ライフサイエンスコーパス: ICL

1 ICL confers an increased risk of opportunistic infection

2 ICL predisposes patients to severe opportunistic infecti

3 ICL repair requires unhooking of the tethered strands by

4 ICL-1 utilizes a bioinspired endoperoxide trigger to rel

5 ICL-labeled cells disappeared from blood almost immediat

6 ICLs are produced upon irradiation under anoxic conditio

7 ICLs are thought to be processed by proteins from a vari

8 characterization of iron-caged luciferin-1 (ICL-1), a bioluminescent probe that enables longitudinal

9 emain unclear.METHODSWe hybridized 34 and 51 ICL patients' sera to a 9,000-human-proteome array and t

10 of autoantibodies from the sera of 51 adult ICL patients (out of a cohort of 72).

11 causes genetic instability without affecting ICL repair.

12 e angle narrowing was detected 1 month after ICL V4c implant, this narrowing remained stable at 3 mon

13 1 month, 3 months, 1 year, and 2 years after ICL implant.

14 95% CI, 10.1%-25.8%) at 5 and 10 years after ICL implantation, respectively.

15 pment and refractive outcomes 10 years after ICL implantation.

16 ms establishes base excision as an alternate ICL repair pathway in bacteria.

17 cterized Escherichia coli protein YcaQ as an ICL repair glycosylase that protects cells against the t

18 BRCA2 function at an ICL protects against DNA2-WRN nuclease-helicase complex

19 tivated when a replication fork stalls at an ICL(2); this triggers monoubiquitination of the ID compl

20 t NEIL3 to replication forks converged at an ICL, but the nature of DNA binding and the effect of the

21 niscent of a replication fork arrested at an ICL.

22 mutants display towards mechlorethamine, an ICL-inducing compound.

23 the structure and extent of processing of an ICL, its bypass may not absolutely require TLS polymeras

24 vivo from DNA replication fork bypass of an ICL.

25 When a replication fork collides with an ICL, it triggers a damage response that promotes multipl

26 -ZF domain on catalysis of base excision and ICL unhooking is unknown.

27 pathways (BER, MMR, NER, NHEJ, HR, TLS, and ICL repair) are specifically discussed for inhibitor dis

28 umulation of CSB at sites of monoadducts and ICLs, but it did not affect recruitment to (although sli

29 glycosylase activity against monoadducts and ICLs.

30 hooks both sides of symmetric and asymmetric ICLs in vitro, and loss or overexpression of ycaQ sensit

31 nd resection and homologous recombination at ICL damage.

32 A2 is necessary for the protection of DNA at ICLs.

33 te can unhook either or both sides of an AZB ICL, providing a basis for understanding the mechanisms

34 of the available patient information before ICL implantation.

35 recognition and the Fanconi anemia (FA)-BRCA ICL repair network.

36 siae, a vestigial FA pathway is present, but ICLs are predominantly repaired by a pathway involving t

37 FANCD2 proteins that subsequently coordinate ICL removal and repair of the ensuing DNA double-strande

38 acts, we describe here a replication-coupled ICL repair pathway that does not require incisions or FA

39 for the repair of DNA interstrand crosslink (ICL) damage.

40 s that participate in interstrand crosslink (ICL) DNA repair and MEC differentiation control.

41 DNA interstrand crosslink (ICL) repair requires a complex network of DNA damage res

42 plication-coupled DNA interstrand crosslink (ICL) repair, the XPF-ERCC1 endonuclease is required for

43 ecombination (HR) and interstrand crosslink (ICL) repair.

44 tion primarily in DNA interstrand crosslink (ICL) repair.

45 genes regulating DNA interstrand crosslink (ICL) repair.

46 itrogen mustard-based interstrand crosslink (ICL) with an 8-atom linker between the crosslinked bases

47 ancer cell line to interstrand-crosslinking (ICL) agents.

48 or the repair of DNA interstrand crosslinks (ICL) and related lesions(1).

