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1 rate, inhibiting CDH1 activity and promoting mitotic progression.
2 ial role in genome integrity maintenance and mitotic progression.
3 R signaling in a pathway to promote faithful mitotic progression.
4 accelerated entry into mitosis, but delayed mitotic progression.
5 modifications at Ser635 had little effect on mitotic progression.
6 r Mad2 and promotes silencing of the SAC and mitotic progression.
7 chestrates accurate chromosome alignment and mitotic progression.
8 SUN proteins in bipolar spindle assembly and mitotic progression.
9 nal activity of SRSF1 is required for normal mitotic progression.
10 d is crucial for proper spindle assembly and mitotic progression.
11 NP-T homolog, that are required for accurate mitotic progression.
12 e loading of Bub3, chromosome alignment, and mitotic progression.
13 APC(Cdc20)) plays pivotal roles in governing mitotic progression.
14 mpletely eliminated Nuf2 binding and blocked mitotic progression.
15 mposed by TIF1gamma knockdown and allows for mitotic progression.
16 genomic oxidized nucleotides with disturbed mitotic progression.
17 dle assembly, pole splitting, and a delay in mitotic progression.
18 essary for locating NIMA back to SPBs during mitotic progression.
19 80 complex formation, and adversely affected mitotic progression.
20 eostat to fine-tune Aurora B activity during mitotic progression.
21 r SMC proliferation via direct regulation of mitotic progression.
22 dissolution of sister chromatid cohesion and mitotic progression.
23 f stable KT-MT fibers (K-fibers), disrupting mitotic progression.
24 me, and the outer nuclear membrane to direct mitotic progression.
25 plicated in playing an important role during mitotic progression.
26 ncomitant increases in apoptosis and altered mitotic progression.
27 mporal regulation of miR159 by APC/C ensures mitotic progression.
28 et), a Mad2-binding protein, is required for mitotic progression.
29 f early mitotic spindle poles and the timely mitotic progression.
30 e regulation of PP2A localization for proper mitotic progression.
31 ylation of KIBRA on Ser(539) plays a role in mitotic progression.
32 omplish normal bipolar spindle formation and mitotic progression.
33 hestrated regulation is important for normal mitotic progression.
34 ation of these pathways results in defective mitotic progression.
35 r at stalled replication forks, facilitating mitotic progression.
36 res, defects in spindle assembly and blocked mitotic progression.
37 on, neither trap had a discernable effect on mitotic progression.
38 to be required in smaller amounts for normal mitotic progression.
39 he genes essential for G(1)/S transition and mitotic progression.
40 re NIMA-related kinases essential for proper mitotic progression.
41 t prolong interphase but instead interrupted mitotic progression.
42 is degraded during G(2) and mitosis to allow mitotic progression.
43 dissolution of sister chromatid cohesion and mitotic progression.
44 ation of Aurora kinase B, a key regulator of mitotic progression.
45 e exosome-independent role in cell cycle and mitotic progression.
46 ssion of the G(2)/M phase genes and impaired mitotic progression.
47 ulatory role for Chk1 phosphorylation during mitotic progression.
48 and another as a factor required for proper mitotic progression.
49 nt translation that is required for accurate mitotic progression.
50 e requirement of S326 phosphorylation during mitotic progression.
51 or NBN did not show a significant slowing of mitotic progression.
52 Both proteins are required for normal mitotic progression.
53 vates the spindle checkpoint, and delays the mitotic progression.
54 oes delay inactivation of Mad2 signaling and mitotic progression.
55 energy sensing to mitochondrial activity for mitotic progression.
56 or of spindle dynamics that is essential for mitotic progression.
57 basic cellular machinery required for robust mitotic progression.
58 rkinetochore tension at metaphase and alters mitotic progression.
59 abrogates the requirement for tankyrase 1 in mitotic progression.
60 crotubule polymerization and cause an extend mitotic progression.
61 hreonine protein kinase essential for normal mitotic progression.
62 AP2 protein level is critical for the normal mitotic progression.
63 is critical for spindle assembly and normal mitotic progression.
64 atwall have previously been shown to disrupt mitotic progression.
65 licing factors and RBPs resulted in aberrant mitotic progression.
66 me (APC/C), a ubiquitin ligase that controls mitotic progression.
67 r spindle assembly, chromosome alignment, or mitotic progression.
68 tant component of this system that regulates mitotic progression.
69 demonstrated that NHK-1 is also required for mitotic progression.
70 me (APC/C), a ubiquitin ligase essential for mitotic progression.
71 ical for G(1)/S transition and essential for mitotic progression.
72 vertebrate Plks, is essential for successful mitotic progression.
73 ulans, dynein is not apparently required for mitotic progression.
