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2 alivary glands, 0.7 Sv for kidneys, and 0.05 Sv for red marrow that are composed of 99.4% alpha, 0.5%
5 ulf Stream transports approximately 31 Sv (1 Sv = 10(6) m(3) s(-1)) of water and 1.3 x 10(15) W of he
6 ed value of up to 30 to 40 sverdrups (Sv) (1 Sv = 10(6) cubic meters per second), and it occurs mainl
7 l overturning in which about 20 sverdrups (1 Sv = 10(6) m(3) s(-1)) upwell in the Southern Ocean, wit
8 erdrups (Sv) (range: 4.0 to 34.9 Sv, where 1 Sv = a flow of ocean water of 10(6) cubic meters per sec
14 infection or IFN-alpha/beta treatment in 129 Sv/Ev and TD-derived BMDC but not in virus-infected or I
15 y comparing the pathogenesis of TR339 in 129 Sv/Ev mice and alpha/beta interferon receptor null (IFN-
18 regulation in BMDCs derived from normal 129 Sv/Ev, IFNAR1-/-, and TD mice following infection with S
22 Interestingly, I-mfa-null embryos on a 129/Sv background had no placental defect, generally survive
23 in model (Arg52Gly, Nkx2-5(+/R52G)) in a 129/Sv background was analyzed by histopathology, surface, a
27 ncy of LOH, whereas Trp53(+/-) mice on a 129/Sv or (C57BL/6 x 129/Sv) mixed background have a very lo
31 eptor heterozygous mutant mice on B6 and 129/Sv backgrounds (B6IR x 129IR) and performed a genome-wid
33 othionein (MT)-knockout (MT-KO) mice and 129/Sv wild-type (WT) controls at 4 mg/kg induced hepatic TN
35 To examine the in vivo function of APC, 129/Sv embryonic stem (ES) cells were transfected with DNA e
37 SGK1 expression is also increased in B-129/Sv-4A11(+/+) mice and paralleled increases seen for NCC.
39 under control of its native promoter (B-129/Sv-4A11(+/+)) develop hypertension (142 +/- 8 versus 113
40 ngiotensinogen are increased 2-fold in B-129/Sv-4A11(+/+), and blockade of the ANGII receptor type 1
41 ndicate that the use of mixed background 129/Sv x C57BL/6 mice to study effects of gene deletions in
44 port that mixed background p21-deficient 129/Sv x C57BL/6 mice showed increased in vitro and in vivo
45 ghly polymorphic, germ-line competent F1(129/Sv-+Tyr+p x CAST/Ei) mouse embryonic stem cell line was
48 e marrow-derived mast cells (BMMCs) from 129/Sv mice showed more robust degranulation upon the engage
52 testinal epithelium of C57Bl/6-ROSA26<-->129/Sv chimeric mice led to precocious differentiation of so
56 s in locomotion, we generated F2 hybrid (129/Sv x C57BL/6) D2 dopamine receptor (D2R)-deficient mice
57 ate in humans, and ablation of PDGF-C in 129/Sv background mice results in death during the perinatal
59 ily kinase Lyn enhanced degranulation in 129/Sv BMMCs but inhibited this response in C57BL/6 cells.
60 f Apc and Axin, and induced apoptosis in 129/Sv but not in neighboring B6-ROSA26 epithelial cells.
61 53 and p21 were significantly reduced in 129/Sv cathepsin K(-/-) OCs and forced expression of catheps
62 h high basal Fyn and Stat5 expression in 129/Sv cells, which was not reduced by TGF-beta1 treatment.
68 ce results in a milder phenotype than in 129/Sv mice, and we present a phenotypic characterization of
71 viously reported that deletion of p21 in 129/Sv x C57BL/6 mixed genetic background mice induced a sev
72 null mutant than in control mice: 11% in 129/Sv//Ev controls, 50% in GKO mice (P = 0.0002), and 33% i
74 alyzed in an intercross between the lean 129/Sv mouse strain and the obesity-prone EL/Suz mouse strai
75 alpha(E) deficiency in mice with a mixed 129/Sv x BALB/c background, but not in mice further backcros
76 suggestive evidence for additional novel 129/Sv resistance QTL on Chr 5 and 17 and susceptibility on
78 ns junctions and basolateral surfaces of 129/Sv (DeltaN89 beta-catenin) intestinal epithelial cells a
80 n contrast, on the genetic background of 129/Sv mice, the same mutation causes severe hyperinsulinemi
84 he BALB/c background, but not C57Bl/6 or 129/Sv, suggests a genetic predisposition toward mammary tum
87 coordinated control of these processes, 129/Sv embryonic stem (ES) cells, transfected with a recombi
89 tial for embryonic viability in the pure 129/Sv background but the presence of C57BL/6 alleles yields
90 ptible B6 mice for GzmB and in resistant 129/Sv mice for GzmA and/or the GzmB cluster, point to granz
94 velops, the highly nephritis-susceptible 129/Sv and DBA/1 mice exhibited significantly increased urin
95 iency of Apobec1 on the TGCT-susceptible 129/Sv inbred background to determine whether dosage of Apob
98 e male mice of the three strains tested: 129/Sv//Ev wild type, gamma interferon (IFN-gamma) knockout
101 ressed in the haploid spermatid and that 129/Sv Sprm-1(-/-) mice are subfertile when compared with wi
104 ed cathepsin K(-/-) mouse strains in the 129/Sv and C57BL/6J backgrounds and found that, only in the
105 backgrounds and found that, only in the 129/Sv background, cathepsin K(-/-) mice exhibit many charac
107 utation (Rac1Asn17) was expressed in the 129/Sv embryonic stem cell-derived component of the small in
108 taN89 beta-catenin) was expressed in the 129/Sv embryonic stem cell-derived component of the small in
109 roduced by Rac1Leu61 or Rac1Asn17 in the 129/Sv epithelium do not spread to adjacent normal C57Bl/6 e
111 f E-cadherin may have helped prevent the 129/Sv gut epithelium from undergoing neoplastic transformat
115 ically to modulate susceptibility in the 129/Sv mouse model of spontaneous TGCTs, we discovered an un
117 re hyperinsulinemia, suggesting that the 129/Sv strain harbors alleles that interact with the insulin
118 t 89% of adult alpha(E)(-/-) mice on the 129/Sv x BALB/c background developed inflammatory skin lesio
119 ely active human Rac1 (Rac1Leu61) in the 129/Sv-derived small intestinal epithelium of C57Bl/6-ROSA26
120 enotype that spontaneously occurs in the 129/Sv-SlJ strain and is characterized by small eyes that la
121 ing progeny from backcrosses between the 129/Sv-Ter/+ and MOLF/Ei strains provided modest evidence th
126 wo different mutant stat1 alleles in the 129/Sv/Ev background, we demonstrate that IFNR-dependent con
127 defensin-producing Paneth cells in their 129/Sv epithelium and also developed intestinal adenomas.