49 been shown to unhook interstrand crosslinks (ICL) in Xenopus extracts, how NEIL3 participants in ICL

50 or the repair of DNA interstrand crosslinks (ICL), a highly toxic lesion that leads to chromosomal in

51 or the repair of DNA interstrand crosslinks (ICL).

52 on and repair of DNA interstrand crosslinks (ICL).

53 Interstrand DNA crosslinks (ICLs) are a toxic form of DNA damage that block DNA repl

54 in the repair of DNA interstrand crosslinks (ICLs) and regulates cellular responses to replication st

55 in the repair of DNA interstrand crosslinks (ICLs) are associated with the genome instability syndrom

56 DNA interstrand crosslinks (ICLs) are generated by endogenous sources and chemothera

57 Interstrand crosslinks (ICLs) are highly toxic DNA lesions that are repaired via

58 Interstrand crosslinks (ICLs) are toxic DNA lesions that cause severe genomic da

59 umor agents form DNA interstrand crosslinks (ICLs), but their clinical efficiency is counteracted by

60 osslinks, especially interstrand crosslinks (ICLs), cause cytotoxicity via blocking replication and t

61 emotherapy cause DNA interstrand crosslinks (ICLs), which covalently link both strands of the double

62 ersensitivity to DNA interstrand crosslinks (ICLs).

63 damage, specifically interstrand crosslinks (ICLs).

64 ducts and trioxsalen interstrand crosslinks (ICLs).

65 optical cavity operating with a 3.29 mum cw ICL is detailed, and a quantitative characterization of

66 gher accumulation of the extremely cytotoxic ICLs and DSBs lesions, which in turn triggers the induct

67 ted benzyl cations alkylated dG, dC, and dA, ICL assay with variation of DNA sequences showed that th

68 pon ICL induction, suggesting that defective ICL repair causes karyomegaly.

69 s (KIN), but it is unclear whether defective ICL repair is responsible or whether Fan1 nuclease activ

70 ng, differentiated state, as well as delayed ICL processing as revealed by a modified Comet assay and

71 D2, and Merit40-null cells exhibited delayed ICL unhooking coupled with reduced end resection and hom

72 cted T-lymphocyte cell line Jurkat delivered ICLs to the BM more efficiently than erythrocytes, and m

73 i and NEIL1 excise unhooked psoralen-derived ICLs in three-stranded DNA via hydrolysis of the glycosi

74 ike DNA glycosylases unhook psoralen-derived ICLs in various DNA structures via a genuine repair mech

75 ne the FA pathway signaling required for DNA ICL repair and genome stability.

76 tment of FAN1 to ICLs or for its role in DNA ICL resistance.

77 Interestingly, Merit40 mutation exacerbated ICL-induced chromosome instability in the context of con

78 ycosylase that protects its host by excising ICLs derived from azinomycin B (AZB), a potent antimicro

79 Following ICL implant, corresponding values fell to 31.2 +/- 11.5,

80 roteins act in a linear hierarchy: following ICL detection on chromatin, the FA core complex monoubiq

81 age and is most rapid and robust as follows: ICLs>DSBs>monoadducts>oxidative lesions.

82 ential use as an immunotherapeutic agent for ICL.

83 al of 107 eyes from 56 patients assessed for ICL implantation at our institution were included in the

84 ld serve to identify suitable candidates for ICL placement.

85 The SIMs of SLX4 are dispensable for ICL repair but important for processing CPT-induced repl

86 ment of Fan1 by Ub-Fancd2 is dispensable for ICL repair.

87 of a favorable architectural environment for ICL repair processing.

88 Monoubiquitination of ID is essential for ICL repair by excision, translesion synthesis and homolo

89 rug Administration's accepted guidelines for ICL sizing, clinicians should be aware of and account fo

90 o stalled replication forks is important for ICL repair.

91 and interaction with BRCA1 are important for ICL resistance when RAP80 is deficient.

