Table 1.

Intracranial effect of tyrosine kinase inhibitors ALK inhibitors and epidermal growth factor receptor (EGFR) inhibitors in trials in non-small cell lung cancer (NSCLC).

Trial	Treatment	IDCR	ICRR
ALK inhibitors
PROFILE 1014 (10)	Crizotinib	56% at 24 weeks	Not described
	PEM + CBDCA or CDDP	25% at 24 weeks	Not described
Pooled analysis of Ref. (11)	Crizotinib	56% at 12 weeks (previously untreated)	18% (previously untreated)
PROFILE 1005 (12)
PROFILE 1007 (13)
ASCEND-1 (14)	Ceritinib	65% (pretreated)	34.5%
		79% (naïve)
ASCEND-2 (15)	Ceritinib	80%	45%
ASCEND-3 (16)	Ceritinib	76.9%	61.5%
NCT01449461 (17)	Brigatinib	83% (measurable)	50%
		85% (non-measurable)	31%
NP28673 (18)	Alectinib	85.3%	58.8% (measurable)
		84.5% (pretreated)	46.4% (non-measurable)
NP28673 and NP28761 (19)	Alectinib	90.0% (measurable BM)	64.0% (measurable BM)
		85.3% (measurable and/or non-measurable BM)	42.6% (measurable and/or non-measurable BM)
			35.8% (prior RT)
			58.5% (non-prior RT)
J-ALEX (20)	Alectinib	92.9%	85.4%
ALTA (21)	Brigatinib	88% (90 mg)	36% (90 mg)
		83% (180 mg)	67% (180 mg)
NCT01970865 (22)	Lorlatinib	Not described	44% (targetable and non-targetable)
			60% (targetable)
EGFR inhibitors
Pooled analysis of published data	Erlotinib or gefitinib	75.7%	51.8%
Fan et al. (23)
Retrospective analysis	Pulsatile high-dose weekly erlotinib	Not described	67%
Grommes et al. (24)
LUX-Lung 3 and LUX-Lung 6 (25)	Afatinib	Not assessed	Not assessed
BLOOM (26)	Osimertinib	Not described	76% (33% LM improvement and 43% LM SD)
BLOOM (27)	AZD3759	Not described	52.4% (measurable)

IDCR, intracranial disease control rate; ICRR, intracranial response rate; PEM, pemetrexed; CBDCA, carboplatin; CDDP, cisplatin; BM, brain metastases; RT, radiotherapy; LM, leptomeningeal metastases; SD, stable disease.