Table 2.

Clinical, pathologic, demographic, molecular characteristics, response to therapy, and progression-free survival in the studied patients

	Clinical, Pathologic and Molecular Characteristics					Efficacy			Toxicity (grade -CTCAE)
patient	age (years)	sex	Smoking history	histology	EGFR mutation	daily dose erlotinib (line of therapy)	response (RECIST)	PFS (months)	rash	diarrhea	other
1	55	M	former (60 py)	adenocarcinoma	delE746_A750	25 mg (1st line)	PR	6	none (0)	none (0)	none
2	64	F	never	adenocarcinoma	delE746_A750	25 mg (1st line)	PR	8+	none (0)	none (0)	none
3	65	F	former (30 py)	adenocarcinoma	delL747_T751 + R776S	25 mg (1st line) ##	PR	11+	none (0)	none (0)	LFT (2)
4	46	M	former (30 py)	NSCLC, poorly differentiated	L858R	25 mg (2nd line)	SD	4	yes (1)	none (0)	none
5	67	F	current (1.5 py)	adenocarcinoma	exon 19 deletion *	25 mg (1st line)	PR	10	yes (1)	none (0)	none
6	69	F	former (0.5 py)	adenocarcinoma	exon 19 deletion *	25 mg (2nd line)	SD	17	none (0)	none (0)	none
7	86	F	former (30 py)	adenocarcinoma	L858R	25 mg # (1st line)	PR	35	none (0)	none (0)	none

EGFR, epidermal growth factor receptor; NSCLC, non-small-cell lung cancer; PFS, progression-free survival; py, pack-years; CTCAE, common terminology criteria for adverse events v3.0; M, male; F, female; RECIST, response evaluation criteria in solid tumors v1.0; PR, partial response; SD, stable disease;

⁺ongoing response; LFT, liver function test abnormalities;

^*exon 19 deletions were detected using length analysis of fluorescently labeled PCR in patients 5 and 6 and no further characterization of the mutation by sequencing was performed;

^#patient 6 had her dose of erlotinib increased to 50 mg/day after initial response to erlotinib 25 mg/day;

^##patient 3 had her dose of erlotinib reduced to 25 mg every other day after LFT abnormalities were noted. All other patients remained on erlotinib 25 mg/day until disease progression. Patients 1-4 were followed at BIDMC and patients 5-7 at MSKCC.