92 (FA) pathway is the principal mechanism for ICL repair in metazoans and is coupled to DNA replicatio

93 itinated ID complex loses its preference for ICL and related branched DNA structures, and becomes a s

94 The Fan1 nuclease, also required for ICL repair, is recruited to ICLs by ubiquitinated (Ub) F

95 extender DNA polymerase is also required for ICL repair.

96 mice, we show that Trp53 is responsible for ICL-induced bone marrow failure and that loss of Trp53 i

97 myopic subjects consecutively scheduled for ICL implant, FDOCT (RTVue; Optovue Inc) iridocorneal ang

98 ibose (dR) and one dR groups will screen for ICLs as modified dinucleosides; the accurate mass neutra

99 Higher ICL yields were observed for compounds with OCH(3) (3b),

100 aster cross-linking reaction rate and higher ICL efficiency than the corresponding 2-nitro analogues.

101 f XPF-ERCC1, RPA and SNM1A might explain how ICL unhooking is achieved in vivo.

102 nd the immunomodulatory effects of rhIL-7 in ICL patients.

103 that a high prevalence of autoantibodies in ICL, some of which are specific for CD4+ T cells, may co

104 ining an efficient SLX4-XPF-ERCC1 complex in ICL repair.

105 constitutive factor in the SLX4 complex, in ICL repair.

106 at PTEN and FANCD2 function cooperatively in ICL repair.

107 Defects in ICL repair result in Fanconi anemia, which is characteri

108 on protein A (RPA), show profound defects in ICL repair.

109 rovide insight into the mechanism of FAN1 in ICL repair and demonstrate that the Fan1 mouse model eff

110 We also establish that PTEN function in ICL repair is dependent on its protein phosphatase activ

111 nucleases, and the DOG-1 (FANCJ) helicase in ICL resolution, influenced by the replicative-status of

112 sent a promising therapeutic intervention in ICL.

113 y or the Slx4-Slx1 nuclease also involved in ICL repair.

114 -1) and transcription-coupled (CSB-1) NER in ICL sensing were exposed.

115 Xenopus extracts, how NEIL3 participants in ICL repair in human cells and its corporation with the c

116 ceptor (TCR) signaling have been reported in ICL, but the mechanistic and causative links remain uncl

117 Cdc48/VCP segregase plays a critical role in ICL repair by unloading the CMG complex from chromatin.

118 No obvious or critical role in ICL repair was seen for non-homologous end-joining (cku-

119 BRCA1 and BRCA2 also play important roles in ICL repair.

120 gs identify a premature T-cell senescence in ICL that might be caused by chronic T-cell activation an

121 ecifically introduces negative supercoils in ICL-containing plasmids in HeLa cell extracts.

122 The increased ICL sensitivity of PTEN-deficient cells is caused, in pa

123 in human cells, and its depletion increases ICL-induced mutagenesis in human cells without altering

124 cover replication-dependent and -independent ICL repair networks, and establish nematodes as a model

125 advance our understanding of FA-independent ICL repair and establish a role for the RecQ4 helicases

126 f BRCA1, NUMB, or HES1 or chemically induced ICL damage in primary murine luminal MECs results in per

127 be recruited to localized trioxsalen-induced ICL damage in human cells, with accumulation being suppr

128 to cleave psoralen- and abasic site-induced ICLs in Xenopus egg extracts.

129 abolish interaction with RFWD3 also inhibit ICL repair, demonstrating that RPA-mediated RFWD3 recrui

130 The heat stability study of the isolated ICL products indicated that dGs were the preferred alkyl

131 rument deploys two interband cascade lasers (ICL) with center wavelengths of 4.3 and 4.4 mum.

132 using mid-infrared interband cascade lasers (ICLs) is a sensitive technique for trace gas sensing.

