ライフサイエンスコーパス: Norway rat

1 t and one missense mutation Ser149Ile in the Norway rat.

2 es use three species: human, house mouse, or Norway rat.

3 sory and auditory areas than the wild-caught Norway rat.

4 studied a relatively short-lived mammal: the Norway rat.

5 w pathways and produce elevated IOP in Brown Norway rats.

6 c abdominal aorta allografts from male Brown-Norway rats.

7 t autoimmune interstitial nephritis in Brown Norway rats.

8 in the liver of Fischer 344, Lewis and Brown Norway rats.

9 marrow cells into lethally irradiated Brown Norway rats.

10 N-gamma-untreated chimeras, Lewis, and Brown Norway rats.

11 number in IFN-gamma-treated Lewis and Brown Norway rats.

12 acheal blood vessels of unanesthetized brown Norway rats.

13 B breakdown in streptozotocin-diabetic Brown Norway rats.

14 ert inflammation or fibrosis) in adult Brown Norway rats.

15 diazoxide significantly lowered IOP in Brown Norway rats.

16 determined in euthanatized, pigmented Brown Norway rats.

17 aser photocoagulation of the retina in Brown-Norway rats.

18 esthetized and mechanically ventilated Brown Norway rats.

19 placed within the vitreous chamber of Brown-Norway rats.

20 leral vein, as previously described in Brown Norway rats.

21 adult (YA; 8 months) male Fischer344 x Brown Norway rats.

22 to an episcleral vein in 20 adult male Brown-Norway rats.

23 PDT was performed in 36 Brown-Norway rats 2 weeks after laser induction of CNV.

24 esent experiment, huddles composed of infant Norway rats (2- or 8-day-olds), which produce heat endog

25 cattle (174/1,156, 15%), dogs (2/212, 0.9%), Norway rats (2/318, 0.6%), farmed swine (267/648, 41.2%)

26 s and are active in a disease relevant brown Norway rat acute OVA model of Th2-driven lung inflammati

27 ae from 30 hamsters (xenografts) or 23 Brown-Norway rats (allografts) were implanted and wrapped in t

28 preservation of livers from fed donor Brown Norway rats and 67% (8/12) survivors with donor livers f

29 bdominal aorta was harvested from male Brown Norway rats and exposed to 0, 200, or 500 ng/ml of IGF-I

30 d in an experimental glaucoma model in Brown Norway rats and in a spontaneous model of glaucoma in th

31 fects from wood mice can substitute those of Norway rats and that both species contributed to negativ

32 Differences between wild Norway rats and their laboratory counterparts were first

33 Brown Norway rats are pretreated with a Lewis bone marrow infu

34 in the thoracic aorta of 36-month-old Brown Norway rats are tetraploid compared with 8% in their 3-m

35 obust retina-to-vSPVZ projection develops in Norway rats around the end of the second postnatal week

36 We therefore evaluated the Brown Norway rat as an alternative small animal model for pneu

37 Fischer-Brown Norway rats at 10 months of age were hindlimb unloaded f

38 IOP was measured in awake Brown Norway rats before surgery and every other day after sal

39 al retinal detachments were created in Brown-Norway rats by injecting 10% hyaluronic acid into the su

40 Retinal detachments were created in Brown Norway rats by injecting 10% hyaluronic acid into the su

41 IOP was raised in brown Norway rats by injecting hypertonic saline into the limb

42 IOP was raised in Brown Norway rats by injecting hypertonic saline into the limb

43 Retinal detachments were created in Brown Norway rats by injection of 1% hyaluronic acid into the

44 helium (RPE) separation was created in Brown-Norway rats by subretinal injection of 1% hyaluronic aci

45 Retinal-RPE separation was created in Brown Norway rats by subretinal injection of 1% hyaluronic aci

46 d-type C57BL mice, IL-6(-/-) mice, and Brown Norway rats by subretinal injection of 1% hyaluronic aci

47 RD was induced in adult Brown Norway rats by subretinal injection of sodium hyaluronat

48 hat an HCV-related hepacivirus discovered in Norway rats can establish high-titer hepatotropic infect

49 Heterotopic brown Norway rat cardiac isografts were removed on postoperati

50 We have established Lewis anti-Brown Norway rat CD4+ T-cell lines and confirmed their reactiv

51 performed in Lewis rat recipients from Brown-Norway rat donors.

