Table 1.

Treatment Emergent Adverse Events with Ixekizumab and Placebo Through 24 Weeks in People with Biologic-Naïve or TNFi-Experienced Psoriatic Arthritis

Safety Outcomes at 24 Weeks33	Placebo	IXEQ4WK	IXEQ2WK	IXE Combined
	N=224	N=229	N=225	N=454
Any infection, n(%)	62 (27.7%)	77 (33.6%)	72 (32%)	149 (32.8%)
Serious infection	0	1 (0.4%)	5 (2.2%)	6 (1.3%)
Candidiasis	1 (0.4%)	4 (1.7%)	8 (3.6%)	13 (2.6%)
Esophageal candidiasis	0	0	1 (0.4%)	1 (0.2%)
Upper respiratory infection	16 (7.1%)	16 (7.0%)	15 (6.7%)	31 (6.8%)
Nasopharyngitis	9 (4.0%)	15 (6.6%)	7 (3.1%)	22 (4.8%)
Bronchitis	7 (3.1%)	4 (1.7%)	7 (3.1%)	11 (2.4%)
Sinusitis	5 (2.2%)	9 (3.9%)	6 (2.7%)	15 (3.3%)
Urinary tract infection	5 (2.2%)	8 (3.5%)	4 (1.8%)	12 (2.6%)
Cytopenia	2 (0.9%)	2 (0.9%)	4 (1.8%)	6 (1.3%)
Hepatic events	10 (4.5%)	7 (3.1%)	11 (4.9%)	18 (4.0%)
Cerebro-cardiovascular events	2 (0.9%)	0	0	0
Depression	3 (1.3%)	4 (1.7%)	4 (1.8%)	8 (1.8%)
Malignancies (excludes NMSC)	0	2 (0.9%)	0	2 (0.4%)
Injection site reactions*	10 (4.5%)	40 (17.5%)	57 (25.3%)	97 (21.4%)
Allergic or hypersensitivity reactions**	4 (1.8%)	10 (4.4%)	14 (6.2%)	24 (5.3%)

Notes: Bold font designates statistically significant differences as calculated in the primary publications: *Injection site reactions were significantly more frequent versus placebo with both ixekizumab doses in the biologic-naïve phase III trial²³ as well as the TNFi-experienced phase III trial,²² **Allergic or hypersensitivity reactions were significantly more frequent versus placebo with both ixekizumab doses in the TNFi-experienced phase III trial.²² Up to 24 weeks, there were no deaths, no occurrence of major cardiovascular adverse events, no inflammatory bowel disease, no interstitial lung disease, no pneumocystis pneumonia, and no active or latent TB.^22,23,33.

Abbreviations: TEAEs, treatment emergent adverse events; NMSC, non-melanoma skin cancer; IXE, ixekizumab; IXEQ4W/IXEQ2W, ixekizumab 80 mg every 4 or every 2 weeks; ADA, adalimumab.