Table 2

Baseline demographics in IMvigor210 cohort after PSM (n=78). Data were analyzed by χ2 test and Wilcoxon test

VariablesFGFR3-mutated
(n=39)
FGFR3-wildtype
(n=39)
P value
Sex, n (%)0.437
Female12 (30.8)8 (20.5)
Male27 (69.2)31 (79.5)
Race, n (%)0.239
Non-white3 (7.7)0 (0.0)
White36 (92.3)39 (100.0)
Intravesical BCG use, n (%)1.000
No23 (59.0)22 (56.4)
Yes16 (41.0)17 (43.6)
Platinum-based chemotherapy use history, n (%)1.000
No9 (23.1)10 (25.6)
Yes30 (76.9)29 (74.4)
Metastatic site, n (%)0.881
Lymph node only3 (7.7)2 (5.1)
Liver9 (23.1)10 (25.6)
Visceral*27 (69.2)27 (69.2)
Baseline ECOG score, n (%)0.383
017 (43.6)20 (51.3)
121 (53.8)16 (41.0)
21 (2.6)3 (7.7)
Tobacco, n (%)0.321
Never14 (35.9)9 (23.1)
Ever25 (64.1)30 (76.9)
Tissue sampling site for sequencing, n (%)0.193
Primary tumor tissue†36 (92.3)31 (79.5)
Metasite tumor tissue‡3 (7.7)8 (20.5)
PD-L1 tumor infiltrating IC level, n (%)0.122
IC015 (38.5)10 (25.6)
IC117 (43.6)14 (35.9)
IC2+7 (17.9)15 (38.5)
TMB (mut/MB), median (IQR)7.2 (5.0–11.3)8.1 (5.0–14.9)0.258
TMB group, n (%)0.471
High (≥10)11 (28.2)15 (38.5)
Low (<10)28 (71.8)24 (61.5)
  • *Visceral metastasis was defined as lung, bone, or any non-lymph node or soft tissue metastasis.

  • †Primary tumor tissue was from bladder, kidney, or ureter.

  • ‡Metasite tumor tissue was from liver, lung, lymph node or other metastatic sites.

  • ECOG, Eastern Cooperative Oncology Group; FGFR3, fibroblast growth factor receptor 3 ; IC, immune cell; PD-L1, programmed death ligand 1; PSM, propensity score matched; TMB, tumor mutation burden.