297 Srebp2, the master transcription factor for cholesterol biosynthesis, which in turn transactivates N
299 ammatory circuit that links perturbations in cholesterol biosynthesis with activation of innate immun
300 hare the same Delta-14 reductase activity in cholesterol biosynthesis, yet little is known about thei