ライフサイエンスコーパス: homozygous mice

1 d aberrant collagen fibers in tibiae of seal homozygous mice.

2 ed by 19% in heterozygous mice and by 69% in homozygous mice.

3 thdrawal (FPW) in wild type mice, but not in homozygous mice.

4 tion of paw withdrawal in both wild type and homozygous mice.

5 ygous mice, but had no significant effect in homozygous mice.

6 no translocation occurred in deltaF508 Cftr homozygous mice.

7 gous mice but the increase was attenuated in homozygous mice.

8 increased in Cx50D47A lenses, especially in homozygous mice.

9 sporters were not significantly decreased in homozygous mice.

10 r of wild-type mice was completely absent in homozygous mice.

11 ficant differences with Zn treatment in male homozygous mice.

12 owed that both cause edema and are lethal in homozygous mice.

13 loss of cerebellar Purkinje neurons in aged homozygous mice.

14 -BP1 and S6 in muscle and adipose tissues of homozygous mice.

15 otoacoustic emissions (SOAEs) in 70% of the homozygous mice.

16 increased in vivo thrombosis, in Pro32Pro33 homozygous mice.

17 gnificantly smaller and less frequent in the homozygous mice.

18 can be used to distinguish heterozygous from homozygous mice.

19 us with more severe deficits detected in the homozygous mice.

20 e of NDUFS4 protein in all tissues tested of homozygous mice.

21 d forkhead box A2 (Foxa2), were decreased in homozygous mice.

22 kidney (but not the brain or fibroblasts) of homozygous mice.

23 d by the early embryonic lethality of HMG-17 homozygous mice.

24 s was not affected by the lack of Arc in GFP homozygous mice.

25 nked with phenotypes of Er-heterozygous and -homozygous mice.

26 activities were significantly reduced in the homozygous mice.

27 weeks of age, the time of seizure onset for homozygous mice.

28 ance in most WT and CF heterozygous, but not homozygous mice.

29 o be essential as has been observed in ERCC1 homozygous -/- mice.

30 d (3H-U69,593) binding were abolished in the homozygous (-/-) mice.

31 ere evaluated in wild-type, heterozygous and homozygous mice 1 week following TBI.

32 Surprisingly, homozygous mice also displayed threefold enlargement by

33 Eyes of adult heterozygous and homozygous mice also were evaluated histologically.

34 cultures from adult ears and kidneys of Atm homozygous mice and found that these cultures immortaliz

35 recessive trait causing a dwarf phenotype in homozygous mice and has been mapped to the distal region

36 alters inner and outer retinal layers in cbs homozygous mice and older cbs heterozygous mice, and it

37 MYCN) extended tumor latency and survival in homozygous mice and prevented oncogenesis in hemizygous

38 l of PR mRNA in ovariectomized wild-type and homozygous mice, and a marked increase in expression aft

39 H67D homozygous mice, C294Y homozygous mice, and H67D/C294Y compound heterozygous mi

40 These changes were more severe in the homozygous mice, and were associated with decreased rod

41 In the cerebella of cdf/cdf homozygous mice, approximately 40% of Purkinje cells are

42 Nevertheless, the homozygous mice are fertile and are normal in gross appe

43 Homozygous mice are hypersusceptible to Staphylococcus a

44 Cones from PDE6alpha'DeltaC homozygous mice are less sensitive to light, and their r

45 e known expression of the VDR in fetal life, homozygous mice are phenotypically normal at birth and d

46 served in older homozygous animals, although homozygous mice are smaller than wild type littermates t

47 Homozygous mice are viable and fertile and have grossly

48 The FAT10 knockout homozygous mice are viable and fertile.

49 However, these homozygous mice are viable, but growth-retarded and infe

50 20(DeltaRRM)mice with a further reduction in homozygous (-/-) mice at only the intact myocyte level.

51 loping GI tract of Ret null heterozygous and homozygous mice at embryonic day (E)12.5 and E14.5.

52 Homozygous mice bearing mutated MyBP-C alleles are viabl

53 -V2475F mutation appears embryonic-lethal in homozygous mice, but heterozygous mice have no alteratio

54 H67D homozygous mice, C294Y homozygous mice, and H67D/C294Y c

55 in wild-type (+/+), heterozygous (+/-), and homozygous (-/-) mice carrying a null mutation of c-fos.

56 Homozygous mice carrying a null mutation for the DARPP-3

57 Remarkably, homozygous mice carrying the alphaA-R49C mutant exhibit

58 delay, and early-onset cerebellar ataxia in homozygous mice carrying the bi-allelic variant.