52 Three chimeras, 3 Lewis, and 2 Brown Norway rats each received intravenous injections of gamm

53 Brown Norway rats, exhibiting substantial age-dependent lipofu

54 Norway rats express MUPs in urine but information about

55 ment organ culture and decrease IOP in Brown Norway rat eyes.

56 The laboratory Norway rat had a larger percentage of dorsolateral corte

57 The Norway rat has important impacts on our life.

58 e drug to induce a similar survival of Brown Norway rat heart allografts with an equal suppression of

59 lograft rejection, Lewis recipients of Brown Norway rat heart grafts were left untreated for the firs

60 Norway rat hepacivirus (NrHV) infection in rats shares H

61 We infected a panel of CC strains with Norway rat hepacivirus and identified several that faile

62 Norway rat hepacivirus is of particular interest, as it

63 utility for reverse genetic studies, and the Norway rat hepacivirus mouse model will facilitate studi

64 Norway rat hepacivirus, closely related to HCV, causes c

65 Lewis rats received full-mismatched Brown Norway rat hindlimb transplants.

66 ERGs were recorded from anaesthetized Brown Norway rats in response to brief full-field flashes pres

67 from all layers of the barrel field in Brown Norway rats in vivo showed that bimodal stimulation (sim

68 odenticide treatments (to control introduced Norway rats) increased Manx shearwater breeding success.

69 Young-adult male Fischer Brown Norway rats, injected with the inhibitory opsin archaerh

70 Thus, the Brown Norway rat is an appealing alternative small animal mode

71 te that the kidney of the normotensive Brown Norway rat is inherently much more susceptible to hypert

72 from both eyes of anaesthetized adult Brown-Norway rats (ketamine: xylazine: acepromazine, 55: 5: 1

73 f sensory cortex in four rodents: laboratory Norway rats (Long Evans; Rattus norvegicus), wild-caught

74 cytolysis of LT-sensitive (Fischer and Brown-Norway) rat macrophages.

75 accumulation of lipofuscin in the aged Brown Norway rat makes it a suitable small animal model for th

76 Retinal imaging was performed in 16 brown norway rats (N = 16 EYES; X = 372 G).

77 Brown Norway rats (N = 16) received unilateral episcleral vein

78 IOP was unilaterally elevated in Brown Norway rats (N = 26) by injection of hypertonic saline a

79 Brown-Norway rats (n = 30) were injected intravitreally with a

80 In Brown-Norway rats, nicotine inhibits several parameters of all

81 P was achieved manometrically in adult Brown Norway rats (nine experimental groups; n=4-7 in each; 10

82 uptake by the abdominal aorta of male Brown Norway rats occurred within 30 min.

83 rticles significantly inhibited RVP in Brown Norway rats one month after administration compared to n

84 by 24 h after sporozoite challenge in Brown Norway rats previously immunized with irradiated Plasmod

85 Elevation of IOP in Brown Norway rats produced increased expression of ET(B) recep

86 ong triplicated alpha-globin paralogs of the Norway rat (Rattus norvegicus) and the deer mouse (Perom

87 m the nest and placed in a cool environment, Norway rat (Rattus norvegicus) pups emit ultrasonic voca

88 s, 1 striped skunk (Mephitis mephitis) and 1 Norway rat (Rattus norvegicus) were seropositive for ant

89 Norway rats (Rattus norvegicus) are hosts for various mi

90 invasive species, we examined the impacts of Norway rats (Rattus norvegicus) introduced to the Aleuti

91 In contrast, infant Norway rats (Rattus norvegicus) produce heat endogenousl

92 Eleven years after invasive Norway rats (Rattus norvegicus) were eradicated from Haw

93 Norway rats (Rattus norvegicus) were introduced to the F

94 In adult Norway rats (Rattus norvegicus), which are nocturnal, th

95 (Long Evans; Rattus norvegicus), wild-caught Norway rats (Rattus norvegicus), wild-caught California

96 or component of the behavioral repertoire of Norway rats (Rattus norvegicus).