133 e.g., Cu(3) Sn) intermetallic coating layer (ICL) is rationally designed to stabilize Sn through a st

134 after 2 years of implantable collamer lens (ICL) V4c (STAAR Surgical AG, Nidau, Switzerland) placeme

135 Importance: Intraocular collamer lenses (ICLs) are posterior chamber phakic lenses that provide a

136 substrate containing a nitrogen mustard-like ICL two nucleotides in the duplex region because FAN1, u

137 show that FAN1 was able to degrade a linear ICL substrate.

138 Interstrand cross-link (ICL) hypersensitivity is a characteristic trait of Fanco

139 is required for DNA interstrand cross-link (ICL) repair and is thus central to the maintenance of ge

140 uring eukaryotic DNA interstrand cross-link (ICL) repair, cross-links are resolved ("unhooked") by nu

141 her constitute a DNA interstrand cross-link (ICL) repair, or the FA pathway.

142 N1's function in DNA interstrand cross-link (ICL) repair.

143 y lethal lesion are interstrand cross-links (ICL), a property exploited by several anti-cancer chemot

144 ooking highly toxic interstrand cross-links (ICLs) and bulky minor groove adducts normally recognized

145 DNA interstrand cross-links (ICLs) are a form of DNA damage that requires the interpl

146 Interstrand cross-links (ICLs) are extremely toxic DNA lesions that create an imp

147 Interstrand cross-links (ICLs) are highly cytotoxic DNA lesions that block DNA re

148 DNA interstrand cross-links (ICLs) are repaired in S phase by a complex, multistep me

149 sDNA) and unhooking interstrand cross-links (ICLs) at fork structures.

150 DNA interstrand cross-links (ICLs) block replication fork progression by inhibiting D

151 rsensitivity to DNA interstrand cross-links (ICLs) but not whole-body irradiation.

152 l for repairing DNA interstrand cross-links (ICLs), but the underlying mechanisms are unclear.

153 ity to generate DNA interstrand cross-links (ICLs), which effectively block the progression of transc

154 ively to repair DNA interstrand cross-links (ICLs).

155 d for repair of DNA interstrand cross-links (ICLs).

156 ectly producing DNA interstrand cross-links (ICLs).

157 very of fluorescent indocarbocyanine lipids (ICLs, DiR, DiD, DiI) as a model lipophilic cargo, via di

158 interaction profile near intracellular loop (ICL) 2/TM3 at the G-protein-coupling interface, suggesti

159 epducin for the beta2AR, intracellular loop (ICL)1-9, was used to decouple beta-arrestin-biased signa

160 In contrast, intracellular loops (ICLs) and C-terminalresidues exited the ribosome into a

161 lalanine (azF) into the intracellular loops (ICLs) and the C-tail of AT1R.

162 e of the glyoxylate shunt, isocitrate lyase (ICL), may mediate survival of Mtb during the acute and c

163 Isocitrate lyase (ICL, types 1 and 2) is the first enzyme of the glyoxylat

164 Idiopathic CD4+ T cell lymphocytopenia (ICL) is a heterogeneous syndrome presenting with persist

165 Idiopathic CD4 lymphopenia (ICL) is a rare syndrome defined by low CD4 T-cell counts

166 BACKGROUNDIdiopathic CD4 lymphopenia (ICL) is defined by persistently low CD4+ cell counts (<3

167 and general utility of glycosylase-mediated ICL repair in other bacteria are unknown.

168 In bacteria, glycosylase-mediated ICL unhooking was described in Streptomyces as a means o

169 4 (RECQL4), as a component of Pso2-mediated ICL repair.

170 Comparison of YcaQ and UvrA-mediated ICL resistance mechanisms establishes base excision as a

171 78 patients undergoing consecutive V4 model ICL implantations, which took place from January 1, 1998

172 enses implanted were as follows: 53 V4 model ICLs of -15.5 D or greater, 73 V4 model ICLs of less tha

173 odel ICLs of -15.5 D or greater, 73 V4 model ICLs of less than -15.5 diopter (D), and 7 V4 model tori

174 d a panel of model unhooked nitrogen mustard ICLs to systematically investigate how the state of an u

175 We observed ICL-induced chromosomal breakage in 9 of 17 (53%) HNSCC

176 Approximately 30% of ICL patients develop autoimmune disease.

177 Application of ICL-1 in a model of systemic bacterial infection reveals

178 to be an important long-term complication of ICL implantation.

