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Table 2 Sample characteristics

From: Soluble amyloid-beta isoforms predict downstream Alzheimer’s disease pathology

Characteristic

CU

A−

A+

T−

T+

N−

N+

Number of individuals

318

60

50

52

58

67

43

Sex (% female)

50%

51.67%

48%

50%

50%

50.75%

48.84%

Age (y)

75.66 ± 5.22

75.37 ± 5.67

76.01 ± 4.67

73.87 ± 4.54

77.26 ± 5.32b***

74.46 ± 4.66

77.52 ± 5.55c**

Education (y)

15.73 ± 2.83

15.42 ± 2.68

16.1 ± 2.99

15.77 ± 2.77

15.69 ± 2.91

15.57 ± 3.1

15.98 ± 2.37

MMSE

29.08 ± 1.03

28.98 ± 1.1

29.2 ± 0.95

29.13 ± 0.93

29.03 ± 1.12

29.01 ± 1.05

29.19 ± 1.01

ADAS-Cog

6.42 ± 2.92

6.09 ± 2.91

6.81 ± 2.92

6.18 ± 2.85

6.64 ± 2.99

6.22 ± 2.69

6.73 ± 3.27

APOE ε4 carriers (%)

24.55%

11.67%

40%a***

15.38%

32.76% b*

19.40%

32.56%

  1. CU: Cognitively Unimpaired; A+: Amyloid-beta positive; A−: Amyloid-beta negative; T+: Tau positive; T−: Tau negative; N+: Neurodegeneration positive; N−: Neurodegeneration negative; y: year; MMSE: Mini-Mental State Examination; ADAS-Cog: Alzheimer’s Disease Assessment Scale-Cognitive subscale. Statistical differences for numerical characteristics were tested using t test. Statistical differences for sex and APOE status were tested using Fisher’s exact test. (*p < 0.05, **p ≤ 0.01, ***p ≤ 0.001)
  2. a significantly different from A−, b significantly different from T−, c significantly different from N−
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Cell & Bioscience

ISSN: 2045-3701

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