97 ar functions in other rodents, including the Norway rat, Rattus norvegicus.

98 It is descended from wild Norway rats, Rattus norvegicus, which despite their name

99 Fischer 344 x Brown Norway rats received fractionated whole-brain irradiatio

100 Brown Norway rats received intravitreal injections of azurocid

101 ere performed between Lewis donors and Brown Norway rat recipients.

102 The present study, in male Fischer Brown Norway rats, seeks to determine the location and functio

103 Two groups of Brown-Norway rats (sensitized and control) were exposed to aer

104 meras, 21 additional Lewis rats, and 6 Brown Norway rats served as controls.

105 IOP elevation in Brown Norway rats showed a trend towards decreased expression

106 EW rats that have been sensitized with Brown Norway rat skin grafts on day -7.

107 When compared with Sprague Dawley and Brown Norway rats, SS rats have lower nociceptive thresholds d

108 Further, an isolated heart model using Brown Norway rats subjected to I/R injury was utilized to eval

109 ed in each of the following tissues of Brown Norway rats: the renal cortex, renal outer medulla, live

110 s sensitive enough to be used in awake Brown Norway rats, though instrument fluctuation may limit its

111 lavian vessels was transplanted from a Brown Norway rat to a Lewis rat.

112 from Lewis rats were transplanted into Brown Norway rats to induce liver rejection in untreated recip

113 Brown Norway rat trachea were transplanted into the greater om

114 Donor allografts from Brown Norway rats treated with University of Wisconsin (UW) so

115 lantations were performed on Lewis and Brown Norway rats using a new model designed by our group.

116 PDT was performed in Brown-Norway rats using laser light at a wavelength of 689 nm,

117 Diabetes was induced in Brown Norway rats using streptozotocin, and retinal vascular p

118 s old) and middle-aged (13 months old) Brown Norway rats via Silastic implants to suppress endogenous

119 The Brown Norway rat was recently described as a bubonic plague mo

120 One eye of Brown-Norway rats was implanted with a cannula tethered to a p

121 ct of diazoxide on IOP in anesthetized Brown Norway rats was measured with a rebound tonometer.

122 ta transplantation from Dark Agouti to Brown Norway rats was performed.

123 and lateral ventricle of anaesthetized Brown-Norway rats were cannulated with fine-gauge needles conn

124 adult, middle age, and old Fischer 344 Brown Norway rats were compared.

125 However, when Lewis, Wistar Furth, or Brown Norway rats were immunized using a similar protocol, no

126 (3 mos) and aged (24 mos) Fisher 344 x Brown Norway rats were immunized with either M. vaccae or vehi

127 Donor lungs from Brown Norway rats were implanted into Lewis recipients and wer

128 To test this hypothesis, male Norway rats were inoculated with Seoul virus and regulat

129 The kidneys of Brown-Norway rats were orthotopically transplanted into bilate

130 Fourteen adult male Brown-Norway rats were studied under anesthesia (ketamine/xyla

131 Left lungs of Brown Norway rats were transplanted into four groups of Lewis

132 Kidneys from normotensive Brown Norway rats were transplanted into unilaterally nephrect

133 effects of nicotine on allergy/asthma, Brown Norway rats were treated with nicotine and sensitized an

134 Sixteen adult Brown Norway rats were-administered unilateral episcleral vein

135 allogeneic tracheal grafts (Lewis and Brown Norway rats) were harvested at 2 and 4 weeks using each

136 Experimental CNV was induced in the Brown-Norway rat with a diode laser.

137 hma, treatment of ovalbumin-challenged Brown Norway rats with 0.3 to 30 mg/kg/day of 3c gave a dose-d

138 nterventions, such as the treatment of Brown Norway rats with agents resulting in polyclonal B cell s

139 PDT was performed in monkey and Brown Norway rats with laser-induced CNV.

140 cynomolgus macaques, BALB/c mice, and brown Norway rats with LcrV-derived peptides, rV10, but not rL

141 gated the relationship between small mammal (Norway rat, wood mouse and pygmy shrew) abundance and Ma