179 d in the defective hematopoietic function of ICL-repair deficient myeloid progenitors.

180 oxylate levels using a chemical inhibitor of ICL restored growth of MS-deficient Mtb, despite inhibit

181 Following systemic injection of ICL-labeled cells in immunodeficient or immunocompetent

182 ase, or "unhook", ICLs, but the mechanism of ICL unhooking remains largely unknown.

183 Moreover, compensatory mechanisms of ICL resistance when FANCJ is deficient have not been exp

184 ir potential contribution to pathogenesis of ICL remain unclear.METHODSWe hybridized 34 and 51 ICL pa

185 The pathogenesis of ICL remains unclear, and whether effector sites are also

186 tion and represents the preferred pathway of ICL repair in a vertebrate cell-free system.

187 The Fanconi anaemia pathway of ICL repair is activated when a replication fork stalls a

188 of NER and DSB/R (P <0022), similar rates of ICL/R, and more condensed chromatin structure compared w

189 rates of NER and DSB/R, comparable rates of ICL/R, more condensed chromatin structure, and higher se

190 d toxic joint DNA molecules during repair of ICL-induced DNA damage.

191 Deep sequencing of ICL repair products showed that the approach and extensi

192 o report that unloading of RPA from sites of ICL induction is perturbed in RFWD3-deficient cells.

193 eby preventing RFWD3 recruitment to sites of ICL-induced replication fork stalling.

194 implicate MERIT40 in the earliest stages of ICL repair and define specific functional interactions b

195 shown to be necessary in the early steps of ICL repair to prevent aberrant nuclease resection, the r

196 pathways; however, a clear understanding of ICL recognition and repair processing in human cells is

197 lication forks stall, even in the absence of ICLs.

198 roduce metabolites that promote formation of ICLs leading to inhibition of trypanosomal growth.

199 ors that protect against the genotoxicity of ICLs generated by trioxsalen/ultraviolet A (TMP/UVA) dur

200 Most measurements of ICLs lack sensitivity and structural information.

201 Repair of ICLs requires sequential incisions, translesion DNA synt

202 ng the mechanisms of base excision repair of ICLs.

203 ecruitment, CSA itself localized at sites of ICLs, DSBs and monoadducts but not at oxidative lesions.

204 onitored protein assembly and disassembly on ICL-containing chromatin.

205 d disease; it also brings a renewed focus on ICL that will likely result in improved diagnostic evalu

206 ation of the classical complement pathway on ICL CD4+ T cells.RESULTSAll ICL patients had a multitude

207 , HMGB1 functions in association with XPA on ICLs and facilitates the formation of a favorable archit

208 vault height (distance between the posterior ICL surface and anterior lens surface) measured a mean (

209 Thus, Fan1 nuclease activity promotes ICL repair in a manner that controls ploidy, a role that

210 in principle explain how Ub-Fancd2 promotes ICL repair, but we show that recruitment of Fan1 by Ub-F

211 ) protein bound to triplex-directed psoralen ICLs (TFO-ICLs) in vitro, cooperatively with NER damage

212 with both NEIL3 and FA pathways in psoralen-ICL repair, suggesting that TRAIP may function upstream

213 unction within the NEIL3 pathway in psoralen-ICL repair.

214 /BRCA pathways are non-epistatic in psoralen-ICL repair.

215 hway is the major pathway to repair psoralen-ICL through a unique DSB-free mechanism in human cells.

