ライフサイエンスコーパス: orthostatic intolerance

1 Women are more susceptible to orthostatic intolerance.

2 a mechanism responsible for postspaceflight orthostatic intolerance.

3 chanism underlying individual variability in orthostatic intolerance.

4 iciency is linked to tachycardia in familial orthostatic intolerance.

5 that may contribute to, rather than offset, orthostatic intolerance.

6 ts in the treatment of patients with chronic orthostatic intolerance.

7 povolemia alone, potentially contributing to orthostatic intolerance.

8 ributes to the pathophysiologic mechanism of orthostatic intolerance.

9 underlie hyperadrenergic states that lead to orthostatic intolerance.

10 an norepinephrine transporter contributes to orthostatic intolerance.

11 d with neuropathic symptoms, mainly pain and orthostatic intolerance.

12 unrefreshing sleep, cognitive deficits, and orthostatic intolerance.

13 changes that might contribute to postflight orthostatic intolerance.

14 esents excessive orthostatic tachycardia and orthostatic intolerance.

15 are probably responsible for the symptoms of orthostatic intolerance across the menstrual cycle in wo

16 y are likely responsible for the symptoms of orthostatic intolerance across the menstrual cycle in wo

17 Orthostatic intolerance after bed rest is characterized

18 of COVID-19 (PASC) often report symptoms of orthostatic intolerance and autonomic dysfunction.

19 In a patient with orthostatic intolerance and her relatives, we measured p

20 ycardia syndrome (POTS) is a chronic form of orthostatic intolerance associated with a significant sy

21 Chronic orthostatic intolerance associated with postural tachyca

22 Starling relationship, which contributes to orthostatic intolerance by causing an excessive reductio

23 rdiovascular adaptation to bed rest leads to orthostatic intolerance, characterized by an excessive f

24 Chronic orthostatic intolerance (COI) is a debilitating autonomi

25 Chronic orthostatic intolerance (COI) occurs in postural tachyca

26 s during head-up tilt (HUT) in patients with orthostatic intolerance during daily life, and to identi

27 orthostatic tolerance during cold stress and orthostatic intolerance during heat stress.

28 by echocardiogram, weight loss > 10 pounds, orthostatic intolerance, fatigue) in combination were hi

29 Patients with idiopathic orthostatic intolerance had lower cardiac vagal barorefl

30 Patients with idiopathic orthostatic intolerance have lower cardiac vagal baroref

31 ion between the chronic fatigue syndrome and orthostatic intolerance; however, treatment with the sal

32 les or stand tests, no astronaut experienced orthostatic intolerance/hypotension during activities of

33 ure (BP) variability also is associated with orthostatic intolerance in certain patient populations a

34 the heart' is implicated in certain types of orthostatic intolerance in humans.

35 ation therapy are more effective in treating orthostatic intolerance in patients with CFS.

36 lt-table testing may be indicated to confirm orthostatic intolerance in subjects with UARS.

37 gnitive reports or physiological evidence of orthostatic intolerance in the form of either orthostati

38 HUT fails to reproduce symptoms of orthostatic intolerance in the majority of patients.

39 dia syndrome (POTS), the most common form of orthostatic intolerance in young people, affects approxi

40 Orthostatic intolerance is a syndrome characterized by l

41 Orthostatic intolerance is characterized by postural tac

42 Orthostatic intolerance is common when astronauts return

43 uced red blood cell masses, hypovolaemia and orthostatic intolerance, marked by greater cardio-accele

44 mild syndrome of orthostatic tachycardia or orthostatic intolerance may appear.

45 ia syndrome (POTS) induces disabling chronic orthostatic intolerance notable for an excessive increas

46 repeated neurocardiogenic presyncope (NCS), orthostatic intolerance occurs without persistent sympat

47 ed by tilt-table testing on 15 subjects with orthostatic intolerance (OI) and UARS, five normotensive

48 Chronic orthostatic intolerance (OI) is characterized by symptom

49 in an individual with the autonomic disorder orthostatic intolerance (OI).

50 ation of HUTT in patients with PASC revealed orthostatic intolerance on HUTT suggestive of autonomic

51 Twenty-three of the 24 had orthostatic intolerance on HUTT, with 4 demonstrating PO

52 y dysfunction, dream enactment behavior, and orthostatic intolerance or hypotension) at a protocol-sp

53 HUTT, with 4 demonstrating POTS, 15 provoked orthostatic intolerance (POI) after nitroglycerin, 3 neu

54 rapy, there were significant improvements in orthostatic intolerance ratio (33.3 [17.8-61.3] to 5.2 [

55 Orthostatic intolerance ratio correlated with autonomic

56 Autonomic p-syn subscores correlated with orthostatic intolerance ratio on tilt (rho=0.63, p=0.000

57 The orthostatic intolerance ratio was calculated by dividing

58 Patients diagnosed with idiopathic orthostatic intolerance report symptoms of lightheadedne

59 oeuvre (r=0.44, p=0.03) and patient-reported orthostatic intolerance (rho=0.57, p=0.006).

60 Peak work capacity, activity level, orthostatic intolerance, salivary cortisol, and natural

61 (P< .001), primarily due to elevation of the orthostatic intolerance, secretomotor, upper gastrointes

62 t almost all patients report severe fatigue, orthostatic intolerance, shortness of breath, and reduct

63 mptomatic patients with PASC to evaluate for orthostatic intolerance suggestive of autonomic dysfunct

64 The burden of orthostatic intolerance symptoms was assessed by the Ort

65 Young women are more susceptible to orthostatic intolerance than men, though the sex-specifi

66 tachycardia syndrome (POTS) is a disorder of orthostatic intolerance that primarily affects women of

67 lization, cardiovascular deconditioning, and orthostatic intolerance upon return to Earth.

68 ental mechanisms associated with post-flight orthostatic intolerance we investigated the interaction

69 ia syndrome (POTS) induces disabling chronic orthostatic intolerance with an excessive increase in he

70 re commonly used in the treatment of chronic orthostatic intolerance with postural tachycardia syndro

71 m onset (hazard ratio 1.67, P < 0.003); (iv) orthostatic intolerance within 1 year of symptom onset (

72 e hypothesized that patients with idiopathic orthostatic intolerance would have impaired cardiac vaga