59 t dendrite complexity is severely reduced in homozygous mice deficient in Reelin signaling both in vi

60 Homozygous mice demonstrate variable expression of abnor

61 Although normal at birth, homozygous mice develop hindlimb paralysis from Day 13,

62 he uncharacterized L4a domain of LAMA5 where homozygous mice develop nephrotic syndrome with severe p

63 Homozygous mice (-/-) develop normally and suffer mild c

64 d onto the PL/J inbred strain, virtually all homozygous mice developed a chronic inflammatory skin di

65 JAK2V617F-homozygous mice developed a severe hematopoietic stem ce

66 ted hypertrophic cardiomyopathy (HCM), while homozygous mice developed both HCM and dilated cardiomyo

67 Homozygous mice developed severe cataracts early, and he

68 Homozygous mice die at embryonic day 14.5 in cardiac fai

69 Most homozygous mice die by 3 months.

70 Homozygous mice die in utero at embryonic days 11.5-12.5

71 As homozygous mice die in utero, we generated FADD-/- embry

72 no death in utero occurred, the majority of homozygous mice die within two weeks after birth.

73 re phenotypically normal, but 50- 85% of the homozygous (-/-) mice died in utero at embryonic day 11.

74 Most homozygous mice died during gastrulation and organogenes

75 The majority ( approximately 90%) of double-homozygous mice died during the neonatal period.

76 All the homozygous mice died perinatally.

77 Homozygous mice died within 12 h of birth.

78 Homozygous mice display defects consistent with HGPS, in

79 The Tmprss3(A306T/A306T) homozygous mice display delayed onset progressive hearin

80 Homozygous mice displayed a stem cell-intrinsic defect i

81 Lens fiber cells of alphaA-R49C homozygous mice displayed an increase in cell death by a

82 The homozygous mice displayed elevated islet hA that correla

83 n CD18 was generated by gene targeting, with homozygous mice displaying increased circulating neutrop

84 n an embryonic failure of NMJ formation, and homozygous mice do not survive postpartum.

85 Ed deleted homozygous mice (Ed-/-) have moderately reduced numbers

86 In the normal homozygous mice, electrical field stimulation caused a b

87 Unexpectedly, homozygous mice (Elovl4(del/del)) display scaly, wrinkle

88 nsive defects were found in the brain of the homozygous mice, especially in the ventral region of the

89 Pde6b(H620Q) homozygous mice exhibit a hypomorphic phenotype with par

90 Pudgy (pu) homozygous mice exhibit clear patterning defects at the

91 al and do not develop brachydactyly, whereas homozygous mice exhibit features resembling RRS.

92 RAG1-S723C homozygous mice exhibit impaired lymphocyte development

93 R249Q homozygous mice exhibited cardiac conduction abnormaliti

94 However, homozygous mice exhibited complete deafness, as well as

95 did not exhibit retinal degeneration whereas homozygous mice exhibited progressive retinal degenerati

96 Ets1(DeltaVII) homozygous mice express no p51-Ets1 and elevated levels

97 transmission were bred to homozygosity, the homozygous mice expressed no GUS enzyme activity but exp

98 e of congenital hypothyroid goiter; further, homozygous mice expressing two cog/cog alleles (linked t

99 formation and bone mass in both F508del-Cftr homozygous mice (F508del Cftr(tm1Eur)) and Cftr(+/+) lit

100 Clock homozygous mice failed to show the dramatic increase in

101 Homozygous mice for all three mutations were fetal letha

102 The supermodel mutation protected homozygous mice from high fat diet-induced obesity, like

103 Microphthalmic eyes of adult homozygous mice had a poorly developed cornea, and the a

104 Furthermore, the homozygous mice had no thyroid gland but had a normal pa

105 and cell size is also found in hypomorphic, homozygous mice harboring a single amino acid mutation (

106 Remarkably, homozygous mice harbouring the cyclin B1 mitosis degrada

107 f these viable Fli1(DeltaCTA)/Fli1(DeltaCTA) homozygous mice has reduced platelet numbers.

108 Double homozygous mice have characteristic defects of the crani

109 Affected homozygous mice have no detectable GALNS enzyme activity

110 Homozygous mice have PCD characterized by hydrocephalus,

111 zygous Fli1(DeltaCTA) mice are viable, while homozygous mice have reduced viability.

112 Homozygous mice have significantly smaller spleens and t

113 No homozygous mice however were identified at birth, consis

114 ect along the anterior-posterior axis in all homozygous mice identified.

115 stablished with wild-type, heterozygous, and homozygous mice in a Mendelian ratio.

116 R activity in the nasal airways of DeltaF508 homozygous mice in vivo.

117 The defect in tlt homozygous mice is limited to the utricle and saccule of

118 t the defect in development in CD8 transgene homozygous mice is the result of a reduction in secondar

119 However, 100% of homozygous mice lack most or all of their corpus callosu

120 c-Fos homozygous mice lack osteoclasts with a failure of the t

121 a3 gene by deletion of exon 5 and found that homozygous (-/-) mice lacked detectable mRNA on Northern

122 se oligonucleotides and in the skin of Acra7 homozygous mice lacking alpha7 nAChR channels.

123 Homozygous mice lacking D3 receptors display increased l

124 e observed alterations of eye development in homozygous mice leading to severe anatomical and morphol

125 he accumulation of H2B-GFP in the nucleus of homozygous mice led to apoptosis within 2 weeks.