74 me (APC/C), a ubiquitin ligase that controls mitotic progression.
75 regulatory proteins to the spindle poles for mitotic progression.
76 tion of hepatocellular metaphase-to-anaphase mitotic progression.
77 , whose activity appears to be essential for mitotic progression.
78 regation relies on the precise regulation of mitotic progression.
79 is an important regulator of hepatocellular mitotic progression.
80 cilitate evasion from apoptosis and aberrant mitotic progression.
81 tion whose degradation is a prerequisite for mitotic progression.
82 hospholigand binding is necessary for proper mitotic progression.
83 that is responsive to DNA damage as well as mitotic progression.
84 ses whose combined function is important for mitotic progression.
85 esent a new signaling pathway that regulates mitotic progression.
86 tants show that both pathways are needed for mitotic progression.
87 organization, as well as in other aspects of mitotic progression.
88 chanisms that regulate Aur-A activity during mitotic progression.
89 elomere elongation, and specifically affects mitotic progression.
90 ted that overexpression of Pin2/TRF1 affects mitotic progression.
91 is known about how Pin2/TRF1 is involved in mitotic progression.
92 multisubunit ubiquitin ligase that mediates mitotic progression.
93 iferative activity due to a potent arrest of mitotic progression.
94 liated cells to promote ciliogenesis without mitotic progression.
95 hugoshins is a fundamental step in mammalian mitotic progression.
96 cells disturbs neither spindle formation nor mitotic progression.
97 s on Cdc55 and Igo2 did not cause defects in mitotic progression.
98 h we show is important for TPX2 function and mitotic progression.
99 , chromosome congression defects and delayed mitotic progression.
100 h chromatin compaction and the regulation of mitotic progression.
101 versatile ubiquitin code is read out during mitotic progression.
102 bule attachment, a condition known to arrest mitotic progression.
103 Delta plays a direct role in the control of mitotic progression.
104 misattached kinetochores to prevent further mitotic progression.
105 SET8 reaccumulation is important for normal mitotic progression.
106 tochore in activating APC/C-Cdc20 for normal mitotic progression.
107 mitotic blockers and agents that accelerate mitotic progression.
108 oss of centromeric cohesion disrupts orderly mitotic progression.
109 ase of the cell cycle, with stable arrest of mitotic progression.
110 atic cells, where DNA damage fails to affect mitotic progression.
111 ers defects in spindle assembly and prevents mitotic progression.
112 otubule spindle function, thereby inhibiting mitotic progression.
114 the yeast Ndc80 tail is required for timely mitotic progression and accurate chromosome segregation.
115 Spindle integrity is critical for efficient mitotic progression and accurate chromosome segregation.
116 -Cyclin A, Cyclin B, and Cyclin B3-influence mitotic progression and are degraded in a stereotyped se
118 applies sophisticated live imaging to assess mitotic progression and cell cycle control in these cell
126 ts by CLASP1, astrin and Kif2b is central to mitotic progression and chromosome segregation fidelity.
130 mitotic apparatus, An-Mlp1 may help monitor mitotic progression and coordinate efficient mitotic exi
132 previously underappreciated role for Ras in mitotic progression and demonstrate a pharmacologically
133 cal link between two important regulators of mitotic progression and demonstrate the critical role of
134 ssential ubiquitin protein ligase, regulates mitotic progression and exit by enhancing degradation of
137 tion mediated by NDR1 kinase is required for mitotic progression and for Sgo1 binding to mitotic cent
139 tify a common function for NudE and NudEL in mitotic progression and identify an alternative mechanis
141 aging, we show that BET inhibition prolonged mitotic progression and induced mitotic cell death, both
142 a, is a novel anticancer agent that inhibits mitotic progression and induces apoptosis in most cancer
143 oforms of cyclin E (LMW-E) overexpression on mitotic progression and its link to genomic instability
144 TM and DNA damage and is required for proper mitotic progression and maintenance of genomic stability
145 escribed mechanism for interrupting faithful mitotic progression and may ultimately inform the design
146 kinase that plays important roles in normal mitotic progression and mitotic checkpoint signaling, co
147 hat Pak1 is required for cell proliferation, mitotic progression and Plk1 activity in HeLa cells.