128 ration via gavage at a dose of 6 g/kg to 129/Sv mice induced hepatic TNF-alpha production in Kupffer
130 Metallothionein-knockout and wild-type 129/Sv mice were pair-fed an ethanol-containing liquid diet
131 on of the Mif gene on a segregating B6 x 129/Sv background (MIF-KO) under ad libitum (AL) feeding and
133 t IgG3-mediated protection in C57BL/6J x 129/Sv mice was associated with lower levels of IFN-gamma an
134 owever, we now report that in C57BL/6J x 129/Sv mice, IgG3 is protective while IgG1 is not protective
138 rp53(+/-) mice on a 129/Sv or (C57BL/6 x 129/Sv) mixed background have a very low frequency of mammar
139 nsfer of the NOD H2(g7) haplotype onto 129S1/Sv, 310 females were produced by NOD x (NOD x 129.H2(g7)
143 eas in the KA-sensitive strains FVB/N, 129T2 Sv/EMS, and CD-1 were significantly larger at 56 days po
145 ce (FVB/N, C3H/He, Balb/cAnN, C57BL/6, 129X1/Sv) fed for three months (eight mice per strain) the est
147 vivo insulin secretion was greatest in 129X1/Sv mice, but the counter-regulatory response to hypoglyc
150 ffectiveness of 5 revealed mean doses of 2.3 Sv for salivary glands, 0.7 Sv for kidneys, and 0.05 Sv
151 The Gulf Stream transports approximately 31 Sv (1 Sv = 10(6) m(3) s(-1)) of water and 1.3 x 10(15) W
155 rculatory diseases combined ranged from 2.5%/Sv [95% confidence interval (CI): 0.8, 4.2] for France t
159 ean doses of 2.3 Sv for salivary glands, 0.7 Sv for kidneys, and 0.05 Sv for red marrow that are comp
161 7 +/- 5.6 sverdrups (Sv) (range: 4.0 to 34.9 Sv, where 1 Sv = a flow of ocean water of 10(6) cubic me
162 ld-type and PPARalpha-null mice on either an Sv/129 or a C57BL/6N background were not markedly differ
163 and EPS enzymes was elevated in both Rv and Sv cells cultured in half-strength medium, compared to t
164 reporting through auditory feedback (Bleeper Sv; Vertec Scientific Ltd; Berkshire, UK) on patient dos
171 ce density of peripheral GBM per glomerulus [Sv(PGBM/glom)] (r = 0.50, P < 0.001) and Vv(Mes/glom) (r
175 BALB/c and C58 (the progenitor strains of LT/Sv) and crosses of these two progenitor strains and foun
176 se I arrest was investigated using strain LT/Sv and LT-related recombinant inbred strains, LTXBO and
179 that these traits are polygenic and that LT/Sv mice inherited a novel combination of permissive alle
180 Strain LT/Sv mice, and strains related to LT/Sv, produce a high percentage of atypical oocytes that a
181 were established on both a mixed 129 OlaHsd/Sv and C57BL/6 background and a pure 129 OlaHsd/Sv backg
183 An excess relative risk estimate of 10.5 per Sv (10 cases) was observed for kidney cancer; this may h
186 etermined in rough (Rv) and isogenic smooth (Sv) variants of A. actinomycetemcomitans cultured in hal
187 pressed in the zebrafish ventral subpallium (Sv, septum), and in the supra-/postcommissurally lying p
188 ntegrated value of up to 30 to 40 sverdrups (Sv) (1 Sv = 10(6) cubic meters per second), and it occur
189 erage overturning is 18.7 +/- 5.6 sverdrups (Sv) (range: 4.0 to 34.9 Sv, where 1 Sv = a flow of ocean
191 usion protein transgenic mice (C57BL/6NTac x Sv/129), and CD40L-deficient mice with spontaneous Pneum
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