126 genesis in AFB1-treated p53 heterozygous and homozygous mice not expressing HBsAg.

127 We assessed the phenotypic spectrum of homozygous mice (Nphs1(tm1Rkl)/Nphs1(tm1Rkl)) compared t

128 The number of homozygous mice observed was lower than expected under m

129 Homozygous mice of both sexes also lack preputial glands

130 as found to be concentration dependent, with homozygous mice presenting extremely high toxicity, whil

131 IL-4Ralpha-/-, beta2-microglobulin-/- double homozygous mice produced less IL-4 than did either IL-4R

132 NMJs in homozygous mice progressively degrade postnataly.

133 173Q mice were embryonic lethal, while R167Q homozygous mice (R167Q+/+) had ~5% of normal HMBS activi

134 When L9'A homozygous mice received a 10 mg/kg nicotine injection,

135 on of cartilage link protein gene (Crtl1) in homozygous mice resulted in a severe chondrodysplasia an

136 In contrast, homozygous mice (RLC-/-) had no RLC-f mRNA or protein an

137 Homozygous mice show large reductions in brain tissue mo

138 Themis(I23N) homozygous mice show reduced CD4(+) and CD8(+) T lymphoc

139 nloaded cardiomyocytes from heterozygous and homozygous mice showed reduced basal sarcomere length wi

140 Islets from RIPCre;KD-mTOR (Homozygous) mice showed reduced mTORC1 and mTORC2 signal

141 in a gene dosage-dependent fashion, with the homozygous mice showing the greatest protection.

142 ss IA Pi3k catalytic subunits; nevertheless, homozygous mice still displayed hypoglycaemia, lower ins

143 enylalanine, or succinylacetone-increased in homozygous mice, suggesting that swst mutants provide a

144 ular damage beginning at 3 weeks of age, and homozygous mice supported up to 97% parenchymal repopula

145 No homozygous mice survive postnatally.

146 Tbx5 deficiency in homozygous mice (Tbx5(del/del)) decreased expression of

147 sis of ALS and FTLD-TDP, we generated TDP-25 homozygous mice (TgTDP-25(+/+)), thereby further increas

148 roexcitatory changes were more pronounced in homozygous mice than in heterozygotes, consistent with t

149 spontaneous null allele of Ednrb results in homozygous mice that are predominantly white and die as

150 Homozygous mice that do not express K4 develop a spectru

151 uman osteocalcin promoter, were crossed with homozygous mice that express loxP-flanked Cnb1 (Cnb1(f/f

152 Med30 causing progressive cardiomyopathy in homozygous mice that, although viable during lactation,

153 In homozygous mice, the extent of anemia generally correlat

154 the most severe phenotype is observed in the homozygous mice, this model will still provide a test-be

155 therefore used the skin of heterozygous and homozygous mice to create a cDNA library, and we report

156 In contrast, EGFPf-positive DRGs from homozygous mice (TRPM8(EGFPf/EGFPf)) had drastically red

157 In these homozygous mice, we observed increased intrinsic efficac

158 for wild-type (+/+), heterozygous (+/-), and homozygous (-/-) mice were 92%, 53%, and <5%, respective

159 n or obese (gold-thioglucose [GTG]-injected) homozygous (-/-) mice were compared with lean or obese a

160 Tes wild-type (+/+), heterozygous (+/-), and homozygous (-/-) mice were divided into four groups: mic

161 The corneas of heterozygous and homozygous mice were characterized by clinical observati

162 mEC layer II neurons of heterozygous and homozygous mice were hyperexcitable and generated long-l

163 Mertk(nmf12) homozygous mice were mated to mice lacking the entire Tn

164 Accordingly, homozygous mice were more severely affected than heteroz

165 tion for the D252H mutant protein, the D252H homozygous mice were more severely affected than null ho

166 gical and developmental abnormalities, while homozygous mice were non-viable.

167 The embryonic and neonatal homozygous mice were reduced in size by approximately 25

168 In a humanized mouse model, AA homozygous mice were similarly protected against stress-

169 Compared to wild-type mice, the GNPTAB homozygous mice were smaller, had elevated levels of ser

170 The lenses of homozygous mice were the first to opacify at any given d

171 Homozygous mice were used instead of the more commonly u

172 c microvesicular steatosis in pubescent male homozygous mice, which is absent in transgenic females.

173 Homozygous mice with a null mutation in the MMP-9/gelati

174 Most importantly, chronic treatment of the homozygous mice with naltrexone did not produce the expe

175 Homozygous mice with the equivalent P465L mutation die i

176 In another mouse model using female NCr nude homozygous mice with U87 xenografts, tumor growth was si

177 2 months of age in the Alb-Cre+/-/Cprlox+/+ (homozygous) mice, with corresponding decreases in liver

178 Interestingly, while such a mutation in homozygous mice would lead to limited survival of approx