148 nd approximately 100 candidate regulators of mitotic progression and proliferation; the availability
149 have shown that pRB inactivation also slows mitotic progression and promotes aneuploidy, but reasons
150 central switch at kinetochores that defines mitotic progression and promotes fidelity by temporally
152 etion of Borealin by RNA interference delays mitotic progression and results in kinetochore-spindle m
153 ecies during mitosis in cancer by disturbing mitotic progression and simultaneously inhibiting the hy
155 ion of oncogenic KRAS in regulating accurate mitotic progression and suggest new avenues to therapeut
156 sults emphasize the importance of CENP-C for mitotic progression and suggest that Vmw110 may be inter
157 H2 terminus of human CENP-A is essential for mitotic progression and that localization of CENP-C, ano
158 ight the potential role of EDD in regulating mitotic progression and the cellular response to perturb
159 he fly ATR orthologue), the abnormalities of mitotic progression and the cyclin B protein level were
160 define an essential role for IKK2 in normal mitotic progression and the maintenance of spindle bipol
161 s1 is a protein kinase that regulates normal mitotic progression and the spindle checkpoint in respon
163 evel of Plk1 depletion caused a 2-h delay of mitotic progression, and a high degree of Plk1 depletion
165 localization of Bub3 was required for normal mitotic progression, and Bub3 and Cdc20 colocalized at t
166 and dynamic regulation of mitotic spindles, mitotic progression, and chromosome segregation fidelity
167 role for Pak in regulating Plk1 activity and mitotic progression, and connect Pak to the complex prot
168 -like kinase 1 (Plk1) is critical for proper mitotic progression, and its association with the centro
169 y of human AURORA-A kinase (AURKA) regulates mitotic progression, and its frequent overexpression in
170 hat Wdr62 interacts with Aurora A to control mitotic progression, and loss of these interactions lead
171 entrosomal Aurora-A kinase (AURKA) regulates mitotic progression, and overexpression and hyperactivat
172 the importance of ROS scavenging for normal mitotic progression, and provide a reference for judicio
173 ession of many late cell cycle genes, delays mitotic progression, and reduces fitness in budding yeas
175 Additionally, hBUBR1 is essential for normal mitotic progression as it prevents cells from prematurel
177 activity of Bora is also required for normal mitotic progression, as knockdown of Bora activates the
178 trate that Golgi disassembly is required for mitotic progression because failure to vesiculate the Go
179 tivating enzyme are zygotically required for mitotic progression but are dispensable for cell viabili
180 g of Golgi cisternae, vesicle tethering, and mitotic progression, but their specific functions are un
181 ears to be essential for the coordination of mitotic progression, but which also plays an unexpected
182 reticulum-localized protein FAM134A impairs mitotic progression by affecting metaphase plate alignme
183 A, cyclin B and Greatwall kinase coordinate mitotic progression by increasing levels of Cdk1-depende
184 lar mechanism by which HPV16E7 perturbs host mitotic progression by interfering Mps1-MAP4 signaling c
185 is the primary upstream kinase that directs mitotic progression by phosphorylation of a large number
186 g protein that controls spindle dynamics and mitotic progression by regulating MT depolymerases.
187 In this study, we show that USP2a mediates mitotic progression by regulating the stability of Auror
188 ome pathway ensures the unidirectionality of mitotic progression by removing cell-cycle regulators re
189 hat this physical interaction is crucial for mitotic progression by targeting polo kinase activity to
190 ured E4F(-/-) blastocysts exhibit defects in mitotic progression, chromosomal missegregation, and inc
191 These defects are associated with impaired mitotic progression coupled with abnormal mitotic spindl
192 or CaM-dependent activation cause defects in mitotic progression, cytokinesis, and ciliary resorption
193 well as wild-type siblings, indicating that mitotic progression delays alone do not alter overall gr
194 g spindle assembly renders Eg5 essential for mitotic progression, demonstrated by the lethal effects
195 ese cells initiated anaphase after a delayed mitotic progression due to the presence of unaligned chr
197 us, our data implicate mnm as a regulator of mitotic progression during the proliferative phase of ey
199 ase Cdc28 is a well established regulator of mitotic progression, evidence for a direct role in mitot
200 1 microtubule-binding domain perturbs normal mitotic progression, explaining the critical role of the
201 est for extended periods, moderate delays in mitotic progression have significant effects on the resu
202 Although these defects transiently delayed mitotic progression, HeLa cells initiated anaphase witho
203 over that Magoh deficiency delays progenitor mitotic progression in a dosage-sensitive fashion, with
204 nstrate that several fundamental features of mitotic progression in adult stem and progenitor cells a
208 ccumulation of genomic 8-oxodG and perturbed mitotic progression in cancer cells, which can be exploi
210 result in defective chromosome alignment and mitotic progression in cells using a CRISPR/Cas9-based r
211 enes are required maternally for egg laying, mitotic progression in early embryos, and embryonic surv
212 that changes in organismal physiology affect mitotic progression in germline stem and progenitor cell
214 ncoprotein E7 of HPV16 but not HPV18 retards mitotic progression in host cell by direct binding to th
216 ntent imaging to identify genes required for mitotic progression in human cancer cells and applied it
217 largely dispensable for rounding and timely mitotic progression in isolated cells, it is needed to d
218 Survivin is induced by OX40 independent of mitotic progression in late G1, and blocking Survivin su
222 nk between 3R and 4R-Tau isoform expression, mitotic progression in neuronal progenitors and post-mit
223 e conserved checkpoint kinase Chk1 regulates mitotic progression in response to DNA damage and replic
224 conserved checkpoint kinase, Chk1, regulates mitotic progression in response to DNA damage by blockin
226 anges, such as dietary intake or age, affect mitotic progression in stem and/or progenitor cells is l
230 hful inheritance of chromosomes by arresting mitotic progression in the presence of kinetochores that
231 ein phosphatases, on different parameters of mitotic progression in the presence or absence of stathm
232 to 14-3-3 may partially modulate hepatocyte mitotic progression, in association with nuclear redistr
233 c kinase responsible for multiple aspects of mitotic progression, including assembly of the outer kin
234 ation of key cell-cycle proteins involved in mitotic progression, including cyclin-dependent kinase 1
237 re linked at least in part to alterations in mitotic progression induced by defective ARF6 cycling.
