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. 2020 Aug 14;26(30):4428–4441. doi: 10.3748/wjg.v26.i30.4428

Table 1.

Clinical characteristics of study population

Characteristic Total (n = 303) Australia (n = 210) Oxford (n = 93)
Gender
Female, n (%) 143 (47) 95 (45) 48 (52)
Median age VDZ given (range, yr) 35 (16-84) 36 (19-78) 35 (16-84)
Median disease duration (range, yr) 6 (0.2-48) 7 (1-48) 5.4 (0.2-39.2)
Montreal classification, n (%)
Age
A1 34 (11) 33 (16) 1 (1)
A2 170 (56) 120 (57) 50 (54)
A3 99 (33) 57 (27) 42 (45)
Location
E1 18 (6) 15 (7) 3 (3)
E2 114 (38) 72 (34) 42 (45)
E3 170 (56) 122 (58) 48 (52)
Missing 1 1 0
Family History, n (%) 29 (12) 22 (15) 7 (7)
First degree 19 12 7
Second degree 10 10 0
None 212 126 86
Smoking, n
Never 226 140 86
Current 9 6 3
Ex smoker 45 41 4
Anti-TNF naïve, n (%) 182 (60) 122 (58.1) 60 (65)
Anti-TNF exposed, n (%) 121 (40) 88 (41.9) 33 (35)
Primary LOR 45 (15) 29 (13.8) 16 (17)
Secondary LOR 61 (20) 47 (22.4) 14 (15)
Side-effects 15 (5) 12 (5.7) 3 (3.2)
Steroids at VDZ initiation, n (%) 191 (63) 134 (64) 57 (61.2)
Prednisone 162 (53) 108 (51) 54 (58)
Budesonide 29 (10) 26 (12) 3 (3)
Immunomodulation at VDZ initiation, n (%) 175 (58) 135 (64) 40 (43)
AZA/6MP 136 (45) 108 (51) 28 (30)
Methotrexate 19 (6) 11 (5) 8 (9)
Tacrolimus 17 (6) 16 (8) 1 (1)
Others (Cyclo&Myco) 3 (1) 0 3 (3)
Mean Partial Mayo before VDZ initiation 5 (2-9) 6 (2-9) 5 (2-9)

VDZ: Vedolizumab; min: Minimum; max: Maximum; TNF: Tumor necrosis factor; Primary LOR: Primary loss of response; Secondary LOR: Secondary loss of response; AZA: Azathioprine; 6MP: 6-mercaptopurine; Cyclo: Ciclosporine; Myco: Mycophenolate; Init, Initiation.