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1 ulin less than 2 ng/ml (95%, euthyroid; 96%, hypothyroid).
2 unction (127 were hyperthyroid, and 168 were hypothyroid).
3 d dysfunction: 19 became hyperthyroid and 14 hypothyroid.
4 eveloped secondary leukemia and three became hypothyroid.
5 indicating that the lungs were functionally hypothyroid.
6 Peripheral tissues are also hypothyroid.
7 tal thyroidectomy and then allowed to become hypothyroid.
8 he most common persistent chronic irAEs were hypothyroid (38 [70.4%]), arthritis (18 [33.3%]), dermat
14 eptor, and affected animals are congenitally hypothyroid and profoundly deaf as a consequence when th
19 ological rat cardiac hypertrophy models with hypothyroid- and hyperthyroid-like changes in the TH tar
20 ver, deletion of SMRT in either euthyroid or hypothyroid animals had little effect on TH signaling.
21 increased SREBP-2 nuclear protein levels in hypothyroid animals results in thyroid hormone-independe
23 n was not derepressed in liver or kidneys of hypothyroid animals, our results indicated that the thyr
24 of direct cardiac effects in the genesis of hypothyroid cardiac dysfunction, the cardiac myocyte was
27 tified in the hypothyroid, mutant progeny of hypothyroid dams by tracking developmental changes in th
35 tination in normal extracts toward levels in hypothyroid extracts, which showed little E3alpha-depend
36 ion, TED duration and clinical signs between hypothyroid eye disease (Ho-TED) and hyperthyroid eye di
37 eatic islets, and that growth retardation in hypothyroid fetal sheep is associated with reductions in
41 rocytes of animals suffering from congenital hypothyroid goiter with defective thyroglobulin, GRP94 a
42 hormone) is an important cause of congenital hypothyroid goiter; further, homozygous mice expressing
44 CAL and PISA were also higher in autoimmune hypothyroid group as compared with the systemically heal
45 were significantly higher in the autoimmune hypothyroid group as compared with the systemically heal
48 severity of periodontitis in the autoimmune hypothyroid group were significantly higher compared wit
51 e and ending at the second poly(A) signal in hypothyroid hearts were 0.26 euthyroid levels (P < 0.05)
57 sults in similar shifts in cone identity and hypothyroid-like gene expression whereas reexpression of
58 downregulated in 2 hypertrophy models with a hypothyroid-like mRNA phenotype, phenylephrine in cultur
59 28.1% and 21.7%, respectively); while in the hypothyroid, low T3, and low T3T4 groups minimal change
60 ydrate intake, kidney function, arrhythmias, hypothyroid, lung disease, osteoarthritis, and rheumatoi
61 tant TSHR (Pro --> Leu at 556) in congenital hypothyroid mice activates osteoclast differentiation, c
64 deleted NCoR1 in the livers of euthyroid and hypothyroid mice and examined the effects on gene expres
65 oid stimulating hormone receptor (Tshr(-/-)) hypothyroid mice by X-ray, histology, transcriptional pr
72 owing in part to reduced food intake, these hypothyroid mice show signs of compensatory up-regulatio
74 tablished by demonstrating that treatment of hypothyroid mice with thyroxine resulted in a specific i
76 in a sequential manner in euthyroid but not hypothyroid mice, thus providing evidence that chondrocy
82 tios (IRRs) of asthma among children born to hypothyroid mothers versus children born to mothers with
86 ed developmental stage was identified in the hypothyroid, mutant progeny of hypothyroid dams by track
87 m 1 month after surgery were randomized into hypothyroid (N=9), euthyroid (N=9), and hyperthyroid (N=
88 s of term infants that weighed <2,500 g, and hypothyroid non-Hispanic white women had higher odds of
91 , and C-reactive protein (CRP) in autoimmune hypothyroid patients and systemically healthy subjects.
94 s-sectional study comprised of 65 autoimmune hypothyroid patients under treatment and 75 systemically
95 thyroid uptake was 4.2% +/- 1.8% for the 300 hypothyroid patients versus 3.8% +/- 1.6% (P = 0.12) for
96 Research Database (NHIRD) of Taiwan of which hypothyroid patients who received a diagnosis between 20
97 hole body scans (84% of euthyroid and 94% of hypothyroid patients) and stimulated thyroglobulin less
102 TSH levels in the euthyroid and subclinical hypothyroid range with incident AF was examined by using
103 high serum thyrotropin (TSH) levels (in the hypothyroid range) while in therapy with L-T4 in tablet.
105 riptional enhancement obtained in T3-treated hypothyroid rat liver (1.8-fold increase) but not in T3-
107 ride and urea transporters and aquaporins in hypothyroid rats (HT) with diminished urinary concentrat
109 muscle UCP3 levels were decreased 3-fold in hypothyroid rats and increased 6-fold in hyperthyroid ra
110 le large dose of L-triiodothyronine given to hypothyroid rats caused a 4.7-fold increase in myocardia
112 us were identical in both euthyroid rats and hypothyroid rats induced by 6-n-propyl-2-thiouracil in d
116 pituitary glands were significantly less in hypothyroid rats than the corresponding normal littermat
117 of MDA-bound proteins, hyperthyroid rats and hypothyroid rats were compared to euthyroid controls.
119 the other hand, in extracts of muscles from hypothyroid rats, where overall proteolysis is reduced b
127 cell proliferation and mass observed in the hypothyroid sheep fetus and may have consequences for pa
128 t rats were treated chemically to induce the hypothyroid state and cause a transition in the ventricu
130 cts with corepressor proteins and mimics the hypothyroid state, regardless of the circulating thyroid
132 cellular carcinoma (HCCs), suggesting that a hypothyroid status favors the onset and progression of p
134 pre-B, and B cells in the bone marrow of the hypothyroid strain of mice are significantly reduced com
135 ls is significantly reduced in the dwarf and hypothyroid strains of mice, which have defects in the p
138 PRO) questionnaire scores for the domains of hypothyroid symptoms and tiredness at 1 year (range, 0-1
140 changes in body weight, serum lipid levels, hypothyroid symptoms as measured by a HRQL questionnaire
142 den at baseline, L-thyroxine did not improve hypothyroid symptoms or tiredness compared with placebo.
143 ticipants with high symptom burden (baseline Hypothyroid Symptoms score >30 or Tiredness score >40) v
144 ferences in the mean change at 1 year in the Hypothyroid Symptoms score (0.2+/-15.3 in the placebo gr
145 two primary outcomes were the change in the Hypothyroid Symptoms score and Tiredness score on a thyr
147 mong the group with high symptom burden, the Hypothyroid Symptoms score improved similarly between th
150 in clinical presentation and the presence of hypothyroid symptoms, especially in pregnancy and in chi
153 ce appear grossly normal, however, when made hypothyroid the repression of many positively regulated
158 ased in TR-beta2-null mice to levels seen in hypothyroid wild-type mice and did not change significan
160 mental and growth delays and were profoundly hypothyroid, with no detectable thyroid hormone and elev
161 increased inflammatory markers were found in hypothyroid WT mice exposed to VILI compared with euthyr