238 forces ( approximately 5 nN) that accelerate mitotic progression, intermediate forces where cells res
240 dy illustrates that such an expert system of mitotic progression is able to highlight the complexity
250 s, Lte1 has dual functions for regulation of mitotic progression: it both induces mitotic exit and pr
251 elling might have important consequences for mitotic progression: it might contribute to produce stro
252 ent, blocks cell proliferation by inhibiting mitotic progression leading to mitotic and postmitotic a
253 s, uncoupling of replication initiation from mitotic progression led to altered genome ploidy in the
254 addition to the anaphase promoting complex, mitotic progression may involve another E3 ubiquitin lig
255 migration; however, more dramatic defects on mitotic progression, mitotic orientation, and mitotic ch
258 leucine zipper kinase (MELK) is critical for mitotic progression of cancer cells; however, its mechan
260 croscopy, we analyzed the dynamic process of mitotic progression of HeLa(H2B)-GFP cells lacking CENP-
266 pattern of protein dephosphorylation during mitotic progression, possibly by a drop of PP2A-B55 acti
267 (-/-) mammary mouse tumours, suggesting that mitotic progression promotes PARP-inhibitor-induced cell
268 centrations that are insufficient to inhibit mitotic progression, PTX induced both p53 and p21 causin
273 ulation, rs11556924 alters the regulation of mitotic progression resulting in an extended mitosis.
274 and loss of IRC15 function leads to delayed mitotic progression, resulting from failure to establish
275 of these cells and emphasized the timing of mitotic progression, spindle structure, and chromosome b
276 ndings reveal a role for SETD6 in regulating mitotic progression, suggesting a pathway through which
277 ive effect of PDGF in SMCs without affecting mitotic progression, suppressed neointimal formation in
278 We found that two genes responsible for mitotic progression, SWI5 and CLB2, exhibit a mitosis-de
279 fiber assembly, ch-TOG/TACC3 recruitment and mitotic progression that also resulted from Nek6 depleti
280 icient fibroblasts exhibit a marked delay in mitotic progression that can be rescued by lentiviral tr
281 an aberrant accumulation of PTTG1 disrupting mitotic progression that could contribute to thyroid car
282 ke kinases is important in the regulation of mitotic progression; this work keys on one member, namel
283 role for EGR-1 in regulating hepatocellular mitotic progression through the spindle assembly checkpo
285 hese results suggest that moderate delays in mitotic progression trigger the initiation of centriole
286 ir response to external forces are linked to mitotic progression under conditions of mechanical confi
287 ce revealed that the pathway is required for mitotic progression under normal growth conditions.
288 The spindle assembly checkpoint (SAC) delays mitotic progression until all sister chromatid pairs ach
289 served role of these checkpoints is to block mitotic progression until DNA replication and repair are
290 The spindle assembly checkpoint arrests mitotic progression until each kinetochore secures a sta
292 on fork progression was observed, but rather mitotic progression was impaired and mitotic DNA synthes
295 The spindle assembly checkpoint (SAC) delays mitotic progression when chromosomes are not properly at
296 Bub1 (KBB) pathway is required during normal mitotic progression when kinetochores are misaligned but
297 fness of the human centromere matures during mitotic progression, which leads to amplified centromere
298 kinase activity might not grossly impact on mitotic progression, while treatment with MRE11A inhibit
299 erase inhibitors by Chk1 siRNA, which showed mitotic progression with 4N DNA content leading to mitot