216 is the major pathway for repairing psoralen-ICL, and the FA/BRCA pathway is only activated when NEIL

217 hanistically, NEIL3 is recruited to psoralen-ICL in a rapid, PARP-dependent manner.

218 ortantly, the NEIL3 pathway repairs psoralen-ICLs without generating double-strand breaks (DSBs), unl

219 We report the synthesis of a putative ICL repair intermediate that mimics the complete process

220 g on the altered protein's ability to repair ICL damage.

221 epair (NER), interstrand cross-links repair (ICL/R), double-strand breaks repair (DSB/R), and chromat

222 TbSNM1, a nuclease that specifically repairs ICLs, are hypersensitive to most ABQ prodrugs, a phenoty

223 ement pathway on ICL CD4+ T cells.RESULTSAll ICL patients had a multitude of autoantibodies mostly di

224 makes identical strong bonds with these same ICLs.

225 activity, caused by elongation of the short ICL-unhooked oligonucleotide (a six-mer in our study) by

226 itro from Jurkat cells resulted in a similar ICL delivery as the injection of intact Jurkat cells.

227 that while purified XPF-ERCC1 incises simple ICL-containing model replication fork structures, the pr

228 oking mechanism for psoralen and abasic site ICLs.

229 The low activity of the Cu-Sn ICL against lithiation/delithiation enables the gradual

230 a result, the Sn anode enhanced by the Cu-Sn ICL shows a significant improvement in cycling stability

231 tion of the metallic Cu phase from the Cu-Sn ICL, which provides a regulatable and appropriate distri

232 on nuclease activity through a site-specific ICL in vitro We noted that stimulation of Pso2 nuclease

233 Here, we use repair of a site-specific ICL in Xenopus egg extracts to study the mechanism of le

234 fore, NBD2 might be critical for stabilizing ICLs 2 and 3 that form a tetrahelix bundle at the NBD2 i

235 tcomes of toric implantable collamer lens (T-ICL) with toric Artiflex (T-Artiflex) lenses.

236 endothelial loss of 2.18% and 1.95% in the T-ICL and T-Artiflex groups, respectively.

237 f success as large as 0.25 +/- 0.22 in the T-ICL group and 0.24 +/- 0.15 in the T-Artiflex group.

238 safety index was mean 1.40 +/- 0.70 in the T-ICL group and 1.20 +/- 0.21 in the T-Artiflex group.

239 A total of 39 eyes (95%) in the T-ICL group and 41 eyes (100%) in the T-Artiflex group wer

240 study compared 82 eyes of 41 patients with T-ICL lenses in one eye and toric Artiflex implantation in

241 bound to triplex-directed psoralen ICLs (TFO-ICLs) in vitro, cooperatively with NER damage recognitio

242 ons and facilitated error-free repair of TFO-ICLs in mouse fibroblasts.

243 re, we demonstrate that HMGB1 recognizes TFO-ICLs in human cells, and its depletion increases ICL-ind

244 ospective single center study indicates that ICL implantation provides good long-term safety and stab

245 Our results show that ICL repair and replication termination both utilize a si

246 focal microscopy of intact BM confirmed that ICLs are delivered independently of the injected cells.

247 P residue was faithfully inserted across the ICL-G by Pol eta, Pol zeta, and Rev1-Pol zeta.

248 eta stalled just after insertion across the ICL.

249 icient human cells significantly altered the ICL-induced mutation spectrum from predominantly T-->A t

250 alone showed a tendency to stall before the ICL, whereas Pol eta stalled just after insertion across

251 cised the substrate predominantly beyond the ICL and, therefore, failed to release the 5' flap.

252 nick, NEIL3 targets both DNA strands in the ICL without generating single-strand breaks.

253 Instead, the ICL is unhooked when one of the two N-glycosyl bonds for

254 n fatty acids accumulated high levels of the ICL aldehyde endproduct, glyoxylate, and increased level

255 l of these pathways require unhooking of the ICL from one strand of a DNA duplex by nucleases, follow

256 Removal of the ICL lesions is vital, as they are physical barriers to e

257 versal, are not an integral component of the ICL repair, pointing to a different mechanism of fork pr

258 e strand of the duplex on either side of the ICL.

