Table 1.

Patient baseline characteristics

Characteristics	Dose-escalation cohort (n = 54)	Dose-expansion cohort (n = 99)	Total (n = 153)
Median age (range), years	51.6 (28–69)	50.2 (24–70)	NA
≤60, n (%)	45 (83.3)	80 (80.8)	125 (81.7)
>60, n (%)	9 (16.7)	19 (19.2)	28 (18.3)
Sex, n (%)
Male	21 (38.9)	49 (49.5)	70 (45.8)
Female	33 (61.1)	50 (50.5)	83 (54.2)
Tumor histology, n (%)
Squamous cell carcinoma	2 (3.7)	2 (2.0)	4 (2.6)
Adenocarcinoma	49 (90.7)	91 (91.9)	140 (91.5)
Othera	3 (5.6)	6 (6.1)	9 (5.9)
ECOG PS, n (%)
0	20 (37.0)	30 (30.3)	50 (30.7)
1	34 (63.0)	69 (69.7)	103 (67.3)
ALK rearrangement status
Positive	46 (85.2)b	91 (91.9)c	137 (89.5)
Negative	8 (14.8)	5 (5.1)	13 (8.5)
Untested	0 (0)	3(3.0)	3 (2.0)
ROS1 rearrangement status
Positive	10 (18.5)b	9 (9.1)c	19 (12.4)
Negative	23 (42.6)	38 (38.4)	61 (39.9)
Untested	21 (38.9)	52 (52.5)	73 (47.7)
CNS measurable or non-measurable metastasis
Yes	22 (40.7)	58 (58.6)	81 (52.9)
No	32 (59.3)	41 (41.4)	72 (47.1)
≥1 line of prior anti-cancer therapy	43 (79.6)	83 (83.8)	126 (82.3)
Prior ALK TKIs
ALK TKI naive	28 (51.9)	42 (42.4)	70 (45.8)
Crizotinib only	21 (38.9)	50 (50.5)	71 (46.4)
Other ALK TKI only	1 (1.9)	2 (2.0)	3 (2.0)
Both crizotinibd and other second-generation ALK TKI	4 (7.4)	5 (5.1)	9 (5.9)

ECOG Eastern Cooperative Oncology Group, PS performance status, ALK anaplastic lymphoma kinase, ROS1 c-ros oncogene 1 receptor kinase, CNS central nervous system, TKI tyrosine kinase inhibitor, NA not available

^aOthers include large cell carcinoma, adenosquamous carcinoma and other undefined pathological subtypes

^bTwo patients with both ALK and ROS1 rearrangement positive status in dose-escalation phase

^cOne patient with both ALK and ROS1 rearrangement positive status in dose-expansion phase

^dOne of the four patients received crizotinib generics