ライフサイエンスコーパス: thalassemia intermedia

1 modifying disease-associated morbidities of -thalassemia intermedia.

2 condition compared with other forms of beta thalassemia intermedia.

3 xhibited increased embryonic death and alpha-thalassemia intermedia.

4 equently evaluated in a murine model of beta-thalassemia intermedia.

5 l hemoglobinuria, beta-thalassemia major, or thalassemia intermedia.

6 lable state reported to exist in severe beta-thalassemia intermedia.

7 two individuals of Greek Cypriot origin with thalassemia intermedia.

8 mouse hereditary anemia model, Hbbth3/+ beta-thalassemia intermedia.

9 eostasis in the Hbbth3/+ mouse model of beta-thalassemia intermedia.

10 of Hbb(Th3/+) mice (Th3/+), a mouse model of thalassemia intermedia.

11 mited iron overload in a mouse model of beta-thalassemia intermedia.

12 of hepatocyte Tfrc in a mouse model of beta-thalassemia intermedia ameliorated hepcidin deficiency a

13 s for this mutation, father and son, who had thalassemia intermedia and an apparent dominant mode of

14 ad in untransfused patients affected by beta-thalassemia intermedia and Hamp modulation provides impr

15 Individuals with beta-thalassemia intermedia and hemoglobinopathies of equival

16 ot cover other hemoglobinopathies, including thalassemia intermedia and sickle cell anemia, in which

17 hydrops fetalis, hemoglobin H disease, beta-thalassemia intermedia, beta-thalassemia major/Cooley's

18 a(A)(2)) could be achieved in mice with beta-thalassemia intermedia following engraftment with bone m

19 Here we used a murine model of beta-thalassemia intermedia (Hbb(th1/th1) mice) to investigat

20 atment of mouse models of HH (Hfe(-/-)) and -thalassemia intermedia (Hbb(th3/+)) with Tmprss6 siRNA f

21 the bone marrow of animals affected by beta-thalassemia intermedia (Hbbth3/+).

22 exacerbates the phenotypic severity of beta-thalassemia intermedia in mice.

23 lso activated to reduce the severity of beta-thalassemia intermedia in the Hbbth1/th1 murine model.

24 beta-Thalassemia intermedia is a disorder characterized by in

25 rload in hereditary hemochromatosis and beta-thalassemia intermedia is caused by hepcidin deficiency.

26 liver, spleen, heart, and kidney tissues of thalassemia intermedia mice (Hbb(th3/+)).

27 In contrast, in anemic beta-thalassemia intermedia mice, there is altered progressio

28 nt but incomplete phenotypic correction in a thalassemia intermedia mouse model.

29 se studies have shown correction of the beta-thalassemia intermedia phenotype and a partial, variable

30 verload and anemia consistent with both beta-thalassemia intermedia (th3/+) and major (th3/th3).

31 pothesis, we exploited a mouse model of beta-thalassemia intermedia, Th3/(+) We observed that HO inhi

32 CD46-transgenic mice and in a mouse model of thalassemia intermedia that our in vivo approach resulte

33 ts with beta-thalassemia major (TM) and beta-thalassemia intermedia (TI) were consecutively recruited

34 emoglobin (HbF) levels and morbidity in beta-thalassemia intermedia (TI), we analyzed data from 63 un

35 of beta-thalassemia, a model for human beta-thalassemia intermedia, we previously demonstrated that

36 is greatly increased in Hbb(th3/+) mice with thalassemia intermedia, where it contributes to the supp

37 In beta-thalassemia intermedia, which does not require blood tra