259 The stalling of Pol eta directly past the ICL is attributed to its autoinhibitory activity, caused

260 stalling by Rev1-Pol zeta directly past the ICL was observed, suggesting that the proposed function

261 ing strand of a replication fork strikes the ICL Here, we report that while purified XPF-ERCC1 incise

262 h variation of DNA sequences showed that the ICL reaction occurred with opposing dG/dC but not with s

263 rticle particle formation was not due to the ICL labeling or complement attack and was observed after

264 ver, the recruitment of XPA and HMGB1 to the ICLs is co-dependent.

265 Inefficient repair of these ICL can lead to leukemia and bone marrow failure.

266 of the non-ubiquitinated ID complex bound to ICL DNA-which we also report here-we show that monoubiqu

267 -associated nuclease 1 (FAN1) contributes to ICL repair, FAN1 mutations predispose to karyomegalic in

268 e mutagenic DNA repair following exposure to ICL-inducing agents.

269 MERIT40 was rapidly recruited to ICL lesions prior to FANCD2, and Merit40-null cells exhi

270 In response to ICL V4c implant, considerable angle narrowing was detect

271 arrying BRCA2 DBD mutations are sensitive to ICL-inducing agents but resistant to HU treatment consis

272 for the initial rapid recruitment of FAN1 to ICLs or for its role in DNA ICL resistance.

273 is central to the pathway, and localizes to ICLs dependent on its monoubiquitination.

274 lso required for ICL repair, is recruited to ICLs by ubiquitinated (Ub) Fancd2.

275 ed for cellular and organismal resistance to ICLs.

276 than -15.5 diopter (D), and 7 V4 model toric ICLs for myopia.

277 This ability of FAN1 to traverse ICLs in DNA could help to elucidate its biological funct

278 ordinates multiple endonucleases that unhook ICLs, resolve homologous recombination intermediates, an

279 for the incisions that release, or "unhook", ICLs, but the mechanism of ICL unhooking remains largely

280 lly investigate how the state of an unhooked ICL affects pol eta activity.

281 length of the duplex surrounding an unhooked ICL critically affects polymerase efficiency.

282 imics the complete processing of an unhooked ICL to a single crosslinked nucleotide, and find that it

283 ucleases, followed by bypass of the unhooked ICL by translesion synthesis (TLS) polymerases.

284 n intermediates, and perhaps remove unhooked ICLs.

285 The structures of the unhooked ICLs remain unknown, yet the position of incisions and p

286 of incisions and processing of the unhooked ICLs significantly influence the efficiency and fidelity

287 Unrepaired ICL damage results in aberrant transdifferentiation to a

288 from Fan1(nd/nd) mice become polyploid upon ICL induction, suggesting that defective ICL repair caus

289 In vertebrates, ICL repair is triggered when replication forks collide w

290 Visian ICL implantation improves visual function in special nee

291 achieved by sulcus implantation of a Visian ICL (STAAR Surgical, Monrovia, California, USA) under ge

292 unilateral intraocular collamer lens (Visian ICL) implantation for moderate to high myopia.

293 However, between 5 and 10% of BM cells were ICL-positive.

294 Treatment of Fan1-deficient mice with ICL-inducing agents results in pronounced thymic and bon

295 mucosal biopsy specimens from patients with ICL and healthy controls were evaluated.

296 uman IL-7 (rhIL-7) per week in patients with ICL who were at risk of disease progression.

297 These data suggest that patients with ICL, despite gut mucosal lymphopenia and local tissue in

298 vated in the colonic mucosa of patients with ICL.

299 was preserved in the mucosa of patients with ICL.

300 depletion sensitized cells to treatment with ICL-inducing agents and led to accumulation of cells in