Table 2.
Clinical efficacy according to F1L CDx assay and CTA results. IQR, interquartile range.
| CTA+ a | CTA+ F1L CDx evaluable | CTA+ F1L CDx unevaluable | P‐values d | ||||
|---|---|---|---|---|---|---|---|
| CTA+ F1L CDx+ | CTA+ F1L CDx− | P‐values c | Total | ||||
| Patients with an NTRK‐fp solid tumour | |||||||
| ORR (95% CI) |
57.4 (43.2–70.8) n = 54 |
72.2 (46.5–90.3) n = 18 |
55.0 (31.5–76.9) n = 20 |
0.446 |
63.2 (47.3–76.6) n = 38 |
43.8 (19.8–70.1) n = 16 |
0.24 |
| Median DoR, months (IQR) |
10.4 (5.7–15.1) n = 54 |
9.2 (5.8–12.8) n = 18 |
12.9 (6.7–14.0) n = 20 |
0.434 |
9.3 (5.7–12.9) n = 38 |
14.1 (8.9–19.2) n = 16 |
0.40 |
| Patients with ROS1‐fp NSCLC | |||||||
| ORR (95% CI) |
78.4 (64.8–88.7) n = 51 b |
72.2 (46.5–90.3) n = 18 |
72.7 (39.0–94.0) n = 11 |
1.00 |
72.4 (54.3–85.3) n = 29 |
86.4 (65.1–97.1) n = 22 |
0.31 |
| Median DoR, months (IQR) |
12.0 (5.6–17.2) n = 51 |
5.6 (3.5–11.4) n = 18 |
17.3 (13.9–18.8) n = 11 |
0.009 |
10.4 (3.7–17.2) n = 29 |
13.3 (8.5–16.4) n = 22) |
0.31 |
ORR values in the CTA+ groups were derived in the ALKA‐372‐001/STARTRK‐1/STARTRK‐2 integrated analysis (May 2018 cut‐off) [17, 20].
Two ROS1‐fp patients were removed per FDA request.
P‐values derived with Wilcoxon rank‐sum test, for comparison between F1L CDx+ and F1L CDx− groups.
P‐values derived from Fisher exact test for categorical factors between the F1L CDx evaluable set and the F1L CDx unevaluable set.